Synthesis and characterization of Fulvestrant and Paclitaxel conjugates with polyamidoamine dendrimer fourth generation

Konrad Wróbel, Stanisław Wołowiec
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Abstract

Introduction and aim. Poorly soluble anticancer drugs can be attached covalently into biologically inert macromolecule in order to administrate a drug as water soluble form. It was proven that covalent linkers, for instance amide or carbamate bonds are susceptible to hydrolysis. Thus the attached drug can be released from the conjugates in tissue, specifically within the targeted cell. We aimed at construction of water soluble conjugates of Fulvestrant and Paclitaxel with PAMAM G4 dendrimer. In order to obtain water soluble conjugates the amine groups were substituted with R-glycidol. Material and methods. Polyamidoamine dendrimer of fourth generation was synthesized and examined by detailed NMR analysis in water and in DMSO. The conjugates were covalently linked to amine groups of PAMAM after activation of Fulvestrant 17-OH group with 4-nitrophenylchloroformate and activation of end-carboxyl group of Paclitaxel succinate. Results. The method of binary conjugate PAMAMG4-Fulvestrant-Paclitaxel synthesis was elaborated and the product was characterized by physicochemical methods. Conclusion. The glycidylated PAMAMG4-Fulvestrant-Paclitaxel conjugate is better soluble in water than unconverted drugs.
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富维司汀与紫杉醇第四代聚胺胺树状大分子缀合物的合成与表征
介绍和目的。难溶性抗癌药物可以以共价方式附着在生物惰性大分子中,以便以水溶性形式给药。事实证明,共价连接物,例如酰胺或氨基甲酸酯键容易水解。因此,附着的药物可以从组织中的偶联物中释放出来,特别是在靶细胞内。以PAMAM - G4树状大分子为载体,构建富维司汀和紫杉醇水溶性缀合物。为了得到水溶性的偶联物,胺基被r -甘二醇取代。材料和方法。合成了第四代聚胺胺树状大分子,并在水中和DMSO中进行了详细的核磁共振分析。在4-硝基苯氯甲酸酯活化富维司汀17-OH基团和琥珀酸紫杉醇端羧基活化后,这些缀合物与PAMAM的胺基共价连接。结果。阐述了二元共轭pamamg4 - fulvestrant -紫杉醇的合成方法,并用物化方法对产物进行了表征。结论。甘油酰化pamamg4 -富维司汀-紫杉醇缀合物比未转化的药物更易溶于水。
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