| Literature DB >> 30498240 |
Khurram Liaqat1,2, Isabelle Schrauwen2, Syed Irfan Raza3,4, Kwanghyuk Lee2, Shabir Hussain2,4, Imen Chakchouk2, Abdul Nasir4, Anushree Acharya2, Izoduwa Abbe2, Muhammad Umair4,5, Muhammad Ansar4, Irfan Ullah4,6, Khadim Shah4,7, Michael J Bamshad8,9, Deborah A Nickerson8, Wasim Ahmad4, Suzanne M Leal10.
Abstract
Sinoatrial node dysfunction and deafness (SANDD) syndrome is rare and characterized by a low heart beat and severe-to-profound deafness. Additional features include fatigue, dizziness, and episodic syncope. The sinoatrial node (SAN) drives heart automaticity and continuously regulates heart rate. The CACNA1D gene encoding the Cav1.3 protein expressed in inner hair cells, atria and SAN, induces loss-of-function in channel activity and underlies SANDD. To date, only one variant c.1208_1209insGGG:p.(G403_V404insG) has been reported for SANDD syndrome. We studied five Pakistani families with SANDD and characterized a new missense variant p.(A376V) in CACNA1D in one family, and further characterized the founder variant p.(G403_V404insG) in four additional pedigrees. We show that affected individuals in the four families which segregate p.(G403_V404insG) share a 1.03 MB haplotype on 3p21.1 suggesting they share a common distant ancestor. In conclusion, we identified new and known variants in CACNA1D in five Pakistani families with SANDD. This study is of clinical importance as the CACNA1D founder variant is only observed in families from the Khyber Pakhtunkhwa (KPK) province, in Pakistan. Therefore, screening patients with congenital deafness for SAN dysfunction in this province could ensure adequate follow-up and prevent cardiac failure associated with SAN.Entities:
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Year: 2018 PMID: 30498240 PMCID: PMC6561484 DOI: 10.1038/s10038-018-0542-8
Source DB: PubMed Journal: J Hum Genet ISSN: 1434-5161 Impact factor: 3.172