Chemical Probes for Blocking of Influenza A M2 Wild-type and S31N Channels
Christina Tzitzoglaki
1
,
Kelly McGuire
2
,
Panagiotis Lagarias
1
,
Athina Konstantinidi
1
,
Anja Hoffmann
3
,
Natalie A. Fokina
4
,
Chunlong Ma
5
,
Santiago Vazquez
6
,
Michaela Schmidtke
3
,
J. Wang
5
,
David D Busath
2
,
Publication type: Journal Article
Publication date: 2020-08-12
scimago Q1
wos Q2
SJR: 1.383
CiteScore: 7.1
Impact factor: 3.8
ISSN: 15548929, 15548937
PubMed ID:
32786258
Biochemistry
General Medicine
Molecular Medicine
Abstract
We report on using the synthetic aminoadamantane-CH2-aryl derivatives 1-6 as sensitive probes for blocking M2 S31N and influenza A virus (IAV) M2 wild-type (WT) channels as well as virus replication in cell culture. The binding kinetics measured using electrophysiology (EP) for M2 S31N channel are very dependent on the length between the adamantane moiety and the first ring of the aryl headgroup realized in 2 and 3 and the girth and length of the adamantane adduct realized in 4 and 5. Study of 1-6 shows that, according to molecular dynamics (MD) simulations and molecular mechanics Poisson-Boltzmann surface area (MM/PBSA) calculations, all bind in the M2 S31N channel with the adamantyl group positioned between V27 and G34 and the aryl group projecting out of the channel with the phenyl (or isoxazole in 6) embedded in the V27 cluster. In this outward binding configuration, an elongation of the ligand by only one methylene in rimantadine 2 or using diamantane or triamantane instead of adamantane in 4 and 5, respectively, causes incomplete entry and facilitates exit, abolishing effective block compared to the amantadine derivatives 1 and 6. In the active M2 S31N blockers 1 and 6, the phenyl and isoxazolyl head groups achieve a deeper binding position and high kon/low koff and high kon/high koff rate constants, compared to inactive 2-5, which have much lower kon and higher koff. Compounds 1-5 block the M2 WT channel by binding in the longer area from V27-H37, in the inward orientation, with high kon and low koff rate constants. Infection of cell cultures by influenza virus containing M2 WT or M2 S31N is inhibited by 1-5 or 1-4 and 6, respectively. While 1 and 6 block infection through the M2 block mechanism in the S31N variant, 2-4 may block M2 S31N virus replication in cell culture through the lysosomotropic effect, just as chloroquine is thought to inhibit SARS-CoV-2 infection.
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Total citations:
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Citations from 2025:
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GOST
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Tzitzoglaki C. et al. Chemical Probes for Blocking of Influenza A M2 Wild-type and S31N Channels // ACS Chemical Biology. 2020. Vol. 15. No. 9. pp. 2331-2337.
GOST all authors (up to 50)
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Tzitzoglaki C., McGuire K., Lagarias P., Konstantinidi A., Hoffmann A., Fokina N. A., Ma C., Papanastasiou I. P., Schreiner P. R., Vazquez S., Schmidtke M., Wang J., Busath D. D., Kolocouris A. Chemical Probes for Blocking of Influenza A M2 Wild-type and S31N Channels // ACS Chemical Biology. 2020. Vol. 15. No. 9. pp. 2331-2337.
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RIS
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TY - JOUR
DO - 10.1021/acschembio.0c00553
UR - https://doi.org/10.1021/acschembio.0c00553
TI - Chemical Probes for Blocking of Influenza A M2 Wild-type and S31N Channels
T2 - ACS Chemical Biology
AU - Tzitzoglaki, Christina
AU - McGuire, Kelly
AU - Lagarias, Panagiotis
AU - Konstantinidi, Athina
AU - Hoffmann, Anja
AU - Fokina, Natalie A.
AU - Ma, Chunlong
AU - Papanastasiou, Ioannis P
AU - Schreiner, Peter R.
AU - Vazquez, Santiago
AU - Schmidtke, Michaela
AU - Wang, J.
AU - Busath, David D
AU - Kolocouris, Antonios
PY - 2020
DA - 2020/08/12
PB - American Chemical Society (ACS)
SP - 2331-2337
IS - 9
VL - 15
PMID - 32786258
SN - 1554-8929
SN - 1554-8937
ER -
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BibTex (up to 50 authors)
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@article{2020_Tzitzoglaki,
author = {Christina Tzitzoglaki and Kelly McGuire and Panagiotis Lagarias and Athina Konstantinidi and Anja Hoffmann and Natalie A. Fokina and Chunlong Ma and Ioannis P Papanastasiou and Peter R. Schreiner and Santiago Vazquez and Michaela Schmidtke and J. Wang and David D Busath and Antonios Kolocouris},
title = {Chemical Probes for Blocking of Influenza A M2 Wild-type and S31N Channels},
journal = {ACS Chemical Biology},
year = {2020},
volume = {15},
publisher = {American Chemical Society (ACS)},
month = {aug},
url = {https://doi.org/10.1021/acschembio.0c00553},
number = {9},
pages = {2331--2337},
doi = {10.1021/acschembio.0c00553}
}
Cite this
MLA
Copy
Tzitzoglaki, Christina, et al. “Chemical Probes for Blocking of Influenza A M2 Wild-type and S31N Channels.” ACS Chemical Biology, vol. 15, no. 9, Aug. 2020, pp. 2331-2337. https://doi.org/10.1021/acschembio.0c00553.