Resident Interstitial Lung Fibroblasts and their Role in Alveolar Stem Cell Niche Development, Homeostasis, Injury, and Regeneration

Ushakumary, Mereena George; Riccetti, Matthew; Perl, Anne‐Karina T.

doi:10.1002/sctm.20-0526

Cited by 64 publications

(47 citation statements)

References 160 publications

(219 reference statements)

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“…For example, understanding the nature and development of lipogenic versus myogenic fibroblast phenotypes might help to develop new therapeutic strategies for pulmonary diseases. Despite a large amount of data, there is still no established view on the grouping of iReFs, and researchers do this in different ways [26,46,93]. Moreover, many markers of these populations may overlap.…”

Section: Discussionmentioning

confidence: 99%

“…Myofibroblast TBX4 [12] ACTA2 [27] PDGFRA [27,[47][48][49] FGF18 [37] ELN [50,51] Matrix fibroblast COL13A1, COL14A1 [52] CD34 [46] PDGFRA [46] Lipofibroblast THY [53] FGF10 [18] TCF21 [54] PLIN2 (ADRP) [55] Leptin [56] PPARγ [57] PDGFRA [46,58] Alveolar niche cell AXIN2 [9] LGR5 [59] WNT2 [5] WNT5A [60] PDGFRA [61,62] In simple terms, one can say that as septa mature, SCMFs produce elastin, contract and ensure the elongation of the septal tips, SCMFs and matrix fibroblasts secrete metalloproteinases and ECM-forming and remodeling proteins to thin the septal tips and ensure structural support, while lipofibroblasts support AT2 cell surfactant production. At the end of alveolarization, adult alveolar niche stem cells become defined, consisting of the lipofibroblast-like MANCs, which support alveolar growth and regeneration [9,19,26,38,59,[63][64][65]. Recent lineage tracing and RNA sequencing (RNAseq) data identified Lgr5 + and Wnt-responsive/PDGFRα + mesenchymal cell subsets within alveolar niches that influence the differentiation of alveolar epithelial cells during repair of the mature lung [59,65].…”

Section: Irefs Type Suggested Markers For the Corresponding Iref Typementioning

confidence: 99%

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Alveologenesis: What Governs Secondary Septa Formation

Алпеева

Vasiliev

Vorotelyak

2021

IJMS

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The simplification of alveoli leads to various lung pathologies such as bronchopulmonary dysplasia and emphysema. Deep insight into the process of emergence of the secondary septa during development and regeneration after pneumonectomy, and into the contribution of the drivers of alveologenesis and neo-alveolarization is required in an efficient search for therapeutic approaches. In this review, we describe the formation of the gas exchange units of the lung as a multifactorial process, which includes changes in the actomyosin cytoskeleton of alveocytes and myofibroblasts, elastogenesis, retinoic acid signaling, and the contribution of alveolar mesenchymal cells in secondary septation. Knowledge of the mechanistic context of alveologenesis remains incomplete. The characterization of the mechanisms that govern the emergence and depletion of αSMA will allow for an understanding of how the niche of fibroblasts is changing. Taking into account the intense studies that have been performed on the pool of lung mesenchymal cells, we present data on the typing of interstitial fibroblasts and their role in the formation and maintenance of alveoli. On the whole, when identifying cell subpopulations in lung mesenchyme, one has to consider the developmental context, the changing cellular functions, and the lability of gene signatures.

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Section: Discussionmentioning

confidence: 99%

Section: Irefs Type Suggested Markers For the Corresponding Iref Typementioning

confidence: 99%

Alveologenesis: What Governs Secondary Septa Formation

Алпеева

Vasiliev

Vorotelyak

2021

IJMS

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“…Myofibroblasts contract the ECM and are absolutely required for alveolarization but are known to aberrantly populate the lung in BPD patients and BDP animal models (27)(28)(29)(30). Lipofibroblasts provide neutral lipids and paracrine ligands to alveolar type II epithelial cells (AT2 cells) and express Pdgfra, Tcf21, Plin2, and Fgf10 (17,(31)(32)(33)(34).…”

Section: Introductionmentioning

confidence: 99%

Maladaptive functional changes in alveolar fibroblasts due to perinatal hyperoxia impair epithelial differentiation

