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A unique class of duocarmycin and CC-1065 analogues subject to reductive activation

机译:一类独特的杜卡霉素和CC-1065类似物经历还原活化

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摘要

N-Acyl O-amino phenol derivatives of CBI-TMI and CBI-indole2 are reported as prototypical members of a new class of reductively activated prodrugs of the duocarmycin and CC-1065 class of antitumor agents. The expectation being that hypoxic tumor environments, with their higher reducing capacity, carry an intrinsic higher concentration of “reducing” nucleophiles (e.g., thiols) capable of activating such derivatives (tunable N–O bond cleavage) increasing their sensitivity to the prodrug treatment. Preliminary studies indicate the prodrugs effectively release the free drug in functional cellular assays for cytotoxic activity approaching or matching the activity of the free drug, yet remain essentially stable and unreactive to in vitro DNA alkylation conditions (<0.1–0.01% free drug release), pH 7.0 phosphate buffer, and exhibit a robust half-life in human plasma (t½ = 3 h). Characterization of a representative O-(acylamino) prodrug in vivo indicate that they approach the potency and exceed the efficacy of the free drug itself (CBI-indole2) indicating that not only is the free drug effectively released from the inactive prodrug, but that they offer additional advantages related to a controlled or targeted release in vivo.
机译:据报道,CBI-TMI和CBI-吲哚2的N-酰基O-氨基苯酚衍生物是杜卡霉素和CC-1065类抗肿瘤剂的一类新的还原活化前药的典型成员。期望低氧肿瘤环境具有较高的还原能力,其内在的较高浓度的“还原”亲核试剂(例如硫醇)能够激活此类衍生物(可调节的N-O键断裂),从而提高其对前药治疗的敏感性。初步研究表明,前药在功能性细胞测定中可有效释放游离药物,以达到接近或匹配游离药物活性的细胞毒性活性,但对体外DNA烷基化条件基本保持稳定且无反应(游离药物释放<0.1–0.01%), pH 7.0磷酸盐缓冲液,在人血浆中具有很强的半衰期(t1 / 2 = 3 h)。体内代表性O-(酰基氨基)前药的表征表明它们接近效价并且超过了游离药物本身(CBI-indole2)的功效,这表明游离药物不仅可以有效地从非活性前药中释放出来,而且提供与体内控释或靶向释放有关的其他优势。

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