Delayed onset of severe hepatitis C-related liver damage following liver transplantation: A matter of concern?

Berenguer, Marina; Aguilera, Victoria; Prieto, M.; Carrasco, Domingo; Rayón, Miguel; Juan, Fernando San; Landaverde, Carmen; Mir, José; Berenguer, J

doi:10.1053/jlts.2003.50240

Cited by 46 publications

(49 citation statements)

References 17 publications

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“…There were 25 pressure evaluations (18 patients) that fulfilled our definition of potentially discrepant results with respect to the expected fibrosis stage or HVPG. The median biopsy length of the entire "discrepant" group was 22 mm (range, [13][14][15][16][17][18][19][20][21][22][23][24][25][26][27][28][29][30] and the number of fragments was 3.5 (range, 2-8) similar to the population as a whole. In the discrepant group, 56% of biopsies did not show severe nodularity/cirrhosis with 4 (range, 1-9) complete portal tracts and 8 (range, 2-13) partial portal tracts.…”

Section: Total Cohortmentioning

confidence: 85%

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Hepatic venous pressure gradient to assess fibrosis and its progression after liver transplantation for HCV cirrhosis

et al. 2007

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Progression of fibrosis following recurrent hepatitis C virus (HCV) infection is frequent after liver transplantation (LT).Histology remains the gold standard to assess fibrosis, but the value of hepatic venous pressure gradient (HVPG) is being explored. We evaluated patients with recurrent HCV infection after LT to assess whether HVPG correlates with liver histology, particularly fibrosis. A total of 90 consecutive patients underwent 170 HVPG measurements concomitant with transjugular liver biopsy (TJB), with 31.5 (range, 6-156) months of follow up. Median biopsy length was 22 mm and total portal tract count was 12 (complete 6, partial 6). Median HVPG was 4 mmHg: 38% of patients Ն6 mmHg (portal hypertension, PHT), 13% Ն10 mmHg. HVPG correlated with Ishak stage (r ϭ 0.73, P Ͻ 0.001) for mild (0-3) and severe fibrosis (4-6), and grade score (r ϭ 0.47, P Ͻ 0.001), but neither correlated with interval from LT nor biopsy length. HVPG was Ն10 mmHg in 15 patients: 12 had stage 5 or 6, and 3 severe portal expansion. HVPG was repeated in 49, between 7 and 60 months with weak correlation to fibrosis score (r ϭ 0.30, P ϭ 0.045). A total of 12 patients with HVPG Ն6 mmHg had fibrosis score Յ3, while 8 patients had normal HVPG but fibrosis stage Ն4. These discrepancies were mostly associated with specific histological features such as perisinusoidal fibrosis rather than errors in measuring HVPG. In 29 with HVPG Ͻ6 mmHg at 1 yr, none decompensated compared to 4 of 13 (31%) with PHT. In conclusion, HVPG correlates with fibrosis and its progression, due to recurrent HCV infection, assessed in TJB. Liver Transpl 13:1305Transpl 13: -1311Transpl 13: , 2007 The severity of portal hypertension (PHT) correlates with the severity of liver disease and cirrhosis, both functionally and histologically 1 and also with the Model for End-Stage Liver Disease, 2 such that it has independent prognostic value separate from clinical and laboratory assessment. 2,3 Hepatic vein catheterisation 4 was modified by Groszmann et al. 5 using a balloon catheter. The measurement of hepatic venous pressure gradient (HVPG) (the difference between wedge hepatic venous pressure [WHVP] Ϫ free hepatic venous pressure) is reproducible 6 and is the preferred technique for evaluating PHT, correlating 1:1 with the direct measurement of portal vein pressure in patients with sinusoidal and postsinusoidal causes of cirrhosis, 7,8 particularly alcoholic and viral-related cirrhosis. Normally HVPG ranges from 1 to 5 mmHg; pressures Ն6 mmHg indicate PHT. 6 WHVP increases with progression of chronic hepatitis and PHT, before histologically detectable cirrhosis. 9 A gradient Ͼ5 mmHg was always associated with significant changes in liver biopsy in 1 study, although a normal gradient did not completely rule out cirrhosis, 10 suggesting that WHVP could provide supplementary information to liver biopsy, with a higher predictive value for assessing stage and activity of chronic liver disease, than routine biochemical tests. 10 Other studies have correlated HVPG both with severit...

