De novo ACTG2 mutations cause congenital distended bladder, microcolon, and intestinal hypoperistalsis.

[megacystis-microcolon-intestinal hypoperistalsis syndrome]

Megacystis-microcolon -intestinal hypoperistalsis syndrome (MMIHS ) is characterized by prenatal -onset distended urinary bladder with functional intestinal obstruction , requiring extensive surgical intervention for survival . While it is believed to be an autosomal recessive disorder , most cases are sporadic . Through whole-exome sequencing in a child with MMIHS , we identified a de novo mutation , p .R 178 L , in the gene encoding the smooth muscle gamma-2 actin , ACTG 2 . We subsequently detected another de novo ACTG 2 mutation , p .R 178 C , in an additional child with MMIHS . Actg 2 transcripts were primarily found in murine urinary bladder and intestinal tissues . Structural analysis and functional experiments suggested that both ACTG 2 mutants interfere with proper polymerization of ACTG 2 into thin filaments , leading to impaired contractility of the smooth muscle . In conclusion , our study suggests a pathogenic mechanism for MMIHS by identifying causative ACTG 2 mutations .