RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy

Kohei Hamanaka; Satoko Miyatake; Eriko Koshimizu; Yoshinori Tsurusaki; Satomi Mitsuhashi; Kazuhiro Iwama; Ahmed N. Alkanaq; Atsushi Fujita; Eri Imagawa; Yuri Uchiyama; Nozomu Tawara; Yukio Ando; Yohei Misumi; Mariko Okubo; Mitsuko Nakashima; Takeshi Mizuguchi; Atsushi Takata; Noriko Miyake; Hirotomo Saitsu; Aritoshi Iida; Ichizo Nishino; Naomichi Matsumoto

doi:10.1038/s41436-018-0360-6

RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy

Kohei Hamanaka
, Satoko Miyatake
, Eriko Koshimizu
, Yoshinori Tsurusaki
, Satomi Mitsuhashi
, Kazuhiro Iwama
, Ahmed N. Alkanaq
, Atsushi Fujita
, Eri Imagawa
, Yuri Uchiyama
, Nozomu Tawara
, Yukio Ando
, Yohei Misumi
, Mariko Okubo
, Mitsuko Nakashima
, Takeshi Mizuguchi
, Atsushi Takata
, Noriko Miyake
, Hirotomo Saitsu
, Aritoshi Iida

Ichizo Nishino, Naomichi Matsumoto

Research output: Contribution to journal › Article › peer-review

30 Scopus citations

Abstract

Purpose: The diagnostic rate for Mendelian diseases by exome sequencing (ES) is typically 20–40%. The low rate is partly because ES misses deep-intronic or synonymous variants leading to aberrant splicing. In this study, we aimed to apply RNA sequencing (RNA-seq) to efficiently detect the aberrant splicings and their related variants. Methods: Aberrant splicing in biopsied muscles from six nemaline myopathy (NM) cases unresolved by ES were analyzed with RNA-seq. Variants related to detected aberrant splicing events were analyzed with Sanger sequencing. Detected variants were screened in NM patients unresolved by ES. Results: We identified a novel deep-intronic NEB pathogenic variant, c.1569+339A>G in one case, and another novel synonymous NEB pathogenic variant, c.24684G>C (p.Ser8228Ser) in three cases. The c.24684G>C variant was observed to be the most frequent among all NEB pathogenic variants in normal Japanese populations with a frequency of 1 in 178 (20 alleles in 3552 individuals), but was previously unrecognized. Expanded screening of the variant identified it in a further four previously unsolved nemaline myopathy cases. Conclusion: These results indicated that RNA-seq may be able to solve a large proportion of previously undiagnosed muscle diseases.

Original language	English
Pages (from-to)	1629-1638
Number of pages	10
Journal	Genetics in Medicine
Volume	21
Issue number	7
DOIs	https://doi.org/10.1038/s41436-018-0360-6
State	Published - 1 Jul 2019
Externally published	Yes

Keywords

NEB
RNA sequencing
deep intron
exome sequencing
nemaline myopathy

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10.1038/s41436-018-0360-6

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Hamanaka, K., Miyatake, S., Koshimizu, E., Tsurusaki, Y., Mitsuhashi, S., Iwama, K., Alkanaq, A. N., Fujita, A., Imagawa, E., Uchiyama, Y., Tawara, N., Ando, Y., Misumi, Y., Okubo, M., Nakashima, M., Mizuguchi, T., Takata, A., Miyake, N., Saitsu, H., ... Matsumoto, N. (2019). RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy. Genetics in Medicine, 21(7), 1629-1638. https://doi.org/10.1038/s41436-018-0360-6

@article{3606eeabac0e4defbcbe494554c0b5d6,

title = "RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy",

abstract = "Purpose: The diagnostic rate for Mendelian diseases by exome sequencing (ES) is typically 20–40\%. The low rate is partly because ES misses deep-intronic or synonymous variants leading to aberrant splicing. In this study, we aimed to apply RNA sequencing (RNA-seq) to efficiently detect the aberrant splicings and their related variants. Methods: Aberrant splicing in biopsied muscles from six nemaline myopathy (NM) cases unresolved by ES were analyzed with RNA-seq. Variants related to detected aberrant splicing events were analyzed with Sanger sequencing. Detected variants were screened in NM patients unresolved by ES. Results: We identified a novel deep-intronic NEB pathogenic variant, c.1569+339A>G in one case, and another novel synonymous NEB pathogenic variant, c.24684G>C (p.Ser8228Ser) in three cases. The c.24684G>C variant was observed to be the most frequent among all NEB pathogenic variants in normal Japanese populations with a frequency of 1 in 178 (20 alleles in 3552 individuals), but was previously unrecognized. Expanded screening of the variant identified it in a further four previously unsolved nemaline myopathy cases. Conclusion: These results indicated that RNA-seq may be able to solve a large proportion of previously undiagnosed muscle diseases.",

keywords = "NEB, RNA sequencing, deep intron, exome sequencing, nemaline myopathy",

author = "Kohei Hamanaka and Satoko Miyatake and Eriko Koshimizu and Yoshinori Tsurusaki and Satomi Mitsuhashi and Kazuhiro Iwama and Alkanaq, \{Ahmed N.\} and Atsushi Fujita and Eri Imagawa and Yuri Uchiyama and Nozomu Tawara and Yukio Ando and Yohei Misumi and Mariko Okubo and Mitsuko Nakashima and Takeshi Mizuguchi and Atsushi Takata and Noriko Miyake and Hirotomo Saitsu and Aritoshi Iida and Ichizo Nishino and Naomichi Matsumoto",

