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原发性胆汁性肝硬化患者肝脏中多种T细胞克隆型的积累。

Accumulation of multiple T-cell clonotypes in the liver of primary biliary cirrhosis.

作者信息

Ohmoto M, Yamamoto K, Nagano T, Matsumoto S, Kobashi H, Okamoto R, Tsuji T

机构信息

First Department of Internal Medicine, Okayama University Medical School, Japan.

出版信息

Hepatology. 1997 Jan;25(1):33-7. doi: 10.1053/jhep.1997.v25.pm0008985261.

Abstract

The histological hallmark of primary biliary cirrhosis (PBC) is the destruction of the interlobular and septal bile ducts accompanied by a dense accumulation of lymphocytes; this constellation of features is termed chronic nonsuppurative destructive cholangitis. To analyze the T cells responsible for bile duct destruction, the T-cell receptor (TCR) Vbeta repertoire was studied in liver biopsy specimens, and also in peripheral blood lymphocytes (PBL) obtained from seven patients with PBC in the early stage (Scheuer's stage I or II). The complementary DNA (cDNA) of each TCR Vbeta1-20 chain was amplified by reverse-transcription polymerase chain reaction (RT-PCR), and the PCR products were examined by single-strand conformation polymorphism (SSCP) analysis. On the RT-PCR/SSCP analysis, a leukemic cell line, HPB-ALL, showed bands in TCR Vbeta 5.2 and Vbeta 6, indicating clonal expansion with distinct TCR. In the PBL from healthy subjects, the PCR products were amplified from many TCR Vbeta and were shown as smears on SSCP, suggesting that PBL consist of diverse T-cell clones. In PBC, many TCR Vbeta products were amplified by RT-PCR in both liver tissues and PBL, and no biased expression of a particular Vbeta was observed. SSCP analysis revealed multiple bands in most Vbeta chains, suggesting the presence of selected but multiple T-cell clones. Both the number and types of Vbeta showing clonal expansion were heterogeneous in the PBC patients. A comparative RT-PCR SSCP analysis of each TCR Vbeta between tissue lymphocytes and PBL revealed the presence of some identical T-cell clones in both the PBC liver and the PBL. These results suggest that T cells infiltrating the liver in PBC consist of multiple clonotypes and that T-cell clones accumulated in the liver are also present in PBL.

摘要

原发性胆汁性肝硬化(PBC)的组织学特征是小叶间胆管和间隔胆管遭到破坏,并伴有淋巴细胞的密集聚集;这一系列特征被称为慢性非化脓性破坏性胆管炎。为了分析导致胆管破坏的T细胞,对肝活检标本以及从7例早期(谢弗I期或II期)PBC患者获取的外周血淋巴细胞(PBL)中的T细胞受体(TCR)Vβ谱进行了研究。通过逆转录聚合酶链反应(RT-PCR)扩增每个TCR Vβ1-20链的互补DNA(cDNA),并通过单链构象多态性(SSCP)分析检测PCR产物。在RT-PCR/SSCP分析中,白血病细胞系HPB-ALL在TCR Vβ5.2和Vβ6显示出条带,表明具有独特TCR的克隆性扩增。在健康受试者的PBL中,PCR产物从许多TCR Vβ中扩增出来,并在SSCP上显示为涂片,表明PBL由多种T细胞克隆组成。在PBC中,肝组织和PBL中的许多TCR Vβ产物都通过RT-PCR扩增,未观察到特定Vβ的偏向性表达。SSCP分析在大多数Vβ链中显示出多条带,表明存在经过选择但多种的T细胞克隆。在PBC患者中,显示克隆性扩增的Vβ的数量和类型是异质性的。对组织淋巴细胞和PBL之间的每个TCR Vβ进行比较RT-PCR SSCP分析,发现在PBC肝脏和PBL中都存在一些相同的T细胞克隆。这些结果表明,浸润PBC肝脏的T细胞由多种克隆型组成,并且在肝脏中积累的T细胞克隆也存在于PBL中。

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