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一种低复制性HIV-2活病毒疫苗可使食蟹猴在受到HIV-2(287)攻击后免受疾病侵害。

A minimally replicative HIV-2 live-virus vaccine protects M. nemestrina from disease after HIV-2(287) challenge.

作者信息

Looney D J, McClure J, Kent S J, Radaelli A, Kraus G, Schmidt A, Steffy K, Greenberg P, Hu S L, Morton W R, Wong-Staal F

机构信息

Infectious Diseases, VA San Diego Healthcare System, California 92161, USA.

出版信息

Virology. 1998 Mar 1;242(1):150-60. doi: 10.1006/viro.1997.8992.

Abstract

M. nemestrina immunized with an apathogenic HIV-2 molecular clone (HIV-2KR) were protected from CD4 decline and disease upon challenge with HIV-2(287), after any immunizing virus could be detected. Higher but not lower inocula of HIV-2KR were protective against intravenous inoculation of either 10(5) or 10(1) TCID50 of HIV-2(287). Protected animals displayed substantial reductions in PBMC proviral burden (1-3 logs), viral titers (1-2 logs), and plasma viral RNA (2-4 logs) compared to unprotected or naive animals as early as 1 week postinfection. Plasma viral RNA became undetectable after 24 weeks in protected animals, but remained high in unprotected animals. No viral RNA was present in the spleen of the protected animal necropsied more than a year after challenge (though viral DNA was still present). No neutralizing responses could be demonstrated, but CTL activity was detected sooner and at higher levels after challenge in protected than in unprotected macaques. In this novel HIV-2 vaccine model, protection was clearly dose-dependent, and clearance of challenge virus RNA from the plasma did not require detectable ongoing replication of the immunizing virus at the time of challenge.

摘要

用无致病性的HIV-2分子克隆(HIV-2KR)免疫的猪尾猕猴,在任何免疫病毒都可被检测到之后,用HIV-2(287)攻击时可免受CD4下降和疾病的影响。较高但不是较低剂量的HIV-2KR对静脉注射10(5)或10(1) TCID50的HIV-2(287)具有保护作用。与未受保护或未免疫的动物相比,受保护的动物早在感染后1周,外周血单核细胞前病毒负荷(1-3个对数)、病毒滴度(1-2个对数)和血浆病毒RNA(2-4个对数)就大幅降低。在受保护的动物中,24周后血浆病毒RNA变得无法检测,但在未受保护的动物中仍保持高水平。在攻击后一年多进行尸检的受保护动物的脾脏中没有病毒RNA(尽管病毒DNA仍然存在)。没有检测到中和反应,但在受保护的猕猴中,攻击后比未受保护的猕猴更快且在更高水平检测到CTL活性。在这个新型的HIV-2疫苗模型中,保护作用明显呈剂量依赖性,并且从血浆中清除攻击病毒RNA并不需要在攻击时检测到免疫病毒的持续复制。

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