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外周B细胞的选择与稳态。

Peripheral B cell selection and homeostasis.

作者信息

Cancro Michael P, Smith Susan Harless

机构信息

University of Pennsylvania School of Medicine, Philadelphia, PA 19104-6082, USA.

出版信息

Immunol Res. 2003;27(2-3):141-8. doi: 10.1385/IR:27:2-3:141.

Abstract

The size and makeup of mature B cell compartments are controlled by the proportion of immature B cells that complete differentiation, coupled with the average lifespan of mature B cells. Thus, determining the selective and homeostatic factors controlling these parameters is key to understanding how the B cell repertoire is established and maintained. Our previous work defined the developmental stages spanning immature B cell formation in the marrow and final maturation in the periphery. More recently, we have focused on the molecular basis for survival and differentiation within these developmental subsets, with emphasis on the role of BLyS and BLyS receptors. Through developmental and kinetic studies in normal and mutant mice, we have found that BLyS controls peripheral B cell numbers in two ways: by varying the proportion of cells that complete transitional B cell development and by serving as the primary determinant of mature follicular B cell lifespan. Ongoing studies are aimed at determining the mechanism of BLyS activity in these subsets, as well as how BLyS responsiveness is integrated with BcR signaling. Additionally, we have begun studies on how these selective and homeostatic processes change with age. Our results indicate that the size and dynamics of most B cell subsets shift with age, suggesting age-associated alterations in both intrinsic and microenvironmental factors that govern these processes.

摘要

成熟B细胞区室的大小和组成由完成分化的未成熟B细胞比例以及成熟B细胞的平均寿命控制。因此,确定控制这些参数的选择性和稳态因素是理解B细胞库如何建立和维持的关键。我们之前的工作定义了从骨髓中未成熟B细胞形成到外周最终成熟的发育阶段。最近,我们专注于这些发育亚群内存活和分化的分子基础,重点是BLyS和BLyS受体的作用。通过对正常和突变小鼠的发育和动力学研究,我们发现BLyS通过两种方式控制外周B细胞数量:通过改变完成过渡性B细胞发育的细胞比例以及作为成熟滤泡B细胞寿命的主要决定因素。正在进行的研究旨在确定BLyS在这些亚群中的活性机制,以及BLyS反应性如何与BcR信号整合。此外,我们已经开始研究这些选择性和稳态过程如何随年龄变化。我们的结果表明,大多数B细胞亚群的大小和动态随年龄而变化,这表明在控制这些过程的内在和微环境因素中存在与年龄相关的改变。

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