Expression of angiotensin type II receptor downregulates Cdk4 synthesis and inhibits cell-cycle progression

Gingras, Bruno; Rodier, Geneviève; Giasson, Edith; Coulombe, Philippe; Chassagne, Catherine; Meloche, Sylvain

doi:10.1038/sj.onc.1206346

Cited by 7 publications

(9 citation statements)

References 49 publications

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“…The AT 2 receptor has been implicated in cardiovascular disease as a beneficial moiety due to its proposed vasodilatory role, ability to inhibit cell growth, induce apoptosis, and inhibit activation of MAPK functions that, overall, appear to counterbalance the actions of the AT 1 receptor (Berk, 2003;Miura et al, 2010). Overall, the AT 2 receptor may play a role in several AT 1 receptor-independent biologic processes (Mifune et al, 2000;Ruiz-Ortega et al, 2000Zhu et al, 2000;Weidekamm et al, 2002;Benndorf et al, 2003;Gingras et al, 2003;Caballero et al, 2004;Zhao et al, 2005b;Mertens et al, 2010). Furthermore, activation of the AT 2 receptor inhibits autophagy mediated by the AT 1 receptor in cardiomyocytes (Porrello et al, 2009).…”

Section: G Pathophysiological Aspects Of Angii Type 2 Receptor Activmentioning

confidence: 99%

“…Activation of the AT 2 receptor inhibits autophagy mediated by the AT 1 receptor in cardiomyocytes (Porrello et al, 2009). Overall, the AT 2 receptor may play a role in several AT 1 receptor-independent biologic processes as well (RuizOrtega et al, 2000(RuizOrtega et al, , 2001aMifune et al, 2000;Weidekamm et al, 2002;Benndorf et al, 2003;Gingras et al, 2003;Caballero et al, 2004;Zhao et al, 2005b;Zhu et al, 2000;Mertens et al, 2010). Notably, activation of the AT 2 receptor in cells of neuronal origin, induced neurite outgrowth, and elongation mediated cellular excitability and migration and, in some cases, caused neuronal cell death (Guimond and Gallo-Payet, 2012).…”

Section: G Pathophysiological Aspects Of Angii Type 2 Receptor Activmentioning

confidence: 99%

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International Union of Basic and Clinical Pharmacology. XCIX. Angiotensin Receptors: Interpreters of Pathophysiological Angiotensinergic Stimuli

et al. 2015

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Section: G Pathophysiological Aspects Of Angii Type 2 Receptor Activmentioning

confidence: 99%

Section: G Pathophysiological Aspects Of Angii Type 2 Receptor Activmentioning

confidence: 99%

International Union of Basic and Clinical Pharmacology. XCIX. Angiotensin Receptors: Interpreters of Pathophysiological Angiotensinergic Stimuli

et al. 2015

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“…49 CKI expression was not influenced in the AT 2 -receptors expressing fibroblasts. 49 Ang II has antiproliferative effects without causing apoptosis in PC12 cells, a pheochromocytoma cell line that exclusively express AT 2 -receptors. 50 Antiproliferative effects of Ang II in PC12 cells are not associated with apoptosis, but represent a differentiation process.…”

Section: Ang II Apoptosis and Antiproliferationmentioning

confidence: 83%

“…48 Overexpression of AT 2 -receptors in fibroblasts had antiproliferative effects without causing apoptosis. 49 This effect was associated with an inhibition of CDK4 and cyclin E expression. 49 CKI expression was not influenced in the AT 2 -receptors expressing fibroblasts.…”

Section: Ang II Apoptosis and Antiproliferationmentioning

confidence: 99%

“…49 This effect was associated with an inhibition of CDK4 and cyclin E expression. 49 CKI expression was not influenced in the AT 2 -receptors expressing fibroblasts. 49 Ang II has antiproliferative effects without causing apoptosis in PC12 cells, a pheochromocytoma cell line that exclusively express AT 2 -receptors.…”

Section: Ang II Apoptosis and Antiproliferationmentioning

confidence: 99%

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Angiotensin II and Cell Cycle Regulation

Wolf

Wenzel

2004

Hypertension

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Abstract-Angiotensin II has emerged as an important growth factor for vascular, cardiac, and renal cells. Depending on the specific cell type and presence of other growth factors, angiotensin II induces proliferation (replication of DNA with subsequent successful division of cells), hypertrophy (increase in cell size, cell protein, and mRNA content without DNA replication), apoptosis (programmed cell death), or differentiation. Such angiotensin II-mediated modulation of growth process may underlie various pathophysiological processes such as atherosclerosis, vascular and cardiac remodeling, and progression of chronic renal disease. Clearly, angiotensin II-induced proliferation requires complete cell progression through the various steps of the cell cycle. In contrast, cells undergoing angiotensin II-mediated hypertrophy are arrested in the G 1 -phase. Upregulation of cell cycle-dependent kinase inhibitors (eg, p27 Kip1 ) plays an important role in this process. Although accumulating evidence suggests that apoptosis is cell cycle-dependent, only few data are currently available concerning the interaction of angiotensin II with the cell cycle machinery in apoptosis. We review the various angiotensin II-mediated growth processes and their relationship to events governing cell cycle regulation.

