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CA19-9 does not predict cholangiocarcinoma in patients with primary sclerosing cholangitis undergoing liver transplantation
Fisher A; Theise ND; Min A; Mor E; Emre S; Pearl A; Schwartz ME; Miller CM; Sheiner PA
The results of liver transplantation in patients with cholangiocarcinoma have been poor. It has been suggested that elevated serum CA19-9 levels predict cholangiocarcinoma in patients with primary sclerosing cholangitis. We analyzed the predictive value of CA19-9 antigen as a marker of cholangiocarcinoma in patients with primary sclerosing cholangitis evaluated for liver transplantation. We reviewed the charts of 26 patients with primary sclerosing cholangitis (stage IV) in whom preoperative serum CA19-9 levels were determined; 22 of 26 underwent liver transplant. Explant specimens were serially sectioned and examined for tumor. In 3 of the 26 patients, cholangiocarcinoma was diagnosed during pretransplantation evaluation; exploratory laparotomy on the last patient showed no evidence of cholangiocarcinoma, and this patient is awaiting transplantation. Twelve of the 26 patients had CA19-9 levels more than double the laboratory reference range (0-37 U/mL) (mean 183.1 +/- 103 U/mL, range 77-415 U/mL). Two of the 12 patients with elevated CA19-9 levels had cholangiocarcinoma. Of the 14 patients with normal levels, two had cholangiocarcinoma. No correlation between elevated CA19-9 and bile duct dysplasia was noted. Sensitivity for serum CA19-9 levels more than twice the reference range is 50%, specificity is 54.5%, positive predictive value is 16.6%. An elevated serum CA19-9 level in a patient with stage IV primary sclerosing cholangitis does not reliably predict coexisting cholangiocarcinoma. Persistently high or rising serum CA19-9 levels do not indicate more urgent need for liver transplantation
PMID: 9346547
ISSN: 1074-3022
CID: 35152
Detection of hepatitis B and hepatitis C viral sequences in fulminant hepatic failure of unknown etiology
Hytiroglou P; Dash S; Haruna Y; Fernandez M; Theise ND; Schwartz M; Miller C; Bodenheimer HC Jr; Thung SN; Gerber MA
In a significant number of patients, the etiology of fulminant hepatic failure (FHF) is unknown. To determine whether hepatitis B virus (HBV) and hepatitis C virus (HCV) play a role in patients without serologic markers of HBV and HCV infection, the authors examined tissue samples from 15 liver explants with massive hepatic necrosis for the presence of viral sequences by the polymerase chain reaction (PCR). The specimens were derived from nine patients with FHF of unknown etiology; two with serum hepatitis B surface antigen (HBsAg); two with antibodies to HCV; one with antibodies to hepatitis A virus (HAV) and anti-HBc of the IgM class; and one with isoniazid toxicity. Nucleic acids were extracted from frozen liver samples. RNA was used as a template for reverse transcription, followed by double PCR with nested primers for the 5'-untranslated region of HCV. DNA was tested by single PCR for S gene sequences of HBV. Hepatitis B virus sequences were detected in the specimens of the two HBsAg positive patients, the anti-HAV/anti-HBc positive patient, and three of nine patients with FHF of unknown etiology. Hepatitis C virus sequences were present in the explant of one patient with FHF of unknown etiology, but not in the two patients with antibodies to HCV. In two specimens with molecular findings of HBV infection (1 from a patient with serum HBsAg and 1 without), there was immunohistochemical evidence of coinfection or superinfection with hepatitis delta virus (HDV). In conclusion, in this patient population, HBV, alone or with HDV or HAV, causes fulminant hepatic failure more often than HCV infection. However, in the majority of patients, the etiology of fulminant hepatic failure remains unknown
PMID: 7572821
ISSN: 0002-9173
CID: 35157
MRI RELIABLY DETECTS MACROREGENERATIVE NODULES AND SMALL HEPATOCELLULAR-CARCINOMA IN CIRRHOTIC LIVERS [Meeting Abstract]
THEISE, ND; KRINSKY, G; MIZRACHI, HH; ROFSKY, N; GOLDENBERG, A; TOBIAS, H; DIFLO, T; WEINREB, J; TEPERMAN, L
ISI:A1995RX69000316
ISSN: 0270-9139
CID: 86726
LIVER-CELL DYSPLASIA OF LARGE-CELL TYPE MAY OFTEN REPRESENT A REACTIVE CHANGE DUE TO CYTOPLASMIC CHOLESTASIS [Meeting Abstract]
NATARAJAN, S; THEISE, ND; THUNG, SN; PARONETTO, F; HYTIROGLOU, P
ISI:A1995RX69001421
ISSN: 0270-9139
CID: 86727
PERISINUSOIDAL CELL ACTIVATION, NEOANGIOGENESIS, AND SINUSOIDAL CAPILLARIZATION IN MACROREGENERATIVE NODULES - EVIDENCE FOR NEOPLASTIC PROGRESSION [Meeting Abstract]
PARK, YN; YANG, CP; THUNG, SN; THEISE, ND
ISI:A1995RX69000313
ISSN: 0270-9139
CID: 98407
OV-6 POSITIVE, HEPPAR1 NEGATIVE OVAL-LIKE CELLS IN HUMAN LIVERS WITH HEPATITIS-C CIRRHOSIS OR WITH ACETAMINOPHEN TOXICITY [Meeting Abstract]
PARK, YN; BRODY, RI; NALESNIK, M; THUNG, SN; THEISE, ND
ISI:A1995RX69000494
ISSN: 0270-9139
CID: 98408
