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自我更新和迁移对早期妊娠子宫自然杀伤细胞群体的贡献。

Contributions from self-renewal and trafficking to the uterine NK cell population of early pregnancy.

作者信息

Chantakru Sirirak, Miller Craig, Roach Lindsay E, Kuziel William A, Maeda Nobuyo, Wang Wan-Chao, Evans Sharon S, Croy B Anne

机构信息

Department of Biomedical Sciences, Building No.40, Ontario Veterinary College, University of Guelph, Guelph, Ontario, Canada, N1G 2W1.

出版信息

J Immunol. 2002 Jan 1;168(1):22-8. doi: 10.4049/jimmunol.168.1.22.

Abstract

Uterine NK (uNK) cells are abundant in human and murine uteri during decidualization. It is unclear whether precursors of uNK (pre-uNK) cells self-renew or are recruited from other sites. To assess self-renewal of pre-uNK cells, uterine segments from NK cell-competent mice were grafted orthotopically into NK/uNK cell-deficient or wild-type mice. Only in wild-type recipients did decidualized grafts contain uNK cells, indicating that pre-uNK cells do not self-renew in uterus. To identify pre-uNK cell sources, thymus, bone marrow, lymph node, or spleen cells were grafted from virgin or pregnant NK cell-competent donors into mated NK/uNK cell-deficient recipients. Cells from secondary lymphoid tissues of pregnant donors gave high level uNK cell reconstitution, which was independent of chemokine receptors CCR2 or CCR5. Pregnancy-induced changes to lymphocyte-endothelial cell interactions were documented using adhesion of human lymphocytes to frozen mouse tissue sections under shear. A dynamic increase was observed in L-selectin- and alpha(4) integrin-dependent adhesion of CD56(bright) NK cells to decidualizing uterus and in human PBL adhesion to lymph node endothelium. These data support a model that attributes the dramatic increases in human and murine uNK cells during decidualization to precursor cell recruitment.

摘要

在蜕膜化过程中,子宫自然杀伤(uNK)细胞在人和小鼠子宫中大量存在。目前尚不清楚uNK细胞的前体细胞(pre - uNK)是自我更新还是从其他部位募集而来。为了评估pre - uNK细胞的自我更新能力,将具有NK细胞功能的小鼠的子宫段原位移植到NK/uNK细胞缺陷或野生型小鼠体内。只有在野生型受体中,蜕膜化的移植物才含有uNK细胞,这表明pre - uNK细胞在子宫中不会自我更新。为了确定pre - uNK细胞的来源,将来自未交配或怀孕的具有NK细胞功能的供体的胸腺、骨髓、淋巴结或脾细胞移植到交配过的NK/uNK细胞缺陷受体中。来自怀孕供体二级淋巴组织的细胞能实现高水平的uNK细胞重建,且这一过程与趋化因子受体CCR2或CCR5无关。利用人淋巴细胞在剪切力作用下与冷冻小鼠组织切片的黏附,记录了怀孕引起的淋巴细胞与内皮细胞相互作用的变化。观察到CD56(明亮型)NK细胞对蜕膜化子宫的L - 选择素和α(4)整合素依赖性黏附以及人外周血淋巴细胞对淋巴结内皮细胞的黏附呈动态增加。这些数据支持了一种模型,该模型将蜕膜化过程中人和小鼠uNK细胞的显著增加归因于前体细胞的募集。

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