| Literature DB >> 28846068 |
Minfeng Chen1,2, Xueping Lei1,2, Changzheng Shi3, Maohua Huang1,2, Xiaobo Li1,2, Baojian Wu1,2, Zhengqiu Li1,2, Weili Han4, Bin Du3, Jianyang Hu1,2, Qiulin Nie1,2, Weiqian Mai1,2, Nan Ma1,2, Nanhui Xu1,2, Xinyi Zhang1,2, Chunlin Fan1,2, Aihua Hong5, Minghan Xia3, Liangping Luo3, Ande Ma4, Hongsheng Li6, Qiang Yu7, Heru Chen1,2, Dongmei Zhang1,2, Wencai Ye1,2.
Abstract
Blood vessels in the tumor periphery have high pericyte coverage and are resistant to vascular disrupting agents (VDAs). VDA treatment resistance leads to a viable peripheral tumor rim that contributes to treatment failure and disease recurrence. Here, we provide evidence to support a hypothesis that shifting the target of VDAs from tumor vessel endothelial cells to pericytes disrupts tumor peripheral vessels and the viable rim, circumventing VDA treatment resistance. Through chemical engineering, we developed Z-GP-DAVLBH (from the tubulin-binding VDA desacetylvinblastine monohydrazide [DAVLBH]) as a prodrug that can be selectively activated by fibroblast activation protein α (FAPα) in tumor pericytes. Z-GP-DAVLBH selectively destroys the cytoskeleton of FAPα-expressing tumor pericytes, disrupting blood vessels both within the core and around the periphery of tumors. As a result, Z-GP-DAVLBH treatment eradicated the otherwise VDA-resistant tumor rim and led to complete regression of tumors in multiple lines of xenografts without producing the drug-related toxicity that is associated with similar doses of DAVLBH. This study demonstrates that targeting tumor pericytes with an FAPα-activated VDA prodrug represents a potential vascular disruption strategy in overcoming tumor resistance to VDA treatments.Entities:
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Year: 2017 PMID: 28846068 PMCID: PMC5617663 DOI: 10.1172/JCI94258
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808