Two novel mutations in myosin binding protein C slow causing distal arthrogryposis type 2 in two large Han Chinese families may suggest important functional role of immunoglobulin domain C2.

Xuefu Li,Yongping Lu,Wei Liu,Yawen Wang,Ning Zhao,Yu Sui,Bomeng Zhong,Miao Jiang,Weitian Han,Hong Wang,Jianxin Li,Tao Cai

doi:10.1371/journal.pone.0117158

Abstract

Distal arthrogryposes (DAs) are a group of disorders that mainly involve the distal parts of the limbs and at least ten different DAs have been described to date. DAs are mostly described as autosomal dominant disorders with variable expressivity and incomplete penetrance, but recently autosomal recessive pattern was reported in distal arthrogryposis type 5D. Mutations in the contractile genes are found in about 50% of all DA patients. Of these genes, mutations in the gene encoding myosin binding protein C slow MYBPC1 were recently identified in two families with distal arthrogryposis type 1B. Here, we described two large Chinese families with autosomal dominant distal arthrogryposis type 2(DA2) with incomplete penetrance and variable expressivity. Some unique overextension contractures of the lower limbs and some distinctive facial features were present in our DA2 pedigrees. We performed follow-up DNA sequencing after linkage mapping and first identified two novel MYBPC1 mutations (c.1075G>A [p.E359K] and c.956C>T [p.P319L]) responsible for these Chinese DA2 families of which one introduced by germline mosacism. Each mutation was found to cosegregate with the DA2 phenotype in each family but not in population controls. Both substitutions occur within C2 immunoglobulin domain, which together with C1 and the M motif constitute the binding site for the S2 subfragment of myosin. Our results expand the phenotypic spectrum of MYBPC1-related arthrogryposis multiplex congenita (AMC). We also proposed the possible molecular mechanisms that may underlie the pathogenesis of DA2 myopathy associated with these two substitutions in MYBPC1.

Highlights

Distal arthrogryposis(DA) is a group of disorders that mainly involve the distal parts of the limbs and are characterized by congenital contractures of two or more different body areas [1]
Since the Hall’s classification of DA was revised [1,2], at least ten different forms of DA (DA1DA10) have been reported and distal arthrogryposes (DAs) were mostly described as autosomal dominant disorders, but recently autosomal recessive pattern was reported in distal arthrogryposis type 5D(DA5D) [3]
Our work represents the first report on the link between myosin-binding protein C1 (MYBPC1) and the DA2 phenotype, of which one was introduced by germline mosacism

Summary

Introduction

Distal arthrogryposis(DA) is a group of disorders that mainly involve the distal parts of the limbs and are characterized by congenital contractures of two or more different body areas [1]. Since the Hall’s classification of DA was revised [1,2], at least ten different forms of DA (DA1DA10) have been reported and distal arthrogryposes (DAs) were mostly described as autosomal dominant disorders, but recently autosomal recessive pattern was reported in distal arthrogryposis type 5D(DA5D) [3]. In the gene discovery studies, DA1 (MIM 108120), DA2B (Sheldon-Hall syndrome [SHS], MIM 601680) and DA2A (Freeman-Sheldon syndrome [FSS], MIM 193700) were suggested most common DAs. DA1, DA2B/SHS and DA2A/FSS share some major diagnostic criteria. DA1, DA2B/SHS and DA2A/FSS share some major diagnostic criteria They can be distinguished from one another based on diagnostic criteria, which include the absence of facial contractures in most individuals with DA1, the presence of mild to moderate facial contractures in SHS [4] and the presence of moderate to severe facial contractures in FSS. Additional features commonly found in FSS include scoliosis, prominent superciliary ridge, blepharophimosis, potosis, strabismus, dental crowding, hypoplastic alae nasi, a long philtrum, and feeding difficulty at birth [2,5,7]

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Conclusion