Burden of Mendelian disorders in a large Middle Eastern biobank

The Qatar Genome Program Research Consortium; Biobank and Sample Preparation; Sequencing and Genotyping group; Applied Bioinformatics Core; Data Management and Computing Infrastructure group; Consortium Lead Principal Investigators (in alphabetical order)

doi:10.1186/s13073-024-01307-6

Burden of Mendelian disorders in a large Middle Eastern biobank

The Qatar Genome Program Research Consortium
, Biobank and Sample Preparation
, Sequencing and Genotyping group
, Applied Bioinformatics Core
, Data Management and Computing Infrastructure group
, Consortium Lead Principal Investigators (in alphabetical order)

Genomics and Translational Biomedicine

Research output: Contribution to journal › Article › peer-review

9 Citations (Scopus)

Abstract

Background: Genome sequencing of large biobanks from under-represented ancestries provides a valuable resource for the interrogation of Mendelian disease burden at world population level, complementing small-scale familial studies. Methods: Here, we interrogate 6045 whole genomes from Qatar—a Middle Eastern population with high consanguinity and understudied mutational burden—enrolled at the national Biobank and phenotyped for 58 clinically-relevant quantitative traits. We examine a curated set of 2648 Mendelian genes from 20 panels, annotating known and novel pathogenic variants and assessing their penetrance and impact on the measured traits. Results: We find that 62.5% of participants are carriers of at least 1 known pathogenic variant relating to recessive conditions, with homozygosity observed in 1 in 150 subjects (0.6%) for which Peninsular Arabs are particularly enriched versus other ancestries (5.8-fold). On average, 52.3 loss-of-function variants were found per genome, 6.5 of which affect a known Mendelian gene. Several variants annotated in ClinVar/HGMD as pathogenic appeared at intermediate frequencies in this cohort (1–3%), highlighting Arab founder effect, while others have exceedingly high frequencies (> 5%) prompting reconsideration as benign. Furthermore, cumulative gene burden analysis revealed 56 genes having gene carrier frequency > 1/50, including 5 ACMG Tier 3 panel genes which would be candidates for adding to newborn screening in the country. Additionally, leveraging 58 biobank traits, we systematically assess the impact of novel/rare variants on phenotypes and discover 39 candidate large-effect variants associating with extreme quantitative traits. Furthermore, through rare variant burden testing, we discover 13 genes with high mutational load, including 5 with impact on traits relevant to disease conditions, including metabolic disorder and type 2 diabetes, consistent with the high prevalence of these conditions in the region. Conclusions: This study on the first phase of the growing Qatar Genome Program cohort provides a comprehensive resource from a Middle Eastern population to understand the global mutational burden in Mendelian genes and their impact on traits in seemingly healthy individuals in high consanguinity settings.

Original language	English
Article number	46
Journal	Genome Medicine
Volume	16
Issue number	1
DOIs	https://doi.org/10.1186/s13073-024-01307-6
Publication status	Published - 8 Apr 2024

Keywords

Arab population
Biobank
Consanguinity
Genome sequencing
Mendelian disorders
Middle East
Pathogenic variants
Qatar
Rare genetic disease

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10.1186/s13073-024-01307-6

Cite this

The Qatar Genome Program Research Consortium, Biobank and Sample Preparation, Sequencing and Genotyping group, Applied Bioinformatics Core, Data Management and Computing Infrastructure group, & Consortium Lead Principal Investigators (in alphabetical order) (2024). Burden of Mendelian disorders in a large Middle Eastern biobank. Genome Medicine, 16(1), Article 46. https://doi.org/10.1186/s13073-024-01307-6

