Recurrence of Primary Biliary Cirrhosis after Liver Transplantation

Neuberger, James; Portmann, Bernard; Macdougall, B.R.D.; Calne, R. Y.; Williams, Roger

doi:10.1056/nejm198201073060101

Cited by 243 publications

(106 citation statements)

References 7 publications

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“…We can only state that we were unable to diagnose the disease using the criteria offered by Neuberger et a1. (10). The reasons we were unable to diagnose recurrent disease with certainty included the different histopathologic appearance of PBC and chronic rejection, the lack of correlation of AMA levels with liver dysfunction and/or hepatic pathology and our ignorance of the effect of cyclosporin therapy on the histopathology of PBC.…”

Section: Pathologic Comparison Of Native Hepatectomies With Pbc and Fmentioning

confidence: 98%

“…The difficulty of using pathologic observations for the diagnosis of PBC after transplantation is underscored by the experience at Cambridge (10). Since their original report, the Cambridge group has identified patients who developed a PBC-like syndrome (clinically and pathologically) after transplantation but did not have the disease originally, nor did they convert to AMA positivity (24).…”

Section: Pathologic Comparison Of Native Hepatectomies With Pbc and Fmentioning

confidence: 99%

“…In addition, because our patients have been maintained on cyclosporin whereas those reported by the Cambridge group having recurrent disease received azathioprine and not cyclosporin, it may be impossible to reconcile the pathologic findings ofthe two groups. Finally, no number of negative cases can prove that PBC or any other disorder cannot recur; only one classic case needs to be documented to prove otherwise (10). Differences in the postoperative course of patients transplanted for PBC have been seen compared to those transplanted for other disorders.…”

Section: Pathologic Comparison Of Native Hepatectomies With Pbc and Fmentioning

confidence: 99%

“…Neuberger et a1. (10) have suggested that recurrent PBC occurs in patients transplanted for this indication. This conclusion was based on the findings of a consistent hepatic histopathology, the presence of AMA and a posttransplant clinical course consistent with PBC.…”

mentioning

confidence: 99%

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Pathologic analysis of liver transplantation for primary biliary cirrhosis

et al. 1988

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A retrospective histopathologic review of all pathologic specimens from 394 adult liver transplant patients was undertaken with clinical correlation to determine if primary biliary cirrhosis has affected the posttrans‐plant course compared to all other indications for liver transplantation and if recurrent primary biliary cirrhosis has occurred after liver transplantation. We also compared the histopathologic features seen in native livers with primary biliary cirrhosis to failed allografts with chronic rejection. One hundred six of the 394 adult patients transplanted during this time (1981 to July, 1986) fulfilled clinicopathologic criteria for a diagnosis of primary biliary cirrhosis. Neither the incidence nor any qualitative pathologic feature of histologically documented acute cellular rejection differentiated subjects transplanted for primary biliary cirrhosis vs. other diseases. No correlation between the titers of antimitochon‐drial antibody and the presence of posttransplant hepatic dysfunction based on liver enzyme profiles or the development of chronic rejection was seen in patients transplanted for primary biliary cirrhosis. Minor differences noted in the posttransplant course of primary biliary cirrhosis patients as compared to other conditions (higher incidence of chronic rejection as a cause of graft failure) was seen, but this did not significantly affect graft or patient survival. Recurrent primary biliary cirrhosis could not be diagnosed with certainty in any patient. A comparison of failed chronically rejected allografts vs. native hepatectomies obtained from patients with primary biliary cirrhosis revealed the presence of chronic obliterative vasculopathy, centrilobular cholestasis, and lack of granulomas, cirrhosis, cholan‐giolar proliferation, copper‐associated protein deposition and Mallory's hyalin in specimens with chronic rejection. In contrast, livers removed from patients with primary biliary cirrhosis demonstrated a mild vasculopathy, cirrhosis, granulomas, copper‐associated protein deposition, Mallory's hyalin and periportal cholestasis. Both conditions demonstrated a nonsuppurative destructive cholangitis with bile duct paucity.

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Section: Pathologic Comparison Of Native Hepatectomies With Pbc and Fmentioning

confidence: 98%

Section: Pathologic Comparison Of Native Hepatectomies With Pbc and Fmentioning

confidence: 99%

Section: Pathologic Comparison Of Native Hepatectomies With Pbc and Fmentioning

confidence: 99%

mentioning

confidence: 99%

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Pathologic analysis of liver transplantation for primary biliary cirrhosis

et al. 1988

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“…The initial report of recurrence of PBC in three patients by Neuberger et al 15 was not confirmed in the Pittsburgh experience. 16 Recurrence of the disease, using the criteria described by Neuberger et al, 15 was not found by Demetris et al 17 in a recent pathologic review of graft specimens obtained from 106 patients with PBC.…”

Section: The Issue Of Recurrence Of the Disease After Transplantationmentioning

confidence: 89%