Rapid and comprehensive diagnostic method for repeat expansion diseases using nanopore sequencing

Author:

Miyatake SatokoORCID,Koshimizu ErikoORCID,Fujita Atsushi,Doi HiroshiORCID,Okubo Masaki,Wada TaishiORCID,Hamanaka Kohei,Ueda Naohisa,Kishida Hitaru,Minase Gaku,Matsuno Atsuhiro,Kodaira Minori,Ogata Katsuhisa,Kato Rumiko,Sugiyama AtsuhikoORCID,Sasaki AyakoORCID,Miyama Takabumi,Satoh Mai,Uchiyama YuriORCID,Tsuchida NaomiORCID,Hamanoue HarukaORCID,Misawa KazuharuORCID,Hayasaka Kiyoshi,Sekijima Yoshiki,Adachi HiroakiORCID,Yoshida KunihiroORCID,Tanaka Fumiaki,Mizuguchi TakeshiORCID,Matsumoto NaomichiORCID

Abstract

AbstractWe developed a diagnostic method for repeat expansion diseases using a long-read sequencer to improve currently available, low throughput diagnostic methods. We employed the real-time target enrichment system of the nanopore GridION sequencer using the adaptive sampling option, in which software-based target assignment is available without prior sample enrichment, and built an analysis pipeline that prioritized the disease-causing loci. Twenty-two patients with various neurological and neuromuscular diseases, including 12 with genetically diagnosed repeat expansion diseases and 10 manifesting cerebellar ataxia, but without genetic diagnosis, were analyzed. We first sequenced the 12 molecularly diagnosed patients and accurately confirmed expanded repeats in all with uniform depth of coverage across the loci. Next, we applied our method and a conventional method to 10 molecularly undiagnosed patients. Our method corrected inaccurate diagnoses of two patients by the conventional method. Our method is superior to conventional diagnostic methods in terms of speed, accuracy, and comprehensiveness.

Funder

Japan Agency for Medical Research and Development

MEXT | Japan Society for the Promotion of Science

Grant for Strategic Research Promotion from Yokohama City University

Publisher

Springer Science and Business Media LLC

Subject

Genetics (clinical),Genetics,Molecular Biology

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