N4-(4-羧基丁基)- α -c与乙二胺引入的葡聚糖缀合物的抗肿瘤特性及其对胞苷脱氨酶的抗性。

Drug design and delivery Pub Date : 1990-10-01
H Onishi, P Pithayanukul, T Nagai
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引用次数: 0

摘要

通过对右旋糖酐的氧化,以及氧化右旋糖酐与二氨基烷烃反应形成的希夫碱的还原,制备了几种引入二氨基烷烃的右旋糖酐,并对其作为药物载体进行了评价。制备了N4-(4-羧基buryryl)-1- β - d -阿拉伯糖醛酸胞嘧啶(glu-ara-C)与这些药物载体的偶联物,并对选定的偶联物进行了体内检测,考察了其对胞苷脱氨酶的抑制作用。通过对BDF1小鼠的化学特性和毒性评价,发现在10%氧化条件下制备的乙二胺引入葡聚糖是最有用的药物载体。从葡萄糖-ara-C和乙二胺引入的葡聚糖2000中获得的结合物在携带L1210白血病细胞的BDF1小鼠中显示出很高的抗肿瘤活性,在相对较低的剂量为100 mg当量ara-C/kg时显著。在1- β - d -阿拉伯糖醛酸胞嘧啶快速降解为1- β - d -阿拉伯糖醛酸胞嘧啶的条件下,葡萄糖-阿拉- c和缀合物不受胞苷脱氨酶的影响。
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Antitumor characteristics of the conjugate of N4-(4-carboxybutyryl)-ara-C with ethylenediamine-introduced dextran and its resistance to cytidine deaminase.

By oxidation of dextran, and reduction of the Schiff bases formed by reaction of the oxidised dextran with diaminoalkanes, several diaminoalkane-introduced dextrans were prepared and evaluated as drug carriers. Conjugates between N4-(4-carboxyburyryl)-1-beta-D-arabinofuranosylcytosine (glu-ara-C) and such drug carriers were prepared, and selected conjugates were tested in vivo, and investigated for inhibitory effects on cytidine deaminase. Ethylenediamine-introduced dextran prepared under 10% oxidation conditions was found to be most useful as a drug carrier from its chemical characteristics and toxicity evaluation in BDF1 mice. The conjugate obtained from glu-ara-C and ethylenediamine-introduced dextran 2000 showed high antitumor activity, significant at the relatively low dose of 100 mg equivalent ara-C/kg, in BDF1 mice bearing L1210 leukemia cells. Glu-ara-C and the conjugate were unaffected by cytidine deaminase under conditions in which 1-beta-D-arabinofuranosylcytosine was degraded rapidly to 1-beta-D-arabinofuranosyluracil.

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