识别和治疗自闭症谱系障碍的病理生理合并症以达到最佳结果。

IF 1.7 Q2 PEDIATRICS
Clinical Medicine Insights-Pediatrics Pub Date : 2016-06-15 eCollection Date: 2016-01-01 DOI:10.4137/CMPed.S38337
Richard E Frye, Daniel A Rossignol
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引用次数: 79

摘要

尽管自闭症谱系障碍(ASD)的患病率持续上升,但没有有效的医学治疗方法成为标准的护理方法。在本文中,我们回顾了一些与ASD相关的病理生理异常及其潜在的相关治疗。总体而言,有证据表明,一些自闭症儿童受到癫痫发作和癫痫、神经递质功能障碍、睡眠障碍、代谢异常(包括叶酸、钴胺素、四氢生物蝶呤、肉碱、氧化还原和线粒体代谢异常)以及免疫和胃肠道疾病的影响。虽然有证据表明这些病理生理异常与ASD之间存在关联,但在许多情况下,与ASD病因及其相关症状的确切关系仍有待进一步确定。尽管存在这些局限性,针对某些病理生理异常的治疗方法已经在一些病例中进行了高质量的研究,而针对其他病理生理异常的治疗方法在许多病例中还没有得到很好的研究。有一些针对ASD的更有前景的治疗领域包括神经递质异常,特别是谷氨酸和乙酰胆碱失衡,睡眠障碍(使用行为治疗和褪黑激素),叶酸、钴胺素、四氢生物蝶呤、肉碱和氧化还原途径的代谢异常。有一些证据表明治疗癫痫和癫痫发作、线粒体和免疫疾病以及胃肠道异常,特别是肠道微生物群失衡,但需要在这些领域进行进一步的临床研究,以更好地确定针对自闭症儿童的治疗方法。显然,ASD研究有一些有前景的领域,可能会导致新的治疗方法,并在未来成为标准的治疗方法,但需要更多的研究来更好地定义受特定病理生理异常影响的ASD儿童亚群,以及针对这些异常的最佳治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Identification and Treatment of Pathophysiological Comorbidities of Autism Spectrum Disorder to Achieve Optimal Outcomes.

Despite the fact that the prevalence of autism spectrum disorder (ASD) continues to rise, no effective medical treatments have become standard of care. In this paper we review some of the pathophysiological abnormalities associated with ASD and their potential associated treatments. Overall, there is evidence for some children with ASD being affected by seizure and epilepsy, neurotransmitter dysfunction, sleep disorders, metabolic abnormalities, including abnormalities in folate, cobalamin, tetrahydrobiopterin, carnitine, redox and mitochondrial metabolism, and immune and gastrointestinal disorders. Although evidence for an association between these pathophysiological abnormalities and ASD exists, the exact relationship to the etiology of ASD and its associated symptoms remains to be further defined in many cases. Despite these limitations, treatments targeting some of these pathophysiological abnormalities have been studied in some cases with high-quality studies, whereas treatments for other pathophysiological abnormalities have not been well studied in many cases. There are some areas of more promising treatments specific for ASD including neurotransmitter abnormalities, particularly imbalances in glutamate and acetylcholine, sleep onset disorder (with behavioral therapy and melatonin), and metabolic abnormalities in folate, cobalamin, tetrahydrobiopterin, carnitine, and redox pathways. There is some evidence for treatments of epilepsy and seizures, mitochondrial and immune disorders, and gastrointestinal abnormalities, particularly imbalances in the enteric microbiome, but further clinical studies are needed in these areas to better define treatments specific to children with ASD. Clearly, there are some promising areas of ASD research that could lead to novel treatments that could become standard of care in the future, but more research is needed to better define subgroups of children with ASD who are affected by specific pathophysiological abnormalities and the optimal treatments for these abnormalities.

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