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Wikipedia

Ketogenic diet

February 15, 2024

This article is about a dietary therapy for epilepsy. For information on ketogenic diets as a lifestyle choice or for weight loss, see Very low-carbohydrate ketogenic diet.

The ketogenic diet is a high-fat, adequate-protein, low-carbohydrate dietary therapy that in conventional medicine is used mainly to treat hard-to-control (refractory) epilepsy in children. The diet forces the body to burn fats rather than carbohydrates.

Testing for ketone bodies in urine

Normally, carbohydrates in food are converted into glucose, which is then transported around the body and is important in fueling brain function. However, if only a little carbohydrate remains in the diet, the liver converts fat into fatty acids and ketone bodies, the latter passing into the brain and replacing glucose as an energy source. An elevated level of ketone bodies in the blood (a state called ketosis) eventually lowers the frequency of epileptic seizures.[1] Around half of children and young people with epilepsy who have tried some form of this diet saw the number of seizures drop by at least half, and the effect persists after discontinuing the diet.[2] Some evidence shows that adults with epilepsy may benefit from the diet and that a less strict regimen, such as a modified Atkins diet, is similarly effective.[1] Side effects may include constipation, high cholesterol, growth slowing, acidosis, and kidney stones.[3]

The original therapeutic diet for paediatric epilepsy provides just enough protein for body growth and repair, and sufficient calories[Note 1] to maintain the correct weight for age and height. The classic therapeutic ketogenic diet was developed for treatment of paediatric epilepsy in the 1920s and was widely used into the next decade, but its popularity waned with the introduction of effective anticonvulsant medications. This classic ketogenic diet contains a 4:1 ketogenic ratio or ratio by weight of fat to combined protein and carbohydrate. This is achieved by excluding high-carbohydrate foods such as starchy fruits and vegetables, bread, pasta, grains, and sugar, while increasing the consumption of foods high in fat such as nuts, cream, and butter.[1] Most dietary fat is made of molecules called long-chain triglycerides (LCTs). However, medium-chain triglycerides (MCTs)—made from fatty acids with shorter carbon chains than LCTs—are more ketogenic. A variant of the classic diet known as the MCT ketogenic diet uses a form of coconut oil, which is rich in MCTs, to provide around half the calories. As less overall fat is needed in this variant of the diet, a greater proportion of carbohydrate and protein can be consumed, allowing a greater variety of food choices.[4][5]

In 1994, Hollywood producer Jim Abrahams, whose son's severe epilepsy was effectively controlled by the diet, created the Charlie Foundation for Ketogenic Therapies to further promote diet therapy. Publicity included an appearance on NBC's Dateline program and ...First Do No Harm (1997), a made-for-television film starring Meryl Streep. The foundation sponsored a research study, the results of which—announced in 1996—marked the beginning of renewed scientific interest in the diet.[1]

Possible therapeutic uses for the ketogenic diet have been studied for many additional neurological disorders, some of which include: Alzheimer's disease, amyotrophic lateral sclerosis, headache, neurotrauma, pain, Parkinson's disease, and sleep disorders.[6]

Epilepsy

Epilepsy is one of the most common neurological disorders after migraine and stroke,[7] affecting around 50 million people worldwide.[8] It is diagnosed in a person having recurrent, unprovoked seizures. These occur when cortical neurons fire excessively, hypersynchronously, or both, leading to temporary disruption of normal brain function. This might affect, for example, the muscles, the senses, consciousness, or a combination. A seizure can be focal (confined to a specific part of the brain) or generalised (spread widely throughout the brain and leading to a loss of consciousness). Epilepsy can occur for a variety of reasons; some forms have been classified into epileptic syndromes, most of which begin in childhood. Epilepsy is considered refractory (not yielding to treatment) when two or three anticonvulsant drugs have failed to control it. About 60% of patients achieve control of their epilepsy with the first drug they use, whereas around 30% do not achieve control with drugs. When drugs fail, other options include epilepsy surgery, vagus nerve stimulation, and the ketogenic diet.[7]

History

The ketogenic diet is a mainstream medical dietary therapy that was developed to reproduce the success and remove the limitations of the non-mainstream use of fasting to treat epilepsy.[Note 2] Although popular in the 1920s and '30s, it was largely abandoned in favour of new anticonvulsant drugs.[1] Most individuals with epilepsy can successfully control their seizures with medication. However, 25–30% fail to achieve such control despite trying a number of different drugs.[9] For this group, and for children in particular, the diet has once again found a role in epilepsy management.[1][10]

Fasting

 
A news report of Dr Hugh Conklin's "water diet" treatment from 1922

Physicians of ancient Greece treated diseases, including epilepsy, by altering their patients' diet. An early treatise in the Hippocratic Corpus, On the Sacred Disease, covers the disease; it dates from c. 400 BC. Its author argued against the prevailing view that epilepsy was supernatural in origin and cure, and proposed that dietary therapy had a rational and physical basis.[Note 3] In the same collection, the author of Epidemics describes the case of a man whose epilepsy is cured as quickly as it had appeared, through complete abstinence of food and drink.[Note 4] The royal physician Erasistratus declared, "One inclining to epilepsy should be made to fast without mercy and be put on short rations."[Note 5] Galen believed an "attenuating diet"[Note 6] might afford a cure in mild cases and be helpful in others.[11]

The first modern study of fasting as a treatment for epilepsy was in France in 1911.[12] Twenty epilepsy patients of all ages were "detoxified" by consuming a low-calorie vegetarian diet, combined with periods of fasting and purging. Two benefited enormously, but most failed to maintain compliance with the imposed restrictions. The diet improved the patients' mental capabilities, in contrast to their medication, potassium bromide, which dulled the mind.[13]

Around this time, Bernarr Macfadden, an American exponent of physical culture, popularised the use of fasting to restore health. His disciple, the osteopathic physician Dr. Hugh William Conklin of Battle Creek, Michigan, began to treat his epilepsy patients by recommending fasting. Conklin conjectured that epileptic seizures were caused when a toxin, secreted from the Peyer's patches in the intestines, was discharged into the bloodstream. He recommended a fast lasting 18 to 25 days to allow this toxin to dissipate. Conklin probably treated hundreds of epilepsy patients with his "water diet" and boasted of a 90% cure rate in children, falling to 50% in adults. Later analysis of Conklin's case records showed 20% of his patients achieved freedom from seizures and 50% had some improvement.[10]

Conklin's fasting therapy was adopted by neurologists in mainstream practice. In 1916, a Dr McMurray wrote to the New York Medical Journal claiming to have successfully treated epilepsy patients with a fast, followed by a starch- and sugar-free diet, since 1912. In 1921, prominent endocrinologist Henry Rawle Geyelin reported his experiences to the American Medical Association convention. He had seen Conklin's success first-hand and had attempted to reproduce the results in 36 of his own patients. He achieved similar results despite having studied the patients for only a short time. Further studies in the 1920s indicated that seizures generally returned after the fast. Charles P. Howland, the parent of one of Conklin's successful patients and a wealthy New York corporate lawyer, gave his brother John Elias Howland a gift of $5,000 to study "the ketosis of starvation". As professor of paediatrics at Johns Hopkins Hospital, John E. Howland used the money to fund research undertaken by neurologist Stanley Cobb and his assistant William G. Lennox.[10]

Diet

In 1921, Rollin Turner Woodyatt reviewed the research on diet and diabetes. He reported that three water-soluble compounds, β-hydroxybutyrate, acetoacetate, and acetone (known collectively as ketone bodies), were produced by the liver in otherwise healthy people when they were starved or if they consumed a very low-carbohydrate, high-fat diet.[10] Dr. Russell Morse Wilder, at the Mayo Clinic, built on this research and coined the term "ketogenic diet" to describe a diet that produced a high level of ketone bodies in the blood (ketonemia) through an excess of fat and lack of carbohydrate. Wilder hoped to obtain the benefits of fasting in a dietary therapy that could be maintained indefinitely. His trial on a few epilepsy patients in 1921 was the first use of the ketogenic diet as a treatment for epilepsy.[10]

Wilder's colleague, paediatrician Mynie Gustav Peterman, later formulated the classic diet, with a ratio of one gram of protein per kilogram of body weight in children, 10–15 g of carbohydrate per day, and the remainder of calories from fat. Peterman's work in the 1920s established the techniques for induction and maintenance of the diet. Peterman documented positive effects (improved alertness, behaviour, and sleep) and adverse effects (nausea and vomiting due to excess ketosis). The diet proved to be very successful in children: Peterman reported in 1925 that 95% of 37 young patients had improved seizure control on the diet and 60% became seizure-free. By 1930, the diet had also been studied in 100 teenagers and adults. Clifford Joseph Barborka Sr., also from the Mayo Clinic, reported that 56% of those older patients improved on the diet and 12% became seizure-free. Although the adult results are similar to modern studies of children, they did not compare as well to contemporary studies. Barborka concluded that adults were least likely to benefit from the diet, and the use of the ketogenic diet in adults was not studied again until 1999.[10][14]

Anticonvulsants and decline

During the 1920s and 1930s, when the only anticonvulsant drugs were the sedative bromides (discovered 1857) and phenobarbital (1912), the ketogenic diet was widely used and studied. This changed in 1938 when H. Houston Merritt Jr. and Tracy Putnam discovered phenytoin (Dilantin), and the focus of research shifted to discovering new drugs. With the introduction of sodium valproate in the 1970s, drugs were available to neurologists that were effective across a broad range of epileptic syndromes and seizure types. The use of the ketogenic diet, by this time, restricted to difficult cases such as Lennox–Gastaut syndrome, declined further.[10]

MCT diet

 
Medium-chain triglyceride (MCT) oil emulsion

In the 1960s, medium-chain triglycerides (MCTs) were found to produce more ketone bodies per unit of energy than normal dietary fats (which are mostly long-chain triglycerides).[15] MCTs are more efficiently absorbed and are rapidly transported to the liver via the hepatic portal system rather than the lymphatic system.[16] The severe carbohydrate restrictions of the classic ketogenic diet made it difficult for parents to produce palatable meals that their children would tolerate. In 1971, Peter Huttenlocher devised a ketogenic diet where about 60% of the calories came from the MCT oil, and this allowed more protein and up to three times as much carbohydrate as the classic ketogenic diet. The oil was mixed with at least twice its volume of skimmed milk, chilled, and sipped during the meal or incorporated into food. He tested it on 12 children and adolescents with intractable seizures. Most children improved in both seizure control and alertness, results that were similar to the classic ketogenic diet. Gastrointestinal upset was a problem, which led one patient to abandon the diet, but meals were easier to prepare and better accepted by the children.[15] The MCT diet replaced the classic ketogenic diet in many hospitals, though some devised diets that were a combination of the two.[10]

Revival

The ketogenic diet achieved national media exposure in the US in October 1994, when NBC's Dateline television programme reported the case of Charlie Abrahams, son of Hollywood producer Jim Abrahams. The two-year-old had epilepsy that had remained uncontrolled by mainstream and alternative therapies. Abrahams discovered a reference to the ketogenic diet in an epilepsy guide for parents and brought Charlie to John M. Freeman at Johns Hopkins Hospital, which had continued to offer the therapy. Under the diet, Charlie's epilepsy was rapidly controlled and his developmental progress resumed. This inspired Abrahams to create the Charlie Foundation to promote the diet and fund research.[10] A multicentre prospective study began in 1994, the results were presented to the American Epilepsy Society in 1996 and were published[17] in 1998. There followed an explosion of scientific interest in the diet. In 1997, Abrahams produced a TV movie, ...First Do No Harm, starring Meryl Streep, in which a young boy's intractable epilepsy is successfully treated by the ketogenic diet.[1]

By 2007, the ketogenic diet was available from around 75 centres in 45 countries, and less restrictive variants, such as the modified Atkins diet, were in use, particularly among older children and adults. The ketogenic diet was also under investigation for the treatment of a wide variety of disorders other than epilepsy.[1]

Efficacy

The ketogenic diet reduces seizure frequency by more than 50% in half of the patients who try it and by more than 90% in a third of patients.[18] Three-quarters of children who respond do so within two weeks, though experts recommend a trial of at least three months before assuming it has been ineffective.[19] Children with refractory epilepsy are more likely to benefit from the ketogenic diet than from trying another anticonvulsant drug.[1] Adolescents and adults may also benefit from the diet, though compliance with oral diet (vs tube fed) remains a problem.[20]

Trial design

Early studies reported high success rates; in one study in 1925, 60% of patients became seizure-free, and another 35% of patients had a 50% reduction in seizure frequency. These studies generally examined a cohort of patients recently treated by the physician (a retrospective study) and selected patients who had successfully maintained the dietary restrictions. However, these studies are difficult to compare to modern trials. One reason is that these older trials suffered from selection bias, as they excluded patients who were unable to start or maintain the diet and thereby selected from patients who would generate better results. In an attempt to control for this bias, modern study design prefers a prospective cohort (the patients in the study are chosen before therapy begins) in which the results are presented for all patients regardless of whether they started or completed the treatment (known as intent-to-treat analysis).[21]

