An Efficient Total Synthesis of Optically Active Tetrodotoxin from Levoglucosenone

Urabe, Daisuke; Nishikawa, Toshio; Isobe, Mitsuaki

doi:10.1002/asia.200600038

Cited by 57 publications

(29 citation statements)

References 49 publications

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“…We verified the purity of synthetic 4,9-anhydroTTX (4) via NMR (Ohyabu et al, 2003;Nishikawa et al, 2004;Urabe et al, 2006) and used it to treat HEK293T cells expressing a single VSSC subtype; however, we observed that the working solution containing 100 nM 4,9-anhydroTTX (4) caused inhibition of Na v 1.6 (Supporting Information Figure S4) when it was stored for half a year, implying that the production of TTX (1) and 4-epiTTX occurred, probably attributable to an equilibrium between TTX (1), 4-epiTTX and 4,9-anhydroTTX (4), which may not support Rosker's results. Indeed, 300 nM 4,9-anhydroTTX (4) preferentially inhibited Na v 1.6 over that of Na v 1.4 and Na v 1.5 (Supporting Information Table S1).…”

Section: Discussionmentioning

confidence: 99%

“…TTX (1) (Ohyabu et al, 2003;Nishikawa et al, 2004;Urabe et al, 2006), CHTX (2) (Adachi et al, 2014a), 8-deoxyTTX (3) (Satake et al, 2014), 4,9-anhydroTTX (4) (Ohyabu et al, 2003;Nishikawa et al, 2004;Urabe et al, 2006), 4,9-anhydroCHTX (5), 4,9-anhydro-8-deoxyTTX (6), 5-deoxyTTX (7) (Satake et al, 2014), 5,11-dideoxyTTX (8) (Nishikawa et al, 1999;Asai et al, 2001;Yotsu-Yamashita et al, 2013), 5,6,11-trideoxyTTX (9) (Adachi et al, 2014b), 4,9-anhydro-5-deoxyTTX (10) (Satake et al, 2014), 4,9-anhydro-5,11-dideoxyTTX (11) (Nishikawa et al, 1999;Asai et al, 2001;Yotsu-Yamashita et al, 2013) and 4,9-anhydro-5,6,11-trideoxyTTX (12) (Adachi et al, 2014b) were synthesized as reported in the literature (Figure 1 KOD-Plus, T4 ligase and the In-Fusion HD Cloning kit were purchased from Takara Bio, Inc. (Kusatsu, Shiga, Japan). PCR primers were purchased from Fasmac Co., Ltd. (Atsugi, Kanagawa, Japan).…”

Section: Methodsmentioning

confidence: 99%

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Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Na_v1.1 to Na_v1.7)

Tsukamoto

Chiba

Wakamori

et al. 2017

British J Pharmacology

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BACKGROUND AND PURPOSEThe development of subtype-selective ligands to inhibit voltage-sensitive sodium channels (VSSCs) has been attempted with the aim of developing therapeutic compounds. Tetrodotoxin (TTX) is a toxin from pufferfish that strongly inhibits VSSCs. Many TTX analogues have been identified from marine and terrestrial sources, although their specificity for particular VSSC subtypes has not been investigated. Herein, we describe the binding of 11 TTX analogues to human VSSC subtypes Na v 1.1-Na v 1.7. EXPERIMENTAL APPROACHEach VSSC subtype was transiently expressed in HEK293T cells. The inhibitory effects of TTX analogues on each subtype were assessed using whole-cell patch-clamp recordings.

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Na_v1.1 to Na_v1.7)

Tsukamoto

Chiba

Wakamori

et al. 2017

British J Pharmacology

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“…It is an anhydrosugar derivative, formed from the combined dehydration and depolymerization of cellulose at relatively low pyrolysis temperatures [34]. Owing to its unique structure, LGO is a promising chemical in modern organic synthesis, for the preparation of natural products [35][36][37], chiral auxiliaries [38,39], etc. Currently, the chemical synthesis of LGO is difficult and economically unfeasible [40,41].…”

Section: Introductionmentioning

confidence: 99%

Selective Production of Levoglucosenone from Catalytic Fast Pyrolysis of Biomass Mechanically Mixed with Solid Phosphoric Acid Catalysts

Zhang

Lü

et al. 2015

Bioenerg. Res.