IMMUNOHISTOCHEMICAL LOCALIZATION OF CATHEPSIN-D IN REGENERATIVE AND NEOPLASTIC LIVER-LESIONS [Meeting Abstract]
STOKES, MB; HYTIROGLOU, P; THUNG, SN; THEISE, ND
ISI:A1995RX69001550
ISSN: 0270-9139
CID: 98409
Carcinoma of the breast in postmenopausal hormone user and nonuser control groups
Squitieri R; Tartter PI; Ahmed S; Brower ST; Theise ND
The risk and prognosis of patients with carcinoma of the breast exposed to postmenopausal hormones are controversial. Carcinoma of the breast from 35 postmenopausal women who had taken hormones were compared with carcinomas from age and histologic matched postmenopausal women who had never taken hormones. Hormone users averaged 1.1 fewer pregnancies (p < 0.005) and 1.4 fewer live births (p < 0.0005). In addition, the carcinomas had significantly lower S-phase fractions (5.36 versus 6.77, p > 0.01) and less nodal involvement (1.2 versus 1.9, p < 0.0005). Estrogen and progesterone receptor content, ploidy and deoxyribonucleic acid index were comparable in both groups. These results indicate that hormone users present with slower growing tumors of earlier stage than nonusers, possibly resulting in improved prognosis
PMID: 8173728
ISSN: 1072-7515
CID: 35158
Hepatitis C in liver allografts
Thung, S N; Shim, K S; Shieh, Y S; Schwartz, M; Theise, N; Borcich, A; Katz, E; Miller, C; Gerber, M A
Recurrent or intercurrent hepatitis C represents significant problems in patients with liver transplants and must be differentiated from hepatic allograft rejection and other conditions affecting allografts. Often, the currently available anti-hepatitis C virus (HCV) tests are not helpful in the differential diagnosis, because preexisting anti-HCV may persist after transplantation or its development may be delayed. We determined the presence of HCV RNA by the reverse double polymerase chain reaction in biopsy specimens of liver allografts from nine patients with acute or chronic hepatitis of uncertain origin and from three patients with cellular allograft rejection. The NS3 region sequences of HCV were detected in seven of nine liver allograft biopsy specimens 6 weeks to 20 months after transplantation. Hepatitis C virus RNA was not detected in two patients. One of these patients was anti-HCV positive, showing mild acute hepatitis 5 weeks after transplantation. Anti-HCV was present in three patients with detectable HCV RNA in the liver but was absent from four other patients with HCV RNA. These findings suggest that HCV is a major cause of acute and chronic hepatitis following liver transplantation, that detection of HCV RNA by polymerase chain reaction in the liver biopsy specimen represents a reliable method for the diagnosis of hepatitis C in liver allografts, and that in some patients HCV may be acquired during transplantation while in others it may represent a recurrent infection.
PMID: 8381267
ISSN: 0003-9985
CID: 3015122
FK506 versus cyclosporine as primary immunosuppressive agent for orthotopic liver allograft recipients. Histologic and immunopathologic observations
Hytiroglou P; Lee R; Sharma K; Theise ND; Schwartz M; Miller C; Thung SN
We investigated possible explanations for the common occurrence of perivenular lesions in liver allografts of patients on FK506 within a few weeks to several months after OLT. Hematoxylin and eosin-stained sections of pre- and postperfusion biopsy specimens and day 7 post-transplant protocol biopsy specimens from 31 patients, randomly assigned to either FK506 or CsA as primary immunosuppressive agent, were reviewed, and immunohistochemical stains for HLA-DR antigen and S-100 protein were performed by the avidin-biotin peroxidase complex method. The histologic features of cellular rejection in the portal tracts of day 7 posttransplant allograft biopsy specimens from patients on FK506 were milder than those from patients on CsA. Immunohistochemical stains for HLA-DR showed intense positivity in a variety of cell types in day 7 posttransplant specimens from both groups, including sinusoidal-lining cells, bile duct epithelial cells, vascular endothelial cells, inflammatory cells, and occasional injured hepatocytes. Although diffuse lobular staining was seen in the majority of cases in both groups, either with or without rejection, liver biopsy specimens from patients on FK506 showed concentration of positively stained cells in perivenular regions more often, and at a lower overall histologic grade of rejection, than specimens from patients on CsA. There were no differences in the number and distribution of S-100 protein-positive dendritic APC between biopsy specimens from FK506 versus CsA-treated patients, or between specimens with and without cellular rejection in either group. It is suggested that the development of perivenular injury, which is seen frequently in allograft biopsy specimens from patients on FK506 obtained at various intervals after transplantation, may be related to drug toxicity rather than to the process of allograft rejection
PMID: 7506452
ISSN: 0041-1337
CID: 35159