@article{5e9be57eb52a4f59a5b3ed23042a8279,

title = "Burden of Mendelian disorders in a large Middle Eastern biobank",

abstract = "Background: Genome sequencing of large biobanks from under-represented ancestries provides a valuable resource for the interrogation of Mendelian disease burden at world population level, complementing small-scale familial studies. Methods: Here, we interrogate 6045 whole genomes from Qatar—a Middle Eastern population with high consanguinity and understudied mutational burden—enrolled at the national Biobank and phenotyped for 58 clinically-relevant quantitative traits. We examine a curated set of 2648 Mendelian genes from 20 panels, annotating known and novel pathogenic variants and assessing their penetrance and impact on the measured traits. Results: We find that 62.5\% of participants are carriers of at least 1 known pathogenic variant relating to recessive conditions, with homozygosity observed in 1 in 150 subjects (0.6\%) for which Peninsular Arabs are particularly enriched versus other ancestries (5.8-fold). On average, 52.3 loss-of-function variants were found per genome, 6.5 of which affect a known Mendelian gene. Several variants annotated in ClinVar/HGMD as pathogenic appeared at intermediate frequencies in this cohort (1–3\%), highlighting Arab founder effect, while others have exceedingly high frequencies (> 5\%) prompting reconsideration as benign. Furthermore, cumulative gene burden analysis revealed 56 genes having gene carrier frequency > 1/50, including 5 ACMG Tier 3 panel genes which would be candidates for adding to newborn screening in the country. Additionally, leveraging 58 biobank traits, we systematically assess the impact of novel/rare variants on phenotypes and discover 39 candidate large-effect variants associating with extreme quantitative traits. Furthermore, through rare variant burden testing, we discover 13 genes with high mutational load, including 5 with impact on traits relevant to disease conditions, including metabolic disorder and type 2 diabetes, consistent with the high prevalence of these conditions in the region. Conclusions: This study on the first phase of the growing Qatar Genome Program cohort provides a comprehensive resource from a Middle Eastern population to understand the global mutational burden in Mendelian genes and their impact on traits in seemingly healthy individuals in high consanguinity settings.",

keywords = "Arab population, Biobank, Consanguinity, Genome sequencing, Mendelian disorders, Middle East, Pathogenic variants, Qatar, Rare genetic disease",

author = "\{The Qatar Genome Program Research Consortium\} and \{Biobank and Sample Preparation\} and \{Sequencing and Genotyping group\} and \{Applied Bioinformatics Core\} and \{Data Management and Computing Infrastructure group\} and \{Consortium Lead Principal Investigators (in alphabetical order)\} and Waleed Aamer and Aljazi Al-Maraghi and Najeeb Syed and Gandhi, \{Geethanjali Devadoss\} and Elbay Aliyev and Al-Kurbi, \{Alya A.\} and Omayma Al-Saei and Muhammad Kohailan and Navaneethakrishnan Krishnamoorthy and Sasirekha Palaniswamy and Khulod Al-Malki and Saleha Abbasi and Nourhen Agrebi and Fatemeh Abbaszadeh and Akil, \{Ammira S.Al Shabeeb\} and Ramin Badii and Tawfeg Ben-Omran and Bernice Lo and Younes Mokrab and Fakhro, \{Khalid A.\} and Ismail, \{Said I.\} and Wadha Al-Muftah and Radja Badji and Hamdi Mbarek and Dima Darwish and Tasnim Fadl and Heba Yasin and Maryem Ennaifar and Rania Abdellatif and Fatima Alkuwari and Muhammad Alvi and Yasser Al-Sarraj and Chadi Saad and Asmaa Althani and Eleni Fethnou and Fatima Qafoud and Eiman Alkhayat and Nahla Afifi and Sara Tomei and Wei Liu and Kun Wang and Stephan Lorenz and Najeeb Syed and Hakeem Almabrazi and Vempalli, \{Fazulur Rehaman\} and Ramzi Temanni and Saqri, \{Tariq Abu\} and Mohammedhusen Khatib and Omar Albagha and Puthen, \{Jithesh V.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

month = apr,

day = "8",

doi = "10.1186/s13073-024-01307-6",

language = "English",

volume = "16",

journal = "Genome Medicine",

issn = "1756-994X",

publisher = "BioMed Central Ltd",

number = "1",

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The Qatar Genome Program Research Consortium, Biobank and Sample Preparation, Sequencing and Genotyping group, Applied Bioinformatics Core, Data Management and Computing Infrastructure group & Consortium Lead Principal Investigators (in alphabetical order) 2024, 'Burden of Mendelian disorders in a large Middle Eastern biobank', Genome Medicine, vol. 16, no. 1, 46. https://doi.org/10.1186/s13073-024-01307-6

