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Model for End-Stage Liver Disease

April 12, 2024

The Model for End-Stage Liver Disease, or MELD, is a scoring system for assessing the severity of chronic liver disease. It was initially developed to predict mortality within three months of surgery in patients who had undergone a transjugular intrahepatic portosystemic shunt (TIPS) procedure,[1] and was subsequently found to be useful in determining prognosis and prioritizing for receipt of a liver transplant.[2][3] This score is now used by the United Network for Organ Sharing (UNOS) and Eurotransplant for prioritizing allocation of liver transplants instead of the older Child-Pugh score.[3][4]

Model for End-Stage Liver Disease
SynonymsMELD
PurposeAssess the severity of chronic liver disease
Based onSerum creatinine, INR, and bilirubin

Determination edit

MELD uses the patient's values for serum bilirubin, serum creatinine, and the international normalized ratio for prothrombin time (INR) to predict survival. It is calculated according to the following formula:[3]

 

MELD scores are reported as whole numbers, so the result of the equation above is rounded.

UNOS has made the following modifications to the score:[5]

  • If the patient has been dialyzed twice within the last 7 days, then the value of serum creatinine should be 4.0 mg/dL
  • Any value less than one is given a value of 1 (i.e. if bilirubin is 0.8 a value of 1.0 is used) to prevent subtraction from any of the three factors, since the natural logarithm of a positive number below 1 (greater than 0 and less than 1) yields a negative value.

The etiology of liver disease was subsequently removed from the model because it posed difficulties such as how to categorize patients with multiple causes of liver disease. Modification of the MELD score by excluding etiology of liver disease did not significantly affect the model's accuracy in predicting three-month survival.

Patients with a diagnosis of liver cancer will be assigned a MELD score based on how advanced the cancer is. [citation needed]

Interpretation edit

In interpreting the MELD Score in hospitalized patients, the 3 month observed mortality (considering 3,437 adult liver transplant candidates with chronic liver disease who were added to the OPTN waiting list at 2A or 2B status between November, 1999, and December, 2001) is:[6]

MELD score Percentage observed mortality
40 or more 71.3%[6]
30–39 52.6%[6]
20–29 19.6%[6]
10–19 6.0%[6]
9 or less 1.9%[6]

Applications of MELD score include:

  • The best outcomes with TIPS occur among patients with a MELD score less than 14.
  • Patients with MELD scores greater than 24 who are reasonable liver transplant candidates are probably best served by foregoing TIPS placement.

History edit

MELD was originally developed at the Mayo Clinic by Dr. Patrick Kamath, and at that point was called the "Mayo End-stage Liver Disease" score. It was derived in a series of patients undergoing TIPS procedures. The original version also included a variable based on the underlying etiology (cause) of the liver disease.[1] The score turned out to be predictive of prognosis in chronic liver disease in general, and—with some modifications—came to be applied as an objective tool in assigning need for a liver transplant. The etiology turned out to be relatively unimportant, and was also regarded as relatively subjective; it was therefore removed from the score.[3]

The successor of MELD, an advanced scoring system, made by collaboration between Massachusetts General Hospital and IBM, called MELD-Plus was introduced in 2017.[7]

Potential of alternative scores to extend life expectancy edit

The United Network for Organ Sharing proposed that MELD-Na score (an extension of MELD) may better rank candidates based on their risk of pre-transplant mortality and is projected to save 50-60 lives total per year.[8] Furthermore, a study published in the New England Journal of Medicine in 2008, estimated that using MELD-Na instead of MELD would save 90 lives for the period from 2005 to 2006.[9] In his viewpoint published in June 2018, co-creator of MELD-Plus, Uri Kartoun, suggested that "...MELD-Plus, if incorporated into hospital systems, could save hundreds of patients every year in the United States alone."[10]

