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Gray baby syndrome

January 01, 1970

Not to be confused with Bronze baby syndrome.

Gray baby syndrome (also termed gray syndrome or grey syndrome) is a rare but serious, even fatal, side effect that occurs in newborn infants (especially premature babies) following the accumulation of the antibiotic chloramphenicol.[1] Chloramphenicol is a broad-spectrum antibiotic that has been used to treat a variety of bacteria infections like Streptococcus pneumoniae as well as typhoid fever, meningococcal sepsis, cholera, and eye infections.[2][3] Chloramphenicol works by binding to ribosomal subunits which blocks transfer ribonucleic acid (RNA) and prevents the synthesis of bacterial proteins.[4][5] Chloramphenicol has also been used to treat neonates born before 37 weeks of the gestational period for prophylactic purposes.[2][6][4] In 1958, newborns born prematurely due to rupture of the amniotic sac were given chloramphenicol to prevent possible infections, and it was noticed that these newborns had a higher mortality rate compared with those who were not treated with the antibiotic.[7] Over the years, chloramphenicol has been used less in clinical practice due to the risks of toxicity not only to neonates, but also to adults due to the risk of aplastic anemia.[3][8][9] Chloramphenicol is now reserved to treat certain severe bacteria infections that were not successfully treated with other antibiotic medications.

Gray baby syndrome
Other namesGrey baby syndrome, gray syndrome, grey syndrome
SpecialtyPediatrics, infectious disease, toxicology
SymptomsVomiting, greenish diarrhea, abdominal distension, hypothermia, pallid cyanosis, irregular respiration, circulatory collapse
ComplicationsBleeding, hepatic failure, anemia, kernicterus, death
Usual onsetNeonates
CausesAccumulation of chloramphenicol
Diagnostic methodproper history taking, monitoring blood level of the drug

Signs and symptoms edit

Since the syndrome is due to the accumulation of chloramphenicol, the signs and symptoms are dose related.[10] According to Kasten's review published in the Mayo Clinic Proceedings, a serum concentration of more than 50 μg/mL is a warning sign,[10] while Hammett-Stabler and John states that the common therapeutics peak level is 10-20 μg/mL and is expected to achieve after 0.5-1.5 hours of intravenous administration in their review of antimicrobial drugs.[11] The common onset of signs and symptoms are 2 to 9 days after the initiation of the medication, which allows the serum concentration to build up to reach the toxic concentration above. Common signs and symptoms include loss of appetite, fussiness, vomiting, ashen gray color of the skin, hypotension (low blood pressure), cyanosis (blue discoloration of lips and skin), hypothermia, cardiovascular collapse, hypotonia (muscle stiffness), abdominal distension, irregular respiration, and increased blood lactate.[6]

Pathophysiology edit

Two pathophysiologic mechanisms are thought to play a role in the development of gray baby syndrome after exposure to chloramphenicol. This condition is due to a lack of glucuronidation reactions occurring in the baby (phase II hepatic metabolism), thus leading to an accumulation of toxic chloramphenicol metabolites:[12]

  1. Metabolism: The UDP-glucuronyl transferase enzyme system in infants, especially premature infants, is not fully developed and incapable of metabolizing the excessive drug load needed to excrete chloramphenicol.[6]
  2. Elimination: Insufficient renal excretion of the unconjugated drug.

Insufficient metabolism and excretion of chloramphenicol leads to increased blood concentrations of the drug, causing blockade of the electron transport of the liver, myocardium, and skeletal muscles. Since the electron transport is an essential part of cellular respiration, its blockade can result in cell damage. In addition, the presence of chloramphenicol weakens the binding of bilirubin and albumin, so increased levels of the drug can lead to high levels of free bilirubin in the blood, resulting in brain damage or kernicterus.[6] If left untreated, possible bleeding, renal (kidney) and/or hepatic (liver) failure, anemia, infection, confusion, weakness, blurred vision, or eventually death are expected. Additionally, chloramphenicol is significantly insoluble due to an absence of acidic and basic groups in its molecular compound. As a result, larger amounts of the medication are required to achieve the desired therapeutic effect. High volumes of a medication that can cause various toxicities is another avenue how chloramphenicol can potentially lead to grey baby syndrome.[13]

