| Literature DB >> 27619239 |
Xu Song1, Zhuoya Wan1, Tijia Chen1, Yao Fu1, Kejun Jiang1, Xiaoli Yi1, Huan Ke1, Jianxia Dong1, Liuqing Yang1, Lin Li1, Xun Sun1, Tao Gong2, Zhirong Zhang3.
Abstract
Finding effective cures against aggressive malignancy remains a major challenge in cancer chemotherapy. Here, we report a "tadpole"-like peptide by covalently conjugating the alanine-alanine-asparagine "tail" residual to the cyclic tumor homing peptide iRGD (CCRGDKGPDC) to afford nRGD, which significantly enhanced tumoricidal effects of doxorubicin, by either co-administered as a physical mixture or as a targeting ligand covalently conjugated to the liposomal carrier. Given twice at an equivalent dose of 5 mg/kg, doxorubicin loaded liposomes modified with nRGD (nRGD-Lipo-Dox) showed excellent antitumor efficacy in 4T1 breast cancer mice, of which 44.4% remained alive for over 90 days without recurrence during the period of investigation. The dramatic improvement in antitumor efficacy was attributed to nRGD-Lipo-Dox which appeared to specifically interact with tumor vascular endothelial cells to achieve efficient tumor penetration, and modulate tumor microenvironment with depletion of tumor associated macrophages.Entities:
Keywords: Legumain; Tumor associated macrophage; Tumor microenvironment; iRGD; nRGD
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Year: 2016 PMID: 27619239 DOI: 10.1016/j.biomaterials.2016.09.001
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479