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Signalling responses linked to betulinic acid‐induced apoptosis are antagonized by MEK inhibitor U0126 in adherent or 3D spheroid melanoma irrespective of p53 status

Rieber

2005

Intl Journal of Cancer

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MEK1/2 inhibitors like U0126 can potentiate or antagonize the antitumor activity of cytotoxic agents such as cisplatin, paclitaxel or vinblastine, depending on the drug or the target cells. We now investigated whether U0126, differentially regulates melanoma signaling in response to UV radiation or betulinic acid, a drug lethal against melanoma. This report shows that U0126 inhibits early response (ERK) kinase activation and cyclin A expression in wt p53 C8161 melanoma exposed to either UV radiation or betulinic acid. However, U0126 does not protect from UV damage, but counteracts betulinic acid-mediated apoptosis in the same cells. Protection from the latter drug by joint treatment with U0126 was also evident in wt p53 MelJuso melanoma and mutant p53 WM164 melanoma. The latter cells were the most responsive to betulinic acid, showing a selective decline in the cdk4 protein, without a comparable change in other key cell cycle proteins like cdc2, cdk2, cdk7 or cyclin A, prior to apoptosis-associated PARP fragmentation. Laser scanning cytometry also showed that betulinic acid induced a significant increase in chromatin condensation in WM164 melanoma irrespective of whether they were in adherent form or as multicellular spheroids. All these betulinic acidinduced changes were counteracted by U0126. Our data show for the first time that (a) cdk4 protein is an early target of betulinic acid-induced apoptosis and (b) unrestricted ERK signaling favours betulinic acid-induced apoptosis, but this is counteracted by U0126, partly through counteracting chromatin condensation and restoring Akt activation decreased by betulinic acid treatment. ' 2005 Wiley-Liss, Inc.Key words: laser scanning cytometry; cdk4; G2; ERK/Akt survival cross talk; apoptosis Constitutive activation of p42/p44 MAPK (mitogen-activated protein) kinases or early response (ERK) kinases occurs in tumor progression in prostate carcinoma and melanoma. 1,2 On the basis of the importance of constitutive ERK activation in tumors, pharmacological inhibitors of MAPK kinases MEK1/2 that activate MAPK/ERK have attracted attention since some of them inhibit ERK activation and block human colon carcinoma growth in vivo. 3,4 Pharmacological inhibition of the MAPK kinases MEK1/2 was recently reported as a useful strategy for killing melanoma cells. 5 However, others have shown that the MEK inhibitor U0126 can normalize the morphology of adherent Ki-ras-transformed rat fibroblasts, 6 inhibit invasion of A375 melanoma through Matrigel 7 and promote B16 melanoma differentiation, 8 without exerting a cytotoxic effect on these tumor cells. Moreover, pharmacological inhibition of ERK activation by U0126 or by PD98059 was reported to strongly attenuate apoptosis induced by high dose etoposide, adryamicin, or UV radiation. 9 Enforced activation of ERK by overexpression of MEK-1/Q56P also sensitized cells to DNA damage-induced apoptosis. 9 In contrast, in vivo studies involving injection of TPras melanoma cells into SCID mice resulted in the development of invasive tumors. App...

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Expression of angiotensin type II receptor downregulates Cdk4 synthesis and inhibits cell-cycle progression

Cited by 7 publications

References 49 publications

International Union of Basic and Clinical Pharmacology. XCIX. Angiotensin Receptors: Interpreters of Pathophysiological Angiotensinergic Stimuli

International Union of Basic and Clinical Pharmacology. XCIX. Angiotensin Receptors: Interpreters of Pathophysiological Angiotensinergic Stimuli

Angiotensin II and Cell Cycle Regulation

Signalling responses linked to betulinic acid‐induced apoptosis are antagonized by MEK inhibitor U0126 in adherent or 3D spheroid melanoma irrespective of p53 status

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