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抗体和CD8 + T细胞相辅相成,对于对高致死性细胞病变病毒的天然抵抗力至关重要。

Antibodies and CD8+ T cells are complementary and essential for natural resistance to a highly lethal cytopathic virus.

作者信息

Fang Min, Sigal Luis J

机构信息

Fox Chase Cancer Center, Basic Sciences Division, Program on Viral Pathogenesis, Philadelphia, PA 19111, USA.

出版信息

J Immunol. 2005 Nov 15;175(10):6829-36. doi: 10.4049/jimmunol.175.10.6829.

Abstract

It is believed that CD8+ T lymphocytes or Abs can independently clear many primary viral infections, including those caused by Orthopoxviruses (OPV), a genus that includes the human pathogens variola and monkeypox and the vaccine species vaccinia virus. However, most experiments addressing the role of Abs and CD8+ T cells in protection have used viruses that are not specific for the host. In the present study, we used the mouse-specific OPV ectromelia virus and mice deficient in CD40, B cells, or CD8+ T cells and adoptive transfers of CD8+ T or B lymphocytes to show that the protection afforded by CD8+ T cells is incomplete. Despite sustained CD8+ T cell responses, in the absence of Ab responses ectromelia virus persists. This results in delayed disease and inexorably leads to death. Therefore, CD8+ T lymphocytes and Abs are not redundant but complementary and essential to survive infections with a highly pathogenic viruses in the natural host.

摘要

据信,CD8 + T淋巴细胞或抗体可独立清除许多原发性病毒感染,包括由正痘病毒(OPV)引起的感染,该病毒属包括人类病原体天花和猴痘以及疫苗株痘苗病毒。然而,大多数研究抗体和CD8 + T细胞在保护作用中角色的实验使用的病毒并非宿主特异性病毒。在本研究中,我们使用小鼠特异性OPV埃可病毒以及缺乏CD40、B细胞或CD8 + T细胞的小鼠,并通过过继转移CD8 + T或B淋巴细胞来表明CD8 + T细胞提供的保护是不完整的。尽管CD8 + T细胞反应持续存在,但在没有抗体反应的情况下,埃可病毒仍会持续存在。这会导致疾病延迟,并不可避免地导致死亡。因此,CD8 + T淋巴细胞和抗体并非多余,而是互补的,对于天然宿主在感染高致病性病毒后存活至关重要。

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