Rapamycin-Induced Endothelial Cell Death and Tumor Vessel Thrombosis Potentiate Cytotoxic Therapy against Pancreatic Cancer

Bruns, Christiane; Koehl, Gudrun E.; Guba, Markus; Yezhelyev, Maksim; Steinbauer, Markus; Seeliger, Hendrik; Schwend, A.; Hoehn, Anna; Jauch, Karl‐Walter; Geissler, Edward K.

doi:10.1158/1078-0432.ccr-03-0502

Cited by 100 publications

(79 citation statements)

References 35 publications

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“…The rapid and focal nature of tumor cell death may reflect acute changes in established blood flow rather than attenuation of vessel proliferation. Rapamycin can promote thrombotic occlusion of tumor vessels (46,47). We observed histologic evidence of vessel occlusion, including clogged and dilated vessels and dying cells with features of ischemic necrosis, in tumors and peritumoral regions that were similar to those described for other types of tumors treated with rapamycin (data not shown).…”

Section: Discussionsupporting

confidence: 79%

Rapamycin inhibits multiple stages of c-Neu/ErbB2–induced tumor progression in a transgenic mouse model of HER2-positive breast cancer

Mosley

Poirier

Seachrist

et al. 2007

Molecular Cancer Therapeutics

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Amplification of the HER2 (ErbB2, c-Neu) proto-oncogene in breast cancer is associated with poor prognosis and high relapse rates. HER2/ErbB2, in conjunction with ErbB3, signals through the Akt/phosphatidylinositol 3-kinase pathway and leads to the activation of mammalian target of rapamycin (mTOR), a critical mRNA translation regulator that controls cell growth. Gene expression analysis of mammary tumors collected from mouse mammary tumor virus-c-Neu transgenic mice revealed that mRNA levels of several mTOR pathway members were either up-regulated (p85/phosphatidylinositol 3-kinase and p70S6 kinase) or down-regulated (eIF-4E-BP1) in a manner expected to enhance signaling through this pathway. Treatment of these mice with the mTOR inhibitor rapamycin caused growth arrest and regression of primary tumors with no evidence of weight loss or generalized toxicity. The treatment effects were due to decreased proliferation, associated with reduced cyclin D1 expression, and increased cell death in primary tumors. Whereas many of the dead epithelial cells had the histopathologic characteristics of ischemic necrosis, rapamycin treatment was not associated with changes in microvascular density or apoptosis. Rapamycin also inhibited cellular proliferation in lung metastases. In summary, data from this preclinical model of ErbB2/Neu-induced breast cancer show that inhibition of the mTOR pathway with rapamycin blocks multiple stages of ErbB2/Neu-induced tumorigenic progression. [Mol Cancer Ther 2007;6(8):2188 -97]

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Section: Discussionsupporting

confidence: 79%

Rapamycin inhibits multiple stages of c-Neu/ErbB2–induced tumor progression in a transgenic mouse model of HER2-positive breast cancer

Mosley

Poirier

Seachrist

et al. 2007

Molecular Cancer Therapeutics

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“…A recent study in SCC cell lines demonstrates that inhibition of mTOR induces activation of Akt and results in antitumor effects in this tumour type (Amornphimoltham et al, 2005). In this model, as well as in other disease types such as pancreas cancer (Bruns et al, 2004), the antitumor effects of mTOR inhibitors appear to be in part related to their antiangiogenic effects. In our previous work, we have determined the susceptibility of a set of SCC cell lines both in vitro and in vivo to EGFR inhibitors (Amador et al, 2004;Jimeno et al, 2006).…”

mentioning

confidence: 69%

“…It is known that mTOR inhibitors work, at least in part, by decreasing angiogenesis (Bruns et al, 2004;Stephan et al, 2004). Western blots.…”