note = "Publisher Copyright: {\textcopyright} 2018, American College of Medical Genetics and Genomics.",

year = "2019",

month = jul,

day = "1",

doi = "10.1038/s41436-018-0360-6",

language = "English",

volume = "21",

pages = "1629--1638",

journal = "Genetics in Medicine",

issn = "1098-3600",

publisher = "Elsevier B.V.",

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}

Hamanaka, K, Miyatake, S, Koshimizu, E, Tsurusaki, Y, Mitsuhashi, S, Iwama, K, Alkanaq, AN, Fujita, A, Imagawa, E, Uchiyama, Y, Tawara, N, Ando, Y, Misumi, Y, Okubo, M, Nakashima, M, Mizuguchi, T, Takata, A, Miyake, N, Saitsu, H, Iida, A, Nishino, I & Matsumoto, N 2019, 'RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy', Genetics in Medicine, vol. 21, no. 7, pp. 1629-1638. https://doi.org/10.1038/s41436-018-0360-6

TY - JOUR

T1 - RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy

AU - Hamanaka, Kohei

AU - Miyatake, Satoko

AU - Koshimizu, Eriko

AU - Tsurusaki, Yoshinori

AU - Mitsuhashi, Satomi

AU - Iwama, Kazuhiro

AU - Alkanaq, Ahmed N.

AU - Fujita, Atsushi

AU - Imagawa, Eri

AU - Uchiyama, Yuri

AU - Tawara, Nozomu

AU - Ando, Yukio

AU - Misumi, Yohei

AU - Okubo, Mariko

AU - Nakashima, Mitsuko

AU - Mizuguchi, Takeshi

AU - Takata, Atsushi

AU - Miyake, Noriko

AU - Saitsu, Hirotomo

AU - Iida, Aritoshi

AU - Nishino, Ichizo

AU - Matsumoto, Naomichi

PY - 2019/7/1

Y1 - 2019/7/1

N2 - Purpose: The diagnostic rate for Mendelian diseases by exome sequencing (ES) is typically 20–40%. The low rate is partly because ES misses deep-intronic or synonymous variants leading to aberrant splicing. In this study, we aimed to apply RNA sequencing (RNA-seq) to efficiently detect the aberrant splicings and their related variants. Methods: Aberrant splicing in biopsied muscles from six nemaline myopathy (NM) cases unresolved by ES were analyzed with RNA-seq. Variants related to detected aberrant splicing events were analyzed with Sanger sequencing. Detected variants were screened in NM patients unresolved by ES. Results: We identified a novel deep-intronic NEB pathogenic variant, c.1569+339A>G in one case, and another novel synonymous NEB pathogenic variant, c.24684G>C (p.Ser8228Ser) in three cases. The c.24684G>C variant was observed to be the most frequent among all NEB pathogenic variants in normal Japanese populations with a frequency of 1 in 178 (20 alleles in 3552 individuals), but was previously unrecognized. Expanded screening of the variant identified it in a further four previously unsolved nemaline myopathy cases. Conclusion: These results indicated that RNA-seq may be able to solve a large proportion of previously undiagnosed muscle diseases.

AB - Purpose: The diagnostic rate for Mendelian diseases by exome sequencing (ES) is typically 20–40%. The low rate is partly because ES misses deep-intronic or synonymous variants leading to aberrant splicing. In this study, we aimed to apply RNA sequencing (RNA-seq) to efficiently detect the aberrant splicings and their related variants. Methods: Aberrant splicing in biopsied muscles from six nemaline myopathy (NM) cases unresolved by ES were analyzed with RNA-seq. Variants related to detected aberrant splicing events were analyzed with Sanger sequencing. Detected variants were screened in NM patients unresolved by ES. Results: We identified a novel deep-intronic NEB pathogenic variant, c.1569+339A>G in one case, and another novel synonymous NEB pathogenic variant, c.24684G>C (p.Ser8228Ser) in three cases. The c.24684G>C variant was observed to be the most frequent among all NEB pathogenic variants in normal Japanese populations with a frequency of 1 in 178 (20 alleles in 3552 individuals), but was previously unrecognized. Expanded screening of the variant identified it in a further four previously unsolved nemaline myopathy cases. Conclusion: These results indicated that RNA-seq may be able to solve a large proportion of previously undiagnosed muscle diseases.

KW - NEB

KW - RNA sequencing

KW - deep intron

KW - exome sequencing

KW - nemaline myopathy

UR - https://www.scopus.com/pages/publications/85057123885

U2 - 10.1038/s41436-018-0360-6

DO - 10.1038/s41436-018-0360-6

M3 - Article

C2 - 30467404

AN - SCOPUS:85057123885

SN - 1098-3600

VL - 21

SP - 1629

EP - 1638

JO - Genetics in Medicine

JF - Genetics in Medicine

IS - 7

ER -

RNA sequencing solved the most common but unrecognized NEB pathogenic variant in Japanese nemaline myopathy

Abstract

Keywords

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