| Literature DB >> 35801078 |
Priyanka Banerjee1, Elizabeth A Olmsted-Davis1, Anita Deswal2, Minh Th Nguyen1,3, Efstratios Koutroumpakis2, Nicholas L Palaskas2, Steven H Lin4, Sivareddy Kotla2, Cielito Reyes-Gibby5, Sai-Ching J Yeung5, Syed Wamique Yusuf2, Momoko Yoshimoto6, Michihiro Kobayashi6, Bing Yu7, Keri Schadler8, Joerg Herrmann9, John P Cooke1, Abhishek Jain10, Eduardo Chini11, Nhat-Tu Le1, Jun-Ichi Abe2.
Abstract
Numerous studies have revealed the critical role of premature senescence induced by various cancer treatment modalities in the pathogenesis of aging-related diseases. Senescence-associated secretory phenotype (SASP) can be induced by telomere dysfunction. Telomeric DNA damage response induced by some cancer treatments can persist for months, possibly accounting for long-term sequelae of cancer treatments. Telomeric DNA damage-induced mitochondrial dysfunction and increased reactive oxygen species production are hallmarks of premature senescence. Recently, we reported that the nucleus-mitochondria positive feedback loop formed by p90 ribosomal S6 kinase (p90RSK) and phosphorylation of S496 on ERK5 (a unique member of the mitogen-activated protein kinase family that is not only a kinase but also a transcriptional co-activator) were vital signaling events that played crucial roles in linking mitochondrial dysfunction, nuclear telomere dysfunction, persistent SASP induction, and atherosclerosis. In this review, we will discuss the role of NAD+ depletion in instigating SASP and its downstream signaling and regulatory mechanisms that lead to the premature onset of atherosclerotic cardiovascular diseases in cancer survivors.Entities:
Keywords: ERK5; NAD+; cardiovascular diseases; p90RSK; senescence-associated secretory phenotype (SASP)
Year: 2022 PMID: 35801078 PMCID: PMC9258520 DOI: 10.20517/jca.2022.13
Source DB: PubMed Journal: J Cardiovasc Aging ISSN: 2768-5993