Another difference between older and newer studies is that the type of patients treated with the ketogenic diet has changed over time. When first developed and used, the ketogenic diet was not a treatment of last resort; in contrast, the children in modern studies have already tried and failed a number of anticonvulsant drugs, so may be assumed to have more difficult-to-treat epilepsy. Early and modern studies also differ because the treatment protocol has changed. In older protocols, the diet was initiated with a prolonged fast, designed to lose 5–10% body weight, and heavily restricted the calorie intake. Concerns over child health and growth led to a relaxation of the diet's restrictions.[21] Fluid restriction was once a feature of the diet, but this led to increased risk of constipation and kidney stones, and is no longer considered beneficial.[18]

Outcomes

A study with an intent-to-treat prospective design was published in 1998 by a team from the Johns Hopkins Hospital[22] and followed-up by a report published in 2001.[23] As with most studies of the ketogenic diet, no control group (patients who did not receive the treatment) was used. The study enrolled 150 children. After three months, 83% of them were still on the diet, 26% had experienced a good reduction in seizures, 31% had had an excellent reduction, and 3% were seizure-free.[Note 7] At 12 months, 55% were still on the diet, 23% had a good response, 20% had an excellent response, and 7% were seizure-free. Those who had discontinued the diet by this stage did so because it was ineffective, too restrictive, or due to illness, and most of those who remained were benefiting from it. The percentage of those still on the diet at two, three, and four years was 39%, 20%, and 12%, respectively. During this period, the most common reason for discontinuing the diet was because the children had become seizure-free or significantly better. At four years, 16% of the original 150 children had a good reduction in seizure frequency, 14% had an excellent reduction, and 13% were seizure-free, though these figures include many who were no longer on the diet. Those remaining on the diet after this duration were typically not seizure-free, but had had an excellent response.[23][24]

It is possible to combine the results of several small studies to produce evidence that is stronger than that available from each study alone—a statistical method known as meta-analysis. One of four such analyses, conducted in 2006, looked at 19 studies on a total of 1,084 patients.[25] It concluded that a third achieved an excellent reduction in seizure frequency and half the patients achieved a good reduction.[18]

A Cochrane systematic review in 2018 found and analysed eleven randomized controlled trials of ketogenic diet in people with epilepsy for whom drugs failed to control their seizures.[2] Six of the trials compared a group assigned to a ketogenic diet with a group not assigned to one. The other trials compared types of diets or ways of introducing them to make them more tolerable.[2] In the largest trial of the ketogenic diet with a non-diet control,[16] nearly 38% of the children and young people had half or fewer seizures with the diet compared 6% with the group not assigned to the diet. Two large trials of the Modified Atkins Diet compared to a non-diet control had similar results, with over 50% of children having half or fewer seizures with the diet compared to around 10% in the control group.[2]

A systematic review in 2018 looked at 16 studies on the ketogenic diet in adults. It concluded that the treatment was becoming more popular for that group of patients, that the efficacy in adults was similar to children, the side effects relatively mild. However, many patients gave up the diet, for various reasons, and the quality of evidence was inferior to studies on children. Health issues include high levels of low-density lipoprotein, high total cholesterol, and weight loss.[26]

Indications and contraindications

 
Experts on the ketogenic diet recommend it be strongly considered for children with uncontrolled epilepsy who have tried and failed two anticonvulsant drugs;[19] most children who start the ketogenic diet have failed at least three times this number.[27]

The ketogenic diet is indicated as an adjunctive (additional) treatment in children and young people with drug-resistant epilepsy.[28][29] It is approved by national clinical guidelines in Scotland,[29] England, and Wales[28] and reimbursed by nearly all US insurance companies.[30] Children with a focal lesion (a single point of brain abnormality causing the epilepsy) who would make suitable candidates for surgery are more likely to become seizure-free with surgery than with the ketogenic diet.[19][31] About a third of epilepsy centres that offer the ketogenic diet also offer a dietary therapy to adults. The two less restrictive dietary variants—the low glycaemic index treatment and the modified Atkins diet—are more appropriate for adolescents and adults, mainly due to better adherence.[19] A liquid form of the ketogenic diet is particularly easy to prepare for, and well tolerated by infants on formula and by others who are tube-fed.[5][32][19]

Advocates for the diet recommend that it be seriously considered after two medications have failed, as the chance of other drugs succeeding is only 10%.[19][33][34] The diet is recommended earlier for some epilepsy and genetic syndromes where it has shown particular usefulness. These include Dravet syndrome, infantile spasms, myoclonic-astatic epilepsy, tuberous sclerosis complex and for children fed by gastrostomy tube.[19][35]

A survey in 2005 of 88 paediatric neurologists in the US found that 36% regularly prescribed the diet after three or more drugs had failed, 24% occasionally prescribed the diet as a last resort, 24% had only prescribed the diet in a few rare cases, and 16% had never prescribed the diet. Several possible explanations exist for this gap between evidence and clinical practice.[36] One major factor may be the lack of adequately trained dietitians who are needed to administer a ketogenic diet programme.[33]

Because the ketogenic diet alters the body's metabolism, it is a first-line therapy in children with certain congenital metabolic diseases such as pyruvate dehydrogenase (E1) deficiency and glucose transporter 1 deficiency syndrome,[37] which prevent the body from using carbohydrates as fuel, leading to a dependency on ketone bodies. The ketogenic diet is beneficial in treating the seizures and some other symptoms in these diseases and is an absolute indication.[38] However, it is absolutely contraindicated in the treatment of other diseases such as pyruvate carboxylase deficiency, porphyria, and other rare genetic disorders of fat metabolism.[19] Persons with a disorder of fatty acid oxidation are unable to metabolise fatty acids, which replace carbohydrates as the major energy source on the diet. On the ketogenic diet, their bodies would consume their own protein stores for fuel, leading to ketoacidosis, and eventually coma and death.[39]

Interactions

The ketogenic diet is usually initiated in combination with the patient's existing anticonvulsant regimen, though patients may be weaned off anticonvulsants if the diet is successful. Some evidence of synergistic benefits is seen when the diet is combined with the vagus nerve stimulator or with the drug zonisamide, and that the diet may be less successful in children receiving phenobarbital.[18]

Adverse effects

The ketogenic diet is not considered a benign, holistic, or all-natural treatment. As with any serious medical therapy, it may result in complications, although these are generally less severe and less frequent than with anticonvulsant medication or surgery.[30] Common but easily treatable short-term side effects include constipation, low-grade acidosis, and hypoglycaemia if an initial fast is undertaken. Raised levels of lipids in the blood affect up to 60% of children[40] and cholesterol levels may increase by around 30%.[30] This can be treated by changes to the fat content of the diet, such as from saturated fats towards polyunsaturated fats, and if persistent, by lowering the ketogenic ratio.[40] Supplements are necessary to counter the dietary deficiency of many micronutrients.[18]

Long-term use of the ketogenic diet in children increases the risk of slowed or stunted growth, bone fractures, and kidney stones.[18] The diet reduces levels of insulin-like growth factor 1, which is important for childhood growth. Like many anticonvulsant drugs, the ketogenic diet has an adverse effect on bone health. Many factors may be involved such as acidosis and suppressed growth hormone.[40] About one in 20 children on the ketogenic diet develop kidney stones (compared with one in several thousand for the general population). A class of anticonvulsants known as carbonic anhydrase inhibitors (topiramate, zonisamide) are known to increase the risk of kidney stones, but the combination of these anticonvulsants and the ketogenic diet does not appear to elevate the risk above that of the diet alone.[41] The stones are treatable and do not justify discontinuation of the diet.[41] Around half of clinics gives oral potassium citrate supplements empirically to all ketogenic diet patients, with some evidence that this reduces the incidence of stone formation. However, has not been tested in a prospective controlled trial.[19] Kidney stone formation (nephrolithiasis) is associated with the diet for four reasons:[41]

  • Excess calcium in the urine (hypercalciuria) occurs due to increased bone demineralisation with acidosis. Bones are mainly composed of calcium phosphate. The phosphate reacts with the acid, and the calcium is excreted by the kidneys.[41]
  • Hypocitraturia: the urine has an abnormally low concentration of citrate, which normally helps to dissolve free calcium.[41]
  • The urine has a low pH, which stops uric acid from dissolving, leading to crystals that act as a nidus for calcium stone formation.[41]
  • Many institutions traditionally restricted the water intake of patients on the diet to 80% of normal daily needs;[41] this practice is no longer encouraged.[18]

In adolescent and adults, common side effects reported include weight loss, constipation, dyslipidemia, and in women, dysmenorrhea.[42]

Implementation

The ketogenic diet is a medical nutrition therapy that involves participants from various disciplines. Team members include a registered paediatric dietitian who coordinates the diet programme; a paediatric neurologist who is experienced in offering the ketogenic diet; and a registered nurse who is familiar with childhood epilepsy. Additional help may come from a medical social worker who works with the family and a pharmacist who can advise on the carbohydrate content of medicines. Lastly, the parents and other caregivers must be educated in many aspects of the diet for it to be safely implemented.[5]

Implementing the diet can present difficulties for caregivers and the patient due to the time commitment involved in measuring and planning meals. Since any unplanned eating can potentially break the nutritional balance required, some people find the discipline needed to maintain the diet challenging and unpleasant. Some people terminate the diet or switch to a less demanding diet, like the modified Atkins diet or the low-glycaemic index treatment diet, because they find the difficulties too great.[43]

Initiation

The Johns Hopkins Hospital protocol for initiating the classic ketogenic diet has been widely adopted.[44] It involves a consultation with the patient and their caregivers and, later, a short hospital admission.[21] Because of the risk of complications during ketogenic diet initiation, most centres begin the diet under close medical supervision in the hospital.[19]

At the initial consultation, patients are screened for conditions that may contraindicate the diet. A dietary history is obtained and the parameters of the diet selected: the ketogenic ratio of fat to combined protein and carbohydrate,[Note 8] the calorie requirements and the fluid intake.[21]

The day before admission to hospital, the proportion of carbohydrate in the diet may be decreased and the patient begins fasting after his or her evening meal.[21] On admission, only calorie- and caffeine-free fluids[39] are allowed until dinner, which consists of "eggnog"[Note 9] restricted to one-third of the typical calories for a meal. The following breakfast and lunch are similar, and on the second day, the "eggnog" dinner is increased to two-thirds of a typical meal's caloric content. By the third day, dinner contains the full calorie quota and is a standard ketogenic meal (not "eggnog"). After a ketogenic breakfast on the fourth day, the patient is discharged. Where possible, the patient's current medicines are changed to carbohydrate-free formulations.[21]

When in the hospital, glucose levels are checked several times daily and the patient is monitored for signs of symptomatic ketosis (which can be treated with a small quantity of orange juice). Lack of energy and lethargy are common, but disappear within two weeks.[17] The parents attend classes over the first three full days, which cover nutrition, managing the diet, preparing meals, avoiding sugar, and handling illness.[21] The level of parental education and commitment required is higher than with medication.[45]

Variations on the Johns Hopkins protocol are common. The initiation can be performed using outpatient clinics rather than requiring a stay in hospital. Often, no initial fast is used (fasting increases the risk of acidosis, hypoglycaemia, and weight loss). Rather than increasing meal sizes over the three-day initiation, some institutions maintain meal size, but alter the ketogenic ratio from 2:1 to 4:1.[19]

For patients who benefit, half achieve a seizure reduction within five days (if the diet starts with an initial fast of one to two days), three-quarters achieve a reduction within two weeks, and 90% achieve a reduction within 23 days. If the diet does not begin with a fast, the time for half of the patients to achieve an improvement is longer (two weeks), but the long-term seizure reduction rates are unaffected.[45] Parents are encouraged to persist with the diet for at least three months before any final consideration is made regarding efficacy.[19]

Maintenance

After initiation, the child regularly visits the hospital outpatient clinic where they are seen by the dietitian and neurologist, and various tests and examinations are performed. These are held every three months for the first year and then every six months thereafter. Infants under one year old are seen more frequently, with the initial visit held after just two to four weeks.[46] A period of minor adjustments is necessary to ensure consistent ketosis is maintained and to better adapt the meal plans to the patient. This fine-tuning is typically done over the telephone with the hospital dietitian[21] and includes changing the number of calories, altering the ketogenic ratio, or adding some MCT or coconut oils to a classic diet.[18] Urinary ketone levels are checked daily to detect whether ketosis has been achieved and to confirm that the patient is following the diet, though the level of ketones does not correlate with an anticonvulsant effect.[21] This is performed using ketone test strips containing nitroprusside, which change colour from buff-pink to maroon in the presence of acetoacetate (one of the three ketone bodies).[47]

