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体外试验未能准确预测新生期诱导的H-2耐受性的存在。

Failure of in vitro assays to predict accurately the existence of neonatally induced H-2 tolerance.

作者信息

Streilein J W, Strome P, Wood P J

机构信息

Department of Microbiology and Immunology, University of Miami School of Medicine, Florida 33136.

出版信息

Transplantation. 1989 Oct;48(4):630-4.

PMID:2529680
Abstract

Tolerogen-specific alloreactivity, in the form of mixed lymphocyte responses and cell mediated lympholysis, was measured in vitro using lymphocytes from mice that received neonatal inoculations of H-2 semiallogeneic hematopoietic cells. It was found that depletion of specific alloreactivity, as detected by these assays, was discernable within the thymus glands within 24 to 48 hr of injection. Reduced in vitro alloreactivity was also apparent among spleen cells obtained from neonatally injected mice that had matured immunologically (8 weeks of life). In mice that accepted their test skin allografts (in vivo evidence of tolerance), tolerogen-specific activity was essentially undetectable in vitro. Unexpectedly, markedly attenuated MLR and CML activity was the characteristic finding in neonatally injected mice that rejected their test grafts (in vivo evidence of lack of tolerance). Thus, in vitro assays failed to be predictive of the in vivo tolerant state. These results indicate that clonal reduction of tolerogen-reactive cells is an expected and persistent consequence of the injection of tolerance conferring inocula into neonatal mice. Moreover, we believe that the state of tolerance is maintained in adult tolerant mice by mechanisms that cannot easily be studied or predicted by the results of in vitro assays.

摘要

采用接受新生期接种H-2半同种异体造血细胞的小鼠淋巴细胞,在体外测量以混合淋巴细胞反应和细胞介导的淋巴细胞溶解形式存在的耐受原特异性同种异体反应性。结果发现,通过这些检测方法检测到的特异性同种异体反应性的耗竭,在注射后24至48小时内可在胸腺中辨别出来。在免疫成熟(8周龄)的新生期注射小鼠获得的脾细胞中,体外同种异体反应性降低也很明显。在接受其试验性皮肤同种异体移植的小鼠(体内耐受证据)中,耐受原特异性活性在体外基本无法检测到。出乎意料的是,在新生期注射后排斥其试验性移植物的小鼠(体内缺乏耐受证据)中,显著减弱的混合淋巴细胞反应(MLR)和细胞介导的淋巴细胞溶解(CML)活性是特征性发现。因此,体外检测未能预测体内耐受状态。这些结果表明,向新生小鼠注射诱导耐受的接种物后,耐受原反应性细胞的克隆减少是预期的且持续存在的结果。此外,我们认为成年耐受小鼠中的耐受状态是通过体外检测结果难以轻易研究或预测的机制维持的。

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