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Bone Morphogenetic Protein-1 (BMP-1)
Bone morphogenetic protein-1 (BMP-1) is a shorter spliced variant of mammalian tolloid (mTld), both of which cleave the C-propeptides of type I procollagen during the synthesis of extracellular matrix collagen fibrils. The fact that BMP-1 and mTld both exhibit procollagen C-proteinase (PCP) activity...
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| Published in: | The Journal of biological chemistry 2003-05, Vol.278 (20), p.18045-18049 |
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| Main Authors: | , , |
| Format: | Article |
| Language: | English |
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| cites | cdi_FETCH-LOGICAL-c1530-73dfb2c8443d93452f91e0b9019cc3499d5c60fc5b6a7f02af1e54e2a19006c3 |
| container_end_page | 18049 |
| container_issue | 20 |
| container_start_page | 18045 |
| container_title | The Journal of biological chemistry |
| container_volume | 278 |
| creator | Hartigan, Nichola Garrigue-Antar, Laure Kadler, Karl E. |
| description | Bone morphogenetic protein-1 (BMP-1) is a shorter spliced variant of mammalian tolloid (mTld), both of which cleave the C-propeptides
of type I procollagen during the synthesis of extracellular matrix collagen fibrils. The fact that BMP-1 and mTld both exhibit
procollagen C-proteinase (PCP) activity and that BMP-1 is the smaller variant might indicate that BMP-1 comprises the minimal
required sequences for PCP activity. BMP-1 comprises a metalloproteinase domain, three CUB domains, and an epidermal growth
factor (EGF)-like domain, which is located between the second and third CUB ( c omplement components C1r/C1s, the sea urchin protein U egf, and B MP-1) domains. In this study we showed the following. 1) The CUB1 domain is required for secretion of the molecule. Domain
swapping experiments, in which CUB1 and other CUB domains were interchanged, resulted in retention of the proteins by cells.
Therefore, CUB1 and its location immediately adjacent to the metalloproteinase domain are essential for secretion of the protein.
2) Mutants lacking the EGF-like and CUB3 domains exhibited full C-proteinase activity. In contrast, mutants lacking the CUB2
domain were poor C-proteinases. 3) Further studies showed that Glu-483 on the β4-β5 loop of CUB2 is essential for C-proteinase
activity of BMP-1. In conclusion, the study showed that the minimal domain structure for PCP activity is considerably shorter
than expected and comprises the metalloproteinase domain and the CUB1 and CUB2 domains of BMP-1. |
| doi_str_mv | 10.1074/jbc.M211448200 |
| format | article |
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of type I procollagen during the synthesis of extracellular matrix collagen fibrils. The fact that BMP-1 and mTld both exhibit
procollagen C-proteinase (PCP) activity and that BMP-1 is the smaller variant might indicate that BMP-1 comprises the minimal
required sequences for PCP activity. BMP-1 comprises a metalloproteinase domain, three CUB domains, and an epidermal growth
factor (EGF)-like domain, which is located between the second and third CUB ( c omplement components C1r/C1s, the sea urchin protein U egf, and B MP-1) domains. In this study we showed the following. 1) The CUB1 domain is required for secretion of the molecule. Domain
swapping experiments, in which CUB1 and other CUB domains were interchanged, resulted in retention of the proteins by cells.
Therefore, CUB1 and its location immediately adjacent to the metalloproteinase domain are essential for secretion of the protein.
2) Mutants lacking the EGF-like and CUB3 domains exhibited full C-proteinase activity. In contrast, mutants lacking the CUB2
domain were poor C-proteinases. 3) Further studies showed that Glu-483 on the β4-β5 loop of CUB2 is essential for C-proteinase
activity of BMP-1. In conclusion, the study showed that the minimal domain structure for PCP activity is considerably shorter
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of type I procollagen during the synthesis of extracellular matrix collagen fibrils. The fact that BMP-1 and mTld both exhibit
procollagen C-proteinase (PCP) activity and that BMP-1 is the smaller variant might indicate that BMP-1 comprises the minimal
required sequences for PCP activity. BMP-1 comprises a metalloproteinase domain, three CUB domains, and an epidermal growth
factor (EGF)-like domain, which is located between the second and third CUB ( c omplement components C1r/C1s, the sea urchin protein U egf, and B MP-1) domains. In this study we showed the following. 1) The CUB1 domain is required for secretion of the molecule. Domain
swapping experiments, in which CUB1 and other CUB domains were interchanged, resulted in retention of the proteins by cells.
Therefore, CUB1 and its location immediately adjacent to the metalloproteinase domain are essential for secretion of the protein.
2) Mutants lacking the EGF-like and CUB3 domains exhibited full C-proteinase activity. In contrast, mutants lacking the CUB2
domain were poor C-proteinases. 3) Further studies showed that Glu-483 on the β4-β5 loop of CUB2 is essential for C-proteinase
activity of BMP-1. In conclusion, the study showed that the minimal domain structure for PCP activity is considerably shorter
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of type I procollagen during the synthesis of extracellular matrix collagen fibrils. The fact that BMP-1 and mTld both exhibit
procollagen C-proteinase (PCP) activity and that BMP-1 is the smaller variant might indicate that BMP-1 comprises the minimal
required sequences for PCP activity. BMP-1 comprises a metalloproteinase domain, three CUB domains, and an epidermal growth
factor (EGF)-like domain, which is located between the second and third CUB ( c omplement components C1r/C1s, the sea urchin protein U egf, and B MP-1) domains. In this study we showed the following. 1) The CUB1 domain is required for secretion of the molecule. Domain
swapping experiments, in which CUB1 and other CUB domains were interchanged, resulted in retention of the proteins by cells.
Therefore, CUB1 and its location immediately adjacent to the metalloproteinase domain are essential for secretion of the protein.
2) Mutants lacking the EGF-like and CUB3 domains exhibited full C-proteinase activity. In contrast, mutants lacking the CUB2
domain were poor C-proteinases. 3) Further studies showed that Glu-483 on the β4-β5 loop of CUB2 is essential for C-proteinase
activity of BMP-1. In conclusion, the study showed that the minimal domain structure for PCP activity is considerably shorter
than expected and comprises the metalloproteinase domain and the CUB1 and CUB2 domains of BMP-1.</abstract><pub>American Society for Biochemistry and Molecular Biology</pub><pmid>12637537</pmid><doi>10.1074/jbc.M211448200</doi><tpages>5</tpages><oa>free_for_read</oa></addata></record> |
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| issn | 0021-9258 1083-351X |
| language | eng |
| recordid | cdi_crossref_primary_10_1074_jbc_M211448200 |
| source | Elsevier ScienceDirect Journals |
| title | Bone Morphogenetic Protein-1 (BMP-1) |
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