MADloy: Robust Detection of Mosaic Loss of Chromosome Y from Genotype-array-intensity Data

Overview

Journal BMC Bioinformatics

Publisher Biomed Central

Specialty Biology

Date 2020 Nov 23

PMID 33225898

Citations 4

Authors

Juan R Gonzalez

Marcos Lopez-Sanchez

Alejandro Caceres

Pere Puig

Tonu Esko

Luis A Perez-Jurado

Affiliations

Soon will be listed here.

Abstract

Background: Accurate protocols and methods to robustly detect the mosaic loss of chromosome Y (mLOY) are needed given its reported role in cancer, several age-related disorders and overall male mortality. Intensity SNP-array data have been used to infer mLOY status and to determine its prominent role in male disease. However, discrepancies of reported findings can be due to the uncertainty and variability of the methods used for mLOY detection and to the differences in the tissue-matrix used.

Results: We created a publicly available software tool called MADloy (Mosaic Alteration Detection for LOY) that incorporates existing methods and includes a new robust approach, allowing efficient calling in large studies and comparisons between methods. MADloy optimizes mLOY calling by correctly modeling the underlying reference population with no-mLOY status and incorporating B-deviation information. We observed improvements in the calling accuracy to previous methods, using experimentally validated samples, and an increment in the statistical power to detect associations with disease and mortality, using simulation studies and real dataset analyses. To understand discrepancies in mLOY detection across different tissues, we applied MADloy to detect the increment of mLOY cellularity in blood on 18 individuals after 3 years and to confirm that its detection in saliva was sub-optimal (41%). We additionally applied MADloy to detect the down-regulation genes in the chromosome Y in kidney and bladder tumors with mLOY, and to perform pathway analyses for the detection of mLOY in blood.

Conclusions: MADloy is a new software tool implemented in R for the easy and robust calling of mLOY status across different tissues aimed to facilitate its study in large epidemiological studies.

Citing Articles

Clonal chromosomal mosaicism and loss of chromosome Y in elderly men increase vulnerability for SARS-CoV-2.

Perez-Jurado L, Caceres A, Balague-Dobon L, Esko T, de Heredia M, Quintela I Commun Biol. 2024; 7(1):202.

PMID: 38374351 PMC: 10876565. DOI: 10.1038/s42003-024-05805-6.

Y chromosome loss in cancer drives growth by evasion of adaptive immunity.

Abdel-Hafiz H, Schafer J, Chen X, Xiao T, Gauntner T, Li Z Nature. 2023; 619(7970):624-631.

PMID: 37344596 PMC: 10975863. DOI: 10.1038/s41586-023-06234-x.

Mendelian Randomisation Confirms the Role of Y-Chromosome Loss in Alzheimer's Disease Aetiopathogenesis in Men.

Garcia-Gonzalez P, de Rojas I, Moreno-Grau S, Montrreal L, Puerta R, Alarcon-Martin E Int J Mol Sci. 2023; 24(2).

PMID: 36674414 PMC: 9863537. DOI: 10.3390/ijms24020898.

Fully exploiting SNP arrays: a systematic review on the tools to extract underlying genomic structure.

Balague-Dobon L, Caceres A, Gonzalez J Brief Bioinform. 2022; 23(2).

PMID: 35211719 PMC: 8921734. DOI: 10.1093/bib/bbac043.

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