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人类和小鼠早期 B 细胞发育:如此相似,但又如此不同。

Human and mouse early B cell development: So similar but so different.

机构信息

Division of Clinical and Experimental Immunology, Institute of Immunology, Center for Pathophysiology, Infectiology and Immunology, Medical University of Vienna, 1090, Vienna, Austria.

Department of Rheumatology and Clinical Immunology, Freiburg University Medical Center, University of Freiburg, 79106, Freiburg, Germany.

出版信息

Immunol Lett. 2023 Sep;261:1-12. doi: 10.1016/j.imlet.2023.07.004. Epub 2023 Jul 11.

Abstract

Early B cell development in the bone marrow ensures the replenishment of the peripheral B cell pool. Immature B cells continuously develop from hematopoietic stem cells, in a process guided by an intricate network of transcription factors as well as chemokine and cytokine signals. Humans and mice possess somewhat similar regulatory mechanisms of B lymphopoiesis. The continuous discovery of monogenetic defects that impact early B cell development in humans substantiates the similarities and differences with B cell development in mice. These differences become relevant when targeted therapeutic approaches are used in patients; therefore, predicting potential immunological adverse events is crucial. In this review, we have provided a phenotypical classification of human and murine early progenitors and B cell stages, based on surface and intracellular protein expression. Further, we have critically compared the role of key transcription factors (Ikaros, E2A, EBF1, PAX5, and Aiolos) and chemo- or cytokine signals (FLT3, c-kit, IL-7R, and CXCR4) during homeostatic and aberrant B lymphopoiesis in both humans and mice.

摘要

骨髓中的早期 B 细胞发育确保了外周 B 细胞池的补充。未成熟的 B 细胞由造血干细胞不断发育而来,这一过程受到转录因子以及趋化因子和细胞因子信号的复杂网络的指导。人类和小鼠具有相似的 B 淋巴细胞发生的调节机制。在人类中不断发现影响早期 B 细胞发育的单基因缺陷,证实了人类和小鼠的 B 细胞发育之间的相似性和差异。当在患者中使用靶向治疗方法时,这些差异变得相关;因此,预测潜在的免疫不良反应至关重要。在这篇综述中,我们根据表面和细胞内蛋白表达,提供了人类和小鼠早期祖细胞和 B 细胞阶段的表型分类。此外,我们还批判性地比较了关键转录因子(Ikaros、E2A、EBF1、PAX5 和 Aiolos)和趋化因子或细胞因子信号(FLT3、c-kit、IL-7R 和 CXCR4)在人类和小鼠中稳态和异常 B 淋巴细胞发生中的作用。

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