Preventing
            <i>Engrailed-1</i>
            activation in fibroblasts yields wound regeneration without scarring

Mascharak, Shamik; desJardins-Park, Heather E.; Davitt, Michael F.; Griffin, Michelle; Borrelli, Mimi R.; Moore, Alessandra L.; Chen, Kellen; Duoto, Bryan; Chinta, Malini; Foster, Deshka S.; Shen, Abra H.; Januszyk, Michael; Kwon, Sun Hyung; Wernig, Gerlinde; Wan, Derrick C.; Lorenz, H. Peter; Gurtner, Geoffrey C.; Longaker, Michael T.

doi:10.1126/science.aba2374

Cited by 290 publications

(188 citation statements)

References 42 publications

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“…Many cell surface and lineage markers have been associated with fibroblasts involved in wound healing, including Pdgfra , Engrailed-1 ( En1 ), and CD26 ( Dpp4 ) ( 22 – 24 ). However, we and others have found expression of such markers to be variable throughout wound tissue ( SI Appendix , Fig.…”

Section: Resultsmentioning

confidence: 99%

“…S10 E ). To further explore these differences, we employed an automated feature extraction algorithm ( 24 ) to quantify ultrastructure characteristics of wound tissue sections, which demonstrated that FAK i -treated wound specimens were more similar to unwounded skin than to vehicle-control wounds, including for both mature and immature collagen fiber intensities ( SI Appendix , Fig. S10 F ).…”

Section: Resultsmentioning

confidence: 99%

“…By POD 2, a subset of fibroblasts appears to have differentiated to form an activated-responder subpopulation, while the remaining outer wound fibroblasts comprise the less differentiated mechanofibrotic cells. The latter fibroblasts highly express known fibrosis-associated markers such as Engrailed-1 ( 23 , 24 ), Col1a1 ( 34 ), Tgbf2 ( 35 ), and Jun ( 36 ). At POD 7, mechanofibrotic cells begin to differentiate in response to mechanotransduction cues as they migrate toward the wound center.…”

Section: Discussionmentioning

confidence: 99%

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Integrated spatial multiomics reveals fibroblast fate during tissue repair

Foster

Januszyk

Yost

et al. 2021

Proc. Natl. Acad. Sci. U.S.A.

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In the skin, tissue injury results in fibrosis in the form of scars composed of dense extracellular matrix deposited by fibroblasts. The therapeutic goal of regenerative wound healing has remained elusive, in part because principles of fibroblast programming and adaptive response to injury remain incompletely understood. Here, we present a multimodal -omics platform for the comprehensive study of cell populations in complex tissue, which has allowed us to characterize the cells involved in wound healing across both time and space. We employ a stented wound model that recapitulates human tissue repair kinetics and multiple Rainbow transgenic lines to precisely track fibroblast fate during the physiologic response to skin injury. Through integrated analysis of single cell chromatin landscapes and gene expression states, coupled with spatial transcriptomic profiling, we are able to impute fibroblast epigenomes with temporospatial resolution. This has allowed us to reveal potential mechanisms controlling fibroblast fate during migration, proliferation, and differentiation following skin injury, and thereby reexamine the canonical phases of wound healing. These findings have broad implications for the study of tissue repair in complex organ systems.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Integrated spatial multiomics reveals fibroblast fate during tissue repair

Foster

Januszyk

Yost

et al. 2021

Proc. Natl. Acad. Sci. U.S.A.

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“…Using genetic lineage tracing, anatomical fate mapping, and live imaging, we found that fascia-resident fibroblasts orchestrate the mobility of the connective tissue into wounds. Fascial mobility is directed by a single fibroblastic cell lineage termed Engrailed-1 lineage positive fibroblasts (EPFs), which is the profibrotic lineage fibroblasts responsible for skin scarring [47][48][49]. This specialized fibroblast type physically drags the fascia into the wound bed and subsequently into the skin surface in mice (Figure 2a).…”

Section: Wound Repair By Subcutaneous Fasciamentioning

confidence: 99%

Furnishing Wound Repair by the Subcutaneous Fascia

Jiang

Rinkevich

2021

IJMS

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Mammals rapidly heal wounds through fibrous connective tissue build up and tissue contraction. Recent findings from mouse attribute wound healing to physical mobilization of a fibroelastic connective tissue layer that resides beneath the skin, termed subcutaneous fascia or superficial fascia, into sites of injury. Fascial mobilization assembles diverse cell types and matrix components needed for rapid wound repair. These observations suggest that the factors directly affecting fascial mobility are responsible for chronic skin wounds and excessive skin scarring. In this review, we discuss the link between the fascia’s unique tissue anatomy, composition, biomechanical, and rheologic properties to its ability to mobilize its tissue assemblage. Fascia is thus at the forefront of tissue pathology and a better understanding of how it is mobilized may crystallize our view of wound healing alterations during aging, diabetes, and fibrous disease and create novel therapeutic strategies for wound repair.

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“…With increasing understanding of the complex roles YAP/TAZ play in lung development, homeostasis, injury repair, and pathologic fibrosis, it has become clear that approaching this pathway in a therapeutic context will not be as simple as global inhibition or activation, in contrast to other organs ( 51 ). While aberrant YAP activation in the epithelium and mesenchyme contribute to failure of repair, initial YAP activation in these cells is likely beneficial for proliferation of progenitor populations and signaling to immune cells ( 12 ).…”

Section: Future Work and Open Questionsmentioning

confidence: 99%

The Role of Hippo/YAP Signaling in Alveolar Repair and Pulmonary Fibrosis

Gokey

Kropski

2021

Front. Med.

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Pulmonary fibrosis is characterized by loss of normal alveoli, accumulation of pathologic activated fibroblasts, and exuberant extracellular matrix deposition that over time can lead to progressive loss of respiratory function and death. This loss of respiratory function is associated with the loss of alveolar type 1 cells (AT1) that play a crucial role in gas exchange and the depletion of the alveolar type 2 cells (AT2) that act as progenitor cells to regenerate the AT1 and AT2 cell populations during repair. Understanding the mechanisms that regulate normal alveolar repair and those associated with pathologic repair is essential to identify potential therapeutic targets to treat or delay progression of fibrotic diseases. The Hippo/YAP developmental signaling pathway has been implicated as a regulator of normal alveolar development and repair. In idiopathic pulmonary fibrosis, aberrant activation of YAP/TAZ has been demonstrated in both the alveolar epithelium and activated fibroblasts associated with increased fibrotic remodeling, and there is emerging interest in this pathway as a target for antifibrotic therapies. In this review, we summarize current evidence as to the role of the Hippo-YAP/TAZ pathway in alveolar development, homeostasis, and repair, and highlight key questions that must be resolved to determine effective strategies to modulate YAP/TAZ signaling to prevent progressive pulmonary fibrosis and enhance adaptive alveolar repair.

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Preventing Engrailed-1 activation in fibroblasts yields wound regeneration without scarring

Cited by 290 publications

References 42 publications

Integrated spatial multiomics reveals fibroblast fate during tissue repair

Integrated spatial multiomics reveals fibroblast fate during tissue repair

Furnishing Wound Repair by the Subcutaneous Fascia

The Role of Hippo/YAP Signaling in Alveolar Repair and Pulmonary Fibrosis

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