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Transcriptional Regulation of Innate and Adaptive Lymphocyte Lineages

机译:先天和适应性淋巴细胞谱系的转录调控。

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摘要

The lymphocyte family has expanded significantly in recent years to include not only the adaptive lymphocytes (T cells, B cells) and NK cells, but also several additional innate lymphoid cell (ILC) types. ILCs lack clonally distributed antigen receptors characteristic of adaptive lymphocytes and instead respond exclusively to signaling via germline-encoded receptors. ILCs resemble T cells more closely than any other leukocyte lineage at the trailscriptome level and express many elements of the core cell transcriptional program, including Notch, Gata3 T47, and Bd11b. We present our current understanding of the shared and distinct transcriptional regulatory mechanisms involved in the development of adaptive T lymphocytes and closely related ILCs. We discuss the possibility that a core set of transcriptional regulators common to ILCs and T cells establish enhancers that enable implementation of closely aligned effector pathways. Studies of the transcriptional regulation of lymphopoiesis will support the development of novel therapeutic approaches to correct early lymphoid developmental defects and aberrant lymphocyte function.
机译:近年来,淋巴细胞家族已显着扩展,不仅包括适应性淋巴细胞(T细胞,B细胞)和NK细胞,还包括其他几种先天性淋巴样细胞(ILC)类型。 ILC缺乏以适应性淋巴细胞为特征的克隆分布的抗原受体,而只能通过种系编码的受体对信号作出反应。在尾迹组水平上,ILC比其他任何白细胞谱系更像T细胞,并表达核心细胞转录程序的许多元素,包括Notch,Gata3 T47和Bd11b。我们目前对参与自适应T淋巴细胞和密切相关的ILC的发展所涉及的共享和独特的转录调控机制的理解目前。我们讨论了ILC和T细胞共有的一组转录调节因子核心建立增强子的可能性,这些增强子使紧密结合的效应子途径得以实施。淋巴细胞生成的转录调控的研究将支持新的治疗方法的开发,以纠正早期的淋巴发育缺陷和异常的淋巴细胞功能。

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