A short-lived increase in seizure frequency may occur during illness or if ketone levels fluctuate. The diet may be modified if seizure frequency remains high, or the child is losing weight.[21] Loss of seizure-control may come from unexpected sources. Even "sugar-free" food can contain carbohydrates such as maltodextrin, sorbitol, starch, and fructose. The sorbitol content of suntan lotion and other skincare products may be high enough for some to be absorbed through the skin and thus negate ketosis.[33]

Discontinuation

About 20% of children on the ketogenic diet achieve freedom from seizures, and many are able to reduce the use of anticonvulsant drugs or eliminate them altogether.[18] Commonly, at around two years on the diet, or after six months of being seizure-free, the diet may be gradually discontinued over two or three months. This is done by lowering the ketogenic ratio until urinary ketosis is no longer detected, and then lifting all calorie restrictions.[48] This timing and method of discontinuation mimics that of anticonvulsant drug therapy in children, where the child has become seizure-free. When the diet is required to treat certain metabolic diseases, the duration will be longer. The total diet duration is up to the treating ketogenic diet team and parents; durations up to 12 years have been studied and found beneficial.[46]

Children who discontinue the diet after achieving seizure freedom have about a 20% risk of seizures returning. The length of time until recurrence is highly variable, but averages two years. This risk of recurrence compares with 10% for resective surgery (where part of the brain is removed) and 30–50% for anticonvulsant therapy. Of those who have a recurrence, just over half can regain freedom from seizures either with anticonvulsants or by returning to the ketogenic diet. Recurrence is more likely if, despite seizure freedom, an electroencephalogram shows epileptiform spikes, which indicate epileptic activity in the brain but are below the level that will cause a seizure. Recurrence is also likely if an MRI scan shows focal abnormalities (for example, as in children with tuberous sclerosis). Such children may remain on the diet longer than average, and children with tuberous sclerosis who achieve seizure freedom could remain on the ketogenic diet indefinitely.[48]

Variants

Classic

 
The ratio of calorific contributions from food components of four diets, by weight

The ketogenic diet is calculated by a dietitian for each child. Age, weight, activity levels, culture, and food preferences all affect the meal plan. First, the energy requirements are set at 80–90% of the recommended daily amounts (RDA) for the child's age (the high-fat diet requires less energy to process than a typical high-carbohydrate diet). Highly active children or those with muscle spasticity require more food energy than this; immobile children require less. The ketogenic ratio of the diet compares the weight of fat to the combined weight of carbohydrate and protein. This is typically 4:1, but children who are younger than 18 months, older than 12 years, or who are obese may be started on a 3:1 ratio. Fat is energy-rich, with 9 kcal/g (38 kJ/g) compared to 4 kcal/g (17 kJ/g) for carbohydrate or protein, so portions on the ketogenic diet are smaller than normal. The quantity of fat in the diet can be calculated from the overall energy requirements and the chosen ketogenic ratio. Next, the protein levels are set to allow for growth and body maintenance, and are around 1 g protein for each kg of body weight. Lastly, the amount of carbohydrate is set according to what allowance is left while maintaining the chosen ratio. Any carbohydrate in medications or supplements must be subtracted from this allowance. The total daily amount of fat, protein, and carbohydrate is then evenly divided across the meals.[39]

A computer program such as KetoCalculator may be used to help generate recipes.[49] The meals often have four components: heavy whipping cream, a protein-rich food (typically meat), a fruit or vegetable and a fat such as butter, vegetable oil, or mayonnaise. Only low-carbohydrate fruits and vegetables are allowed, which excludes bananas, potatoes, peas, and corn. Suitable fruits are divided into two groups based on the amount of carbohydrate they contain, and vegetables are similarly divided into two groups. Foods within each of these four groups may be freely substituted to allow for variation without needing to recalculate portion sizes. For example, cooked broccoli, Brussels sprouts, cauliflower, and green beans are all equivalent. Fresh, canned, or frozen foods are equivalent, but raw and cooked vegetables differ, and processed foods are an additional complication. Parents are required to be precise when measuring food quantities on an electronic scale accurate to 1 g. The child must eat the whole meal and cannot have extra portions; any snacks must be incorporated into the meal plan. A small amount of MCT oil may be used to help with constipation or to increase ketosis.[39]

The classic ketogenic diet is not a balanced diet and only contains tiny portions of fresh fruit and vegetables, fortified cereals, and calcium-rich foods. In particular, the B vitamins, calcium, and vitamin D must be artificially supplemented. This is achieved by taking two sugar-free supplements designed for the patient's age: a multivitamin with minerals and calcium with vitamin D.[18] A typical day of food for a child on a 4:1 ratio, 1,500 kcal (6,300 kJ) ketogenic diet comprises three small meals and three small snacks:[30]

Sample meal plan for one day
Meal Menu idea Ingredients
Breakfast Egg with bacon
  • 28 g egg (about half an egg)
  • 11 g bacon (about half a slice)
  • 37 g of 36% heavy whipping cream
  • 23 g butter
  • 9 g slice of apple (about 5% of one apple)
Morning snack Peanut butter ball

(serving size: 0.5 ounce)

  • 6 g peanut butter
  • 9 g butter
Lunch Tuna salad
  • 28 g tuna fish
  • 30 g mayonnaise
  • 10 g celery
  • 36 g of 36% heavy whipping cream
  • 15 g lettuce (one large leaf)
Afternoon snack Keto yogurt

(serving size: 1.3 ounces)

  • 18 g of 36% heavy whipping cream
  • 17 g sour cream
  • 4 g strawberries (about half of one small strawberry)
  • artificial sweetener
Dinner Cheeseburger (no bun)
  • 22 g minced (ground) beef
  • 10 g American cheese (half a slice of cheese)
  • 26 g butter
  • 38 g of 36% heavy whipping cream
  • 10 g lettuce (one medium leaf)
  • 11 g green beans (one spoonful)
Evening snack Keto custard

(serving size: 1.2 ounces)

  • 25 g of 36% heavy whipping cream
  • 9 g egg (half a tablespoon)
  • Pure, unsweetened vanilla flavouring

MCT oil

Normal dietary fat contains mostly long-chain triglycerides (LCTs). Medium-chain triglycerides (MCTs) are more ketogenic than LCTs because they generate more ketones per unit of energy when metabolised. Their use allows for a diet with a lower proportion of fat and a greater proportion of protein and carbohydrate,[18] leading to more food choices and larger portion sizes.[4] The original MCT diet developed by Peter Huttenlocher in the 1970s derived 60% of its calories from MCT oil.[15] Consuming that quantity of MCT oil caused abdominal cramps, diarrhoea, and vomiting in some children. A figure of 45% is regarded as a balance between achieving good ketosis and minimising gastrointestinal complaints. The classical and modified MCT ketogenic diets are equally effective and differences in tolerability are not statistically significant.[46] The MCT diet is less popular in the United States; MCT oil is more expensive than other dietary fats and is not covered by insurance companies.[18]

Modified Atkins

First reported in 2003, the idea of using a form of the Atkins diet to treat epilepsy came about after parents and patients discovered that the induction phase of the Atkins diet controlled seizures. The ketogenic diet team at Johns Hopkins Hospital modified the Atkins diet by removing the aim of achieving weight loss, extending the induction phase indefinitely, and specifically encouraging fat consumption. Compared with the ketogenic diet, the modified Atkins diet (MAD) places no limit on calories or protein, and the lower overall ketogenic ratio (about 1:1) does not need to be consistently maintained by all meals of the day. The MAD does not begin with a fast or with a stay in hospital and requires less dietitian support than the ketogenic diet. Carbohydrates are initially limited to 10 g per day in children or 20 g per day in adults, and are increased to 20–30 g per day after a month or so, depending on the effect on seizure control or tolerance of the restrictions. Like the ketogenic diet, the MAD requires vitamin and mineral supplements and children are carefully and periodically monitored at outpatient clinics.[50]

The modified Atkins diet reduces seizure frequency by more than 50% in 43% of patients who try it and by more than 90% in 27% of patients.[18] While the strength of evidence is low for the modified Atkins, it has been known to show seizure freedom in some infants.[51] Few adverse effects have been reported, though cholesterol is increased and the diet has not been studied long term.[50] Although based on a smaller data set (126 adults and children from 11 studies over five centres), these results from 2009 compare favorably with the traditional ketogenic diet.[18]

Low glycemic index treatment

The low glycemic index treatment (LGIT)[52] is an attempt to achieve the stable blood glucose levels seen in children on the classic ketogenic diet while using a much less restrictive regimen. The hypothesis is that stable blood glucose may be one of the mechanisms of action involved in the ketogenic diet,[46] which occurs because the absorption of the limited carbohydrates is slowed by the high fat content.[5] Although it is also a high-fat diet (with approximately 60% calories from fat),[5][Note 8] the LGIT allows more carbohydrate than either the classic ketogenic diet or the modified Atkins diet, approximately 40–60 g per day.[18] However, the types of carbohydrates consumed are restricted to those that have a glycaemic index lower than 50. Like the modified Atkins diet, the LGIT is initiated and maintained at outpatient clinics and does not require precise weighing of food or intensive dietitian support. Both are offered at most centres that run ketogenic diet programmes, and in some centres they are often the primary dietary therapy for adolescents.[46]

Short-term results for the LGIT indicate that at one month approximately half of the patients experience a greater than 50% reduction in seizure frequency, with overall figures approaching that of the ketogenic diet. The data (coming from one centre's experience with 76 children up to the year 2009) also indicate fewer side effects than the ketogenic diet and that it is better tolerated, with more palatable meals.[18][53]

Prescribed formulations

 
Measuring KetoCal – a powdered formula for administering the classic ketogenic diet

Infants and patients fed via a gastrostomy tube can also be given a ketogenic diet. Parents make up a prescribed powdered formula, such as KetoCal, into a liquid feed.[21] Gastrostomy feeding avoids any issues with palatability, and bottle-fed infants readily accept the ketogenic formula.[33] Some studies have found this liquid feed to be more efficacious and associated with lower total cholesterol than a solid ketogenic diet.[18] KetoCal is a nutritionally complete food containing milk protein and is supplemented with amino acids, fat, carbohydrate, vitamins, minerals and trace elements. It is used to administer the 4:1 ratio classic ketogenic diet in children over one year. The formula is available in both 3:1 and 4:1 ratios, either unflavoured or in an artificially sweetened vanilla flavour and is suitable for tube or oral feeding.[54] Other formula products include KetoVolve[55] and Ketonia.[56] Alternatively, a liquid ketogenic diet may be produced by combining Ross Carbohydrate Free soy formula with Microlipid and Polycose.[56]

Worldwide

In theory, there are no restrictions on where the ketogenic diet might be used, and it can cost less than modern anticonvulsants. However, fasting and dietary changes are affected by religious and cultural issues. A culture where food is often prepared by grandparents or hired help means more people must be educated about the diet. When families dine together, sharing the same meal, it can be difficult to separate the child's meal. In many countries, food labelling is not mandatory, so calculating macronutrients such as fat, protein and carbohydrates can be difficult. In some countries, it may be hard to find sugar-free forms of medicines and supplements, to purchase an accurate electronic scale, or to afford MCT oils.[57]

In Asia, the traditional diet includes rice and noodles as the main source of energy, making their elimination difficult. Therefore, the MCT-oil form of the diet, which allows more carbohydrate, has proved useful. In India, religious beliefs commonly affect the diet: for instance, Hindus consider cows sacred animals not to be killed and eaten, Islam forbids consumption of pork, and strict vegetarians of the Jain faith do not eat root vegetables. The Indian ketogenic diet is started without a fast due to cultural opposition towards fasting in children. The low-fat, high-carbohydrate nature of the normal Indian and Asian diet means that their ketogenic diets typically have a lower ketogenic ratio (1:1) than in America and Europe. However, they appear to be just as effective.[57]

In many developing countries, the ketogenic diet is expensive because dairy fats and meat are more expensive than grain, fruit, and vegetables. The modified Atkins diet has been proposed as a lower-cost alternative for those countries; the slightly more expensive food bill can be offset by a reduction in pharmaceutical costs if the diet is successful. The modified Atkins diet is less complex to explain and prepare and requires less support from a dietitian.[58]

