Selenoproteins and the senescence-associated epitranscriptome

Author:

Lee May Y12,Ojeda-Britez Stephen1,Ehrbar Dylan234,Samwer Antonia5,Begley Thomas J234,Melendez J Andres12ORCID

Affiliation:

1. College of Nanoscale Science and Engineering, SUNY Polytechnic Institute, Albany, NY 12203, USA

2. The RNA Institute, University at Albany, Albany, NY 12222, USA

3. Department of Biological Sciences, University at Albany, Albany, NY 12222, USA

4. RNA Epitranscriptomics and Proteomics Resource, University at Albany, Albany, NY 12222, USA

5. Munich International School, Starnberg 82319, Germany

Abstract

Selenium is a naturally found trace element, which provides multiple benefits including antioxidant, anticancer, and antiaging, as well as boosting immunity. One unique feature of selenium is its incorporation as selenocysteine, a rare 21st amino acid, into selenoproteins. Twenty-five human selenoproteins have been discovered, and a majority of these serve as crucial antioxidant enzymes for redox homeostasis. Unlike other amino acids, incorporation of selenocysteine requires a distinctive UGA stop codon recoding mechanism. Although many studies correlating selenium, selenoproteins, aging, and senescence have been performed, it has not yet been explored if the upstream events regulating selenoprotein synthesis play a role in senescence-associated pathologies. The epitranscriptomic writer alkylation repair homolog 8 (ALKBH8) is critical for selenoprotein production, and its deficiency can significantly decrease levels of selenoproteins that are essential for reactive oxygen species (ROS) detoxification, and increase oxidative stress, one of the major drivers of cellular senescence. Here, we review the potential role of epitranscriptomic marks that govern selenocysteine utilization in regulating the senescence program.

Funder

National Institute of General Medical Sciences

National Institute of Environmental Health Sciences

New York Sate Center for Advanced Technology in Nanomaterial and Nanoelectronics

Publisher

SAGE Publications

Subject

General Biochemistry, Genetics and Molecular Biology

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