Literature DB >> 19410661

Immunotherapy with tumor-targeted superantigens (TTS) in combination with docetaxel results in synergistic anti-tumor effects.

Anette Sundstedt1, Mona Celander, Marie Wallén Ohman, Göran Forsberg, Gunnar Hedlund.   

Abstract

In this study we explored the possibility of combining immunotherapy against cancer with the well-established cytostatic drug docetaxel. Tumor-targeted superantigens (TTS) utilizes the powerful T cell activating property of a superantigen such as staphylococcal enterotoxin A (SEA) in fusion with an anti-tumor Fab-fragment to target this T cell activity against tumor cells. TTS fusion proteins are efficient in a number of experimental tumor models including the B16 mouse melanoma transfected with a human tumor-associated antigen (GA733-2 or EpCam) recognized by the C215 monoclonal antibody. The distinct mechanisms of action of TTS and docetaxel provide the prerequisites for successful combination treatment. However, as a result of the anti-proliferative properties of cytostatic drugs, chemotherapy may modify TTS induced immune activation during combination treatment. Here we evaluated the anti-tumor effects of combining C215Fab-SEA with docetaxel against B16-C215 tumors growing in the lung of C57Bl/6 mice. Both compounds generated a significant reduction in the number of B16-C215 lung tumors when administered alone. Prior treatment with docetaxel at therapeutic doses did not interfere with superantigen induced T cell activation but rather appeared to enhance the response, while simultaneous treatment was suppressive. Combining TTS and docetaxel significantly improved tumor therapy, further reducing the number of lung tumors as compared to mono therapies. Importantly, the combination treatment at timely settings synergistically prolonged long term survival in B16-C215 tumor bearing mice. The results of this study demonstrate that TTS immunotherapy is highly compatible with docetaxel and suggest a significant potential of the combination for human cancer therapy.

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Year:  2009        PMID: 19410661     DOI: 10.1016/j.intimp.2009.04.013

Source DB:  PubMed          Journal:  Int Immunopharmacol        ISSN: 1567-5769            Impact factor:   4.932


  7 in total

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Journal:  Oncol Lett       Date:  2018-05-17       Impact factor: 2.967

3.  Human TGFalpha-derived peptide TGFalphaL3 fused with superantigen for immunotherapy of EGFR-expressing tumours.

Authors:  Quanbin Xu; Xiaojuan Zhang; Junjie Yue; Chuanxuan Liu; Cheng Cao; Hui Zhong; Qingjun Ma
Journal:  BMC Biotechnol       Date:  2010-12-22       Impact factor: 2.563

4.  Superantigens increase the survival of mice bearing T cell lymphomas by inducing apoptosis of neoplastic cells.

Authors:  Juliana Mundiñano; Paula M Berguer; Gabriel Cabrera; Daniela Lorenzo; Irene Nepomnaschy; Isabel Piazzon
Journal:  PLoS One       Date:  2010-12-22       Impact factor: 3.240

5.  In Silico Design and Analysis of TGFαL3-SEB Fusion Protein as "a New Antitumor Agent" Candidate by Ligand-Targeted Superantigens Technique.

Authors:  Abbas Ali Imani-Fooladi; Forough Yousefi; Seyed Fazloallah Mousavi; Jafar Amani
Journal:  Iran J Cancer Prev       Date:  2014

6.  A B-Cell Superantigen Induces the Apoptosis of Murine and Human Malignant B Cells.

Authors:  Daniela Lorenzo; Alejandra Duarte; Juliana Mundiñano; Paula Berguer; Irene Nepomnaschy; Isabel Piazzon
Journal:  PLoS One       Date:  2016-09-07       Impact factor: 3.240

7.  Novel antibody-based proteins for cancer immunotherapy.

Authors:  Jaheli Fuenmayor; Ramon F Montaño
Journal:  Cancers (Basel)       Date:  2011-08-19       Impact factor: 6.639

  7 in total

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