Mechanism of action

Seizure pathology

Ketone bodies
 
β-hydroxybutyrate
 
acetoacetic acid
 
acetone

The brain is composed of a network of neurons that transmit signals by propagating nerve impulses. The propagation of this impulse from one neuron to another is typically controlled by neurotransmitters, though there are also electrical pathways between some neurons. Neurotransmitters can inhibit impulse firing (primarily done by γ-aminobutyric acid, or GABA) or they can excite the neuron into firing (primarily done by glutamate). A neuron that releases inhibitory neurotransmitters from its terminals is called an inhibitory neuron, while one that releases excitatory neurotransmitters is an excitatory neuron. When the normal balance between inhibition and excitation is significantly disrupted in all or part of the brain, a seizure can occur. The GABA system is an important target for anticonvulsant drugs, since seizures may be discouraged by increasing GABA synthesis, decreasing its breakdown, or enhancing its effect on neurons.[7]

The nerve impulse is characterised by a great influx of sodium ions through channels in the neuron's cell membrane followed by an efflux of potassium ions through other channels. The neuron is unable to fire again for a short time (known as the refractory period), which is mediated by another potassium channel. The flow through these ion channels is governed by a "gate" which is opened by either a voltage change or a chemical messenger known as a ligand (such as a neurotransmitter). These channels are another target for anticonvulsant drugs.[7]

There are many ways in which epilepsy occurs. Examples of pathological physiology include: unusual excitatory connections within the neuronal network of the brain; abnormal neuron structure leading to altered current flow; decreased inhibitory neurotransmitter synthesis; ineffective receptors for inhibitory neurotransmitters; insufficient breakdown of excitatory neurotransmitters leading to excess; immature synapse development; and impaired function of ionic channels.[7]

Seizure control

Although many hypotheses have been put forward to explain how the ketogenic diet works, it remains a mystery. Disproven hypotheses include systemic acidosis (high levels of acid in the blood), electrolyte changes and hypoglycaemia (low blood glucose).[21] Although many biochemical changes are known to occur in the brain of a patient on the ketogenic diet, it is not known which of these has an anticonvulsant effect. The lack of understanding in this area is similar to the situation with many anticonvulsant drugs.[59]

On the ketogenic diet, carbohydrates are restricted and so cannot provide for all the metabolic needs of the body. Instead, fatty acids are used as the major source of fuel. These are used through fatty-acid oxidation in the cell's mitochondria (the energy-producing parts of the cell). Humans can convert some amino acids into glucose by a process called gluconeogenesis, but cannot do this by using fatty acids.[60] Since amino acids are needed to make proteins, which are essential for growth and repair of body tissues, these cannot be used only to produce glucose. This could pose a problem for the brain, since it is normally fuelled solely by glucose, and most fatty acids do not cross the blood–brain barrier. However, the liver can use long-chain fatty acids to synthesise the three ketone bodies β-hydroxybutyrate, acetoacetate and acetone. These ketone bodies enter the brain and partially substitute for blood glucose as a source of energy.[59]

The ketone bodies are possibly anticonvulsant; in animal models, acetoacetate and acetone protect against seizures. The ketogenic diet results in adaptive changes to brain energy metabolism that increase the energy reserves; ketone bodies are a more efficient fuel than glucose, and the number of mitochondria is increased. This may help the neurons to remain stable in the face of increased energy demand during a seizure, and may confer a neuroprotective effect.[59]

The ketogenic diet has been studied in at least 14 rodent animal models of seizures. It is protective in many of these models and has a different protection profile than any known anticonvulsant. Conversely, fenofibrate, not used clinically as an antiepileptic, exhibits experimental anticonvulsant properties in adult rats comparable to the ketogenic diet.[61] This, together with studies showing its efficacy in patients who have failed to achieve seizure control on half a dozen drugs, suggests a unique mechanism of action.[59]

Anticonvulsants suppress epileptic seizures, but they neither cure nor prevent the development of seizure susceptibility. The development of epilepsy (epileptogenesis) is a process that is poorly understood. A few anticonvulsants (valproate, levetiracetam and benzodiazepines) have shown antiepileptogenic properties in animal models of epileptogenesis. However, no anticonvulsant has ever achieved this in a clinical trial in humans. The ketogenic diet has been found to have antiepileptogenic properties in rats.[59]

Other medical applications

The ketogenic diet has been studied for potential therapeutic use in various neurological disorders other than epilepsy: Alzheimer's disease (AD),[62] amyotrophic lateral sclerosis (ALS), autism, headache, neurotrauma, pain, Parkinson's disease (PD) and sleep disorders.[6] As of 2022 there is no clinical evidence that a ketogenic diet is effective to treat cancer.[63]

See also

Explanatory notes

  1. ^ In this article, kcal stands for calories as a unit of measure (4.1868 kJ), and calories stands for "energy" from food.
  2. ^ Unless otherwise stated, the term fasting in this article refers to going without food while maintaining calorie-free fluid intake.
  3. ^ Hippocrates, On the Sacred Disease, ch. 18; vol. 6.
  4. ^ Hippocrates, Epidemics, VII, 46; vol. 5.
  5. ^ Galen, De venae sect. adv. Erasistrateos Romae degentes, c. 8; vol. 11.
  6. ^ Galen, De victu attenuante, c. 1.
  7. ^ A good reduction is defined here to mean a 50–90% decrease in seizure frequency. An excellent reduction is a 90–99% decrease.
  8. ^ a b The ketogenic ratio k can be converted to the portion of calories from fat f using the Atwater coefficients of 9 and 4 kcal/g for fat and combined carbohydrate and water respectively. The equation is: f = 9 k/9 k + 4. For example, a 4:1 diet derives 90% of calories from fat. The inverse equation is k = 4 f/9 (1 - f).
  9. ^ Ketogenic "eggnog" is used during induction and is a drink with the required ketogenic ratio. For example, a 4:1 ratio eggnog would contain 60 g of 36% heavy whipping cream, 25 g pasteurised raw egg, saccharin and vanilla flavour. This contains 245 kcal (1,025 kJ), 4 g protein, 2 g carbohydrate and 24 g fat (24:6 = 4:1).[17] The eggnog may also be cooked to make a custard, or frozen to make ice cream.[39]

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Further reading

  • Freeman JM, Kossoff EH, Freeman JB, Kelly MT. The Ketogenic Diet: A Treatment for Children and Others with Epilepsy. 4th ed. New York: Demos; 2007. ISBN 1932603182.
  • Lowery R, Wilson J. The Ketogenic Bible: The Authoritative Guide to Ketosis. 1st ed. Victory Belt Publishing; 2017. ISBN 978-1628601046.

External links

  • Diet Review: Ketogenic Diet for Weight Loss, from the Harvard University School of Public Health
  • Ketogenic diet at Curlie
  • Matthew's Friends, a UK charity and information resource
  • The Charlie Foundation, a US charity and information resource
  • Epilepsy.com: Dietary Therapies & Ketogenic News, information and regular research news updates

