Krt14 and Krt15 differentially regulate regenerative properties and differentiation potential of airway basal cells

Keratin expression dynamically changes in airway basal cells (BCs) after acute and chronic injury, yet the functional consequences of these changes on BC behavior remain unknown. In bronchiolitis obliterans (BO) after lung transplantation, BC clonogenicity declines, which is associated with a switch...

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Published inJCI insight Vol. 8; no. 2
Main Authors Ievlev, Vitaly, Lynch, Thomas J, Freischlag, Kyle W, Gries, Caitlyn B, Shah, Anit, Pai, Albert C, Ahlers, Bethany A, Park, Soo, Engelhardt, John F, Parekh, Kalpaj R
Format Journal Article
LanguageEnglish
Published United States American Society for Clinical Investigation 24.01.2023
American Society for Clinical investigation
Subjects
Animals
Bronchiolitis Obliterans
Cell Differentiation
Keratins
Lung Transplantation
Mice
Phenotype
Pulmonology
Stem cells
Pulmonology
Adult stem cells
Respiration
Mouse models
Stem cells
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Summary:Keratin expression dynamically changes in airway basal cells (BCs) after acute and chronic injury, yet the functional consequences of these changes on BC behavior remain unknown. In bronchiolitis obliterans (BO) after lung transplantation, BC clonogenicity declines, which is associated with a switch from keratin15 (Krt15) to keratin14 (Krt14). We investigated these keratins' roles using Crispr-KO in vitro and in vivo and found that Krt14-KO and Krt15-KO produce contrasting phenotypes in terms of differentiation and clonogenicity. Primary mouse Krt14-KO BCs did not differentiate into club and ciliated cells but had enhanced clonogenicity. By contrast, Krt15-KO did not alter BC differentiation but impaired clonogenicity in vitro and reduced the number of label-retaining BCs in vivo after injury. Krt14, but not Krt15, bound the tumor suppressor stratifin (Sfn). Disruption of Krt14, but not of Krt15, reduced Sfn protein abundance and increased expression of the oncogene dNp63a during BC differentiation, whereas dNp63a levels were reduced in Krt15-KO BCs. Overall, the phenotype of Krt15-KO BCs contrasts with Krt14-KO phenotype and resembles the phenotype in BO with decreased clonogenicity, increased Krt14, and decreased dNp63a expression. This work demonstrates that Krt14 and Krt15 functionally regulate BC behavior, which is relevant in chronic disease states like BO.
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ISSN:2379-3708
2379-3708
DOI:10.1172/jci.insight.162041