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仙台病毒肺炎:疾病过程中γδT细胞早期募集的证据。

Sendai virus pneumonia: evidence for the early recruitment of gamma delta T cells during the disease course.

作者信息

Ogasawara T, Emoto M, Kiyotani K, Shimokata K, Yoshida T, Nagai Y, Yoshikai Y

机构信息

First Department of Internal Medicine, Nagoya University School of Medicine, Japan.

出版信息

J Virol. 1994 Jun;68(6):4022-7. doi: 10.1128/JVI.68.6.4022-4027.1994.

Abstract

We previously reported that gamma delta T cells appeared and could play a protective role early in infections with intracellular bacteria such as Listeria monocytogenes, Mycobacterium bovis BCG, and Salmonella choleraesuis. To extend these findings to virus infection, we examined the developmental sequence of gamma delta T cells in bronchoalveolar lavage during the course of Sendai virus infection in C57BL/6 mice. To produce a natural but nonlethal infection course as far as possible, we used a sublethal dose of a wild-type virus which had not been subjected to serial passages in a chicken embryo, hence retaining full virulence for mice. Virus titers in lungs reached a peak on day 6 and then decreased to an undetectable level by day 10. This time course of virus reproduction was immediately and coincidentally followed by the developmental course of gamma delta T cells, in which the cell number peaked on day 7 and then decreased to a marginal level by day 10. On the other hand, the alpha beta T-cell number continued to increase until day 10 and remained at a high level thereafter. The early-appearing gamma delta T cells were CD4-, CD8-, IL-2R alpha- beta+, CD44+, Mel-14-, and LFA-1 alpha/beta+ in phenotype and used V gamma 1/2 and V gamma 4 and V delta 3, V delta 4, V delta 5, and V delta 6. The gamma delta T cells were responding to macrophages from infected mice when the cells were cultured in vitro. Furthermore, the expression of endogenous heat shock protein (hsp) was infection specific, and its level appeared to correlate with the gamma delta T-cell development. These results suggest that the early recruitment of gamma delta T cells, which proliferate in response to endogenous hsp+ cells, is also characteristic of this virus infection, although this view appears to be contradictory to earlier reports.

摘要

我们先前报道,γδ T细胞会出现,并在细胞内细菌(如单核细胞增生李斯特菌、卡介苗和猪霍乱沙门氏菌)感染早期发挥保护作用。为了将这些发现扩展到病毒感染,我们研究了C57BL/6小鼠感染仙台病毒过程中支气管肺泡灌洗中γδ T细胞的发育序列。为了尽可能产生自然但非致死性的感染过程,我们使用了亚致死剂量的野生型病毒,该病毒未在鸡胚中连续传代,因此对小鼠仍保留全部毒力。肺中的病毒滴度在第6天达到峰值,然后在第10天降至无法检测的水平。病毒繁殖的这个时间进程紧接着γδ T细胞的发育进程,其中细胞数量在第7天达到峰值,然后在第10天降至边缘水平。另一方面,αβ T细胞数量持续增加直至第10天,此后保持在高水平。早期出现的γδ T细胞表型为CD4 -、CD8 -、IL - 2Rαβ +、CD44 +、Mel - 14 -和LFA - 1α/β +,并使用Vγ1/2和Vγ4以及Vδ3、Vδ4、Vδ5和Vδ6。当γδ T细胞在体外培养时,它们对来自感染小鼠的巨噬细胞有反应。此外,内源性热休克蛋白(hsp)的表达具有感染特异性,其水平似乎与γδ T细胞的发育相关。这些结果表明,尽管这一观点似乎与早期报道相矛盾,但γδ T细胞的早期募集也是这种病毒感染的特征,γδ T细胞会对内源性hsp +细胞作出反应而增殖。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b10e/236909/5c052f28d5b8/jvirol00015-0582-a.jpg

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