2019
DOI: 10.1074/mcp.ra118.001046
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Identification of Novel Natural Substrates of Fibroblast Activation Protein-alpha by Differential Degradomics and Proteomics

Abstract: Fibroblast activation protein-␣ (FAP) can hydrolyze the postproline bond. We identified endogenous substrates of FAP in fibroblasts that were previously naive to both FAP and its proteolytic activity. FAP-dependent cleavage sites were identified in many extracellular matrix (ECM) and ECM-associated proteins including collagens and lysyl oxidase-like-1, and CSF-1, CXCL-5 and C1qT6. Quantitative proteomic analysis implicated FAP in ECM-cell interactions, coagulation and metabolism. This study greatly expands the… Show more

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Cited by 44 publications
(31 citation statements)
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References 93 publications
(107 reference statements)
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“…Our discovery that ablating the FAP enzyme activity is sufficient to generate these metabolic outcomes indicates that these outcomes are driven by bioactive natural substrates of FAP. The known metabolism-associated substrates of FAP are FGF-21, GLP-1, NPY and PYY [1,3,5,20], and possibly nucleobindin-1 [44]. We showed here that GLP-1 activity is not altered and so is unlikely to be a physiological substrate of FAP.…”
Section: Discussionmentioning
confidence: 54%
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“…Our discovery that ablating the FAP enzyme activity is sufficient to generate these metabolic outcomes indicates that these outcomes are driven by bioactive natural substrates of FAP. The known metabolism-associated substrates of FAP are FGF-21, GLP-1, NPY and PYY [1,3,5,20], and possibly nucleobindin-1 [44]. We showed here that GLP-1 activity is not altered and so is unlikely to be a physiological substrate of FAP.…”
Section: Discussionmentioning
confidence: 54%
“…FAP has previously been found only in activated fibroblasts, so the new observation of its expression in b-cells commences a paradigm shift in understanding FAP functions. In DIO, FAP is probably acting on nonextracellular matrix substrates derived from b-cells and neighbouring cells, perhaps some that were identified in our recent degradomics study [1]. FAP is relatively abundant in mouse serum, so that is probably a major site of substrate degradation, including FGF-21.…”
Section: Discussionmentioning
confidence: 81%
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