5-iodo-2'-deoxyuridine-protein conjugates: synthesis and enzymatic degradation.

J Baranowska-Kortylewicz, S J Adelstein, A I Kassis
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引用次数: 7

Abstract

Several halogenated analogs of thymidine and cytidine possess antineoplastic and antiviral activity. They are also powerful sensitizers of bacterial and mammalian cells to lethal effects of x-irradiation. An important factor limiting the effectiveness of these agents in therapy is their extremely short half-life in circulation due to rapid hepatic dehalogenation. An approach to this problem is to deliver the drug directly to its target using monoclonal antibodies. This study evaluates the lysosomotropic delivery systems of halogenated pyrimidines using 5-iodo-2'-deoxyuridine [IUdR] as a model. IUdR, derivatized and activated at either the 3'- or the 5'-position forms covalent adducts with the epsilon-amino groups of the lysine residues in proteins (bovine serum albumin [BSA], and immunoglobulins [IgG]). Two methods suitable for conjugation of IUdR to proteins involving either the formation of acyl-imidazoles in the reaction of IUdR succinates with N,N'-carbonyldiimidazole or the preparation of N-succinimidyl esters of IUdR succinates were established. Both derivatives express comparable reactivity toward proteins. The degree of IUdR incorporation is easily controlled by the ratio of reagents. The succinate "arm" linking IUdR to protein is susceptible to lysosomal hydrolysis in vitro releasing intact IUdR. The half-life of the IUdR-IgG conjugate in the presence of the lysosomal enzymes was shown to be approximately twice that of the IUdR-BSA conjugate.

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5-碘-2'-脱氧尿苷蛋白缀合物:合成和酶降解。
胸苷和胞苷的几种卤代类似物具有抗肿瘤和抗病毒活性。它们也是细菌和哺乳动物细胞对x射线致死效应的强致敏剂。限制这些药物在治疗中的有效性的一个重要因素是它们在循环中的半衰期极短,由于快速的肝去卤。解决这个问题的一种方法是使用单克隆抗体将药物直接输送到其靶点。本研究以5-碘-2'-脱氧尿苷[IUdR]为模型,评价了卤代嘧啶的溶酶体性传递系统。IUdR在蛋白质(牛血清白蛋白[BSA]和免疫球蛋白[IgG])的3'或5'位置衍生和活化,与赖氨酸残基的ε -氨基形成共价加合物。建立了两种适合于IUdR与蛋白质偶联的方法,即在IUdR琥珀酸酯与N,N'-羰基二咪唑反应中形成酰基咪唑或制备IUdR琥珀酸酯的N-琥珀酰亚胺酯。这两种衍生物对蛋白质的反应性相当。IUdR的掺入程度很容易通过试剂的比例来控制。连接IUdR与蛋白质的琥珀酸“臂”在体外易受溶酶体水解释放完整的IUdR。在溶酶体酶存在下,IUdR-IgG偶联物的半衰期大约是IUdR-BSA偶联物的两倍。
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