| Literature DB >> 32613234 |
Yuwen Zhao1,2, Lixia Qin1,2, Hongxu Pan1, Zhenhua Liu1,2, Li Jiang1, Yan He1, Qian Zeng1, Xun Zhou1, Xiaoxia Zhou1, Yangjie Zhou1, Zhenghuan Fang3, Zheng Wang4, Yaqin Xiang1, Honglan Yang1, Yige Wang1, Kailin Zhang1, Rui Zhang1, Runcheng He1, Xiaoting Zhou1, Zhou Zhou1, Nannan Yang1, Dongxiao Liang1, Juan Chen1, Xuxiang Zhang1, Yao Zhou1, Hongli Liu1, Penghui Deng1, Kun Xu1, Ke Xu1, Chaojun Zhou1, Junfei Zhong1, Qian Xu1, Qiying Sun4, Bin Li2, Guihu Zhao2, Tao Wang5, Ling Chen6, Huifang Shang7, Weiguo Liu8, Piu Chan9,10, Zheng Xue11, Qing Wang12, Li Guo13, Xuejing Wang14, Changshui Xu15, Zhentao Zhang16, Tao Chen17, Lifang Lei18, Hainan Zhang19, Chunyu Wang19, Jieqiong Tan3, Xinxiang Yan2, Lu Shen1,2, Hong Jiang1,2, Zhuohua Zhang3, Zhengmao Hu3, Kun Xia3, Zhenyu Yue20, Jinchen Li1,2,3,4, Jifeng Guo1,2,3, Beisha Tang1,2,3,4.
Abstract
This study aimed to determine the mutational spectrum of familial Parkinson's disease and sporadic early-onset Parkinson's disease (sEOPD) in a mainland Chinese population and the clinical features of mutation carriers. We performed multiplex ligation-dependent probe amplification assays and whole-exome sequencing for 1676 unrelated patients with Parkinson's disease in a mainland Chinese population, including 192 probands from families with autosomal-recessive Parkinson's disease, 242 probands from families with autosomal-dominant Parkinson's disease, and 1242 sEOPD patients (age at onset ≤ 50). According to standards and guidelines from the American College of Medical Genetics and Genomics, pathogenic/likely pathogenic variants in 23 known Parkinson's disease-associated genes occurred more frequently in the autosomal-recessive Parkinson's disease cohort (65 of 192, 33.85%) than in the autosomal-dominant Parkinson's disease cohort (10 of 242, 4.13%) and the sEOPD cohort (57 of 1242, 4.59%), which leads to an overall molecular diagnostic yield of 7.88% (132 of 1676). We found that PRKN was the most frequently mutated gene (n = 83, 4.95%) and present the first evidence of an SNCA duplication and LRRK2 p.N1437D variant in mainland China. In addition, several novel pathogenic/likely pathogenic variants including LRRK2 (p.V1447M and p.Y1645S), ATP13A2 (p.R735X and p.A819D), FBXO7 (p.G67E), LRP10 (c.322dupC/p.G109Rfs*51) and TMEM230 (c.429delT/p.P144Qfs*2) were identified in our cohort. Furthermore, the age at onset of the 132 probands with genetic diagnoses (median, 31.5 years) was about 14.5 years earlier than that of patients without molecular diagnoses (i.e. non-carriers, median 46.0 years). Specifically, the age at onset of Parkinson's disease patients with pathogenic/likely pathogenic variants in ATP13A2, PLA2G6, PRKN, or PINK1 was significantly lower than that of non-carriers, while the age at onset of carriers with other gene pathogenic/likely pathogenic variants was similar to that of non-carriers. The clinical spectrum of Parkinson's disease-associated gene carriers in this mainland Chinese population was similar to that of other populations. We also detected 61 probands with GBA possibly pathogenic variants (3.64%) and 59 probands with GBA p.L444P (3.52%). These results shed insight into the genetic spectrum and clinical manifestations of Parkinson's disease in mainland China and expand the existing repertoire of pathogenic or likely pathogenic variants involved in known Parkinson's disease-associated genes. Our data highlight the importance of genetic testing in Parkinson's disease patients with age at onset < 40 years, especially in those from families with a recessive inheritance pattern, who may benefit from early diagnosis and treatment.Entities:
Keywords: Parkinson’s disease; age at onset; disease-associated gene; pathogenic or likely pathogenic variant; whole-exome sequencing
Year: 2020 PMID: 32613234 DOI: 10.1093/brain/awaa167
Source DB: PubMed Journal: Brain ISSN: 0006-8950 Impact factor: 13.501