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一個口服的选择性肽环氧酮的蛋白酶抑制剂的设计与合成中英文对照
3028
J. Med. Chem. 2009, 52, 3028–3038
Design and Synthesis of an Orally Bioavailable and Selective Peptide Epoxyketone Proteasome
Inhibitor (PR-047)
Proteasome inhibition has been validated as a therapeutic modality in the treatment of multiple myeloma
and Non-Hodgkin’s lymphoma. Car?lzomib, an epoxyketone currently undergoing clinical trials in malignant
diseases, is a highly selective inhibitor of the chymotrypsin-like (CT-L) activity of the proteasome. A chemistry
effort was initiated to discover orally bioavailable analogues of car?lzomib, which would have potential for
improved dosing ?exibility and patient convenience over intravenously administered agents. The lead
compound, 2-Me-5-thiazole-Ser(OMe)-Ser(OMe)-Phe-ketoepoxide (58) (PR-047), selectively inhibited CT-L
activity of both the constitutive proteasome ( 5) and immunoproteasome (LMP7) and demonstrated an
absolute bioavailability of up to 39% in rodents and dogs. It was well tolerated with repeated oral
administration at doses resulting in 80% proteasome inhibition in most tissues and elicited an antitumor
response equivalent to intravenously administered car?lzomib in multiple human tumor xenograft and mouse
syngeneic models. The favorable pharmacologic pro?le supports its further development for the treatment
of malignant diseases.
Introduction
The proteasome is a multicatalytic protease complex that is
responsible for the ubiquitin-dependent turnover of cellular
proteins.1-3 Proteasome substrates include misfolded or mis-
assembled proteins as well as short-lived components of
signaling cascades that regulate cell proliferation and survival
pathways. Inhibition of the proteasome leads to an accumulation
of substrate proteins and results in cell death.4 The proteasome
consists of a 20S proteolytic core and two 19S regulatory caps
that assemble with the core at either end to form a 26S
complex.5,6 Two distinct forms of the 26S proteasome, the
constitutive proteasome and the immunoprotea
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