Diagnosis edit

Gray baby syndrome should be suspected in a new born with abdominal distension, progressive pallid cyanosis, irregular respirations, and refusal to breastfeed. The cause of gray baby syndrome can come from the direct use of intravenous or oral chloramphenicol in neonates.[6] Direct chronological relation between the use of the medication and signs and symptoms of the syndrome should be found in the previous medical history. In terms of the possible route of chloramphenicol, gray baby syndrome may not come from the mother's use of chloramphenicol during pregnancy or breastfeeding. According to the Drug and Lactation database (LactMed), it states that "milk concentrations are not sufficient to induce gray baby syndrome".[14] It is also reported that the syndrome may not develop in infants when their mothers use the medication in their late period of pregnancy.[15] According to the Oxford Review, chloramphenicol given to mothers during their pregnancy did not result in gray baby syndrome, but was caused by infants receiving supra-therapeutic doses of chloramphenicol after birth.[16] The presentation of symptoms can depend on the level of exposure of the drug to the baby, given its dose-related nature. A broad diagnosis is usually needed for babies who present with cyanosis. To support the diagnosis, blood work should be done to determine the level of serum chloramphenicol, and to further evaluate chloramphenicol toxicity, a complete blood panel including levels of serum ketones, glucose (due to the risk of hypoglycemia), metabolic panel should be completed to help determine if an infant has the syndrome.[6] Other tools used to help with diagnosis include CT scans, ultrasound, and electrocardiogram.[6]

Prevention edit

Since the syndrome is a side effect of chloramphenicol, the prevention is primarily related to the proper use of the medication. The WHO Model Formulary for Children 2010 recommends to reserve chloramphenicol for life-threatening infections.[15] As well as using chloramphenicol only when necessary, it should also be used in short periods of time to also prevent the potential for toxicity.[4] In particular, this medication should not be prescribed especially in neonates less than one week old due to the significant risk of toxicity. Preterm infants especially should not be administered chloramphenicol.[4] Gray baby syndrome has been noted to be dose-dependent as it typically occurs in neonates who have received a daily dose greater than 200 milligrams.[6]

When chloramphenicol is necessary, the condition can be prevented by using chloramphenicol at the recommended doses and monitoring blood levels,[17][18][19][20] or alternatively, third generation cephalosporins can be effectively substituted for the drug, without the associated toxicity.[21] Also, repeated course of administration and prolonged treatment should be avoided as much as possible.[15] In terms of hepatic development in neonates, it take only weeks from birth for them to develop their UDPGT expression and function to be at an adult-like level, while the function is only about 1% in the late pregnancy, even right before birth-giving.[22] According to MSD Manuals, chloramphenicol should not be given to neonates with younger than 1 month of age with more than a dose of 25 mg/kg/day to start with.[23] The serum concentration of the medication should be monitored to titrate to a therapeutic level and to prevent toxicity. Medication reconciliation of other medications that neonates may be taking that can decrease blood cell count should be monitored because of this medication's ability to suppress bone marrow activity.[4] Rifampicin and trimethoprim are examples of medications with bone marrow suppression abilities and are contraindicated for concomitant use with chloramphenicol.[4] In regards to bone marrow suppression, chloramphenicol has two major etiological manifestations. The first mechanism of bone marrow suppression affects the formation of blood cells such as erythrocytes, and this can be reversible since it is an early sign of toxicity. The second form of bone marrow suppression is bone marrow aplasia, which is associated with being late into toxicity and cannot be reversed in some cases.[24] Chloramphenicol is contraindicated in persons who are breastfeeding due to the risk of toxic effects in the baby, but if maternal use of chloramphenicol cannot be avoided, close monitoring of the baby's symptoms such as feeding difficulties, and blood work is recommended.[25][26]

