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Paired-like homeobox gene (PHOX2B) nonpolyalanine repeat expansion mutations (NPARMs): genotype-phenotype correlation in congenital central hypoventilation syndrome (CCHS).

突变 基因 外显子 错义突变 医学 基因型 外显子组测序 无义突变
作者
Amy Zhou,Casey M. Rand,Sara M. Hockney,Grace Niewijk,Patrick Reineke,Virginia Speare,Elizabeth Berry-Kravis,Lili Zhou,Lawrence J. Jennings,Min Yu,Isabella Ceccherini,Tiziana Bachetti,Melanie Pennock,Kai Lee Yap,Debra E. Weese-Mayer
出处
期刊:Genetics in Medicine [Springer Nature]
卷期号:23 (9): 1656-1663 被引量:2
标识
DOI:10.1038/s41436-021-01178-x
摘要

Abstract Purpose CCHS is an extremely rare congenital disorder requiring artificial ventilation as life support. Typically caused by heterozygous polyalanine repeat expansion mutations (PARMs) in the PHOX2B gene, identification of a relationship between PARM length and phenotype severity has enabled anticipatory management. However, for patients with non-PARMs in PHOX2B (NPARMs, ~10% of CCHS patients), a genotype–phenotype correlation has not been established. This comprehensive report of PHOX2B NPARMs and associated phenotypes, aims at elucidating potential genotype–phenotype correlations that will guide anticipatory management. Methods An international collaboration (clinical, commercial, and research laboratories) was established to collect/share information on novel and previously published PHOX2B NPARM cases. Variants were categorized by type and gene location. Categorical data were analyzed with chi-square and Fisher's exact test; further pairwise comparisons were made on significant results. Results Three hundred two individuals with PHOX2B NPARMs were identified, including 139 previously unreported cases. Findings demonstrate significant associations between key phenotypic manifestations of CCHS and variant type, location, and predicted effect on protein function. Conclusion This study presents the largest cohort of PHOX2B NPARMs and associated phenotype data to date, enabling genotype–phenotype studies that will advance personalized, anticipatory management and help elucidate pathological mechanisms. Further characterization of PHOX2B NPARMs demands longitudinal clinical follow-up through international registries.
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