Deletion of 2 amino acids in IHH in a Japanese family with brachydactyly type A1

Nozomu Ozaki; Hiroko Okuda; Hatasu Kobayashi; Kouji H. Harada; Sumiko Inoue; Shohab Youssefian; Akio Koizumi

doi:10.1186/s12920-021-01042-6

BMC Medical Genomics (Jul 2021)

Deletion of 2 amino acids in IHH in a Japanese family with brachydactyly type A1

Nozomu Ozaki,
Hiroko Okuda,
Hatasu Kobayashi,
Kouji H. Harada,
Sumiko Inoue,
Shohab Youssefian,
Akio Koizumi

Affiliations

Nozomu Ozaki: Department of Pediatrics, Kadono-Sanjo Children’s Clinic
Hiroko Okuda: Department of Pain Pharmacogenetics, Kyoto University Graduate School of Medicine
Hatasu Kobayashi: Environmental and Molecular Medicine, Mie University Graduate School of Medicine
Kouji H. Harada: Department of Health and Environmental Sciences, Kyoto University Graduate School of Medicine
Sumiko Inoue: Department of Pain Pharmacogenetics, Kyoto University Graduate School of Medicine
Shohab Youssefian: Department of Pain Pharmacogenetics, Kyoto University Graduate School of Medicine
Akio Koizumi: Department of Pain Pharmacogenetics, Kyoto University Graduate School of Medicine

DOI: https://doi.org/10.1186/s12920-021-01042-6
Journal volume & issue: Vol. 14, no. 1
pp. 1 – 8

Abstract

Read online

Abstract Background Brachydactyly type A1 (BDA1) is an autosomal dominant disorder characterized by uniform shortening of the middle phalanges in all digits. It is associated with variants in the Indian Hedgehog (IHH) gene, which plays a key role in endochondral ossification. To date, heterozygous pathogenic IHH variants involving several codons, which are restricted to a specific region of the N-terminal active fragment of IHH, have been reported. The purpose of this study was to identify the pathogenic variant in a Japanese family with BDA1 and to evaluate its pathogenesis with regard to previous reports. Methods The proband, a 9-year-old boy, his siblings, and his father had shortened digits and a short stature of variable severity. Based on physical examinations, radiographic findings and family history, they were diagnosed with BDA1. This family is the first case of an isolated malformation in Japan. Sanger sequencing of IHH was performed on these individuals and on the proband’s unaffected mother. The significance of the variants was assessed using three-dimensional analysis methods. Results Sanger sequencing showed a novel IHH heterozygous variant, NM_002181.4:c.544_549delTCAAAG(p.Ser182Lys183del) [NC_000002.12:g.219057461_219057466del].. These two residues are located outside the cluster region considered a hotspot of pathogenic variants. Three-dimensional modelling showed that S182 and K183 are located on the same surface as other residues associated with BDA1. Analysis of residue interactions across the interface between IHH and its interacting receptor protein revealed the presence of hydrogen bonds between them. Conclusions We report a novel variant, NM_002181.4:c.544_549delTCAAAG (p.Ser182Lys183del) [NC_000002.12:g.219057461_219057466del] in a Japanese family with BDA1. Indeed, neither variations in codons 182 or 183 nor with such two-amino-acid deletions in IHH have been reported previously. Although these two residues are located outside the cluster region considered a hotspot of pathogenic variants, we speculate that this variant causes BDA1 through impaired interactions between IHH and target receptor proteins in the same manner as other pathogenic variants located in the cluster region. This report expands the genetic spectrum of BDA1.

Published in BMC Medical Genomics

ISSN: 1755-8794 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine; Science: Biology (General): Genetics
Website: https://bmcmedgenomics.biomedcentral.com

About the journal

Abstract

Keywords