| Literature DB >> 32738303 |
Shuzhang Liang1, Xin Shi2, Chunxiao Yu3, Xuelian Shao1, Haitao Zhou3, Xueyu Li1, Cheng Chang3, Kaa Seng Lai1, Jinmin Ma1, Ruilin Zhang4.
Abstract
Heterotaxy syndrome (HS) involves dysfunction of multiple systems resulting from abnormal left-right (LR) body patterning. Most HS patients present with complex congenital heart diseases (CHD), the disability and mortality of HS patients are extremely high. HS has great heterogeneity in phenotypes and genotypes, which have rendered gene discovery challenging. The aim of this study was to identify novel genes that underlie pathogenesis of HS patients with CHD. Whole exome sequencing was performed in 25 unrelated HS cases and 100 healthy controls; 19 nonsynonymous variants in 6 novel candidate genes (FLNA, ITGA1, PCNT, KIF7, GLI1, KMT2D) were identified. The functions of candidate genes were further analyzed in zebrafish model by CRISPR/Cas9 technique. Genome-editing was successfully introduced into the gene loci of flna, kmt2d and kif7, but the phenotypes were heterogenous. Disruption of each gene disturbed normal cardiac looping while kif7 knockout had a more prominent effect on liver budding and pitx2 expression. Our results revealed three potential HS pathogenic genes with probably different molecular mechanisms.Entities:
Keywords: Congenital heart disease; Heterotaxy syndrome; Rare variant; Whole exome sequencing
Year: 2020 PMID: 32738303 DOI: 10.1016/j.bbadis.2020.165906
Source DB: PubMed Journal: Biochim Biophys Acta Mol Basis Dis ISSN: 0925-4439 Impact factor: 5.187