Literature DB >> 25588114

Synthesis, stereochemical analysis, and derivatization of myricanol provide new probes that promote autophagic tau clearance.

Mackenzie D Martin1, Laurent Calcul2, Courtney Smith2, Umesh K Jinwal1, Sarah N Fontaine1, April Darling1, Kent Seeley2, Lukasz Wojtas2, Malathi Narayan1, Jason E Gestwicki3, Garry R Smith4, Allen B Reitz4, Bill J Baker2, Chad A Dickey1,2,5.   

Abstract

We previously discovered that one specific scalemic preparation of myricanol (1), a constituent of Myrica cerifera (bayberry/southern wax myrtle) root bark, could lower the levels of the microtubule-associated protein tau (MAPT). The significance is that tau accumulates in a number of neurodegenerative diseases, the most common being Alzheimer's disease (AD). Herein, a new synthetic route to prepare myricanol using a suitable boronic acid pinacol ester intermediate is reported. An X-ray crystal structure of the isolated myricanol (1) was obtained and showed a co-crystal consisting of (+)-aR,11S-myricanol (2) and (-)-aS,11R-myricanol (3) coformers. Surprisingly, 3, obtained from chiral separation from 1, reduced tau levels in both cultured cells and ex vivo brain slices from a mouse model of tauopathy at reasonable mid-to-low micromolar potency, whereas 2 did not. SILAC proteomics and cell assays revealed that 3 promoted tau degradation through an autophagic mechanism, which was in contrast to that of other tau-lowering compounds previously identified by our group. During the course of structure-activity relationship (SAR) development, we prepared compound 13 by acid-catalyzed dehydration of 1. 13 had undergone an unexpected structural rearrangement through the isomyricanol substitution pattern (e.g., 16), as verified by X-ray structural analysis. Compound 13 displayed robust tau-lowering activity, and, importantly, its enantiomers reduced tau levels similarly. Therefore, the semisynthetic analogue 13 provides a foundation for further development as a tau-lowering agent without its SAR being based on chirality.

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Year:  2015        PMID: 25588114      PMCID: PMC4971885          DOI: 10.1021/cb501013w

Source DB:  PubMed          Journal:  ACS Chem Biol        ISSN: 1554-8929            Impact factor:   5.100


  42 in total

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Journal:  J Neurosci       Date:  2005-11-16       Impact factor: 6.167

2.  New substructure filters for removal of pan assay interference compounds (PAINS) from screening libraries and for their exclusion in bioassays.

Authors:  Jonathan B Baell; Georgina A Holloway
Journal:  J Med Chem       Date:  2010-04-08       Impact factor: 7.446

3.  SILAC-based proteomic analysis to investigate the impact of amyloid precursor protein expression in neuronal-like B103 cells.

Authors:  Dale Chaput; Lisa Hornbeck Kirouac; Harris Bell-Temin; Stanley M Stevens; Jaya Padmanabhan
Journal:  Electrophoresis       Date:  2012-12       Impact factor: 3.535

Review 4.  HSP90 inhibitors: current development and potential in cancer therapy.

Authors:  Katerina Sidera; Evangelia Patsavoudi
Journal:  Recent Pat Anticancer Drug Discov       Date:  2014-01       Impact factor: 4.169

5.  Methods in mammalian autophagy research.

Authors:  Noboru Mizushima; Tamotsu Yoshimori; Beth Levine
Journal:  Cell       Date:  2010-02-05       Impact factor: 41.582

6.  A caspase cleaved form of tau is preferentially degraded through the autophagy pathway.

Authors:  Philip J Dolan; Gail V W Johnson
Journal:  J Biol Chem       Date:  2010-05-13       Impact factor: 5.157

7.  Tau accumulation activates the unfolded protein response by impairing endoplasmic reticulum-associated degradation.

Authors:  Jose F Abisambra; Umesh K Jinwal; Laura J Blair; John C O'Leary; Qingyou Li; Sarah Brady; Li Wang; Chantal E Guidi; Bo Zhang; Bryce A Nordhues; Matthew Cockman; Amirthaa Suntharalingham; Pengfei Li; Ying Jin; Christopher A Atkins; Chad A Dickey
Journal:  J Neurosci       Date:  2013-05-29       Impact factor: 6.167

8.  Allosteric heat shock protein 70 inhibitors rapidly rescue synaptic plasticity deficits by reducing aberrant tau.

Authors:  Jose Abisambra; Umesh K Jinwal; Yoshinari Miyata; Justin Rogers; Laura Blair; Xiaokai Li; Sandlin P Seguin; Li Wang; Ying Jin; Justin Bacon; Sarah Brady; Matthew Cockman; Chantal Guidi; Juan Zhang; John Koren; Zapporah T Young; Christopher A Atkins; Bo Zhang; Lisa Y Lawson; Edwin J Weeber; Jeffrey L Brodsky; Jason E Gestwicki; Chad A Dickey
Journal:  Biol Psychiatry       Date:  2013-04-19       Impact factor: 13.382

Review 9.  Tanespimycin: the opportunities and challenges of targeting heat shock protein 90.

Authors:  Charles Erlichman
Journal:  Expert Opin Investig Drugs       Date:  2009-06       Impact factor: 6.206

Review 10.  Fyn kinase inhibition as a novel therapy for Alzheimer's disease.

Authors:  Haakon B Nygaard; Christopher H van Dyck; Stephen M Strittmatter
Journal:  Alzheimers Res Ther       Date:  2014-02-05       Impact factor: 6.982

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  3 in total

1.  Inhibition of Both Hsp70 Activity and Tau Aggregation in Vitro Best Predicts Tau Lowering Activity of Small Molecules.

Authors:  Mackenzie D Martin; Jeremy D Baker; Amirthaa Suntharalingam; Bryce A Nordhues; Lindsey B Shelton; Dali Zheng; Jonathan J Sabbagh; Timothy A J Haystead; Jason E Gestwicki; Chad A Dickey
Journal:  ACS Chem Biol       Date:  2016-05-26       Impact factor: 5.100

2.  Myricanol rescues dexamethasone-induced muscle dysfunction via a sirtuin 1-dependent mechanism.

Authors:  Shengnan Shen; Qiwen Liao; Jingxin Liu; Ruile Pan; Simon Ming-Yuen Lee; Ligen Lin
Journal:  J Cachexia Sarcopenia Muscle       Date:  2019-02-21       Impact factor: 12.910

3.  Tau pathology reduction with SM07883, a novel, potent, and selective oral DYRK1A inhibitor: A potential therapeutic for Alzheimer's disease.

Authors:  Benoît Melchior; Gopi Kumar Mittapalli; Carolyn Lai; Karen Duong-Polk; Joshua Stewart; Bora Güner; Brian Hofilena; Amanda Tjitro; Scott D Anderson; David S Herman; Luis Dellamary; Christopher J Swearingen; K C Sunil; Yusuf Yazici
Journal:  Aging Cell       Date:  2019-07-03       Impact factor: 9.304

  3 in total

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