An Essential Role for Fibronectin Extra Type III Domain A in Pulmonary Fibrosis

Muro, Andrés F.; Moretti, Federico A.; Moore, Bethany B.; Yan, Mei; Atrasz, Rachelle G.; Wilke, Carol A.; Flaherty, Kevin R.; Martínez, Fernando J.; Tsui, Jessica; Sheppard, Dean; Baralle, Francisco E.; Toews, Galen B.; White, Eric S.

doi:10.1164/rccm.200708-1291oc

Cited by 262 publications

(265 citation statements)

References 37 publications

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“…This same mutation has been reported in a 34-year-old man with moderate aplastic anemia that did not respond to immunosuppression and has short telomere lengths as measured by flow-fluorescence in situ hybridization (8). The development of pulmonary fibrosis versus bone marrow dysfunction in telomerase mutation carriers may be related to secondary ''hits,'' such as environmental toxins (cigarette smoking), fibrosis-prone intrinsic host mesenchymal responses to injury (34,35), or other susceptibilities. Understanding the influences on the development of lung disease in telomerase mutation carriers will be important to delineate.…”

Section: Table 3 Distribution Of Case Subects and Control Subjects Ssupporting

confidence: 52%

Telomere Shortening in Familial and Sporadic Pulmonary Fibrosis

Cronkhite

Xing²,

Raghu

et al. 2008

Am J Respir Crit Care Med

478

394

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Section: Table 3 Distribution Of Case Subects and Control Subjects Ssupporting

confidence: 52%

Telomere Shortening in Familial and Sporadic Pulmonary Fibrosis

Cronkhite

Xing²,

Raghu

et al. 2008

Am J Respir Crit Care Med

478

394

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“…Mechanistically, the authors identified a critical role for matrix-dependent suppression of miR-29 in engaging increased translation of matrix proteins when fibroblasts were seeded on IPF-derived matrices (5), elucidating a mechanism by which fibrotic matrix programs cells to produce greater amounts of matrix (Figure 1). Delineating the profibrotic cues that exist within pathological matrices will require intensive efforts, but several matrix or matrixassociated protein candidates have been identified that confer profibrotic signals and correlate with fibrotic pathologies (2), including fibulin-1 (10), osteopontin (11,12), periostin (13,14), connective tissue growth factor (15), and fibronectin (16,17).…”

Section: Matrix and Mesenchyme In Lung Diseasesmentioning

confidence: 99%

Matrix, Mesenchyme, and Mechanotransduction

Tschumperlin

2015

Annals ATS

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The extracellular matrix (ECM) of the lung serves as both a scaffold for resident cells and a mechanical support for respiratory function. The ECM is deposited during development and undergoes continuous turnover and maintenance during organ growth and homeostasis. Cells of the mesenchyme, including the tissue resident fibroblast, take a leading role in depositing and organizing the matrix and do so in an anatomically distinct fashion, with differing composition, organization, and mechanical properties within the airways, vessels, and alveoli of the lung. Recent technological advancements have allowed the lung's ECM biochemical composition and mechanical properties to be studied with improved resolution, thereby identifying novel disease-related changes in ECM characteristics. In parallel, efforts to study cells seeded on normal and disease-derived matrices have illustrated the powerful role the ECM can play in altering key functions of lung resident cells. The mechanical properties of the matrix have been identified as an important modifier of cell-matrix adhesions, with matrices of pathologic stiffness promoting profibrotic signaling and cell function. Ongoing work is identifying both mechanically activated pathways in mesenchymal cells and diseaserelated ECM molecules that biochemically regulate cell function. Uncovering the control systems by which cells respond to and regulate the matrix, and the failures in these systems that underlie aberrant repair, remains a major challenge. Progress in this area will be an essential element in efforts to engineer functional lung tissue for regenerative approaches and will be key to identifying new therapeutic strategies for lung diseases characterized by disturbed matrix architecture.

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“…The protein fibronectin (FN) is a major component of the ECM, and an excessive and disordered FN matrix is present in fibrotic diseases (15) and hypertrophic scars (16). FN matrix assembly is mediated by integrin receptors and regulated by intracellular signals, cytoskeletal organization, and availability of FN (17).…”

Section: The Extracellular Matrix (Ecm)mentioning

confidence: 99%

Regulation of Matrix Assembly through Rigidity-dependent Fibronectin Conformational Changes

Carraher

Schwarzbauer

2013

Journal of Biological Chemistry

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Background: Cell behavior is affected by changes in extracellular matrix stiffness during disease progression. Results: Fibronectin matrix assembly is inhibited on soft substrates but can be restored by manipulating cell-fibronectin binding or by partially unfolding substrate fibronectin. Conclusion: On soft substrates, cells are deficient in integrin-fibronectin bond strength and therefore cannot induce fibronectin conformational changes required for assembly. Significance: Rigidity-dependent changes in fibronectin conformation provide a novel mechanism for mechanotransduction.

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An Essential Role for Fibronectin Extra Type III Domain A in Pulmonary Fibrosis

Cited by 262 publications

References 37 publications

Telomere Shortening in Familial and Sporadic Pulmonary Fibrosis

Telomere Shortening in Familial and Sporadic Pulmonary Fibrosis

Matrix, Mesenchyme, and Mechanotransduction

Regulation of Matrix Assembly through Rigidity-dependent Fibronectin Conformational Changes

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