AI Article Synopsis

  • The study investigates the role of club cells, a type of airway epithelial cell, in lung defense, suggesting there are different subpopulations with specific functions.
  • Researchers used single-cell RNA sequencing to identify three distinct types of club cells: progenitor, proliferating, and effector, each with unique characteristics and roles within lung tissue.
  • The findings indicate that smoking negatively impacts the differentiation and function of these club cell subpopulations, leading to fewer effector cells and more mucus-producing cells, which may contribute to lung health issues in smokers.

Article Abstract

The club cell, a small airway epithelial (SAE) cell, plays a central role in human lung host defense. We hypothesized that subpopulations of club cells with distinct functions may exist. The SAE of healthy nonsmokers and healthy cigarette smokers were evaluated by single-cell RNA sequencing, and unsupervised clustering revealed subpopulations of SCGCB1A1KRT5MUC5AC club cells. Club cell heterogeneity was supported by evaluations of SAE tissue sections, brushed SAE cells, and in vitro air-liquid interface cultures. Three subpopulations included: (1) progenitor; (2) proliferating; and (3) effector club cells. The progenitor club cell population expressed high levels of mitochondrial, ribosomal proteins, and KRT5 relative to other club cell populations and included a differentiation branch point leading to mucous cell production. The small proliferating population expressed high levels of cyclins and proliferation markers. The effector club cell cluster expressed genes related to host defense, xenobiotic metabolism, and barrier functions associated with club cell function. Comparison of smokers vs. nonsmokers demonstrated that smoking limited the extent of differentiation of all three subclusters and altered SAM pointed domain-containing Ets transcription factor (SPDEF)-regulated transcription in the effector cell population leading to a change in the location of the branch point for mucous cell production, a potential explanation for the concomitant reduction in effector club cells and increase in mucous cells in smokers. These observations provide insights into both the makeup of human SAE club cell subpopulations and the smoking-induced changes in club cell biology.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8426481PMC
http://dx.doi.org/10.1038/s41525-021-00237-1DOI Listing

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