Treatment edit

Chloramphenicol therapy should be stopped immediately if objective or subjective signs of gray baby syndrome are suspected since gray baby syndrome can be fatal for the infant if it is not diagnosed early on as it can lead to anemia, shock, and end-organ damage.[6] After discontinuing the antibiotic, the side effects caused by the toxicity should be treated. This includes treating hypoglycemia to help prevent hemodynamic instability, as well as increasing the temperature of the infant if they have developed hypothermia.[6] Since symptoms of gray baby syndrome are correlated with elevated serum chloramphenicol concentrations, exchange transfusion may be required to remove the drug, charcoal column hemoperfusion is a type of transfusion that has shown significant effects but is associated with numerous side effects.[18] The associated side effects isn't the only reason why this method of treatment is not a first line therapy. According to the American Journal of Kidney Diseases, elevated cartridge prices and viable lifespan of the product are deterring factors to consider.[27] Phenobarbital and theophylline are two drugs in particular that have shown significant efficacy with charcoal hemoperfusion, aside from its most significant indication for chronic aluminum toxicity in people with end-stage renal disease (ESRD) traditionally.[27] Sometimes, phenobarbital is used to induce UDP-glucuronyl transferase enzyme function. For hemodynamically unstable neonates, supportive care measures such as resuscitation, oxygenation, and treatment for hypothermia are common practices when cessation of chloramphenicol alone is insufficient.[6] With sepsis being a complication of severe gray baby syndrome, usage of broad-spectrum antibiotics such as vancomycin, for example, is a recommended treatment option. Third generation antibiotics have also proven efficacy in treating gray baby-induced sepsis.[6]

