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卡介苗感染期间早期出现的携带γ/δ的T细胞。

Early appearing gamma/delta-bearing T cells during infection with Calmétte Guérin bacillus.

作者信息

Inoue T, Yoshikai Y, Matsuzaki G, Nomoto K

机构信息

Department of Immunology, Kyushu University, Fukuoka, Japan.

出版信息

J Immunol. 1991 Apr 15;146(8):2754-62.

PMID:1707921
Abstract

To search for a potential role of TCR gamma/delta T cells in host-defense against mycobacterial infection, we analyzed the kinetics, repertoire, specificity, and cytokine production of gamma/delta T cells in the peritoneal exudate cells (PEC), lymph node (LN) cells and spleen cells during an i.p. infection with a sublethal dose (5 x 10(5) of viable Bacillus Calmétte-Guérin (BCG) in mice. In the PEC on day 7 after infection, approximately 26% of the CD3+ cells were CD4-CD8-, most of which expressed TCR gamma/delta on their surface. However, the PEC on day 28 contained an increased number of alpha/beta T cells that were CD4+8- or CD4-8+ and the proportion of gamma/delta T cells in the PEC reciprocally decreased to 18% of the CD3+ cells. The kinetics of gamma/delta and alpha/beta T cells in the LN during BCG infection showed in much the same pattern as that seen in the PEC. When purified CD4-CD8- cells in the LN on day 7 after BCG infection were cultured with sonicated BCG lysate, PPD derived from Mycobacterium tuberculosis or recombinant 65 kDa heat shock protein derived from Mycobacterium bovis, the gamma/delta T cells on this stage significantly proliferated and secreted IL-2 in response to sonicated BCG lysate and PPD but not to 65 kDa heat shock protein. V gene segment usage analysis with PCR method revealed that purified protein derivative-reactive gamma/delta T cells preferentially used V gamma 1/2/V delta 6, whereas gamma/delta T cells polyclonally expanded in response to the BCG lysate. These results suggest that gamma/delta T cells specific for mycobacterial antigens preceding alpha/beta T cells in appearance during infection may serve as a first line of defense against mycobacterial infection.

摘要

为了探寻TCRγ/δ T细胞在宿主抗分枝杆菌感染防御中的潜在作用,我们分析了小鼠腹腔注射亚致死剂量(5×10⁵)活卡介苗(BCG)后,腹腔渗出细胞(PEC)、淋巴结(LN)细胞和脾细胞中γ/δ T细胞的动力学、谱系、特异性及细胞因子产生情况。感染后第7天的PEC中,约26%的CD3⁺细胞为CD4⁻CD8⁻,其中大多数细胞表面表达TCRγ/δ。然而,第28天的PEC中,α/β T细胞数量增加,为CD4⁺8⁻或CD4⁻8⁺,PEC中γ/δ T细胞的比例相应降至CD3⁺细胞的18%。BCG感染期间LN中γ/δ和α/β T细胞的动力学表现与PEC中的情况大致相同。将BCG感染后第7天LN中纯化的CD4⁻CD8⁻细胞与超声处理的BCG裂解物、结核分枝杆菌来源的PPD或牛分枝杆菌来源的重组65 kDa热休克蛋白一起培养时,此阶段的γ/δ T细胞对超声处理的BCG裂解物和PPD有显著增殖并分泌IL - 2,但对65 kDa热休克蛋白无反应。用PCR方法进行V基因片段使用分析表明,纯化蛋白衍生物反应性γ/δ T细胞优先使用Vγ1/2/Vδ6,而γ/δ T细胞对BCG裂解物呈多克隆扩增。这些结果表明,感染期间在α/β T细胞之前出现的针对分枝杆菌抗原的γ/δ T细胞可能作为抗分枝杆菌感染的第一道防线。

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