Loss-of-function variants in myocardin cause congenital megabladder in humans and mice
Arjan C. Houweling, … , Adrian S. Woolf, Esther E. Creemers
Arjan C. Houweling, … , Adrian S. Woolf, Esther E. Creemers
Published December 2, 2019; First published September 12, 2019
Citation Information: J Clin Invest. 2019;129(12):5374-5380. https://doi.org/10.1172/JCI128545.
View: Text | PDF
Categories: Concise Communication Muscle biology

Loss-of-function variants in myocardin cause congenital megabladder in humans and mice

Abstract

Myocardin (MYOCD) is the founding member of a class of transcriptional coactivators that bind the serum-response factor to activate gene expression programs critical in smooth muscle (SM) and cardiac muscle development. Insights into the molecular functions of MYOCD have been obtained from cell culture studies, and to date, knowledge about in vivo roles of MYOCD comes exclusively from experimental animals. Here, we defined an often lethal congenital human disease associated with inheritance of pathogenic MYOCD variants. This disease manifested as a massively dilated urinary bladder, or megabladder, with disrupted SM in its wall. We provided evidence that monoallelic loss-of-function variants in MYOCD caused congenital megabladder in males only, whereas biallelic variants were associated with disease in both sexes, with a phenotype additionally involving the cardiovascular system. These results were supported by cosegregation of MYOCD variants with the phenotype in 4 unrelated families by in vitro transactivation studies in which pathogenic variants resulted in abrogated SM gene expression and by the finding of megabladder in 2 distinct mouse models with reduced Myocd activity. In conclusion, we have demonstrated that variants in MYOCD result in human disease, and the collective findings highlight a vital role for MYOCD in mammalian organogenesis.

Authors

Arjan C. Houweling, Glenda M. Beaman, Alex V. Postma, T. Blair Gainous, Klaske D. Lichtenbelt, Francesco Brancati, Filipa M. Lopes, Ingeborg van der Made, Abeltje M. Polstra, Michael L. Robinson, Kevin D. Wright, Jamie M. Ellingford, Ashley R. Jackson, Eline Overwater, Rita Genesio, Silvio Romano, Letizia Camerota, Emanuela D’Angelo, Elizabeth J. Meijers-Heijboer, Vincent M. Christoffels, Kirk M. McHugh, Brian L. Black, William G. Newman, Adrian S. Woolf, Esther E. Creemers

×

Figure 1

Identification of MYOCD variants in 4 families with congenital megabladder.

Options: View larger image (or click on image) Download as PowerPoint
Identification of MYOCD variants in 4 families with congenital megabladd...
(A) Pedigrees of 4 families presenting with congenital megabladder. Affected individuals are marked with black symbols. Available genotypes are shown beneath symbols. Slashed symbols denote deceased individuals. Gestational age is indicated above the symbol. Gray symbols denote stillbirths with external features consistent with PBS. N, normal bladder ultrasound; P with arrow, proband of the family; npe, normal prenatal echo. (B) Schematic diagram showing functional domains within MYOCD and location of the identified mutations (7). Conservation of respective amino acid positions with the mutated residues are highlighted. (C) Ultrasound images showing enlarged bladder of indicated fetuses of families B and C; asterisks denote bladder.