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Cirrhosis

January 01, 1970

Cirrhosis, also known as liver cirrhosis or hepatic cirrhosis, and end-stage liver disease, is the impaired liver function caused by the formation of scar tissue known as fibrosis due to damage caused by liver disease.[6] Damage to the liver leads to repair of liver tissue and subsequent formation of scar tissue. Over time, scar tissue can replace normal functioning tissue, leading to the impaired liver function of cirrhosis.[6][7] The disease typically develops slowly over months or years.[1] Early symptoms may include tiredness, weakness, loss of appetite, unexplained weight loss, nausea and vomiting, and discomfort in the right upper quadrant of the abdomen.[8] As the disease worsens, symptoms may include itchiness, swelling in the lower legs, fluid build-up in the abdomen, jaundice, bruising easily, and the development of spider-like blood vessels in the skin.[8] The fluid build-up in the abdomen may develop into spontaneous infections.[1] More serious complications include hepatic encephalopathy, bleeding from dilated veins in the esophagus, stomach, or intestines, and liver cancer.[9] Stages of cirrhosis include compensated cirrhosis and decompensated cirrhosis.[10]

Cirrhosis
Other namesCirrhosis of the liver, hepatic cirrhosis
Cross-section of human liver with cirrhosis
Pronunciation
SpecialtyGastroenterology, Hepatology
SymptomsTiredness, itchiness, swelling in the lower legs, jaundice, easily bruising, fluid build-up in the abdomen[1]
ComplicationsSpontaneous bacterial peritonitis, hepatic encephalopathy, dilated veins in the esophagus, liver cancer[1]
Usual onsetOver months, years or decades[1]
DurationLong term[1]
CausesAlcoholic liver disease, hepatitis B, hepatitis C, non-alcoholic steatohepatitis
Diagnostic methodBlood tests, medical imaging, liver biopsy[2][1]
PreventionVaccination (such as hepatitis B), avoiding alcohol,[1] losing weight, exercising, low-carbohydrate diet, controlling hypertension and diabetes may help in those with NAFLD or NASH
TreatmentDepends on underlying cause[3]
Frequency2.8 million (2015)[4]
Deaths1.3 million (2015)[5]

Cirrhosis is most commonly caused by alcoholic liver disease, non-alcoholic steatohepatitis (NASH – the progressive form of non-alcoholic fatty liver disease),[11] heroin abuse,[12] chronic hepatitis B, and chronic hepatitis C.[8][13] Heavy drinking over a number of years can cause alcoholic liver disease.[14] Liver damage has also been attributed to heroin usage over an extended period of time as well.[15] NASH has a number of causes, including obesity, high blood pressure, abnormal levels of cholesterol, type 2 diabetes, and metabolic syndrome.[16] Less common causes of cirrhosis include autoimmune hepatitis, primary biliary cholangitis, and primary sclerosing cholangitis that disrupts bile duct function, genetic disorders such as Wilson's disease and hereditary hemochromatosis, and chronic heart failure with liver congestion.[8]

Diagnosis is based on blood tests, medical imaging, and liver biopsy.[2][1]

Hepatitis B vaccine can prevent hepatitis B and the development of cirrhosis, but no vaccination against hepatitis C is available.[1] No specific treatment for cirrhosis is known, but many of the underlying causes may be treated by a number of medications that may slow or prevent worsening of the condition.[3] Hepatitis B and C may be treatable with antiviral medications.[1] Avoiding alcohol is recommended in all cases.[1] Autoimmune hepatitis may be treated with steroid medications.[1] Ursodiol may be useful if the disease is due to blockage of the bile duct.[1] Other medications may be useful for complications such as abdominal or leg swelling, hepatic encephalopathy, and dilated esophageal veins.[1] If cirrhosis leads to liver failure, a liver transplant may be an option.[16]

Cirrhosis affected about 2.8 million people and resulted in 1.3 million deaths in 2015.[4][5] Of these deaths, alcohol caused 348,000 (27%), hepatitis C caused 326,000 (25%), and hepatitis B caused 371,000 (28%).[5] In the United States, more men die of cirrhosis than women.[1] The first known description of the condition is by Hippocrates in the fifth century BCE.[17] The term "cirrhosis" was derived in 1819 from the Greek word "kirrhos", which describes the yellowish color of a diseased liver.[18]

Signs and symptoms edit

 
Person with cirrhosis and associated pain in the right upper region of the abdomen

Cirrhosis can take quite a long time to develop, and symptoms may be slow to emerge.[8] Some early symptoms include tiredness, weakness, loss of appetite, weight loss, and nausea.[8] Early signs may also include redness on the palms known as palmer erythema.[10] People may also feel discomfort in the right upper abdomen around the liver.[8]

As cirrhosis progresses, symptoms can include neurological changes.[8] This can consist of cognitive impairments, confusion, memory loss, sleep disorders, and personality changes.[8]Steatorrhea or presence of undigested fats in stool is also a symptom of cirrhosis.[19]

Worsening cirrhosis can cause a build-up of fluid in different parts of the body such as the legs (edema) and abdomen (ascites).[8] Other signs of advancing disease include itchy skin, bruising easily, dark urine, and yellowing of the skin.[8]

Liver dysfunction edit

These features are a direct consequence of liver cells not functioning:

Portal hypertension edit

Liver cirrhosis makes it hard for blood to flow in the portal venous system.[30] This resistance creates a backup of blood and increases pressure.[30] This results in portal hypertension. Effects of portal hypertension include:

Other nonspecific signs edit

Some signs that may be present include changes in the nails (such as Muehrcke's lines, Terry's nails, and nail clubbing).[34][35] Additional changes may be seen in the hands (Dupuytren's contracture) as well as the skin/bones (hypertrophic osteoarthropathy).[24]

Advanced disease edit

As the disease progresses, complications may develop. In some people, these may be the first signs of the disease.

Causes edit

Cirrhosis has many possible causes, and more than one cause may be present. History taking is of importance in trying to determine the most likely cause.[2] Globally, 57% of cirrhosis is attributable to either hepatitis B (30%) or hepatitis C (27%).[38][39] Alcohol use disorder is another major cause, accounting for about 20–40% of the cases.[39][24]

Common causes edit

 
Hepatitis C viral particles and the liver
  • Alcoholic liver disease (ALD, or alcoholic cirrhosis) develops for 10–20% of individuals who drink heavily for a decade or more.[40] Alcohol seems to injure the liver by blocking the normal metabolism of protein, fats, and carbohydrates.[41] This injury happens through the formation of acetaldehyde from alcohol. Acetaldehyde is reactive and leads to the accumulation of other reactive products in the liver.[24] People with ALD may also have concurrent alcoholic hepatitis. Associated symptoms are fever, hepatomegaly, jaundice, and anorexia.[41] AST and ALT blood levels are both elevated, but at less than 300 IU/liter, with an AST:ALT ratio > 2.0, a value rarely seen in other liver diseases.[42] In the United States, 40% of cirrhosis-related deaths are due to alcohol.[24]
  • In non-alcoholic fatty liver disease (NAFLD), fat builds up in the liver and eventually causes scar tissue.[43] This type of disorder can be caused by obesity, diabetes, malnutrition, coronary artery disease, and steroids.[43][44] Though similar in signs to alcoholic liver disease, no history of notable alcohol use is found. Blood tests and medical imaging are used to diagnose NAFLD and NASH, and sometimes a liver biopsy is needed.[31]
  • Chronic hepatitis C, an infection with the hepatitis C virus, causes inflammation of the liver and a variable grade of damage to the organ.[36] Over several decades, this inflammation and damage can lead to cirrhosis. Among people with chronic hepatitis C, 20–30% develop cirrhosis.[36][24] Cirrhosis caused by hepatitis C and alcoholic liver disease are the most common reasons for liver transplant.[24] Both hepatitis C and hepatitis B–related cirrhosis can also be attributed with heroin addiction.[45]
  • Chronic hepatitis B causes liver inflammation and injury that over several decades can lead to cirrhosis.[36] Hepatitis D is dependent on the presence of hepatitis B and accelerates cirrhosis in co-infection.[36]

Less common causes edit

Pathophysiology edit

The liver plays a vital role in the synthesis of proteins (for example, albumin, clotting factors and complement), detoxification, and storage (for example, of vitamin A and glycogen). In addition, it participates in the metabolism of lipids and carbohydrates.[citation needed]

Cirrhosis is often preceded by hepatitis and fatty liver (steatosis), independent of the cause. If the cause is removed at this stage, the changes are fully reversible.[citation needed]

The pathological hallmark of cirrhosis is the development of scar tissue that replaces normal tissue. This scar tissue blocks the portal flow of blood through the organ, raising the blood pressure and disturbing normal function. Research has shown the pivotal role of the stellate cell, that normally stores vitamin A, in the development of cirrhosis. Damage to the liver tissue from inflammation leads to the activation of stellate cells, which increases fibrosis through the production of myofibroblasts, and obstructs hepatic blood flow.[49] In addition, stellate cells secrete TGF beta 1, which leads to a fibrotic response and proliferation of connective tissue. TGF-β1 have been implicated in the process of activating hepatic stellate cells (HSCs) with the magnitude of fibrosis being in proportion to increase in TGF β levels. ACTA2 is associated with TGF β pathway that enhances contractile properties of HSCs leading to fibrosis.[50] Furthermore, HSCs secrete TIMP1 and TIMP2, naturally occurring inhibitors of matrix metalloproteinases (MMPs), which prevent MMPs from breaking down the fibrotic material in the extracellular matrix.[51][52]

As this cascade of processes continues, fibrous tissue bands (septa) separate hepatocyte nodules, which eventually replace the entire liver architecture, leading to decreased blood flow throughout. The spleen becomes congested, and enlarged, resulting in its retention of platelets, which are needed for normal blood clotting. Portal hypertension is responsible for the most severe complications of cirrhosis.[citation needed]

Diagnosis edit

 
Caudate lobe hypertrophy on ultrasound due to cirrhosis
 
Hepatofugal (non-forward) flow in portal vein

The diagnosis of cirrhosis in an individual is based on multiple factors.[24] Cirrhosis may be suspected from laboratory findings, physical exam, and the person's medical history. Imaging is generally obtained to evaluate the liver.[24] A liver biopsy will confirm the diagnosis; however, is generally not required.[36]

Imaging edit

Ultrasound is routinely used in the evaluation of cirrhosis.[36] It may show a small and shrunken liver in advanced disease. On ultrasound, there is increased echogenicity with irregular appearing areas.[53] Other suggestive findings are an enlarged caudate lobe, widening of the fissures and enlargement of the spleen.[54] An enlarged spleen, which normally measures less than 11–12 cm (4.3–4.7 in) in adults, may suggest underlying portal hypertension.[55] Ultrasound may also screen for hepatocellular carcinoma and portal hypertension.[36] This is done by assessing flow in the hepatic vein.[56] An increased portal vein pulsatility may be seen. However, this may be a sign of elevated right atrial pressure.[57] Portal vein pulsatility are usually measured by a pulsatility indices (PI).[56] A number above a certain values indicates cirrhosis (see table below).

