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小鼠对细菌脂多糖反应的遗传控制。II. 一个影响参与脂多糖激活骨髓来源淋巴细胞的膜成分的基因。

Genetic control of responses to bacterial lipopolysaccharides in mice. II. A gene that influences a membrane component involved in the activation of bone marrow-derived lymphocytes by lipipolysaccharides.

作者信息

Watson J, Riblet R

出版信息

J Immunol. 1975 May;114(5):1462-8.

PMID:123543
Abstract

C3H/HeJ mice contain a defect in a single autosomal locus which is not linked to the H-2 histocompatibility or the heavy chain allotype loci that restrict immune, mitogenic, and polyclonal responses to bacterial lipopolysaccharides (LPS). Adult thymectomized C3H/HeJ mice that have been irradiated and reconstituted with C3HeB/FeJ bone marrow cells respond well to LPS. Cell-mixing experiments using C3H/HEJ-C3HeB/FeJ spleen cultures show that the failure of C3H/HeJ spleen cells to support responses to LPS is not due to nonspecific or LPS-induced suppressive events, or the lack of accessory cell types. C3H/HeJ and C3HeB/FeJ spleen cells bind LPS and respond to other B cell mitogens equally well. We suggest that the B lymphocytes of C3H/HeJ mice have a defect in a membrane component that is activated via interaction with LPS, and initiates the intracellular events that lead to cell proliferation.

摘要

C3H/HeJ小鼠在一个常染色体位点存在缺陷,该位点与H-2组织相容性或重链同种异型位点无关,后者限制了对细菌脂多糖(LPS)的免疫、促有丝分裂和多克隆反应。经照射并用C3HeB/FeJ骨髓细胞重建的成年去胸腺C3H/HeJ小鼠对LPS反应良好。使用C3H/HEJ-C3HeB/FeJ脾细胞培养物进行的细胞混合实验表明,C3H/HeJ脾细胞无法支持对LPS的反应,这并非由于非特异性或LPS诱导的抑制事件,也不是由于缺乏辅助细胞类型。C3H/HeJ和C3HeB/FeJ脾细胞结合LPS,并对其他B细胞有丝分裂原产生同等良好的反应。我们认为,C3H/HeJ小鼠的B淋巴细胞在一种膜成分上存在缺陷,该膜成分通过与LPS相互作用而被激活,并启动导致细胞增殖的细胞内事件。

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Genetic control of responses to bacterial lipopolysaccharides in mice. II. A gene that influences a membrane component involved in the activation of bone marrow-derived lymphocytes by lipipolysaccharides.小鼠对细菌脂多糖反应的遗传控制。II. 一个影响参与脂多糖激活骨髓来源淋巴细胞的膜成分的基因。
J Immunol. 1975 May;114(5):1462-8.
2
Genetic control of responses to bacterial lipopolysaccharides in mice. I. Evidence for a single gene that influences mitogenic and immunogenic respones to lipopolysaccharides.小鼠对细菌脂多糖反应的遗传控制。I. 影响对脂多糖促有丝分裂和免疫原性反应的单个基因的证据。
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Immunologic properties of bacterial lipopolysaccharide (LPS). IV. Cellular basis of the unresponsiveness of C3H/HeJ mouse spleen cells to LPS-induced mitogenesis.细菌脂多糖(LPS)的免疫学特性。IV. C3H/HeJ小鼠脾细胞对LPS诱导的有丝分裂原反应无反应性的细胞基础。
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Immunologic responsiveness of the C3H/HeJ mouse: differential ability of butanol-extracted lipopolysaccharide (LPS) to evoke LPS-mediated effects.C3H/HeJ小鼠的免疫反应性:丁醇提取的脂多糖(LPS)引发LPS介导效应的差异能力。
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