Novel variants associated with Stargardt disease in Chinese patients

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Novel variants associated with Stargardt disease in Chinese patients. / Hu, Fangyuan; Gao, Fengjuan; Li, Jiankang; Xu, Ping; Wang, Dandan; Chen, Fang; Zhang, Shenghai; Wu, Jihong.

I: Gene, Bind 754, 144890, 2020.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Hu, F, Gao, F, Li, J, Xu, P, Wang, D, Chen, F, Zhang, S & Wu, J 2020, 'Novel variants associated with Stargardt disease in Chinese patients', Gene, bind 754, 144890. https://doi.org/10.1016/j.gene.2020.144890

APA

Hu, F., Gao, F., Li, J., Xu, P., Wang, D., Chen, F., Zhang, S., & Wu, J. (2020). Novel variants associated with Stargardt disease in Chinese patients. Gene, 754, [144890]. https://doi.org/10.1016/j.gene.2020.144890

Vancouver

Hu F, Gao F, Li J, Xu P, Wang D, Chen F o.a. Novel variants associated with Stargardt disease in Chinese patients. Gene. 2020;754. 144890. https://doi.org/10.1016/j.gene.2020.144890

Author

Hu, Fangyuan ; Gao, Fengjuan ; Li, Jiankang ; Xu, Ping ; Wang, Dandan ; Chen, Fang ; Zhang, Shenghai ; Wu, Jihong. / Novel variants associated with Stargardt disease in Chinese patients. I: Gene. 2020 ; Bind 754.

Bibtex

@article{d3f0ea87c5c1409597086f83475b7fa2,
title = "Novel variants associated with Stargardt disease in Chinese patients",
abstract = "Purpose: Stargardt disease (STGD) is the most frequent cause of hereditary macular dystrophy in childhood. Variants in the ABCA4, ELOVL4, PROM1, BEST1, and PRPH2 genes have been detected in patients with autosomal recessive or dominant STGD. This study was aimed at identifying the novel disease-associated variants in Chinese patients with STGD. Methods: Ten Chinese families and two sporadic cases with STGD (n = 32) were enrolled in the study. All subjects underwent genetic analysis with next-generation sequencing (NGS), which was based on a specially customized capture panel targeting exons and untranslated regions (UTRs) of 792 genes related to common hereditary ophthalmopathy. Variants were analyzed to assess possible pathogenicity. Results: Fourteen disease-associated variants of ABCA4 were detected in 9 Chinese families with autosomal recessive STGD, including 11 pathogenic variants and 3 likely pathogenic variants. Variant c.4253 + 4C > T in ABCA4 was identified as one de novo variant. Of the 14 distinct variants in ABCA4, 7 novel variants were found. In addition, one known variant of PROM1, c.1117C > T (p.Arg373Cys), was detected in one family and one sporadic case with autosomal dominant STGD, respectively. One novel missense variant of ELOVL4, c.59A > G (p.Asn20Ser), was found in one sporadic case with autosomal dominant STGD. The potential deleterious effects of these novel variants were confirmed through intensive analysis. Conclusion: By panel-based NGS, 8 novel disease-associated variants are identified in two genes responsible for STGD, including ABCA4 and ELOVL4. Our results further extend the mutation spectrum of these two genes in Chinese patients with STGD. One ABCA4 c.4253 + 4C > T variant is identified as a de novo splicing variant.",
keywords = "Chinese patients, Next-generation sequencing, Novel pathogenic variants, STGD",
author = "Fangyuan Hu and Fengjuan Gao and Jiankang Li and Ping Xu and Dandan Wang and Fang Chen and Shenghai Zhang and Jihong Wu",
year = "2020",
doi = "10.1016/j.gene.2020.144890",
language = "English",
volume = "754",
journal = "Gene",
issn = "0378-1119",
publisher = "Elsevier",