References edit

  1. ^ McIntyre J, Choonara I (2004). "Drug toxicity in the neonate". Biology of the Neonate. 86 (4): 218–21. doi:10.1159/000079656. PMID 15249753. S2CID 29906856.
  2. ^ a b Deveci A, Coban AY (September 2014). "Optimum management of Citrobacter koseri infection". Expert Review of Anti-Infective Therapy. 12 (9): 1137–42. doi:10.1586/14787210.2014.944505. PMID 25088467. S2CID 37304019.
  3. ^ a b "Chloramphenicol", LiverTox: Clinical and Research Information on Drug-Induced Liver Injury, Bethesda (MD): National Institute of Diabetes and Digestive and Kidney Diseases, 2012, PMID 31643435, retrieved 2021-08-02
  4. ^ a b c d e f Oong GC, Tadi P (2021). "Chloramphenicol". StatPearls. Treasure Island (FL): StatPearls Publishing. PMID 32310426. Retrieved 2021-08-02.
  5. ^ Vázquez-Laslop N, Mankin AS (September 2018). "Context-Specific Action of Ribosomal Antibiotics". Annual Review of Microbiology. 72 (1): 185–207. doi:10.1146/annurev-micro-090817-062329. PMC 8742604. PMID 29906204.
  6. ^ a b c d e f g h i j k l Cummings ED, Kong EL, Edens MA (2021). "Gray Baby Syndrome". StatPearls. Treasure Island (FL): StatPearls Publishing. PMID 28846297. Retrieved 2021-07-30.
  7. ^ Powell DA, Nahata MC (April 1982). "Chloramphenicol: new perspectives on an old drug". Drug Intelligence & Clinical Pharmacy. 16 (4): 295–300. doi:10.1177/106002808201600404. PMID 7040026. S2CID 103247.
  8. ^ Ingebrigtsen SG, Didriksen A, Johannessen M, Škalko-Basnet N, Holsæter AM (June 2017). "Old drug, new wrapping – A possible comeback for chloramphenicol?". International Journal of Pharmaceutics. 526 (1–2): 538–546. doi:10.1016/j.ijpharm.2017.05.025. hdl:10037/12466. PMID 28506801.
  9. ^ Beninger P (December 2018). "Pharmacovigilance: An Overview". Clinical Therapeutics. 40 (12): 1991–2004. doi:10.1016/j.clinthera.2018.07.012. PMID 30126707.
  10. ^ a b Kasten MJ (1999). "Clindamycin, metronidazole, and chloramphenicol". Mayo Clinic Proceedings. 74 (8): 825–33. doi:10.4065/74.8.825. PMID 10473362.
  11. ^ Hammett-Stabler CA, Johns T (1998). "Laboratory guidelines for monitoring of antimicrobial drugs". Clinical Chemistry. 44 (5): 1129–40. doi:10.1093/clinchem/44.5.1129. PMID 9590397.
  12. ^ Chambers HF (2005). "Chapter 46. Protein Synthesis Inhibitors and Miscellaneous Antibacterial Agents". In Brunton EL, Lazo JS, Parker K (eds.). Goodman & Gilman's The Pharmacological Basis of Therapeutics (11th ed.). New York: McGraw-Hill. pp. 1173–1202. ISBN 978-0-07-142280-2.
  13. ^ Meissner HC, Smith AL (1979). "The current status of chloramphenicol". Pediatrics. 64 (3): 348–56. doi:10.1542/peds.64.3.348. PMID 384354. S2CID 33410918.
  14. ^ "Chloramphenicol". Drugs and Lactation Database (LactMed). Bethesda (MD): National Library of Medicine (US). 2006. PMID 30000554. Retrieved 2021-07-30.
  15. ^ a b c "Chloramphenicol". WHO model formulary for children 2010. World Health Organization. 2010. pp. 99–101. hdl:10665/44309. ISBN 978-92-4-159932-0.
  16. ^ Yu PA, Tran EL, Parker CM, Kim HJ, Yee EL, Smith PW, et al. (2020). "Safety of Antimicrobials During Pregnancy: A Systematic Review of Antimicrobials Considered for Treatment and Postexposure Prophylaxis of Plague". Clinical Infectious Diseases. 70 (Suppl 1): S37–S50. doi:10.1093/cid/ciz1231. PMC 10867625. PMID 32435799.
  17. ^ Feder HM (1986). "Chloramphenicol: what we have learned in the last decade". Southern Medical Journal. 79 (9): 1129–34. doi:10.1097/00007611-198609000-00022. PMID 3529436.
  18. ^ a b Mulhall A, de Louvois J, Hurley R (1983). "Chloramphenicol toxicity in neonates: its incidence and prevention". British Medical Journal. 287 (6403): 1424–7. doi:10.1136/bmj.287.6403.1424. PMC 1549666. PMID 6416440.
  19. ^ Forster J, Hufschmidt C, Niederhoff H, Künzer W (1985). "[Need for the determination of chloramphenicol levels in the treatment of bacterial-purulent meningitis with chloramphenicol succinate in infants and small children]". Monatsschrift Kinderheilkunde. 133 (4): 209–13. PMID 4000136.
  20. ^ Meyers RS, Thackray J, Matson KL, McPherson C, Lubsch L, Hellinga RC, Hoff DS (2020). "Key Potentially Inappropriate Drugs in Pediatrics: The KIDs List". The Journal of Pediatric Pharmacology and Therapeutics. 25 (3): 175–191. doi:10.5863/1551-6776-25.3.175. PMC 7134587. PMID 32265601.
  21. ^ Aggarwal R, Sarkar N, Deorari AK, Paul VK (2001). "Sepsis in the newborn". Indian Journal of Pediatrics. 68 (12): 1143–7. doi:10.1007/BF02722932. PMID 11838570. S2CID 20554642.
  22. ^ Grijalva J, Vakili K (2013). "Neonatal liver physiology". Seminars in Pediatric Surgery. 22 (4): 185–9. doi:10.1053/j.sempedsurg.2013.10.006. PMID 24331092.
  23. ^ Werth, Brian J (2020). "Chloramphenicol". MSD Manual Professional Edition. Retrieved 2021-07-30.
  24. ^ Padberg S (2016). "Chloramphenicol". In Schaefer C, Peters P, Miller RK (eds.). Meyler's Side Effects of Drugs: The International Encyclopedia of Adverse Drug Reactions and Interactions (Sixteenth ed.). Amsterdam. pp. 229–236. doi:10.1016/B978-0-444-53717-1.00472-8. ISBN 978-0-444-53716-4.{{cite book}}: CS1 maint: location missing publisher (link)
  25. ^ Padberg S (2015). "Anti-infectives". Drugs During Pregnancy and Lactation (Third ed.). Academic Press. pp. 687–703. doi:10.1016/B978-0-12-408078-2.00029-9. ISBN 9780124080782.
  26. ^ National Toxicology Program (2011). "NTP 12th Report on Carcinogens". Report on Carcinogens: Carcinogen Profiles. 12: iii–499. ISSN 1551-8280. PMID 21822324.
  27. ^ a b Shalkham AS, Kirrane BM, Hoffman RS, Goldfarb DS, Nelson LS (2006). "The availability and use of charcoal hemoperfusion in the treatment of poisoned patients". American Journal of Kidney Diseases. 48 (2): 239–41. doi:10.1053/j.ajkd.2006.04.080. PMID 16860189.

