A Founder Mutation in The GMPPB gene [c.1000G > A (p.Asp334Asn)] Causes a Mild Form of Limb-girdle Muscular Dystrophy/congenital Myasthenic Syndrome (LGMD/CMS) in South Indian Patients

Overview

Journal Neurogenetics

Specialty Neurology

Date 2021 Aug 1

PMID 34333724

Citations 5

Authors

Kiran Polavarapu

Aradhna Mathur

Aditi Joshi

Saraswati Nashi

Veeramani Preethish-Kumar

Mainak Bardhan

Pooja Sharma

Shaista Parveen

Malika Seth

Seena Vengalil

Tanushree Chawla

Leena Shingavi

Uzma Shamim

Sushmita Nayak

A Vivekanand

Ana Topf

Andreas Roos

Rita Horvath

Hanns Lochmuller

Bevinahalli Nandeesh

Gautham Arunachal

Atchayaram Nalini

Mohammed Faruq

Affiliations

Soon will be listed here.

Abstract

Twelve patients from seven unrelated South Indian families with a limb-girdle muscular dystrophy-congenital myasthenic syndrome (LGMD/CMS) phenotype and recessive inheritance underwent deep clinical phenotyping, electrophysiological evaluation, muscle histopathology, and next-generation sequencing/Sanger sequencing-based identification of the genetic defect. Homozygosity mapping was performed using high-throughput genome-wide genotyping for mapping the mutation and to evaluate the founder effect. The age of disease onset among patients ranged from childhood to 40 years of age. The key clinical manifestations observed were progressive fatigable limb-girdle weakness, muscle hypertrophy/atrophy, and preferential weakness in a dystrophic pattern. The ages at last follow-up ranged from 30 to 64 years; nine were independently ambulant, two required assistance, and one was wheelchair-bound. Lower limb muscle MRI showed varying degrees of fat replacement in the glutei, hamstrings, anterior leg muscles, and medial gastrocnemius. All patients showed significant decrement on repetitive nerve stimulation (RNS). Muscle biopsy in 7 patients revealed varying degrees of dystrophic and neurogenic changes. Treatment with pyridostigmine and/or salbutamol resulted in variable improvement in 10 patients. Genetic analysis showed an identical homozygous GMPPB mutation c.1000G > A (p.Asp334Asn) in all affected patients. A region of homozygosity (6Mbp) was observed flanking the c.1000G > A change in carrier chromosomes. This study identifies c.1000G > A in GMPPB as a common founder mutation in an ethnic community of South Indian descent with milder yet variable degree of clinical presentation of GMPPB-associated LGMD-CMS.

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