Literature DB >> 19545790

Differential effect triggered by a heparan mimetic of the RGTA family preventing oral mucositis without tumor protection.

Monica Mangoni1, Xiaoli Yue, Christophe Morin, Dominique Violot, Valerie Frascogna, Yungan Tao, Paule Opolon, Marine Castaing, Anne Auperin, Giampaolo Biti, Denis Barritault, Marie-Catherine Vozenin-Brotons, Eric Deutsch, Jean Bourhis.   

Abstract

PURPOSE: Oral mucositis is a common side effect induced by radio/chemotherapy in patients with head and neck cancer. Although it dramatically impairs patient quality of life, no efficient and safe therapeutic solution is available today. Therefore, we investigated the protective efficacy of a new heparan mimetic biopolymer, RGTA-OTR4131, used alone or in combination with amifostine, for oral mucositis and simultaneously evaluated its effect on tumor growth in vitro and in vivo. METHODS AND MATERIALS: A single dose of 16.5 Gy was selectively delivered to the snout of mice, and the effects of OTR4131 or amifostine-OTR4131 were analyzed by macroscopic scoring and histology. The effect of OTR4131 administration on tumor growth was then investigated in vitro and in xenograft models using two cell lines (HEP-2 and HT-29).
RESULTS: Amifostine and OTR4131 significantly decreased the severity and duration of lip mucosal reactions. However, amifostine has to be administered before irradiation, whereas the most impressive protection was obtained when OTR4131 was injected 24 h after irradiation. In addition, OTR4131 was well tolerated, and the combination of amifostine and OTR4131 further enhanced mucosal protection. At the tumor level, OTR4131 did not modify HEP-2 cell line clonogenic survival in vitro or protect xenografted tumor cells from radiotherapy. Of interest, high doses of OTR4131 significantly decreased clonogenic survival of HT-29 cells.
CONCLUSIONS: RGTAs-OTR4131 is a well-tolerated, natural agent that effectively reduces radio-induced mucositis without affecting tumor sensitivity to irradiation. This suggests a possible transfer into the clinic for patients' benefit.

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Year:  2009        PMID: 19545790     DOI: 10.1016/j.ijrobp.2009.03.006

Source DB:  PubMed          Journal:  Int J Radiat Oncol Biol Phys        ISSN: 0360-3016            Impact factor:   7.038


  7 in total

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Journal:  Int Wound J       Date:  2010-11-16       Impact factor: 3.315

2.  Refractory sickle cell leg ulcer: is heparan sulphate a new hope?

Authors:  Shady Hayek; Saad Dibo; Joe Baroud; Amir Ibrahim; Denis Barritault
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Authors:  Sandrine Jacquet-Guibon; Anne-Gaelle Dupays; Virginie Coudry; Nathalie Crevier-Denoix; Sandrine Leroy; Fernando Siñeriz; Franck Chiappini; Denis Barritault; Jean-Marie Denoix
Journal:  PLoS One       Date:  2018-03-09       Impact factor: 3.240

Review 4.  RGTA® or ReGeneraTing Agents mimic heparan sulfate in regenerative medicine: from concept to curing patients.

Authors:  Denis Barritault; Marie Gilbert-Sirieix; Kim Lee Rice; Fernando Siñeriz; Dulce Papy-Garcia; Christophe Baudouin; Pascal Desgranges; Gilbert Zakine; Jean-Louis Saffar; Johan van Neck
Journal:  Glycoconj J       Date:  2016-12-07       Impact factor: 2.916

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Authors:  Yacine Khelif; Jérôme Toutain; Marie-Sophie Quittet; Sandrine Chantepie; Xavier Laffray; Samuel Valable; Didier Divoux; Fernando Sineriz; Emanuelle Pascolo-Rebouillat; Dulce Papy-Garcia; Denis Barritault; Omar Touzani; Myriam Bernaudin
Journal:  Theranostics       Date:  2018-11-12       Impact factor: 11.556

6.  A Rapid Response to Matrix Therapy With RGTA in Severe Epidermolysis Bullosa.

Authors:  Ali Al Malaq; Denis Barritault
Journal:  Eplasty       Date:  2012-10-17

7.  Differential therapeutic effects of PARP and ATR inhibition combined with radiotherapy in the treatment of subcutaneous versus orthotopic lung tumour models.

Authors:  Vanessa Tran Chau; Winchygn Liu; Marine Gerbé de Thoré; Lydia Meziani; Michele Mondini; Mark J O'Connor; Eric Deutsch; Céline Clémenson
Journal:  Br J Cancer       Date:  2020-06-17       Impact factor: 7.640

  7 in total

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