光动力疗法
纳米医学
光敏剂
康布雷他汀
癌症研究
体内
化学
药理学
外渗
癌症治疗
医学
癌症
纳米技术
内科学
材料科学
病理
纳米颗粒
细胞生物学
微管
生物
有机化学
生物技术
微管蛋白
作者
Yibin Liu,Fu‐An Deng,Rongrong Zheng,Xiayun Chen,Linping Zhao,Baixue Yu,Ali Chen,Xueyan Jiang,Hong Cheng,Shiying Li
标识
DOI:10.1016/j.jcis.2021.12.128
摘要
Tumor vascular blockade is a promising strategy for adjuvant cancer treatment. In this work, a self-delivery nanomedicine is developed based on a vascular disruptor and photosensitizer for tumor synergistic therapy. Specifically, this nanomedicine (designated as CeCA) is comprised of combretastatin A4 (CA4) and chlorine e6 (Ce6) by self-assembly technique. Among which, CA4 could not only induce tubulin inhibition for chemotherapy but also disrupt the vasculature to cause tumor hemorrhage. Moreover, Ce6 is able to generate lots of singlet oxygen (1O2) for synergistic photodynamic therapy (PDT) under light irradiation. It is interesting that the carrier-free CeCA possessed a favorable stability and an improved cellular uptake behavior. After intravenous administration, CeCA prefers to accumulate at tumor site for vascular disruption-supplemented chemo-photodynamic therapy. Notably, CeCA is prepared without additional carriers, which avoids the system toxicity raised by excipients. Consequently, CeCA greatly inhibits the tumor growth and leads to a low side effect in vivo. It might open a window in the development of self-supplementary nanomedicine for synergistic tumor treatment.
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