| Literature DB >> 32655342 |
Nebojsa Zecevic1, Vladimir Arsenijevic2, Emmanouil Manolakos3, Ioannis Papoulidis3, Georgios Theocharis3, Anastasios Sartsidis3, Tryfon Tsagas4, Ioannis Tziotis4, Themistoklis Dagklis5, Georgios Kalogeros6, Ioannis Tsakiridis5, Milica Filipovic Stankovic7, Makarios Eleftheriades8.
Abstract
Mutations in the skeletal muscle ryanodine receptor (RYR1) gene have been linked to malignant hyperthermia susceptibility, central core disease, and minicore myopathy with external ophthalmoplegia. RYR1 is an intracellular calcium release channel and plays a crucial role in the sarcoplasmic reticulum and transverse tubule connection. Here, we report 2 fetuses from the same parents with compound heterozygous mutations in the RYR1 gene (c.10347+1G>A and c.10456-2Α>G) who presented with fetal akinesia and polyhydramnios at 27 and 19 weeks of gestation with intrauterine growth restriction in the third pregnancy. The prospective parents of the fetuses were heterozygous carriers for c.10456-2Α>G (mother) and c.10347+1G>A (father). Both mutations affect splice sites resulting in dysfunctional protein forms probably missing crucial domains of the C-terminus. Our findings reveal a new RYR1 splice site mutation (c.10456-2Α>G) that may be associated with the clinical features of myopathies, expanding the RYR1 spectrum related to these pathologies.Entities:
Keywords: Compound heterozygous mutations; Fetal akinesia; Myopathies; Next-generation sequencing; Skeletal muscle ryanodine receptor
Year: 2020 PMID: 32655342 PMCID: PMC7325118 DOI: 10.1159/000507034
Source DB: PubMed Journal: Mol Syndromol ISSN: 1661-8769