遗传学
生物
基因
转录组
先证者
错义突变
基因组
表型
突变
基因表达
作者
Waheed Awotoye,Peter Mossey,Jacqueline B. Hetmanski,Lord Jephthah Joojo Gowans,Mekonen Eshete,Wasiu Lanre Adeyemo,Azeez Alade,Erliang Zeng,Olawale Adamson,Thirona Naicker,Deepti Anand,Chinyere Adeleke,Tamara Busch,Mary Li,Aline Petrin,Babatunde S. Aregbesola,Ramat Oyebunmi Braimah,Fadekemi Olufunmilayo Oginni,Ayodeji O. Oladele,Abimbola Oladayo
标识
DOI:10.1038/s41598-022-15885-1
摘要
The majority (85%) of nonsyndromic cleft lip with or without cleft palate (nsCL/P) cases occur sporadically, suggesting a role for de novo mutations (DNMs) in the etiology of nsCL/P. To identify high impact protein-altering DNMs that contribute to the risk of nsCL/P, we conducted whole-genome sequencing (WGS) analyses in 130 African case-parent trios (affected probands and unaffected parents). We identified 162 high confidence protein-altering DNMs some of which are based on available evidence, contribute to the risk of nsCL/P. These include novel protein-truncating DNMs in the ACTL6A, ARHGAP10, MINK1, TMEM5 and TTN genes; as well as missense variants in ACAN, DHRS3, DLX6, EPHB2, FKBP10, KMT2D, RECQL4, SEMA3C, SEMA4D, SHH, TP63, and TULP4. Many of these protein-altering DNMs were predicted to be pathogenic. Analysis using mouse transcriptomics data showed that some of these genes are expressed during the development of primary and secondary palate. Gene-set enrichment analysis of the protein-altering DNMs identified palatal development and neural crest migration among the few processes that were significantly enriched. These processes are directly involved in the etiopathogenesis of clefting. The analysis of the coding sequence in the WGS data provides more evidence of the opportunity for novel findings in the African genome.
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