Pulsatility indices (PI)
Index Calculation Cutoff
Average-based (Max – Min) / Average[56] 0.5[56]
Max-relative (Max – Min) / Max[58] 0.5[58][59]–0.54[59]

Other scans include CT of the abdomen and MRI.[36] A CT scan is non-invasive and may be helpful in the diagnosis.[36] Compared to the ultrasound, CT scans tend to be more expensive. MRI provides excellent evaluation; however, is a high expense.[36]

 
Liver cirrhosis on CT imaging of the abdomen in transverse view

Cirrhosis is also diagnosable through a variety of new elastography techniques.[60][61] When a liver becomes cirrhotic it will generally become stiffer. Determining the stiffness through imaging can determine the location and severity of disease. Techniques include transient elastography, acoustic radiation force impulse imaging, supersonic shear imaging and magnetic resonance elastography.[62] Transient elastography and magnetic resonance elastography can help identify the stage of fibrosis.[63] Compared to a biopsy, elastography can sample a much larger area and is painless.[64] It shows a reasonable correlation with the severity of cirrhosis.[63] Other modalities have been introduced which are incorporated into ultrasonagraphy systems. These include 2-dimensional shear wave elastography and point shear wave elastography which uses acoustic radiation force impulse imaging.[11]

Rarely are diseases of the bile ducts, such as primary sclerosing cholangitis, causes of cirrhosis.[36] Imaging of the bile ducts, such as ERCP or MRCP (MRI of biliary tract and pancreas) may aid in the diagnosis.[36]

Lab findings edit

The best predictors of cirrhosis are ascites, platelet count < 160,000/mm3, spider angiomata, and a Bonacini cirrhosis discriminant score greater than 7 (as the sum of scores for platelet count, ALT/AST ratio and INR as per table).[65]

Bonacini score[66]
Score Platelet count x109 ALT/AST ratio INR
0 >340 >1.7 <1.1
1 280-340 1.2-1.7 1.1-1.4
2 220-279 0.6-1.19 >1.4
3 160–219 <0.6 ...
4 100-159 ... ...
5 40-99 ... ...
6 <40 ... ...

These findings are typical in cirrhosis:

  • Thrombocytopenia, typically multifactorial, is due to alcoholic marrow suppression, sepsis, lack of folate, platelet sequestering in the spleen, and decreased thrombopoietin.[42] However, this rarely results in a platelet count < 50,000/mL.[67]
  • Aminotransferases AST and ALT are moderately elevated, with AST > ALT. However, normal aminotransferase levels do not preclude cirrhosis.[42]
  • Alkaline phosphatase – slightly elevated but less than 2–3 times the upper limit of normal.[citation needed]
  • Gamma-glutamyl transferase – correlates with AP levels. Typically much higher in chronic liver disease from alcohol.[67]
  • Bilirubin levels are normal when compensated, but may elevate as cirrhosis progresses.[citation needed]
  • Albumin levels fall as the synthetic function of the liver declines with worsening cirrhosis since albumin is exclusively synthesized in the liver.
  • Prothrombin time increases, since the liver synthesizes clotting factors.
  • Globulins increase due to shunting of bacterial antigens away from the liver to lymphoid tissue.
  • Serum sodium levels fall(hyponatremia) due to inability to excrete free water resulting from high levels of ADH and aldosterone.
  • Leukopenia and neutropenia are due to splenomegaly with splenic margination.[citation needed]
  • Coagulation defects occur, as the liver produces most of the coagulation factors, thus coagulopathy correlates with worsening liver disease.
  • Glucagon is increased in cirrhosis.[24]
  • Vasoactive intestinal peptide is increased as blood is shunted into the intestinal system because of portal hypertension.
  • Vasodilators are increased (such as nitric oxide and carbon monoxide) reducing afterload with compensatory increase in cardiac output, mixed venous oxygen saturation.[68]
  • Renin is increased (as well as sodium retention in kidneys) secondary to a fall in systemic vascular resistance.[69]

FibroTest is a biomarker for fibrosis that may be used instead of a biopsy.[70]

Other laboratory studies performed in newly diagnosed cirrhosis may include:

  • Serology for hepatitis viruses, autoantibodies (ANA, anti-smooth muscle, antimitochondria, anti-LKM)
  • Ferritin[71][72] and transferrin saturation: markers of iron overload as in hemochromatosis, copper and ceruloplasmin: markers of copper overload as in Wilson's disease
  • Immunoglobulin levels (IgG, IgM, IgA) – these immunoglobins are nonspecific, but may help in distinguishing various causes.
    • IgG level is elevated in chronic hepatitis, alcoholic and autoimmune hepatitis. It's slow and sustained increase is seen in viral hepatitis.
    • IgM significantly increased in primary biliary cirrhosis and moderately increased in viral hepatitis and cirrhosis.
    • IgA is increased in alcoholic cirrhosis and primary biliary cirrhosis.[citation needed]
  • Cholesterol and glucose
  • Alpha 1-antitrypsin

Markers of inflammation and immune cell activation are typically elevated in cirrhotic patients, especially in the decompensated disease stage:

A recent study identified 15 microbial biomarkers from the gut microbiota.[78] These could potentially be used to discriminate patients with liver cirrhosis from healthy individuals.

Pathology edit

 
Micrograph showing cirrhosis, trichrome stain

The gold standard for diagnosis of cirrhosis is a liver biopsy. This is usually carried out as a fine-needle approach, through the skin (percutaneous), or internal jugular vein (transjugular).[79] Endoscopic ultrasound-guided liver biopsy (EUS), using the percutaneous or transjugular route, has become a good alternative to use.[80][79] EUS can target liver areas that are widely separated,[81] and can deliver bi-lobar biopsies.[80] A biopsy is not necessary if the clinical, laboratory, and radiologic data suggest cirrhosis. Furthermore, a small but significant risk of complications is associated with liver biopsy, and cirrhosis itself predisposes for complications caused by liver biopsy.[82]

Once the biopsy is obtained, a pathologist will study the sample. Cirrhosis is defined by its features on microscopy: (1) the presence of regenerating nodules of hepatocytes and (2) the presence of fibrosis, or the deposition of connective tissue between these nodules. The pattern of fibrosis seen can depend on the underlying insult that led to cirrhosis. Fibrosis can also proliferate even if the underlying process that caused it has resolved or ceased. The fibrosis in cirrhosis can lead to destruction of other normal tissues in the liver: including the sinusoids, the space of Disse, and other vascular structures, which leads to altered resistance to blood flow in the liver, and portal hypertension.[83]

  •  
    No fibrosis, but mild zone 3 steatosis, in which collagen fibres (pink–red, arrow) are confined to portal tracts (P) (Van Gieson's stain)[84]
  •  
    Histopathology of steatohepatitis with mild fibrosis in the form of fibrous expansion (Van Gieson's stain)[84]
  •  
    Histopathology of steatohepatitis with moderate fibrosis, with thin fibrous bridges (Van Gieson's stain)[84]
  •  
    Histopathology of steatohepatitis with established cirrhosis, with thick bands of fibrosis (Van Gieson's stain)[84]
  •  
    Trichrome stain, showing cirrhosis as a nodular texture surrounded by fibrosis (wherein collagen is stained blue).

As cirrhosis can be caused by many different entities which injure the liver in different ways, cause-specific abnormalities may be seen. For example, in chronic hepatitis B, there is infiltration of the liver parenchyma with lymphocytes.[83] In congestive hepatopathy there are erythrocytes and a greater amount of fibrosis in the tissue surrounding the hepatic veins.[85] In primary biliary cholangitis, there is fibrosis around the bile duct, the presence of granulomas and pooling of bile.[86] Lastly in alcoholic cirrhosis, there is infiltration of the liver with neutrophils.[83]

Macroscopically, the liver is initially enlarged, but with the progression of the disease, it becomes smaller. Its surface is irregular, the consistency is firm, and if associated with steatosis the color is yellow. Depending on the size of the nodules, there are three macroscopic types: micronodular, macronodular, and mixed cirrhosis. In the micronodular form (Laennec's cirrhosis or portal cirrhosis), regenerating nodules are under 3 mm. In macronodular cirrhosis (post-necrotic cirrhosis), the nodules are larger than 3 mm. Mixed cirrhosis consists of nodules of different sizes.[87]

  •  
    Micronodular cirrhosis, with diffuse areas of pallor
  •  
    Pale macronodules of cirrhosis
  •  
    Cirrhosis leading to hepatocellular carcinoma

Grading edit

The severity of cirrhosis is commonly classified with the Child–Pugh score (also known as the Child–Pugh–Turcotte score).[88] This system was devised in 1964 by Child and Turcotte, and modified in 1973 by Pugh and others.[89] It was first established to determine who would benefit from elective surgery for portal decompression.[88] This scoring system uses multiple lab values including bilirubin, albumin, and INR.[90] The presence of ascites and severity of encephalopathy is also included in the scoring.[90] The classification system includes class A, B, or C.[90] Class A has a favorable prognosis while class C is at high risk of death.

Child-Pugh Score in Relation to Liver Function, Prognosis and Post-op Mortality[90][88]
Child-Pugh Class Points Liver Function Prognosis Abdominal surgery post-operative mortality
Child-Pugh Class A 5–6 points Good liver function 15–20 years 10%
Child-Pugh Class B 7–9 points Moderately impaired liver function 30%
Child-Pugh Class C 10–15 points Advanced liver dysfunction 1–3 years 82%

The Child-Pugh score is a validated predictor of mortality after a major surgery.[88] For example, Child class A patients have a 10% mortality rate and Child class B patients have a 30% mortality rate while Child class C patients have a 70–80% mortality rate after abdominal surgery.[88] Elective surgery is usually reserved for those in Child class A patients. There is an increased risk for child class B individuals and they may require medical optimization. Overall, it is not recommended for Child class C patients to undergo elective surgery.[88]

In the past, the Child-Pugh classification was used to determine people who were candidates for a liver transplant.[88] Child-Pugh class B is usually an indication for evaluation for transplant.[90] However, there were many issues when applying this score to liver transplant eligibility.[88] Thus, the MELD score was created.