February 15, 2024
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This article is about a dietary therapy for epilepsy For information on ketogenic diets as a lifestyle choice or for weight loss see Very low carbohydrate ketogenic diet The ketogenic diet is a high fat adequate protein low carbohydrate dietary therapy that in conventional medicine is used mainly to treat hard to control refractory epilepsy in children The diet forces the body to burn fats rather than carbohydrates Testing for ketone bodies in urineNormally carbohydrates in food are converted into glucose which is then transported around the body and is important in fueling brain function However if only a little carbohydrate remains in the diet the liver converts fat into fatty acids and ketone bodies the latter passing into the brain and replacing glucose as an energy source An elevated level of ketone bodies in the blood a state called ketosis eventually lowers the frequency of epileptic seizures 1 Around half of children and young people with epilepsy who have tried some form of this diet saw the number of seizures drop by at least half and the effect persists after discontinuing the diet 2 Some evidence shows that adults with epilepsy may benefit from the diet and that a less strict regimen such as a modified Atkins diet is similarly effective 1 Side effects may include constipation high cholesterol growth slowing acidosis and kidney stones 3 The original therapeutic diet for paediatric epilepsy provides just enough protein for body growth and repair and sufficient calories Note 1 to maintain the correct weight for age and height The classic therapeutic ketogenic diet was developed for treatment of paediatric epilepsy in the 1920s and was widely used into the next decade but its popularity waned with the introduction of effective anticonvulsant medications This classic ketogenic diet contains a 4 1 ketogenic ratio or ratio by weight of fat to combined protein and carbohydrate This is achieved by excluding high carbohydrate foods such as starchy fruits and vegetables bread pasta grains and sugar while increasing the consumption of foods high in fat such as nuts cream and butter 1 Most dietary fat is made of molecules called long chain triglycerides LCTs However medium chain triglycerides MCTs made from fatty acids with shorter carbon chains than LCTs are more ketogenic A variant of the classic diet known as the MCT ketogenic diet uses a form of coconut oil which is rich in MCTs to provide around half the calories As less overall fat is needed in this variant of the diet a greater proportion of carbohydrate and protein can be consumed allowing a greater variety of food choices 4 5 In 1994 Hollywood producer Jim Abrahams whose son s severe epilepsy was effectively controlled by the diet created the Charlie Foundation for Ketogenic Therapies to further promote diet therapy Publicity included an appearance on NBC s Dateline program and First Do No Harm 1997 a made for television film starring Meryl Streep The foundation sponsored a research study the results of which announced in 1996 marked the beginning of renewed scientific interest in the diet 1 Possible therapeutic uses for the ketogenic diet have been studied for many additional neurological disorders some of which include Alzheimer s disease amyotrophic lateral sclerosis headache neurotrauma pain Parkinson s disease and sleep disorders 6 Contents 1 Epilepsy 2 History 2 1 Fasting 2 2 Diet 2 3 Anticonvulsants and decline 2 4 MCT diet 2 5 Revival 3 Efficacy 3 1 Trial design 3 2 Outcomes 4 Indications and contraindications 5 Interactions 6 Adverse effects 7 Implementation 7 1 Initiation 7 2 Maintenance 7 3 Discontinuation 8 Variants 8 1 Classic 8 2 MCT oil 8 3 Modified Atkins 8 4 Low glycemic index treatment 8 5 Prescribed formulations 8 6 Worldwide 9 Mechanism of action 9 1 Seizure pathology 9 2 Seizure control 10 Other medical applications 11 See also 12 Explanatory notes 13 References 14 Further reading 15 External linksEpilepsyEpilepsy is one of the most common neurological disorders after migraine and stroke 7 affecting around 50 million people worldwide 8 It is diagnosed in a person having recurrent unprovoked seizures These occur when cortical neurons fire excessively hypersynchronously or both leading to temporary disruption of normal brain function This might affect for example the muscles the senses consciousness or a combination A seizure can be focal confined to a specific part of the brain or generalised spread widely throughout the brain and leading to a loss of consciousness Epilepsy can occur for a variety of reasons some forms have been classified into epileptic syndromes most of which begin in childhood Epilepsy is considered refractory not yielding to treatment when two or three anticonvulsant drugs have failed to control it About 60 of patients achieve control of their epilepsy with the first drug they use whereas around 30 do not achieve control with drugs When drugs fail other options include epilepsy surgery vagus nerve stimulation and the ketogenic diet 7 HistoryThe ketogenic diet is a mainstream medical dietary therapy that was developed to reproduce the success and remove the limitations of the non mainstream use of fasting to treat epilepsy Note 2 Although popular in the 1920s and 30s it was largely abandoned in favour of new anticonvulsant drugs 1 Most individuals with epilepsy can successfully control their seizures with medication However 25 30 fail to achieve such control despite trying a number of different drugs 9 For this group and for children in particular the diet has once again found a role in epilepsy management 1 10 Fasting nbsp A news report of Dr Hugh Conklin s water diet treatment from 1922Physicians of ancient Greece treated diseases including epilepsy by altering their patients diet An early treatise in the Hippocratic Corpus On the Sacred Disease covers the disease it dates from c 400 BC Its author argued against the prevailing view that epilepsy was supernatural in origin and cure and proposed that dietary therapy had a rational and physical basis Note 3 In the same collection the author of Epidemics describes the case of a man whose epilepsy is cured as quickly as it had appeared through complete abstinence of food and drink Note 4 The royal physician Erasistratus declared One inclining to epilepsy should be made to fast without mercy and be put on short rations Note 5 Galen believed an attenuating diet Note 6 might afford a cure in mild cases and be helpful in others 11 The first modern study of fasting as a treatment for epilepsy was in France in 1911 12 Twenty epilepsy patients of all ages were detoxified by consuming a low calorie vegetarian diet combined with periods of fasting and purging Two benefited enormously but most failed to maintain compliance with the imposed restrictions The diet improved the patients mental capabilities in contrast to their medication potassium bromide which dulled the mind 13 Around this time Bernarr Macfadden an American exponent of physical culture popularised the use of fasting to restore health His disciple the osteopathic physician Dr Hugh William Conklin of Battle Creek Michigan began to treat his epilepsy patients by recommending fasting Conklin conjectured that epileptic seizures were caused when a toxin secreted from the Peyer s patches in the intestines was discharged into the bloodstream He recommended a fast lasting 18 to 25 days to allow this toxin to dissipate Conklin probably treated hundreds of epilepsy patients with his water diet and boasted of a 90 cure rate in children falling to 50 in adults Later analysis of Conklin s case records showed 20 of his patients achieved freedom from seizures and 50 had some improvement 10 Conklin s fasting therapy was adopted by neurologists in mainstream practice In 1916 a Dr McMurray wrote to the New York Medical Journal claiming to have successfully treated epilepsy patients with a fast followed by a starch and sugar free diet since 1912 In 1921 prominent endocrinologist Henry Rawle Geyelin reported his experiences to the American Medical Association convention He had seen Conklin s success first hand and had attempted to reproduce the results in 36 of his own patients He achieved similar results despite having studied the patients for only a short time Further studies in the 1920s indicated that seizures generally returned after the fast Charles P Howland the parent of one of Conklin s successful patients and a wealthy New York corporate lawyer gave his brother John Elias Howland a gift of 5 000 to study the ketosis of starvation As professor of paediatrics at Johns Hopkins Hospital John E Howland used the money to fund research undertaken by neurologist Stanley Cobb and his assistant William G Lennox 10 Diet In 1921 Rollin Turner Woodyatt reviewed the research on diet and diabetes He reported that three water soluble compounds b hydroxybutyrate acetoacetate and acetone known collectively as ketone bodies were produced by the liver in otherwise healthy people when they were starved or if they consumed a very low carbohydrate high fat diet 10 Dr Russell Morse Wilder at the Mayo Clinic built on this research and coined the term ketogenic diet to describe a diet that produced a high level of ketone bodies in the blood ketonemia through an excess of fat and lack of carbohydrate Wilder hoped to obtain the benefits of fasting in a dietary therapy that could be maintained indefinitely His trial on a few epilepsy patients in 1921 was the first use of the ketogenic diet as a treatment for epilepsy 10 Wilder s colleague paediatrician Mynie Gustav Peterman later formulated the classic diet with a ratio of one gram of protein per kilogram of body weight in children 10 15 g of carbohydrate per day and the remainder of calories from fat Peterman s work in the 1920s established the techniques for induction and maintenance of the diet Peterman documented positive effects improved alertness behaviour and sleep and adverse effects nausea and vomiting due to excess ketosis The diet proved to be very successful in children Peterman reported in 1925 that 95 of 37 young patients had improved seizure control on the diet and 60 became seizure free By 1930 the diet had also been studied in 100 teenagers and adults Clifford Joseph Barborka Sr also from the Mayo Clinic reported that 56 of those older patients improved on the diet and 12 became seizure free Although the adult results are similar to modern studies of children they did not compare as well to contemporary studies Barborka concluded that adults were least likely to benefit from the diet and the use of the ketogenic diet in adults was not studied again until 1999 10 14 Anticonvulsants and decline During the 1920s and 1930s when the only anticonvulsant drugs were the sedative bromides discovered 1857 and phenobarbital 1912 the ketogenic diet was widely used and studied This changed in 1938 when H Houston Merritt Jr and Tracy Putnam discovered phenytoin Dilantin and the focus of research shifted to discovering new drugs With the introduction of sodium valproate in the 1970s drugs were available to neurologists that were effective across a broad range of epileptic syndromes and seizure types The use of the ketogenic diet by this time restricted to difficult cases such as Lennox Gastaut syndrome declined further 10 MCT diet nbsp Medium chain triglyceride MCT oil emulsionIn the 1960s medium chain triglycerides MCTs were found to produce more ketone bodies per unit of energy than normal dietary fats which are mostly long chain triglycerides 15 MCTs are more efficiently absorbed and are rapidly transported to the liver via the hepatic portal system rather than the lymphatic system 16 The severe carbohydrate restrictions of the classic ketogenic diet made it difficult for parents to produce palatable meals that their children would tolerate In 1971 Peter Huttenlocher devised a ketogenic diet where about 60 of the calories came from the MCT oil and this allowed more protein and up to three times as much carbohydrate as the classic ketogenic diet The oil was mixed with at least twice its volume of skimmed milk chilled and sipped during the meal or incorporated into food He tested it on 12 children and adolescents with intractable seizures Most children improved in both seizure control and alertness results that were similar to the classic ketogenic diet Gastrointestinal upset was a problem which led one patient to abandon the diet but meals were easier to prepare and better accepted by the children 15 The MCT diet replaced the classic ketogenic diet in many hospitals though some devised diets that were a combination of the two 10 Revival The ketogenic diet achieved national media exposure in the US in October 1994 when NBC s Dateline television programme reported the case of Charlie Abrahams son of Hollywood producer Jim Abrahams The two year old had epilepsy that had remained uncontrolled by mainstream and alternative therapies Abrahams discovered a reference to the ketogenic diet in an epilepsy guide for parents and brought Charlie to John M Freeman at Johns Hopkins Hospital which had continued to offer the therapy Under the diet Charlie s epilepsy was rapidly controlled and his developmental progress resumed This inspired Abrahams to create the Charlie Foundation to promote the diet and fund research 10 A multicentre prospective study began in 1994 the results were presented to the American Epilepsy Society in 1996 and were published 17 in 1998 There followed an explosion of scientific interest in the diet In 1997 Abrahams produced a TV movie First Do No Harm starring Meryl Streep in which a young boy s intractable epilepsy is successfully treated by the ketogenic diet 1 By 2007 the ketogenic diet was available from around 75 centres in 45 countries and less restrictive variants such as the modified Atkins diet were in use particularly among older children and adults The ketogenic diet was also under investigation for the treatment of a wide variety of disorders other than epilepsy 1 EfficacyThe ketogenic diet reduces seizure frequency by more than 50 in half of the patients who try it and by more than 90 in a third of patients 18 Three quarters of children who respond do so within two weeks though experts recommend a trial of at least three months before assuming it has been ineffective 19 Children with refractory epilepsy are more likely to benefit from the ketogenic diet than from trying another anticonvulsant drug 1 Adolescents and adults may also benefit from the diet though compliance with oral diet vs tube fed remains a problem 20 Trial design Early studies reported high success rates in one study in 1925 60 of patients became seizure free and another 35 of patients had a 50 reduction in seizure frequency These studies generally examined a cohort of patients recently treated by the physician a retrospective study and selected patients who had successfully maintained the dietary restrictions However these studies are difficult to compare to modern trials One reason is that these older trials suffered from selection bias as they excluded patients who were unable to start or maintain the diet and thereby selected from patients who would generate better results In an attempt to control for this bias modern study design prefers a prospective cohort the patients in the study are chosen before therapy begins in which the results are presented for all patients regardless of whether they started or completed the treatment known as intent to treat analysis 21 Another difference between older and newer studies is that the type of patients treated with the ketogenic diet has changed over time When first developed and used the ketogenic diet was not a treatment of last resort in contrast the children in modern studies have already tried and failed a number of anticonvulsant drugs so may be assumed to have more difficult to treat