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正常肝脏、慢性活动性肝炎、肝硬化及肝细胞癌中的凝集素结合模式。一项免疫组织化学和免疫电子显微镜研究。

Lectin binding patterns in normal liver, chronic active hepatitis, liver cirrhosis, and hepatocellular carcinoma. An immunohistochemical and immunoelectron microscopic study.

作者信息

Murakami I, Sarker A B, Hayashi K, Akagi T

机构信息

Second Department of Pathology, Okayama University Medical School.

出版信息

Acta Pathol Jpn. 1992 Aug;42(8):566-72. doi: 10.1111/j.1440-1827.1992.tb03106.x.

DOI:10.1111/j.1440-1827.1992.tb03106.x
PMID:1333146
Abstract

We studied the binding patterns of 14 lectins in human normal and cirrhotic liver (LC) tissues and hepatocellular carcinomas (HCC) using the ABC method. Lectins were divided into 4 groups according to their binding patterns in normal tissues: (A) PHA, MPA, LcH, RCA-I, and WGA, which bound to hepatocytes and all three types of sinusoidal cells; (B) BPA, GS-I, PNA, and SBA, which bound to Kupffer cells and endothelia of interlobular arteries and veins and bile duct epithelia in the portal tract, but not to hepatocytes; (C) UEA-I, which bound only to endothelia of interlobular arteries and veins and bile duct epithelia in the portal tract; (D) LBA, Lotus, LPA, and SJA, which showed no binding. Thus group B lectins may be useful markers of Kupffer cells. Only electron microscopic examination revealed the precise binding sites of lectins in sinusoidal cells and hepatocytes. Hepatocyte cell surface polarities demonstrated by lectin binding in LC and HCC were different from those in the normal liver. The binding pattern of PHA to LC hepatocytes changed from a membranous to both a membranous and a cytoplasmic pattern, and that of LcH to HCC cells changed to dot-like staining in the cytoplasm. These changes of polarities in LC and HCC might be caused by changes in the distribution of lectin-binding carbohydrates or by the altered glycosylation of glycoconjugates.

摘要

我们采用ABC法研究了14种凝集素在人正常肝脏、肝硬化组织及肝细胞癌组织中的结合模式。根据凝集素在正常组织中的结合模式,将其分为4组:(A)PHA、MPA、LcH、RCA-I和WGA,它们与肝细胞及所有三种类型的窦状隙细胞结合;(B)BPA、GS-I、PNA和SBA,它们与库普弗细胞、小叶间动静脉内皮及门管区胆管上皮结合,但不与肝细胞结合;(C)UEA-I,仅与小叶间动静脉内皮及门管区胆管上皮结合;(D)LBA、Lotus、LPA和SJA,无结合现象。因此,B组凝集素可能是库普弗细胞的有用标志物。只有电子显微镜检查揭示了凝集素在窦状隙细胞和肝细胞中的精确结合位点。凝集素结合显示的肝硬化及肝细胞癌中肝细胞表面极性与正常肝脏不同。PHA与肝硬化肝细胞的结合模式从膜性变为膜性和胞质内均有,LcH与肝癌细胞的结合模式变为胞质内点状染色。肝硬化及肝细胞癌中这些极性变化可能是由于凝集素结合碳水化合物分布改变或糖缀合物糖基化改变所致。

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