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我们如何设计出更好的疫苗来预防女性感染艾滋病毒?

How can we design better vaccines to prevent HIV infection in women?

作者信息

Rafferty Hannah, Sibeko Sengeziwe, Rowland-Jones Sarah

机构信息

Nuffield Department of Medicine, University of Oxford Oxford, UK.

出版信息

Front Microbiol. 2014 Nov 4;5:572. doi: 10.3389/fmicb.2014.00572. eCollection 2014.

Abstract

The human immunodeficiency virus (HIV) burden in women continues to increase, and heterosexual contact is now the most common route of infection worldwide. Effective protection of women against HIV-1 infection may require a vaccine specifically targeting mucosal immune responses in the female genital tract (FGT). To achieve this goal, a much better understanding of the immunology of the FGT is needed. Here we review the architecture of the immune system of the FGT, recent studies of potential methods to achieve the goal of mucosal protection in women, including systemic-prime, mucosal-boost, FGT-tropic vectors and immune response altering adjuvants. Advances in other fields that enhance our understanding of female genital immune correlates and the interplay between hormonal and immunological systems may also help to achieve protection of women from HIV infection.

摘要

女性人群中的人类免疫缺陷病毒(HIV)负担持续上升,异性接触现已成为全球最常见的感染途径。有效保护女性免受HIV-1感染可能需要一种专门针对女性生殖道(FGT)黏膜免疫反应的疫苗。为实现这一目标,需要对FGT的免疫学有更深入的了解。在此,我们综述了FGT免疫系统的结构,以及近期关于实现女性黏膜保护目标的潜在方法的研究,包括系统初免、黏膜加强免疫、FGT嗜性载体和改变免疫反应的佐剂。其他领域的进展有助于增进我们对女性生殖器免疫相关因素以及激素和免疫系统之间相互作用的理解,这也可能有助于实现保护女性免受HIV感染的目标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c215/4219488/32c76a0a5a10/fmicb-05-00572-g0001.jpg

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