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Section: Total Cohortmentioning

confidence: 85%

“…17 Fibrosis associated with recurrent HCV infection after liver transplantation (LT). [18][19][20] progresses faster to cirrhosis and decompensation compared to the pretransplantation HCV setting. 21 Transjugular liver biopsy (TJB) 22 enables multiple cores of tissue to be obtained 23 and is easily combined with hemodynamic evaluations.…”

mentioning

confidence: 99%

Hepatic venous pressure gradient to assess fibrosis and its progression after liver transplantation for HCV cirrhosis

et al. 2007

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“…Considerations such as potential morbidity and mortality, cost, inconvenience, use of resources, and potential impact of unexplained histopathological findings should be weighed against potential individual and/or societal benefits. 4,[19][20][21][22][23][24] These include (1) early detection of clinically inapparent disease, 19,24 (2) recognition of nonalcoholic steatohepatitis as a significant cause of cryptogenic cirrhosis in the United States 25 but not in England, 26 (3) identification of recipients that might be successfully weaned from immunosuppression, 27 (4) recognition of late-onset rapid hepatitis C virus (HCV) progression, 21 and (5) impact of alcohol use. 20 Approximately 75% of biopsies from long-surviving recipients with abnormal liver tests or symptoms show significant histopathological abnormalities.…”

Section: Immunological Considerationsmentioning

confidence: 99%

“…20 Approximately 75% of biopsies from long-surviving recipients with abnormal liver tests or symptoms show significant histopathological abnormalities. 4,[19][20][21][22][23] These abnormalities are usually attributable to recurrent disease or biliary tract strictures, some of which occur as a late complication of preservation injury. 4,[19][20][21][22][23] The incidence and significance of histopathological abnormalities in long-surviving recipients without abnormal liver tests or symptoms is dependent on the original disease: up to 25% show significant abnormalities when obtained from recipients with original diseases that commonly recur (e.g., HCV, PBC, AIH).…”

Section: Immunological Considerationsmentioning

confidence: 99%

“…4,[19][20][21][22][23] These abnormalities are usually attributable to recurrent disease or biliary tract strictures, some of which occur as a late complication of preservation injury. 4,[19][20][21][22][23] The incidence and significance of histopathological abnormalities in long-surviving recipients without abnormal liver tests or symptoms is dependent on the original disease: up to 25% show significant abnormalities when obtained from recipients with original diseases that commonly recur (e.g., HCV, PBC, AIH). 4,[19][20][21][22][23] Even in the absence of recurrent disease, minor histopathological abnormalities appear in approximately two thirds of biopsies obtained from long-surviving asymptomatic recipients with normal liver tests.…”

Section: Immunological Considerationsmentioning

confidence: 99%

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Liver biopsy interpretation for causes of late liver allograft dysfunction

2006

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Evaluation of needle biopsies and extensive clinicopathological correlation play an important role in the determination of liver allograft dysfunction occurring more than 1 year after transplantation. Interpretation of these biopsies can be quite difficult because of the high incidence of recurrent diseases that show histopathological, clinical, and serological features that overlap with each other and with rejection. Also, more than one insult can contribute to allograft injury. In an attempt to enable centers to compare and pool results, improve therapy, and better understand pathophysiological disease mechanisms, the Banff Working Group on Liver Allograft Pathology herein proposes a set of consensus criteria for the most common and problematic causes of late liver allograft dysfunction, including late-onset acute and chronic rejection, recurrent and new-onset viral and autoimmune hepatitis, biliary strictures, and recurrent primary biliary cirrhosis and primary sclerosing cholangitis. A discussion of differential diagnosis is also presented. (HEPATOLOGY 2006;44:489-501.)

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