The Model for End-Stage Liver Disease (MELD) score was later developed and approved in 2002.[91] It was approved by the United Network for Organ Sharing (UNOS) as a way to determine the allocation of liver transplants to awaiting people in the United States.[92] It is also used as a validated survival predictor of cirrhosis, alcoholic hepatitis, acute liver failure, and acute hepatitis.[93] The variables included bilirubin, INR, creatinine, and dialysis frequency.[93] In 2016, sodium was added to the variables and the score is often referred to as MELD-Na.[94]

MELD-Plus is a further risk score to assess severity of chronic liver disease. It was developed in 2017 as a result of a collaboration between Massachusetts General Hospital and IBM.[95] Nine variables were identified as effective predictors for 90-day mortality after a discharge from a cirrhosis-related hospital admission.[95] The variables include all Model for End-Stage Liver Disease (MELD)'s components, as well as sodium, albumin, total cholesterol, white blood cell count, age, and length of stay.[95]

The hepatic venous pressure gradient (difference in venous pressure between incoming and outgoing blood to the liver) also determines the severity of cirrhosis, although it is hard to measure. A value of 16 mm or more means a greatly increased risk of death.[96][unreliable medical source?]

Prevention edit

Key prevention strategies for cirrhosis are population-wide interventions to reduce alcohol intake (through pricing strategies, public health campaigns, and personal counseling), programs to reduce the transmission of viral hepatitis, and screening of relatives of people with hereditary liver diseases.[97]

Little is known about factors affecting cirrhosis risk and progression. However, many studies have provided increasing evidence for the protective effects of coffee consumption against the progression of liver disease. These effects are more noticeable in liver disease that is associated with alcohol use disorder. Coffee has antioxidant and antifibrotic effects. Caffeine may not be the important component; polyphenols may be more important. Drinking two or more cups of coffee a day is associated with improvements in the liver enzymes ALT, AST, and GGT. Even in those with liver disease, coffee consumption can lower fibrosis and cirrhosis.[98]

Treatment edit

Generally, liver damage from cirrhosis cannot be reversed, but treatment can stop or delay further progression and reduce complications. A healthy diet is encouraged, as cirrhosis may be an energy-consuming process. A recommended diet consists of high-protein, high-fiber diet plus supplementation with branched-chain amino acids.[99] Close follow-up is often necessary. Antibiotics are prescribed for infections, and various medications can help with itching. Laxatives, such as lactulose, decrease the risk of constipation. Carvedilol increases survival benefit for people with cirrhosis and portal hypertension.[100]Diuretics in combination with low salt diet reduce fluid in body which helps reduce oedema.[101]

Alcoholic cirrhosis caused by alcohol use disorder is treated by abstaining from alcohol. Treatment for hepatitis-related cirrhosis involves medications used to treat the different types of hepatitis, such as interferon for viral hepatitis and corticosteroids for autoimmune hepatitis.[citation needed]

Cirrhosis caused by Wilson's disease is treated by removing the copper which builds up in organs.[2] This is carried out using chelation therapy such as penicillamine. When the cause is an iron overload, iron is removed using a chelation agent such as deferoxamine or by bloodletting.[citation needed]

As of 2021, there are recent studies studying drugs to prevent cirrhosis caused by non-alcoholic fatty liver disease (NAFLD or NASH). A drug called semaglutide was shown to provide greater NASH resolution versus placebo. No improvement in fibrosis was observed.[102] A combination of cilofexor/firsocostat was studied in people with bridging fibrosis and cirrhosis. It was observed to have led to improvements in NASH activity with a potential antifibrotic effect.[103] Lanifibranor is also shown to prevent worsening fibrosis.[104]

Preventing further liver damage edit

Regardless of the underlying cause of cirrhosis, consumption of alcohol and other potentially damaging substances is discouraged. There is no evidence that supports the avoidance or dose reduction of paracetamol in people with compensated cirrhosis; it is thus considered a safe analgesic for said individuals.[105]

People who are at risk of being exposed to hepatitis A and hepatitis B should consider vaccines against these diseases.[citation needed]

Treating the cause of cirrhosis prevents further damage; for example, giving oral antivirals such as entecavir and tenofovir where cirrhosis is due to hepatitis B prevents progression of cirrhosis. Similarly, control of weight and diabetes prevents deterioration in cirrhosis due to non-alcoholic fatty liver disease.[106]

People with cirrhosis or liver damage are often advised to avoid drugs that could further harm the liver.[107] These include several drugs such as anti-depressants, certain antibiotics, and NSAIDs (like ibuprofen).[107] These agents are hepatotoxic as they are metabolized by the liver. If a medication that harms the liver is still recommended by a doctor, the dosage can be adjusted to aim for minimal stress on the liver.[citation needed]

Lifestyle edit

According to a 2018 systematic review based on studies that implemented 8 to 14 week-long exercise programs, there is currently insufficient scientific evidence regarding either the beneficial or harmful effects of physical exercise in people with cirrhosis on all-cause mortality, morbidity (including both serious and non-serious adverse events), health-related quality of life, exercise capacity and anthropomorphic measures.[108] These conclusions were based on low to very low quality research, which imposes the need to develop further research with higher quality, especially to evaluate its effects on clinical outcomes.[citation needed]

Transplantation edit

Main article: Liver transplantation

If complications cannot be controlled or when the liver ceases functioning, liver transplantation is necessary. Survival from liver transplantation has been improving over the 1990s, and the five-year survival rate is now around 80%. The survival rate depends largely on the severity of disease and other medical risk factors in the recipient.[109] In the United States, the MELD score is used to prioritize patients for transplantation.[110] Transplantation necessitates the use of immune suppressants (ciclosporin or tacrolimus).

Decompensated cirrhosis edit

Manifestations of decompensation in cirrhosis include gastrointestinal bleeding, hepatic encephalopathy, jaundice or ascites. In patients with previously stable cirrhosis, decompensation may occur due to various causes, such as constipation, infection (of any source), increased alcohol intake, medication, bleeding from esophageal varices or dehydration. It may take the form of any of the complications of cirrhosis listed below.

People with decompensated cirrhosis generally require admission to a hospital, with close monitoring of the fluid balance, mental status, and emphasis on adequate nutrition and medical treatment – often with diuretics, antibiotics, laxatives or enemas, thiamine and occasionally steroids, acetylcysteine and pentoxifylline.[111] Administration of saline is avoided, as it would add to the already high total body sodium content that typically occurs in cirrhosis. Life expectancy without liver transplant is low, at most three years.

Palliative care edit

Palliative care is specialized medical care that focuses on providing patients with relief from the symptoms, pain, and stress of a serious illness, such as cirrhosis. The goal of palliative care is to improve quality of life for both the patient and the patient's family and it is appropriate at any stage and for any type of cirrhosis.[112]

Especially in the later stages, people with cirrhosis experience significant symptoms such as abdominal swelling, itching, leg edema, and chronic abdominal pain which would be amenable for treatment through palliative care.[113] Because the disease is not curable without a transplant, palliative care can also help with discussions regarding the person's wishes concerning health care power of attorney, do not resuscitate decisions and life support, and potentially hospice.[113] Despite proven benefit, people with cirrhosis are rarely referred to palliative care.[114]

Immunity edit

Cirrhosis is known to cause immune dysfunction in numerous ways. It impedes the immune system from working normally.[citation needed]

Bleeding and blood clot risk edit

Cirrhosis can increase the risk of bleeding. The liver produces various proteins in the coagulation cascade (coagulation factors II, VII, IX, X, V, and VI). When damaged, the liver is impaired in its production of these proteins.[115] This will ultimately increase bleeding as clotting factors are diminished. Clotting function is estimated by lab values, mainly platelet count, prothrombin time (PT), and international normalized ratio (INR).

The American Gastroenterological Association (AGA) provided recommendations in 2021 in regards to coagulopathy management of cirrhotic patients in certain scenarios.[115]

  • The AGA does not recommend for extensive pre-procedural testing, including repeated measurements of PT/INR or platelet count before patients with stable cirrhosis undergo common gastrointestinal procedures. Nor do they suggest the routine use of blood products, such as platelets, for bleeding prevention.[115] Cirrhosis is stable when there are no changes in baseline abnormalities of coagulation lab values.
  • For patients with stable cirrhosis and low platelet count undergoing common low-risk procedures, the AGA does not recommend the routine use of thrombopoietin receptor agonists for bleeding prevention.[115]
  • In hospitalized patients who meet standard guidelines for clot prevention, the AGA suggests standard prevention.[115]
  • The AGA does not recommend in routine screening for portal vein thrombosis. If there is a portal vein thrombosis, the AGA suggests treatment by anticoagulation.[115]
  • In the case of cirrhosis with atrial fibrillation, the AGA recommends using anticoagulation over no anticoagulation.[115]

Complications edit

Ascites edit

Salt restriction is often necessary, as cirrhosis leads to accumulation of salt (sodium retention). Diuretics may be necessary to suppress ascites. Diuretic options for inpatient treatment include aldosterone antagonists (spironolactone) and loop diuretics. Aldosterone antagonists are preferred for people who can take oral medications and are not in need of an urgent volume reduction. Loop diuretics can be added as additional therapy.[116]

Where salt restriction and the use of diuretics are ineffective then paracentesis may be the preferred option.[117] This procedure requires the insertion of a plastic tube into the peritoneal cavity. Human serum albumin solution is usually given to prevent complications from the rapid volume reduction. In addition to being more rapid than diuretics, 4–5 liters of paracentesis is more successful in comparison to diuretic therapy.[116]

Esophageal and gastric variceal bleeding edit

For portal hypertension, nonselective beta blockers such as propranolol or nadolol are commonly used to lower blood pressure over the portal system. In severe complications from portal hypertension, transjugular intrahepatic portosystemic shunting (TIPS) is occasionally indicated to relieve pressure on the portal vein. As this shunting can worsen hepatic encephalopathy, it is reserved for those patients at low risk of encephalopathy. TIPS is generally regarded only as a bridge to liver transplantation[118] or as a palliative measure.[citation needed] Balloon-occluded retrograde transvenous obliteration can be used to treat gastric variceal bleeding.[119]