}

RIS

TY - JOUR

T1 - Novel variants associated with Stargardt disease in Chinese patients

AU - Hu, Fangyuan

AU - Gao, Fengjuan

AU - Li, Jiankang

AU - Xu, Ping

AU - Wang, Dandan

AU - Chen, Fang

AU - Zhang, Shenghai

AU - Wu, Jihong

PY - 2020

Y1 - 2020

N2 - Purpose: Stargardt disease (STGD) is the most frequent cause of hereditary macular dystrophy in childhood. Variants in the ABCA4, ELOVL4, PROM1, BEST1, and PRPH2 genes have been detected in patients with autosomal recessive or dominant STGD. This study was aimed at identifying the novel disease-associated variants in Chinese patients with STGD. Methods: Ten Chinese families and two sporadic cases with STGD (n = 32) were enrolled in the study. All subjects underwent genetic analysis with next-generation sequencing (NGS), which was based on a specially customized capture panel targeting exons and untranslated regions (UTRs) of 792 genes related to common hereditary ophthalmopathy. Variants were analyzed to assess possible pathogenicity. Results: Fourteen disease-associated variants of ABCA4 were detected in 9 Chinese families with autosomal recessive STGD, including 11 pathogenic variants and 3 likely pathogenic variants. Variant c.4253 + 4C > T in ABCA4 was identified as one de novo variant. Of the 14 distinct variants in ABCA4, 7 novel variants were found. In addition, one known variant of PROM1, c.1117C > T (p.Arg373Cys), was detected in one family and one sporadic case with autosomal dominant STGD, respectively. One novel missense variant of ELOVL4, c.59A > G (p.Asn20Ser), was found in one sporadic case with autosomal dominant STGD. The potential deleterious effects of these novel variants were confirmed through intensive analysis. Conclusion: By panel-based NGS, 8 novel disease-associated variants are identified in two genes responsible for STGD, including ABCA4 and ELOVL4. Our results further extend the mutation spectrum of these two genes in Chinese patients with STGD. One ABCA4 c.4253 + 4C > T variant is identified as a de novo splicing variant.

AB - Purpose: Stargardt disease (STGD) is the most frequent cause of hereditary macular dystrophy in childhood. Variants in the ABCA4, ELOVL4, PROM1, BEST1, and PRPH2 genes have been detected in patients with autosomal recessive or dominant STGD. This study was aimed at identifying the novel disease-associated variants in Chinese patients with STGD. Methods: Ten Chinese families and two sporadic cases with STGD (n = 32) were enrolled in the study. All subjects underwent genetic analysis with next-generation sequencing (NGS), which was based on a specially customized capture panel targeting exons and untranslated regions (UTRs) of 792 genes related to common hereditary ophthalmopathy. Variants were analyzed to assess possible pathogenicity. Results: Fourteen disease-associated variants of ABCA4 were detected in 9 Chinese families with autosomal recessive STGD, including 11 pathogenic variants and 3 likely pathogenic variants. Variant c.4253 + 4C > T in ABCA4 was identified as one de novo variant. Of the 14 distinct variants in ABCA4, 7 novel variants were found. In addition, one known variant of PROM1, c.1117C > T (p.Arg373Cys), was detected in one family and one sporadic case with autosomal dominant STGD, respectively. One novel missense variant of ELOVL4, c.59A > G (p.Asn20Ser), was found in one sporadic case with autosomal dominant STGD. The potential deleterious effects of these novel variants were confirmed through intensive analysis. Conclusion: By panel-based NGS, 8 novel disease-associated variants are identified in two genes responsible for STGD, including ABCA4 and ELOVL4. Our results further extend the mutation spectrum of these two genes in Chinese patients with STGD. One ABCA4 c.4253 + 4C > T variant is identified as a de novo splicing variant.

KW - Chinese patients

KW - Next-generation sequencing

KW - Novel pathogenic variants

KW - STGD

U2 - 10.1016/j.gene.2020.144890

DO - 10.1016/j.gene.2020.144890

M3 - Journal article

C2 - 32534057

AN - SCOPUS:85086662895

VL - 754

JO - Gene

JF - Gene

SN - 0378-1119

M1 - 144890

ER -

ID: 244276905