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Proteomics for blood biomarker exploration of severe mental illness: pitfalls of the past and potential for the future

机译:蛋白质组学用于探索严重精神疾病的血液生物标志物:过去的陷阱和未来的潜力

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Recent improvements in high-throughput proteomic approaches are likely to constitute an essential advance in biomarker discovery, holding promise for improved personalized care and drug development. These methodologies have been applied to study multivariate protein patterns and provide valuable data of peripheral tissues. To highlight findings of the last decade for three of the most common psychiatric disorders, namely schizophrenia (SZ), bipolar disorder (BD), and major depressive disorder (MDD), we queried PubMed. Here we delve into the findings from thirty studies, which used proteomics and multiplex immunoassay approaches for peripheral blood biomarker exploration. In an explorative approach, we ran enrichment analyses in peripheral blood according to these results and ascertained the overlap between proteomic findings and genetic loci identified in genome-wide association studies (GWAS). The studies we appraised demonstrate that proteomics for psychiatric research has been heterogeneous in aims and methods and limited by insufficient sample sizes, poorly defined case definitions, methodological inhomogeneity, and confounding results constraining the conclusions that can be extracted from them. Here, we discuss possibilities for overcoming methodological challenges for the implementation of proteomic signatures in psychiatric diagnosis and offer an outlook for future investigations. To fulfill the promise of proteomics in mental disease diagnostics, future research will need large, well-defined cohorts in combination with state-of-the-art technologies.
机译:高通量蛋白质组学方法的最新改进可能会构成生物标志物发现方面的重要进步,有望改善个性化护理和药物开发。这些方法已被用于研究多元蛋白质模式并提供周围组织的有价值的数据。为了强调过去十年中三种最常见的精神疾病(即精神分裂症(SZ),躁郁症(BD)和重度抑郁症(MDD))的发现,我们询问了PubMed。在这里,我们深入研究了三十项研究的发现,这些研究使用蛋白质组学和多重免疫测定方法进行外周血生物标记物探索。在探索性方法中,我们根据这些结果在外周血中进行了富集分析,并确定了蛋白质组学发现与全基因组关联研究(GWAS)中确定的遗传基因座之间的重叠。我们评估的研究表明,用于精神病学研究的蛋白质组学在目标和方法上是异质的,并且受到样本量不足,定义不清的病例定义,方法学不均一性以及混杂的结果的限制,这些结论限制了可以从中提取的结论。在这里,我们讨论了在精神病学诊断中克服蛋白质组学签名的方法挑战的可能性,并为将来的研究提供了前景。为了实现蛋白质组学在精神疾病诊断中的应用前景,未来的研究将需要大型,定义明确的研究对象,并结合最新技术。

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