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Both CD4+ and CD8+ T cells are involved in protection against HSV-1 induced corneal scarring

机译:CD4 +和CD8 + T细胞均参与针对HSV-1诱导的角膜瘢痕形成的保护

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摘要

AIM—To determine the relative impact of CD4+ T cells and CD8+ T cells in protecting mice against ocular HSV-1 challenge.
METHODS—CD4+ T cell knockout mice (CD4−/− mice), CD8+ T cell knockout mice (CD8−/− mice), and mice depleted for CD4+ or CD8+ T cells by antibody (CD4+ depleted and CD8+ depleted mice), were examined for their ability to withstand HSV-1 ocular challenge. The parental mice for both knockout mice were C57BL/6J.
RESULTS—These results suggest that: (1) both CD4+ deficient mice (CD4−/− and CD4+ depleted mice) and CD8+ deficient mice (CD8−/−, and CD8+ depleted mice) developed significantly more corneal scarring than their C57BL/6J parental strain; (2) the duration of virus clearance from the eyes of the CD4+ deficient mice was 4 days longer than that of the CD8+ deficient mice; and (3) the severity of corneal scarring in the CD4+ deficient mice was approximately twice that of the CD8+ deficient mice.
CONCLUSIONS—It was reported here that: (1) CD4+ and CD8+ T cells were both involved in protection against lethal ocular HSV-1 infection; and (2) CD4+ and CD8+ T cells were both involved in protection against HSV-1 induced corneal scarring.

机译:目的:确定CD4 + T细胞和CD8 + T细胞在保护小鼠免受HSV-1攻击方面的相对影响。
方法-CD4 + T细胞敲除小鼠(CD4-/-小鼠),CD8 + T细胞敲除小鼠(检查了CD8-/-小鼠)和通过抗体而耗尽了CD4 +或CD8 + T细胞的小鼠(CD4 +耗尽的小鼠和CD8 +耗尽的小鼠)抵抗HSV-1眼球攻击的能力。结果,两个敲除小鼠的亲本小鼠均为C57BL / 6J。这些结果表明:(1)CD4 +缺陷小鼠(CD4-/-和CD4 +缺陷小鼠)和CD8 +缺陷小鼠(CD8-/-,和CD8 +耗竭的小鼠)比其C57BL / 6J亲本株产生的角膜瘢痕明显增多; (2)从CD4 +缺陷小鼠的眼睛清除病毒的持续时间比CD8 +缺陷小鼠的清除病毒的时间长4天; (3)CD4 +缺陷小鼠的角膜瘢痕严重程度大约是CD8 +缺陷小鼠的两倍。
结论—在此报道:(1)CD4 +和CD8 + T细胞均参与了抗CD4 +和CD8 + T细胞的保护作用致命的眼HSV-1感染; (2)CD4 +和CD8 + T细胞均参与了针对HSV-1诱导的角膜瘢痕形成的保护作用。

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