| Literature DB >> 26950165 |
Li Ran1, Xiaohua Tan2, Yanchun Li1, Huafeng Zhang1, Ruihua Ma3, Tiantian Ji3, Wenqian Dong1, Tong Tong1, Yuying Liu1, Degao Chen1, Xiaonan Yin1, Xiaoyu Liang1, Ke Tang1, Jingwei Ma1, Yi Zhang1, Xuetao Cao1, Zhuowei Hu4, Xiaofeng Qin5, Bo Huang6.
Abstract
Oncolytic viruses have been utilized for the treatment of various cancers. However, delivery of the viral particles to tumor cells remains a major challenge. Microparticles (MP) are vesicle forms of plasma membrane fragments of 0.1-1 μm in size that are shed by cells. We have previously shown the delivery of chemotherapeutic drugs using tumor cell-derived MPs (T-MP). Here we report that T-MPs can be utilized as a unique carrier system to deliver oncolytic adenoviruses to human tumors, leading to highly efficient cytolysis of tumor cells needed for in vivo treatment efficacy. This T-MP-mediated oncolytic virotherapy approach holds multiple advantages, including: 1) delivery of oncolytic adenovirus by T-MPs is able to avoid the antiviral effect of host antibodies; 2) delivery of oncolytic adenovirus by T-MPs is not limited by virus-specific receptor that mediates the entry of virus into tumor cells; 3) T-MPs are apt at delivering oncolytic adenoviruses to the nucleus of tumor cells as well as to stem-like tumor-repopulating cells for the desired purpose of killing them. These findings highlight a novel oncolytic adenovirus delivery system with highly promising clinical applications.Entities:
Keywords: Cancer therapy; Delivery system; Microparticles; Oncolytic adenovirus
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Year: 2016 PMID: 26950165 DOI: 10.1016/j.biomaterials.2016.02.025
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479