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PDBsum entry 4lwi
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References listed in PDB file
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Key reference
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Title
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Discovery of potent n-(Isoxazol-5-Yl)amides as hsp90 inhibitors.
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Authors
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D.Chen,
A.Shen,
J.Li,
F.Shi,
W.Chen,
J.Ren,
H.Liu,
Y.Xu,
X.Wang,
X.Yang,
Y.Sun,
M.Yang,
J.He,
Y.Wang,
L.Zhang,
M.Huang,
M.Geng,
B.Xiong,
J.Shen.
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Ref.
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Eur J Med Chem, 2014,
87,
765-781.
[DOI no: ]
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PubMed id
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Abstract
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HSP90 is ubiquitously overexpressed in a broad spectrum of human cancers and has
been recognized as an attractive target for cancer treatment. Here, we described
the fragment screening, synthesis and structure-activity relationship studies of
small molecule inhibitors with 4,5-diarylisoxazole scaffold targeting HSP90.
Among them, the compound
N-(3-(2,4-dihydroxy-5-isopropylphenyl)-4-(4-((4-morpholinopiperidin-1-yl)methyl)phenyl)isoxazol-5-yl)cyclopropanecarboxamide
(108) showed high affinity for binding to HSP90 (FP binding assay, IC50 = 0.030
μM) and inhibited the proliferation of various human cancer cell lines with
averaging GI50 about 88 nM. Compound 108 exhibited its functional inhibition of
HSP90 by depleting key signaling pathways and concomitantly elevating of HSP70
and HSP27 in U-87MG cells. Further in vivo studies showed that compound 108
strongly suppressed the tumor growth of human glioblastoma xenograft model
U-87MG with T/C = 18.35% at 50 mg/kg q3w/2.5w. Moreover, compound 108 also
exhibited good pharmacokinetic properties. Together, our study implicates that
compound 108 is a promising candidate of HSP90 inhibitor and is currently
advanced to preclinical study.
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