Captopril inhibits tumour growth in a xenograft model of human renal cell carcinoma

Hii, S. I.; Nicol, David; Gotley, D. C.; Thompson, Les; Green, M. K.; Jonsson, Julie R.

doi:10.1038/bjc.1998.145

Cited by 123 publications

(80 citation statements)

References 22 publications

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“…However, Ang II is known to stimulate neovascularisation (Fernandez et al, 1985), which in some cases is a requirement for tumour growth, while in vitro it stimulates cell replication in the absence of blood vessels (Paquet et al, 1990). ACE inhibitors retard growth of cancer cells in vitro (Reddy et al, 1995) and inhibit tumour growth in vivo (Hii et al, 1998), possibly through an effect on angiogenesis, while long-term use of ACE inhibitors may protect against the development of cancer (Lever et al, 1998). These results suggest that imidapril may inhibit growth of the MAC16 tumour by a mechanism unrelated to its effect on cachexia, and thus it is not possible to determine unequivocally whether imidapril has a direct anticachectic effect in this model.…”

Section: Discussionmentioning

confidence: 99%

Angiotensin II directly induces muscle protein catabolism through the ubiquitin–proteasome proteolytic pathway and may play a role in cancer cachexia

2005

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The ability of angiotensin I (Ang I) and II (Ang II) to induce directly protein degradation in skeletal muscle has been studied in murine myotubes. Angiotensin I stimulated protein degradation with a parabolic dose -response curve and with a maximal effect between 0.05 and 0.1 mM. The effect was attenuated by coincubation with the angiotensin-converting enzyme (ACE) inhibitor imidaprilat, suggesting that angiotensin I stimulated protein degradation through conversion to Ang II. Angiotensin II also stimulated protein breakdown with a similar dose -response curve, and with a maximal effect between 1 and 2.5 mM. Total protein degradation, induced by both Ang I and Ang II, was attenuated by the proteasome inhibitors lactacystin (5 mM) and MG132 (10 mM), suggesting that the effect was mediated through upregulation of the ubiquitin -proteasome proteolytic pathway. Both Ang I and Ang II stimulated an increased proteasome 'chymotrypsin-like' enzyme activity as well as an increase in protein expression of 20S proteasome a-subunits, the 19S subunits MSS1 and p42, at the same concentrations as those inducing protein degradation. The effect of Ang I was attenuated by imidaprilat, confirming that it arose from conversion to Ang II. These results suggest that Ang II stimulates protein degradation in myotubes through induction of the ubiquitin -proteasome pathway. Protein degradation induced by Ang II was inhibited by insulin-like growth factor and by the polyunsaturated fatty acid, eicosapentaenoic acid. These results suggest that Ang II has the potential to cause muscle atrophy through an increase in protein degradation. The highly lipophilic ACE inhibitor imidapril (Vitort) (30 mg kg À1 ) attenuated the development of weight loss in mice bearing the MAC16 tumour, suggesting that Ang II may play a role in the development of cachexia in this model.

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Section: Discussionmentioning

confidence: 99%

Angiotensin II directly induces muscle protein catabolism through the ubiquitin–proteasome proteolytic pathway and may play a role in cancer cachexia

2005

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“…Tumor-bearing mice were administered captopril in their drinking water at 1, 10, 50, or 100 mg/kg/d; these are typical, murine therapeutic dosages. 23,24 Captopril attenuated tumor growth in a dose-dependent fashion ( Fig. 2A).…”

Section: Resultsmentioning

confidence: 99%

Angiotensin converting enzyme inhibitors and angiotensin II receptor antagonist attenuate tumor growth via polarization of neutrophils toward an antitumor phenotype

et al. 2015

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“…8 Investigation is needed beyond the observation period of most of these studies, 56 and additional experimental studies are needed also to study the mechanisms by which agents blocking the RAS may obtain their inhibitory effect on tumour growth and metastasis. 31 Angiotensin-converting enzyme inhibitors should be investigated in properly designed prospective clinical trials of patients with cancer. This approach faces the same problems as in trials with MMP inhibitors and other biological modifiers: identification of patients with minimal tumour burden, useful surrogate end points along with decisions about what doses to use.…”

Section: Discussionmentioning

confidence: 99%

“…In mice treated with captopril, there was a significant doserelated reduction in tumour development. 31 Pulmonary metastases of renal cell carcinoma showed prominent AT 1 receptor expression in both mice and humans, and candesartan treatment dramatically prevented lung metastatic nodules in mice, along with the inhibition of neovascularization and VGEF expression, compared with control mice. 32 Pancreatic adenocarcinoma Experimental studies using cultured hamster pancreatic cancer cells have shown that captopril and the ACEi CGS 13945 decreased cell proliferation, as well as the cell proliferation antigen (PCNA), a DNA polymerase cofactor that is used as a marker for synthesis phase.…”

Section: Renal Cell Carcinomamentioning

confidence: 95%

Angiotensin inhibition and malignancies: a review

Rosenthal

Gavras

2009

J Hum Hypertens

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After an early report that patients treated with angiotensin-converting enzyme (ACE) inhibitors had a lower than expected incidence of cancers, there was a large number of publications investigating the possible pathophysiological mechanism mediating this effect, as well as population studies comparing the incidence of cancers in patients treated with agents inhibiting the reninangiotensin system with their incidence in the general population. Several mechanisms are proposed to explain a potential anti-tumour activity of such agents in vitro in experimental animal models. However, the population studies are mostly inconclusive, although they do suggest a possible interaction between ACE genotypes and susceptibility to altered behaviour of certain tumours.

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Captopril inhibits tumour growth in a xenograft model of human renal cell carcinoma

Cited by 123 publications

References 22 publications

Angiotensin II directly induces muscle protein catabolism through the ubiquitin–proteasome proteolytic pathway and may play a role in cancer cachexia

Angiotensin II directly induces muscle protein catabolism through the ubiquitin–proteasome proteolytic pathway and may play a role in cancer cachexia

Angiotensin converting enzyme inhibitors and angiotensin II receptor antagonist attenuate tumor growth via polarization of neutrophils toward an antitumor phenotype

Angiotensin inhibition and malignancies: a review

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