Intermittent exposure to whole cigarette smoke alters the differentiation of primary small airway epithelial cells in the air-liquid interface culture

Gindele, Julia A.; Kiechle, Tobias; Benediktus, Kerstin; Birk, Gerald; Brendel, Michael; Heinemann, Fabian; Wohnhaas, Christian T.; LeBlanc, Michelle; Zhang, Haijun; Schymeinsky, Jürgen

Intermittent exposure to whole cigarette smoke alters the differentiation of primary small airway epithelial cells in the air-liquid interface culture

Dateien

Gindele_2-fbi23l1hryuo3.pdfGröße: 6.37 MBDownloads: 211

Datum

2020

URI (zitierfähiger Link)

http://nbn-resolving.de/urn:nbn:de:bsz:352-2-fbi23l1hryuo3

DOI (zitierfähiger Link)

https://doi.org/10.1038/s41598-020-63345-5

Open Access-Veröffentlichung

Open Access Gold

Publikationstyp

Zeitschriftenartikel

Publikationsstatus

Published

Erschienen in

Scientific Reports. Springer Nature. 2020, 10, 6257. eISSN 2045-2322. Available under: doi: 10.1038/s41598-020-63345-5

Zusammenfassung

Cigarette smoke (CS) is the leading risk factor to develop COPD. Therefore, the pathologic effects of whole CS on the differentiation of primary small airway epithelial cells (SAEC) were investigated, using cells from three healthy donors and three COPD patients, cultured under ALI (air-liquid interface) conditions. The analysis of the epithelial physiology demonstrated that CS impaired barrier formation and reduced cilia beat activity. Although, COPD-derived ALI cultures preserved some features known from COPD patients, CS-induced effects were similarly pronounced in ALI cultures from patients compared to healthy controls. RNA sequencing analyses revealed the deregulation of marker genes for basal and secretory cells upon CS exposure. The comparison between gene signatures obtained from the in vitro model (CS vs. air) with a published data set from human epithelial brushes (smoker vs. non-smoker) revealed a high degree of similarity between deregulated genes and pathways induced by CS. Taken together, whole cigarette smoke alters the differentiation of small airway basal cells in vitro. The established model showed a good translatability to the situation in vivo. Thus, the model can help to identify and test novel therapeutic approaches to restore the impaired epithelial repair mechanisms in COPD, which is still a high medical need.

Fachgebiet (DDC)

570 Biowissenschaften, Biologie

Zitieren

ISO 690

GINDELE, Julia A., Tobias KIECHLE, Kerstin BENEDIKTUS, Gerald BIRK, Michael BRENDEL, Fabian HEINEMANN, Christian T. WOHNHAAS, Michelle LEBLANC, Haijun ZHANG, Jürgen SCHYMEINSKY, 2020. Intermittent exposure to whole cigarette smoke alters the differentiation of primary small airway epithelial cells in the air-liquid interface culture. In: Scientific Reports. Springer Nature. 2020, 10, 6257. eISSN 2045-2322. Available under: doi: 10.1038/s41598-020-63345-5

BibTex

@article{Gindele2020-04-10Inter-51355,
  year={2020},
  doi={10.1038/s41598-020-63345-5},
  title={Intermittent exposure to whole cigarette smoke alters the differentiation of primary small airway epithelial cells in the air-liquid interface culture},
  volume={10},
  journal={Scientific Reports},
  author={Gindele, Julia A. and Kiechle, Tobias and Benediktus, Kerstin and Birk, Gerald and Brendel, Michael and Heinemann, Fabian and Wohnhaas, Christian T. and LeBlanc, Michelle and Zhang, Haijun and Schymeinsky, Jürgen},
  note={Article Number: 6257}
}

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    <dcterms:abstract xml:lang="eng">Cigarette smoke (CS) is the leading risk factor to develop COPD. Therefore, the pathologic effects of whole CS on the differentiation of primary small airway epithelial cells (SAEC) were investigated, using cells from three healthy donors and three COPD patients, cultured under ALI (air-liquid interface) conditions. The analysis of the epithelial physiology demonstrated that CS impaired barrier formation and reduced cilia beat activity. Although, COPD-derived ALI cultures preserved some features known from COPD patients, CS-induced effects were similarly pronounced in ALI cultures from patients compared to healthy controls. RNA sequencing analyses revealed the deregulation of marker genes for basal and secretory cells upon CS exposure. The comparison between gene signatures obtained from the in vitro model (CS vs. air) with a published data set from human epithelial brushes (smoker vs. non-smoker) revealed a high degree of similarity between deregulated genes and pathways induced by CS. Taken together, whole cigarette smoke alters the differentiation of small airway basal cells in vitro. The established model showed a good translatability to the situation in vivo. Thus, the model can help to identify and test novel therapeutic approaches to restore the impaired epithelial repair mechanisms in COPD, which is still a high medical need.</dcterms:abstract>
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Begutachtet

Ja