Secondary findings in a large Pakistani cohort tested with whole genome sequencing

Author:

Skrahin Aliaksandr1ORCID,Cheema Huma Arshad2,Hussain Maqbool3,Rana Nuzhat Noureen4,Rehman Khalil Ur5ORCID,Kumar Raman6,Oprea Gabriela1,Ameziane Najim1,Rolfs Arndt17,Skrahina Volha1

Affiliation:

1. Arcensus GmbH, Rostock, Germany

2. University of Child Health Sciences, the Children’s Hospital, Lahore, Pakistan

3. Pakistan Institute of Medical Sciences, Islamabad, Pakistan

4. The Children’s Hospital and the Institute of Child Health, Multan, Pakistan

5. Town Women and Children Hospital, Peshawar, Pakistan

6. Liaquat National Hospital, Karachi, Pakistan

7. University of Rostock, Medical Faculty, Rostock, Germany

Abstract

Studies on genomic secondary findings (SFs) are diverse in participants’ characteristics, sequencing methods, and versions of the ACMG SF list. Based on whole genome sequencing and the version 3.1 of the ACMG SF list, we studied SFs in 863 individuals from five different regions in Pakistan. We identified 24 ACMG SFs in 23 (2.7%) of 863 individuals: 18 of 24 were related to cardiovascular disease and four to cancer syndromes. In addition to ACMG SFs, we identified 16 (1.9%) participants with pathogenic and likely pathogenic variants in genes that were not related to the participants’ clinical conditions but with clear medical actionability (non-ACMG SFs): 4 of 16 were related to eye diseases, two to metabolic disorders, and two to urinary system disorders. By testing a large Pakistani cohort with whole genome sequencing, we concluded that in countries such as Pakistan, the ACMG SF list could be expanded, and our non-ACMG SF list is one example.

Publisher

Life Science Alliance, LLC

Subject

Health, Toxicology and Mutagenesis,Plant Science,Biochemistry, Genetics and Molecular Biology (miscellaneous),Ecology

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