Selective inhibition of proprotein convertases represses the metastatic potential of human colorectal tumor cells

Scamuffa, Nathalie; Siegfried, Géraldine; Bontemps, Yannick; Ma, Liming; Basak, Ajoy; Cherel, Ghislaine; Calvo, Fabien; Seidah, Nabil G.; Khatib, Abdel‐Majid

doi:10.1172/jci32040

Cited by 112 publications

(123 citation statements)

References 44 publications

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“…This should be considerd when pPC inhibitors are used in the context of cancer therapies as suggested by several laboratories, based on findings that pPCs promote tumor growth and metastasis (52). However, we note that PC7 could also protect tumors from NK cell-mediated attack by securing high MHC I levels despite low TAP or tapasin function in malignant cells.…”

Section: Discussionmentioning

confidence: 79%

Post-Endoplasmic Reticulum Rescue of Unstable MHC Class I Requires Proprotein Convertase PC7

Leonhardt

Fiegl

Rufer

et al. 2010

The Journal of Immunology

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The function of the peptide-loading complex (PLC) is to facilitate loading of MHC class I (MHC I) molecules with antigenic peptides in the endoplasmic reticulum and to drive the selection of these ligands toward a set of high-affinity binders. When the PLC fails to perform properly, as frequently observed in virus-infected or tumor cells, structurally unstable MHC I peptide complexes are generated, which are prone to disintegrate instead of presenting Ags to cytotoxic T cells. In this study we show that a second quality control checkpoint dependent on the serine protease proprotein convertase 7 (PC7) can rescue unstable MHC I, whereas the related convertase furin is completely dispensable. Cells with a malfunctioning PLC and silenced for PC7 have substantially reduced MHC I surface levels caused by high instability and significantly delayed surface accumulation of these molecules. Instead of acquiring stability along the secretory route, MHC I appears to get largely routed to lysosomes for degradation in these cells. Moreover, mass spectrometry analysis provides evidence that lack of PLC quality control and/or loss of PC7 expression alters the MHC I-presented peptide profile. Finally, using exogenously applied peptide precursors, we show that liberation of MHC I epitopes may directly require PC7. We demonstrate for the first time an important function for PC7 in MHC I-mediated Ag presentation.

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Section: Discussionmentioning

confidence: 79%

Post-Endoplasmic Reticulum Rescue of Unstable MHC Class I Requires Proprotein Convertase PC7

Leonhardt

Fiegl

Rufer

et al. 2010

The Journal of Immunology

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“…Members of the proprotein convertase family, including furin, cleave various proteins at RXKR, RXRR, RR, and KR sequences (23). HUVECs were cotransfected with plasmids encoding ANGPTL4 and ␣1-anti-trypsin Portland (␣1-PDX), a potent inhibitor of all proprotein convertases (24). We demonstrated that ␣1-PDX was efficiently transfected (green fluorescent protein expression from pIRES2-EGFP plasmid encoding ␣1-PDX; data not shown).…”

Section: Proprotein Convertases Are Involved In the Proteolytic Procementioning

confidence: 97%

Interaction of the coiled‐coil domain with glycosaminoglycans protects angiopoietin‐like 4 from proteolysis and regulates its antiangiogenic activity

et al. 2008

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Angiopoietin-like 4 (ANGPTL4) is involved in angiogenesis and lipid metabolism. It is secreted by liver and adipose tissues and cleaved to generate circulating coiled-coil domain (CCD) and fibrinogen-like domain (FLD) fragments. The full-length ANGPTL4 produced by hypoxic endothelial cells interacts with the extracellular matrix (ECM). The ECM-bound and soluble forms of ANGPTL4 have antiangiogenic properties. We carried out a structure-function analysis to investigate the regulation of ANGPTL4 bioactivity in endothelial cells. We found that the recombinant CCD binds to the ECM, whereas the FLD is released into the medium. The CCD, like the full-length ANGPTL4, binds to heparan and dermatan sulfates in surface plasmon resonance assays and inhibits endothelial cell adhesion, motility, and tubule-like formation. In endothelial cells, ANGPTL4 is processed in the secretion medium after release from the ECM. This processing is altered by the proprotein convertases inhibitor alpha1-PDX and abolished by the mutation of the (161)RRKR(164) cleavage site without modification of the ECM binding and release. These data suggest that the full-length form, which interacts with heparan sulfate proteoglycans via its CCD, is protected from proteolysis by proprotein convertases and constitutes the major active pool of ANGPTL4 in hypoxic endothelial cells.

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“…The primary mechanism for prorenin activation has been considered to be through cleavage by prohormone convertases (Benjannet et al 1992), which may be highly expressed in cancer, including breast tumours, and this is associated with greater oestrogen dependency (Cheng et al 1997(Cheng et al , 2001). Of course, prohormone convertases may be involved in tumorigenic processes that do not involve either prorenin or angiotensin II (Siegfried et al 2003, Scamuffa et al 2008. Alternatively, the discovery of a specific prorenin receptor that binds prorenin and activates intracellular signalling pathways while at the same time activating its enzymic activity in the absence of cleavage opens new possibilities (Nguyen & Contrepas 2008, Nguyen 2011.…”

Section: Localisation Of Ras Componentsmentioning

confidence: 99%

The renin–angiotensin system in the breast and breast cancer

Vinson¹,

Barker²,

Puddefoot³

2011

Endocrine-Related Cancer

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Much evidence now suggests that angiotensin II has roles in normal functions of the breast that may be altered or attenuated in cancer. Both angiotensin type 1 (AT1) and type 2 (AT2) receptors are present particularly in the secretory epithelium. Additionally, all the elements of a tissue renin-angiotensin system, angiotensinogen, prorenin and angiotensin-converting enzyme (ACE), are also present and distributed in different cell types in a manner suggesting a close relationship with sites of angiotensin II activity. These findings are consistent with the concept that stromal elements and myoepithelium are instrumental in maintaining normal epithelial structure and function. In disease, this system becomes disrupted, particularly in invasive carcinoma. Both AT1 and AT2 receptors are present in tumours and may be up-regulated in some. Experimentally, angiotensin II, acting via the AT1 receptor, increases tumour cell proliferation and angiogenesis, both these are inhibited by blocking its production or function. Epidemiological evidence on the effect of expression levels of ACE or the distribution of ACE or AT1 receptor variants in many types of cancer gives indirect support to these concepts. It is possible that there is a case for the therapeutic use of high doses of ACE inhibitors and AT1 receptor blockers in breast cancer, as there may be for AT2 receptor agonists, though this awaits full investigation. Attention is drawn to the possibility of blocking specific AT1-mediated intracellular signalling pathways, for example by AT1-directed antibodies, which exploit the possibility that the extracellular N-terminus of the AT1 receptor may have previously unsuspected signalling roles.

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Selective inhibition of proprotein convertases represses the metastatic potential of human colorectal tumor cells

Cited by 112 publications

References 44 publications

Post-Endoplasmic Reticulum Rescue of Unstable MHC Class I Requires Proprotein Convertase PC7

Post-Endoplasmic Reticulum Rescue of Unstable MHC Class I Requires Proprotein Convertase PC7

Interaction of the coiled‐coil domain with glycosaminoglycans protects angiopoietin‐like 4 from proteolysis and regulates its antiangiogenic activity

The renin–angiotensin system in the breast and breast cancer

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