Section: Discussionmentioning

confidence: 99%

Dual EGFR and mTOR targeting in squamous cell carcinoma models, and development of early markers of efficacy

et al. 2007

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The epidermal growth factor receptor (EGFR) is a validated target in squamous cell carcinoma (SCC) of the head and neck. Most patients, however, do not respond or develop resistance to this agent. Mammalian target of rapamycin (mTOR) is involved in the pathogenesis of SCC of the head and neck (SCCHN). This study aimed to determine if targeting mTOR in combination with EGFR is effective in SCC, and to develop early pharmacodynamic markers of efficacy. Two SCC cell lines, one resistant (HEP2) and one of intermediate susceptibility (Detroit 562) to EGFR inhibitors, were xenografted in vivo and treated with an mTOR inhibitor (temsirolimus), an EGFR inhibitor (erlotinib) or a combination of both. Temsirolimus exerted superior growth arrest in both cell lines than erlotinib. The combined treatment resulted in synergistic antitumor effects in the Detroit 562 cell line. Immunohistochemical assessment of pharmacodynamic effects in fine-needle aspiration (FNA) biopsies early after treatment using phospho MAPK, Phospho-P70 and Ki67 as end points demonstrated pathway abrogation in the Detroit 562 tumours treated with the combination, the only group where regressions were seen. In conclusion, an mTOR inhibitor showed antitumor activity in EGFR-resistant SCC cell lines. Marked antitumor effects were associated with dual pathway inhibition, which were detected by early FNA biopsies.

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“…Moreover, other investigators have demonstrated synergistic growth-inhibitory effects by combined treatment of gemcitabine and rapamycin in another orthotopic model of L3.6pl pancreatic cancer cells. 43 They have revealed that rapamycin induced apoptosis of endothelial cells and tumor vessel thrombosis in this model and suggested that combining rapamycin with other cytotoxic drugs could be a feasible therapy of pancreatic cancer. From these data, we speculate that an antiangiogenic effect of CCI-779 might be involved in the mechanism of its synergistic antitumor activity in this study.…”

Section: Discussionmentioning

confidence: 90%

In vivo antitumor effect of the mTOR inhibitor CCI‐779 and gemcitabine in xenograft models of human pancreatic cancer

Ito

Fujimoto

Mori

et al. 2005

Intl Journal of Cancer

109

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Mammalian target of rapamycin (mTOR) is considered to be a major effector of cell growth and proliferation that controls protein synthesis through a large number of downstream targets. We investigated the expression of the phosphatidylinositol 3 0 -kinase (PI3K)/mTOR signaling pathway in human pancreatic cancer cells and tissues, and the in vivo antitumor effects of the mTOR inhibitor CCI-779 with/without gemcitabine in xenograft models of human pancreatic cancer. We found that the Akt, mTOR and p70 S6 kinase (S6K1) from the PI3K/mTOR signaling pathway were activated in all of the pancreatic cancer cell lines examined. When surgically resected tissue specimens of pancreatic ductal adenocarcinoma were examined, phosphorylation of Akt, mTOR and S6K1 was detected in 50, 55 and 65% of the specimens, respectively. Although CCI-779 had no additive or synergistic antiproliferative effect when combined with gemcitabine in vitro, it showed significant antitumor activity in the AsPC-1 subcutaneous xenograft model as both a single agent and in combination with gemictabine. Furthermore, in the Suit-2 peritoneal dissemination xenograft model, the combination of these 2 drugs achieved significantly better survival when compared with CCI-779 or gemcitabine alone. These results demonstrate promising activity of the mTOR inhibitor CCI-779 against human pancreatic cancer, and suggest that the inhibition of mTOR signaling can be exploited as a potentially tumor-selective therapeutic strategy. ' 2005 Wiley-Liss, Inc.

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Rapamycin-Induced Endothelial Cell Death and Tumor Vessel Thrombosis Potentiate Cytotoxic Therapy against Pancreatic Cancer

Cited by 100 publications

References 35 publications

Rapamycin inhibits multiple stages of c-Neu/ErbB2–induced tumor progression in a transgenic mouse model of HER2-positive breast cancer

Rapamycin inhibits multiple stages of c-Neu/ErbB2–induced tumor progression in a transgenic mouse model of HER2-positive breast cancer

Dual EGFR and mTOR targeting in squamous cell carcinoma models, and development of early markers of efficacy

In vivo antitumor effect of the mTOR inhibitor CCI‐779 and gemcitabine in xenograft models of human pancreatic cancer

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