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人淋巴结和脾脏中的边缘区B细胞表现出体细胞超突变并呈现克隆性扩增。

Marginal-zone B cells in the human lymph node and spleen show somatic hypermutations and display clonal expansion.

作者信息

Tierens A, Delabie J, Michiels L, Vandenberghe P, De Wolf-Peeters C

机构信息

Departments of Pathology and Hematology, University Hospitals of Leuven, Leuven, Belgium.

出版信息

Blood. 1999 Jan 1;93(1):226-34.

PMID:9864165
Abstract

Splenic marginal-zone B cells, marginal-zone B cells of Peyer's patches in the gut, and nodal marginal-zone B cells (also identified as monocytoid B cells) share a similar morphology and immunophenotype. These cells likely represent a distinct subset of B cells in humans and rodents, but their precise ontogenetic relationship as well as their origin from B cells of the germinal center is still debated. To study this, we performed a mutation analysis of the rearranged immunoglobulin variable genes (VH) of microdissected single nodal and splenic marginal-zone cells. In addition, we investigated the presence of proliferating cells and B-cell clones in the human splenic and nodal marginal zone as well as adjacent germinal centers. This was performed by immunohistochemical staining for the Ki-67 antigen and denaturing gradient gel analysis of amplified immunoglobulin heavy chain genes' complementarity determining region 3 of microdissected cell clusters. A variable subset of nodal and splenic marginal-zone B cells showed somatic mutations in their rearranged VH genes, indicating that both virgin and memory B cells are present in the nodal and splenic marginal zone. Nodal and splenic marginal-zone B cells preferentially rearranged VH3 family genes such as DP47, DP49, DP54, and DP58. A preferential rearrangement of the same VH genes has been shown by others in the peripheral CD5(-) IgM+ B cells. These data suggest that the splenic and nodal marginal-zone B cells are closely related B-cell subsets. We also showed that marginal-zone B cells may cycle and that clones of B cells are frequently detected in the nodal as well as the splenic marginal zone. These clones are not related to those present in adjacent germinal centers. These data favor the hypothesis that clonal expansion occurs in the marginal zone. Whether the somatic hypermutation mechanism is activated during the clonal expansion in the marginal zone and which type of immune response triggers the clonal expansion need to be elucidated.

摘要

脾脏边缘区B细胞、肠道派尔集合淋巴结的边缘区B细胞以及淋巴结边缘区B细胞(也被鉴定为单核样B细胞)具有相似的形态和免疫表型。这些细胞可能代表人类和啮齿动物中一个独特的B细胞亚群,但其确切的个体发生关系以及它们源自生发中心B细胞的情况仍存在争议。为了研究这一点,我们对显微切割的单个淋巴结和脾脏边缘区细胞的重排免疫球蛋白可变基因(VH)进行了突变分析。此外,我们研究了人脾脏和淋巴结边缘区以及相邻生发中心中增殖细胞和B细胞克隆的存在情况。这是通过对Ki-67抗原进行免疫组织化学染色以及对显微切割的细胞簇的扩增免疫球蛋白重链基因互补决定区3进行变性梯度凝胶分析来完成的。可变比例的淋巴结和脾脏边缘区B细胞在其重排的VH基因中显示出体细胞突变,表明在淋巴结和脾脏边缘区既有未成熟B细胞也有记忆B细胞。淋巴结和脾脏边缘区B细胞优先重排VH3家族基因,如DP47、DP49、DP54和DP58。其他人在周围CD5(-) IgM+ B细胞中也发现了相同VH基因的优先重排。这些数据表明脾脏和淋巴结边缘区B细胞是密切相关的B细胞亚群。我们还表明边缘区B细胞可能会循环,并且在淋巴结以及脾脏边缘区经常检测到B细胞克隆。这些克隆与相邻生发中心中的克隆无关。这些数据支持边缘区发生克隆扩增的假说。边缘区克隆扩增过程中体细胞超突变机制是否被激活以及哪种免疫反应类型触发克隆扩增还有待阐明。

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