Gastroscopy (endoscopic examination of the esophagus, stomach, and duodenum) is performed in cases of established cirrhosis. If esophageal varices are found, prophylactic local therapy may be applied such as sclerotherapy or banding, and beta blockers may be used.[120][121][122]

Hepatic encephalopathy edit

Hepatic encephalopathy is a potential complication of cirrhosis.[24] It may lead to functional neurological impairment ranging from mild confusion to coma.[24] Hepatic encephalopathy is primarily caused by the accumulation of ammonia in the blood, which causes neurotoxicity when crossing the blood-brain barrier. Ammonia is normally metabolized by the liver; as cirrhosis causes both decreased liver function and increased portosystemic shunting (allowing blood to bypass the liver), systemic ammonia levels gradually rise and lead to encephalopathy.[123]

Most pharmaceutical approaches to treating hepatic encephalopathy focus on reducing ammonia levels.[124] Per 2014 guidelines,[125] the first-line treatment involves the use of lactulose, a non-absorbable disaccharide which decreases the pH level of the colon when it is metabolized by intestinal bacteria. The lower colonic pH causes increased conversion of ammonia into ammonium, which is then excreted from the body.[126] Rifaximin, an antibiotic that inhibits the function of ammonia-producing bacteria in the gastrointestinal tract,[127] is recommended for use in combination with lactulose as prophylaxis against recurrent episodes of hepatic encephalopathy.[125][128][129]

In addition to pharmacotherapy, providing proper hydration and nutritional support is also essential.[124] Appropriate quantities of protein uptake is encouraged.[130] Several factors may precipitate hepatic encephalopathy, which include alcohol use, excess protein, gastrointestinal bleeding, infection, constipation, and vomiting/diarrhea.[124] Drugs such as benzodiazepines, diuretics, or narcotics can also precipitate encephalopathic events.[124] A low protein diet is recommended with gastrointestinal bleeding.[130]

The severity of hepatic encephalopathy is determined by assessing the patient's mental status. This is generally a subjective assessment, although several attempts at creating criteria to help standardize this assessment have been published. One example is the West Haven criteria, reproduced below.

Grading of hepatic encephalopathy[131]
Grade Mental status
Grade 1: Mild Changes in behavior
Mild confusion
Slurred speech
Disordered sleep
Grade 2: Moderate Lethargy
Moderate confusion
Grade 3: Severe Stupor
Incoherent
Sleeping but arousable
Grade 4: Coma Coma/Unresponsive

Hepatorenal syndrome edit

Hepatorenal syndrome is a serious complication of end-stage cirrhosis when kidney damage is also involved.[132]

Spontaneous bacterial peritonitis edit

People with ascites due to cirrhosis are at risk of spontaneous bacterial peritonitis.

Portal hypertensive gastropathy edit

Portal hypertensive gastropathy refers to changes in the mucosa of the stomach in people with portal hypertension, and is associated with cirrhosis severity.[133]

Infection edit

Cirrhosis can cause immune system dysfunction, leading to infection. Signs and symptoms of infection may be nonspecific and are more difficult to recognize (for example, worsening encephalopathy but no fever).[134] Moreover, infections in cirrhosis are major triggers for other complications (ascites, variceal bleeding, hepatic encephalopathy, organ failures, death).[134][75][77]

Hepatocellular carcinoma edit

Hepatocellular carcinoma is the most common primary liver cancer, and the most common cause of death in people with cirrhosis.[135] Screening using an MRI scan can detect this cancer and is often carried out for early signs which has been shown to improve outcomes.[2][136]

Epidemiology edit

 
Cirrhosis deaths per million persons in 2012
  9-44
  45-68
  69–88
  89–104
  105–122
  123–152
  153–169
  170–204
  205–282
  283–867
 
Disability-adjusted life year for cirrhosis of the liver per 100,000 inhabitants in 2004.[137]
  no data
  <50
  50-100
  100-200
  200-300
  300-400
  400-500
  500-600
  600-700
  700-800
  800-900
  900–1000
  >1000

Each year, approximately one million deaths are due to complications of cirrhosis, making cirrhosis the 11th most common cause of death globally.[138] Cirrhosis and chronic liver disease were the tenth leading cause of death for men and the twelfth for women in the United States in 2001, killing about 27,000 people each year.[139]

The cause of cirrhosis can vary; alcohol and non-alcoholic fatty liver disease are main causes in western and industrialized countries, whereas viral hepatitis is the predominant cause in low and middle-income countries.[138] Cirrhosis is more common in men than in women.[140] The cost of cirrhosis in terms of human suffering, hospital costs, and lost productivity is high.

Globally, age-standardized disability-adjusted life year (DALY) rates have decreased from 1990 to 2017, with the values going from 656.4 years per 100,000 people to 510.7 years per 100,000 people.[141] In males DALY rates have decreased from 903.1 years per 100,000 population in 1990, to 719.3 years per 100,000 population in 2017; in females the DALY rates have decreased from 415.5 years per 100,000 population in 1990, to 307.6 years per 100,000 population in 2017.[141] However, globally the total number of DALYs have increased by 10.9 million from 1990 to 2017, reaching the value of 41.4 million DALYs.[141]

Etymology edit

The word "cirrhosis" is a neologism derived from Greek: κίρρωσις; kirrhos κιρρός, meaning "yellowish, tawny" (the orange yellow colour of the diseased liver) and the suffix -osis, i.e. "condition" in medical terminology.[142][143][144] While the clinical entity was known before, René Laennec gave it this name in an 1819 paper.[18]

See also edit

References edit

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External links edit

  • at the National Digestive Diseases Information Clearinghouse (NDDIC). NIH Publication No. 04-1134, December 2003.
  • "Cirrhosis". MedlinePlus. U.S. National Library of Medicine.

