Synthesis and SAR of acyclic HCV NS3 protease inhibitors with novel P4-benzoxaborole moieties

Authors :: Li, Xianfeng
Zhang, Suoming
Zhang, Yong-Kang
Liu, Yang
Ding, Charles Z.
Zhou, Yasheen
Plattner, Jacob J.
Baker, Stephen J.
Bu, Wei
Liu, Liang
Kazmierski, Wieslaw M.
Duan, Maosheng
Grimes, Richard M.
Wright, Lois L.
Smith, Gary K.
Jarvest, Richard L.
Ji, Jing-Jing
Cooper, Joel P.
Tallant, Matthew D.
Crosby, Renae M.
Source :: Bioorganic & Medicinal Chemistry Letters. Apr2011, Vol. 21 Issue 7, p2048-2054. 7p.
Publication Year :: 2011
Abstract: Abstract: We have synthesized and evaluated a new series of acyclic P4-benzoxaborole-based HCV NS3 protease inhibitors. Structure–activity relationships were investigated, leading to the identification of compounds 5g and 17 with low nanomolar potency in the enzymatic and cell-based replicon assay. The linker-truncated compound 5j was found to exhibit improved absorption and oral bioavailability in rats, suggesting that further reduction of molecular weight and polar surface area could result in improved drug-like properties of this novel series. [Copyright &y& Elsevier]

Subjects :: *PROTEASE inhibitors
*BORON compounds
*INORGANIC synthesis
*MOLECULAR structure
*DRUG bioavailability
*BIOLOGICAL assay
*LABORATORY rats
*MOLECULAR weights

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