Ji Ai-Ling, Zhang Xia, Chen Wei-Wei, Huang Wen-Juan
Department of Neurology, The Third People Hospital of Xuzhou, Xuzhou, China.
Department of Neurology, Xuzhou Central Hospital, Xuzhou, China.
J Med Genet. 2017 Mar;54(3):145-154. doi: 10.1136/jmedgenet-2016-104271. Epub 2017 Jan 13.
Recent genetic discoveries have dramatically changed our understanding of two major neurodegenerative conditions. Amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) are common, devastating diseases of the brain. For decades, ALS and FTD were classified as movement and cognitive disorders, respectively, due to their distinct clinical phenotypes. The recent identification of () as the major gene causative of familial forms of ALS and FTD uncovered a new reality of a continuous FTD/ALS spectrum. The finding that up to 50% of all patients present some degree of ALS FTD phenotypes supports this ALS/FTD continuum. Now >100 genes are known to contribute to ALS/FTD, with a few major contributors that are reviewed below. The low penetrance of mutations, its contribution to sporadic cases, and its combination with other genes support an oligogenic model where two or more genes contribute to disease risk, onset, progression and phenotype: from 'pure' ALS or FTD to combined ALS/FTD. These advances in the genetics of ALS/FTD will soon lead to a better mechanistic understanding of the pathobiology of the disease, which should result in the development of effective therapies in the near future.
最近的遗传学发现极大地改变了我们对两种主要神经退行性疾病的理解。肌萎缩侧索硬化症(ALS)和额颞叶痴呆(FTD)是常见的、毁灭性的脑部疾病。几十年来,由于其不同的临床表型,ALS和FTD分别被归类为运动和认知障碍。最近将()鉴定为家族性ALS和FTD的主要致病基因,揭示了FTD/ALS连续谱的新情况。高达50%的患者表现出某种程度的ALS-FTD表型这一发现支持了这种ALS/FTD连续性。现在已知有超过100个基因与ALS/FTD有关,下面将对一些主要的相关基因进行综述。()突变的低外显率、其对散发性病例的影响以及它与其他基因的组合支持了一种寡基因模型,即两个或更多基因会影响疾病风险、发病、进展和表型:从“纯粹”的ALS或FTD到合并的ALS/FTD。ALS/FTD遗传学的这些进展很快将使我们对该疾病的病理生物学有更好的机制理解,这有望在不久的将来带来有效治疗方法的开发。
