Keshri Riya, Detraux Damien, Phal Ashish, McCurdy Clara, Jhajharia Samriddhi, Chan Tung Ching, Mathieu Julie, Ruohola-Baker Hannele
Department of Biochemistry, School of Medicine, University of Washington, Seattle, WA, United States.
Institute for Stem Cell and Regenerative Medicine, School of Medicine, University of Washington, Seattle, WA, United States.
Front Cell Dev Biol. 2024 Feb 2;12:1343106. doi: 10.3389/fcell.2024.1343106. eCollection 2024.
Tissue repair is significantly compromised in the aging human body resulting in critical disease conditions (such as myocardial infarction or Alzheimer's disease) and imposing a tremendous burden on global health. Reprogramming approaches (partial or direct reprogramming) are considered fruitful in addressing this unmet medical need. However, the efficacy, cellular maturity and specific targeting are still major challenges of direct reprogramming. Here we describe novel approaches in direct reprogramming that address these challenges. Extracellular signaling pathways (Receptor tyrosine kinases, RTK and Receptor Serine/Theronine Kinase, RSTK) and epigenetic marks remain central in rewiring the cellular program to determine the cell fate. We propose that modern protein design technologies (AI-designed minibinders regulating RTKs/RSTK, epigenetic enzymes, or pioneer factors) have potential to solve the aforementioned challenges. An efficient transdifferentiation/direct reprogramming may in the future provide molecular strategies to collectively reduce aging, fibrosis, and degenerative diseases.
在衰老的人体中,组织修复能力显著受损,导致严重疾病(如心肌梗死或阿尔茨海默病),给全球健康带来巨大负担。重编程方法(部分重编程或直接重编程)被认为在满足这一未被满足的医疗需求方面卓有成效。然而,直接重编程的疗效、细胞成熟度和特异性靶向性仍是主要挑战。在此,我们描述了直接重编程中应对这些挑战的新方法。细胞外信号通路(受体酪氨酸激酶,RTK和受体丝氨酸/苏氨酸激酶,RSTK)和表观遗传标记在重新连接细胞程序以决定细胞命运方面仍然至关重要。我们认为现代蛋白质设计技术(人工智能设计的调节RTKs/RSTK、表观遗传酶或先驱因子的微型结合剂)有潜力解决上述挑战。高效的转分化/直接重编程未来可能会提供集体减少衰老、纤维化和退行性疾病的分子策略。
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