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翻译:翻译 MTOR 和 RAS 相关信号通路在自闭症谱系障碍中的作用:模型、机制和治疗。

Translating the Role of mTOR- and RAS-Associated Signalopathies in Autism Spectrum Disorder: Models, Mechanisms and Treatment.

机构信息

Institute for Microscopic Anatomy and Neurobiology, University Medical Center of the Johannes Gutenberg-University, 55131 Mainz, Germany.

Autism Therapy and Research Center of Excellence, Department of Child and Adolescent Psychiatry, Psychosomatics and Psychotherapy, University Hospital Frankfurt, 60528 Frankfurt am Main, Germany.

出版信息

Genes (Basel). 2021 Oct 30;12(11):1746. doi: 10.3390/genes12111746.

Abstract

Mutations affecting mTOR or RAS signaling underlie defined syndromes (the so-called mTORopathies and RASopathies) with high risk for Autism Spectrum Disorder (ASD). These syndromes show a broad variety of somatic phenotypes including cancers, skin abnormalities, heart disease and facial dysmorphisms. Less well studied are the neuropsychiatric symptoms such as ASD. Here, we assess the relevance of these signalopathies in ASD reviewing genetic, human cell model, rodent studies and clinical trials. We conclude that signalopathies have an increased liability for ASD and that, in particular, ASD individuals with dysmorphic features and intellectual disability (ID) have a higher chance for disruptive mutations in RAS- and mTOR-related genes. Studies on rodent and human cell models confirm aberrant neuronal development as the underlying pathology. Human studies further suggest that multiple hits are necessary to induce the respective phenotypes. Recent clinical trials do only report improvements for comorbid conditions such as epilepsy or cancer but not for behavioral aspects. Animal models show that treatment during early development can rescue behavioral phenotypes. Taken together, we suggest investigating the differential roles of mTOR and RAS signaling in both human and rodent models, and to test drug treatment both during and after neuronal development in the available model systems.

摘要

影响 mTOR 或 RAS 信号的突变是明确综合征(所谓的 mTOR 病和 RAS 病)的基础,这些综合征患自闭症谱系障碍(ASD)的风险很高。这些综合征表现出广泛的躯体表型,包括癌症、皮肤异常、心脏病和面部畸形。研究较少的是神经精神症状,如 ASD。在这里,我们通过评估遗传、人类细胞模型、啮齿动物研究和临床试验来评估这些信号病在 ASD 中的相关性。我们得出结论,信号病与 ASD 的关联性增加,特别是具有畸形特征和智力障碍(ID)的 ASD 个体,在 RAS 和 mTOR 相关基因中发生破坏性突变的可能性更高。关于啮齿动物和人类细胞模型的研究证实了异常的神经元发育是潜在的病理学。人类研究进一步表明,需要多次打击才能诱导相应的表型。最近的临床试验仅报告了对合并症(如癫痫或癌症)的改善,但对行为方面没有改善。动物模型表明,在早期发育期间进行治疗可以挽救行为表型。总之,我们建议在人类和啮齿动物模型中研究 mTOR 和 RAS 信号的差异作用,并在现有模型系统中测试在神经元发育期间和之后进行药物治疗。

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