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首页> 外文期刊>Cancer letters >Epidermal growth factor receptor-targeted photosensitizer selectively inhibits EGFR signaling and induces targeted phototoxicity in ovarian cancer cells
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Epidermal growth factor receptor-targeted photosensitizer selectively inhibits EGFR signaling and induces targeted phototoxicity in ovarian cancer cells

机译:表皮生长因子受体靶向的光敏剂选择性抑制EGFR信号传导并诱导卵巢癌细胞靶向光毒性

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摘要

Targeted photosensitizer delivery to EGFR-expressing cells was achieved in the present study using a high purity, targeted photoimmunoconjugate (PIC). When the PDT agent, benzoporphyrin derivative monoacid ring A (BPD) was coupled to an EGFR-targeting antibody (cetuximab), we observed altered cellular localization and selective phototoxicity of EGFR-positive cells, but no phototoxicity of EGFR-negative cells. Cetuximab in the PIC formulation blocked EGF-induced activation of the EGFR and downstream signaling pathways. Our results suggest that photoimmunotargeting is a useful dual strategy for the selective destruction of cancer cells and also exerts the receptor-blocking biological function of the antibody.
机译:在本研究中,使用高纯度,靶向光免疫偶联物(PIC)实现了向EGFR表达细胞的靶向光敏剂递送。当PDT剂苯并卟啉衍生物单酸环A(BPD)与EGFR靶向抗体(cetuximab)偶联时,我们观察到改变的细胞定位和EGFR阳性细胞的选择性光毒性,但未观察到EGFR阴性细胞的光毒性。 PIC制剂中的西妥昔单抗阻断了EGF诱导的EGFR激活和下游信号通路。我们的结果表明,光免疫靶向是选择性破坏癌细胞的有用双重策略,并且还发挥了抗体的受体阻断生物学功能。

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