| Literature DB >> 26438971 |
Lin Tao1, Feng Zhu2, Feng Xu3, Zhe Chen4, Yu Yang Jiang5, Yu Zong Chen6.
Abstract
Recent investigations have suggested that anticancer therapeutics may be enhanced by co-targeting the primary anticancer target and the corresponding drug escape pathways. Whether this strategy confers statistically significant clinical advantage has not been systematically investigated. This question was probed by the evaluation of the clinical status and the multiple targets of 23 approved and 136 clinical trial multi-target anticancer drugs with particular focus on those co-targeting EGFR, HER2, Abl, VEGFR2, mTOR, PI3K, Alk, MEK, KIT, and DNA topoisomerase, and some of the 14, 7, 13, 20, 6, 5, 7, 2, 4 and 10 cancer drug escape pathways respectively. Most of the approved (73.9%) and phase III (75.0%), the majority of the Phase II (62.8%) and I (53.6%), and the minority of the discontinued (35.3%) multi-target drugs were found to co-target cancer drug escape pathways. This suggests that co-targeting anticancer targets and drug escape pathways confer significant clinical advantage and such strategy can be more extensively explored.Entities:
Keywords: Afatinib (Pubmed CID: 10184653); Anticancer; Co-target; Drug escape pathways; Erlotinib (Pubmed CID: 176870); Gefitinib (Pubmed CID: 123631); Lenvatinib (Pubmed CID: 9823820); Multi-target; Pazopanib (Pubmed CID: 10113978); Systematically; XL647 (Pubmed CID: 10458325)
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Year: 2015 PMID: 26438971 DOI: 10.1016/j.phrs.2015.09.019
Source DB: PubMed Journal: Pharmacol Res ISSN: 1043-6618 Impact factor: 7.658