4.7 Article

Transcriptional changes of the aging lung

Journal

AGING CELL
Volume 22, Issue 10, Pages -

Publisher

WILEY
DOI: 10.1111/acel.13969

Keywords

aging; inflammation; lung; senescence; single-cell RNA-seq

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This study provides a comprehensive and systemic analysis of the molecular signatures of lung aging using single-cell gene expression analysis. The research reveals that aging has a heterogeneous effect on lung cells, with some populations showing more transcriptional changes while others remain stable. The findings also highlight the importance of inflammation and immune response regulation in age-related lung pathologies.
Aging is a natural process associated with declined organ function and higher susceptibility to developing chronic diseases. A systemic single-cell type-based study provides a unique opportunity to understand the mechanisms behind age-related pathologies. Here, we use single-cell gene expression analysis comparing healthy young and aged human lungs from nonsmoker donors to investigate age-related transcriptional changes. Our data suggest that aging has a heterogenous effect on lung cells, as some populations are more transcriptionally dynamic while others remain stable in aged individuals. We found that monocytes and alveolar macrophages were the most transcriptionally affected populations. These changes were related to inflammation and regulation of the immune response. Additionally, we calculated the LungAge score, which reveals the diversity of lung cell types during aging. Changes in DNA damage repair, fatty acid metabolism, and inflammation are essential for age prediction. Finally, we quantified the senescence score in aged lungs and found that the more biased cells toward senescence are immune and progenitor cells. Our study provides a comprehensive and systemic analysis of the molecular signatures of lung aging. Our LungAge signature can be used to predict molecular signatures of physiological aging and to detect common signatures of age-related lung diseases.

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