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当多种免疫反应控制 HIV 感染时,免疫逃逸的速度就会消失。

The rate of immune escape vanishes when multiple immune responses control an HIV infection.

机构信息

Theoretical Biology and Bioinformatics, Utrecht University, 3584 CH Utrecht, The Netherlands.

出版信息

J Immunol. 2013 Sep 15;191(6):3277-86. doi: 10.4049/jimmunol.1300962. Epub 2013 Aug 12.

Abstract

During the first months of HIV infection, the virus typically evolves several immune escape mutations. These mutations are found in epitopes in viral proteins and reduce the impact of the CD8⁺ T cells specific for these epitopes. Recent data show that only a subset of the epitopes escapes, that most of these escapes evolve early, and that the rate of immune escape slows down considerably. To investigate why the evolution of immune escape slows down over the time of infection, we have extended a consensus mathematical model to allow several immune responses to control the virus together. In the extended model, most escapes also occur early, and the immune escape rate becomes small later, and typically only a minority of the epitopes escape. We show that escaping one of the many immune responses provides little advantage after viral setpoint has been approached because the total killing rate hardly depends on the breadth of the immune response. If the breadth of the immune response slowly wanes during disease progression, the model predicts an increase in the rate of immune escape at late stages of infection. Overall, the most striking prediction of the model is that HIV evolves a small number of immune escapes, in both relative and absolute terms, when the CTL immune response is broad.

摘要

在 HIV 感染的最初几个月,病毒通常会进化出几种免疫逃避突变。这些突变存在于病毒蛋白的表位中,降低了针对这些表位的 CD8⁺ T 细胞的作用。最近的数据表明,只有一部分表位发生逃避,大多数逃避发生在早期,免疫逃避的速度会大大减慢。为了研究为什么随着感染时间的推移,免疫逃避的进化会减慢,我们将一个共识数学模型扩展到允许几个免疫反应一起控制病毒。在扩展模型中,大多数逃避也发生在早期,免疫逃避率在后期变得很小,通常只有少数表位逃避。我们表明,在病毒基准点被接近后,逃避多种免疫反应中的一种几乎没有优势,因为总杀伤率几乎不取决于免疫反应的广度。如果免疫反应的广度在疾病进展过程中缓慢减弱,那么该模型预测感染后期的免疫逃避率会增加。总的来说,该模型最显著的预测是,当 CTL 免疫反应广泛时,HIV 会以相对和绝对的方式产生少量的免疫逃避。

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