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In Silico Structural and Functional Annotation of Nine Essential Hypothetical Proteins from Streptococcus pneumoniae

机译:在Silico结构和功能注释九种基本假设蛋白的肺炎链球菌

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The ability of Streptococcus pneumoniae to induce infections relies on its virulence factor machinery. A previous CRISPR interference (CRISPRi) study had identified 254 essential proteins that may be responsible for the pathogenicity of S. pneumoniae serotype 2 strain D39. However, 39 of them were functionally and structurally uncharacterized. Hence, by using in silico approach, this study aimed to annotate the function and structure of these un-annotated proteins. Initially, all 39 proteins went through primary screening for template availability and pathogenicity. From there, 11 of them were selected and underwent further physicochemical, functional, and structural categorization through an integrated bioinformatics approach by means of amino acid sequence- and structure-based analyses. The obtained data revealed that 9 targeted proteins showed a high possibility to be involved in either cell viability or cell pathogenicity mechanism of the bacterium, with SPD_1333 and SPD_1743 being the two most promising proteins to be further studied. Findings from this study can help in facilitating a better understanding of pathogenic ability of this microorganism and enhance drug development and target identification processes in the aim of improving pneumococcal disease control.
机译:肺炎链球菌诱导感染的能力依赖于其毒力因子机械。先前的CRISPR干扰(CRISPRI)研究已经确定了254项必需蛋白质,可能对S.肺炎血管型2菌株D39的致病性负责。然而,其中39个在功能上和结构上无表明。因此,通过使用Silico方法,该研究旨在注释这些未注释的蛋白质的功能和结构。最初,所有39种蛋白质都经过初级筛查进行模板可用性和致病性。从那里,通过氨基酸序列和结构的分析,通过集成的生物信息化方法选择11种它们,并经历了进一步的物理化学,功能和结构分类。所获得的数据显示,9个靶向蛋白质显示出涉及细胞活力或细胞病原性机制的高可能与SPD_1333和SPD_1743是进一步研究的两个最有前途的蛋白质。本研究的调查结果可以帮助促进这种微生物的致病能力,并提高药物开发和目标鉴定过程,以改善肺炎球菌疾病控制。

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