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

Thomaston, Jessica L.; Konstantinidi, Athina; Liu, Lijun; Lambrinidis, George; Tan, Jian; Caffrey, Martin; Wang, Junyang; DeGrado, William F.; Kolocouris, Antonios

doi:10.1021/acs.biochem.9b00971

Cited by 32 publications

(62 citation statements)

References 90 publications

(172 reference statements)

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“…-S31N (19-49) in complex with (4) (PDB: 2LY0; ). (C) X-ray crystal structure of M2-V27A (22-46) in complex with spiro-adamantyl amine (9) (PDB: 6NV1; Thomaston et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

“…Among these, Ser31Asn is the prevalent mutation in more than 95% of adamantane-resistant strains (Dong et al, 2015;Nelson et al, 2009), although a recent study reported a potential rise in the frequency of virus strains containing the Val27Ala and Ser31Asn double mutations (Durrant et al, 2014). A recent crystallography study reported that elimination of hydrophobic contacts that are essential for adamantane drug binding is the underlying cause behind adamantane resistance to Val27Ala mutant (Thomaston et al, 2020). In contrast to the Val27Ala single mutation that results in complete resistance to amantadine, M2 sequences containing Ser31Asn can still be inhibited by amantadine in vitro, albeit with approximately 200-fold higher concentrations in TEVC experiments and plaque reduction assays (PRAs) and substantially higher than what is therapeutically-achievable (Wang et al, 2013a).…”

Section: The Rise Of Drug-resistant M2mentioning

confidence: 99%

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Put a cork in it: Plugging the M2 viral ion channel to sink influenza

et al. 2020

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Highlights• The M2 protein of influenza A is a proton-gated proton channel that is required for viral replication • Current influenza strains are resistant to licensed M2 antivirals, so new therapies that target M2 are needed • The structure and function of M2, rise of drug resistance mutations, and current antiviral strategies are discussed AbstractThe ongoing threat of seasonal and pandemic influenza to human health requires antivirals that can effectively supplement existing vaccination strategies. The M2 protein of influenza A virus (IAV) is a proton-gated, proton-selective ion channel that is required for virus replication and is an established antiviral target. While licensed adamantane-based M2 antivirals have been historically used, M2 mutations that confer major adamantane resistance are now so prevalent in circulating virus strains that these drugs are no longer recommended. Here we review the current understanding of IAV M2 structure and function, mechanisms of inhibition, the rise of drug resistance mutations, and ongoing efforts to develop new antivirals that target resistant forms of M2.

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“…-S31N (19-49) in complex with (4) (PDB: 2LY0; ). (C) X-ray crystal structure of M2-V27A (22-46) in complex with spiro-adamantyl amine (9) (PDB: 6NV1; Thomaston et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

Section: The Rise Of Drug-resistant M2mentioning

confidence: 99%

Put a cork in it: Plugging the M2 viral ion channel to sink influenza

et al. 2020

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“…Upon drug-resistance V27A mutation, this interaction is lost. Recentlydeveloped spiro-amantadyl amine effectively binds to A27 of the pore (Figure 2B) [136]. Recently, new amantadine derivatives effective against double mutants M2-S31N/L26I and M2-S31N/V27A viral strains have been developed by Musharrafieh et al [91].…”

Section: M2 Ion Channel Blockers (Amantadine/rimantadine)mentioning

confidence: 99%

Anti-Influenza Drug Discovery and Development: Targeting the Virus and Its Host by All Possible Means

Terrier

Slama‐Schwok

2021

Antiviral Drug Discovery and Development

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Influenza infections remain a major and recurrent source of public health concern. Together with vaccines, antiviral drugs play a key role in the prevention and treatment of influenza virus infection and disease. Today, the number of antiviral molecules approved for the treatment of influenza is relatively limited and their use is threatened by the emergence of viral strains with resistance mutations. There is therefore a real need to expand the prophylactic and therapeutic arsenal. This chapter summarizes the state of the art in drug discovery and development for the treatment of influenza virus infections, with a focus on both virus-targeting and host-cell-targeting strategies. Novel antiviral strategies targeting other viral proteins or targeting the host cell, some of which are based on drug repurposing, may be used in combination to strengthen our therapeutic arsenal against this major pathogen.

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“…3 Several groups published high resolution structures and data from mutation experiments showing that M2 protein channel is blocked by 1 and 2 via a M2 pore-binding mechanism. [4][5][6][7][8][9] Additionally, amantadine variants, especially those with hydrophobic adducts, can act as lysosomotropic drugs, 10 which accumulate in intracellular vesicles through membrane permeation by the electroneutral form and increase intravesicular pH, causing endosome and/or trans-Golgi network neutralization and inhibition of viral reproduction. 11 Noteworthy, SARS-CoV-2 is inhibited by chloroquine, probably because it acts as a lysosomotropic drug.…”

Section: Introductionmentioning

confidence: 99%

Amantadine Variants Activity Against Multiple Influenza A Viruses

Stampolaki

Tzitzoglaki

Liolios

et al. 2021

Preprint

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Future pandemic influenza necessitates the development of new drugs against the current circulating, amantadine and rimantadine drugs resistant, influenza A M2 S31N viruses. The possibility of an antigenic shift to M2 S31 necessitates ranking the biological activities of amantadine variants. Several amantadine variants have been tested by different laboratories, but various M2 wild type influenza A strains have been used with different sensitivity against amantadine and the unambiguous comparison between potencies is not straightforward. Here, we compared the anti-influenza activities of 57 synthetic amantadine variants against influenza A WSN/33 viruses with amantadine-sensitive M2 WT, with a range of over three digits providing a reference set of potencies for structure-activity relationships, and amantadine-resistant M2 S31N proteins (and observed no potent compounds). 17 compounds were selected and tested against M2 L26F, V27A, A30T, G34E viruses. We tested few reference compounds using electrophysiology and explored point mutations which both showed that M2 is the target of potent antiviral potency against the M2 WT, L26F, V27A viruses. Major findings are: (a) Several amantadine variants from Kolocouris group block only M2 WT and M2 L26F-mediated proton current and the corresponding viruses replication. (b) A compound from Vazquez’s group is a triple blocker of M2 WT, L26F, V27A channels and viruses replication. (c) A compound from Vazquez’s group blocks only M2 L26 channel and virus replication. (d) Several compounds from Kolocouris group have potent activity against several influenza A M2 WT and three M2 S31N viruses, eg. the pandemic A/H1N1/California/07/2009 (H1N1pdm09) or A/H1N1/PuertoRico/08/1934 without blocking M2 S31N. The compounds and their cocktails while not to be more toxic than amantadine might be useful for re-purposing of amantadine class of drugs in the case (i) of the prevalence of M2 L26F and or M2 V27A strains (ii) of an antigenic shift of the virus to M2 WT and (iii) because they inhibited a broad panel of M2 WT and M2 S31N viruses including the H1N1pdm09). (d) We showed that the mechanism of antiviral activity against A/California/07/2009 or A/PR/08/1934 and possibly also M2 WT viruses compared to WSN/33 viruses is not due to inhibition of an early stage of virus infection or a late stage of M2 channel function during endocytosis or inhibition of HA binding to host cells or a different pH for HA fusion or a lysosomotropic effect.

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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

Cited by 32 publications

References 90 publications

Put a cork in it: Plugging the M2 viral ion channel to sink influenza

Put a cork in it: Plugging the M2 viral ion channel to sink influenza

Anti-Influenza Drug Discovery and Development: Targeting the Virus and Its Host by All Possible Means

Amantadine Variants Activity Against Multiple Influenza A Viruses

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