Secondary findings in 622 Turkish clinical exome sequencing data

GEÇKİNLİ, BİLGEN BİLGE; ARMAN, AHMET; ÇEBİ, ALPER HAN; GÜNEY, AHMET İLTER; ATA, PINAR; Ates, Esra Arslan; TÜRKYILMAZ, AYBERK; Yildirim, Ozlem; ALAVANDA, CEREN; Polat, Hamza; Demir, Senol

dc.contributor.author	GEÇKİNLİ, BİLGEN BİLGE
dc.contributor.author	ARMAN, AHMET
dc.contributor.author	ÇEBİ, ALPER HAN
dc.contributor.author	GÜNEY, AHMET İLTER
dc.contributor.author	ATA, PINAR
dc.contributor.author	Ates, Esra Arslan
dc.contributor.author	TÜRKYILMAZ, AYBERK
dc.contributor.author	Yildirim, Ozlem
dc.contributor.author	ALAVANDA, CEREN
dc.contributor.author	Polat, Hamza
dc.contributor.author	Demir, Senol
dc.date.accessioned	2021-12-10T13:03:00Z
dc.date.available	2021-12-10T13:03:00Z
dc.identifier.citation	Ates E. A. , TÜRKYILMAZ A., Yildirim O., ALAVANDA C., Polat H., Demir S., ÇEBİ A. H. , GEÇKİNLİ B. B. , GÜNEY A. İ. , ATA P., et al., "Secondary findings in 622 Turkish clinical exome sequencing data", JOURNAL OF HUMAN GENETICS, 2021
dc.identifier.issn	1434-5161
dc.identifier.other	vv_1032021
dc.identifier.other	av_ea901714-aaab-4578-b383-fab2f2ac1821
dc.identifier.uri	http://hdl.handle.net/20.500.12627/175290
dc.identifier.uri	https://doi.org/10.1038/s10038-021-00936-8
dc.description.abstract	CES (Clinical Exome Sequencing) is a method that we use to diagnose rare diseases with nonspesific clinical features. Besides primary indication for testing genetic information may be detected about diseases which have not yet emerged. ACMG guidelines recommend to report pathogenic variations in medically actionable 59 genes. In this study we evaluated CES data of 622 cases which were tested for various indications. According to ACMG recommendations 59 genes were screened for reportable variations. The detected variations were reviewed using distinct databases and ACMG variation classification guidelines. Among 622 cases 13 (2.1%) had reportable variations including oncogenetic, cardiogenetic disorders, and malignant hyperthermia susceptibility-related genes. In 15 cases (2.4%) heterozygous pathogenic and likely pathogenic variations were detected in genes showing autosomal recessive inheritance. Ten novel variations causing truncated protein or splicing defect were reported. We detected 11 variations having conflicting interpretations in databases and 30 novel variations, predicted as likely pathogenic via insilico analysis tools which further evaluations are needed. As to our knowledge this is the first study investigating secondary findings in Turkish population. To extract the information that may lead to prevent severe morbidities and mortalities from big data is a valuable and lifesaving effort. Results of this study will contrbute to existing knowledge about secondary findings in exome sequencing and will be a pioneer for studies in Turkish population.
dc.language.iso	eng
dc.subject	Yaşam Bilimleri
dc.subject	Moleküler Biyoloji ve Genetik
dc.subject	Temel Bilimler
dc.subject	Genetics
dc.subject	Molecular Biology
dc.subject	Genetics (clinical)
dc.subject	Life Sciences
dc.subject	Health Sciences
dc.subject	Sağlık Bilimleri
dc.subject	Tıp
dc.subject	Yaşam Bilimleri (LIFE)
dc.subject	Moleküler Biyoloji ve Genetik
dc.subject	GENETİK VE HAYAT
dc.subject	Dahili Tıp Bilimleri
dc.subject	Tıbbi Genetik
dc.title	Secondary findings in 622 Turkish clinical exome sequencing data
dc.type	Makale
dc.relation.journal	JOURNAL OF HUMAN GENETICS
dc.contributor.department	Marmara Üniversitesi , ,
dc.contributor.firstauthorID	2638123

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