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Heterogeneity of Cellular Senescence, Senotyping, and Targeting by Senolytics and Senomorphics in Lung Diseases
Said Ali Ozdemir, Md Imam Faizan, Gagandeep Kaur, Sadiya Bi Shaikh, Khursheed Ul Islam, Irfan Rahman
International Journal of Molecular Sciences · 2025 · ▲ 9 citations
Genomic instability
Deregulated nutrient-sensing
Cellular senescence
Chronic inflammation
Rapamycin / mTOR inhibition
Metformin
Senolytics
Human
Review
Abstract
Cellular senescence(definition), a state of stable cell cycle arrest accompanied by a complex senescence-associated secretory phenotype (SASP), is a fundamental biological process implicated as a key driver of lung aging and lung age-related diseases (LARDs). This review provides a comprehensive overview of the rapidly evolving field of senotyping based on cellular heterogeneity in lung development and aging in health and disease. It also delves into the molecular mechanisms driving senescence and SASP production, highlighting pathways such as p53/p21, p16INK4a/RB, mTOR(definition), and p38 MAPK as therapeutic targets. The involvement of various novel SASP proteins, such as GDP15, cytokines/chemokines, growth factors, and DNA damage response proteins. We further highlight the effectiveness of senotherapeutics in mitigating the detrimental effects of senescent cell (SnC) accumulation within the lungs. It also outlines two main therapeutic approaches: senolytics(definition), which selectively trigger apoptosis in SnCs, and senomorphics (also known as senostatics), which mitigate the detrimental effects of the SASP without necessarily removing the senescent cells. Various classes of senolytic and senomorphic drugs are currently in clinical trials including natural products (e.g., quercetin, fisetin, resveratrol) and repurposed drugs (e.g., dasatinib, navitoclax, metformin, rapamycin(definition)) that has demonstrated therapeutic promise in improving tissue function, alleviating LARDs, and extending health span. We discuss the future of these strategies in lung research and further elaborate upon the usability of novel approaches including HSP90 inhibitors, senolytic CAR-T cells, Antibody drug conjugate and galactose-modified prodrugs in influencing the field of personalized medicine in future. Overall, this comprehensive review highlights the progress made so far and the challenges faced in the field of cellular senescence including SnC heterogeneity, states of senescence, senotyping, immunosenescence, drug delivery, target specificity, long-term safety, and the need for robust cell-based biomarkers. Future perspectives, such as advanced delivery systems, and combination therapies, are considered critical for translating the potential of senotherapeutics into effective clinical applications for age-related pulmonary diseases/conditions.
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- 10.3390/ijms26199687
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- 2026-06-15 MST
Cite this
APA
Ozdemir, S.A., Faizan, M.I., Kaur, G., Shaikh, S.B., Islam, K.U., & Rahman, I. (2025). Heterogeneity of Cellular Senescence, Senotyping, and Targeting by Senolytics and Senomorphics in Lung Diseases. <em>International Journal of Molecular Sciences</em>. https://doi.org/10.3390/ijms26199687
Vancouver
Ozdemir SA, Faizan MI, Kaur G, Shaikh SB, Islam KU, Rahman I. Heterogeneity of Cellular Senescence, Senotyping, and Targeting by Senolytics and Senomorphics in Lung Diseases. International Journal of Molecular Sciences. 2025. doi:10.3390/ijms26199687.
BibTeX
@article{said2025Hetero,
title = {Heterogeneity of Cellular Senescence, Senotyping, and Targeting by Senolytics and Senomorphics in Lung Diseases},
author = {Said Ali Ozdemir and Md Imam Faizan and Gagandeep Kaur and Sadiya Bi Shaikh and Khursheed Ul Islam and Irfan Rahman},
journal = {International Journal of Molecular Sciences},
year = {2025},
doi = {10.3390/ijms26199687},
}
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