January 01, 1970
cirrhosis, also, known, liver, cirrhosis, hepatic, cirrhosis, stage, liver, disease, impaired, liver, function, caused, formation, scar, tissue, known, fibrosis, damage, caused, liver, disease, damage, liver, leads, repair, liver, tissue, subsequent, formation. Cirrhosis also known as liver cirrhosis or hepatic cirrhosis and end stage liver disease is the impaired liver function caused by the formation of scar tissue known as fibrosis due to damage caused by liver disease 6 Damage to the liver leads to repair of liver tissue and subsequent formation of scar tissue Over time scar tissue can replace normal functioning tissue leading to the impaired liver function of cirrhosis 6 7 The disease typically develops slowly over months or years 1 Early symptoms may include tiredness weakness loss of appetite unexplained weight loss nausea and vomiting and discomfort in the right upper quadrant of the abdomen 8 As the disease worsens symptoms may include itchiness swelling in the lower legs fluid build up in the abdomen jaundice bruising easily and the development of spider like blood vessels in the skin 8 The fluid build up in the abdomen may develop into spontaneous infections 1 More serious complications include hepatic encephalopathy bleeding from dilated veins in the esophagus stomach or intestines and liver cancer 9 Stages of cirrhosis include compensated cirrhosis and decompensated cirrhosis 10 CirrhosisOther namesCirrhosis of the liver hepatic cirrhosisCross section of human liver with cirrhosisPronunciation s ɪ ˈ r oʊ s ɪ s SpecialtyGastroenterology HepatologySymptomsTiredness itchiness swelling in the lower legs jaundice easily bruising fluid build up in the abdomen 1 ComplicationsSpontaneous bacterial peritonitis hepatic encephalopathy dilated veins in the esophagus liver cancer 1 Usual onsetOver months years or decades 1 DurationLong term 1 CausesAlcoholic liver disease hepatitis B hepatitis C non alcoholic steatohepatitisDiagnostic methodBlood tests medical imaging liver biopsy 2 1 PreventionVaccination such as hepatitis B avoiding alcohol 1 losing weight exercising low carbohydrate diet controlling hypertension and diabetes may help in those with NAFLD or NASHTreatmentDepends on underlying cause 3 Frequency2 8 million 2015 4 Deaths1 3 million 2015 5 Cirrhosis is most commonly caused by alcoholic liver disease non alcoholic steatohepatitis NASH the progressive form of non alcoholic fatty liver disease 11 heroin abuse 12 chronic hepatitis B and chronic hepatitis C 8 13 Heavy drinking over a number of years can cause alcoholic liver disease 14 Liver damage has also been attributed to heroin usage over an extended period of time as well 15 NASH has a number of causes including obesity high blood pressure abnormal levels of cholesterol type 2 diabetes and metabolic syndrome 16 Less common causes of cirrhosis include autoimmune hepatitis primary biliary cholangitis and primary sclerosing cholangitis that disrupts bile duct function genetic disorders such as Wilson s disease and hereditary hemochromatosis and chronic heart failure with liver congestion 8 Diagnosis is based on blood tests medical imaging and liver biopsy 2 1 Hepatitis B vaccine can prevent hepatitis B and the development of cirrhosis but no vaccination against hepatitis C is available 1 No specific treatment for cirrhosis is known but many of the underlying causes may be treated by a number of medications that may slow or prevent worsening of the condition 3 Hepatitis B and C may be treatable with antiviral medications 1 Avoiding alcohol is recommended in all cases 1 Autoimmune hepatitis may be treated with steroid medications 1 Ursodiol may be useful if the disease is due to blockage of the bile duct 1 Other medications may be useful for complications such as abdominal or leg swelling hepatic encephalopathy and dilated esophageal veins 1 If cirrhosis leads to liver failure a liver transplant may be an option 16 Cirrhosis affected about 2 8 million people and resulted in 1 3 million deaths in 2015 4 5 Of these deaths alcohol caused 348 000 27 hepatitis C caused 326 000 25 and hepatitis B caused 371 000 28 5 In the United States more men die of cirrhosis than women 1 The first known description of the condition is by Hippocrates in the fifth century BCE 17 The term cirrhosis was derived in 1819 from the Greek word kirrhos which describes the yellowish color of a diseased liver 18 Contents 1 Signs and symptoms 1 1 Liver dysfunction 1 2 Portal hypertension 1 3 Other nonspecific signs 1 4 Advanced disease 2 Causes 2 1 Common causes 2 2 Less common causes 3 Pathophysiology 4 Diagnosis 4 1 Imaging 4 2 Lab findings 4 3 Pathology 5 Grading 6 Prevention 7 Treatment 7 1 Preventing further liver damage 7 2 Lifestyle 7 3 Transplantation 7 4 Decompensated cirrhosis 7 5 Palliative care 7 6 Immunity 7 7 Bleeding and blood clot risk 8 Complications 8 1 Ascites 8 2 Esophageal and gastric variceal bleeding 8 3 Hepatic encephalopathy 8 4 Hepatorenal syndrome 8 5 Spontaneous bacterial peritonitis 8 6 Portal hypertensive gastropathy 8 7 Infection 8 8 Hepatocellular carcinoma 9 Epidemiology 10 Etymology 11 See also 12 References 13 External linksSigns and symptoms edit nbsp Person with cirrhosis and associated pain in the right upper region of the abdomen Cirrhosis can take quite a long time to develop and symptoms may be slow to emerge 8 Some early symptoms include tiredness weakness loss of appetite weight loss and nausea 8 Early signs may also include redness on the palms known as palmer erythema 10 People may also feel discomfort in the right upper abdomen around the liver 8 As cirrhosis progresses symptoms can include neurological changes 8 This can consist of cognitive impairments confusion memory loss sleep disorders and personality changes 8 Steatorrhea or presence of undigested fats in stool is also a symptom of cirrhosis 19 Worsening cirrhosis can cause a build up of fluid in different parts of the body such as the legs edema and abdomen ascites 8 Other signs of advancing disease include itchy skin bruising easily dark urine and yellowing of the skin 8 Liver dysfunction edit These features are a direct consequence of liver cells not functioning Spider angiomata or spider nevi happen when there is dilatation of vasculature beneath the skin surface 20 There is a central red spot with reddish extensions that radiate outward This creates a visual effect that resembles a spider It occurs in about one third of cases 20 The likely cause is an increase in estrogen 20 Cirrhosis causes a rise of estrogen due to increased conversion of androgens into estrogen 21 Palmar erythema a reddening of the palm below the thumb and little finger is seen in about 23 of cirrhosis cases and results from increased circulating estrogen levels 22 Gynecomastia or the increase of breast size in men is caused by increased estradiol a potent type of estrogen 23 This can occur in up to two thirds of cases 24 Hypogonadism signifies a decreased functionality of the gonads 25 This can result in impotence infertility loss of sexual drive and testicular atrophy A swollen scrotum may also be evident 26 Liver size can be enlarged normal or shrunken in people with cirrhosis 27 As the disease progresses the liver will typically shrink due to the result of scarring 28 Jaundice is the yellowing of the skin It can additionally cause yellowing of mucous membranes notably of the white of the eyes This phenomenon is due to increased levels of bilirubin which may also cause the urine to be dark colored 29 Portal hypertension edit source source source source source source source source track track track track track track track track Liver cirrhosis makes it hard for blood to flow in the portal venous system 30 This resistance creates a backup of blood and increases pressure 30 This results in portal hypertension Effects of portal hypertension include Ascites is a build up of fluid in the peritoneal cavity in the abdomen 31 An enlarged spleen in 35 50 of cases 6 Esophageal varices and gastric varices result from collateral circulation in the esophagus and stomach a process called portacaval anastomosis 32 When the blood vessels in this circulation become enlarged they are called varices Varices are more likely to rupture at this point 7 Variceal rupture often leads to severe bleeding which can be fatal 32 Caput medusae are dilated paraumbilical collateral veins due to portal hypertension 30 Blood from the portal venous system may be forced through the paraumbilical veins and ultimately to the abdominal wall veins The created pattern resembles the head of Medusa hence the name 7 Cruveilhier Baumgarten bruit is bruit in the epigastric region on examination by stethoscope 33 It is due to extra connections forming between the portal system and the paraumbilical veins 33 Other nonspecific signs edit Some signs that may be present include changes in the nails such as Muehrcke s lines Terry s nails and nail clubbing 34 35 Additional changes may be seen in the hands Dupuytren s contracture as well as the skin bones hypertrophic osteoarthropathy 24 Advanced disease edit As the disease progresses complications may develop In some people these may be the first signs of the disease Bruising and bleeding can result from decreased production of clotting factors 36 Hepatic encephalopathy HE occurs when ammonia and related substances build up in the blood 36 This build up affects brain function when they are not cleared from the blood by the liver Symptoms can include unresponsiveness forgetfulness trouble concentrating changes in sleep habits or psychosis One classic physical examination finding is asterixis 24 This is the asynchronous flapping of outstretched dorsiflexed hands 24 Fetor hepaticus is a musty breath odor resulting from increased dimethyl sulfide and is a feature of HE 37 Sensitivity to medication can be caused by decreased metabolism of the active compounds Acute kidney injury particularly hepatorenal syndrome 24 Cachexia associated with muscle wasting and weakness 36 Causes editCirrhosis has many possible causes and more than one cause may be present History taking is of importance in trying to determine the most likely cause 2 Globally 57 of cirrhosis is attributable to either hepatitis B 30 or hepatitis C 27 38 39 Alcohol use disorder is another major cause accounting for about 20 40 of the cases 39 24 Common causes edit nbsp Hepatitis C viral particles and the liver Alcoholic liver disease ALD or alcoholic cirrhosis develops for 10 20 of individuals who drink heavily for a decade or more 40 Alcohol seems to injure the liver by blocking the normal metabolism of protein fats and carbohydrates 41 This injury happens through the formation of acetaldehyde from alcohol Acetaldehyde is reactive and leads to the accumulation of other reactive products in the liver 24 People with ALD may also have concurrent alcoholic hepatitis Associated symptoms are fever hepatomegaly jaundice and anorexia 41 AST and ALT blood levels are both elevated but at less than 300 IU liter with an AST ALT ratio gt 2 0 a value rarely seen in other liver diseases 42 In the United States 40 of cirrhosis related deaths are due to alcohol 24 In non alcoholic fatty liver disease NAFLD fat builds up in the liver and eventually causes scar tissue 43 This type of disorder can be caused by obesity diabetes malnutrition coronary artery disease and steroids 43 44 Though similar in signs to alcoholic liver disease no history of notable alcohol use is found Blood tests and medical imaging are used to diagnose NAFLD and NASH and sometimes a liver biopsy is needed 31 Chronic hepatitis C an infection with the hepatitis C virus causes inflammation of the liver and a variable grade of damage to the organ 36 Over several decades this inflammation and damage can lead to cirrhosis Among people with chronic hepatitis C 20 30 develop cirrhosis 36 24 Cirrhosis caused by hepatitis C and alcoholic liver disease are the most common reasons for liver transplant 24 Both hepatitis C and hepatitis B related cirrhosis can also be attributed with heroin addiction 45 Chronic hepatitis B causes liver inflammation and injury that over several decades can lead to cirrhosis 36 Hepatitis D is dependent on the presence of hepatitis B and accelerates cirrhosis in co infection 36 Less common causes edit In primary biliary cholangitis previously known as primary biliary cirrhosis the bile ducts become damaged by an autoimmune process 36 This leads to liver damage 43 Some people may have no symptoms While other people could present with fatigue pruritus or skin hyperpigmentation 46 The liver is typically enlarged which is referred to as hepatomegaly 46 Rises in alkaline phosphatase cholesterol and