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混合异基因嵌合体中的自然杀伤细胞耐受性。

NK cell tolerance in mixed allogeneic chimeras.

作者信息

Zhao Yong, Ohdan Hideki, Manilay Jennifer O, Sykes Megan

机构信息

Bone Marrow Transplantation Section, Transplantation Biology Research Center, Surgical Service, Massachusetts General Hospital/Harvard Medical School, Boston, MA 02129, USA.

出版信息

J Immunol. 2003 Jun 1;170(11):5398-405. doi: 10.4049/jimmunol.170.11.5398.

Abstract

Alterations in inhibitory receptor expression on NK cells have been detected in mixed allogeneic chimeras and in mosaic MHC class I-expressing transgenic mice. However, it is not known whether or not NK cells are tolerant to host and donor Ags in mixed chimeras. In vitro studies have shown a lack of mutual tolerance of separated donor and host NK cells obtained from mixed chimeras. Using BALB/c-->B6 fully MHC-mismatched mixed chimeras, we have now investigated this question in vivo. Neither donor nor host NK cells in mixed chimeras showed evidence for activation, as indicated by expression of B220 and Thy-1.2 on NK cells in chimeric mice at levels similar to those in nonchimeric control mice. Lethally irradiated, established mixed BALB/c--> B6 chimeras rejected a low dose of beta(2)-microglobulin-deficient bone marrow cells (BMC) efficiently but did not reject BALB/c or B6 BMCs. In contrast, similarly conditioned B6 mice rejected both BALB/c and beta(2)-microglobulin-deficient BMCs. Thus, NK cells were specifically tolerant to the donor and the host in mixed allogeneic chimeras. The similar growth of RMA lymphoma cells in both chimeric and control B6 mice further supports the conclusion that donor BALB/c NK cells are tolerant to B6 Ags in chimeras. Administration of a high dose of exogenous IL-2 could not break NK cell tolerance in chimeric mice, suggesting that NK cell tolerance in chimeras is not due to a lack of activating cytokine. No reduction in the level of expression of the activating receptor Ly-49D, recognizing a donor MHC molecule, was detected among recipient NK cells in mixed chimeras. Thus, the present studies demonstrate that NK cells in mixed chimeras are stably tolerant to both donor and host Ags, by mechanisms that are as yet unexplained.

摘要

在混合异基因嵌合体和表达镶嵌型MHC I类分子的转基因小鼠中,已检测到NK细胞上抑制性受体表达的改变。然而,尚不清楚在混合嵌合体中NK细胞是否对宿主和供体抗原具有耐受性。体外研究表明,从混合嵌合体中分离出的供体和宿主NK细胞缺乏相互耐受性。利用BALB/c→B6完全MHC不匹配的混合嵌合体,我们现在在体内研究了这个问题。混合嵌合体中的供体和宿主NK细胞均未显示激活迹象,嵌合小鼠中NK细胞上B220和Thy-1.2的表达水平与非嵌合对照小鼠相似。经致死剂量照射建立的混合BALB/c→B6嵌合体有效地排斥了低剂量的β2-微球蛋白缺陷骨髓细胞(BMC),但不排斥BALB/c或B6 BMC。相比之下,经过类似处理的B6小鼠排斥BALB/c和β2-微球蛋白缺陷的BMC。因此,NK细胞在混合异基因嵌合体中对供体和宿主具有特异性耐受性。RMA淋巴瘤细胞在嵌合和对照B6小鼠中的相似生长进一步支持了这样的结论,即嵌合体中供体BALB/c NK细胞对B6抗原具有耐受性。给予高剂量的外源性IL-2不能打破嵌合小鼠中的NK细胞耐受性,这表明嵌合体中NK细胞的耐受性不是由于缺乏激活细胞因子。在混合嵌合体的受体NK细胞中,未检测到识别供体MHC分子的激活受体Ly-49D表达水平的降低。因此,本研究表明,混合嵌合体中的NK细胞通过尚未阐明的机制对供体和宿主抗原均具有稳定的耐受性。

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