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Chemo-enzymatic Synthesis of Propionyl-ester-linked Taxol-monosaccharide Conjugate and its Drug Delivery System Using Hybrid-Bio-nanocapsules Targeting Brain Glioma Cells

机译:化学-酶法合成丙酰基-酯连接的紫杉醇-单糖缀合物及其药物递送系统使用针对脑胶质瘤细胞的杂交生物纳米胶囊。

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摘要

Taxol is recognized as one of the most potent anticancer agents used in the treatment of breast and ovarian cancers, which are common cancers in women. To overcome its shortcomings, that is, its low water-solubility that reduces drug loading capacity of DDS carriers when incorporating taxol, chemo-enzymatic synthesis of ester-linked taxol-glucose conjugate, i.e., 7-propionyltaxol 2″-O-α-D-glucoside, as a water soluble taxol prodrug was achieved by using a-glucosidase as a glucosylation catalyst. The water-solubility of 7-propionyltaxol 2″-O-α-D-glucoside (25 mM) was 63 fold higher than that of taxol (0.4 mM). The pre-S1 peptide which displays on the surface of bio-nanocapsules, which are nanoparticles composed of the hepatitis B virus surface antigen, was replaced with the antibody affinity motif of protein A. Conjugation of such bio-nanocapsules with anti-human epidermal growth factor receptor antibody gave hybrid bio-nanocapsules. The hybrid bio-nanocapsules were effective for delivering 7-propionyltaxol 2″-O-α-D-glucoside to human brain glioma cells. 7-Propionyltaxol 2″-O-α-D-glucoside was effectively hydrolyzed to give taxol in 95% by human glioma cells. The drug loading capacity of hybrid bio-nanocapsules incorporating 7-propionyltaxol 2″-O-α-D-glucoside was 120 times higher than that incorporating taxol itself.
机译:紫杉醇被认为是用于治疗乳腺癌和卵巢癌的最有效的抗癌药之一,乳腺癌和卵巢癌是女性的常见癌症。为了克服其缺点,即其低水溶性,在掺入紫杉醇时降低了DDS载体的载药量,化学酶法合成了酯连接的紫杉醇-葡萄糖偶联物,即7-丙酰紫杉醇2”-O-α-通过使用α-葡糖苷酶作为葡糖基化催化剂来获得作为水溶性紫杉醇前药的D-葡糖苷。 7-丙酰紫杉醇2″-O-α-D-葡萄糖苷(25mM)的水溶性比紫杉醇(0.4mM)高63倍。在生物纳米球表面上显示的pre-S1肽是由乙型肝炎病毒表面抗原组成的纳米颗粒,被蛋白质A的抗体亲和基序取代。此类生物纳米球与抗人表皮生长的结合因子受体抗体产生了杂交生物纳米粒。杂交生物纳米粒有效地将7-丙酰紫杉醇2″-O-α-D-葡萄糖苷递送至人脑神经胶质瘤细胞。人类神经胶质瘤细胞可有效水解7-丙酰紫杉醇2″-O-α-D-葡萄糖苷,得到95%的紫杉醇。掺入7-丙酰紫杉醇2″-O-α-D-葡萄糖苷的杂化生物纳米胶囊的载药量比掺入紫杉醇本身的载药量高120倍。

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