The genetic cause of neurodevelopmental disorders in 30 consanguineous families.

Details

Serval ID
serval:BIB_0769912C0633
Type
Article: article from journal or magazin.
Collection
Publications
Institution
Title
The genetic cause of neurodevelopmental disorders in 30 consanguineous families.
Journal
Frontiers in medicine
Author(s)
Paracha S.A., Nawaz S., Tahir Sarwar M., Shaheen A., Zaman G., Ahmed J., Shah F., Khwaja S., Jan A., Khan N., Kamal M.A., Alam Q., Abbas S., Farman S., Waqas A., Alkathiri A., Hamadi A., Santoni F., Ullah N., Khalid B., Antonarakis S.E., Fakhro K.A., Umair M., Ansar M.
ISSN
2296-858X (Print)
ISSN-L
2296-858X
Publication state
Published
Issued date
2024
Peer-reviewed
Oui
Volume
11
Pages
1424753
Language
english
Notes
Publication types: Journal Article
Publication Status: epublish
Abstract
This study aims to clinically and genetically assess 30 unrelated consanguineous Pakistani families from various ethnic backgrounds, all exhibiting features of neurodevelopmental disorders (NDDs).
We conducted clinical, genetic, biochemical, and molecular analyses on 30 consanguineous families with NDDs enrolled from various regions of Pakistan. The likely molecular causes of primary microcephaly and NDDs were identified. Detailed clinical investigations and molecular diagnoses were performed using whole exome sequencing (WES) of the proband, followed by Sanger sequencing for validation and segregation in the available family members of the affected families.
WES identified likely disease-causing homozygous variants in 30 unrelated consanguineous families. Six families presented newly described variants in known NDD-related genes: ABAT (c.1439 T > G; p.Phe480Cys) [OMIM613163], SLC12A6 (c.2865_2865insT; p.Glu955Asnfs*5) [OMIM 218000], SHANK3 (c.1305-3_1,305-2delTT; p.Gln29-_Gly305del) [OMIM 606232], BCKDK (c.356_356insC; p.Gly119Alafs*24) [OMIM 614923], DDHD2 (c.2065G > T; p.Asp689Tyr) [OMIM 615033], ERCC2 (c.1255G > A; p.Glu419Lys) [OMIM 610756]. Additionally, 12 families had previously reported disease-causing variants associated with different types of NDDs: ATRX (c.109C > T; p.Arg37*) [OMIM 309580], GPR56 [ADGRG1] (c.1423C > T; p.Arg475*) [OMIM 606854], NAGLU (c.1694G > A; p.Arg565Gln) [OMIM 252920], DOLK (c.3G > A; p.Met1Ile) [OMIM 610768], GPT2 (c.815C > T; p.Ser272Leu) [OMIM 616281], DYNC1I2 (c.607 + 1G > A; p.?) [OMIM 618492], FBXL3 (c.885delT; p.Leu295Phefs25*) [OMIM 606220], LINGO1 (c.869G > A; p.Arg290His) [OMIM 618103], and ASPM (c.3978G > A; Trp1326*, c.9557C > G; p.Ser3186*, c.6994C > T; p.Arg2332*) [OMIM 608716]. All the identified variants showed segregation compatible with autosomal recessive inheritance.
In the present study, we observed a high frequency of ASPM variants in the genetic analysis of 30 consanguineous families exhibiting features of NDDs, particularly those associated with autosomal recessive primary microcephaly. These findings contribute to studies on genotype-phenotype correlation, genetic counseling for families, and a deeper understanding of human brain function and development.
Keywords
30 families, ASPM, WES, consanguineous marriages, neurodevelopmental disorders, novel variants
Pubmed
Web of science
Open Access
Yes
Create date
20/09/2024 14:44
Last modification date
31/10/2024 7:13
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