Literature DB >> 20925470

Temozolomide: therapeutic limitations in the treatment of adult high-grade gliomas.

Marc C Chamberlain1.   

Abstract

Temozolomide-based chemotherapy represents an incremental improvement in the treatment of patients with high-grade gliomas. Notwithstanding a survival benefit in a subset of patients with high-grade gliomas, temozolomide (TMZ; Temodar®, Schering-Plough Pharmaceuticals, NJ, USA) is the primarily palliative treatment for the vast majority of patients. Indeed, for patients with newly diagnosed glioblastoma, the median increase in survival for treatment with TMZ and radiotherapy is only 2.5 months compared with radiotherapy alone. Additionally, recent studies suggest that 60-75% of patients with glioblastoma derive no benefit from treatment with TMZ. For the treatment of recurrent anaplastic gliomas, more than 50% of patients fail TMZ treatment with cancer progression at 6 months, demonstrating that TMZ is only a modestly effective chemotherapy. In addition, 15-20% of patients treated with TMZ develop clinically significant toxicity, which can leave further treatment unsafe. Despite the availability of TMZ, there is still a substantial need for a chemotherapeutic agent that is more effective and safe. In fact, there still remains a significant unmet need for more effective treatments of high-grade gliomas (improved palliation or cure), whether that treatment be by surgery, radiotherapy, chemotherapy or any yet to be developed type of treatment, such as 'targeted therapies'.

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Year:  2010        PMID: 20925470     DOI: 10.1586/ern.10.32

Source DB:  PubMed          Journal:  Expert Rev Neurother        ISSN: 1473-7175            Impact factor:   4.618


  69 in total

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4.  Lidocaine suppresses glioma cell proliferation by inhibiting TRPM7 channels.

Authors:  Tiandong Leng; Suizhen Lin; Zhigang Xiong; Jun Lin
Journal:  Int J Physiol Pathophysiol Pharmacol       Date:  2017-04-15

5.  Oxidative cytotoxic agent withaferin A resensitizes temozolomide-resistant glioblastomas via MGMT depletion and induces apoptosis through Akt/mTOR pathway inhibitory modulation.

Authors:  Patrick T Grogan; Jann N Sarkaria; Barbara N Timmermann; Mark S Cohen
Journal:  Invest New Drugs       Date:  2014-04-10       Impact factor: 3.850

6.  miR-125b inhibits Connexin43 and promotes glioma growth.

Authors:  Zheng Jin; Songbai Xu; Hongquan Yu; Boyu Yang; Hongguang Zhao; Gang Zhao
Journal:  Cell Mol Neurobiol       Date:  2013-09-18       Impact factor: 5.046

7.  Metformin selectively affects human glioblastoma tumor-initiating cell viability: A role for metformin-induced inhibition of Akt.

Authors:  Roberto Würth; Alessandra Pattarozzi; Monica Gatti; Adirano Bajetto; Alessandro Corsaro; Alessia Parodi; Rodolfo Sirito; Michela Massollo; Cecilia Marini; Gianluigi Zona; Daniela Fenoglio; Gianmario Sambuceti; Gilberto Filaci; Antonio Daga; Federica Barbieri; Tullio Florio
Journal:  Cell Cycle       Date:  2012-12-19       Impact factor: 4.534

8.  TRPM7 channel inhibition mediates midazolam-induced proliferation loss in human malignant glioma.

Authors:  Jingkao Chen; Yunling Dou; Xiaoke Zheng; Tiandong Leng; Xiaofang Lu; Ying Ouyang; Huawei Sun; Fan Xing; Jialuo Mai; Jiayu Gu; Bingzheng Lu; Guangmei Yan; Jun Lin; Wenbo Zhu
Journal:  Tumour Biol       Date:  2016-09-14

9.  Encapsulation of temozolomide in a tumor-targeting nanocomplex enhances anti-cancer efficacy and reduces toxicity in a mouse model of glioblastoma.

Authors:  Sang-Soo Kim; Antonina Rait; Eric Kim; James DeMarco; Kathleen F Pirollo; Esther H Chang
Journal:  Cancer Lett       Date:  2015-09-02       Impact factor: 8.679

10.  Overexpression of SASH1 related to the decreased invasion ability of human glioma U251 cells.

Authors:  Liu Yang; Mei Liu; Zhikai Gu; Jianguo Chen; Yaohua Yan; Jian Li
Journal:  Tumour Biol       Date:  2012-08-23
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