epilepsy Early and modern studies also differ because the treatment protocol has changed In older protocols the diet was initiated with a prolonged fast designed to lose 5 10 body weight and heavily restricted the calorie intake Concerns over child health and growth led to a relaxation of the diet s restrictions 21 Fluid restriction was once a feature of the diet but this led to increased risk of constipation and kidney stones and is no longer considered beneficial 18 Outcomes A study with an intent to treat prospective design was published in 1998 by a team from the Johns Hopkins Hospital 22 and followed up by a report published in 2001 23 As with most studies of the ketogenic diet no control group patients who did not receive the treatment was used The study enrolled 150 children After three months 83 of them were still on the diet 26 had experienced a good reduction in seizures 31 had had an excellent reduction and 3 were seizure free Note 7 At 12 months 55 were still on the diet 23 had a good response 20 had an excellent response and 7 were seizure free Those who had discontinued the diet by this stage did so because it was ineffective too restrictive or due to illness and most of those who remained were benefiting from it The percentage of those still on the diet at two three and four years was 39 20 and 12 respectively During this period the most common reason for discontinuing the diet was because the children had become seizure free or significantly better At four years 16 of the original 150 children had a good reduction in seizure frequency 14 had an excellent reduction and 13 were seizure free though these figures include many who were no longer on the diet Those remaining on the diet after this duration were typically not seizure free but had had an excellent response 23 24 It is possible to combine the results of several small studies to produce evidence that is stronger than that available from each study alone a statistical method known as meta analysis One of four such analyses conducted in 2006 looked at 19 studies on a total of 1 084 patients 25 It concluded that a third achieved an excellent reduction in seizure frequency and half the patients achieved a good reduction 18 A Cochrane systematic review in 2018 found and analysed eleven randomized controlled trials of ketogenic diet in people with epilepsy for whom drugs failed to control their seizures 2 Six of the trials compared a group assigned to a ketogenic diet with a group not assigned to one The other trials compared types of diets or ways of introducing them to make them more tolerable 2 In the largest trial of the ketogenic diet with a non diet control 16 nearly 38 of the children and young people had half or fewer seizures with the diet compared 6 with the group not assigned to the diet Two large trials of the Modified Atkins Diet compared to a non diet control had similar results with over 50 of children having half or fewer seizures with the diet compared to around 10 in the control group 2 A systematic review in 2018 looked at 16 studies on the ketogenic diet in adults It concluded that the treatment was becoming more popular for that group of patients that the efficacy in adults was similar to children the side effects relatively mild However many patients gave up the diet for various reasons and the quality of evidence was inferior to studies on children Health issues include high levels of low density lipoprotein high total cholesterol and weight loss 26 Indications and contraindications nbsp Experts on the ketogenic diet recommend it be strongly considered for children with uncontrolled epilepsy who have tried and failed two anticonvulsant drugs 19 most children who start the ketogenic diet have failed at least three times this number 27 The ketogenic diet is indicated as an adjunctive additional treatment in children and young people with drug resistant epilepsy 28 29 It is approved by national clinical guidelines in Scotland 29 England and Wales 28 and reimbursed by nearly all US insurance companies 30 Children with a focal lesion a single point of brain abnormality causing the epilepsy who would make suitable candidates for surgery are more likely to become seizure free with surgery than with the ketogenic diet 19 31 About a third of epilepsy centres that offer the ketogenic diet also offer a dietary therapy to adults The two less restrictive dietary variants the low glycaemic index treatment and the modified Atkins diet are more appropriate for adolescents and adults mainly due to better adherence 19 A liquid form of the ketogenic diet is particularly easy to prepare for and well tolerated by infants on formula and by others who are tube fed 5 32 19 Advocates for the diet recommend that it be seriously considered after two medications have failed as the chance of other drugs succeeding is only 10 19 33 34 The diet is recommended earlier for some epilepsy and genetic syndromes where it has shown particular usefulness These include Dravet syndrome infantile spasms myoclonic astatic epilepsy tuberous sclerosis complex and for children fed by gastrostomy tube 19 35 A survey in 2005 of 88 paediatric neurologists in the US found that 36 regularly prescribed the diet after three or more drugs had failed 24 occasionally prescribed the diet as a last resort 24 had only prescribed the diet in a few rare cases and 16 had never prescribed the diet Several possible explanations exist for this gap between evidence and clinical practice 36 One major factor may be the lack of adequately trained dietitians who are needed to administer a ketogenic diet programme 33 Because the ketogenic diet alters the body s metabolism it is a first line therapy in children with certain congenital metabolic diseases such as pyruvate dehydrogenase E1 deficiency and glucose transporter 1 deficiency syndrome 37 which prevent the body from using carbohydrates as fuel leading to a dependency on ketone bodies The ketogenic diet is beneficial in treating the seizures and some other symptoms in these diseases and is an absolute indication 38 However it is absolutely contraindicated in the treatment of other diseases such as pyruvate carboxylase deficiency porphyria and other rare genetic disorders of fat metabolism 19 Persons with a disorder of fatty acid oxidation are unable to metabolise fatty acids which replace carbohydrates as the major energy source on the diet On the ketogenic diet their bodies would consume their own protein stores for fuel leading to ketoacidosis and eventually coma and death 39 InteractionsThe ketogenic diet is usually initiated in combination with the patient s existing anticonvulsant regimen though patients may be weaned off anticonvulsants if the diet is successful Some evidence of synergistic benefits is seen when the diet is combined with the vagus nerve stimulator or with the drug zonisamide and that the diet may be less successful in children receiving phenobarbital 18 Adverse effectsThe ketogenic diet is not considered a benign holistic or all natural treatment As with any serious medical therapy it may result in complications although these are generally less severe and less frequent than with anticonvulsant medication or surgery 30 Common but easily treatable short term side effects include constipation low grade acidosis and hypoglycaemia if an initial fast is undertaken Raised levels of lipids in the blood affect up to 60 of children 40 and cholesterol levels may increase by around 30 30 This can be treated by changes to the fat content of the diet such as from saturated fats towards polyunsaturated fats and if persistent by lowering the ketogenic ratio 40 Supplements are necessary to counter the dietary deficiency of many micronutrients 18 Long term use of the ketogenic diet in children increases the risk of slowed or stunted growth bone fractures and kidney stones 18 The diet reduces levels of insulin like growth factor 1 which is important for childhood growth Like many anticonvulsant drugs the ketogenic diet has an adverse effect on bone health Many factors may be involved such as acidosis and suppressed growth hormone 40 About one in 20 children on the ketogenic diet develop kidney stones compared with one in several thousand for the general population A class of anticonvulsants known as carbonic anhydrase inhibitors topiramate zonisamide are known to increase the risk of kidney stones but the combination of these anticonvulsants and the ketogenic diet does not appear to elevate the risk above that of the diet alone 41 The stones are treatable and do not justify discontinuation of the diet 41 Around half of clinics gives oral potassium citrate supplements empirically to all ketogenic diet patients with some evidence that this reduces the incidence of stone formation However has not been tested in a prospective controlled trial 19 Kidney stone formation nephrolithiasis is associated with the diet for four reasons 41 Excess calcium in the urine hypercalciuria occurs due to increased bone demineralisation with acidosis Bones are mainly composed of calcium phosphate The phosphate reacts with the acid and the calcium is excreted by the kidneys 41 Hypocitraturia the urine has an abnormally low concentration of citrate which normally helps to dissolve free calcium 41 The urine has a low pH which stops uric acid from dissolving leading to crystals that act as a nidus for calcium stone formation 41 Many institutions traditionally restricted the water intake of patients on the diet to 80 of normal daily needs 41 this practice is no longer encouraged 18 In adolescent and adults common side effects reported include weight loss constipation dyslipidemia and in women dysmenorrhea 42 ImplementationThe ketogenic diet is a medical nutrition therapy that involves participants from various disciplines Team members include a registered paediatric dietitian who coordinates the diet programme a paediatric neurologist who is experienced in offering the ketogenic diet and a registered nurse who is familiar with childhood epilepsy Additional help may come from a medical social worker who works with the family and a pharmacist who can advise on the carbohydrate content of medicines Lastly the parents and other caregivers must be educated in many aspects of the diet for it to be safely implemented 5 Implementing the diet can present difficulties for caregivers and the patient due to the time commitment involved in measuring and planning meals Since any unplanned eating can potentially break the nutritional balance required some people find the discipline needed to maintain the diet challenging and unpleasant Some people terminate the diet or switch to a less demanding diet like the modified Atkins diet or the low glycaemic index treatment diet because they find the difficulties too great 43 Initiation The Johns Hopkins Hospital protocol for initiating the classic ketogenic diet has been widely adopted 44 It involves a consultation with the patient and their caregivers and later a short hospital admission 21 Because of the risk of complications during ketogenic diet initiation most centres begin the diet under close medical supervision in the hospital 19 At the initial consultation patients are screened for conditions that may contraindicate the diet A dietary history is obtained and the parameters of the diet selected the ketogenic ratio of fat to combined protein and carbohydrate Note 8 the calorie requirements and the fluid intake 21 The day before admission to hospital the proportion of carbohydrate in the diet may be decreased and the patient begins fasting after his or her evening meal 21 On admission only calorie and caffeine free fluids 39 are allowed until dinner which consists of eggnog Note 9 restricted to one third of the typical calories for a meal The following breakfast and lunch are similar and on the second day the eggnog dinner is increased to two thirds of a typical meal s caloric content By the third day dinner contains the full calorie quota and is a standard ketogenic meal not eggnog After a ketogenic breakfast on the fourth day the patient is discharged Where possible the patient s current medicines are changed to carbohydrate free formulations 21 When in the hospital glucose levels are checked several times daily and the patient is monitored for signs of symptomatic ketosis which can be treated with a small quantity of orange juice Lack of energy and lethargy are common but disappear within two weeks 17 The parents attend classes over the first three full days which cover nutrition managing the diet preparing meals avoiding sugar and handling illness 21 The level of parental education and commitment required is higher than with medication 45 Variations on the Johns Hopkins protocol are common The initiation can be performed using outpatient clinics rather than requiring a stay in hospital Often no initial fast is used fasting increases the risk of acidosis hypoglycaemia and weight loss Rather than increasing meal sizes over the three day initiation some institutions maintain meal size but alter the ketogenic ratio from 2 1 to 4 1 19 For patients who benefit half achieve a seizure reduction within five days if the diet starts with an initial fast of one to two days three quarters achieve a reduction within two weeks and 90 achieve a reduction within 23 days If the diet does not begin with a fast the time for half of the patients to achieve an improvement is longer two weeks but the long term seizure reduction rates are unaffected 45 Parents are encouraged to persist with the diet for at least three months before any final consideration is made regarding efficacy 19 Maintenance After initiation the child regularly visits the hospital outpatient clinic where they are seen by the dietitian and neurologist and various tests and examinations are performed These are held every three months for the first year and then every six months thereafter Infants under one year old are seen more frequently with the initial visit held after just two to four weeks 46 A period of minor adjustments is necessary to ensure consistent ketosis is maintained and to better adapt the meal plans to the patient This fine tuning is typically done over the telephone with the hospital dietitian 21 and includes changing the number of calories altering the ketogenic ratio or adding some MCT or coconut oils to a classic diet 18 Urinary ketone levels are checked daily to detect whether ketosis has been achieved and to confirm that the patient is following the diet though the level of ketones does not correlate with an anticonvulsant effect 21 This is performed using ketone test strips containing nitroprusside which change colour from buff pink to maroon in the presence of acetoacetate one of the three ketone bodies 47 A short lived increase in seizure frequency may occur during illness or if ketone levels fluctuate The diet may be modified if seizure frequency remains high or the child is losing weight 21 Loss of seizure control may come from unexpected sources Even sugar free food can contain carbohydrates such as maltodextrin sorbitol starch and fructose The sorbitol content of suntan lotion and other skincare products may be high enough for some to be absorbed through the skin and thus negate ketosis 33 Discontinuation About 20 of children on the ketogenic diet achieve freedom from seizures and many are able to reduce the use of anticonvulsant drugs or eliminate them altogether 18 Commonly at around two years on the diet or after six months of being seizure free the diet may be gradually discontinued over two or three months This is done by lowering the ketogenic ratio until urinary ketosis is no longer detected and then lifting all calorie restrictions 48 This timing and method of discontinuation mimics that of anticonvulsant drug therapy in children where the child has become seizure free When the diet is required to treat certain metabolic diseases the duration