bilirubin levels occur Patients are usually positive for anti mitochondrial antibodies 46 Primary sclerosing cholangitis is a disorder of the bile ducts that presents with pruritus steatorrhea fat soluble vitamin deficiencies and metabolic bone disease A strong association with inflammatory bowel disease is seen especially ulcerative colitis 24 Autoimmune hepatitis is caused by an attack of the liver by lymphocytes This causes inflammation and eventually scarring as well as cirrhosis Findings include elevations in serum globulins especially gamma globulins 24 Hereditary hemochromatosis usually presents with skin hyperpigmentation diabetes mellitus pseudogout or cardiomyopathy All of these are due to signs of iron overload 24 36 Family history of cirrhosis is common as well Wilson s disease is an autosomal recessive disorder characterized by low ceruloplasmin in the blood and increased copper of the liver 43 36 Copper in the urine is also elevated People with Wilson s disease may also have Kayser Fleischer rings in the cornea and altered mental status 43 36 Indian childhood cirrhosis is a form of neonatal cholestasis characterized by deposition of copper in the liver 36 47 Alpha 1 antitrypsin deficiency is an autosomal co dominant disorder of low levels of the enzyme alpha 1 antitrypsin 24 Cardiac cirrhosis is due to chronic right sided heart failure which leads to liver congestion 24 Galactosemia 48 Glycogen storage disease type IV 36 Cystic fibrosis 24 Hepatotoxic drugs or toxins such as acetaminophen paracetamol methotrexate or amiodarone 36 Pathophysiology editThe liver plays a vital role in the synthesis of proteins for example albumin clotting factors and complement detoxification and storage for example of vitamin A and glycogen In addition it participates in the metabolism of lipids and carbohydrates citation needed Cirrhosis is often preceded by hepatitis and fatty liver steatosis independent of the cause If the cause is removed at this stage the changes are fully reversible citation needed The pathological hallmark of cirrhosis is the development of scar tissue that replaces normal tissue This scar tissue blocks the portal flow of blood through the organ raising the blood pressure and disturbing normal function Research has shown the pivotal role of the stellate cell that normally stores vitamin A in the development of cirrhosis Damage to the liver tissue from inflammation leads to the activation of stellate cells which increases fibrosis through the production of myofibroblasts and obstructs hepatic blood flow 49 In addition stellate cells secrete TGF beta 1 which leads to a fibrotic response and proliferation of connective tissue TGF b1 have been implicated in the process of activating hepatic stellate cells HSCs with the magnitude of fibrosis being in proportion to increase in TGF b levels ACTA2 is associated with TGF b pathway that enhances contractile properties of HSCs leading to fibrosis 50 Furthermore HSCs secrete TIMP1 and TIMP2 naturally occurring inhibitors of matrix metalloproteinases MMPs which prevent MMPs from breaking down the fibrotic material in the extracellular matrix 51 52 As this cascade of processes continues fibrous tissue bands septa separate hepatocyte nodules which eventually replace the entire liver architecture leading to decreased blood flow throughout The spleen becomes congested and enlarged resulting in its retention of platelets which are needed for normal blood clotting Portal hypertension is responsible for the most severe complications of cirrhosis citation needed Diagnosis edit nbsp Caudate lobe hypertrophy on ultrasound due to cirrhosis nbsp Hepatofugal non forward flow in portal vein The diagnosis of cirrhosis in an individual is based on multiple factors 24 Cirrhosis may be suspected from laboratory findings physical exam and the person s medical history Imaging is generally obtained to evaluate the liver 24 A liver biopsy will confirm the diagnosis however is generally not required 36 Imaging edit Ultrasound is routinely used in the evaluation of cirrhosis 36 It may show a small and shrunken liver in advanced disease On ultrasound there is increased echogenicity with irregular appearing areas 53 Other suggestive findings are an enlarged caudate lobe widening of the fissures and enlargement of the spleen 54 An enlarged spleen which normally measures less than 11 12 cm 4 3 4 7 in in adults may suggest underlying portal hypertension 55 Ultrasound may also screen for hepatocellular carcinoma and portal hypertension 36 This is done by assessing flow in the hepatic vein 56 An increased portal vein pulsatility may be seen However this may be a sign of elevated right atrial pressure 57 Portal vein pulsatility are usually measured by a pulsatility indices PI 56 A number above a certain values indicates cirrhosis see table below Pulsatility indices PI Index Calculation Cutoff Average based Max Min Average 56 0 5 56 Max relative Max Min Max 58 0 5 58 59 0 54 59 Other scans include CT of the abdomen and MRI 36 A CT scan is non invasive and may be helpful in the diagnosis 36 Compared to the ultrasound CT scans tend to be more expensive MRI provides excellent evaluation however is a high expense 36 nbsp Liver cirrhosis on CT imaging of the abdomen in transverse view Cirrhosis is also diagnosable through a variety of new elastography techniques 60 61 When a liver becomes cirrhotic it will generally become stiffer Determining the stiffness through imaging can determine the location and severity of disease Techniques include transient elastography acoustic radiation force impulse imaging supersonic shear imaging and magnetic resonance elastography 62 Transient elastography and magnetic resonance elastography can help identify the stage of fibrosis 63 Compared to a biopsy elastography can sample a much larger area and is painless 64 It shows a reasonable correlation with the severity of cirrhosis 63 Other modalities have been introduced which are incorporated into ultrasonagraphy systems These include 2 dimensional shear wave elastography and point shear wave elastography which uses acoustic radiation force impulse imaging 11 Rarely are diseases of the bile ducts such as primary sclerosing cholangitis causes of cirrhosis 36 Imaging of the bile ducts such as ERCP or MRCP MRI of biliary tract and pancreas may aid in the diagnosis 36 Lab findings edit The best predictors of cirrhosis are ascites platelet count lt 160 000 mm3 spider angiomata and a Bonacini cirrhosis discriminant score greater than 7 as the sum of scores for platelet count ALT AST ratio and INR as per table 65 Bonacini score 66 Score Platelet count x109 ALT AST ratio INR 0 gt 340 gt 1 7 lt 1 1 1 280 340 1 2 1 7 1 1 1 4 2 220 279 0 6 1 19 gt 1 4 3 160 219 lt 0 6 4 100 159 5 40 99 6 lt 40 These findings are typical in cirrhosis Thrombocytopenia typically multifactorial is due to alcoholic marrow suppression sepsis lack of folate platelet sequestering in the spleen and decreased thrombopoietin 42 However this rarely results in a platelet count lt 50 000 mL 67 Aminotransferases AST and ALT are moderately elevated with AST gt ALT However normal aminotransferase levels do not preclude cirrhosis 42 Alkaline phosphatase slightly elevated but less than 2 3 times the upper limit of normal citation needed Gamma glutamyl transferase correlates with AP levels Typically much higher in chronic liver disease from alcohol 67 Bilirubin levels are normal when compensated but may elevate as cirrhosis progresses citation needed Albumin levels fall as the synthetic function of the liver declines with worsening cirrhosis since albumin is exclusively synthesized in the liver Prothrombin time increases since the liver synthesizes clotting factors Globulins increase due to shunting of bacterial antigens away from the liver to lymphoid tissue Serum sodium levels fall hyponatremia due to inability to excrete free water resulting from high levels of ADH and aldosterone Leukopenia and neutropenia are due to splenomegaly with splenic margination citation needed Coagulation defects occur as the liver produces most of the coagulation factors thus coagulopathy correlates with worsening liver disease Glucagon is increased in cirrhosis 24 Vasoactive intestinal peptide is increased as blood is shunted into the intestinal system because of portal hypertension Vasodilators are increased such as nitric oxide and carbon monoxide reducing afterload with compensatory increase in cardiac output mixed venous oxygen saturation 68 Renin is increased as well as sodium retention in kidneys secondary to a fall in systemic vascular resistance 69 FibroTest is a biomarker for fibrosis that may be used instead of a biopsy 70 Other laboratory studies performed in newly diagnosed cirrhosis may include Serology for hepatitis viruses autoantibodies ANA anti smooth muscle antimitochondria anti LKM Ferritin 71 72 and transferrin saturation markers of iron overload as in hemochromatosis copper and ceruloplasmin markers of copper overload as in Wilson s disease Immunoglobulin levels IgG IgM IgA these immunoglobins are nonspecific but may help in distinguishing various causes IgG level is elevated in chronic hepatitis alcoholic and autoimmune hepatitis It s slow and sustained increase is seen in viral hepatitis IgM significantly increased in primary biliary cirrhosis and moderately increased in viral hepatitis and cirrhosis IgA is increased in alcoholic cirrhosis and primary biliary cirrhosis citation needed Cholesterol and glucose Alpha 1 antitrypsin Markers of inflammation and immune cell activation are typically elevated in cirrhotic patients especially in the decompensated disease stage C reactive protein CRP 73 Procalcitonin PCT 73 Presepsin 74 soluble CD14 73 soluble CD163 75 soluble CD206 mannose receptor 76 soluble TREM 1 77 A recent study identified 15 microbial biomarkers from the gut microbiota 78 These could potentially be used to discriminate patients with liver cirrhosis from healthy individuals Pathology edit nbsp Micrograph showing cirrhosis trichrome stain The gold standard for diagnosis of cirrhosis is a liver biopsy This is usually carried out as a fine needle approach through the skin percutaneous or internal jugular vein transjugular 79 Endoscopic ultrasound guided liver biopsy EUS using the percutaneous or transjugular route has become a good alternative to use 80 79 EUS can target liver areas that are widely separated 81 and can deliver bi lobar biopsies 80 A biopsy is not necessary if the clinical laboratory and radiologic data suggest cirrhosis Furthermore a small but significant risk of complications is associated with liver biopsy and cirrhosis itself predisposes for complications caused by liver biopsy 82 Once the biopsy is obtained a pathologist will study the sample Cirrhosis is defined by its features on microscopy 1 the presence of regenerating nodules of hepatocytes and 2 the presence of fibrosis or the deposition of connective tissue between these nodules The pattern of fibrosis seen can depend on the underlying insult that led to cirrhosis Fibrosis can also proliferate even if the underlying process that caused it has resolved or ceased The fibrosis in cirrhosis can lead to destruction of other normal tissues in the liver including the sinusoids the space of Disse and other vascular structures which leads to altered resistance to blood flow in the liver and portal hypertension 83 nbsp No fibrosis but mild zone 3 steatosis in which collagen fibres pink red arrow are confined to portal tracts P Van Gieson s stain 84 nbsp Histopathology of steatohepatitis with mild fibrosis in the form of fibrous expansion Van Gieson s stain 84 nbsp Histopathology of steatohepatitis with moderate fibrosis with thin fibrous bridges Van Gieson s stain 84 nbsp Histopathology of steatohepatitis with established cirrhosis with thick bands of fibrosis Van Gieson s stain 84 nbsp Trichrome stain showing cirrhosis as a nodular texture surrounded by fibrosis wherein collagen is stained blue As cirrhosis can be caused by many different entities which injure the liver in different ways cause specific abnormalities may be seen For example in chronic hepatitis B there is infiltration of the liver parenchyma with lymphocytes 83 In congestive hepatopathy there are erythrocytes and a greater amount of fibrosis in the tissue surrounding the hepatic veins 85 In primary biliary cholangitis there is fibrosis around the bile duct the presence of granulomas and pooling of bile 86 Lastly in alcoholic cirrhosis there is infiltration of the liver with neutrophils 83 Macroscopically the liver is initially enlarged but with the progression of the disease it becomes smaller Its surface is irregular the consistency is firm and if