Litcius/Paper detail

Selective ablation of primary and paracrine senescent cells by targeting iron dyshomeostasis

Tesfahun Dessale Admasu, Kristie Kim, Michael Rae, Roberto A. Avelar, Ryan L. Gonciarz, Abdelhadi Rebbaa, João Pedro de Magalhães, Adam R. Renslo, Alexandra Stolzing, Amit Sharma

2023Cell Reports45 citationsDOIOpen Access PDF

Abstract

Senescent cells can spread the senescent phenotype to other cells by secreting senescence-associated secretory phenotype factors. The resulting paracrine senescent cells make a significant contribution to the burden of senescent cell accumulation with age. Previous efforts made to characterize paracrine senescence are unreliable due to analyses being based on mixed populations of senescent and non-senescent cells. Here, we use dipeptidyl peptidase-4 (DPP4) as a surface maker to isolate senescent cells from mixed populations. Using this technique, we enrich the percentage of paracrine senescence from 40% to 85%. We then use this enriched culture to characterize DPP4 + primary and paracrine senescent cells. We observe ferroptosis dysregulation and ferrous iron accumulation as a common phenomenon in both primary and paracrine senescent cells. Finally, we identify ferroptosis induction and ferrous iron-activatable prodrug as a broad-spectrum senolytic approach to ablate multiple types of primary and paracrine senescent cells.

Topics & Concepts

Paracrine signallingSenescenceCell biologyPhenotypeBiologyGeneticsGeneReceptorTelomeres, Telomerase, and SenescenceFerroptosis and cancer prognosisMicroRNA in disease regulation