Synergistic anti-cancer effects of immunotoxin and cyclosporin in vitro and in vivo

Andersson, Yvonne; Engebraaten, Olav; Fodstad, Øystein

doi:10.1038/sj.bjc.6605312

Cited by 38 publications

(46 citation statements)

References 33 publications

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“…3). The same finding was reported by Andersson et al 15 in a preclinical study of Cyclosporin A in combination with immunotoxins. The range of RAHA concentration in the different groups in the present study may be explained by the myelotoxicity, as the production of RAHA might be lower when the number of white blood cells is decreased, or by individual differences.…”

supporting

confidence: 77%

“…14 Since we use immunocompetent animals, some immunosuppressive treatment should probably be used to prevent the development of immune response to the therapeutic mouse/human chimeric antibodies. We selected and evaluated Cyclosporin A according to Andersson et al 15 To the best of our knowledge, studies on RIT with subsequent administration of unlabeled mAbs have only been conducted in xenograft models of lymphomas, and not on solid tumors or in syngeneic animal models.…”

mentioning

confidence: 99%

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Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Eriksson

Ohlsson²,

Nilsson³

et al. 2012

Cancer Biotherapy and Radiopharmaceuticals

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Metastatic disease after successful treatment of the primary tumor continues to be a therapeutic challenge. Enhancement of therapeutic effects by the administration of unlabeled monoclonal antibodies (mAbs) after radioimmunotherapy (RIT) may provide a means of preventing or delaying the development of metastatic disease. In the present study, Brown Norway rats with syngeneic grafted colon carcinomas were administered the minimal effective therapeutic dose of 400 MBq/kg lutetium-177 ( 177 Lu)-DOTA-BR96. After 2 weeks, half of the animals were given 15 mg/kg unlabeled mAb BR96 as consolidation therapy. Treatment response and toxicity were monitored 100 days after the treatment with unlabeled BR96. The treatment with unlabeled mAb after RIT resulted in a complete response (CR) in 19 of 19 animals, while RIT alone resulted in a CR in 17 of 19 animals. The additional treatment did not affect the number of animals with metastatic disease or the time to clinical symptoms of metastases. RIT resulted in reversible myelotoxicity. The unlabeled mAb BR96 did not cause any additional toxicity, making it possible to repeat the consolidation therapy.

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confidence: 77%

mentioning

confidence: 99%

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Eriksson

Ohlsson²,

Nilsson³

et al. 2012

Cancer Biotherapy and Radiopharmaceuticals

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“…In another case of ovarian metastasis of hepatocellular carcinoma sirolimus but not tacrolimus induced a long tumor free survival [30], and in a study of hepatocellular cancer, patients treated with sirolimus experienced a longer survival than patients in the tacrolimus group [31]. Finally, cyclosporin A added to immunotoxins caused synergistic cytotoxicity and strongly inhibited formation of metastases in a cervical cancer model in nude mice [32]. Thus, decreased expression of FKBP65 correlates with malignant conversion in ovarian carcinogenesis, and immunosuppression seems to improve survival.…”

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confidence: 92%

Expression of FK506 binding protein 65 (FKBP65) is decreased in epithelial ovarian cancer cells compared to benign tumor cells and to ovarian epithelium

et al. 2011

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FK506 binding protein 65 (FKBP65) belongs to a group of proteins termed immunophilins that have a high binding affinity to immunosuppressant drugs as FK506 (tacrolimus) and rapamycin (sirolimus). Treatment of female premenopausal women with tacrolimus, which binds to FKBP65, has been reported to be followed by a strongly increased risk of ovarian cysts. We performed the present study to reveal how FKBP65 is expressed in the ovary and in ovarian tumors and to see if this expression might be related to ovarian tumor development, a relationship we have found in colorectal cancer. Biopsies from prospectively collected samples from ovaries and benign, borderline, and invasive ovarian tumors were analyzed for expression of FKBP65 by immunohistochemistry. The expression was compared to survival and several clinicopathological parameters. FKBP65 is strongly expressed in ovarian epithelium and in benign ovarian tumor cells. In the ovary, a positive staining was also found in endothelial cells of blood vessels. In non-invasive and in invasive malignant tumor cells, a decreased staining was observed, which was not correlated to stage, histology, or survival. A significant inversed correlation to expression of p53 was found. The differential expression of FKBP65 indicates a role in ovarian physiology as well as in ovarian tumor development. Our observations and the chromosomal localization of the FKBP65 gene indicate a tumor suppressor function of the FKBP65 protein in ovarian carcinogenesis.