associated with steatosis the color is yellow Depending on the size of the nodules there are three macroscopic types micronodular macronodular and mixed cirrhosis In the micronodular form Laennec s cirrhosis or portal cirrhosis regenerating nodules are under 3 mm In macronodular cirrhosis post necrotic cirrhosis the nodules are larger than 3 mm Mixed cirrhosis consists of nodules of different sizes 87 nbsp Micronodular cirrhosis with diffuse areas of pallor nbsp Pale macronodules of cirrhosis nbsp Cirrhosis leading to hepatocellular carcinomaGrading editThe severity of cirrhosis is commonly classified with the Child Pugh score also known as the Child Pugh Turcotte score 88 This system was devised in 1964 by Child and Turcotte and modified in 1973 by Pugh and others 89 It was first established to determine who would benefit from elective surgery for portal decompression 88 This scoring system uses multiple lab values including bilirubin albumin and INR 90 The presence of ascites and severity of encephalopathy is also included in the scoring 90 The classification system includes class A B or C 90 Class A has a favorable prognosis while class C is at high risk of death Child Pugh Score in Relation to Liver Function Prognosis and Post op Mortality 90 88 Child Pugh Class Points Liver Function Prognosis Abdominal surgery post operative mortality Child Pugh Class A 5 6 points Good liver function 15 20 years 10 Child Pugh Class B 7 9 points Moderately impaired liver function 30 Child Pugh Class C 10 15 points Advanced liver dysfunction 1 3 years 82 The Child Pugh score is a validated predictor of mortality after a major surgery 88 For example Child class A patients have a 10 mortality rate and Child class B patients have a 30 mortality rate while Child class C patients have a 70 80 mortality rate after abdominal surgery 88 Elective surgery is usually reserved for those in Child class A patients There is an increased risk for child class B individuals and they may require medical optimization Overall it is not recommended for Child class C patients to undergo elective surgery 88 In the past the Child Pugh classification was used to determine people who were candidates for a liver transplant 88 Child Pugh class B is usually an indication for evaluation for transplant 90 However there were many issues when applying this score to liver transplant eligibility 88 Thus the MELD score was created The Model for End Stage Liver Disease MELD score was later developed and approved in 2002 91 It was approved by the United Network for Organ Sharing UNOS as a way to determine the allocation of liver transplants to awaiting people in the United States 92 It is also used as a validated survival predictor of cirrhosis alcoholic hepatitis acute liver failure and acute hepatitis 93 The variables included bilirubin INR creatinine and dialysis frequency 93 In 2016 sodium was added to the variables and the score is often referred to as MELD Na 94 MELD Plus is a further risk score to assess severity of chronic liver disease It was developed in 2017 as a result of a collaboration between Massachusetts General Hospital and IBM 95 Nine variables were identified as effective predictors for 90 day mortality after a discharge from a cirrhosis related hospital admission 95 The variables include all Model for End Stage Liver Disease MELD s components as well as sodium albumin total cholesterol white blood cell count age and length of stay 95 The hepatic venous pressure gradient difference in venous pressure between incoming and outgoing blood to the liver also determines the severity of cirrhosis although it is hard to measure A value of 16 mm or more means a greatly increased risk of death 96 unreliable medical source Prevention editKey prevention strategies for cirrhosis are population wide interventions to reduce alcohol intake through pricing strategies public health campaigns and personal counseling programs to reduce the transmission of viral hepatitis and screening of relatives of people with hereditary liver diseases 97 Little is known about factors affecting cirrhosis risk and progression However many studies have provided increasing evidence for the protective effects of coffee consumption against the progression of liver disease These effects are more noticeable in liver disease that is associated with alcohol use disorder Coffee has antioxidant and antifibrotic effects Caffeine may not be the important component polyphenols may be more important Drinking two or more cups of coffee a day is associated with improvements in the liver enzymes ALT AST and GGT Even in those with liver disease coffee consumption can lower fibrosis and cirrhosis 98 Treatment editGenerally liver damage from cirrhosis cannot be reversed but treatment can stop or delay further progression and reduce complications A healthy diet is encouraged as cirrhosis may be an energy consuming process A recommended diet consists of high protein high fiber diet plus supplementation with branched chain amino acids 99 Close follow up is often necessary Antibiotics are prescribed for infections and various medications can help with itching Laxatives such as lactulose decrease the risk of constipation Carvedilol increases survival benefit for people with cirrhosis and portal hypertension 100 Diuretics in combination with low salt diet reduce fluid in body which helps reduce oedema 101 Alcoholic cirrhosis caused by alcohol use disorder is treated by abstaining from alcohol Treatment for hepatitis related cirrhosis involves medications used to treat the different types of hepatitis such as interferon for viral hepatitis and corticosteroids for autoimmune hepatitis citation needed Cirrhosis caused by Wilson s disease is treated by removing the copper which builds up in organs 2 This is carried out using chelation therapy such as penicillamine When the cause is an iron overload iron is removed using a chelation agent such as deferoxamine or by bloodletting citation needed As of 2021 there are recent studies studying drugs to prevent cirrhosis caused by non alcoholic fatty liver disease NAFLD or NASH A drug called semaglutide was shown to provide greater NASH resolution versus placebo No improvement in fibrosis was observed 102 A combination of cilofexor firsocostat was studied in people with bridging fibrosis and cirrhosis It was observed to have led to improvements in NASH activity with a potential antifibrotic effect 103 Lanifibranor is also shown to prevent worsening fibrosis 104 Preventing further liver damage edit Regardless of the underlying cause of cirrhosis consumption of alcohol and other potentially damaging substances is discouraged There is no evidence that supports the avoidance or dose reduction of paracetamol in people with compensated cirrhosis it is thus considered a safe analgesic for said individuals 105 People who are at risk of being exposed to hepatitis A and hepatitis B should consider vaccines against these diseases citation needed Treating the cause of cirrhosis prevents further damage for example giving oral antivirals such as entecavir and tenofovir where cirrhosis is due to hepatitis B prevents progression of cirrhosis Similarly control of weight and diabetes prevents deterioration in cirrhosis due to non alcoholic fatty liver disease 106 People with cirrhosis or liver damage are often advised to avoid drugs that could further harm the liver 107 These include several drugs such as anti depressants certain antibiotics and NSAIDs like ibuprofen 107 These agents are hepatotoxic as they are metabolized by the liver If a medication that harms the liver is still recommended by a doctor the dosage can be adjusted to aim for minimal stress on the liver citation needed Lifestyle edit According to a 2018 systematic review based on studies that implemented 8 to 14 week long exercise programs there is currently insufficient scientific evidence regarding either the beneficial or harmful effects of physical exercise in people with cirrhosis on all cause mortality morbidity including both serious and non serious adverse events health related quality of life exercise capacity and anthropomorphic measures 108 These conclusions were based on low to very low quality research which imposes the need to develop further research with higher quality especially to evaluate its effects on clinical outcomes citation needed Transplantation edit Main article Liver transplantation If complications cannot be controlled or when the liver ceases functioning liver transplantation is necessary Survival from liver transplantation has been improving over the 1990s and the five year survival rate is now around 80 The survival rate depends largely on the severity of disease and other medical risk factors in the recipient 109 In the United States the MELD score is used to prioritize patients for transplantation 110 Transplantation necessitates the use of immune suppressants ciclosporin or tacrolimus Decompensated cirrhosis edit Manifestations of decompensation in cirrhosis include gastrointestinal bleeding hepatic encephalopathy jaundice or ascites In patients with previously stable cirrhosis decompensation may occur due to various causes such as constipation infection of any source increased alcohol intake medication bleeding from esophageal varices or dehydration It may take the form of any of the complications of cirrhosis listed below People with decompensated cirrhosis generally require admission to a hospital with close monitoring of the fluid balance mental status and emphasis on adequate nutrition and medical treatment often with diuretics antibiotics laxatives or enemas thiamine and occasionally steroids acetylcysteine and pentoxifylline 111 Administration of saline is avoided as it would add to the already high total body sodium content that typically occurs in cirrhosis Life expectancy without liver transplant is low at most three years Palliative care edit Palliative care is specialized medical care that focuses on providing patients with relief from the symptoms pain and stress of a serious illness such as cirrhosis The goal of palliative care is to improve quality of life for both the patient and the patient s family and it is appropriate at any stage and for any type of cirrhosis 112 Especially in the later stages people with cirrhosis experience significant symptoms such as abdominal swelling itching leg edema and chronic abdominal pain which would be amenable for treatment through palliative care 113 Because the disease is not curable without a transplant palliative care can also help with discussions regarding the person s wishes concerning health care power of attorney do not resuscitate decisions and life support and potentially hospice 113 Despite proven benefit people with cirrhosis are rarely referred to palliative care 114 Immunity edit Cirrhosis is known to cause immune dysfunction in numerous ways It impedes the immune system from working normally citation needed Bleeding and blood clot risk edit Cirrhosis can increase the risk of bleeding The liver produces various proteins in the coagulation cascade coagulation factors II VII IX X V and VI When damaged the liver is impaired in its production of these proteins 115 This will ultimately increase bleeding as clotting factors are diminished Clotting function is estimated by lab values mainly platelet count prothrombin time PT and international normalized ratio INR The American Gastroenterological Association AGA provided recommendations in 2021 in regards to coagulopathy management of cirrhotic patients in certain scenarios 115 The AGA does not recommend for extensive pre procedural testing including repeated measurements of PT INR or platelet count before patients with stable cirrhosis undergo common gastrointestinal procedures Nor do they suggest the routine use of blood products such as platelets for bleeding prevention 115 Cirrhosis is stable when there are no changes in baseline abnormalities of coagulation lab values For patients with stable cirrhosis and low platelet count undergoing common low risk procedures the AGA does not recommend the routine use of thrombopoietin receptor agonists for bleeding prevention 115 In hospitalized patients who meet standard guidelines for clot prevention the AGA suggests standard prevention 115 The AGA does not recommend in routine screening for portal vein thrombosis If there is a portal vein thrombosis the AGA suggests treatment by anticoagulation 115 In the case of cirrhosis with atrial fibrillation the AGA recommends using anticoagulation over no anticoagulation 115 Complications editAscites edit Salt restriction is often necessary as cirrhosis leads to accumulation of salt sodium retention Diuretics may be necessary to