Fluorescence-Based Detection of Ferrous Iron in Senescent Cells

铁质 细胞内 生物标志物 衰老 荧光 体外 细胞生物学 老化 化学 细胞 缺铁 生物物理学 活性氧 生物化学 生物 医学 内科学 遗传学 有机化学 物理 量子力学 贫血
作者
Kyle J. Parella,Charles Manhardt,Danny Capucilli,Brandon S. Moyer,Hanna Colegrove,Kelsey Moody,Meegan B. Sleeper,Andrew Bañas,Abdelhadi Rebbaa,Aaron J. Wolfe
出处
期刊:Rejuvenation Research [Mary Ann Liebert, Inc.]
卷期号:24 (6): 456-463 被引量:6
标识
DOI:10.1089/rej.2021.0075
摘要

A major limitation in aging research is the lack of reliable biomarkers to assess phenotypic changes with age or monitor response to antiaging interventions. This study investigates the role of intracellular ferrous iron (Fe2+) as a potential biomarker of senescence. Iron is known to accumulate in various tissues with age and recent studies have demonstrated that its level increases dramatically in senescent cells. The current techniques used to measure the accumulation of iron are cumbersome and only measure total iron not specific isotopes such as the redox reactive Fe2+. It is still to be determined whether the damaging form of iron (Fe2+) is specifically elevated in senescent cells. In this study, we assessed the potential use of a newly discovered Fe2+ reactive probe (SiRhoNox-1) for selective labeling of senescent cells in vitro. For this we have generated various senescent cell models and subjected them to SiRhoNox-1 labeling. Our results indicate that SiRhoNox-1 selectivity labels live senescent cells and was more specific and faster than current staining such as SA-βGal or a derived fluorescent probe C12FDG. Together these findings suggest that SiRhoNox-1 may serve as a convenient tool to detect senescent cells based on their ferrous iron level.

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