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证据表明,在小鼠体内 NK 细胞 Ly-49 的发育途径是被预先设定好的。

Evidence for Prescribed NK Cell Ly-49 Developmental Pathways in Mice.

机构信息

Department of Molecular and Cell Biology, School of Natural Sciences, University of California, Merced, Merced, CA 95343.

Department of Applied Mathematics, School of Natural Sciences, University of California, Merced, Merced, CA 95343; and.

出版信息

J Immunol. 2021 Mar 15;206(6):1215-1227. doi: 10.4049/jimmunol.2000613. Epub 2021 Jan 25.

Abstract

Previous studies of NK cell inhibitory Ly-49 genes showed their expression is stochastic. However, relatively few studies have examined the mechanisms governing acquisition of inhibitory receptors in conjunction with activating Ly-49 receptors and NK cell development. We hypothesized that the surface expression of activating Ly-49 receptors is nonrandom and is influenced by inhibitory Ly-49 receptors. We analyzed NK cell "clusters" defined by combinatorial expression of activating (Ly-49H and Ly-49D) and inhibitory (Ly-49I and Ly-49G2) receptors in C57BL/6 mice. Using the product rule to evaluate the interdependencies of the Ly-49 receptors, we found evidence for a tightly regulated expression at the immature NK cell stage, with the highest interdependencies between clusters that express at least one activating receptor. Further analysis demonstrated that certain NK clusters predominated at the immature (CD27CD11b), transitional (CD27CD11b), and mature (CD27CD11b) NK cell stages. Using parallel in vitro culture and in vivo transplantation of sorted NK clusters, we discovered nonrandom expression of Ly-49 receptors, suggesting that prescribed pathways of NK cluster differentiation exist. Our data infer that surface expression of Ly-49I is an important step in NK cell maturation. Ki-67 expression and cell counts confirmed that immature NK cells proliferate more than mature NK cells. We found that MHC class I is particularly important for regulation of Ly-49D and Ly-49G2, even though no known MHC class I ligand for these receptors is present in B6 mice. Our data indicate that surface expression of both activating and inhibitory Ly-49 receptors on NK cell clusters occurs in a nonrandom process correlated to their maturation stage.

摘要

先前关于 NK 细胞抑制性 Ly-49 基因的研究表明,其表达是随机的。然而,相对较少的研究检查了与激活性 Ly-49 受体和 NK 细胞发育一起控制抑制性受体获得的机制。我们假设激活性 Ly-49 受体的表面表达是非随机的,并受抑制性 Ly-49 受体的影响。我们分析了 C57BL/6 小鼠中通过激活(Ly-49H 和 Ly-49D)和抑制(Ly-49I 和 Ly-49G2)受体组合表达定义的 NK 细胞“簇”。使用乘积法则评估 Ly-49 受体的相互依存关系,我们发现证据表明在不成熟 NK 细胞阶段存在严格调控的表达,具有至少一个激活受体的簇之间具有最高的相互依存关系。进一步的分析表明,某些 NK 簇在不成熟(CD27CD11b)、过渡(CD27CD11b)和成熟(CD27CD11b)NK 细胞阶段占主导地位。通过平行的体外培养和分选 NK 簇的体内移植,我们发现 Ly-49 受体的非随机表达,表明存在 NK 簇分化的规定途径。我们的数据推断出 Ly-49I 的表面表达是 NK 细胞成熟的重要步骤。Ki-67 表达和细胞计数证实不成熟 NK 细胞比成熟 NK 细胞增殖更多。我们发现 MHC 类 I 对 Ly-49D 和 Ly-49G2 的调节特别重要,即使在 B6 小鼠中不存在这些受体的已知 MHC 类 I 配体。我们的数据表明,NK 细胞簇上的激活和抑制性 Ly-49 受体的表面表达以与它们的成熟阶段相关的非随机过程发生。

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