See also edit

References edit

  1. ^ a b Malinchoc, Michael; Kamath, Patrick S; Gordon, Fredric D; Peine, Craig J; Rank, Jeffrey; Ter Borg, Pieter C.J (2000). "A model to predict poor survival in patients undergoing transjugular intrahepatic portosystemic shunts". Hepatology. 31 (4): 864–71. doi:10.1053/he.2000.5852. PMID 10733541.
  2. ^ Kamath, P; Wiesner, R. H; Malinchoc, M; Kremers, W; Therneau, T. M; Kosberg, C. L; d'Amico, G; Dickson, E. R; Kim, W. R (2001). "A model to predict survival in patients with end-stage liver disease". Hepatology. 33 (2): 464–70. doi:10.1053/jhep.2001.22172. PMID 11172350. S2CID 72518575.
  3. ^ a b c d Kamath, Patrick S; Kim, W. Ray (2007). "The model for end-stage liver disease (MELD)". Hepatology. 45 (3): 797–805. doi:10.1002/hep.21563. PMID 17326206.
  4. ^ Jung, G.E; Encke, J; Schmidt, J; Rahmel, A (2008). "Model for end-stage liver disease". Der Chirurg. 79 (2): 157–63. doi:10.1007/s00104-008-1463-4. PMID 18214398. S2CID 25562795.
  5. ^ UNOS (2009-01-28). "MELD/PELD calculator documentation" (PDF). Retrieved 2010-02-21.
  6. ^ a b c d e f Wiesner, Russell; Edwards, Erick; Freeman, Richard; Harper, Ann; Kim, Ray; Kamath, Patrick; Kremers, Walter; Lake, John; Howard, Todd; Merion, Robert M.; Wolfe, Robert A.; Krom, Ruud (2003-01-01). "Model for end-stage liver disease (MELD) and allocation of donor livers". Gastroenterology. 124 (1): 91–96. doi:10.1053/gast.2003.50016. ISSN 0016-5085. PMID 12512033.
  7. ^ Kartoun, Uri; Corey, Kathleen E; Simon, Tracey G; Zheng, Hui; Aggarwal, Rahul; Ng, Kenney; Shaw, Stanley Y (2017). "The MELD-Plus: A generalizable prediction risk score in cirrhosis". PLOS ONE. 12 (10): e0186301. Bibcode:2017PLoSO..1286301K. doi:10.1371/journal.pone.0186301. PMC 5656314. PMID 29069090.
  8. ^ "OPTN/UNOS Liver and Intestinal Organ Transplantation Committee Report to the Board of Directors" (PDF). hrsa.gov. June 2014. Retrieved 26 April 2023.
  9. ^ Kim, WR; Biggins, SW; Kremers, WK; Wiesner, RH; Kamath, PS; Benson, JT; Edwards, E; Therneau, TM (2008). "Hyponatremia and mortality among patients on the liver-transplant waiting list". N Engl J Med. 359 (10): 1018–6. doi:10.1056/NEJMoa0801209. PMC 4374557. PMID 18768945.
  10. ^ Kartoun, Uri (2018). "Toward an accelerated adoption of data-driven findings in medicine". Medicine, Health Care and Philosophy. 22 (1): 153–157. doi:10.1007/s11019-018-9845-y. PMID 29882052. S2CID 46973857.

External links edit

Library resources about
Model for End-Stage Liver Disease
  • Model for End-Stage Liver Disease Calculator from MDCalc

