Supramolecular Senolytics via Intracellular Oligomerization of Peptides in Response to Elevated Reactive Oxygen Species Levels in Aging Cells

化学 细胞生物学 细胞内 线粒体 活性氧 自噬 细胞凋亡 视网膜色素上皮 视网膜 生物化学 生物
作者
Sangpil Kim,Jae‐Byoung Chae,Dohyun Kim,Chulwoo Park,Youjung Sim,Hyungwoo Lee,Gaeun Park,Jae-Eun Lee,Seong‐Ho Hong,Batakrishna Jana,Chaekyu Kim,Hyewon Chung,Ja‐Hyoung Ryu
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:145 (40): 21991-22008 被引量:19
标识
DOI:10.1021/jacs.3c06898
摘要

Senolytics, which eliminate senescent cells from tissues, represent an emerging therapeutic strategy for various age-related diseases. Most senolytics target antiapoptotic proteins, which are overexpressed in senescent cells, limiting specificity and inducing severe side effects. To overcome these limitations, we constructed self-assembling senolytics targeting senescent cells with an intracellular oligomerization system. Intracellular aryl-dithiol-containing peptide oligomerization occurred only inside the mitochondria of senescent cells due to selective localization of the peptides by RGD-mediated cellular uptake into integrin αvβ3-overexpressed senescent cells and elevated levels of reactive oxygen species, which can be used as a chemical fuel for disulfide formation. This oligomerization results in an artificial protein-like nanoassembly with a stable α-helix secondary structure, which can disrupt the mitochondrial membrane via multivalent interactions because the mitochondrial membrane of senescent cells has weaker integrity than that of normal cells. These three specificities (integrin αvβ3, high ROS, and weak mitochondrial membrane integrity) of senescent cells work in combination; therefore, this intramitochondrial oligomerization system can selectively induce apoptosis of senescent cells without side effects on normal cells. Significant reductions in key senescence markers and amelioration of retinal degeneration were observed after elimination of the senescent retinal pigment epithelium by this peptide senolytic in an age-related macular degeneration mouse model and in aged mice, and this effect was accompanied by improved visual function. This system provides a strategy for the treatment of age-related diseases using supramolecular senolytics.
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