Interfacial interaction and lateral association of cross-seeding assemblies between hIAPP and rIAPP oligomers

Literature Information

Publication Date 2015-02-16
DOI 10.1039/C4CP05658B
Impact Factor 3.676
Authors

Mingzhen Zhang, Rundong Hu, Hong Chen, Yung Chang, Xiong Gong, Fufeng Liu, Jie Zheng


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Abstract

Cross-sequence interactions between different amyloid peptides are important not only for the fundamental understanding of amyloid aggregation and polymorphism mechanisms, but also for probing a potential molecular link between different amyloid diseases. Here, we computationally modeled and simulated a series of hybrid hIAPP (human islet amyloid polypeptide)–rIAPP (rat islet amyloid polypeptide) assemblies and probed their structural stability, lateral association, and interfacial interactions using combined peptide-packing search, molecular dynamics (MD) simulations, and the Monte Carlo sampling method. We then identified a number of stable and highly populated hIAPP–rIAPP assemblies at the lowest energy states, in which hIAPP and rIAPP oligomers were stacked laterally on top of each other to form supramolecular β-sheet double layers in an antiparallel fashion. These hIAPP–rIAPP assemblies adopted different interfaces formed by C-terminal β-sheets of hIAPP and rIAPP oligomers (hCCr), N-terminal β-sheets of hIAPP and rIAPP oligomers (hNNr), and alternative N-terminal/C-terminal β-sheets of hIAPP and rIAPP oligomers (hNCr and hCNr). Different interfaces along with distinct interfacial residue packings provided different driving interfacial forces to laterally associate two β-sheet layers of hIAPP and rIAPP together for forming polymorphic hIAPP–rIAPP assemblies. Such lateral association between hIAPP and rIAPP not only explained the experimentally observed cross-seeding behavior of hIAPP and rIAPP, but also demonstrated the co-existence of polymorphic amyloid cross-seeding species. A cross-seeding mechanism for hIAPP and rIAPP aggregation was proposed on the basis of our simulated models and experimental data. This work provides a better understanding of cross-seeding aggregation and polymorphism mechanisms of amyloidogenesis.

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Physical Chemistry Chemical Physics

Physical Chemistry Chemical Physics
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