Novel Pathogenic ACAN Variants in Non-syndromic Short Stature Patients

Overview

Journal Clin Chim Acta

Specialty Biochemistry

Date 2017 Apr 12

PMID 28396070

Citations 23

Authors

Xuyun Hu

Baoheng Gui

Jiasun Su

Hongdou Li

Niu Li

Tingting Yu

Qinle Zhang

Yufei Xu

Guoqiang Li

Yulin Chen

Yanrong Qing

Chuan Li

Jingsi Luo

Xin Fan

Yu Ding

Juan Li

Jian Wang

Xiumin Wang

Shaoke Chen

Yiping Shen

Affiliations

Soon will be listed here.

Abstract

Background: Pathogenic variants of ACAN have been reported to cause spondyloepiphyseal dysplasia Kimberley type, spondyloepimetaphyseal dysplasia, familial osteochondritis dissecans and idiopathic short stature with normal to advanced bone age. A recent international cohort study significantly expanded the ACAN mutation spectrum, further delineated the heterogeneous clinical characteristics of ACAN mutation patients. The prevalence of ACAN mutation in short stature patients is yet unknown.

Methods: Here we set to assess the frequency of ACAN variants among a cohort of 218 Chinese children with non-syndromic short stature.

Results: We identified three novel truncating variants at the 5' end of ACAN gene. All these pathogenic variants co-segregate with severe short stature phenotype in families. In addition, none of the probands showed significant advanced bone age. All affected individuals showed no signs of significant dysmorphic features or skeletal abnormities. The prevalence of ACAN defect in this cohort is estimated to be 1.4% (3/218). It is higher among families with parents also affected with severe short stature, up to 7.0% (3/43) if parental height is <2.5 SD or 16.7% (3/18) if parental height is <3.0 SD.

Conclusion: Our data suggest that ACAN mutation is a relative common cause of familial severe short stature.

Citing Articles

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Genotype and phenotype in patients with ACAN gene variants: Three cases and literature review.

Tang W, Wu K, Zhou Q, Tang Y, Fu J, Dong G Mol Genet Genomic Med. 2024; 12(4):e2439.

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Deng S, Hou L, Xia D, Li X, Peng X, Xiao X Front Endocrinol (Lausanne). 2022; 13:1015954.

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