Elucidating the multi-targeted anti-amyloid activity and enhanced islet amyloid polypeptide binding of β-wrapins

被引:13
|
作者
Orr, Asuka A. [1 ]
Shaykhalishahi, Hamed [2 ]
Mirecka, Ewa A. [2 ]
Jonnalagadda, Sai Vamshi R. [1 ]
Hoyer, Wolfgang [2 ,3 ]
Tamamis, Phanourios [1 ]
机构
[1] Texas A&M Univ, Artie McFerrin Dept Chem Engn, College Stn, TX 77843 USA
[2] Heinrich Heine Univ Dusseldorf, Inst Phys Biol, D-40204 Dusseldorf, Germany
[3] Res Ctr Julich, Inst Struct Biochem ICS 6, D-52425 Julich, Germany
基金
欧洲研究理事会;
关键词
Protein aggregation; Intrinsically disordered proteins; alpha-synuclein; Amyloid-beta; Amylin; Molecular dynamics; MOLECULAR-DYNAMICS SIMULATIONS; TYPE-2; DIABETES-MELLITUS; ALZHEIMERS-DISEASE; CROSS-TALK; PROTEIN; AGGREGATION; HAIRPIN; DESIGN; RISK; INHIBITION;
D O I
10.1016/j.compchemeng.2018.02.013
中图分类号
TP39 [计算机的应用];
学科分类号
081203 ; 0835 ;
摘要
beta-wrapins are engineered binding proteins stabilizing the beta-hairpin conformations of amyloidogenic proteins islet amyloid polypeptide (IAPP), amyloid-beta, and oz-synuclein, thus inhibiting their amyloid propensity. Here, we use computational and experimental methods to investigate the molecular recognition of IAPP by beta-wrapins. We show that the multi-targeted, IAPP, amyloid-beta and alpha-synuclein, binding properties of beta-wrapins originate mainly from optimized interactions between beta-wrapin residues and sets of residues in the three amyloidogenic proteins with similar physicochemical properties. Our results suggest that IAPP is a comparatively promiscuous beta-wrapin target, probably due to the low number of charged residues in the IAPP beta-hairpin motif. The sub-micromolar affinity of beta-wrapin HI18, specifically selected against IAPP, is achieved in part by salt-bridge formation between HI18 residue Glu10 and the IAPP Nterminal residue Lys1, both located in the flexible N-termini of the interacting proteins. Our findings provide insights towards developing novel protein-based single- or multi-targeted therapeutics. (C) 2018 The Authors. Published by Elsevier Ltd.
引用
收藏
页码:322 / 332
页数:11
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