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克氏锥虫序列数据库在通过计算机模拟和体外筛选鉴定潜在疫苗候选物中的应用。

Utility of the Trypanosoma cruzi sequence database for identification of potential vaccine candidates by in silico and in vitro screening.

作者信息

Bhatia Vandanajay, Sinha Mala, Luxon Bruce, Garg Nisha

机构信息

Department of Microbiology and Immunology, University of Texas Medical Branch, 301 University Blvd, Galveston 77555, USA.

出版信息

Infect Immun. 2004 Nov;72(11):6245-54. doi: 10.1128/IAI.72.11.6245-6254.2004.

Abstract

Glycosylphosphatidylinositol (GPI)-anchored proteins are abundantly expressed in the infective and intracellular stages of Trypanosoma cruzi and are recognized as antigenic targets by both the humoral and cellular arms of the immune system. Previously, we demonstrated the efficacy of genes encoding GPI-anchored proteins in eliciting partially protective immunity to T. cruzi infection and disease, suggesting their utility as vaccine candidates. For the identification of additional vaccine targets, in this study we screened the T. cruzi expressed sequence tag (EST) and genomic sequence survey (GSS) databases. By applying a variety of web-based genome-mining tools to the analysis of approximately 2,500 sequences, we identified 348 (37.6%) EST and 260 (17.4%) GSS sequences encoding novel parasite-specific proteins. Of these, 19 sequences exhibited the characteristics of secreted and/or membrane-associated GPI proteins. Eight of the selected sequences were amplified to obtain genes TcG1, TcG2, TcG3, TcG4, TcG5, TcG6, TcG7, and TcG8 (TcG1-TcG8) which are expressed in different developmental stages of the parasite and conserved in the genome of a variety of T. cruzi strains. Flow cytometry confirmed the expression of the antigens encoded by the cloned genes as surface proteins in trypomastigote and/or amastigote stages of T. cruzi. When delivered as a DNA vaccine, genes TcG1-TcG6 elicited a parasite-specific antibody response in mice. Except for TcG5, antisera to genes TcG1-TcG6 exhibited trypanolytic activity against the trypomastigote forms of T. cruzi, a property known to correlate with the immune control of T. cruzi. Taken together, our results validate the applicability of bioinformatics in genome mining, resulting in the identification of T. cruzi membrane-associated proteins that are potential vaccine candidates.

摘要

糖基磷脂酰肌醇(GPI)锚定蛋白在克氏锥虫的感染期和细胞内阶段大量表达,并且被免疫系统的体液免疫和细胞免疫分支识别为抗原靶点。此前,我们证明了编码GPI锚定蛋白的基因在引发对克氏锥虫感染和疾病的部分保护性免疫方面的功效,表明它们作为候选疫苗具有实用性。为了鉴定更多的疫苗靶点,在本研究中我们筛选了克氏锥虫表达序列标签(EST)和基因组序列勘测(GSS)数据库。通过应用各种基于网络的基因组挖掘工具对大约2500个序列进行分析,我们鉴定出348个(37.6%)EST序列和260个(17.4%)GSS序列,它们编码新的寄生虫特异性蛋白。其中,19个序列表现出分泌型和/或膜相关GPI蛋白的特征。选择的8个序列被扩增以获得基因TcG1、TcG2、TcG3、TcG4、TcG5、TcG6、TcG7和TcG8(TcG1-TcG8),这些基因在寄生虫的不同发育阶段表达,并且在多种克氏锥虫菌株的基因组中保守。流式细胞术证实了克隆基因编码的抗原在克氏锥虫的锥鞭毛体和/或无鞭毛体阶段作为表面蛋白表达。当作为DNA疫苗递送时,基因TcG1-TcG6在小鼠中引发了寄生虫特异性抗体反应。除了TcG5之外,针对基因TcG1-TcG6的抗血清对克氏锥虫的锥鞭毛体形式表现出溶锥虫活性,这一特性已知与克氏锥虫的免疫控制相关。综上所述,我们的结果验证了生物信息学在基因组挖掘中的适用性,从而鉴定出了克氏锥虫膜相关蛋白,它们是潜在的候选疫苗。

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