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Loss of Y chromosome: An emerging next-generation biomarker for disease prediction and early detection?

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ELSEVIER
DOI: 10.1016/j.mrrev.2021.108389

关键词

Mosaic chromosomal alterations; Genomic instability; Clonal mosaicism; Micronuclei; Mosaic loss of X chromosome; Extreme downregulation of Y chromosome

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Mosaic loss of Y chromosome (LOY) in blood cells is a significant risk factor for future mortality and various diseases in males. LOY has the potential to be a novel biomarker for genomics-driven disease prediction and early detection.
As human life expectancy increases substantially and aging is the primary risk factor for most chronic diseases, there is an urgent need for advancing the development of post-genomic era biomarkers that can be used for disease prediction and early detection (DPED). Mosaic loss of Y chromosome (LOY) is the state of nullisomy Y in sub-groups of somatic cells acquired from different post-zygotic development stages and onwards throughout the lifespan. Multiple large-cohort based epidemiology studies have found that LOY in blood cells is a significant risk factor for future mortality and various diseases in males. Many features intrinsic to LOY analysis may be leveraged to enhance its use as a non-invasive, sensitive, reliable, high throughput-biomarker for DPED. Here, we review the emerging literatures in LOY studies and highlight ten strengths for using LOY as a novel biomarker for genomics-driven DPED diagnostics. Meanwhile, the current limitations in this area are also discussed. We conclude by identifying some important knowledge gaps regarding the consequences of malsegregation of the Y chromosome and propose further steps that are required before clinical implementation of LOY. Taken together, we think that LOY has substantial potential as a biomarker for DPED, despite some hurdles that still need to be addressed before its integration into healthcare becomes acceptable.

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