| Chinese Medical Journal, 2009, Vol. 122 No. 16:1947-1951 |
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| Endostatin derivative angiogenesis inhibitors |
| ZHENG Meng-jie |
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| Keywords:
angiogenesis·endostatin, tumor |
| Abstract: |
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Objective To throw light on the superiority of the anti-angiogenesis activity of endostatin (ES) derivatives by reviewing the recent progress in the field of ES molecular structure modification.
Data sources The data used in this article were mainly from PubMed with relevant English articles published from 1971 to May 2008. The search terms were “endostatin” and “angiothesis”.
Study selection Articles involved in the ES molecular structure modification and the original milestone articles were selected.
Results A number of ES derivatives were designed and studied to improve its clinical relevance. The modified ES with polyethylene glycol (PEG), low molecular weight heparin (LMWH) and IgG Fc domain extended the circulation half-life. Meanwhile the recombinant ESs showed more potent anti-tumor activity than native ES in mouse xenografts. Mutated ES also changed its anti-angiogenesis activity.
Conclusions The anti-angiogenesis treatment remains a promising tumor therapeutic strategy. New ES derivatives would be a good choice to meet the future challenge on clinical application of ES.
Chinese Medical Journal 2009;122(16):1947-1951
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This study was supported by : Simcere Internal Funds(No. SIM-52) |
| Free Full Text [ HTML
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] Abstract download [TXT | XML] |
ZHENG Meng-jie Department of New Drug R&D, Jiangsu Simcere Pharmaceutical R&D Co., Ltd., Nanjing, Jiangsu 210042, China
Correspondence to:
ZHENG Meng-jie
Department of New Drug R&D, Jiangsu Simcere Pharmaceutical R&D Co., Ltd., Nanjing, Jiangsu 210042, China
(Tel:86-25-85566666 ext 1785 Email:zhengmengjie@simcere.com )
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