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Solid phosphoric acid (SPA) catalysts with different carriers were prepared and used for catalytic fast pyrolysis of poplar wood to produce levoglucosenone (LGO), a valuable anhydrosugar derivative that can be used in various organic synthesis applications. Pyrolysis-gas chromatography/mass spectrometry (Py-GC/MS) experiments were performed to evaluate the catalytic capabilities of these catalysts under different reaction conditions. The results indicated that SPA catalyst prepared with the SBA-15 carrier exhibited the best catalytic capability for selectively producing LGO. Both the catalytic pyrolysis temperature and catalyst-to-biomass ratio affected the pyrolytic products greatly. The maximal LGO yield reached as high as 8.2 wt% from poplar wood, obtained at the pyrolysis temperature of 300°C and the catalyst-to-biomass ratio of 1. The by-products during the catalytic pyrolysis process were mainly acetic acid (AA) and furfural (FF). In addition, the SPA catalyst possessed better catalytic capability than the liquid phosphoric acid (H 3 PO 4 ) catalyst to produce LGO.

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“…23 To prepare cyclic carbamate 57, compound 56 was heated with K 2 CO 3 to generate the isocyanate, which to our surprise resulted in the clean removal of the N-trichloroacetyl group in 56. 24 Although the resulting pentahydroxy amine 60 was successfully transformed into guanidine 61 on condensation with Boc-protected 2-methylisothiourea, product 61 could not be transformed into tetrodotoxin (6).…”

Section: New Deprotection Conditions For the Removal Of The N-trichlomentioning

confidence: 95%

Multifunctionality of the N-Trichloroacetyl Group Developed in the Synthesis of Tetrodotoxin, a Puffer Fish Toxin

Nishikawa

Urabe²,

Adachi

et al. 2015

Synlett

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This account describes a serendipitous discovery and the development of unique reactions associated with trichloroacetamide during synthetic studies of tetrodotoxin in our laboratory. The reactions include site-selective hydroxylation using the neighboring-group participation of trichloroacetamide, guanidinylation from a trichloroacetamide, protecting-group transformation, and removal of the N-trichloroacetyl group. These studies indicate the importance of the total synthesis of densely functionalized natural products as a field for the development of new reactions. 1 Introduction 2 Improvement of the Conditions for the Overman Rearrangement to Introduce Trichloroacetamide 3 Site-Selective Hydroxylation Using the Neighboring-Group Participation of Trichloroacetamide 4 Guanidine Synthesis 5 Protecting-Group Transformation of the N-Trichloroacetyl Group 6 New Deprotection Conditions for the Removal of the N-Trichloroacetyl Group 7 Conclusion Key words protecting groups, tetrodotoxin, trichloroacetamide, neighboring-group effects, protecting-group transformations 2 Improvement of the Conditions for the Overman Rearrangement to Introduce TrichloroacetamideThe [3,3]-sigmatropic rearrangement of allylic trichloroacetimidate to allylic trichloroacetamide is known as the Overman rearrangement after his discovery in 1974. 7 We

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An Efficient Total Synthesis of Optically Active Tetrodotoxin from Levoglucosenone

Cited by 57 publications

References 49 publications

Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Na_v1.1 to Na_v1.7)

Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Na_v1.1 to Na_v1.7)

Selective Production of Levoglucosenone from Catalytic Fast Pyrolysis of Biomass Mechanically Mixed with Solid Phosphoric Acid Catalysts

Multifunctionality of the N-Trichloroacetyl Group Developed in the Synthesis of Tetrodotoxin, a Puffer Fish Toxin

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An Efficient Total Synthesis of Optically Active Tetrodotoxin from Levoglucosenone

Cited by 57 publications

References 49 publications

Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Nav1.1 to Nav1.7)

Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Nav1.1 to Nav1.7)

Selective Production of Levoglucosenone from Catalytic Fast Pyrolysis of Biomass Mechanically Mixed with Solid Phosphoric Acid Catalysts

Multifunctionality of the N-Trichloroacetyl Group Developed in the Synthesis of Tetrodotoxin, a Puffer Fish Toxin

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Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Na_v1.1 to Na_v1.7)

Differential binding of tetrodotoxin and its derivatives to voltage‐sensitive sodium channel subtypes (Na_v1.1 to Na_v1.7)