Yin Jiang, Niu Chunying, Cherney Maia M, Zhang Jianmin, Huitema Carly, Eltis Lindsay D, Vederas John C, James Michael N G
Group in Protein Structure and Function, Department of Biochemistry, University of Alberta, Edmonton, AB, Canada T6G 2H7.
J Mol Biol. 2007 Aug 24;371(4):1060-74. doi: 10.1016/j.jmb.2007.06.001. Epub 2007 Jun 8.
The 3C-like main peptidase 3CL(pro) is a viral polyprotein processing enzyme essential for the viability of the Severe Acute Respiratory Syndrome coronavirus (SARS-CoV). While it is generalized that 3CL(pro) and the structurally related 3C(pro) viral peptidases cleave their substrates via a mechanism similar to that underlying the peptide hydrolysis by chymotrypsin-like serine proteinases (CLSPs), some of the hypothesized key intermediates have not been structurally characterized. Here, we present three crystal structures of SARS 3CL(pro) in complex with each of two members of a new class of peptide-based phthalhydrazide inhibitors. Both inhibitors form an unusual thiiranium ring with the nucleophilic sulfur atom of Cys145, trapping the enzyme's catalytic residues in configurations similar to the intermediate states proposed to exist during the hydrolysis of native substrates. Most significantly, our crystallographic data are consistent with a scenario in which a water molecule, possibly via indirect coordination from the carbonyl oxygen of Thr26, has initiated nucleophilic attack on the enzyme-bound inhibitor. Our data suggest that this structure resembles that of the proposed tetrahedral intermediate during the deacylation step of normal peptidyl cleavage.
3C样主要蛋白酶3CL(pro)是一种病毒多蛋白加工酶,对严重急性呼吸综合征冠状病毒(SARS-CoV)的存活至关重要。虽然普遍认为3CL(pro)和结构相关的3C(pro)病毒蛋白酶通过类似于胰凝乳蛋白酶样丝氨酸蛋白酶(CLSPs)肽水解的机制切割其底物,但一些假设的关键中间体尚未进行结构表征。在此,我们展示了SARS 3CL(pro)与一类新型基于肽的邻苯二甲酰肼抑制剂的两个成员分别形成复合物的三种晶体结构。两种抑制剂都与Cys145的亲核硫原子形成了一个不寻常的硫杂环丙烷环,将酶的催化残基捕获在类似于天然底物水解过程中所提出的中间状态的构型中。最重要的是,我们的晶体学数据与一种情况一致,即一个水分子可能通过Thr26的羰基氧的间接配位,对酶结合的抑制剂发起了亲核攻击。我们的数据表明,这种结构类似于正常肽基裂解去酰化步骤中所提出的四面体中间体的结构。
