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胸腺外生理性 T 系祖细胞活性仅局限于表达 CD127、CD90 或高水平 CD117 的细胞。

Extra-thymic physiological T lineage progenitor activity is exclusively confined to cells expressing either CD127, CD90, or high levels of CD117.

机构信息

Institute for Immunology, Hannover Medical School, Hannover, Germany.

出版信息

PLoS One. 2012;7(2):e30864. doi: 10.1371/journal.pone.0030864. Epub 2012 Feb 15.

Abstract

T cell development depends on continuous recruitment of progenitors from bone marrow (BM) to the thymus via peripheral blood. However, both phenotype and functional characteristics of physiological T cell precursors remain ill-defined. Here, we characterized a putative CD135(+)CD27(+) T cell progenitor population, which lacked expression of CD127, CD90, and high levels of CD117 and was therefore termed triple negative precursor (TNP). TNPs were present in both BM and blood and displayed robust T lineage potential, but virtually no myeloid or B lineage potential, in vitro. However, TNPs did not efficiently generate T lineage progeny after intravenous or intrathymic transfer, suggesting that a physiological thymic microenvironment does not optimally support T cell differentiation from TNPs. Thus, we propose that physiological T cell precursors are confined to populations expressing either CD127, CD90, or high levels of CD117 in addition to CD135 and CD27 and that TNPs may have other physiological functions.

摘要

T 细胞的发育依赖于祖细胞通过外周血从骨髓(BM)不断募集到胸腺。然而,生理 T 细胞前体的表型和功能特征仍未被明确界定。在这里,我们描述了一种假定的 CD135(+)CD27(+)T 细胞祖细胞群体,该群体缺乏 CD127、CD90 的表达,以及高水平的 CD117,因此被称为三阴性前体(TNP)。TNP 存在于 BM 和血液中,具有强大的 T 细胞谱系潜能,但在体外几乎没有髓系或 B 细胞谱系潜能。然而,TNP 并不能有效地在静脉内或胸腺内转移后产生 T 细胞谱系后代,这表明生理胸腺微环境不能最优地支持 TNP 从 T 细胞分化。因此,我们提出生理 T 细胞前体局限于除 CD135 和 CD27 之外还表达 CD127、CD90 或高水平 CD117 的群体,而 TNP 可能具有其他生理功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a165/3280270/fbe23709556c/pone.0030864.g001.jpg

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