Opposite Roles of Furin and PC5A in N-Cadherin Processing
We recently demonstrated that lack of Furin-processing of the N-cadherin precursor (proNCAD) in highly invasive melanoma and brain tumor cells results in the cell-surface expression of a nonadhesive protein favoring cell migration and invasion in vitro. Quantitative polymerase chain reaction analys...
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2012-10-01
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| Series: | Neoplasia: An International Journal for Oncology Research |
| Online Access: | http://www.sciencedirect.com/science/article/pii/S1476558612800200 |
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doaj-134a3339e6dc451da3660c6b7cdbafa92020-11-24T23:17:55ZengElsevierNeoplasia: An International Journal for Oncology Research1476-55862012-10-01141088089210.1593/neo.121250Opposite Roles of Furin and PC5A in N-Cadherin ProcessingDeborah Maret0Mohamad Seyed Sadr1Emad Seyed Sadr2David R Colman3Rolando F Del Maestro4Nabil G Seidah5Brain Tumor Research Centre, Montreal Neurological Institute, McGill University, Montréal, Québec, CanadaBrain Tumor Research Centre, Montreal Neurological Institute, McGill University, Montréal, Québec, CanadaBrain Tumor Research Centre, Montreal Neurological Institute, McGill University, Montréal, Québec, CanadaBrain Tumor Research Centre, Montreal Neurological Institute, McGill University, Montréal, Québec, CanadaBrain Tumor Research Centre, Montreal Neurological Institute, McGill University, Montréal, Québec, CanadaInstitut de Recherches Cliniques de Montré;al, Université de Montreal, Montreal, Québec, Canada We recently demonstrated that lack of Furin-processing of the N-cadherin precursor (proNCAD) in highly invasive melanoma and brain tumor cells results in the cell-surface expression of a nonadhesive protein favoring cell migration and invasion in vitro. Quantitative polymerase chain reaction analysis of malignant human brain tumor cells revealed that of all proprotein convertases (PCs) only the levels of Furin and PC5A are modulated, being inversely (Furin) or directly (PC5A) correlated with brain tumor invasive capacity. Intriguingly, the N-terminal sequence following the Furin-activated NCAD site (RQKR↓DW161, mouse nomenclature) reveals a second putative PC-processing site (RIRSDR↓DK189) located in the first extracellular domain. Cleavage at this site would abolish the adhesive functions of NCAD because of the loss of the critical Trp161. This was confirmed upon analysis of the fate of the endogenous prosegment of proNCAD in human malignant glioma cells expressing high levels of Furin and low levels of PC5A (U343) or high levels of PC5A and negligible Furin levels (U251). Cellular analyses revealed that Furin is the best activating convertase releasing an ∼17-kDa prosegment, whereas PC5A is the major inactivating enzyme resulting in the secretion of an ∼20-kDa product. Like expression of proNCAD at the cell surface, cleavage of the NCAD molecule at RIRSDR↓DK189 renders the U251 cancer cells less adhesive to one another and more migratory. Our work modifies the present view on posttranslational processing and surface expression of classic cadherins and clarifies how NCAD possesses a range of adhesive potentials and plays a critical role in tumor progression. http://www.sciencedirect.com/science/article/pii/S1476558612800200 |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Deborah Maret Mohamad Seyed Sadr Emad Seyed Sadr David R Colman Rolando F Del Maestro Nabil G Seidah |
| spellingShingle |
Deborah Maret Mohamad Seyed Sadr Emad Seyed Sadr David R Colman Rolando F Del Maestro Nabil G Seidah Opposite Roles of Furin and PC5A in N-Cadherin Processing Neoplasia: An International Journal for Oncology Research |
| author_facet |
Deborah Maret Mohamad Seyed Sadr Emad Seyed Sadr David R Colman Rolando F Del Maestro Nabil G Seidah |
| author_sort |
Deborah Maret |
| title |
Opposite Roles of Furin and PC5A in N-Cadherin Processing |
| title_short |
Opposite Roles of Furin and PC5A in N-Cadherin Processing |
| title_full |
Opposite Roles of Furin and PC5A in N-Cadherin Processing |
| title_fullStr |
Opposite Roles of Furin and PC5A in N-Cadherin Processing |
| title_full_unstemmed |
Opposite Roles of Furin and PC5A in N-Cadherin Processing |
| title_sort |
opposite roles of furin and pc5a in n-cadherin processing |
| publisher |
Elsevier |
| series |
Neoplasia: An International Journal for Oncology Research |
| issn |
1476-5586 |
| publishDate |
2012-10-01 |
| description |
We recently demonstrated that lack of Furin-processing of the N-cadherin precursor (proNCAD) in highly invasive melanoma and brain tumor cells results in the cell-surface expression of a nonadhesive protein favoring cell migration and invasion in vitro. Quantitative polymerase chain reaction analysis of malignant human brain tumor cells revealed that of all proprotein convertases (PCs) only the levels of Furin and PC5A are modulated, being inversely (Furin) or directly (PC5A) correlated with brain tumor invasive capacity. Intriguingly, the N-terminal sequence following the Furin-activated NCAD site (RQKR↓DW161, mouse nomenclature) reveals a second putative PC-processing site (RIRSDR↓DK189) located in the first extracellular domain. Cleavage at this site would abolish the adhesive functions of NCAD because of the loss of the critical Trp161. This was confirmed upon analysis of the fate of the endogenous prosegment of proNCAD in human malignant glioma cells expressing high levels of Furin and low levels of PC5A (U343) or high levels of PC5A and negligible Furin levels (U251). Cellular analyses revealed that Furin is the best activating convertase releasing an ∼17-kDa prosegment, whereas PC5A is the major inactivating enzyme resulting in the secretion of an ∼20-kDa product. Like expression of proNCAD at the cell surface, cleavage of the NCAD molecule at RIRSDR↓DK189 renders the U251 cancer cells less adhesive to one another and more migratory. Our work modifies the present view on posttranslational processing and surface expression of classic cadherins and clarifies how NCAD possesses a range of adhesive potentials and plays a critical role in tumor progression.
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| url |
http://www.sciencedirect.com/science/article/pii/S1476558612800200 |
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