Binding of Procollagen C-Proteinase Enhancer-1 (PCPE-1) to Heparin/Heparan Sulfate

Weiss, Tali; Ricard‐Blum, Sylvie; Moschcovich, Laura; Wineman, Eitan; Mesilaty, Shlomit; Kessler, Efrat

doi:10.1074/jbc.m110.141366

Cited by 35 publications

(47 citation statements)

References 37 publications

(59 reference statements)

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“…PCPE2, like PCPE1, consists of two cubulin (CUB) domains (CUB1 and CUB2) involved in protein-protein interaction. While several studies have been published addressing the physiological role of PCPE1 ( 13,14 ), the function of PCPE2 remains unclear. PCPE2-defi cient (PCPE2 KO) mice are viable and fertile, and they do not show gross developmental abnormalities ( 15 ).…”

Section: Identifi Cation Of Mature and Pro-apoa-i Formsmentioning

confidence: 99%

Disruption of the murine procollagen C-proteinase enhancer 2 gene causes accumulation of pro-apoA-I and increased HDL levels

Francone

Ishida

Llera-Moya

et al. 2011

Journal of Lipid Research

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Section: Identifi Cation Of Mature and Pro-apoa-i Formsmentioning

confidence: 99%

Disruption of the murine procollagen C-proteinase enhancer 2 gene causes accumulation of pro-apoA-I and increased HDL levels

Francone

Ishida

Llera-Moya

et al. 2011

Journal of Lipid Research

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“…Moreover, enhancement of pCP activity by PCPE1 is potentiated by heparin or heparan sulfate, both of which bind the PCPE1 NTR domain, procollagen, and BMP1 (85,86), suggesting that heparan sulfate proteoglycans (HSPGs) may foster procollagen processing in vivo by bolstering formation of PCPE-procollagen-B/TP complexes (85,86). HSPGs may also bind PCPEs to cell surfaces (86). PCPE1 enhancement of B/TPs seems specific to pCP activity, as PCPE1 failed to enhance cleavage of a number of other substrates in vitro (87).…”

Section: Pcp Enhancersmentioning

confidence: 99%

“…The CUB domains of PCPE1 bind procollagen (82) in a cooperative manner (83), and its NTR domain can bind BMP1 and mTLL1 (84,85), suggesting that PCPE1 may act as a linker that enhances procollagen-B/TP interactions. Moreover, enhancement of pCP activity by PCPE1 is potentiated by heparin or heparan sulfate, both of which bind the PCPE1 NTR domain, procollagen, and BMP1 (85,86), suggesting that heparan sulfate proteoglycans (HSPGs) may foster procollagen processing in vivo by bolstering formation of PCPE-procollagen-B/TP complexes (85,86). HSPGs may also bind PCPEs to cell surfaces (86).…”

Section: Pcp Enhancersmentioning

confidence: 99%

Metalloproteinases in Drosophila to Humans That Are Central Players in Developmental Processes

Muir

Greenspan

2011

Journal of Biological Chemistry

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Many secreted proteins are synthesized as precursors with propeptides that must be cleaved to yield the mature functional form of the molecule. In addition, various growth factors occur in extracellular latent complexes with protein antagonists and are activated upon cleavage of such antagonists. Research in the separate fields of embryonic patterning and extracellular matrix formation has identified members of the BMP1/Tolloid-like family of metalloproteinases as key players in these types of biosynthetic processing events in species ranging from Drosophila to humans. Bone morphogenic proteins (BMPs)2 were first defined by the ability to induce de novo bone formation and were first identified in bone extracts (1). Although all other BMPs are members of the TGF␤ superfamily of growth factors, BMP1 is a metalloproteinase, the first demonstrated role of which was as a procollagen C-proteinase (pCP) (2) that cleaves C-propeptides from procollagen precursors to produce mature monomers of the major fibrillar collagens I-III. This activity is crucial to bone biology, as collagen I is the major protein component of bone and is essential to bone structure/function. After initial cloning of mammalian BMP1, Tolloid (TLD), the protein product of a zygotically active gene involved in dorsoventral patterning of Drosophila embryos, was shown to have a domain structure resembling that of BMP1 (3) and was later shown to exert patterning effects by activating the TGF␤-like BMP decapentaplegic (DPP) (4). Subsequently, BMP1 and TLD have become prototypes of the BMP1/TLD-like proteinase (B/TP) family. B/TPs in a broad range of species are now implicated in processes that include extracellular matrix (ECM) formation and mineralization, embryonic patterning, growth factor activation, and generation of anti-angiogenic protein fragments, all via cleavage of a growing list of substrates.

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“…3, A-D). PCPE2 enhances procollagen processing and is abundantly expressed in the heart, aorta, adipose tissue, and trabecular meshwork (27,29,38). The expression of PCPE1, which is related to PCPE2, was not increased as a result of PCPE2 deletion (Fig.…”

Section: Discussionmentioning

confidence: 95%

“…The tandem CUB domains are followed by a C-terminal netrin-like (NTR) domain (27,29). CUB domains are commonly found in extracellular membrane proteins that mediate protein-protein interactions (33)(34)(35)(36), whereas NTR domains bind to cell surface glycosaminoglycans (37,38), presumably anchoring PCPE2 to the extracellular matrix. Interestingly, BMP1, in addition to catalyzing procollagen processing, removes the apoA-I six-amino acid propeptide (39).…”

mentioning

confidence: 99%

Procollagen C-endopeptidase Enhancer Protein 2 (PCPE2) Reduces Atherosclerosis in Mice by Enhancing Scavenger Receptor Class B1 (SR-BI)-mediated High-density Lipoprotein (HDL)-Cholesteryl Ester Uptake

Pollard

Blesso

Zabalawi

et al. 2015

Journal of Biological Chemistry

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Background: Extracellular matrix protein PCPE2 is linked to alterations in HDL size and concentration. Results: PCPE2 protects against diet-induced atherosclerosis by promoting HDL catabolism, reverse cholesterol transport, and SR-BI-mediated uptake of HDL-cholesteryl ester. Conclusion: PCPE2 mediates HDL function by reducing lipid and immune cell accumulation in the artery. Significance: These findings establish a role for the extracellular matrix glycoprotein PCPE2 in SR-BI-mediated HDL function and the prevention of atherosclerosis.

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Binding of Procollagen C-Proteinase Enhancer-1 (PCPE-1) to Heparin/Heparan Sulfate

Cited by 35 publications

References 37 publications

Disruption of the murine procollagen C-proteinase enhancer 2 gene causes accumulation of pro-apoA-I and increased HDL levels

Disruption of the murine procollagen C-proteinase enhancer 2 gene causes accumulation of pro-apoA-I and increased HDL levels

Metalloproteinases in Drosophila to Humans That Are Central Players in Developmental Processes

Procollagen C-endopeptidase Enhancer Protein 2 (PCPE2) Reduces Atherosclerosis in Mice by Enhancing Scavenger Receptor Class B1 (SR-BI)-mediated High-density Lipoprotein (HDL)-Cholesteryl Ester Uptake

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