Further reading edit

  • Krasinski K, Perkin R, Rutledge J (1982). "Gray baby syndrome revisited". Clinical Pediatrics. 21 (9): 571–2. doi:10.1177/000992288202100910. PMID 7105617. S2CID 31417519.
  • Feigin RD, Cherry JD, Demmler-Harrison GJ, Kaplan SL, eds. (2009). "Ch.248. Antibacterial therapeutic agents". Feigin & Cherry's textbook of pediatric infectious diseases (6th ed.). Philadelphia, PA: Saunders/Elsevier. ISBN 978-1-4160-4044-6.

External links edit

January 01, 1970
gray, baby, syndrome, confused, with, bronze, baby, syndrome, also, termed, gray, syndrome, grey, syndrome, rare, serious, even, fatal, side, effect, that, occurs, newborn, infants, especially, premature, babies, following, accumulation, antibiotic, chloramphe. Not to be confused with Bronze baby syndrome Gray baby syndrome also termed gray syndrome or grey syndrome is a rare but serious even fatal side effect that occurs in newborn infants especially premature babies following the accumulation of the antibiotic chloramphenicol 1 Chloramphenicol is a broad spectrum antibiotic that has been used to treat a variety of bacteria infections like Streptococcus pneumoniae as well as typhoid fever meningococcal sepsis cholera and eye infections 2 3 Chloramphenicol works by binding to ribosomal subunits which blocks transfer ribonucleic acid RNA and prevents the synthesis of bacterial proteins 4 5 Chloramphenicol has also been used to treat neonates born before 37 weeks of the gestational period for prophylactic purposes 2 6 4 In 1958 newborns born prematurely due to rupture of the amniotic sac were given chloramphenicol to prevent possible infections and it was noticed that these newborns had a higher mortality rate compared with those who were not treated with the antibiotic 7 Over the years chloramphenicol has been used less in clinical practice due to the risks of toxicity not only to neonates but also to adults due to the risk of aplastic anemia 3 8 9 Chloramphenicol is now reserved to treat certain severe bacteria infections that were not successfully treated with other antibiotic medications Gray baby syndromeOther namesGrey baby syndrome gray syndrome grey syndromeSpecialtyPediatrics infectious disease toxicologySymptomsVomiting greenish diarrhea abdominal distension hypothermia pallid cyanosis irregular respiration circulatory collapseComplicationsBleeding hepatic failure anemia kernicterus deathUsual onsetNeonatesCausesAccumulation of chloramphenicolDiagnostic methodproper history taking monitoring blood level of the drug Contents 1 Signs and symptoms 2 Pathophysiology 3 Diagnosis 4 Prevention 5 Treatment 6 References 7 Further reading 8 External linksSigns and symptoms editSince the syndrome is due to the accumulation of chloramphenicol the signs and symptoms are dose related 10 According to Kasten s review published in the Mayo Clinic Proceedings a serum concentration of more than 50 mg mL is a warning sign 10 while Hammett Stabler and John states that the common therapeutics peak level is 10 20 mg mL and is expected to achieve after 0 5 1 5 hours of intravenous administration in their review of antimicrobial drugs 11 The common onset of signs and symptoms are 2 to 9 days after the initiation of the medication which allows the serum concentration to build up to reach the toxic concentration above Common signs and symptoms include loss of appetite fussiness vomiting ashen gray color of the skin hypotension low blood pressure cyanosis blue discoloration of lips and skin hypothermia cardiovascular collapse hypotonia muscle stiffness abdominal distension irregular respiration and increased blood lactate 6 Pathophysiology editTwo pathophysiologic mechanisms are thought to play a role in the development of gray baby syndrome after exposure to chloramphenicol This condition is due to a lack of glucuronidation reactions occurring in the baby phase II hepatic metabolism thus leading to an accumulation of toxic chloramphenicol metabolites 12 Metabolism The UDP glucuronyl transferase enzyme system in infants especially premature infants is not fully developed and incapable of metabolizing the excessive drug load needed to excrete chloramphenicol 6 Elimination Insufficient renal excretion of the unconjugated drug Insufficient metabolism and excretion of chloramphenicol leads to increased blood concentrations of the