Genomic and phenotypic delineation of congenital microcephaly

Shaheen, Ranad; Maddirevula, Sateesh; Ewida, Nour; Alsahli, Saud; Abdel-Salam, Ghada M. H.; Zaki, Maha S.; Tala, Saeed Al; Alhashem, Amal; Softah, Ameen; Al-Owain, Mohammed; Alazami, Anas M.; Abadel, Basma; Patel, Nisha; Al-Sheddi, Tarfa; Alomar, Rana; Alobeid, Eman; Ibrahim, Niema; Hashem, Mais; Abdulwahab, Firdous; Hamad, Muddathir; Tabarki, Brahim; Alwadei, Ali H.; Alhazzani, Fahad; Bashiri, Fahad A.; Kentab, Amal; Şahintürk, Serdar; Sherr, Elliott; Fregeau, Brieana; Sogati, Samira; Alshahwan, Saad Ali M.; Alkhalifi, Salwa; Alhumaidi, Zainab; Temtamy, Samia; Aglan, Mona; Otaify, Ghada; Girisha, Katta M.; Tulbah, Maha; Seidahmed, Mohammed Zain; Salih, Mustafa A.; Abouelhoda, Mohamed; Momin, Afaque Ahmad Imtiyaz; Saffar, Muna Al; Partlow, Jennifer N.; Arold, Stefan T.; Faqeih, Eissa; Walsh, Christopher; Alkuraya, Fowzan S.

Type

Article

KAUST Department

Biological and Environmental Sciences and Engineering (BESE) Division
Bioscience Program
Computational Bioscience Research Center (CBRC)
Computer, Electrical and Mathematical Sciences and Engineering (CEMSE) Division

Date

2018-09-14

Permanent link to this record

http://hdl.handle.net/10754/630528

Metadata

Show full item record

Abstract

Congenital microcephaly (CM) is an important birth defect with long term neurological sequelae. We aimed to perform detailed phenotypic and genomic analysis of patients with Mendelian forms of CM.Clinical phenotyping, targeted or exome sequencing, and autozygome analysis.We describe 150 patients (104 families) with 56 Mendelian forms of CM. Our data show little overlap with the genetic causes of postnatal microcephaly. We also show that a broad definition of primary microcephaly -as an autosomal recessive form of nonsyndromic CM with severe postnatal deceleration of occipitofrontal circumference-is highly sensitive but has a limited specificity. In addition, we expand the overlap between primary microcephaly and microcephalic primordial dwarfism both clinically (short stature in >52% of patients with primary microcephaly) and molecularly (e.g., we report the first instance of CEP135-related microcephalic primordial dwarfism). We expand the allelic and locus heterogeneity of CM by reporting 37 novel likely disease-causing variants in 27 disease genes, confirming the candidacy of ANKLE2, YARS, FRMD4A, and THG1L, and proposing the candidacy of BPTF, MAP1B, CCNH, and PPFIBP1.Our study refines the phenotype of CM, expands its genetics heterogeneity, and informs the workup of children born with this developmental brain defect.

Citation

Shaheen R, Maddirevula S, Ewida N, Alsahli S, Abdel-Salam GMH, et al. (2018) Genomic and phenotypic delineation of congenital microcephaly. Genetics in Medicine. Available: http://dx.doi.org/10.1038/s41436-018-0140-3.

Sponsors

This work was supported by the King Salman Center for Disability Research (F.S.A.), King Abdulaziz City for Science and Technology (13-BIO1113-20, F.S.A.), and the Saudi Human Genome Program (F.S.A.). M.A.S. was supported by the Deanship of Scientific Research, King Saud University, Riyadh, Saudi Arabia through the research group project number RGP-VPP-301. The research by S.T.A. and A.A.M. reported in this publication was supported by funding from King Abdullah University of Science and Technology (KAUST). C.A.W. was supported by the Manton Center for Orphan Disease Research and a grant from the National Institute of Neurological Disorders and Stroke (R01 NS035129) and is an Investigator of the Howard Hughes Medical Institute. We thank the study families for their enthusiastic participation and the Sequencing and Genotyping Core Facilities at King Faisal Specialist Hospital and Research Centre (KFSHRC) for their technical help.