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GUCY2C lysosomotropic endocytosis delivers immunotoxin therapy to metastatic colorectal cancer.

机译:GUCY2C溶酶体内吞作用为转移性结直肠癌提供免疫毒素治疗。

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摘要

The emergence of targeted cancer therapy has been limited by the paucity of determinants which are tumor-specific and generally associated with disease, and have cell dynamics which effectively deploy cytotoxic payloads. Guanylyl cyclase C (GUCY2C) may be ideal for targeting because it is normally expressed only in insulated barrier compartments, including intestine and brain, but over-expressed by systemic metastatic colorectal tumors. Here, we reveal that GUCY2C rapidly internalizes from the cell surface to lysosomes in intestinal and colorectal cancer cells. Endocytosis is independent of ligand binding and receptor activation, and is mediated by clathrin. This mechanism suggests a design for immunotoxins comprising a GUCY2C-directed monoclonal antibody conjugated through a reducible disulfide linkage to ricin A chain, which is activated to a potent cytotoxin in lysosomes. Indeed, this immunotoxin specifically killed GUCY2C-expressing colorectal cancer cells in a lysosomal- and clathrin-dependent fashion. Moreover, this immunotoxin reduced pulmonary tumors u3e80% (p
机译:靶向性癌症治疗的出现受到缺乏决定因素的限制,这些决定因素是肿瘤特异性的并且通常与疾病相关,并且具有有效部署细胞毒性有效载荷的细胞动力学。鸟苷酸环化酶C(GUCY2C)可能是靶向的理想选择,因为它通常仅在包括肠和脑在内的隔热屏障区室中表达,但在全身性转移性结直肠肿瘤中过表达。在这里,我们揭示了GUCY2C在肠道和大肠癌细胞中从细胞表面迅速内化到溶酶体。内吞作用独立于配体结合和受体激活,并由网格蛋白介导。该机制提示了一种针对免疫毒素的设计,该免疫毒素包括通过可还原的二硫键与蓖麻毒蛋白A链偶联的GUCY2C定向单克隆抗体,蓖麻蛋白A链被溶酶体中的有效细胞毒素激活。实际上,这种免疫毒素以溶酶体和网格蛋白依赖性方式特异性杀死表达GUCY2C的结直肠癌细胞。而且,这种免疫毒素减少了肺部肿瘤的发生率

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