drug causing blockade of the electron transport of the liver myocardium and skeletal muscles Since the electron transport is an essential part of cellular respiration its blockade can result in cell damage In addition the presence of chloramphenicol weakens the binding of bilirubin and albumin so increased levels of the drug can lead to high levels of free bilirubin in the blood resulting in brain damage or kernicterus 6 If left untreated possible bleeding renal kidney and or hepatic liver failure anemia infection confusion weakness blurred vision or eventually death are expected Additionally chloramphenicol is significantly insoluble due to an absence of acidic and basic groups in its molecular compound As a result larger amounts of the medication are required to achieve the desired therapeutic effect High volumes of a medication that can cause various toxicities is another avenue how chloramphenicol can potentially lead to grey baby syndrome 13 Diagnosis editGray baby syndrome should be suspected in a new born with abdominal distension progressive pallid cyanosis irregular respirations and refusal to breastfeed The cause of gray baby syndrome can come from the direct use of intravenous or oral chloramphenicol in neonates 6 Direct chronological relation between the use of the medication and signs and symptoms of the syndrome should be found in the previous medical history In terms of the possible route of chloramphenicol gray baby syndrome may not come from the mother s use of chloramphenicol during pregnancy or breastfeeding According to the Drug and Lactation database LactMed it states that milk concentrations are not sufficient to induce gray baby syndrome 14 It is also reported that the syndrome may not develop in infants when their mothers use the medication in their late period of pregnancy 15 According to the Oxford Review chloramphenicol given to mothers during their pregnancy did not result in gray baby syndrome but was caused by infants receiving supra therapeutic doses of chloramphenicol after birth 16 The presentation of symptoms can depend on the level of exposure of the drug to the baby given its dose related nature A broad diagnosis is usually needed for babies who present with cyanosis To support the diagnosis blood work should be done to determine the level of serum chloramphenicol and to further evaluate chloramphenicol toxicity a complete blood panel including levels of serum ketones glucose due to the risk of hypoglycemia metabolic panel should be completed to help determine if an infant has the syndrome 6 Other tools used to help with diagnosis include CT scans ultrasound and electrocardiogram 6 Prevention editSince the syndrome is a side effect of chloramphenicol the prevention is primarily related to the proper use of the medication The WHO Model Formulary for Children 2010 recommends to reserve chloramphenicol for life threatening infections 15 As well as using chloramphenicol only when necessary it should also be used in short periods of time to also prevent the potential for toxicity 4 In particular this medication should not be prescribed especially in neonates less than one week old due to the significant risk of toxicity Preterm infants especially should not be administered chloramphenicol 4 Gray baby syndrome has been noted to be dose dependent as it typically occurs in neonates who have received a daily dose greater than 200 milligrams 6 When chloramphenicol is necessary the condition can be prevented by using chloramphenicol at the recommended doses and monitoring blood levels 17 18 19 20 or alternatively third generation cephalosporins can be effectively substituted for the drug without the associated toxicity 21 Also repeated course of administration and prolonged treatment should be avoided as much as possible 15 In terms of hepatic development in neonates it take only weeks from birth for them to develop their UDPGT expression and function to be at an adult like level while the function is only about 1 in the late pregnancy even right before birth giving 22 According to MSD Manuals chloramphenicol should not be given to neonates with younger than 1 month of age with more than a dose of 25 mg kg day to start with 23 The serum concentration of the medication should be monitored to titrate to a therapeutic level and to prevent toxicity Medication