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构建用于双结构域CD4分子表面表达的人阴道乳酸杆菌菌株。

Engineering of a human vaginal Lactobacillus strain for surface expression of two-domain CD4 molecules.

作者信息

Liu Xiaowen, Lagenaur Laurel A, Lee Peter P, Xu Qiang

机构信息

Osel, Inc., 4008 Burton Drive, Santa Clara, CA 95054, USA.

出版信息

Appl Environ Microbiol. 2008 Aug;74(15):4626-35. doi: 10.1128/AEM.00104-08. Epub 2008 Jun 6.

Abstract

Women are at significant risk of heterosexually transmitted human immunodeficiency virus (HIV) infection, with the mucosal epithelium of the cervix and vagina serving as a major portal of entry. The cervicovaginal mucosa naturally harbors dynamic microflora composed predominantly of lactobacilli, which may be genetically modified to serve as a more efficient protective barrier against the heterosexual transmission of HIV. We selected a vaginal strain of Lactobacillus, L. jensenii 1153, for genetic modification to display surface-anchored anti-HIV proteins. Genomic sequencing analyses revealed that L. jensenii 1153 encodes several unique high-molecular-weight cell wall-anchored proteins with a C-terminal cell wall sorting LPQTG motif. In this report, we employed these proteins to express a surface-anchored two-domain CD4 (2D CD4) molecule in L. jensenii 1153. Our studies indicated that the C-terminal cell wall sorting signal LPQTG motif alone is insufficient to drive the surface expression of heterologous proteins, and the display of surface-anchored 2D CD4 molecules required native sequences of a defined length upstream of the unique C-terminal LPQTG cell wall sorting signal and the positively charged C terminus in a Lactobacillus-based expression system. The modified L. jensenii strain displayed 2D CD4 molecules that were uniformly distributed on bacterial surfaces. The surface-anchored 2D CD4 molecule was recognized by a conformation-dependent anti-CD4 antibody, suggesting that the expressed proteins adopted a native conformation. The establishment of this Lactobacillus-based surface expression system, with potential broad applicability, represents a major step toward developing an inexpensive yet durable approach to topical microbicides for the mitigation of heterosexual transmission of HIV and other mucosally transmitted viral pathogens.

摘要

女性面临着通过异性性行为感染人类免疫缺陷病毒(HIV)的重大风险,宫颈和阴道的黏膜上皮是主要的病毒入侵门户。宫颈阴道黏膜自然存在着以乳酸杆菌为主的动态微生物群,可对其进行基因改造,使其成为预防HIV异性传播的更有效保护屏障。我们选择了一种阴道乳酸杆菌菌株——詹氏乳酸杆菌1153进行基因改造,以展示表面锚定的抗HIV蛋白。基因组测序分析表明,詹氏乳酸杆菌1153编码几种独特的高分子量细胞壁锚定蛋白,其C端具有细胞壁分选LPQTG基序。在本报告中,我们利用这些蛋白在詹氏乳酸杆菌1153中表达表面锚定的双结构域CD4(2D CD4)分子。我们的研究表明,仅C端细胞壁分选信号LPQTG基序不足以驱动异源蛋白的表面表达,在基于乳酸杆菌的表达系统中,表面锚定的2D CD4分子的展示需要在独特的C端LPQTG细胞壁分选信号上游有特定长度的天然序列以及带正电荷的C端。改造后的詹氏乳酸杆菌菌株展示出均匀分布在细菌表面的2D CD4分子。表面锚定的2D CD4分子可被构象依赖性抗CD4抗体识别,这表明表达的蛋白呈现天然构象。这种具有潜在广泛适用性的基于乳酸杆菌的表面表达系统的建立,是朝着开发一种廉价且持久的局部杀菌剂方法迈出的重要一步,该方法可减轻HIV及其他黏膜传播病毒病原体的异性传播。

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