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一种针对人类免疫缺陷病毒阳性人群设计的复制受限重组牛分枝杆菌卡介苗(BCG)疫苗,相较于卡介苗,更安全且更有效。

A Replication-Limited Recombinant Mycobacterium bovis BCG vaccine against tuberculosis designed for human immunodeficiency virus-positive persons is safer and more efficacious than BCG.

作者信息

Tullius Michael V, Harth Günter, Maslesa-Galic Sasa, Dillon Barbara J, Horwitz Marcus A

机构信息

Division of Infectious Diseases, Department of Medicine, School of Medicine, UCLA, Los Angeles, CA 90095-1688, USA.

出版信息

Infect Immun. 2008 Nov;76(11):5200-14. doi: 10.1128/IAI.00434-08. Epub 2008 Aug 25.

Abstract

Tuberculosis is the leading cause of death in AIDS patients, yet the current tuberculosis vaccine, Mycobacterium bovis bacillus Calmette-Guérin (BCG), is contraindicated for immunocompromised individuals, including human immunodeficiency virus-positive persons, because it can cause disseminated disease; moreover, its efficacy is suboptimal. To address these problems, we have engineered BCG mutants that grow normally in vitro in the presence of a supplement, are preloadable with supplement to allow limited growth in vivo, and express the highly immunoprotective Mycobacterium tuberculosis 30-kDa major secretory protein. The limited replication in vivo renders these vaccines safer than BCG in SCID mice yet is sufficient to induce potent cell-mediated and protective immunity in the outbred guinea pig model of pulmonary tuberculosis. In the case of one vaccine, rBCG(mbtB)30, protection was superior to that with BCG (0.3-log fewer CFU of M. tuberculosis in the lung [P < 0.04] and 0.6-log fewer CFU in the spleen [P = 0.001] in aerosol-challenged animals [means for three experiments]); hence, rBCG(mbtB)30 is the first live mycobacterial vaccine that is both more attenuated than BCG in the SCID mouse and more potent than BCG in the guinea pig. Our study demonstrates the feasibility of developing safer and more potent vaccines against tuberculosis. The novel approach of engineering a replication-limited vaccine expressing a recombinant immunoprotective antigen and preloading it with a required nutrient, such as iron, that is capable of being stored should be generally applicable to other live vaccine vectors targeting intracellular pathogens.

摘要

结核病是艾滋病患者的主要死因,然而目前的结核病疫苗——卡介苗(BCG),对包括人类免疫缺陷病毒阳性者在内的免疫功能低下个体是禁忌的,因为它可导致播散性疾病;此外,其效力也不理想。为解决这些问题,我们构建了卡介苗突变体,它们在添加物存在的情况下能在体外正常生长,可预先加载添加物以允许在体内有限生长,并表达高度免疫保护性的结核分枝杆菌30 kDa主要分泌蛋白。在体内的有限复制使这些疫苗在严重联合免疫缺陷(SCID)小鼠中比卡介苗更安全,但足以在远交系豚鼠肺结核模型中诱导强大的细胞介导免疫和保护性免疫。对于一种疫苗rBCG(mbtB)30,其保护效果优于卡介苗(在气溶胶攻击的动物中,肺部结核分枝杆菌的菌落形成单位(CFU)少0.3个对数[P < 0.04],脾脏中少0.6个对数[P = 0.001] [三次实验的平均值]);因此,rBCG(mbtB)30是第一种在SCID小鼠中比卡介苗更减毒且在豚鼠中比卡介苗更有效的活分枝杆菌疫苗。我们的研究证明了开发更安全、更有效的抗结核疫苗的可行性。构建一种表达重组免疫保护性抗原并预先加载一种能够储存的必需营养素(如铁)的复制受限疫苗的新方法,应该普遍适用于其他针对细胞内病原体的活疫苗载体。

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