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慢性乙型肝炎患者肝脏中前S1、前S2、S和X肽的表达与病毒复制的关系

Expression of pre-S1, pre-S2, S and X peptides in relation to viral replication in livers with chronic hepatitis B.

作者信息

Suzuki K, Uchida T, Shikata T, Moriyama M, Arakawa Y, Mizokami M, Mima F

机构信息

Department of Pathology, Nihon University School of Medicine, Tokyo, Japan.

出版信息

Liver. 1990 Dec;10(6):355-64. doi: 10.1111/j.1600-0676.1990.tb00481.x.

Abstract

The expression of large (pre-S1), middle (pre-S2), major S (S) polypeptides of the envelope (HBs) and X peptides of hepatitis B virus (HBV) was investigated in 37 liver specimens with chronic hepatitis B by indirect immunoperoxidase staining. Primary antisera utilized were polyclonal ones against HBs (poly-HBs), core (HBc) and X and monoclonal ones against pre-S1, pre-S2 and S with (particle-S) or without (peptide-S) conformational structure. The localization of HBs proteins in hepatocytes was classified into three types: diffuse, membranous and inclusion. The peptide-S and pre-S2 were expressed at nearly the same frequency as poly-HBs in all types, whereas particle-S was found less frequently (18/29 cases) in the inclusion type, and pre-S1 was recognized relatively rarely (9/33 cases) in the membranous type. As for staining intensity, peptide-S and pre-S2 were almost identical to poly-HBs which stained the most strongly among all three staining types. Particle-S was similar to poly-HBs in the membranous type, but was weak in the inclusion type in the majority. While pre-S1 was stained in a similar intensity to poly-HBs in the diffuse and inclusion types, it was weak or negative in the membranous type. Thus, envelope particles indicated by particle-S staining appeared to be located most frequently in the membranous type, but their assembly might be suppressed in the inclusion type where pre-S1 was well expressed. The X peptide was more frequently detected in the liver with serum HBe antigen and/or HBV DNA. The X peptide was stained exclusively in the cytoplasm of hepatocytes and was correlated with the cytoplasmic HBc antigen. The X peptide was not observed differently between cases with and those without cirrhosis. This suggests that the expression of X peptide tends to occur with virus replication but not with disease progression.

摘要

通过间接免疫过氧化物酶染色法,对37例慢性乙型肝炎肝脏标本中乙型肝炎病毒(HBV)包膜的大(前S1)、中(前S2)、主S(S)多肽以及X肽的表达情况进行了研究。使用的一抗包括抗HBs(多克隆抗-HBs)、核心(HBc)和X的多克隆抗体,以及抗前S1、前S2和S的单克隆抗体,其中抗S单克隆抗体具有(颗粒-S)或不具有(肽-S)构象结构。HBs蛋白在肝细胞中的定位分为三种类型:弥漫型、膜型和包涵体型。肽-S和前S2在所有类型中的表达频率与多克隆抗-HBs几乎相同,而颗粒-S在包涵体型中出现的频率较低(18/29例),前S1在膜型中相对较少被识别(9/33例)。至于染色强度,肽-S和前S2与多克隆抗-HBs几乎相同,多克隆抗-HBs在所有三种染色类型中染色最强。颗粒-S在膜型中与多克隆抗-HBs相似,但在大多数包涵体型中较弱。虽然前S1在弥漫型和包涵体型中的染色强度与多克隆抗-HBs相似,但在膜型中较弱或为阴性。因此,颗粒-S染色所示的包膜颗粒似乎最常位于膜型中,但在包涵体型中其组装可能受到抑制,而前S1在包涵体型中表达良好。X肽在血清HBe抗原和/或HBV DNA阳性的肝脏中更频繁地被检测到。X肽仅在肝细胞的细胞质中染色,并且与细胞质HBc抗原相关。在有肝硬化和无肝硬化的病例之间未观察到X肽有差异。这表明X肽的表达倾向于与病毒复制相关,而与疾病进展无关。

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