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全身淋巴组织照射导致小鼠胸腺髓质短暂耗竭以及髓质基质细胞持续异常。

Total lymphoid irradiation leads to transient depletion of the mouse thymic medulla and persistent abnormalities among medullary stromal cells.

作者信息

Adkins B, Gandour D, Strober S, Weissman I

机构信息

Department of Pathology, Stanford University School of Medicine, CA 94305.

出版信息

J Immunol. 1988 May 15;140(10):3373-9.

PMID:2452185
Abstract

Mice given multiple doses of sublethal irradiation to both the thymus and the peripheral lymphoid tissues showed major transient, and some persistent disruptions in general thymic architecture and in thymic stromal components. At 2 wk after total lymphoid irradiation (TLI), the thymus lacked identifiable medullary regions by immunohistochemical analyses. Medullary stromal cells expression MHC Ag or a medullary epithelial cell Ag, as well as medullary macrophages, were undetectable. Instead, the processes of cortical epithelial cells were observed throughout the entire thymus. Strikingly, thymocyte subsets with mature phenotypes (CD4+CD8- and CD4-CD8+) were present in the apparent absence of a medulla. This early, gross effect was rapidly reversed such that by 1 to 2 mo after TLI, medullary areas with MHC Ag-positive cells were evident. However, abnormalities in a subset of medullary stromal cells appeared to be more persistent. Medullary epithelial cells, identified by the MD1 mAb, were greatly reduced in number and abnormally organized for at least 4 mo after TLI. In addition, macrophages containing endogenous peroxidase activity, normally abundant in medullary regions, were undetectable at all times examined after TLI. Therefore, this irradiation regimen induced both transient and long term effects in the thymus, primarily in medullary regions. These results suggest that TLI may be used as an experimental tool for studying the impact of selective depletion of medullary stromal cells on the development of specific T cell functions.

摘要

接受多次亚致死剂量照射的小鼠,其胸腺和外周淋巴组织均出现了主要的短暂性以及一些持续性的胸腺总体结构和胸腺基质成分破坏。在全身淋巴照射(TLI)后2周,通过免疫组织化学分析发现胸腺缺乏可识别的髓质区域。髓质基质细胞表达的MHC抗原或髓质上皮细胞抗原以及髓质巨噬细胞均无法检测到。相反,在整个胸腺中都观察到了皮质上皮细胞的突起。引人注目的是,在明显没有髓质的情况下却存在具有成熟表型的胸腺细胞亚群(CD4 + CD8 - 和CD4 - CD8 +)。这种早期的总体效应迅速逆转,以至于在TLI后1至2个月,带有MHC抗原阳性细胞的髓质区域明显可见。然而,一部分髓质基质细胞的异常似乎更具持续性。由MD1单克隆抗体识别的髓质上皮细胞数量大幅减少,并且在TLI后至少4个月内组织异常。此外,在TLI后的所有检查时间点,通常在髓质区域丰富的含有内源性过氧化物酶活性的巨噬细胞均无法检测到。因此,这种照射方案在胸腺中诱导了短暂和长期的效应,主要发生在髓质区域。这些结果表明,TLI可作为一种实验工具,用于研究选择性清除髓质基质细胞对特定T细胞功能发育的影响。

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