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首页> 外文期刊>Expert opinion on therapeutic targets >New therapeutic targets in immune disorders: ItpkB, Orai1 and UNC93B.
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New therapeutic targets in immune disorders: ItpkB, Orai1 and UNC93B.

机译:免疫疾病的新治疗靶标:ItpkB,Orai1和UNC93B。

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摘要

BACKGROUND: Sequencing of the murine and human genomes has enabled large-scale functional genomics approaches to target identification. This holds the promise of drastically accelerating target discovery. Moreover, by providing an initial validation coincident with target identification, cell based cDNA or small interfering RNA (siRNA) screens and in particular genome-wide in vivo approaches, including forward or reverse genetics and analyses of natural gene polymorphisms, can move the relatively late step of target validation to the beginning of the process, reducing the risk of pursuing targets with little in vivo relevance. OBJECTIVE: We critically discuss the value of combining functional genomics with traditional approaches for accelerating target identification and validation. METHODS: We evaluate the potentials of inositol (1,4,5)trisphosphate 3-kinase B (ItpkB), Orai1 and UNC93B, three particularly interesting proteins that were recently identified through functional genomics, as targets in immune disorders. RESULTS/CONCLUSION: Combining functional genomics with traditional approaches can accelerate target discovery and validation, but requires a follow-up platform that integrates and analyzes all relevant data for assessment of the clinical potential of the growing number of novel targets.
机译:背景:鼠类和人类基因组的测序已使大规模的功能基因组学方法能够进行靶标鉴定。这有望大大加快目标发现的速度。此外,通过提供与靶标识别相吻合的初始验证,基于细胞的cDNA或小分子干扰RNA(siRNA)筛选,尤其是全基因组体内方法,包括正向或反向遗传学和天然基因多态性分析,可以相对较晚地发展。目标验证的第一步,直至过程的开始,从而降低了在体内相关性很小的情况下追求目标的风险。目的:我们批判性地讨论了将功能基因组学与传统方法相结合以加速目标识别和验证的价值。方法:我们评估了肌醇(1,4,5)三磷酸3激酶B(ItpkB),Orai1和UNC93B的潜力,这是最近通过功能基因组学鉴定的三种特别有趣的蛋白质,它们是免疫疾病的靶标。结果/结论:将功能基因组学与传统方法相结合可以加快靶标的发现和验证,但是需要一个后续平台,该平台可以整合和分析所有相关数据,以评估越来越多的新型靶标的临床潜力。

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