Genome, HLA and polygenic risk score analyses for prevalent and persistent cervical human papillomavirus (HPV) infections

Author:

Adebamowo Sally N.ORCID,Adeyemo AdebowaleORCID,Adebayo Amos,Achara Peter,Alabi Bunmi,Bakare Rasheed A.,Famooto Ayotunde O.,Obende Kayode,Offiong Richard,Olaniyan Olayinka,Ologun Sanni,Rotimi CharlesORCID,Abdullahi Saurayya S.,Abdulsalam Maryam,Adebiyi Ruxton,Adekanmbi Victor,Adelekun Bukunmi,Adeyemo Segun,Akabueze Gerald,Akpobome Bernice,Akpomiemie Stella,Alabi Gabriel O.,Anichebe Chinyere,Anyanwu Claire,Ayogu Miriam C.,Bako Dorcas J.,Bamisaiye Patience,Blessing Nkechi U.,Chinye Osa A.,Dakum Patrick,Dareng Eileen,Dwana Grace,Erhunmwonsere Juliet I.,Eze Emelda O.,Fagbohun Tolani A.,Filade Temitope,Gbolahan Toluwalope,Anaedobe Gloria C.,Ibezim Stella,Iwaloye Racheal,James Jesse,Kehinde Dayo,Makinde Fiyinfoluwa,Mase Jessica,Mensah Charles,Nwoko Florence A.,Obende Kayode,Odonye George,Odubore Folake,Odunyemi Funmi,Odutola Michael,Oguama Uzoamaka,Oguoma Tochukwu,Oladimeji Temitayo,Olawande Toyosi,Olukomogbon Temitope,Oluwole Sefunmi,Omenuko Gladys,Onwuka Nkiruka,Owoade Yinka,Ugorji Thelma C.,Yohanna Syntyche,Yusuf Ibrahim,Adebamowo Clement A.ORCID,

Abstract

AbstractGenetic variants that underlie susceptibility to cervical high-risk human papillomavirus (hrHPV) infections are largely unknown. We conducted discovery genome-wide association studies (GWAS), replication, meta-analysis and colocalization, generated polygenic risk scores (PRS) and examined the association of classical HLA alleles and cervical hrHPV infections in a cohort of over 10,000 women. We identified genome-wide significant variants for prevalent hrHPV around LDB2 and for persistent hrHPV near TPTE2, SMAD2, and CDH12, which code for proteins that are significantly expressed in the human endocervix. Genetic variants associated with persistent hrHPV are in genes enriched for the antigen processing and presentation gene set. HLA-DRB1*13:02, HLA-DQB1*05:02 and HLA-DRB1*03:01 were associated with increased risk, and HLA-DRB1*15:03 was associated with decreased risk of persistent hrHPV. The analyses of peptide binding predictions showed that HLA-DRB1 alleles that were positively associated with persistent hrHPV showed weaker binding with peptides derived from hrHPV proteins and vice versa. The PRS for persistent hrHPV with the best model fit, had a P-value threshold (PT) of 0.001 and a p-value of 0.06 (-log10(0.06) = 1.22). The findings of this study expand our understanding of genetic risk factors for hrHPV infection and persistence and highlight the roles of MHC class II molecules in hrHPV infection.

Publisher

Springer Science and Business Media LLC

Subject

Genetics (clinical),Genetics

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