Effect of polygenic scores of telomere length alleles on telomere length in newborns and parents

Author:

Lee Yunsung1ORCID,Jugessur Astanand12,Gjessing Håkon K.12,Harris Jennifer R.1,Susser Ezra3,Magnus Per1,Aviv Abraham45ORCID

Affiliation:

1. Centre for Fertility and Health Norwegian Institute of Public Health Oslo Norway

2. Department of Global Public Health and Primary Care University of Bergen Bergen Norway

3. Mailman School of Public Health Columbia University, and New York State Psychiatric Institute New York New York USA

4. Center of Human Development and Aging, New Jersey Medical School Rutgers University Newark New Jersey USA

5. Department of Pediatrics, New Jersey Medical School Rutgers University Newark New Jersey USA

Abstract

AbstractIn adults, polygenic scores (PGSs) of telomere length (TL) alleles explain about 4.5% of the variance in TL, as measured by quantitative polymerase chain reaction (qPCR). Yet, these PGSs strongly infer a causal role of telomeres in aging‐related diseases. To better understand the determinants of TL through the lifespan, it is essential to examine to what extent these PGSs explain TL in newborns. This study investigates the effect of PGSs on TL in both newborns and their parents, with TL measured by Southern blotting and expressed in base‐pairs (bp). Additionally, the study explores the impact of PGSs related to transmitted or non‐transmitted alleles on TL in newborns. For parents and newborns, the PGS effects on TL were 172 bp (p =  2.03 × 10−15) and 161 bp (p =  3.06 × 10−8), explaining 6.6% and 5.2% of the TL variance, respectively. The strongest PGS effect was shown for maternally transmitted alleles in newborn girls, amounting to 214 bp (p =  3.77 × 10−6) and explaining 7.8% of the TL variance. The PGS effect of non‐transmitted alleles was 56 bp (p = 0.0593) and explained 0.6% of the TL variance. Our findings highlight the importance of TL genetics in understanding early‐life determinants of TL. They point to the potential utility of PGSs composed of TL alleles in identifying susceptibility to aging‐related diseases from birth and reveal the presence of sexual dimorphism in the effect of TL alleles on TL in newborns. Finally, we attribute the higher TL variance explained by PGSs in our study to TL measurement by Southern blotting.

Funder

National Institutes of Health

Norges Forskningsråd

Publisher

Wiley

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