reconciliation of other medications that neonates may be taking that can decrease blood cell count should be monitored because of this medication s ability to suppress bone marrow activity 4 Rifampicin and trimethoprim are examples of medications with bone marrow suppression abilities and are contraindicated for concomitant use with chloramphenicol 4 In regards to bone marrow suppression chloramphenicol has two major etiological manifestations The first mechanism of bone marrow suppression affects the formation of blood cells such as erythrocytes and this can be reversible since it is an early sign of toxicity The second form of bone marrow suppression is bone marrow aplasia which is associated with being late into toxicity and cannot be reversed in some cases 24 Chloramphenicol is contraindicated in persons who are breastfeeding due to the risk of toxic effects in the baby but if maternal use of chloramphenicol cannot be avoided close monitoring of the baby s symptoms such as feeding difficulties and blood work is recommended 25 26 Treatment editChloramphenicol therapy should be stopped immediately if objective or subjective signs of gray baby syndrome are suspected since gray baby syndrome can be fatal for the infant if it is not diagnosed early on as it can lead to anemia shock and end organ damage 6 After discontinuing the antibiotic the side effects caused by the toxicity should be treated This includes treating hypoglycemia to help prevent hemodynamic instability as well as increasing the temperature of the infant if they have developed hypothermia 6 Since symptoms of gray baby syndrome are correlated with elevated serum chloramphenicol concentrations exchange transfusion may be required to remove the drug charcoal column hemoperfusion is a type of transfusion that has shown significant effects but is associated with numerous side effects 18 The associated side effects isn t the only reason why this method of treatment is not a first line therapy According to the American Journal of Kidney Diseases elevated cartridge prices and viable lifespan of the product are deterring factors to consider 27 Phenobarbital and theophylline are two drugs in particular that have shown significant efficacy with charcoal hemoperfusion aside from its most significant indication for chronic aluminum toxicity in people with end stage renal disease ESRD traditionally 27 Sometimes phenobarbital is used to induce UDP glucuronyl transferase enzyme function For hemodynamically unstable neonates supportive care measures such as resuscitation oxygenation and treatment for hypothermia are common practices when cessation of chloramphenicol alone is insufficient 6 With sepsis being a complication of severe gray baby syndrome usage of broad spectrum antibiotics such as vancomycin for example is a recommended treatment option Third generation antibiotics have also proven efficacy in treating gray baby induced sepsis 6 References edit McIntyre J Choonara I 2004 Drug toxicity in the neonate Biology of the Neonate 86 4 218 21 doi 10 1159 000079656 PMID 15249753 S2CID 29906856 a b Deveci A Coban AY September 2014 Optimum management of Citrobacter koseri infection Expert Review of Anti Infective Therapy 12 9 1137 42 doi 10 1586 14787210 2014 944505 PMID 25088467 S2CID 37304019 a b Chloramphenicol LiverTox Clinical and Research Information on Drug Induced Liver Injury Bethesda MD National Institute of Diabetes and Digestive and Kidney Diseases 2012 PMID 31643435 retrieved 2021 08 02 a b c d e f Oong GC Tadi P 2021 Chloramphenicol StatPearls Treasure Island FL StatPearls Publishing PMID 32310426 Retrieved 2021 08 02 Vazquez Laslop N Mankin AS September 2018 Context Specific Action of Ribosomal Antibiotics Annual Review of Microbiology 72 1 185 207 doi 10 1146 annurev micro 090817 062329 PMC 8742604 PMID 29906204 a b c d e f g h i j k l Cummings ED Kong EL Edens MA 2021 Gray Baby Syndrome StatPearls Treasure Island FL StatPearls Publishing PMID 28846297 Retrieved 2021 07 30 Powell DA Nahata MC April 1982 Chloramphenicol new perspectives on an old drug Drug Intelligence amp Clinical Pharmacy 16 4 295 300 doi 10 1177 106002808201600404 PMID 7040026 S2CID 103247 Ingebrigtsen SG Didriksen A Johannessen M Skalko Basnet N Holsaeter AM June 2017 Old drug new wrapping A possible comeback for chloramphenicol International