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Titlebook: Camptothecins in Cancer Therapy; Val R. Adams,Thomas G. Burke Book 2005 Humana Press 2005 DNA.biochemistry.brain.brain tumors.cancer.cance

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發(fā)表于 2025-3-25 04:22:43 | 只看該作者
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發(fā)表于 2025-3-26 02:23:11 | 只看該作者
Clinical Experience With 9-Aminocamptothecinical research. Thus a careful review of the early clinical and pharmacological trials of 9-AC may help us to understand why 9-AC has not shown more meaningful antitumor activity and may also provide important lessons for the future drug development of novel camptothecins and other topoisomerase I (TOP-I) targeting agents.
27#
發(fā)表于 2025-3-26 07:43:18 | 只看該作者
Irinotecan–.). In turn, SN-38 can be conjugated to SN-38 β-glucuronide (.,.). CPT-11 is also metabolized to an aminopentanocarboxylic (APC), metabolite (. Fig. 1), and other minor, mostly inactive, products by cytochrome P450 3A4/5 (.–.).
28#
發(fā)表于 2025-3-26 11:29:28 | 只看該作者
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發(fā)表于 2025-3-26 15:56:49 | 只看該作者
Neuroinflammation in Alzheimer’s Diseaseication reaction (.). The rate of relegation is normally much faster than is the rate of cleavage (.). This ensures that the steady state concentration of the covalent 3′-phosphotyrosyl TOP-I-DNA complex is extremely low. Several DNA lesions and drugs, however, have been shown to stabilize the coval
30#
發(fā)表于 2025-3-26 19:51:26 | 只看該作者
https://doi.org/10.1007/978-3-662-05426-0OH DNA end attacks the phosphotyrosyl bond to restore the phosphodiester backbone bond and liberate the enzyme. The formation of a covalent Top1p-DNA complex is the hallmark of topoisomerase-catalyzed reactions and acts to conserve the energy of the cleaved DNA bond such that the concerted nicking a
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