Riccetti¹,

Ushakumary²,

Waltamath³

et al. 2022

JCI Insight

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Infants born prematurely worldwide have up to a 50% chance of developing bronchopulmonary dysplasia (BPD), a clinical morbidity characterized by dysregulated lung alveolarization and microvascular development. It is known that PDGFR alpha–positive (PDGFRA + ) fibroblasts are critical for alveolarization and that PDGFRA + fibroblasts are reduced in BPD. A better understanding of fibroblast heterogeneity and functional activation status during pathogenesis is required to develop mesenchymal population–targeted therapies for BPD. In this study, we utilized a neonatal hyperoxia mouse model (90% O 2 postnatal days 0–7, PN0–PN7) and performed studies on sorted PDGFRA + cells during injury and room air recovery. After hyperoxia injury, PDGFRA + matrix and myofibroblasts decreased and PDGFRA + lipofibroblasts increased by transcriptional signature and population size. PDGFRA + matrix and myofibroblasts recovered during repair (PN10). After 7 days of in vivo hyperoxia, PDGFRA + sorted fibroblasts had reduced contractility in vitro, reflecting loss of myofibroblast commitment. Organoids made with PN7 PDGFRA + fibroblasts from hyperoxia in mice exhibited reduced alveolar type 1 cell differentiation, suggesting reduced alveolar niche-supporting PDGFRA + matrix fibroblast function. Pathway analysis predicted reduced WNT signaling in hyperoxia fibroblasts. In alveolar organoids from hyperoxia-exposed fibroblasts, WNT activation by CHIR increased the size and number of alveolar organoids and enhanced alveolar type 2 cell differentiation.

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“…However, very little is currently known about the role of L-MSCs in postnatal lung development and in BPD. Lung stromal cells, including lipofibroblasts, myofibroblasts and matrix fibroblasts are a potent source of inter-cellular signaling and are known to play an important role in BPD pathogenesis [12]. However, how L-MSCs communicate with other cell populations and contribute to the development of BPD remains unknown.…”

Section: Introductionmentioning

confidence: 99%

Single-cell RNA sequencing-based characterization of resident lung mesenchymal stromal cells in bronchopulmonary dysplasia

Mižíková

Lesage

Cyr-Depauw

et al. 2021

Preprint

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Late lung development is a period of alveolar and microvascular formation, which is pivotal in ensuring sufficient and effective gas exchange. Defects in late lung development manifest in premature infants as a chronic lung disease named bronchopulmonary dysplasia (BPD). Numerous studies demonstrated the therapeutic properties of exogenous bone marrow and umbilical cord-derived mesenchymal stromal cells (MSCs) in experimental BPD. However, very little is known regarding the regenerative capacity of resident lung MSCs (L-MSCs) during normal development and in BPD. In this study we aimed to characterize the L-MSC population in homeostasis and upon injury. We used single-cell RNA sequencing (scRNA-seq) to profile in situ Ly6a+ L-MSCs in the lungs of normal and O2-exposed neonatal mice (a well-established model to mimic BPD) at three developmental timepoints (postnatal days 3, 7 and 14). Hyperoxia exposure increased the number, and altered the expression profile of L-MSCs, particularly by increasing the expression of multiple pro-inflammatory, pro-fibrotic, and anti-angiogenic genes. In order to identify potential changes induced in the L-MSCs transcriptome by storage and culture, we profiled 15,000 Ly6a+ L-MSCs after in vitro culture. We observed great differences in expression profiles of in situ and cultured L-MSCs, particularly those derived from healthy lungs. Additionally, we have identified the location of L-MSCs in the developing lung and propose Serpinf1 as a novel, culture-stable marker of L-MSCs. Finally, cell communication analysis suggests inflammatory signals from immune and endothelial cells as main drivers of hyperoxia-induced changes in L-MSCs transcriptome.

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Resident Interstitial Lung Fibroblasts and their Role in Alveolar Stem Cell Niche Development, Homeostasis, Injury, and Regeneration

Cited by 64 publications

References 160 publications

Alveologenesis: What Governs Secondary Septa Formation

Alveologenesis: What Governs Secondary Septa Formation

Maladaptive functional changes in alveolar fibroblasts due to perinatal hyperoxia impair epithelial differentiation

Single-cell RNA sequencing-based characterization of resident lung mesenchymal stromal cells in bronchopulmonary dysplasia

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