Journal of Pharmaceutics 526 1 2 538 546 doi 10 1016 j ijpharm 2017 05 025 hdl 10037 12466 PMID 28506801 Beninger P December 2018 Pharmacovigilance An Overview Clinical Therapeutics 40 12 1991 2004 doi 10 1016 j clinthera 2018 07 012 PMID 30126707 a b Kasten MJ 1999 Clindamycin metronidazole and chloramphenicol Mayo Clinic Proceedings 74 8 825 33 doi 10 4065 74 8 825 PMID 10473362 Hammett Stabler CA Johns T 1998 Laboratory guidelines for monitoring of antimicrobial drugs Clinical Chemistry 44 5 1129 40 doi 10 1093 clinchem 44 5 1129 PMID 9590397 Chambers HF 2005 Chapter 46 Protein Synthesis Inhibitors and Miscellaneous Antibacterial Agents In Brunton EL Lazo JS Parker K eds Goodman amp Gilman s The Pharmacological Basis of Therapeutics 11th ed New York McGraw Hill pp 1173 1202 ISBN 978 0 07 142280 2 Meissner HC Smith AL 1979 The current status of chloramphenicol Pediatrics 64 3 348 56 doi 10 1542 peds 64 3 348 PMID 384354 S2CID 33410918 Chloramphenicol Drugs and Lactation Database LactMed Bethesda MD National Library of Medicine US 2006 PMID 30000554 Retrieved 2021 07 30 a b c Chloramphenicol WHO model formulary for children 2010 World Health Organization 2010 pp 99 101 hdl 10665 44309 ISBN 978 92 4 159932 0 Yu PA Tran EL Parker CM Kim HJ Yee EL Smith PW et al 2020 Safety of Antimicrobials During Pregnancy A Systematic Review of Antimicrobials Considered for Treatment and Postexposure Prophylaxis of Plague Clinical Infectious Diseases 70 Suppl 1 S37 S50 doi 10 1093 cid ciz1231 PMC 10867625 PMID 32435799 Feder HM 1986 Chloramphenicol what we have learned in the last decade Southern Medical Journal 79 9 1129 34 doi 10 1097 00007611 198609000 00022 PMID 3529436 a b Mulhall A de Louvois J Hurley R 1983 Chloramphenicol toxicity in neonates its incidence and prevention British Medical Journal 287 6403 1424 7 doi 10 1136 bmj 287 6403 1424 PMC 1549666 PMID 6416440 Forster J Hufschmidt C Niederhoff H Kunzer W 1985 Need for the determination of chloramphenicol levels in the treatment of bacterial purulent meningitis with chloramphenicol succinate in infants and small children Monatsschrift Kinderheilkunde 133 4 209 13 PMID 4000136 Meyers RS Thackray J Matson KL McPherson C Lubsch L Hellinga RC Hoff DS 2020 Key Potentially Inappropriate Drugs in Pediatrics The KIDs List The Journal of Pediatric Pharmacology and Therapeutics 25 3 175 191 doi 10 5863 1551 6776 25 3 175 PMC 7134587 PMID 32265601 Aggarwal R Sarkar N Deorari AK Paul VK 2001 Sepsis in the newborn Indian Journal of Pediatrics 68 12 1143 7 doi 10 1007 BF02722932 PMID 11838570 S2CID 20554642 Grijalva J Vakili K 2013 Neonatal liver physiology Seminars in Pediatric Surgery 22 4 185 9 doi 10 1053 j sempedsurg 2013 10 006 PMID 24331092 Werth Brian J 2020 Chloramphenicol MSD Manual Professional Edition Retrieved 2021 07 30 Padberg S 2016 Chloramphenicol In Schaefer C Peters P Miller RK eds Meyler s Side Effects of Drugs The International Encyclopedia of Adverse Drug Reactions and Interactions Sixteenth ed Amsterdam pp 229 236 doi 10 1016 B978 0 444 53717 1 00472 8 ISBN 978 0 444 53716 4 a href Template Cite book html title Template Cite book cite book a CS1 maint location missing publisher link Padberg S 2015 Anti infectives Drugs During Pregnancy and Lactation Third ed Academic Press pp 687 703 doi 10 1016 B978 0 12 408078 2 00029 9 ISBN 9780124080782 National Toxicology Program 2011 NTP 12th Report on Carcinogens Report on Carcinogens Carcinogen Profiles 12 iii 499 ISSN 1551 8280 PMID 21822324 a b Shalkham AS Kirrane BM Hoffman RS Goldfarb DS Nelson LS 2006 The availability and use of charcoal hemoperfusion in the treatment of poisoned patients American Journal of Kidney Diseases 48 2 239 41 doi 10 1053 j ajkd 2006 04 080 PMID 16860189 Further reading editKrasinski K Perkin R Rutledge J 1982 Gray baby syndrome revisited Clinical Pediatrics 21 9 571 2 doi 10 1177 000992288202100910 PMID 7105617 S2CID 31417519 Feigin RD Cherry JD Demmler Harrison GJ Kaplan SL eds 2009 Ch 248 Antibacterial therapeutic agents Feigin amp Cherry s textbook of pediatric infectious diseases 6th ed Philadelphia PA Saunders Elsevier ISBN 978 1 4160 4044 6 External links edit Retrieved from https en wikipedia org w index php title Gray baby syndrome amp oldid 1208849522, wikipedia, wiki, book, books, library,

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