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嗅觉神经元细胞作为一种有前景的工具,可用于实现神经精神疾病药物发现中的“可药用基因组”方法。

Olfactory neuronal cells as a promising tool to realize the "druggable genome" approach for drug discovery in neuropsychiatric disorders.

作者信息

Mihaljevic Marina, Lam Max, Ayala-Grosso Carlos, Davis-Batt Finn, Schretlen David J, Ishizuka Koko, Yang Kun, Sawa Akira

机构信息

Department of Neuroscience, Johns Hopkins University School of Medicine, Baltimore, MD, United States.

IMH Neuropsychiatric Genomics Laboratory, Institute of Mental Health, Singapore, Singapore.

出版信息

Front Neurosci. 2023 Mar 10;16:1081124. doi: 10.3389/fnins.2022.1081124. eCollection 2022.

Abstract

"Druggable genome" is a novel concept that emphasizes the importance of using the information of genome-wide genetic studies for drug discovery and development. Successful precedents of "druggable genome" have recently emerged for some disorders by combining genomic and gene expression profiles with medical and pharmacological knowledge. One of the key premises for the success is the good access to disease-relevant tissues from "living" patients in which we may observe molecular expression changes in association with symptomatic alteration. Thus, given brain biopsies are ethically and practically difficult, the application of the "druggable genome" approach is challenging for neuropsychiatric disorders. Here, to fill this gap, we propose the use of olfactory neuronal cells (ONCs) biopsied and established via nasal biopsy from living subjects. By using candidate genes that were proposed in a study in which genetic information, postmortem brain expression profiles, and pharmacological knowledge were considered for cognition in the general population, we addressed the utility of ONCs in the "druggable genome" approach by using the clinical and cell resources of an established psychosis cohort in our group. Through this pilot effort, we underscored the gene as a possible druggable candidate for early-stage psychosis. The gene expression was associated with verbal memory, but not with other dimensions in cognition, nor psychiatric manifestations (positive and negative symptoms). The association between this candidate molecule and verbal memory was also confirmed at the protein level. By using ONCs from living subjects, we now provide more specific information regarding molecular expression and clinical phenotypes. The use of ONCs also provides the opportunity of validating the relationship not only at the RNA level but also protein level, leading to the potential of functional assays in the future. Taken together, we now provide evidence that supports the utility of ONCs as a tool for the "druggable genome" approach in translational psychiatry.

摘要

“可药物化基因组”是一个新颖的概念,强调利用全基因组遗传研究信息进行药物发现和开发的重要性。最近,通过将基因组和基因表达谱与医学和药理学知识相结合,“可药物化基因组”在某些疾病方面出现了成功的先例。成功的关键前提之一是能够从“活体”患者获取与疾病相关的组织,在这些组织中我们可以观察到与症状改变相关的分子表达变化。因此,鉴于脑活检在伦理和实际操作上都存在困难,“可药物化基因组”方法在神经精神疾病中的应用具有挑战性。在此,为填补这一空白,我们提议使用从活体受试者经鼻活检获取并建立的嗅觉神经元细胞(ONCs)。通过使用在一项针对普通人群认知的研究中提出的候选基因,该研究考虑了遗传信息、死后大脑表达谱和药理学知识,我们利用本团队已建立的精神病队列的临床和细胞资源,探讨了ONCs在“可药物化基因组”方法中的效用。通过这项初步研究,我们强调了该基因作为早期精神病可能的可药物化候选基因。该基因表达与言语记忆相关,但与认知的其他维度或精神症状(阳性和阴性症状)无关。这种候选分子与言语记忆之间的关联在蛋白质水平也得到了证实。通过使用来自活体受试者的ONCs,我们现在提供了关于分子表达和临床表型的更具体信息。ONCs的使用还提供了不仅在RNA水平而且在蛋白质水平验证这种关系的机会,从而为未来的功能测定带来了潜力。综上所述,我们现在提供的证据支持了ONCs作为转化精神病学中“可药物化基因组”方法工具的效用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/73e2/10038100/8082295ec6c9/fnins-16-1081124-g0001.jpg

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