Comparative Perturbation Effects Exerted by the Influenza A M2 WT Protein Inhibitors Amantadine and the Spiro[pyrrolidine-2,2′-adamantane] Variant AK13 to Membrane Bilayers Studied Using Biophysical Experiments and Molecular Dynamics Simulations

Konstantinidi, Athina; Naziris, Nikolaos; Kiriakidi, Sofia; Sartori, Barbara; Kolokouris, Dimitris; Amentisch, Heinz; Mali, Gregor; Ntountaniotis, Dimitrios; Demetzos, Costas; Mavromoustakos, Thomas; Kolocouris, Antonios

doi:10.1021/acs.jpcb.8b07071

Cited by 13 publications

(16 citation statements)

References 63 publications

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“…According to 31 P NMR spectra, the ternary system DMPC + M2TM (x=0.03) + Amt (x=0.05) or AK13 (x=0.05) produced σ Ι -σ II values almost identical to those of DMPC + M2TM (x=0.03) at the gel phase indicating that Amt and AK13 at concentration x=0.05 do not perturb further the phosphate groups region in the presence of M2TM. This is consistent with results from our previous paper 29 showing that at these concentrations the drugs did not change σ II −σ I value compared to pure DMPC. Only when the concentration of the drug was x=0.08 in the DMPC + Aamt system did the σ Ι -σ II value increase by 4 ppm compared to the pure DMPC.…”

Section: Dsc Resultssupporting

confidence: 93%

“…Only when the concentration of the drug was x=0.08 in the DMPC + Aamt system did the σ Ι -σ II value increase by 4 ppm compared to the pure DMPC. 29 As discussed previously in these two preparations the Aamt drug is inserted in the M2TM pore and the excess of molecules is distributed mainly in the bilayers. The observance of peaks with identical linewidths as those reported in our previous publication 29 where drugs perturbed DMPC bilayers not containing M2TM is an indication that Aamt drugs insert into and affect the lipid bilayer (see asterisks in Figure 6; Table 7).…”

Section: Dsc Resultsmentioning

confidence: 85%

“…19,[27][28] In a previous work, the effects of the M2 WT channel blockers Amt and AK13 on DMPC bilayers ( Figure 1) were compared using DSC, x-ray scattering, ssNMR spectroscopy, and MD simulations. 29 It was found that the two drugs localized in the polar head area of the DMPC bilayers, stabilized through hydrogen bonding with sn-2 carbonyls in their amine form, and phosphate oxygens in their ammonium form. Such localization of the drugs explain their strong perturbing effect evidenced by all biophysical methodologies applied, and may be involved in a step for their insertion into M2 protein pore and effecting its conformational plasticity.…”

Section: Introductionmentioning

confidence: 99%

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Influenza A M2 Spans the Membrane Bilayer, Perturbs its Organization and Differentiates the Effect of Amantadine and Spiro[pyrrolidine-2,2'-adamantane] AK13 on Lipids

Konstantinidi¹,

Naziris²,

Sartori³

et al. 2019

Preprint

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The investigation and observations made for the M2TM, excess aminoadamantane ligands in DMPC were made using the simpler version of biophysical methods including SDC, SAXS and WAXS, MD simulations and ssNMR. 1H, 31P ssNMR and MD simulations, showed that M2TM in apo form or drug-bound form span the membrane interacting strongly with lipid acyl chain tails and the phosphate groups of the polar head surface. The MD simulations showed that the drugs anchor through their ammonium group with the lipid phosphate and occasionally with M2TM asparagine-44 carboxylate groups. The 13C ssNMR experiments allow the inspection of excess drug molecules and the assessment of its impact on the lipid head-group region. At low peptide concentrations of influenza A M2TM tetramer in DPMC bilayer, two lipid domains were observed that likely correspond to the M2TM boundary lipids and the bulk-like lipids. At high peptide concentrations, one domain was identified which constitute essentially all of the lipids which behave as boundary. This effect is likely due, according to the MD simulations, to the preference of AK13 to locate in closer vicinity to M2TM compared to Amt as well as the stronger ionic interactions of Amt primary ammonium group with phosphate groups, compared with the secondary buried ammonium group in AK13.<br>

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Section: Dsc Resultssupporting

confidence: 93%

Section: Dsc Resultsmentioning

confidence: 85%

Section: Introductionmentioning

confidence: 99%

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Influenza A M2 Spans the Membrane Bilayer, Perturbs its Organization and Differentiates the Effect of Amantadine and Spiro[pyrrolidine-2,2'-adamantane] AK13 on Lipids