TY - JOUR

T1 - Burden of Mendelian disorders in a large Middle Eastern biobank

AU - The Qatar Genome Program Research Consortium

AU - Biobank and Sample Preparation

AU - Sequencing and Genotyping group

AU - Applied Bioinformatics Core

AU - Data Management and Computing Infrastructure group

AU - Consortium Lead Principal Investigators (in alphabetical order)

AU - Aamer, Waleed

AU - Al-Maraghi, Aljazi

AU - Syed, Najeeb

AU - Gandhi, Geethanjali Devadoss

AU - Aliyev, Elbay

AU - Al-Kurbi, Alya A.

AU - Al-Saei, Omayma

AU - Kohailan, Muhammad

AU - Krishnamoorthy, Navaneethakrishnan

AU - Palaniswamy, Sasirekha

AU - Al-Malki, Khulod

AU - Abbasi, Saleha

AU - Agrebi, Nourhen

AU - Abbaszadeh, Fatemeh

AU - Akil, Ammira S.Al Shabeeb

AU - Badii, Ramin

AU - Ben-Omran, Tawfeg

AU - Lo, Bernice

AU - Mokrab, Younes

AU - Fakhro, Khalid A.

AU - Ismail, Said I.

AU - Al-Muftah, Wadha

AU - Badji, Radja

AU - Mbarek, Hamdi

AU - Darwish, Dima

AU - Fadl, Tasnim

AU - Yasin, Heba

AU - Ennaifar, Maryem

AU - Abdellatif, Rania

AU - Alkuwari, Fatima

AU - Alvi, Muhammad

AU - Al-Sarraj, Yasser

AU - Saad, Chadi

AU - Althani, Asmaa

AU - Fethnou, Eleni

AU - Qafoud, Fatima

AU - Alkhayat, Eiman

AU - Afifi, Nahla

AU - Tomei, Sara

AU - Liu, Wei

AU - Wang, Kun

AU - Lorenz, Stephan

AU - Syed, Najeeb

AU - Almabrazi, Hakeem

AU - Vempalli, Fazulur Rehaman

AU - Temanni, Ramzi

AU - Saqri, Tariq Abu

AU - Khatib, Mohammedhusen

AU - Albagha, Omar

AU - Puthen, Jithesh V.

PY - 2024/4/8

Y1 - 2024/4/8

N2 - Background: Genome sequencing of large biobanks from under-represented ancestries provides a valuable resource for the interrogation of Mendelian disease burden at world population level, complementing small-scale familial studies. Methods: Here, we interrogate 6045 whole genomes from Qatar—a Middle Eastern population with high consanguinity and understudied mutational burden—enrolled at the national Biobank and phenotyped for 58 clinically-relevant quantitative traits. We examine a curated set of 2648 Mendelian genes from 20 panels, annotating known and novel pathogenic variants and assessing their penetrance and impact on the measured traits. Results: We find that 62.5% of participants are carriers of at least 1 known pathogenic variant relating to recessive conditions, with homozygosity observed in 1 in 150 subjects (0.6%) for which Peninsular Arabs are particularly enriched versus other ancestries (5.8-fold). On average, 52.3 loss-of-function variants were found per genome, 6.5 of which affect a known Mendelian gene. Several variants annotated in ClinVar/HGMD as pathogenic appeared at intermediate frequencies in this cohort (1–3%), highlighting Arab founder effect, while others have exceedingly high frequencies (> 5%) prompting reconsideration as benign. Furthermore, cumulative gene burden analysis revealed 56 genes having gene carrier frequency > 1/50, including 5 ACMG Tier 3 panel genes which would be candidates for adding to newborn screening in the country. Additionally, leveraging 58 biobank traits, we systematically assess the impact of novel/rare variants on phenotypes and discover 39 candidate large-effect variants associating with extreme quantitative traits. Furthermore, through rare variant burden testing, we discover 13 genes with high mutational load, including 5 with impact on traits relevant to disease conditions, including metabolic disorder and type 2 diabetes, consistent with the high prevalence of these conditions in the region. Conclusions: This study on the first phase of the growing Qatar Genome Program cohort provides a comprehensive resource from a Middle Eastern population to understand the global mutational burden in Mendelian genes and their impact on traits in seemingly healthy individuals in high consanguinity settings.

