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Cytotoxicity and Selectivity in Skin Cancer by SapC-DOPS Nanovesicles

机译:细胞毒性和选择性皮肤癌由sapC-DOps纳囊泡

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摘要

Squamous cell carcinoma (SCC) and melanoma are malignant human cancers of the skin with an annual mortality that exceed 10,000 cases every year in the USA alone. In this study, the lysosomal protein saposin C (SapC) and the phospholipid dioloylphosphatidylserine (DOPS) were assembled into cancer-selective nanovesicles (SapC-DOPS) and successfully tested using several in vitro and in vivo skin cancer models. Using MTT assay that measures the percentage of cell death, SapC-DOPS cytotoxic effect on three skin tumor cell lines (squamous cell carcinoma, SK-MEL-28, and MeWo) was compared to two normal nontumorigenic skin cells lines, normal immortalized keratinocyte (NIK) and human fibroblast cell (HFC). We observed that the nanovesicles selectively killed the skin cancer cells by inducing apoptotic cell death whereas untransformed skin cancer cells remained unaffected. Using subcutaneous skin tumor xenografts, animals treated with SapC-DOPS by subcutaneous injection showed a 79.4 % tumor reduced compared to the control after 4 days of treatment. We observed that the nanovesicles killed skin cancer cells by inducing apoptotic cell death compared to the control as revealed by TUNEL staining of xenograft tumor sections.
机译:鳞状细胞癌(SCC)和黑色素瘤是皮肤恶性人类癌症,仅在美国每年的年死亡率就超过10,000例。在这项研究中,溶酶体蛋白saposin C(SapC)和磷脂二oloyl磷脂酰丝氨酸(DOPS)被组装成癌症选择性纳米囊泡(SapC-DOPS),并使用几种体外和体内皮肤癌模型成功进行了测试。使用MTT法测量细胞死亡百分比,将SapC-DOPS对三种皮肤肿瘤细胞系(鳞状细胞癌,SK-MEL-28和MeWo)的细胞毒性作用与两种正常的非致瘤性皮肤细胞系,永生化的角质形成细胞( NIK)和人类成纤维细胞(HFC)。我们观察到,纳米囊泡通过诱导凋亡细胞死亡选择性地杀死皮肤癌细胞,而未转化的皮肤癌细胞仍然不受影响。使用皮下皮肤肿瘤异种移植物,经皮下注射SapC-DOPS处理的动物与对照组相比,治疗4天后肿瘤减少了79.4%。我们观察到,与对照相比,纳米囊泡通过诱导凋亡性细胞死亡杀死了皮肤癌细胞,这通过异种移植肿瘤切片的TUNEL染色揭示。

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