Proteasome Inhibition in Multiple Myeloma: Head-to-Head Comparison of Currently Available Proteasome Inhibitors

被引:90
作者
Besse, Andrej [1 ]
Besse, Lenka [1 ]
Kraus, Marianne [1 ]
Mendez-Lopez, Max [1 ]
Bader, Juergen [1 ]
Xin, Bo-Tao [2 ,3 ]
de Bruin, Gerjan [2 ,3 ]
Maurits, Elmer [2 ,3 ]
Overkleeft, Herman S. [2 ,3 ]
Driessen, Christoph [1 ]
机构
[1] Cantonal Hosp St gallen, Dept Oncol & Hematol, Expt Oncol & Hematol, Rorschacher Str 95, CH-9007 St Gallen, Switzerland
[2] Leiden Inst Chem, Gorlaeus Labs, NL-2333 CC Leiden, Netherlands
[3] Netherlands Prote Ctr, NL-2333 CC Leiden, Netherlands
基金
瑞士国家科学基金会;
关键词
ACTIVE-SITES; CARFILZOMIB; BORTEZOMIB; CELLS; PROTEOLYSIS; RESISTANCE; EFFICACY; APPROVAL; OVERCOME;
D O I
10.1016/j.chembiol.2018.11.007
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Proteasome inhibitors (PIs) are a backbone of multiple myeloma (MM) therapy. The proteasome harbors six proteolytically active subunits (beta 1, beta 2, beta 5), while b5 was identified as rate-limiting and is a primary target of clinically available PIs. The most effective pattern of subunit inhibition provided by these PIs for cytotoxic activity in MM is unknown. A head-to-head comparison of clinically available PIs shows that in the clinically relevant setting only the co-inhibition of beta 1 or beta 2 with beta 5 activity achieves meaningful functional proteasome inhibition and cytotoxicity, while the selective beta 2/beta 5 inhibition of both constitutive and immunoproteasome is the most cytotoxic. In the long-term setting, selective inhibition of beta 5 subunit is sufficient to induce cytotoxicity in PI-sensitive, but not in PI-resistant MM, and the beta 5/beta 2 co-inhibition is the most cytotoxic in PI-resistant MM. These results give a rational basis for selecting individual PIs for the treatment of MM.
引用
收藏
页码:340 / +
页数:15
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