Genetics of Response to ECT, TMS, Ketamine and Esketamine.

Clio E Franklin, Murat Altinay, Kala Bailey, Mahendra T Bhati, Brent R Carr, Susan K Conroy, Khurshid Khurshid, William M McDonald, Brian J Mickey, James W Murrough, Sean M Nestor, Thomas Nickl-Jockschat, Irving M Reti, Gerard Sanacora, Nicholas T Trapp, Biju Viswanath, Jesse H Wright, Peter P Zandi, James B Potash
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Abstract

Treatment-resistant mood disorders are often managed with intensive interventions that include electroconvulsive therapy (ECT), transcranial magnetic stimulation (TMS), ketamine, and esketamine, but the role of genetics in clinical response to those interventions is yet to be clearly determined. Here, we review the current literature on the genetics of response to these treatment modalities. To date, the limited number of studies done to investigate genetic predictors of treatment response have primarily focused on single variants in candidate genes, and none of these have been consistently reproducible. The majority of candidate gene studies examine the effect of variants in the COMT and BDNF genes on treatment response. There are a limited number of genome-wide association studies (GWAS) looking at treatment response, though they are almost all underpowered, with only one study including a sample size > 1000. As a result, there have been few single nucleotide polymorphisms (SNPs) found to be associated with treatment response at a statistically significant level, all in genes other than COMT and BDNF. The challenge is now to generate data from a large group of patients undergoing these therapies in order to more robustly assess the genetic factors affecting treatment response. This will not only help establish genetic predictors of response, but also potentially develop differential predictors of response to available treatments, which could provide clinicians with critical information to aid in deciding which treatment modality to recommend for treatment-resistant depression. We are currently pursuing such a strategy in our 50-site worldwide Gen-ECT-ic consortium.

对电痉挛、经颅磁刺激、氯胺酮和艾氯胺酮反应的遗传学研究。
难治性情绪障碍通常采用强化干预措施进行治疗,包括电痉挛治疗(ECT)、经颅磁刺激(TMS)、氯胺酮和艾氯胺酮,但遗传学在这些干预措施的临床反应中的作用尚未明确确定。在这里,我们回顾了目前的文献对这些治疗方式的反应遗传学。迄今为止,研究治疗反应的遗传预测因子的研究数量有限,主要集中在候选基因的单一变异上,而且这些研究都没有一致的可重复性。大多数候选基因研究检查了COMT和BDNF基因变异对治疗反应的影响。研究治疗反应的全基因组关联研究(GWAS)数量有限,尽管它们几乎都不够有力,只有一项研究的样本量为1000人。因此,除了COMT和BDNF基因外,很少有单核苷酸多态性(SNPs)被发现与治疗反应有统计学意义上的相关性。现在的挑战是从接受这些治疗的一大组患者中产生数据,以便更可靠地评估影响治疗反应的遗传因素。这不仅有助于建立反应的遗传预测因子,而且还可能开发对现有治疗反应的差异预测因子,这可以为临床医生提供关键信息,帮助他们决定推荐哪种治疗方式来治疗难治性抑郁症。目前,我们正在全球50个基地的Gen-ECT-ic联盟中推行这一战略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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