Intratumoral Injection of INGN 241, a Nonreplicating Adenovector Expressing the Melanoma-Differentiation Associated Gene-7 (mda-7/IL24): Biologic Outcome in Advanced Cancer Patients

Tong, Alex W.; Nemunaitis, John; Su, Dan; Zhang, Yuan; Cunningham, Casey; Senzer, Neil; Netto, George J.; Rich, Dawn; Mhashilkar, Abner; Parker, Kathryn; Coffee, Keith; Ramesh, Rajagopal; Ekmekçioglu, Sühendan; Grimm, Elizabeth A.; Hood, Jill; Merritt, James A.; Chada, Sunil

doi:10.1016/j.ymthe.2004.09.021

Cited by 178 publications

(205 citation statements)

References 34 publications

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“…Forced expression of E-cadherin in cultured cells, and transgenic mouse models of carcinogenesis, results in impaired metastatic and invasive phenotypes. 33,34 Here, we show that Herceptin, alone and in combination with Ad-mda7, is able to upregulate specifically E-cadherin in Her-2 þ cells, and to sequester its binding partner b-catenin to the plasma membrane (Figure 5a and b, left panel), thereby inhibiting its nuclear translocation and inhibiting b-catenin-induced transcriptional activation of cell migration and cell proliferation signals.…”

Section: Discussionmentioning

confidence: 71%

“…Differences in tumor size were analyzed for significance by the Student's t-test. Enhanced in vitro growth inhibitory and cytotoxic activity of Ad-mda7 and Herceptin in Her-2 þ breast cancer cells The antiproliferative effects of Ad-mda7 in various cancer cell types have been demonstrated in previous studies; [16][17][18][19][20][21][22][24][25][26][27][28][29][30][31][32][33][34]36 and the relevance of these findings to the clinical setting is supported by in vivo lung and breast xenograft models. 17,21 To corroborate that the Her-2 receptors expressed by the breast cancer cells are functional, we evaluated cell death in MDA-MB-453 and MCF-7 lines treated with increasing amounts of Herceptin (0-100 mg/ ml).…”

Section: Discussionmentioning

confidence: 80%

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Combinatorial synergy induced by adenoviral-mediated mda-7 and Herceptin in Her-2+ breast cancer cells

et al. 2006

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The melanoma differentiation-associated gene-7 (mda-7) is a member of the interleukin-10 cytokine family and a novel tumor suppressor gene. Adenoviral-mediated mda-7 (Ad-mda7) gene transfer has tumor-specific growth inhibitory and proapoptotic effects in a broad spectrum of cancer cells. In breast cancer cells, adenoviral-induced mda-7 expression triggers antiproliferative effects by downregulation of survival signals, such as Bcl-2 and Akt. The anti-human epidermal growth factor receptor-2 (Her-2) monoclonal antibody, Trastuzumab (Herceptin), increases the sensitivity of Her-2/neu-overexpressing breast cancer cells to chemotherapeutic agents and radiotherapy. In this study, we evaluate the effects of treatment with Ad-mda7 and Herceptin combination therapy in a panel of Her-2/neu-overexpressing cell lines, and in established tumors in nude mice. Compared to individual treatments, the combination of Ad-mda7 and Herceptin elicits supra-additive antitumor activity in Her-2/neuoverexpressing tumor cell lines: increased cell death, cell cycle block and apoptosis. The Ad-mda7 and Herceptin interaction was shown to be synergistic by isobologram analysis. Ad-mda7 does not alter cell surface Her-2/neu levels, but the combination of Ad-mda7 þ Herceptin results in increased expression of cell surface E-cadherin with concomitant translocation of b-catenin from the nucleus to the cell membrane. In vivo, the combination of Ad-mda7 and Herceptin showed significantly increased antitumor activity (Po0.003) against Her-2/neu-overexpressing tumors. These data suggest that the combination of Ad-mda7 with Herceptin may be a novel therapy for breast cancer patients whose tumors overexpress Her-2/neu. The observed synergistic effect may improve treatment options for otherwise poorly responsive, Her-2-positive, breast cancer patients. Cancer Gene Therapy (2006) 13, 958-968.

