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CD8 + 2型T细胞会加重小鼠急性疱疹病毒感染的严重程度。

CD8+ type-2 T cells enhance the severity of acute herpes virus infection in mice.

作者信息

Ikemoto K, Pollard R B, Fukumoto T, Morimatsu M, Suzuki F

机构信息

Department of Neurology, Yamaguchi University School of Medicine, Japan.

出版信息

Immunol Lett. 1995 Jul-Aug;47(1-2):63-72. doi: 10.1016/0165-2478(95)00063-b.

Abstract

The role of CD8+ suppressor T cells in acute herpes simplex virus type 1 (HSV) infection was investigated in mice. CD8+ CD11b+ TCR-gamma/delta + suppressor T cells (HSV-STC) were demonstrated in spleens of mice infected intraperitoneally (i.p.) with HSV. When HSV-STC from mice infected with a 10 LD50 of HSV (donors) were adoptively transferred to mice 3 days after being infected with a 1 LD50 dose of HSV (recipients), the morbidity and mortality of recipients were greatly increased (mean survival time in days (MSD): 9.4 days; mortality, 100%) as compared with controls that received CD4+ T cells or a whole T-cell lysate from donors (MSD, > 19.6 days or > 19.1 days; mortality, 38% or 50%). The morbidity and mortality of mice exposed to a 1 LD50 of HSV were also increased when they were continuously treated with recombinant murine IL-4. However, the survival rate of mice exposed to a 10 LD50 of HSV increased after multiple treatments of these mice with anti-IL-4 monoclonal antibody. IL-4-producing cells were detected in a population of HSV-STC, and IL-4 was produced when these cells were cultured in the presence of UV-inactivated HSV in vitro. These results indicate that IL-4 plays an important role in the progression of acute HSV infection and, through the production of IL-4, HSV-STC may increase the severity of the acute-phase infection of HSV in mice.

摘要

在小鼠中研究了CD8 +抑制性T细胞在急性1型单纯疱疹病毒(HSV)感染中的作用。在经腹腔注射(i.p.)HSV感染的小鼠脾脏中证实了CD8 + CD11b + TCR-γ/δ +抑制性T细胞(HSV-STC)。当将来自感染10 LD50 HSV的小鼠(供体)的HSV-STC在感染1 LD50剂量HSV(受体)3天后过继转移至小鼠时,与接受供体CD4 + T细胞或全T细胞裂解物的对照组相比,受体的发病率和死亡率大大增加(平均存活天数(MSD):9.4天;死亡率,100%)(MSD,> 19.6天或> 19.1天;死亡率,38%或50%)。当用重组鼠IL-4连续处理时,暴露于1 LD50 HSV的小鼠的发病率和死亡率也增加。然而,在用抗IL-4单克隆抗体对这些小鼠进行多次处理后,暴露于10 LD50 HSV的小鼠的存活率增加。在HSV-STC群体中检测到产生IL-4的细胞,并且当这些细胞在体外紫外线灭活的HSV存在下培养时产生IL-4。这些结果表明,IL-4在急性HSV感染的进展中起重要作用,并且通过产生IL-4,HSV-STC可能会增加小鼠HSV急性期感染的严重程度。

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