Wang Ying, Xin Dingcheng, Liu Kaijian, Xiang Jiannan
Biomedical Engineering Center, Hunan University, Changsha, 410082, China.
Pharm Res. 2009 Apr;26(4):785-93. doi: 10.1007/s11095-008-9762-5. Epub 2008 Nov 18.
The heparin-paclitaxel conjugates using amino acid as linker (HD2), with low anticoagulant activity, the similar anticancer activity as paclitaxel, offer great potential for further investigation.
Two types of heparin-paclitaxel conjugates (HD) have been developed, in which O-acetylated heparin as carrier conjugates with paclitaxel by direct ester bond (HD1) and by inserting different amino acids as spacers, including valine, leucine, and phenylalanine (HD2a, HD2b, and HD2c), respectively. Specifically, mixed anhydride groups of carrier as activating intermediates mediate the synthesis of prodrugs. The HD conjugates are characterized by (1)H NMR, FT-IR and GPC. The percentage weight of drug and hydrolysis rate for HD are detected by UV and HPLC. The anticoagulant activity and cell cycle of MCF-7 of HD are measured by APTT and FCM, respectively.
HD2 conjugates show better solubility and faster hydrolysis rates than those of HD1. Meanwhile, the anticoagulant activity of HD is reduced and FCM analysis show that MCF-7 cells treated with HD are arrested in the G2/M phase of cell cycle.
Amino acids as linkers between paclitaxel and carrier are appropriate to facilitate the release of paclitaxel from carrier. Mixed anhydrides mediate the synthesis of prodrugs and HD2 conjugates are expected to further investigate in vivo experiment.
以氨基酸为连接子的肝素 - 紫杉醇缀合物(HD2)具有低抗凝活性,抗癌活性与紫杉醇相似,具有很大的进一步研究潜力。
已开发出两种类型的肝素 - 紫杉醇缀合物(HD),其中以O - 乙酰化肝素为载体,通过直接酯键与紫杉醇缀合(HD1),并通过插入不同的氨基酸作为间隔基,分别包括缬氨酸、亮氨酸和苯丙氨酸(HD2a、HD2b和HD2c)。具体而言,载体的混合酸酐基团作为活化中间体介导前药的合成。HD缀合物通过(1)H NMR、FT - IR和GPC进行表征。HD的药物重量百分比和水解速率通过UV和HPLC检测。HD的抗凝活性和MCF - 7细胞周期分别通过APTT和FCM测量。
HD2缀合物比HD1具有更好的溶解性和更快的水解速率。同时,HD的抗凝活性降低,FCM分析表明用HD处理的MCF - 7细胞停滞在细胞周期的G2/M期。
氨基酸作为紫杉醇与载体之间的连接子有利于紫杉醇从载体中释放。混合酸酐介导前药的合成,HD2缀合物有望进一步进行体内实验研究。
