作者
Ryohei Katayama,Bin Gong,Noriko Togashi,Masaharu Miyamoto,Masaki Kiga,Shiho Iwasaki,Yasuki Kamai,Yoshihiro Tominaga,Yasuyuki Takeda,Yoshiko Kagoshima,Yuki Shimizu,Yosuke Seto,Tomoko Oh‐hara,Sumie Koike,Naoki Nakao,Hiroyuki Hanzawa,K. Watanabe,Satoshi Yoda,Noriko Yanagitani,Aaron N. Hata,Alice T. Shaw,Makoto Nishio,Naoya Fujita,Takeshi Isoyama
摘要
Abstract ROS1 gene rearrangement was observed in around 1–2 % of NSCLC patients and in several other cancers such as cholangiocarcinoma, glioblastoma, or colorectal cancer. Crizotinib, an ALK/ROS1/MET inhibitor, is highly effective against ROS1 -rearranged lung cancer and is used in clinic. However, crizotinib resistance is an emerging issue, and several resistance mechanisms, such as secondary kinase-domain mutations (e.g., ROS1-G2032R) have been identified in crizotinib-refractory patients. Here we characterize a new selective ROS1/NTRK inhibitor, DS-6051b, in preclinical models of ROS1- or NTRK-rearranged cancers. DS-6051b induces dramatic growth inhibition of both wild type and G2032R mutant ROS1–rearranged cancers or NTRK-rearranged cancers in vitro and in vivo . Here we report that DS-6051b is effective in treating ROS1- or NTRK-rearranged cancer in preclinical models, including crizotinib-resistant ROS1 positive cancer with secondary kinase domain mutations especially G2032R mutation which is highly resistant to crizotinib as well as lorlatinib and entrectinib, next generation ROS1 inhibitors.
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