Genetic Mosaicism in Calmodulinopathy

Lisa M Wren; Juan Jiménez-Jáimez; Saleh Al-Ghamdi; Jumana Y Al-Aama; Amnah Bdeir; Zuhair N Al-Hassnan; Jyn L Kuan; Roger Y Foo; Franck Potet; Christopher N Johnson; Miriam C Aziz; Gemma L Carvill; Juan-Pablo Kaski; Lia Crotti; Francesca Perin; Lorenzo Monserrat; Paul W Burridge; Peter J Schwartz; Walter J Chazin; Zahurul A Bhuiyan; Alfred L George Jr

doi:10.1161/CIRCGEN.119.002581

Genetic Mosaicism in Calmodulinopathy

Circ Genom Precis Med. 2019 Sep;12(9):375-385. doi: 10.1161/CIRCGEN.119.002581. Epub 2019 Aug 27.

Authors

Lisa M Wren¹, Juan Jiménez-Jáimez², Saleh Al-Ghamdi³, Jumana Y Al-Aama^{4

5}, Amnah Bdeir⁵, Zuhair N Al-Hassnan⁶, Jyn L Kuan⁷, Roger Y Foo⁷, Franck Potet¹, Christopher N Johnson⁸, Miriam C Aziz⁹, Gemma L Carvill⁹, Juan-Pablo Kaski¹⁰, Lia Crotti^{11

12

13}, Francesca Perin¹⁴, Lorenzo Monserrat¹³, Paul W Burridge¹, Peter J Schwartz¹², Walter J Chazin⁸, Zahurul A Bhuiyan¹⁵, Alfred L George Jr¹

Affiliations

¹ From the Department of Pharmacology (L.M.W., F.P., P.W.B., A.L.G.), Northwestern University Feinberg School of Medicine, Chicago, IL.
² Cardiology Department (J.J.-J.), Virgen de las Nieves Hospital, Granada, Spain.
³ Cardiac Sciences Department, Section of Pediatric Cardiology, King Abdulaziz Cardiac Center, Ministry of National Guard Health Affairs, Riyadh (S.A.-G.).
⁴ Department of Genetic Medicine, Faculty of Medicine (J.Y.A.-A.), King Abdulaziz University, Jeddah.
⁵ Princess Al Jawhara Albrahim Center of Excellence in Research of Hereditary Disorders (J.Y.A.-A., A.B.), King Abdulaziz University, Jeddah.
⁶ The Cardiovascular Genetics Program, King Faisal Specialist Hospital and Research Center, Riyadh, Saudi Arabia (Z.N.A.-H.).
⁷ Department of Cardiology, National University Heart Center and Cardiovascular Research Institute, National University of Singapore (J.L.K., R.Y.F.).
⁸ Department of Biochemistry and Center for Structural Biology, Vanderbilt University, Nashville, TN (C.N.J., W.J.C.).
⁹ Department of Neurology (M.C.A., G.L.C.), Northwestern University Feinberg School of Medicine, Chicago, IL.
¹⁰ Institute of Cardiovascular Science, University College London, United Kingdom (J.-P.K.).
¹¹ Department of Medicine and Surgery, University of Milano-Bicocca (L.C.).
¹² IRCCS Istituto Auxologico Italiano, Center for Cardiac Arrhythmias of Genetic Origin and Laboratory of Cardiovascular Genetics, Milan, Italy (L.C., P.J.S.).
¹³ Cardiology Department, Health in Code SL, A Coruña, Spain (L.M.).
¹⁴ Pediatric Cardiology Division (F.P.), Virgen de las Nieves Hospital, Granada, Spain.
¹⁵ Unité de Recherche Cardiogénétique, Service de Médecine Génétique, Centre Hospitalier Universitaire Vaudois (CHUV), Lausanne, Switzerland (Z.A.B.).

Abstract

Background: CaM (calmodulin) mutations are associated with congenital arrhythmia susceptibility (calmodulinopathy) and are most often de novo. In this report, we sought to broaden the genotype-phenotype spectrum of calmodulinopathies with 2 novel calmodulin mutations and to investigate mosaicism in 2 affected families.

Methods: CaM mutations were identified in 4 independent cases by DNA sequencing. Biochemical and electrophysiological studies were performed to determine functional consequences of each mutation.

Results: Genetic studies identified 2 novel CaM variants (CALM3-E141K in 2 cases; CALM1-E141V) and one previously reported CaM pathogenic variant (CALM3-D130G) among 4 probands with shared clinical features of prolonged QTc interval (range 505-725 ms) and documented ventricular arrhythmia. A fatal outcome occurred for 2 of the cases. The parents of all probands were asymptomatic with normal QTc duration. However, 2 of the families had multiple affected offspring or multiple occurrences of intrauterine fetal demise. The mother from the family with recurrent intrauterine fetal demise exhibited the CALM3-E141K mutant allele in 25% of next-generation sequencing reads indicating somatic mosaicism, whereas CALM3-D130G was present in 6% of captured molecules of the paternal DNA sample, also indicating mosaicism. Two novel mutations (E141K and E141V) impaired Ca²⁺ binding affinity to the C-domain of CaM. Human-induced pluripotent stem cell-derived cardiomyocytes overexpressing mutant or wild-type CaM showed that both mutants impaired Ca²⁺-dependent inactivation of L-type Ca²⁺ channels and prolonged action potential duration.

Conclusions: We report 2 families with somatic mosaicism associated with arrhythmogenic calmodulinopathy, and demonstrate dysregulation of L-type Ca²⁺ channels by 2 novel CaM mutations affecting the same residue. Parental mosaicism should be suspected in families with unexplained fetal arrhythmia or fetal demise combined with a documented CaM mutation.

Keywords: arrhythmia; calmodulin; genotype; long QT syndrome; mosaicism.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Arrhythmias, Cardiac / congenital
Arrhythmias, Cardiac / genetics*
Arrhythmias, Cardiac / metabolism
Arrhythmias, Cardiac / physiopathology
Base Sequence
Calcium / metabolism
Calmodulin / genetics*
Calmodulin / metabolism
Child, Preschool
Electrophysiology
Female
Genetic Predisposition to Disease
Humans
Infant
Infant, Newborn
Male
Mosaicism*
Mutation, Missense
Pedigree

Substances

CALM1 protein, human
CALM3 protein, human
Calmodulin
Calcium

Abstract

Publication types

MeSH terms

Substances

Grants and funding