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“…Both the 425.3PE and 9.2.27PE have antitumor activity in vitro and in vivo in different cancer types. 1,[3][4][5][6] We hypothesized that by combining ITs with agents that target different signaling pathways in cancer cells, enhanced cytotoxic effect of the ITs would be achieved.…”

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confidence: 99%

“…ITs are taken up through endocytosis, processed within the cell, and cell death is caused by inhibition of protein synthesis through adenosine diphosphate-ribosylation of elongation factor 2 and induction of apoptosis. [1][2][3][4] Apoptosis is commonly associated with activation of caspases, inactivation of the DNA repair enzyme poly-(adenosine diphosphate-ribose) polymerase (PARP), chromatin condensation, and fragmentation of DNA. Our ITs consist of the Pseudomonas exotoxin A (PE) linked to antibodies targeting the epidermal growth factor receptor or the high molecular weight-melanoma associated antigen, the 425.3 and the 9.2.27 antibody, respectively.…”

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confidence: 99%

Triphenylmethyl Derivatives Enhances the Anticancer Effect of Immunotoxins

Risberg

Guldvik

Palchaudhuri

et al. 2011

Journal of Immunotherapy

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The combined use of several drugs targeting different cellular functions is one approach to achieve tumor control in cancer. We studied the effects of Pseudomonas exotoxin A (PE)-based immunotoxins (ITs), the 9.2.27PE and the 425.3PE, together with 2 different triphenylmethyl derivatives, triphenylmethyl phosphonates and phosphonochloridates (TPMP)-I-2 and 4BI. Combining the triphenylmethyl derivatives with ITs enhanced the cytotoxic effect of the ITs, with TPMP-I-2 in combination with the 425.3PE (targeting the epidermal growth factor receptor) being the most promising combination. The cytotoxicity involving signs of apoptosis was observed in cancer cells from different origins in vitro. It is interesting to note that treatment with IT, TPMP-I-2, or 4BI alone or in combination resulted in strongly decreased protein levels of stearoyl-CoA desaturase. Stearoyl-CoA desaturase is the rate-limiting enzyme for converting saturated fatty acids into monounsaturated fatty acids needed for membrane genesis. Furthermore, the combination of 425.3PE and TPMP-I-2 prolonged the survival time of nude rats in a simulated micrometastatic cervical cancer model. In addition, we demonstrate that a combination of the 425.3PE and 4BI was more effective in reducing tumor growth in a breast cancer model in nude mice compared with either agent alone.

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Synergistic anti-cancer effects of immunotoxin and cyclosporin in vitro and in vivo

Cited by 38 publications

References 33 publications

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Expression of FK506 binding protein 65 (FKBP65) is decreased in epithelial ovarian cancer cells compared to benign tumor cells and to ovarian epithelium

Triphenylmethyl Derivatives Enhances the Anticancer Effect of Immunotoxins

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Synergistic anti-cancer effects of immunotoxin and cyclosporin in vitro and in vivo

Cited by 38 publications

References 33 publications

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with 177Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with 177Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Expression of FK506 binding protein 65 (FKBP65) is decreased in epithelial ovarian cancer cells compared to benign tumor cells and to ovarian epithelium

Triphenylmethyl Derivatives Enhances the Anticancer Effect of Immunotoxins

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Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model

Treatment with Unlabeled mAb BR96 After Radioimmunotherapy with ¹⁷⁷Lu-DOTA-BR96 in a Syngeneic Rat Colon Carcinoma Model