Deciphering the Inhibitory Mechanism of Naphthoquinone-Dopamine on the Aggregation of Tau Core Fragments PHF6* and PHF6

Yu Zou; Bote Qi; Jingwang Tan; Lulu Guan; Qingwen Zhang; Yunxiang Sun; Fengjuan Huang

doi:10.1021/acschemneuro.3c00434

Deciphering the Inhibitory Mechanism of Naphthoquinone-Dopamine on the Aggregation of Tau Core Fragments PHF6* and PHF6

ACS Chem Neurosci. 2023 Sep 6;14(17):3265-3277. doi: 10.1021/acschemneuro.3c00434. Epub 2023 Aug 16.

Authors

Yu Zou¹, Bote Qi¹, Jingwang Tan¹, Lulu Guan¹, Qingwen Zhang², Yunxiang Sun³, Fengjuan Huang⁴

Affiliations

¹ Department of Sport and Exercise Science, College of Education, Zhejiang University, 866 Yuhangtang Road, Hangzhou 310058, Zhejiang, P. R. China.
² College of Physical Education, Shanghai University of Sport, 399 Changhai Road, Shanghai 200438, P. R. China.
³ Department of Physics, Ningbo University, 818 Fenghua Road, Ningbo 315211, Zhejiang, P. R. China.
⁴ Ningbo Institute of Innovation for Combined Medicine and Engineering (NIIME), Ningbo Medical Center Lihuili Hospital, Ningbo 315211, Zhejiang, P. R. China.

PMID: 37585669
DOI: 10.1021/acschemneuro.3c00434

Abstract

The formation of neurofibrillary tangles by abnormal aggregation of tau protein is considered to be an important pathological characteristic of tauopathies, including Alzheimer's disease and chronic traumatic encephalopathy. Two hexapeptides ²⁷⁵VQIINK²⁸⁰ and ³⁰⁶VQIVYK³¹¹ in the microtubule binding region, named PHF6* and PHF6, are known to be aggregation-prone and responsible for tau fibrillization. Previous experiments reported that naphthoquinone-dopamine (NQDA) could effectively inhibit the aggregation of PHF6* and PHF6 and disrupt the fibrillar aggregates into nontoxic species, displaying a dual effect on the amyloid aggregation. However, the underlying molecular mechanism remains mostly elusive. Herein, we performed all-atom molecular dynamics (MD) simulations for 114 μs in total to systematically investigate the impacts of NQDA on the oligomerization of PHF6* and PHF6. The conformational ensembles of PHF6* and PHF6 peptides generated by replica exchange MD simulations show that NQDA could effectively prevent the hydrogen bond formation, reduce the ability of peptides to self-assemble into long β-strand and large β-sheets, and induce peptides to form a loosely packed and coil-rich oligomer. The interaction analysis shows that the binding of NQDA to PHF6* is mainly through hydrophobic interactions with residue I277 and hydrogen bonding interactions with Q276; for the PHF6 peptides, NQDA displays a strong π-π stacking interaction with residue Y310, thus impeding the Y310-Y310 π-π stacking and I308-Y310 CH-π interactions. The DA group of NQDA displays a stronger cation-π interaction than the NQ group, while the NQ group exhibits a stronger π-π stacking interaction. MD simulations demonstrate that NQDA prevents the conformational conversion to β-sheet-rich aggregates and displays an inhibitory effect on the oligomerization dynamics of PHF6* and PHF6. Our results provide a complete picture of inhibitory mechanisms of NQDA on PHF6* and PHF6 oligomerization, which may pave the way for designing drug candidates for the treatment of tauopathies.

Keywords: PHF6; PHF6*; aggregation; inhibitory mechanism; molecular dynamics simulation; naphthoquinone−dopamine.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Alzheimer Disease* / metabolism
Dopamine
Humans
Molecular Dynamics Simulation
Naphthoquinones*
Peptides / therapeutic use
Repressor Proteins / metabolism
tau Proteins / metabolism

Substances

tau Proteins
urinary gonadotropin fragment
Dopamine
Naphthoquinones
Peptides
PHF6 protein, human
Repressor Proteins