will be longer The total diet duration is up to the treating ketogenic diet team and parents durations up to 12 years have been studied and found beneficial 46 Children who discontinue the diet after achieving seizure freedom have about a 20 risk of seizures returning The length of time until recurrence is highly variable but averages two years This risk of recurrence compares with 10 for resective surgery where part of the brain is removed and 30 50 for anticonvulsant therapy Of those who have a recurrence just over half can regain freedom from seizures either with anticonvulsants or by returning to the ketogenic diet Recurrence is more likely if despite seizure freedom an electroencephalogram shows epileptiform spikes which indicate epileptic activity in the brain but are below the level that will cause a seizure Recurrence is also likely if an MRI scan shows focal abnormalities for example as in children with tuberous sclerosis Such children may remain on the diet longer than average and children with tuberous sclerosis who achieve seizure freedom could remain on the ketogenic diet indefinitely 48 VariantsClassic nbsp The ratio of calorific contributions from food components of four diets by weightThe ketogenic diet is calculated by a dietitian for each child Age weight activity levels culture and food preferences all affect the meal plan First the energy requirements are set at 80 90 of the recommended daily amounts RDA for the child s age the high fat diet requires less energy to process than a typical high carbohydrate diet Highly active children or those with muscle spasticity require more food energy than this immobile children require less The ketogenic ratio of the diet compares the weight of fat to the combined weight of carbohydrate and protein This is typically 4 1 but children who are younger than 18 months older than 12 years or who are obese may be started on a 3 1 ratio Fat is energy rich with 9 kcal g 38 kJ g compared to 4 kcal g 17 kJ g for carbohydrate or protein so portions on the ketogenic diet are smaller than normal The quantity of fat in the diet can be calculated from the overall energy requirements and the chosen ketogenic ratio Next the protein levels are set to allow for growth and body maintenance and are around 1 g protein for each kg of body weight Lastly the amount of carbohydrate is set according to what allowance is left while maintaining the chosen ratio Any carbohydrate in medications or supplements must be subtracted from this allowance The total daily amount of fat protein and carbohydrate is then evenly divided across the meals 39 A computer program such as KetoCalculator may be used to help generate recipes 49 The meals often have four components heavy whipping cream a protein rich food typically meat a fruit or vegetable and a fat such as butter vegetable oil or mayonnaise Only low carbohydrate fruits and vegetables are allowed which excludes bananas potatoes peas and corn Suitable fruits are divided into two groups based on the amount of carbohydrate they contain and vegetables are similarly divided into two groups Foods within each of these four groups may be freely substituted to allow for variation without needing to recalculate portion sizes For example cooked broccoli Brussels sprouts cauliflower and green beans are all equivalent Fresh canned or frozen foods are equivalent but raw and cooked vegetables differ and processed foods are an additional complication Parents are required to be precise when measuring food quantities on an electronic scale accurate to 1 g The child must eat the whole meal and cannot have extra portions any snacks must be incorporated into the meal plan A small amount of MCT oil may be used to help with constipation or to increase ketosis 39 The classic ketogenic diet is not a balanced diet and only contains tiny portions of fresh fruit and vegetables fortified cereals and calcium rich foods In particular the B vitamins calcium and vitamin D must be artificially supplemented This is achieved by taking two sugar free supplements designed for the patient s age a multivitamin with minerals and calcium with vitamin D 18 A typical day of food for a child on a 4 1 ratio 1 500 kcal 6 300 kJ ketogenic diet comprises three small meals and three small snacks 30 Sample meal plan for one day Meal Menu idea IngredientsBreakfast Egg with bacon 28 g egg about half an egg 11 g bacon about half a slice 37 g of 36 heavy whipping cream 23 g butter 9 g slice of apple about 5 of one apple Morning snack Peanut butter ball serving size 0 5 ounce 6 g peanut butter 9 g butterLunch Tuna salad 28 g tuna fish 30 g mayonnaise 10 g celery 36 g of 36 heavy whipping cream 15 g lettuce one large leaf Afternoon snack Keto yogurt serving size 1 3 ounces 18 g of 36 heavy whipping cream 17 g sour cream 4 g strawberries about half of one small strawberry artificial sweetenerDinner Cheeseburger no bun 22 g minced ground beef 10 g American cheese half a slice of cheese 26 g butter 38 g of 36 heavy whipping cream 10 g lettuce one medium leaf 11 g green beans one spoonful Evening snack Keto custard serving size 1 2 ounces 25 g of 36 heavy whipping cream 9 g egg half a tablespoon Pure unsweetened vanilla flavouringMCT oil Normal dietary fat contains mostly long chain triglycerides LCTs Medium chain triglycerides MCTs are more ketogenic than LCTs because they generate more ketones per unit of energy when metabolised Their use allows for a diet with a lower proportion of fat and a greater proportion of protein and carbohydrate 18 leading to more food choices and larger portion sizes 4 The original MCT diet developed by Peter Huttenlocher in the 1970s derived 60 of its calories from MCT oil 15 Consuming that quantity of MCT oil caused abdominal cramps diarrhoea and vomiting in some children A figure of 45 is regarded as a balance between achieving good ketosis and minimising gastrointestinal complaints The classical and modified MCT ketogenic diets are equally effective and differences in tolerability are not statistically significant 46 The MCT diet is less popular in the United States MCT oil is more expensive than other dietary fats and is not covered by insurance companies 18 Modified Atkins First reported in 2003 the idea of using a form of the Atkins diet to treat epilepsy came about after parents and patients discovered that the induction phase of the Atkins diet controlled seizures The ketogenic diet team at Johns Hopkins Hospital modified the Atkins diet by removing the aim of achieving weight loss extending the induction phase indefinitely and specifically encouraging fat consumption Compared with the ketogenic diet the modified Atkins diet MAD places no limit on calories or protein and the lower overall ketogenic ratio about 1 1 does not need to be consistently maintained by all meals of the day The MAD does not begin with a fast or with a stay in hospital and requires less dietitian support than the ketogenic diet Carbohydrates are initially limited to 10 g per day in children or 20 g per day in adults and are increased to 20 30 g per day after a month or so depending on the effect on seizure control or tolerance of the restrictions Like the ketogenic diet the MAD requires vitamin and mineral supplements and children are carefully and periodically monitored at outpatient clinics 50 The modified Atkins diet reduces seizure frequency by more than 50 in 43 of patients who try it and by more than 90 in 27 of patients 18 While the strength of evidence is low for the modified Atkins it has been known to show seizure freedom in some infants 51 Few adverse effects have been reported though cholesterol is increased and the diet has not been studied long term 50 Although based on a smaller data set 126 adults and children from 11 studies over five centres these results from 2009 compare favorably with the traditional ketogenic diet 18 Low glycemic index treatment The low glycemic index treatment LGIT 52 is an attempt to achieve the stable blood glucose levels seen in children on the classic ketogenic diet while using a much less restrictive regimen The hypothesis is that stable blood glucose may be one of the mechanisms of action involved in the ketogenic diet 46 which occurs because the absorption of the limited carbohydrates is slowed by the high fat content 5 Although it is also a high fat diet with approximately 60 calories from fat 5 Note 8 the LGIT allows more carbohydrate than either the classic ketogenic diet or the modified Atkins diet approximately 40 60 g per day 18 However the types of carbohydrates consumed are restricted to those that have a glycaemic index lower than 50 Like the modified Atkins diet the LGIT is initiated and maintained at outpatient clinics and does not require precise weighing of food or intensive dietitian support Both are offered at most centres that run ketogenic diet programmes and in some centres they are often the primary dietary therapy for adolescents 46 Short term results for the LGIT indicate that at one month approximately half of the patients experience a greater than 50 reduction in seizure frequency with overall figures approaching that of the ketogenic diet The data coming from one centre s experience with 76 children up to the year 2009 also indicate fewer side effects than the ketogenic diet and that it is better tolerated with more palatable meals 18 53 Prescribed formulations nbsp Measuring KetoCal a powdered formula for administering the classic ketogenic dietInfants and patients fed via a gastrostomy tube can also be given a ketogenic diet Parents make up a prescribed powdered formula such as KetoCal into a liquid feed 21 Gastrostomy feeding avoids any issues with palatability and bottle fed infants readily accept the ketogenic formula 33 Some studies have found this liquid feed to be more efficacious and associated with lower total cholesterol than a solid ketogenic diet 18 KetoCal is a nutritionally complete food containing milk protein and is supplemented with amino acids fat carbohydrate vitamins minerals and trace elements It is used to administer the 4 1 ratio classic ketogenic diet in children over one year The formula is available in both 3 1 and 4 1 ratios either unflavoured or in an artificially sweetened vanilla flavour and is suitable for tube or oral feeding 54 Other formula products include KetoVolve 55 and Ketonia 56 Alternatively a liquid ketogenic diet may be produced by combining Ross Carbohydrate Free soy formula with Microlipid and Polycose 56 Worldwide In theory there are no restrictions on where the ketogenic diet might be used and it can cost less than modern anticonvulsants However fasting and dietary changes are affected by religious and cultural issues A culture where food is often prepared by grandparents or hired help means more people must be educated about the diet When families dine together sharing the same meal it can be difficult to separate the child s meal In many countries food labelling is not mandatory so calculating macronutrients such as fat protein and carbohydrates can be difficult In some countries it may be hard to find sugar free forms of medicines and supplements to purchase an accurate electronic scale or to afford MCT oils 57 In Asia the traditional diet includes rice and noodles as the main source of energy making their elimination difficult Therefore the MCT oil form of the diet which allows more carbohydrate has proved useful In India religious beliefs commonly affect the diet for instance Hindus consider cows sacred animals not to be killed and eaten Islam forbids consumption of pork and strict vegetarians of the Jain faith do not eat root vegetables The Indian ketogenic diet is started without a fast due to cultural opposition towards fasting in children The low fat high carbohydrate nature of the normal Indian and Asian diet means that their ketogenic diets typically have a lower ketogenic ratio 1 1 than in America and Europe However they appear to be just as effective 57 In many developing countries the ketogenic diet is expensive because dairy fats and meat are more expensive than grain fruit and vegetables The modified Atkins diet has been proposed as a lower cost alternative for those countries the slightly more expensive food bill can be offset by a reduction in pharmaceutical costs if the diet is successful The modified Atkins diet is less complex to explain and prepare and requires less support from a dietitian 58 Mechanism of actionSeizure pathology Ketone bodies nbsp b hydroxybutyrate nbsp acetoacetic acid nbsp acetone The brain is composed of a network of neurons that transmit signals by propagating nerve impulses The propagation of this impulse from one neuron to another is typically controlled by neurotransmitters though there are also electrical pathways between some neurons Neurotransmitters can inhibit impulse firing primarily done by g aminobutyric acid or GABA or they can excite the neuron into firing primarily done by glutamate A neuron that releases inhibitory neurotransmitters from its terminals is called an inhibitory neuron while one that releases excitatory neurotransmitters is an excitatory neuron When the normal balance between inhibition and excitation is significantly disrupted in all or part of the brain a seizure can occur The GABA system is an important target for anticonvulsant drugs since seizures may be discouraged by increasing GABA synthesis decreasing its breakdown or enhancing its effect on neurons 7 The nerve impulse is characterised by a great influx of sodium ions through channels in the neuron s cell membrane followed by an efflux of potassium ions through other channels The neuron is unable to fire again for a short time known as the refractory period which is mediated by another potassium channel The flow through these ion channels is governed by a gate which is opened by either a voltage change or a chemical messenger known as a ligand such as a neurotransmitter These channels are another target for anticonvulsant drugs 7 There are many ways in which epilepsy occurs Examples of pathological physiology include unusual excitatory connections within the neuronal network of the brain abnormal neuron structure leading to altered current flow decreased inhibitory neurotransmitter synthesis ineffective receptors for inhibitory neurotransmitters insufficient breakdown of excitatory neurotransmitters leading to excess immature synapse development and impaired function of ionic channels 7 Seizure control Although many hypotheses have been put forward to explain how the ketogenic diet works it remains a mystery Disproven hypotheses include systemic acidosis high levels of acid in the blood electrolyte changes and hypoglycaemia low blood glucose 21 Although many biochemical changes are known to occur in the brain of a patient on the ketogenic diet it is not known which of these has an anticonvulsant effect The lack of understanding in this area is similar to the situation with many anticonvulsant drugs 59 On the ketogenic diet carbohydrates are restricted and so cannot provide for all the metabolic needs of the body Instead fatty acids are used as the major source of fuel These are used through fatty acid oxidation in the cell s mitochondria the energy producing parts of the cell Humans can convert some amino acids into glucose by a process called gluconeogenesis but cannot do this by using fatty acids 60 Since amino acids are needed to make proteins which are essential for growth and repair of body tissues these cannot be used only to produce glucose This could pose a problem for the brain since it is normally fuelled solely by glucose and most fatty acids do not cross the blood brain barrier However the liver can use long chain fatty acids to synthesise the three ketone bodies b hydroxybutyrate acetoacetate and acetone These ketone bodies enter the brain and partially substitute for blood glucose as a source of energy 59 The ketone bodies are