一个小回顾:弥合自闭症谱系障碍和疼痛合并症之间的差距。

IF 2 Q3 CLINICAL NEUROLOGY
Chad O Brown, Jarryll Uy, Karun K Singh
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引用次数: 3

摘要

背景:疼痛是一种复杂的神经生物学反应,有多种原因;然而,自闭症谱系障碍(ASD)患者经常报告慢性疼痛,病因不明。最近的研究旨在确定ASD小鼠和人类模型疼痛的因果机制。近年来,人们努力更好地记录和探索临床观察到的ASD患者的继发表型。随着新的测序研究在ASD内更大的队列中变得更加有力,特定基因及其变体往往没有被表征或验证。在这篇综述中,我们强调了ASD风险基因通常表现为疼痛合并症。目的:这篇小型综述在神经发育障碍和疼痛研究两个领域的文献之间架起了桥梁。我们讨论了ASD的遗传景观及其与疼痛表型的联系的重要性。结果:在与ASD相关的众多基因中,很少有基因与不同程度的疼痛合并症有关。这些基因的突变,如SCN9A、SHANK3和CNTNAP2,导致神经元功能的改变,产生对疼痛的不同反应,在小鼠和人类模型中都有显示。结论:有必要利用新技术来进一步了解ASD风险基因及其对疼痛的影响。其次,有必要将未来与疼痛相关的ASD风险基因与他们自己的队列联系起来,因为需要更好地了解这一亚群。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A mini-review: Bridging the gap between autism spectrum disorder and pain comorbidities.

Background: Pain is a complex neurobiological response with a multitude of causes; however, patients with autism spectrum disorder (ASD) often report chronic pain with no known etiology. Recent research has been aimed toward identifying the causal mechanisms of pain in mouse and human models of ASD. In recent years, efforts have been made to better document and explore secondary phenotypes observed in ASD patients in the clinic. As new sequencing studies have become more powered with larger cohorts within ASD, specific genes and their variants are often left uncharacterized or validated. In this review we highlight ASD risk genes often presented with pain comorbidities.

Aims: This mini-review bridges the gap between two fields of literature, neurodevelopmental disorders and pain research. We discuss the importance of the genetic landscape of ASD and its links to pain phenotypes.

Results: Among the numerous genes implicated in ASD, few have been implicated with varying severities of pain comorbidity. Mutations in these genes, such as SCN9A, SHANK3, and CNTNAP2, lead to altered neuronal function that produce different responses to pain, shown in both mouse and human models.

Conclusion: There is a necessity to use new technologies to advance the current understanding of ASD risk genes and their contributions to pain. Secondly, there is a need to power future ASD risk genes associated with pain with their own cohort, because a better understanding is needed of this subpopulation.

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来源期刊
CiteScore
3.70
自引率
12.50%
发文量
36
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