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Targeting the tumour microenvironment with an enzyme-responsive drug delivery system for the efficient therapy of breast and pancreatic cancers

机译:用酶反应药物递送系统靶向肿瘤微环境可有效治疗乳腺癌和胰腺癌

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摘要

The development of novel therapeutic strategies allowing the destruction of tumour cells while sparing healthy tissues is one of the main challenges of cancer chemotherapy. Here, we report on the design and antitumour activity of a low-molecular-weight drug delivery system programmed for the selective release of the potent monomethylauristatin E in the tumour microenvironment of solid tumours. After intravenous administration, this compound binds covalently to plasmatic albumin through Michael addition, thereby enabling its passive accumulation in tumours where extracellular β-glucuronidase initiates the selective release of the drug. This targeting device produces outstanding therapeutic efficacy on orthotopic triple-negative mammary and pancreatic tumours in mice (50% and 33% of mice with the respective tumours cured), leading to impressive reduction or even disappearance of tumours without inducing side effects.
机译:允许破坏肿瘤细胞同时保留健康组织的新型治疗策略的发展是癌症化学疗法的主要挑战之一。在这里,我们报道了一种低分子量药物递送系统的设计和抗肿瘤活性,该系统设计用于在实体瘤的肿瘤微环境中选择性释放有效的单甲基奥他汀E。静脉内给药后,该化合物通过迈克尔加成与血浆白蛋白共价结合,从而使其能够在肿瘤中被动蓄积,其中细胞外β-葡萄糖醛酸苷酸酶开始选择性释放药物。该靶向装置对小鼠的原位三阴性乳腺和胰腺肿瘤(分别治愈了50%和33%的小鼠)产生了出色的治疗效果,从而导致了令人印象深刻的肿瘤减少甚至消失而没有引起副作用。

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