possibly anticonvulsant in animal models acetoacetate and acetone protect against seizures The ketogenic diet results in adaptive changes to brain energy metabolism that increase the energy reserves ketone bodies are a more efficient fuel than glucose and the number of mitochondria is increased This may help the neurons to remain stable in the face of increased energy demand during a seizure and may confer a neuroprotective effect 59 The ketogenic diet has been studied in at least 14 rodent animal models of seizures It is protective in many of these models and has a different protection profile than any known anticonvulsant Conversely fenofibrate not used clinically as an antiepileptic exhibits experimental anticonvulsant properties in adult rats comparable to the ketogenic diet 61 This together with studies showing its efficacy in patients who have failed to achieve seizure control on half a dozen drugs suggests a unique mechanism of action 59 Anticonvulsants suppress epileptic seizures but they neither cure nor prevent the development of seizure susceptibility The development of epilepsy epileptogenesis is a process that is poorly understood A few anticonvulsants valproate levetiracetam and benzodiazepines have shown antiepileptogenic properties in animal models of epileptogenesis However no anticonvulsant has ever achieved this in a clinical trial in humans The ketogenic diet has been found to have antiepileptogenic properties in rats 59 Other medical applicationsThe ketogenic diet has been studied for potential therapeutic use in various neurological disorders other than epilepsy Alzheimer s disease AD 62 amyotrophic lateral sclerosis ALS autism headache neurotrauma pain Parkinson s disease PD and sleep disorders 6 As of 2022 there is no clinical evidence that a ketogenic diet is effective to treat cancer 63 See also nbsp Medicine portal nbsp Food portalList of dietsExplanatory notes In this article kcal stands for calories as a unit of measure 4 1868 kJ and calories stands for energy from food Unless otherwise stated the term fasting in this article refers to going without food while maintaining calorie free fluid intake Hippocrates On the Sacred Disease ch 18 vol 6 Hippocrates Epidemics VII 46 vol 5 Galen De venae sect adv Erasistrateos Romae degentes c 8 vol 11 Galen De victu attenuante c 1 A good reduction is defined here to mean a 50 90 decrease in seizure frequency An excellent reduction is a 90 99 decrease a b The ketogenic ratio k can be converted to the portion of calories from fat f using the Atwater coefficients of 9 and 4 kcal g for fat and combined carbohydrate and water respectively The equation is f 9 k 9 k 4 For example a 4 1 diet derives 90 of calories from fat The inverse equation is k 4 f 9 1 f Ketogenic eggnog is used during induction and is a drink with the required ketogenic ratio For example a 4 1 ratio eggnog would contain 60 g of 36 heavy whipping cream 25 g pasteurised raw egg saccharin and vanilla flavour This contains 245 kcal 1 025 kJ 4 g protein 2 g carbohydrate and 24 g fat 24 6 4 1 17 The eggnog may also be cooked to make a custard or frozen to make ice cream 39 References a b c d e f g h i Freeman JM Kossoff EH Hartman AL The ketogenic diet one decade later Pediatrics 2007 Mar 119 3 535 543 doi 10 1542 peds 2006 2447 PMID 17332207 a b c d Martin McGill KJ Jackson CF Bresnahan R Levy RG Cooper PN Ketogenic diets for drug resistant epilepsy Cochrane Database Syst Rev 2018 Nov 7 11 CD001903 doi 10 1002 14651858 CD001903 pub4 PMID 30403286 Kossoff EH Wang HS Dietary therapies for epilepsy Biomed J 2013 Jan Feb 36 1 2 8 doi 10 4103 2319 4170 107152 PMID 23515147 a b Liu YM Medium chain triglyceride MCT ketogenic therapy Epilepsia 2008 Nov 49 Suppl 8 33 36 doi 10 1111 j 1528 1167 2008 01830 x PMID 19049583 a b c d e Zupec Kania BA Spellman E An overview of the ketogenic diet for pediatric epilepsy Nutr Clin Pract 2008 Dec 2009 Jan 23 6 589 596 doi 10 1177 0884533608326138 PMID 19033218 a b Gano LB Patel M Rho JM Ketogenic diets mitochondria and neurological diseases J Lipid Res 2014 Nov 55 11 2211 2228 doi 10 1194 jlr R048975 PMID 24847102 a b c d e Stafstrom CE An introduction to seizures and epilepsy In Stafstrom CE Rho JM editors Epilepsy and the ketogenic diet Totowa Humana Press 2004 ISBN 1588292959 de Boer HM Mula M Sander JW The global burden and stigma of epilepsy Epilepsy Behav 2008 May 12 4 540 546 doi 10 1016 j yebeh 2007 12 019 PMID 18280210 Cai QY Zhou ZJ Luo R Gan J Li SP Mu DZ Wan CM Safety and tolerability of the ketogenic diet used for the treatment of refractory childhood epilepsy a systematic review of published prospective studies World J Pediatr 2017 Dec 13 6 528 536 doi 10 1007 s12519 017 0053 2 PMID 28702868 a b c d e f g h i Wheless JW History and origin of the ketogenic diet PDF In Stafstrom CE Rho JM editors Epilepsy and the ketogenic diet Totowa Humana Press 2004 ISBN 1588292959 Temkin O The falling sickness a history of epilepsy from the Greeks to the beginnings of modern neurology 2nd ed Baltimore Johns Hopkins University Press 1971 pp 33 57 66 67 71 78 ISBN 0801848490 Guelpa G Marie A La lutte contre l epilepsie par la desintoxication et par la reeducation alimentaire Rev Ther med Chirurg 1911 78 8 13 As cited by Bailey 2005 Bailey EE Pfeifer HH Thiele EA The use of diet in the treatment of epilepsy Epilepsy Behav 2005 Feb 6 1 4 8 doi 10 1016 j yebeh 2004 10 006 PMID 15652725 Kossoff EH Do ketogenic diets work for adults with epilepsy Yes epilepsy com 2007 March Cited 24 October 2009 a b c Huttenlocher PR Wilbourn AJ Signore JM Medium chain triglycerides as a therapy for intractable childhood epilepsy Neurology 1971 Nov 21 11 1097 1103 doi 10 1212 wnl 21 11 1097 PMID 5166216 a b Neal EG Chaffe H Schwartz RH Lawson MS Edwards N Fitzsimmons G et al The ketogenic diet for the treatment of childhood epilepsy a randomised controlled trial Lancet Neurol 2008 Jun 7 6 500 506 doi 10 1016 S1474 4422 08 70092 9 PMID 18456557 a b c Vining EP Freeman JM Ballaban Gil K Camfield CS Camfield PR Holmes GL et al A multicenter study of the efficacy of the ketogenic diet Arch Neurol 1998 Nov 55 11 1433 1437 doi 10 1001 archneur 55 11 1433 PMID 9823827 a b c d e f g h i j k l m n o p q Kossoff EH Zupec Kania BA Rho JM Ketogenic diets an update for child neurologists J Child Neurol 2009 Aug 24 8 979 988 doi 10 1177 0883073809337162 PMID 19535814 a b c d e f g h i j k l Kossoff EH Zupec Kania BA Auvin S Ballaban Gil KR Christina Bergqvist AG Blackford R Buchhalter JR Caraballo RH Cross JH Dahlin MG Donner EJ Guzel O Jehle RS Klepper J Kang HC Lambrechts DA Liu YMC Nathan JK Nordli DR Jr Pfeifer HH Rho JM Scheffer IE Sharma S Stafstrom CE Thiele EA Turner Z Vaccarezza MM van der Louw EJTM Veggiotti P Wheless JW Wirrell EC Charlie Foundation Matthew s Friends Practice Committee of the Child Neurology Society Optimal clinical management of children receiving dietary therapies for epilepsy Updated recommendations of the International Ketogenic Diet Study Group Epilepsia Open 2018 May 21 3 2 175 192 doi 10 1002 epi4 12225 PMID 29881797 Husari KS Cervenka MC The ketogenic diet all grown up Ketogenic diet therapies for adults Epilepsy Res 2020 May 162 106319 doi 10 1016 j eplepsyres 2020 106319 PMID 32199222 a b c d e f g h i j k l Hartman AL Vining EP Clinical aspects of the ketogenic diet Epilepsia 2007 Jan 48 1 31 42 doi 10 1111 j 1528 1167 2007 00914 x PMID 17241206 Freeman JM Vining EP Pillas DJ Pyzik PL Casey JC Kelly LM The efficacy of the ketogenic diet 1998 a prospective evaluation of intervention in 150 children Pediatrics 1998 Dec 102 6 1358 1363 doi 10 1542 peds 102 6 1358 PMID 9832569 Lay summary JHMI Office of Communications and Public Affairs Updated 7 December 1998 Cited 6 March 2008 a b Hemingway C Freeman JM Pillas DJ Pyzik PL The ketogenic diet a 3 to 6 year follow up of 150 children enrolled prospectively Pediatrics 2001 Oct 108 4 898 905 doi 10 1542 peds 108 4 898 PMID 11581442 Kossoff EH Rho JM Ketogenic diets evidence for short and long term efficacy Neurotherapeutics 2009 Apr 6 2 406 414 doi 10 1016 j nurt 2009 01 005 PMID 19332337 Henderson CB Filloux FM Alder SC Lyon JL Caplin DA Efficacy of the ketogenic diet as a treatment option for epilepsy meta analysis J Child Neurol 2006 Mar 21 3 193 198 doi 10 2310 7010 2006 00044 PMID 16901419 Liu H Yang Y Wang Y Tang H Zhang F Zhang Y Zhao Y Ketogenic diet for treatment of intractable epilepsy in adults A meta analysis of observational studies Epilepsia Open 2018 Feb 19 3 1 9 17 doi 10 1002 epi4 12098 PMID 29588983 Bergqvist AGC Indications and Contraindications of the Ketogenic diet In Stafstrom CE Rho JM editors Epilepsy and the ketogenic diet Totowa Humana Press 2004 pp 53 61 ISBN 1588292959 a b Epilepsies diagnosis and management National Institute for Health and Care Excellence NICE Published January 2012 Updated February 2016 Cited March 2018 ISBN 978 1473117907 a b Scottish Intercollegiate Guidelines Network Guideline 81 Diagnosis and management of epilepsies in children and young people A national clinical guideline PDF Edinburgh Royal College of Physicians 2005 ISBN 1899893245 a b c d Turner Z Kossoff EH The ketogenic and Atkins diets recipes for seizure control PDF Pract Gastroenterol 2006 Jun 29 6 53 56 58 61 62 64 Stainman RS Turner Z Rubenstein JE Kossoff EH Decreased relative efficacy of the ketogenic diet for children with surgically approachable epilepsy Seizure 2007 Oct 16 7 615 619 doi 10 1016 j seizure 2007 04 010 PMID 17544706 Kossoff EH McGrogan JR Freeman JM Benefits of an all liquid ketogenic diet Epilepsia 2004 Sep 45 9 1163 doi 10 1111 j 0013 9580 2004 18504 x PMID 15329084 a b c d Kossoff EH Freeman JM The ketogenic diet the physician s perspective In Stafstrom CE Rho JM editors Epilepsy and the ketogenic diet Totowa Humana Press 2004 pp 53 61 ISBN 1588292959 Spendiff S The diet that can treat epilepsy Guardian 2008 Aug 15 Sect Health amp wellbeing Wang S Fallah A Optimal management of seizures associated with tuberous sclerosis complex current and emerging options Neuropsychiatr Dis Treat 2014 Oct 23 10 2021 2030 doi 10 2147 NDT S51789 PMID 25364257 Mastriani KS Williams VC Hulsey TC Wheless JW Maria BL Evidence based versus reported epilepsy management practices J Child Neurol 2008 Feb 15 23 5 507 514 doi 10 1177 0883073807309785 PMID 18281618 Wang D Pascual JM De Vivo D Glucose Transporter Type 1 Deficiency Syndrome In Adam MP Ardinger HH Pagon RA Wallace SE Bean LJH Stephens K Amemiya A editors GeneReviews Seattle WA University of Washington Seattle 1993 2018 2002 Jul 30 updated 2018 Mar 1 PMID 20301603 Huffman J Kossoff EH State of the ketogenic diet s in epilepsy PDF Curr Neurol Neurosci Rep 2006 Jul 6 4 332 340 doi 10 1007 s11910 006 0027 6 PMID 16822355 a b c d e Zupec Kania B Werner RR Zupanc ML Clinical Use of the Ketogenic Diet The Dietitian s Role In Stafstrom CE Rho JM editors Epilepsy and the ketogenic diet Totowa Humana Press 2004 pp 63 81 ISBN 1588292959 a b c Bergqvist AG Long term monitoring of the ketogenic diet Do s and Don ts Epilepsy Res 2011 Aug 18 100 3 261 266 doi 10 1016 j eplepsyres 2011 05 020 PMID 21855296 a b c d e f g Sampath A Kossoff EH Furth SL Pyzik PL Vining EP Kidney stones and the ketogenic diet risk factors and prevention PDF J Child Neurol 2007 Apr 22 4 375 378 doi 10 1177 0883073807301926 PMID 17621514 Kossoff E Is there a role for the ketogenic diet beyond childhood In Freeman J Veggiotti P Lanzi G Tagliabue A Perucca E The ketogenic diet from molecular mechanisms to clinical effects Epilepsy Res 2006 Feb 68 2 145 180 doi 10 1016 j eplepsyres 2005 10 003 PMID 16523530 Vogelstein F Epilepsy s Big Fat Miracle The New York Times 2010 Nov 17 Kim DY Rho JM The ketogenic diet and epilepsy Curr Opin Clin Nutr Metab Care 2008 Mar 11 2 113 120 doi 10 1097 MCO 0b013e3282f44c06 PMID 18301085 a b Kossoff EH Laux LC Blackford R Morrison PF Pyzik PL Hamdy RM et al When do seizures usually improve with the ketogenic diet PDF Epilepsia 2008 Feb 49 2 329 333 doi 10 1111 j 1528 1167 2007 01417 x PMID 18028405 a b c d e Kossoff EH Zupec Kania BA Amark PE Ballaban Gil KR Bergqvist AG Blackford R et al Optimal clinical management of children receiving the ketogenic diet recommendations of the International Ketogenic Diet Study Group Epilepsia 2009 Feb 50 2 304 317 doi 10 1111 j 1528 1167 2008 01765 x PMID 18823325 Musa Veloso K Cunnane SC Measuring and interpreting ketosis and fatty acid profiles in patients on a high fat ketogenic diet In Stafstrom CE Rho JM editors Epilepsy and the ketogenic diet Totowa Humana Press 2004 pp 129 141 ISBN 1588292959 a b Martinez CC Pyzik PL Kossoff EH Discontinuing the ketogenic diet in seizure free children recurrence and risk factors Epilepsia 2007 Jan 48 1 187 190 doi 10 1111 j 1528 1167 2006 00911 x PMID 17241227 Zupec Kania B KetoCalculator a web based calculator for the ketogenic diet Epilepsia 2008 Nov 49 Suppl 8 14 16 doi 10 1111 j 1528 1167 2008 01824 x PMID 19049577 a b Kossoff EH Dorward JL The modified Atkins diet Epilepsia 2008 Nov 49 Suppl 8 37 41 doi 10 1111 j 1528 1167 2008 01831 x PMID 19049584 Treadwell Jonathan R Wu Mingche Tsou Amy Y 25 October 2022 Management of Infantile Epilepsies Report Agency for Healthcare Research and Quality AHRQ doi 10 23970 ahrqepccer252 Pfeifer Heidi H Low glycemic index treatment Epilepsy Foundation 22 August 2013 Cited 31 March 2018 Muzykewicz DA Lyczkowski DA Memon N Conant KD Pfeifer HH Thiele EA Efficacy safety and tolerability of the low glycemic index treatment in pediatric epilepsy Epilepsia 2009 May 50 5 1118 1126 doi 10 1111 j 1528 1167 2008 01959 x PMID 19220406 KetoCal Product Information Nutricia North America Cited 8 June 2018 KetoVOLVE 4 1 Ratio Powder Solace Nutrition Cited 17 June 2013 a b Kossoff EH The Ketogenic Diet in a bottle Keto News Epilepsy com Updated July 2009 Cited 29 November 2009 a b Kossoff EH McGrogan JR Worldwide use of the ketogenic diet Epilepsia 2005 Feb 46 2 280 289 doi 10 1111 j 0013 9580 2005 42704 x PMID 15679509 Kossoff EH Dorward JL Molinero MR Holden KR The modified Atkins diet a potential treatment for developing countries Epilepsia 2008 Sep 49 9 1646 1647 doi 10 1111 j 1528 1167 2008 01580 6 x PMID 18782218 a b c d e Hartman AL Gasior M Vining EP Rogawski MA The neuropharmacology of the ketogenic diet Pediatr Neurol 2007 May 36 5 281 292 doi 10 1016 j pediatrneurol 2007 02 008 PMID 17509459 Kerndt PR Naughton JL Driscoll CE Loxterkamp DA Fasting the history pathophysiology and complications West J Med 1982 Nov 137 5 379 399 PMID 6758355 Porta N Vallee L Lecointe C Bouchaert E Staels B Bordet R Auvin S Fenofibrate a peroxisome proliferator activated receptor alpha agonist exerts anticonvulsive properties Epilepsia 2009 Apr 50 4 943 948 doi 10 1111 j 1528 1167 2008 01901 x PMID 19054409 Broom GM et al The ketogenic diet as a potential treatment and prevention strategy for Alzheimer s disease Nutrition 2019 Apr 60 118 121 doi 10 1016 j nut 2018 10 003 PMID 30554068 Romer M et al The use of ketogenic diets in cancer patients a systematic review Clin Exp Med 2021 Nov 21 4 501 536 doi 10 1007 s10238 021 00710 2 PMC 8505380 PMID 33813635Further readingFreeman JM Kossoff EH Freeman JB Kelly MT The Ketogenic Diet A Treatment for Children and Others with Epilepsy 4th ed New York Demos 2007 ISBN 1932603182 Lowery R Wilson J The Ketogenic Bible The Authoritative Guide to Ketosis 1st ed Victory Belt Publishing 2017 ISBN 978 1628601046 External linksDiet Review Ketogenic Diet for Weight Loss from the Harvard University School of Public Health Ketogenic diet at Curlie Matthew s Friends a UK charity and information resource The Charlie Foundation a US charity and information resource Epilepsy com Dietary Therapies amp Ketogenic News information and regular research news updates Retrieved from https en wikipedia org w index php title Ketogenic diet amp oldid 1197457177, wikipedia, wiki, book, books, library,

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