Dimerization of Pyramidalized 3,4,8,9‐Tetramethyltetracyclo [4.4.0.0<sup>3,9</sup>.0<sup>4,8</sup>]dec‐1(6)‐ene to a Hydrocarbon Featuring Four Cyclohexane Rings in Boat Conformations

Rey-Carrizo, Matías; Barniol‐Xicota, Marta; Font-Bardı́a, Mercè; Vázquez, Santiago

doi:10.1002/ange.201403985

Cited by 6 publications

(1 citation statement)

References 44 publications

(13 reference statements)

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“…19,20 Overall, the V27A mutation is becoming more prevalent in circulating populations of influenza, 18 so there has been interest in designing drugs to target it. [21][22][23][24][25][26] Here we present X-ray crystal structures of the drug-resistant V27A mutant of M2 bound to a spiro-adamantyl amine inhibitor, using both M2 and M2 constructs for crystallization trials. Spiro-adamantyl amine was developed by molecular dynamics simulation-directed design and was able to inhibit the conductance of protons in both the V27A mutant and the WT channel in two electrode voltage clamp (TEVC) assays using Xenopus oocytes, with an IC 50 of 0.3 μM against the V27A channel and an IC 50 of 18.7 μM against the WT channel (compare to IC 50 = 15.7 μM for amantadine against the WT channel).…”

Section: Introductionmentioning

confidence: 99%

X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance

et al. 2020

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The V27A mutation confers adamantane resistance to the influenza A matrix 2 (M2) proton channel and is becoming more prevalent in circulating populations of influenza A virus. We have used X-ray crystallography to solve structures of a spiro-adamantyl amine inhibitor bound to M2(22-46) V27A and also to M2(21-61) V27A in the Inward closed conformation. The spiroadamantyl amine binding site is nearly identical for the two crystal structures. Compared to the M2 "wild type" (WT) with valine at position 27, we observe that the channel pore is wider at its N-terminus as a result of the V27A mutation and that this removes V27 side chain hydrophobic interactions that are important for binding of amantadine and rimantadine. The spiro-adamantyl amine inhibitor blocks proton conductance in both the WT and V27A mutant channels by shifting its binding site in the pore depending on which residue is present at position 27. Additionally, in the structure of the M2(21-61) V27A construct, the C-terminus of the channel is tightly packed relative to the M2(22-46) construct. We observe that residues Asp44, Arg45, and Phe48 face the center of the channel pore and would be well-positioned to interact with protons exiting the M2 channel after passing through the His37 gate. A 300 ns molecular dynamics (MD) simulation of *

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Section: Introductionmentioning

confidence: 99%

X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance

et al. 2020

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Fluor in einer C‐F‐Bindung als Schlüssel für die Käfigbildung

2018

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Fluorine in a C−F Bond as the Key to Cage Formation

2018

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Cage molecules have long been employed to trap reactive or transient species, as their rigid nature allows them to enforce situations that otherwise would not persist. In this Minireview, we discuss our use of rigid cage structures to investigate the close noncovalent interactions of fluorine with other functional groups and determine how mutual proximity affects both physical properties and reactivity. Unusual covalent interactions of fluorine are also explored: the cage can close to form the first solution-phase C-F-C fluoronium ion.

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Dimerization of Pyramidalized 3,4,8,9‐Tetramethyltetracyclo [4.4.0.0^3,9.0^4,8]dec‐1(6)‐ene to a Hydrocarbon Featuring Four Cyclohexane Rings in Boat Conformations

Cited by 6 publications

References 44 publications

X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance

X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance

Fluor in einer C‐F‐Bindung als Schlüssel für die Käfigbildung

Fluorine in a C−F Bond as the Key to Cage Formation

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Dimerization of Pyramidalized 3,4,8,9‐Tetramethyltetracyclo [4.4.0.03,9.04,8]dec‐1(6)‐ene to a Hydrocarbon Featuring Four Cyclohexane Rings in Boat Conformations

Cited by 6 publications

References 44 publications

X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance

X-ray Crystal Structures of the Influenza M2 Proton Channel Drug-Resistant V27A Mutant Bound to a Spiro-Adamantyl Amine Inhibitor Reveal the Mechanism of Adamantane Resistance

Fluor in einer C‐F‐Bindung als Schlüssel für die Käfigbildung

Fluorine in a C−F Bond as the Key to Cage Formation

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Product

Resources

About

Dimerization of Pyramidalized 3,4,8,9‐Tetramethyltetracyclo [4.4.0.0^3,9.0^4,8]dec‐1(6)‐ene to a Hydrocarbon Featuring Four Cyclohexane Rings in Boat Conformations