Publication Type : Journal Article
Publisher : American Journal of Medical Genetics, Part A
Source : American Journal of Medical Genetics, Part A, Volume 158 A, Number 11, p.2820-2828 (2012)
Keywords : adolescent, adult, amino acid sequence, Arthropathy, article, Base Sequence, bone dysplasia, CCN Intercellular Signaling Proteins, child, clinical article, clinical feature, consanguinity, European Continental Ancestry Group, family, female, gene, gene mutation, Gene Order, gene sequence, heterozygosity, homozygosity, human, Humans, India, Indian, infant, joint contracture, joint swelling, male, middle aged, missense mutation, Molecular Sequence Data, Mutation, mutational analysis, Neurogenic, Pedigree, Preschool, preschool child, priority journal, progressive pseudorheumatoid dysplasia, school child, Sequence Alignment, WISP3 gene, Young Adult
Campus : Kochi
School : School of Medicine
Department : Paediatrics
Year : 2012
Abstract : Progressive pseudorheumatoid dysplasia (PPD) is a progressive skeletal syndrome characterized by stiffness, swelling and pain in multiple joints with associated osteoporosis in affected patients. Radiographically, the predominant features resemble a spondyloepiphyseal dysplasia. Mutations in the WISP3 gene are known to cause this autosomal recessive condition. To date, only a limited number of studies have looked into the spectrum of mutations causing PPD. We report on clinical features and WISP3 mutations in a large series of Indian patients with this rare skeletal dysplasia. Families with at least one member showing clinical and radiologic features of PPD were recruited for the study. Symptoms, signs and radiographic findings were documented in 35 patients from 25 unrelated families. Swelling of small joints of hands and contractures are the most common presenting features. Mutation analysis was carried out by bidirectional sequencing of the WISP3 gene in all 35 patients. We summarize the clinical features of 35 patients with PPD and report on 11 different homozygous mutations and one instance of compound heterozygosity. Eight (c.233GA, c.340TC, c.348CA, c.433TC, c.682TC, c.802TG, c.947_951delAATTT, and c.1010GA) are novel mutations and three (c.156CA, c.248GA, and c.739_740delTG) have been reported previously. One missense mutation (c.1010GA; p.Cys337Tyr) appears to be the most common in our population being seen in 10 unrelated families. This is the largest cohort of patients with PPD in the literature and the first report from India on mutation analysis of WISP3. We also review all the mutations reported in WISP3 till date. © 2012 Wiley Periodicals, Inc.
Cite this Research Publication : Aa Dalal, Bhavani, S. La, Togarrati, P. Pa, Bierhals, Tb, Nandineni, M. Rc, Danda, Sd, Danda, De, Shah, Hf, Vijayan, Sf, Gowrishankar, Kg, Phadke, S. Rh, Bidchol, A. Mi, Rao, A. Pj, Nampoothiri, Sk, Kutsche, Kb, and Girisha, K. Mi, “Analysis of the WISP3 gene in Indian families with progressive pseudorheumatoid dysplasia”, American Journal of Medical Genetics, Part A, vol. 158 A, pp. 2820-2828, 2012.