April 12, 2024
model, stage, liver, disease, meld, scoring, system, assessing, severity, chronic, liver, disease, initially, developed, predict, mortality, within, three, months, surgery, patients, undergone, transjugular, intrahepatic, portosystemic, shunt, tips, procedure,. The Model for End Stage Liver Disease or MELD is a scoring system for assessing the severity of chronic liver disease It was initially developed to predict mortality within three months of surgery in patients who had undergone a transjugular intrahepatic portosystemic shunt TIPS procedure 1 and was subsequently found to be useful in determining prognosis and prioritizing for receipt of a liver transplant 2 3 This score is now used by the United Network for Organ Sharing UNOS and Eurotransplant for prioritizing allocation of liver transplants instead of the older Child Pugh score 3 4 Model for End Stage Liver DiseaseSynonymsMELDPurposeAssess the severity of chronic liver diseaseBased onSerum creatinine INR and bilirubin Contents 1 Determination 2 Interpretation 3 History 4 Potential of alternative scores to extend life expectancy 5 See also 6 References 7 External linksDetermination editMELD uses the patient s values for serum bilirubin serum creatinine and the international normalized ratio for prothrombin time INR to predict survival It is calculated according to the following formula 3 MELD def3 78 ln serum bilirubin mg dL 11 2 ln INR 9 57 ln serum creatinine mg dL 6 43 displaystyle mathrm MELD overset mathrm def 3 78 times ln left text serum bilirubin mg dL right 11 2 times ln text INR 9 57 times ln left text serum creatinine mg dL right 6 43 nbsp MELD scores are reported as whole numbers so the result of the equation above is rounded UNOS has made the following modifications to the score 5 If the patient has been dialyzed twice within the last 7 days then the value of serum creatinine should be 4 0 mg dL Any value less than one is given a value of 1 i e if bilirubin is 0 8 a value of 1 0 is used to prevent subtraction from any of the three factors since the natural logarithm of a positive number below 1 greater than 0 and less than 1 yields a negative value The etiology of liver disease was subsequently removed from the model because it posed difficulties such as how to categorize patients with multiple causes of liver disease Modification of the MELD score by excluding etiology of liver disease did not significantly affect the model s accuracy in predicting three month survival Patients with a diagnosis of liver cancer will be assigned a MELD score based on how advanced the cancer is citation needed Interpretation editIn interpreting the MELD Score in hospitalized patients the 3 month observed mortality considering 3 437 adult liver transplant candidates with chronic liver disease who were added to the OPTN waiting list at 2A or 2B status between November 1999 and December 2001 is 6 MELD score Percentage observed mortality40 or more 71 3 6 30 39 52 6 6 20 29 19 6 6 10 19 6 0 6 9 or less 1 9 6 Applications of MELD score include The best outcomes with TIPS occur among patients with a MELD score less than 14 Patients with MELD scores greater than 24 who are reasonable liver transplant candidates are probably best served by foregoing TIPS placement History editMELD was originally developed at the Mayo Clinic by Dr Patrick Kamath and at that point was called the Mayo End stage Liver Disease score It was derived in a series of patients undergoing TIPS procedures The original version also included a variable based on the underlying etiology cause of the liver disease 1 The score turned out to be predictive of prognosis in chronic liver disease in general and with some modifications came to be applied as an objective tool in assigning need for a liver transplant The etiology turned out to be relatively unimportant and was also regarded as relatively subjective it was therefore removed from the score 3 The successor of MELD an advanced scoring system made by collaboration between Massachusetts General Hospital and IBM called MELD Plus was introduced in 2017 7 Potential of alternative scores to extend life expectancy editThe United Network for Organ Sharing proposed that MELD Na score an extension of MELD may better rank candidates based on their risk of pre transplant mortality and is projected to save 50 60 lives total per year 8 Furthermore a study published in the New England Journal of Medicine in 2008 estimated that using MELD Na instead of MELD would save 90 lives for the period from 2005 to 2006 9 In his viewpoint published in June 2018 co creator of MELD Plus Uri Kartoun suggested that MELD Plus if incorporated into hospital systems could save hundreds of patients every year in the United States alone 10 See also editPediatric End Stage Liver Disease Milan criteria Child Pugh score MELD Plus MELD Na MELD 3 0References edit a b Malinchoc Michael Kamath Patrick S Gordon Fredric D Peine Craig J Rank Jeffrey Ter Borg Pieter C J 2000 A model to predict poor survival in patients undergoing transjugular intrahepatic portosystemic shunts Hepatology 31 4 864 71 doi 10 1053 he 2000 5852 PMID 10733541 Kamath P Wiesner R H Malinchoc M Kremers W Therneau T M Kosberg C L d Amico G Dickson E R Kim W R 2001 A model to predict survival in patients with end stage liver disease Hepatology 33 2 464 70 doi 10 1053 jhep 2001 22172 PMID 11172350 S2CID 72518575 a b c d Kamath Patrick S Kim W Ray 2007 The model for end stage liver disease MELD Hepatology 45 3 797 805 doi 10 1002 hep 21563 PMID 17326206 Jung G E Encke J Schmidt J Rahmel A 2008 Model for end stage liver disease Der Chirurg 79 2 157 63 doi 10 1007 s00104 008 1463 4 PMID 18214398 S2CID 25562795 UNOS 2009 01 28 MELD PELD calculator documentation PDF Retrieved 2010 02 21 a b c d e f Wiesner Russell Edwards Erick Freeman Richard Harper Ann Kim Ray Kamath Patrick Kremers Walter Lake John Howard Todd Merion Robert M Wolfe Robert A Krom Ruud 2003 01 01 Model for end stage liver disease MELD and allocation of donor livers Gastroenterology 124 1 91 96 doi 10 1053 gast 2003 50016 ISSN 0016 5085 PMID 12512033 Kartoun Uri Corey Kathleen E Simon Tracey G Zheng Hui Aggarwal Rahul Ng Kenney Shaw Stanley Y 2017 The MELD Plus A generalizable prediction risk score in cirrhosis PLOS ONE 12 10 e0186301 Bibcode 2017PLoSO 1286301K doi 10 1371 journal pone 0186301 PMC 5656314 PMID 29069090 OPTN UNOS Liver and Intestinal Organ Transplantation Committee Report to the Board of Directors PDF hrsa gov June 2014 Retrieved 26 April 2023 Kim WR Biggins SW Kremers WK Wiesner RH Kamath PS Benson JT Edwards E Therneau TM 2008 Hyponatremia and mortality among patients on the liver transplant waiting list N Engl J Med 359 10 1018 6 doi 10 1056 NEJMoa0801209 PMC 4374557 PMID 18768945 Kartoun Uri 2018 Toward an accelerated adoption of data driven findings in medicine Medicine Health Care and Philosophy 22 1 153 157 doi 10 1007 s11019 018 9845 y PMID 29882052 S2CID 46973857 External links editLibrary resources about Model for End Stage Liver Disease Resources in your library Resources in other libraries Model for End Stage Liver Disease Calculator from MDCalc Online calculator for MELD score UNOS modification Retrieved from https en wikipedia org w index php title Model for End Stage Liver Disease amp oldid 1186453591, wikipedia, wiki, book, books, library,

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