suppress ascites Diuretic options for inpatient treatment include aldosterone antagonists spironolactone and loop diuretics Aldosterone antagonists are preferred for people who can take oral medications and are not in need of an urgent volume reduction Loop diuretics can be added as additional therapy 116 Where salt restriction and the use of diuretics are ineffective then paracentesis may be the preferred option 117 This procedure requires the insertion of a plastic tube into the peritoneal cavity Human serum albumin solution is usually given to prevent complications from the rapid volume reduction In addition to being more rapid than diuretics 4 5 liters of paracentesis is more successful in comparison to diuretic therapy 116 Esophageal and gastric variceal bleeding edit For portal hypertension nonselective beta blockers such as propranolol or nadolol are commonly used to lower blood pressure over the portal system In severe complications from portal hypertension transjugular intrahepatic portosystemic shunting TIPS is occasionally indicated to relieve pressure on the portal vein As this shunting can worsen hepatic encephalopathy it is reserved for those patients at low risk of encephalopathy TIPS is generally regarded only as a bridge to liver transplantation 118 or as a palliative measure citation needed Balloon occluded retrograde transvenous obliteration can be used to treat gastric variceal bleeding 119 Gastroscopy endoscopic examination of the esophagus stomach and duodenum is performed in cases of established cirrhosis If esophageal varices are found prophylactic local therapy may be applied such as sclerotherapy or banding and beta blockers may be used 120 121 122 Hepatic encephalopathy edit Hepatic encephalopathy is a potential complication of cirrhosis 24 It may lead to functional neurological impairment ranging from mild confusion to coma 24 Hepatic encephalopathy is primarily caused by the accumulation of ammonia in the blood which causes neurotoxicity when crossing the blood brain barrier Ammonia is normally metabolized by the liver as cirrhosis causes both decreased liver function and increased portosystemic shunting allowing blood to bypass the liver systemic ammonia levels gradually rise and lead to encephalopathy 123 Most pharmaceutical approaches to treating hepatic encephalopathy focus on reducing ammonia levels 124 Per 2014 guidelines 125 the first line treatment involves the use of lactulose a non absorbable disaccharide which decreases the pH level of the colon when it is metabolized by intestinal bacteria The lower colonic pH causes increased conversion of ammonia into ammonium which is then excreted from the body 126 Rifaximin an antibiotic that inhibits the function of ammonia producing bacteria in the gastrointestinal tract 127 is recommended for use in combination with lactulose as prophylaxis against recurrent episodes of hepatic encephalopathy 125 128 129 In addition to pharmacotherapy providing proper hydration and nutritional support is also essential 124 Appropriate quantities of protein uptake is encouraged 130 Several factors may precipitate hepatic encephalopathy which include alcohol use excess protein gastrointestinal bleeding infection constipation and vomiting diarrhea 124 Drugs such as benzodiazepines diuretics or narcotics can also precipitate encephalopathic events 124 A low protein diet is recommended with gastrointestinal bleeding 130 The severity of hepatic encephalopathy is determined by assessing the patient s mental status This is generally a subjective assessment although several attempts at creating criteria to help standardize this assessment have been published One example is the West Haven criteria reproduced below Grading of hepatic encephalopathy 131 Grade Mental status Grade 1 Mild Changes in behavior Mild confusion Slurred speech Disordered sleep Grade 2 Moderate Lethargy Moderate confusion Grade 3 Severe Stupor Incoherent Sleeping but arousable Grade 4 Coma Coma Unresponsive Hepatorenal syndrome edit Hepatorenal syndrome is a serious complication of end stage cirrhosis when kidney damage is also involved 132 Spontaneous bacterial peritonitis edit People with ascites due to cirrhosis are at risk of spontaneous bacterial peritonitis Portal hypertensive gastropathy edit Portal hypertensive gastropathy refers to changes in the mucosa of the stomach in people with portal hypertension and is associated with cirrhosis severity 133 Infection edit Cirrhosis can cause immune system dysfunction leading to infection Signs and symptoms of infection may be nonspecific and are more difficult to recognize for example worsening encephalopathy but no fever 134 Moreover infections in cirrhosis are major triggers for other complications ascites variceal bleeding hepatic encephalopathy organ failures death 134 75 77 Hepatocellular carcinoma edit Hepatocellular carcinoma is the most common primary liver cancer and the most common cause of death in people with cirrhosis 135 Screening using an MRI scan can detect this cancer and is often carried out for early signs which has been shown to improve outcomes 2 136 Epidemiology edit nbsp Cirrhosis deaths per million persons in 2012 9 44 45 68 69 88 89 104 105 122 123 152 153 169 170 204 205 282 283 867 nbsp Disability adjusted life year for cirrhosis of the liver per 100 000 inhabitants in 2004 137 no data lt 50 50 100 100 200 200 300 300 400 400 500 500 600 600 700 700 800 800 900 900 1000 gt 1000 Each year approximately one million deaths are due to complications of cirrhosis making cirrhosis the 11th most common cause of death globally 138 Cirrhosis and chronic liver disease were the tenth leading cause of death for men and the twelfth for women in the United States in 2001 killing about 27 000 people each year 139 The cause of cirrhosis can vary alcohol and non alcoholic fatty liver disease are main causes in western and industrialized countries whereas viral hepatitis is the predominant cause in low and middle income countries 138 Cirrhosis is more common in men than in women 140 The cost of cirrhosis in terms of human suffering hospital costs and lost productivity is high Globally age standardized disability adjusted life year DALY rates have decreased from 1990 to 2017 with the values going from 656 4 years per 100 000 people to 510 7 years per 100 000 people 141 In males DALY rates have decreased from 903 1 years per 100 000 population in 1990 to 719 3 years per 100 000 population in 2017 in females the DALY rates have decreased from 415 5 years per 100 000 population in 1990 to 307 6 years per 100 000 population in 2017 141 However globally the total number of DALYs have increased by 10 9 million from 1990 to 2017 reaching the value of 41 4 million DALYs 141 Etymology editThe word cirrhosis is a neologism derived from Greek kirrwsis kirrhos kirros meaning yellowish tawny the orange yellow colour of the diseased liver and the suffix osis i e condition in medical terminology 142 143 144 While the clinical entity was known before Rene Laennec gave it this name in an 1819 paper 18 See also editLiver failureReferences edit a b c d e f g h i j k l m n o p Cirrhosis National Institute of Diabetes and Digestive and Kidney Diseases April 23 2014 Archived from the original on 9 June 2015 Retrieved 19 May 2015 a b c d e Ferri FF 2019 Ferri s clinical advisor 2019 5 books in 1 Philadelphia PA pp 337 339 ISBN 978 0 323 53042 2 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link a b Treatment for Cirrhosis NIDDK National Institute of Diabetes and Digestive and Kidney Diseases Archived from the original on 20 March 2021 Retrieved 6 March 2021 a b Vos T Allen C Arora M Barber RM Bhutta ZA Brown A et al October 2016 Global regional and national incidence prevalence and years lived with disability for 310 diseases and injuries 1990 2015 a systematic analysis for the Global Burden of Disease Study 2015 Lancet 388 10053 1545 1602 doi 10 1016 S0140 6736 16 31678 6 PMC 5055577 PMID 27733282 a b c Wang H Naghavi M Allen C Barber RM Bhutta ZA Carter A et al GBD 2015 Mortality and Causes of Death Collaborators October 2016 Global regional and national life expectancy all cause mortality and cause specific mortality for 249 causes of death 1980 2015 a systematic analysis for the Global Burden of Disease Study 2015 Lancet 388 10053 1459 1544 doi 10 1016 s0140 6736 16 31012 1 PMC 5388903 PMID 27733281 a b c Cirrhosis nhs uk 29 June 2020 Archived from the original on 5 October 2017 Retrieved 8 February 2021 a b c Dooley JS Lok AS Garcia Tsao G Pinzani M 8 June 2018 Sherlock s diseases of the liver and biliary system 13th ed Hoboken NJ p 82 ISBN 978 1 119 23756 3 OCLC 1019837000 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link a b c d e f g h i j k Symptoms amp Causes of Cirrhosis NIDDK National Institute of Diabetes and Digestive and Kidney Diseases Archived from the original on 8 February 2021 Retrieved 8 February 2021 Definition amp Facts for Cirrhosis NIDDK National Institute of Diabetes and Digestive and Kidney Diseases Archived from the original on 2021 03 11 Retrieved 2021 03 10 a b Cirrhosis of the liver cleveland clinic 2024 a b Castera L Friedrich Rust M Loomba R April 2019 Noninvasive Assessment of Liver Disease in Patients With Nonalcoholic Fatty Liver Disease Gastroenterology 156 5 1264 1281 e4 doi 10 1053 j gastro 2018 12 036 PMC 7505052 PMID 30660725 Ilic G Karadzic R Kostic Banovic L Stojanovic J Antovic A February 2010 Ultrastructural Changes In The Liver Of Intravenous Heroin Addiction Bosnian Journal of Basic Medical Sciences Vol 10 no 1 Journal of the Association of Basic Medical Sciences pp 36 43 PMC 5596609 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Retrieved 2022 03 16 a b c Portal Hypertension www hopkinsmedicine org Retrieved 2022 03 16 a b Diagnosis of NAFLD amp NASH NIDDK National Institute of Diabetes and Digestive and Kidney Diseases Archived from the original on 4 March 2021 Retrieved 9 March 2021 a b Meseeha M Attia M 2022 Esophageal Varices StatPearls Treasure Island FL StatPearls Publishing PMID 28846255 Retrieved 2022 03 16 a b Masoodi I Farooq O Singh R Ahmad N Bhat M Wani A January 2009 Courveilhier baumgarten syndrome a rare syndrome revisited International Journal of Health Sciences 3 1 97 99 PMC 3068787 PMID 21475517 Witkowska AB Jasterzbski TJ Schwartz RA 2017 Terry s Nails A Sign of Systemic Disease Indian Journal of Dermatology 62 3 309 311 doi 10 4103 ijd IJD 98 17 inactive 31 January 2024 PMC 5448267 PMID 28584375 a href Template Cite journal html title Template Cite journal cite journal a CS1 maint DOI inactive as of January 2024 link Abd El Meged MM 2019 04 01 Patterns of nail changes in chronic liver diseases Sohag Medical Journal 23 2 166 170 doi 10 21608 smj 2019 47672 ISSN 1687 8353 S2CID 203813520 a b c d e f g h i j k l m n o p q r s t u v Friedman L 2018 Handbook of Liver Disease 4e Elsevier ISBN 978 0 323 47874 8 Brennan D What Is Fetor Hepaticus WebMD Retrieved 2022 03 17 Samji NS Buggs AM Roy PK 2021 10 17 Anand BS ed Viral Hepatitis Background Pathophysiology Etiology Medscape WebMD LLC a b Perz JF Armstrong GL Farrington LA Hutin YJ Bell BP October 2006 The contributions of hepatitis B virus and hepatitis C virus infections to cirrhosis and primary liver cancer worldwide Journal of Hepatology 45 4 529 538 doi 10 1016 j jhep 2006 05 013 PMID 16879891 Cirrhosis of the Liver American Liver Foundation Retrieved 2022 03 17 a b Stickel F Datz C Hampe J Bataller R March 2017 Pathophysiology and Management of Alcoholic Liver Disease Update 2016 Gut and Liver 11 2 173 188 doi 10 5009 gnl16477 PMC 5347641 PMID 28274107 a b c Friedman LS 2014 Current medical diagnosis and treatment 2014 S l Mcgraw Hill pp Chapter 16 Liver Biliary Tract amp Pancreas Disorders ISBN 978 0 07 180633 6 a b c d e Machado MV Diehl AM 2018 Pathogenesis of Nonalcoholic Fatty Liver Disease In Sanyal AJ Boyer TD Terrault NA Lindor KD eds Zakim and Boyer s Hepatology pp 369 390 doi 10 1016 c2013 0 19055 1 ISBN 978 0 323 37591 7 Golabi P Paik JM Arshad T Younossi Y Mishra A Younossi ZM August 2020 Mortality of NAFLD According to the Body Composition and Presence of Metabolic Abnormalities Hepatology Communications 4 8 1136 1148 doi 10 1002 hep4 1534 PMC 7395070 PMID 32766474 Heroin Addiction Health Conditions Bedrock Recovery Center Retrieved August 7 2022 a b c Primary Biliary Cholangitis Symptoms Causes Treatments Cleveland Clinic Retrieved 2022 03 17 Coenen IC Houwen RH January 2019 Indian childhood cirrhosis and other disorders of copper handling Clinical and Translational Perspectives on Wiloson Disease Academic Press pp 449 453 doi 10 1016 B978 0 12 810532 0 00044 6 ISBN 978 0 12 810532 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