Genetic factors are considered to play a critical role in patients with early-onset Parkinson’s disease (EOPD). The genetic spectrum of EOPD patients has been extensively investigated in Caucasian populations but rarely in the Chinese population. In this study, a total of 21 unrelated Chinese EOPD patients were enrolled. Multiplex ligation-dependent probe amplification assay and whole-exome sequencing were performed, followed by Sanger sequencing. Detailed clinical features were presented. Two novel likely pathogenic variants (p.Q648X in ATP13A2 and p.N521fs in PINK1) and 10 previously reported Parkin pathogenic variations (exon 2 deletion, exon 3–4 deletion, exon 4 deletion, exon 6–7 deletion, exon 7 deletion; p.G284R, p.G329 V, p.R366W, p.N428fs, p.M458 L) were identified in 9 out of 21 (42.86%) patients. The frequency (33.33%) of Parkin variations is much higher in our cohort than that in the East Asian population. The patient carrying the ATP13A2 variant showed no response to levodopa treatment. Our findings broaden the genetic spectrum and clinical features of EOPD patients.
Hee Gyung Kang, Hyun Kyung Lee, Yo Han Ahn, Je‐Gun Joung, Jae‐Yong Nam, Nayoung K. D. Kim, Jung Min Ko, Min Hyun Cho, Jae Il Shin, Joon Kim, Hye Won Park, Young Seo Park, Il Soo Ha, Woo Yeong Chung, Dae‐Yeol Lee, Su Young Kim, Woong‐Yang Park, Hae Il Cheong
Mario Lucariello, Enrique Vidal, Silvia M. Vidal, Mauricio A. Sáez, Laura M. Roa, Dori Huertas, Mercè Pineda, Esther Dalfó, Joaquı́n Dopazo, Paola Jurado, Judith Armstrong, Manel Esteller
Luca A. Lotta, Giacomo Tuana, Jin Yu, Ida Martinelli, Mark L. Wang, Fuli Yu, Serena M. Passamonti, Emanuela Pappalardo, Walker Hale, Donna M. Muzny, Frits R. Rosendaal, Richard A. Gibbs, Flora Peyvandi
Nienke van Engelen, Ronald R. de Krijger, Michelle M Kleisman, Lennart Kester, Saskia Hopman, Mariëtte E.G. Kranendonk, Marijn A. Vermeulen, Carli Tops, Seok‐Young Kim, Hans Clevers, Kornelia Neveling, Roland P. Kuiper, Marjolijn C.J. Jongmans
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