Integrin α6β4 identifies an adult distal lung epithelial population with regenerative potential in mice

Chapman, Harold A.; Li, Xiaopeng; Alexander, Jonathan P.; Brumwell, Alexis; Lorizio, Walter; Tan, Kevin S. W.; Sonnenberg, Arnoud; Wei, Ying; Vu, Thiennu H.

doi:10.1172/jci57673

Cited by 387 publications

(277 citation statements)

References 27 publications

(30 reference statements)

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“…However, a new study showed that cells labeled with the Scgb1a1CREER contribute extensively to the alveoli regener ation after bleomycininduced lung injury, suggesting that the contribution of Clara cells to lung regeneration can vary depend ing on the type of injury . Consistent with the role of Scgb1a1+ cells during lung repair after bleomycin induced injury, lineage tracing of alveolar type 2 cells using SPCCREER demonstrated that SPCderived cells are re placed by SPCnegative progenitors during lung repair after bleomycin inhalation (Chapman et al, 2011). K14CREER lin eage tracing suggested that K14/K5positive cells appear in the bronchioles a few days postinfection of H1N1 virus and give rise to migrating K5positive clusters of cells at the sites of interbronchiolar lung damage (Kumar et al, 2011).…”

Section: The Airway Systemmentioning

confidence: 73%

Tracing epithelial stem cells during development, homeostasis, and repair

Keymeulen¹,

Blanpain²

2012

J Exp Med

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Section: The Airway Systemmentioning

confidence: 73%

Tracing epithelial stem cells during development, homeostasis, and repair

Keymeulen¹,

Blanpain²

2012

J Exp Med

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“…In the alveolar space, where gas exchange is carried out by alveolar epithelial type 1 (AT1) cells, the surfactant-expressing AT2 cells can function as stem cells 60,142 . Another alveolar cell population, expressing α6β4 integrin, can also produce alveolar epithelia 142,143 . Bronchioalveolar stem cells (BASCs), which reside between the airway and alveolar space, can give rise to both epithelial lineages 56,114,144–146 .…”

Section: Figurementioning

confidence: 99%

Non-small-cell lung cancers: a heterogeneous set of diseases

et al. 2014

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Non-small-cell lung cancers (NSCLCs), the most common lung cancers, are known to have diverse pathological features. During the past decade, in-depth analyses of lung cancer genomes and signalling pathways have further defined NSCLCs as a group of distinct diseases with genetic and cellular heterogeneity. Consequently, an impressive list of potential therapeutic targets was unveiled, drastically altering the clinical evaluation and treatment of patients. Many targeted therapies have been developed with compelling clinical proofs of concept; however, treatment responses are typically short-lived. Further studies of the tumour microenvironment have uncovered new possible avenues to control this deadly disease, including immunotherapy.

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“…To determine which of the mesenchymal lineages identified preferentially promote alveolar cell growth and self-renewal, alveolar organoid assays were performed using mature AT2 cells isolated from Sftpc CreERT2 : R26R EYFP adult mice (Barkauskas et al, 2013; Chapman et al, 2011). The five different mesenchymal lineages or populations were combined with AT2 cells to form organoids and were subsequently counted, sectioned for IHC, and isolated for gene expression analysis (Fig.…”

Section: Resultsmentioning

confidence: 99%

Distinct Mesenchymal Lineages and Niches Promote Epithelial Self-Renewal and Myofibrogenesis in the Lung

Zepp

Zacharias

Frank

et al. 2017

Cell

462

559

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The lung is an architecturally complex organ comprised of a heterogeneous mixture of various epithelial and mesenchymal lineages. We have used single-cell RNA-sequencing and signaling lineage reporters to generate a spatial and transcriptional map of the lung mesenchyme. We find that each mesenchymal lineage has a distinct spatial address and transcriptional profile leading to unique niche regulatory functions. The Mesenchymal Alveolar Niche Cell is Wnt responsive, expresses Pdgfrα, and is critical for alveolar epithelial cell growth and self-renewal. In contrast, the Axin2+ Myofibrogenic Progenitor cell preferentially generates pathologically deleterious myofibroblasts after injury. Analysis of the secretome and receptome of the alveolar niche reveals functional pathways that mediate growth and self-renewal of alveolar type 2 progenitor cells including IL-6/Stat3, Bmp, and Fgf signaling. These studies define the cellular and molecular framework of lung mesenchymal niches and reveal the functional importance of developmental pathways promoting self-renewal versus pathological response to tissue injury.

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Integrin α6β4 identifies an adult distal lung epithelial population with regenerative potential in mice

Cited by 387 publications

References 27 publications

Tracing epithelial stem cells during development, homeostasis, and repair

Tracing epithelial stem cells during development, homeostasis, and repair

Non-small-cell lung cancers: a heterogeneous set of diseases

Distinct Mesenchymal Lineages and Niches Promote Epithelial Self-Renewal and Myofibrogenesis in the Lung

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