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IL-7: the global builder of the innate lymphoid network and beyond one niche at a time

机译:IL-7:天生淋巴结网络的全球建设者及以后一次一个利基

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摘要

The development and homeostasis of adaptive and innate lymphocytes is dependent on the stromal cytokine IL-7. The initial priming of immune responses to pathogenic challenges is executed by innate lymphoid cells (ILCs) with programmed capacity to rapidly secrete effector cytokines. How ILCs are controlled by IL-7 in distinct anatomical locale has evolved into a more complex problem as IL-7 receptor is not only expressed on ILCs, but also on surrounding neighbors, including vascular endothelium and mesenchymal cells that compete for limiting IL-7. For the generation of γδ T and B cells IL-7 is required for the production of antigen receptors, and it is likely that IL-7 performs critical function in facilitating ILC effector programming in addition to its regulatory actions on cell survival and proliferation. Most of our current understanding of the highly calibrated regulatory circuits of IL-7 function and IL-7 receptor signaling has derived from studies of adaptive, conventional lymphocytes. Here we highlight recent advances in mapping the gene circuits and cellular interactions that regulate temporospatial activities of IL-7 in diverse macro and micro niches that have direct relevance to deciphering the sphere of impact of IL-7 on ILC differentiation.
机译:适应性和先天淋巴细胞的开发和稳态取决于基质细胞因子IL-7。免疫应答对致病挑战的初始引发是通过先天淋巴细胞(ILC)进行的,其具有迅速分泌效应细胞因子的程序化能力。 IL-7在不同的解剖学区域中如何控制IL-7已经发展成为更复杂的问题,因为IL-7受体不仅在ILC上表达,而且在周围的邻居上,包括血管内皮和间充质细胞,用于限制IL-7 。对于γδT和B细胞的产生,抗原受体所需的IL-7是IL-7所需的,并且IL-7除了对细胞存活和增殖的调节作用之外,IL-7还在促进ILC效应器编程方面进行关键功能。大多数人目前对IL-7功能高度校准的调节电路和IL-7受体信号传导的理解源自适应性,常规淋巴细胞的研究。在这里,我们突出了近期映射基因电路和细胞相互作用的最新进展,该研究在不同于宏观和微地位中调节IL-7的时间间隙活动,这些宏观和微利骨头具有与解密IL-7对ILC分化的影响的直接相关的直接相关性。

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