Accelerating Novel Candidate Gene Discovery in Neurogenetic Disorders via Whole-Exome Sequencing of Prescreened Multiplex Consanguineous Families

Alazami, Anas M.; Nisha, Patel; Shamseldin, Hanan E.; Anazi, Shamsa; Al‐Dosari, Mohammed S.; Alzahrani, Fatema; Hijazi, Hadia; Alshammari, Muneera; Aldahmesh, Mohammed A.; Salih, Mustafa A.; Faqeih, Eissa; Alhashem, Amal; Bashiri, Fahad A.; Al‐Owain, Mohammed; Kentab, Amal Y.; Sogaty, Sameera; Tala, Saeed Al; Temsah, Mohamad-Hani; Tulbah, Maha; Aljelaify, Rasha; AlShahwan, Saad; Seidahmed, Mohammed Zain; Alhadid, Adnan A.; Aldhalaan, Hesham; AlQallaf, Fatema; Kurdi, Wesam; Alfadhel, Majid; Babay, Zainab; Alsogheer, Mohammad; Kaya, Namik; Al‐Hassnan, Zuhair N.; Abdel-Salam, Ghada M.H.; Al‐Sannaa, Nouriya; Mutairi, Fuad Al; Khashab, Heba Y. El; Bohlega, Saeed; Jia, Xiaofei; Nguyen, Henry C.; Hammami, Rakad; Adly, Nouran; Mohamed, Jawahir Y.; Abdulwahab, Firdous; Ibrahim, Niema; Naim, Ewa A.; Al-Younes, Banan; Meyer, Brian F.; Hashem, Mais; Shaheen, Ranad; Xiong, Yong; Abouelhoda, Mohamed; Aldeeri, Abdulrahman; Monies, Dorota; Alkuraya, Fowzan S.

doi:10.1016/j.celrep.2014.12.015

Cited by 372 publications

(336 citation statements)

References 41 publications

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“…7,10 This prompted us to examine the yield of this approach for dysmorphology syndromes in the same setting, i.e., multiplex consanguineous families. Another reason for limiting our study to multiplex families is that the presence of more than one affected individual with the same apparently novel phenotype facilitates the recognition of the core phenotypic features of the syndrome, notwithstanding the known phenomenon of clinical variability.…”

Section: Discussionmentioning

confidence: 99%

“…For both whole-exome and whole-genome sequencing, the candidacy of the resulting variants was based on their physical location within the autozygome of the affected individual, their population frequency, and the predicted effect on the protein as described previously. 10,14 …”

Section: Autozygome Analysismentioning

confidence: 99%

“…16 In 67% (21/31) of families, the strong candidate variant was identified in a gene that was novel at the time of analysis. These include 11 genes that we published previously 10 and 10 that we describe for the first time here ( Table 2).…”

Section: Clinical Characterization Of Apparently Novel Dysmorphologymentioning

confidence: 99%

“…[7][8][9] Recently, we published the identification of 33 novel candidate genes for various neurocognitive phenotypes, and at least 6 of these were independently found to be mutated by other investigators in the few months since the article appeared online (unpublished data). 10 However, we are not aware of any similar effort to accelerate the discovery of novel candidate genes specifically in the setting of dysmorphology syndromes. In this article, we describe our experience with members of 31 multiplex consanguineous families who appeared to have novel dysmorphology syndromes at the time of their initial evaluation; 15 of them are reported here for the first time.…”

Section: Introductionmentioning

confidence: 99%

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Accelerating matchmaking of novel dysmorphology syndromes through clinical and genomic characterization of a large cohort

Shaheen

Patel

Shamseldin

et al. 2016

Genetics in Medicine

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Purpose: Dysmorphology syndromes are among the most common referrals to clinical genetics specialists. Inability to match the dysmorphology pattern to a known syndrome can pose a major diagnostic challenge. With an aim to accelerate the establishment of new syndromes and their genetic etiology, we describe our experience with multiplex consanguineous families that appeared to represent novel autosomal recessive dysmorphology syndromes at the time of evaluation. Methods:Combined autozygome/exome analysis of multiplex consanguineous families with apparently novel dysmorphology syndromes.Results: Consistent with the apparent novelty of the phenotypes, our analysis revealed a strong candidate variant in genes that were novel at the time of the analysis in the majority of cases, and 10 of these genes are published here for the first time as novel candidates (CDK9, NEK9, ZNF668, TTC28, MBL2, CADPS, CACNA1H, HYAL2, CTU2, and C3ORF17). A significant minority of the phenotypes (6/31, 19%), however, were caused by genes known to cause Mendelian phenotypes, thus expanding the phenotypic spectrum of the diseases linked to these genes. The conspicuous inheritance pattern and the highly specific phenotypes appear to have contributed to the high yield (90%) of plausible molecular diagnoses in our study cohort. Conclusion:Reporting detailed clinical and genomic analysis of a large series of apparently novel dysmorphology syndromes will likely lead to a trend to accelerate the establishment of novel syndromes and their underlying genes through open exchange of data for the benefit of patients, their families, health-care providers, and the research community.

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Section: Discussionmentioning

confidence: 99%

Section: Autozygome Analysismentioning

confidence: 99%

Section: Clinical Characterization Of Apparently Novel Dysmorphologymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Accelerating matchmaking of novel dysmorphology syndromes through clinical and genomic characterization of a large cohort

Shaheen

Patel

Shamseldin

et al. 2016

Genetics in Medicine

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“…[14][15][16][17][18][19][20] In addition, WES has also shown to be a powerful tool for identifying autosomal-recessive and X-linked variants in persons with ID. [19][20][21][22][23][24] Here we used WES to identify underlying genetic causes for CVI.…”

Section: Introductionmentioning

confidence: 99%

Novel genetic causes for cerebral visual impairment

et al. 2015

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Diagnostic Yield and Novel Candidate Genes by Exome Sequencing in 152 Consanguineous Families With Neurodevelopmental Disorders

et al. 2017

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Because of the high diagnostic yield of 36.8% and the possibility of identifying treatable diseases or the coexistence of several disease-causing variants, using exome sequencing as a first-line diagnostic approach in consanguineous families with neurodevelopmental disorders is recommended. Furthermore, the literature is enriched with 52 convincing candidate genes that are awaiting confirmation in independent families.

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Accelerating Novel Candidate Gene Discovery in Neurogenetic Disorders via Whole-Exome Sequencing of Prescreened Multiplex Consanguineous Families

Cited by 372 publications

References 41 publications

Accelerating matchmaking of novel dysmorphology syndromes through clinical and genomic characterization of a large cohort

Accelerating matchmaking of novel dysmorphology syndromes through clinical and genomic characterization of a large cohort

Novel genetic causes for cerebral visual impairment

Diagnostic Yield and Novel Candidate Genes by Exome Sequencing in 152 Consanguineous Families With Neurodevelopmental Disorders

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