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在小鼠中,流感病毒特异性 CTL 免疫优势等级由高亲和力 T 细胞的相对频率决定。

The influenza virus-specific CTL immunodominance hierarchy in mice is determined by the relative frequency of high-avidity T cells.

机构信息

Department of Microbiology and Immunology, University of Melbourne, at The Peter Doherty Institute for Infection and Immunity, Parkville, Victoria 3010, Australia.

出版信息

J Immunol. 2014 May 1;192(9):4061-8. doi: 10.4049/jimmunol.1301403. Epub 2014 Apr 2.

Abstract

Virus-specific CTL responses typically fall into reproducible hierarchies with particular epitopes eliciting either immunodominant or subdominant responses after viral challenge. The recently acquired capacity to directly enumerate naive CTL precursors (CTLps) in both mice and humans has implicated CTLp frequency as a key predictor of immune response magnitude after Ag challenge. However, recent studies have indicated that naive CTLp frequencies do not necessarily predict the size of the Ag-driven response, indicating an important role for differential CTLp recruitment and/or expansion. This study characterizes the early emergence of various influenza epitope-specific CTL responses at multiple sites in C57BL/6 mice, and probes the role of Ag dose and TCR avidity in dictating immune response hierarchies. Despite large naive CTLp numbers, subdominance was found to arise largely as a consequence of the abrupt and premature cessation of CTL proliferation, at least for one epitope specificity. Investigation into the possible drivers of the poor proliferation observed for subdominant specificities showed that the immunodominance hierarchy endured irrespective of epitope abundance, and correlated with the prevalence of high-avidity T cells in both the naive and immune compartments. Our study strongly indicates that the quality, and not simply the quantity, of antiviral CTLs dictate response magnitude.

摘要

病毒特异性 CTL 反应通常呈现可重复的层次结构,特定表位在病毒攻击后引发免疫优势或亚优势反应。最近人们获得了在小鼠和人类中直接计数幼稚 CTL 前体 (CTLp) 的能力,这表明 CTLp 频率是 Ag 挑战后免疫反应幅度的关键预测因子。然而,最近的研究表明,幼稚 CTLp 频率不一定能预测 Ag 驱动反应的大小,这表明 CTLp 的募集和/或扩增存在差异。本研究描述了 C57BL/6 小鼠多个部位多种流感表位特异性 CTL 反应的早期出现,并探讨了 Ag 剂量和 TCR 亲和力在决定免疫反应层次结构中的作用。尽管存在大量的幼稚 CTLp,但亚优势主要是由于 CTL 增殖的突然和过早停止而产生的,至少对于一种表位特异性是如此。对观察到的亚优势特异性增殖不良的可能驱动因素的调查表明,免疫优势层次结构不受表位丰度的影响,并与幼稚和免疫区室中高亲和力 T 细胞的流行程度相关。我们的研究强烈表明,抗病毒 CTL 的质量(而不仅仅是数量)决定了反应的幅度。

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