Konstantinidi¹,

Naziris²,

Sartori³

et al. 2019

Preprint

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“…Levofloxacin [236][237][238], Clarithromycin [236], Isoniazid N -acylated derivatives [239], Rifampicin [234,240], Mangostin [241], Trimethoprim [242], Negamycin [243] Potential antibiotic Kanamycin A [133], nTZDpa and its derivatives [244], Cholic acid derived amphiphiles [245], γ-terpineol [246], Bithionol [247] Antimicrobial compound Chlorhexidine [248][249][250], Triclosan [251], Octenidine [250] Antiparasitic Praziquantel [252] Antiviral drugs Darunavir [253], Amantadine [254][255][256], Spiro[pyrrolidine-2,2 -adamantane] [254,255], 20,30-dideoxyadenosine (Didanosine) [242], Saffron [257] Antifungal drug Itraconazole, [184,186,187,258], Nystatin [259], Amphotericin B [260] Rheumatoid arthritis Lapatinib [213] Nonsteroidal antiinflammatory drugs, inhibitor of cyclooxygenase-1 and -2…”

Section: Application and Target Drugs And Pharmaceuticsmentioning

confidence: 99%

Mechanistic Understanding from Molecular Dynamics in Pharmaceutical Research 2: Lipid Membrane in Drug Design

2021

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We review the use of molecular dynamics (MD) simulation as a drug design tool in the context of the role that the lipid membrane can play in drug action, i.e., the interaction between candidate drug molecules and lipid membranes. In the standard “lock and key” paradigm, only the interaction between the drug and a specific active site of a specific protein is considered; the environment in which the drug acts is, from a biophysical perspective, far more complex than this. The possible mechanisms though which a drug can be designed to tinker with physiological processes are significantly broader than merely fitting to a single active site of a single protein. In this paper, we focus on the role of the lipid membrane, arguably the most important element outside the proteins themselves, as a case study. We discuss work that has been carried out, using MD simulation, concerning the transfection of drugs through membranes that act as biological barriers in the path of the drugs, the behavior of drug molecules within membranes, how their collective behavior can affect the structure and properties of the membrane and, finally, the role lipid membranes, to which the vast majority of drug target proteins are associated, can play in mediating the interaction between drug and target protein. This review paper is the second in a two-part series covering MD simulation as a tool in pharmaceutical research; both are designed as pedagogical review papers aimed at both pharmaceutical scientists interested in exploring how the tool of MD simulation can be applied to their research and computational scientists interested in exploring the possibility of a pharmaceutical context for their research.

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“…In the case of DPPC, the main transition curve was influenced the least by the drug molecule, potentiating the absence of the drug molecule from the membrane interior or its distribution in a more homogeneous manner. However, in the case of the chimeric systems, the formation of a shoulder on the main transition, along with all other alterations, is an indication of the creation of drug-related domains [31]. After exposure to an acidic environment, the drug-loaded chimeric bilayer transitions exhibited no shoulders and the transition enthalpy ∆H m decreased, particularly for DPPC:PDMAEMA-b-PLMA 1 (Figure 3B).…”

Section: Thermotropic Behavior Of Chimeric Bilayers With Tram-34mentioning

confidence: 98%

Chimeric Stimuli-Responsive Liposomes as Nanocarriers for the Delivery of the Anti-Glioma Agent TRAM-34

Naziris

Pippa

Sereti

et al. 2021

IJMS

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Nanocarriers are delivery platforms of drugs, peptides, nucleic acids and other therapeutic molecules that are indicated for severe human diseases. Gliomas are the most frequent type of brain tumor, with glioblastoma being the most common and malignant type. The current state of glioma treatment requires innovative approaches that will lead to efficient and safe therapies. Advanced nanosystems and stimuli-responsive materials are available and well-studied technologies that may contribute to this effort. The present study deals with the development of functional chimeric nanocarriers composed of a phospholipid and a diblock copolymer, for the incorporation, delivery and pH-responsive release of the antiglioma agent TRAM-34 inside glioblastoma cells. Nanocarrier analysis included light scattering, protein incubation and electron microscopy, and fluorescence anisotropy and thermal analysis techniques were also applied. Biological assays were carried out in order to evaluate the nanocarrier nanotoxicity in vitro and in vivo, as well as to evaluate antiglioma activity. The nanosystems were able to successfully manifest functional properties under pH conditions, and their biocompatibility and cellular internalization were also evident. The chimeric nanoplatforms presented herein have shown promise for biomedical applications so far and should be further studied in terms of their ability to deliver TRAM-34 and other therapeutic molecules to glioblastoma cells.

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Comparative Perturbation Effects Exerted by the Influenza A M2 WT Protein Inhibitors Amantadine and the Spiro[pyrrolidine-2,2′-adamantane] Variant AK13 to Membrane Bilayers Studied Using Biophysical Experiments and Molecular Dynamics Simulations

Cited by 13 publications

References 63 publications

Influenza A M2 Spans the Membrane Bilayer, Perturbs its Organization and Differentiates the Effect of Amantadine and Spiro[pyrrolidine-2,2'-adamantane] AK13 on Lipids

Influenza A M2 Spans the Membrane Bilayer, Perturbs its Organization and Differentiates the Effect of Amantadine and Spiro[pyrrolidine-2,2'-adamantane] AK13 on Lipids

Mechanistic Understanding from Molecular Dynamics in Pharmaceutical Research 2: Lipid Membrane in Drug Design

Chimeric Stimuli-Responsive Liposomes as Nanocarriers for the Delivery of the Anti-Glioma Agent TRAM-34

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