AB - Background: Genome sequencing of large biobanks from under-represented ancestries provides a valuable resource for the interrogation of Mendelian disease burden at world population level, complementing small-scale familial studies. Methods: Here, we interrogate 6045 whole genomes from Qatar—a Middle Eastern population with high consanguinity and understudied mutational burden—enrolled at the national Biobank and phenotyped for 58 clinically-relevant quantitative traits. We examine a curated set of 2648 Mendelian genes from 20 panels, annotating known and novel pathogenic variants and assessing their penetrance and impact on the measured traits. Results: We find that 62.5% of participants are carriers of at least 1 known pathogenic variant relating to recessive conditions, with homozygosity observed in 1 in 150 subjects (0.6%) for which Peninsular Arabs are particularly enriched versus other ancestries (5.8-fold). On average, 52.3 loss-of-function variants were found per genome, 6.5 of which affect a known Mendelian gene. Several variants annotated in ClinVar/HGMD as pathogenic appeared at intermediate frequencies in this cohort (1–3%), highlighting Arab founder effect, while others have exceedingly high frequencies (> 5%) prompting reconsideration as benign. Furthermore, cumulative gene burden analysis revealed 56 genes having gene carrier frequency > 1/50, including 5 ACMG Tier 3 panel genes which would be candidates for adding to newborn screening in the country. Additionally, leveraging 58 biobank traits, we systematically assess the impact of novel/rare variants on phenotypes and discover 39 candidate large-effect variants associating with extreme quantitative traits. Furthermore, through rare variant burden testing, we discover 13 genes with high mutational load, including 5 with impact on traits relevant to disease conditions, including metabolic disorder and type 2 diabetes, consistent with the high prevalence of these conditions in the region. Conclusions: This study on the first phase of the growing Qatar Genome Program cohort provides a comprehensive resource from a Middle Eastern population to understand the global mutational burden in Mendelian genes and their impact on traits in seemingly healthy individuals in high consanguinity settings.

KW - Arab population

KW - Biobank

KW - Consanguinity

KW - Genome sequencing

KW - Mendelian disorders

KW - Middle East

KW - Pathogenic variants

KW - Qatar

KW - Rare genetic disease

UR - https://www.scopus.com/pages/publications/85189641836

U2 - 10.1186/s13073-024-01307-6

DO - 10.1186/s13073-024-01307-6

M3 - Article

C2 - 38584274

AN - SCOPUS:85189641836

SN - 1756-994X

VL - 16

JO - Genome Medicine

JF - Genome Medicine

IS - 1

M1 - 46

ER -

The Qatar Genome Program Research Consortium, Biobank and Sample Preparation, Sequencing and Genotyping group, Applied Bioinformatics Core, Data Management and Computing Infrastructure group, Consortium Lead Principal Investigators (in alphabetical order). Burden of Mendelian disorders in a large Middle Eastern biobank. Genome Medicine. 2024 Apr 8;16(1):46. doi: 10.1186/s13073-024-01307-6

Burden of Mendelian disorders in a large Middle Eastern biobank

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