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Senolytics rejuvenate aging cardiomyopathy in human cardiac organoids. | LitMetric

AI Article Synopsis

  • - Human cardiac organoids (hCardioids) are used to closely mimic the human heart for studying age-related heart conditions and the effects of senolytic therapies, which could potentially reverse aging-related cardiomyopathy.
  • - In the experiment, hCardioids treated with the chemotherapy drug doxorubicin (DOXO) showed increased signs of aging, such as oxidative stress and reduced heart cell proliferation, confirming an age-related decline in heart function.
  • - The combination treatment of two senolytics, dasatinib and quercetin, successfully reversed the aging effects in hCardioids, improving their function, reducing markers of cellular aging, and restoring the population of cardiac progenitor cells, indicating a potential therapeutic

Article Abstract

Background: Human cardiac organoids closely replicate the architecture and function of the human heart, offering a potential accurate platform for studying cellular and molecular features of aging cardiomyopathy. Senolytics have shown potential in addressing age-related pathologies but their potential to reverse aging-related human cardiomyopathy remains largely unexplored.

Methods: We employed human iPSC-derived cardiac organoids (hCOs/hCardioids) to model doxorubicin(DOXO)-induced cardiomyopathy in an aged context. hCardioids were treated with DOXO and subsequently with a combination of two senolytics: dasatinib (D) and quercetin (Q).

Results: DOXO-treated hCardioids exhibited significantly increased oxidative stress, DNA damage (pH2AX), cellular senescence (p16) and decreased cell proliferation associated with a senescence-associated secretory phenotype (SASP). DOXO-treated hCardioids were considerably deprived of cardiac progenitors and displayed reduced cardiomyocyte proliferation as well as contractility. These distinctive aging-associated characteristics were confirmed by global RNA-sequencing analysis. Treatment with D+Q reversed these effects, reducing oxidative stress and senescence markers, alleviating SASP, and restoring hCardioids viability and function. Additionally, senolytics replenished cardiac progenitors and reversed the cardiomyocyte proliferation deficit.

Conclusions: Doxorubicin triggers an age-associated phenotype in hCardioids reliably modelling the main cellular and molecular features of aging cardiomyopathy. Senescence is a key mechanism of the aged-hCOs phenotype as senolytics rejuvenated aged-hCardioids restoring their structure and function while reverting the age-associated regenerative deficit.

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Source
http://dx.doi.org/10.1016/j.mad.2024.112007DOI Listing

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