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A Cancer Gene Therapy Approach that Targets Tumor-associated Hyaluronan

机译:针对肿瘤相关透明质酸的癌症基因治疗方法

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The extracellular matrix glycosaminoglycan hyaluronan plays a key role in the development and pathogenesis of malignant disease. Reflecting its functional importance, the molecule is expressed at greatly elevated levels within many solid tumors. Although little explored, differences in the level of hyaluronan present in normal and malignant tissues could potentially be exploited to more effectively target gene therapy to tumor sites in vivo. As a first step toward this goal, we describe here a family of chimeric proteins in which the extracellular ligand-binding domain of the hyaluronan receptor CD44 is fused in-frame to the cytoplasmic “death domain” of the pro-apoptotic protein Fas. Although these chimeric proteins can be stably expressed on the surface of transduced tumor cells in the absence of hyaluronan, upon interaction with the ligand, apoptosis is rapidly induced. Both exogenous and endogenous tumor- produced hyaluronan can function as triggers, dramatically reducing clonogenic potential. Together, these studies help validate a broadly applicable gene therapy approach in which the presence of particular multivalent ligands within the tumor microenvironment can be exploited for therapeutic gain.
机译:细胞外基质糖胺聚糖透明质酸在恶性疾病的发展和发病机理中起关键作用。反映其功能重要性,该分子在许多实体瘤中以大大升高的水平表达。尽管很少进行探索,但是正常和恶性组织中存在的透明质酸水平的差异可能会被用来更有效地将基因治疗靶向体内肿瘤部位。作为朝着这个目标迈出的第一步,我们在这里描述一个嵌合蛋白家族,其中透明质酸受体CD44的胞外配体结合结构域与促凋亡蛋白Fas的胞质“死亡结构域”框内融合。尽管这些嵌合蛋白可以在不存在乙酰透明质酸的情况下在转导的肿瘤细胞表面上稳定表达,但与配体相互作用后,细胞凋亡迅速被诱导。肿瘤产生的外源性和内源性透明质酸均可以作为触发物,从而大大降低克隆形成的潜力。总之,这些研究有助于验证一种广泛适用的基因治疗方法,其中可以利用肿瘤微环境中特定多价配体的存在来获得治疗收益。

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