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Section: Discussionmentioning

confidence: 71%

Section: Discussionmentioning

confidence: 80%

Combinatorial synergy induced by adenoviral-mediated mda-7 and Herceptin in Her-2+ breast cancer cells

et al. 2006

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“…A phase I trial using intratumoral injections of Ad-IL-24 (INGN 241) was conducted in patients with refractory cancer. [14][15][16] As expected, INGN 241 can induce apoptosis in a large percentage of tumor volume via a single intratumoral injection. However, as the INGN 241 virus is nonreplicating, the clinically significant response can be seen only with repeat injection of INGN 241.…”

Section: Introductionmentioning

confidence: 57%

The antitumor activity of TRAIL and IL-24 with replicating oncolytic adenovirus in colorectal cancer

Zhao

Dong

et al. 2006

Cancer Gene Ther

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Melanoma differentiation associated gene-7 (Mda-7)/IL-24 was previously cloned into ZD55 (an adenovirus with E1B55 deleted) to form ZD55-IL-24, which had much better antitumor effect than Ad-IL-24. According to its good antitumor properties, ZD55-IL-24 has been used in preclinical studies. But ZD55-IL-24 alone still could not completely eradicate established tumors in all nude mice. It was reported that IL-24 could induce and enhance the activity of tumor necrosis factor-related apoptosis-inducing ligand (TRAIL) (a member of tumor necrosis factor (TNF) superfamily). Accordingly, the combined use of ZD55-IL-24 and ZD55-TRAIL was carried out in this study. Treatment with both ZD55-IL-24 and ZD55-TRAIL could induce more significant apoptosis in cancer cells in vitro compared with ZD55-IL-24 or ZD55-TRAIL alone. The combination of the two replicative adenoviruses had better antitumor activity in vivo than that of single oncolytic adenovirus and led to complete eradication of xenograft tumors in all treated mice. Upregulation of TRAIL was observed in tumor cells infected with ZD55-IL-24 and studies of the apoptotic cascade regulators indicate that ZD55-IL-24 could further enhance the activation of apoptosis through the TNF family of death receptors. We demonstrated for the first time the potential therapeutic effect of combined ZD55-IL-24 with ZD55-TRAIL for the targeted therapy of cancer.

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“…The results obtained from this trial demonstrate both safety and clinical efficacy. 22 In addition to its direct apoptosis-inducing properties, Ad.mda-7 also shows antiangiogenic, immunostimulatory and potent 'bystander' antitumor activities. 23,24 These exciting results provide direct support for using mda-7/ IL-24 in developing an effective gene-based therapy for cancer.…”

Section: Introductionmentioning

confidence: 99%

Enhanced delivery of mda-7/IL-24 using a serotype chimeric adenovirus (Ad.5/3) improves therapeutic efficacy in low CAR prostate cancer cells

Dash

Dmitriev

et al. 2010

Cancer Gene Ther

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Intratumoral Injection of INGN 241, a Nonreplicating Adenovector Expressing the Melanoma-Differentiation Associated Gene-7 (mda-7/IL24): Biologic Outcome in Advanced Cancer Patients

Cited by 178 publications

References 34 publications

Combinatorial synergy induced by adenoviral-mediated mda-7 and Herceptin in Her-2+ breast cancer cells

Combinatorial synergy induced by adenoviral-mediated mda-7 and Herceptin in Her-2+ breast cancer cells

The antitumor activity of TRAIL and IL-24 with replicating oncolytic adenovirus in colorectal cancer

Enhanced delivery of mda-7/IL-24 using a serotype chimeric adenovirus (Ad.5/3) improves therapeutic efficacy in low CAR prostate cancer cells

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