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The experimental identification of NgBeO molecules, followed by the recent theoretical exploration of super-strong NgBO+ (Ng = He-Rn) ions motivated us to investigate the stability of iso-electronic NgBNH+ (Ng = He-Rn) ions using various ab initio-based quantum chemical methods. The hydrogen-like chemical behavior of gold in small clusters and molecules also inspired us to study the nature of the bonding interactions in NgBNAu+ ions compared to that in NgBNH+ ions. The calculated Ng-B bond lengths in the predicted ions have been found to be much lower than the corresponding covalent limits, indicating a covalent Ng-B interaction in both the NgBNH+ and NgBNAu+ ions. In addition, the Ng-B bond dissociation energies are found to be in the range of 136.7-422.8 kJ mol-1 for NgBNH+ and 77.4-319.1 kJ mol-1 for NgBNAu+, implying the stable nature of the predicted ions. Interestingly, the Ng-B bond length (except for Ne) is the lowest reported to date together with the highest He-B and Ne-B binding energies considering all the neutral and cationic complexes containing Ng-B bonding motifs. Moreover, the natural bonding orbital (NBO) and electron density-based atoms-in-molecule (AIM) analysis reveal the covalent nature of the Ng-B bond in the predicted ions. Furthermore, the energy decomposition analysis together with the natural bond orbital in the chemical valence (EDA-NOCV) studies indicate that the orbital interaction energy is the main contributor to the total attraction energy in the Ng-B bonds. All the calculated results indicate the hydrogen-like chemical behavior of gold in the predicted NgBNM+ ions, showing further evidence of the concept of "gold-hydrogen analogy". Also, for comparison, the corresponding Cu and Ag analogs are investigated. All the computed results together with the experimental identification of the NgMX (Ng = Ar-Xe; M = Cu, Ag, Au; X = F, Cl), ArOH+, and NgBeO (Ng = Ar-Xe) systems clearly indicate that it may be possible to prepare and characterize the predicted NgBNM+ ions experimentally using suitable technique(s).
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Deep eutectic solvents (DES) are considered a novel class of environmentally benign molecular solvents that are considered as potential solvents for nuclear fuel reprocessing, material recycling, and many other technological applications in both research and industry. However, there is a complete dearth of understanding pertaining to the behavior of metal ions in DES. Herein, we have investigated the speciation, complexation behavior, photochemistry, and redox properties and tried to obtain insight into the chemical aspects of the europium ion in DES (synthesized from heptyltriphenylphosphonium bromide and decanoic acid). The same has been probed using time-resolved photoluminescence (TRPL), cyclic voltammetry (CV), synchrotron-based extended X-ray absorption fine structure (EXAFS) spectroscopy, and density functional theory (DFT) calculations. TRPL indicated the stabilization of europium in the +3 oxidation state, favoring the potential of the Eu(III)-DES complex to emit red light under near UV excitation and the existence of inefficient energy transfer between DES and Eu3+. EXAFS analysis revealed the presence of Eu-O and Eu-Br, which represent the local surroundings of Eu3+ in the Eu(III)-DES complex. TRPL measurement has also suggested two distinct local environments of europium ions in the complex. DFT calculations supported the EXAFS findings, confirming that the Eu(III)-DES structure involves not only the oxygen atom of decanoic acid but also the oxygen atoms from the nitrate ions, contributing to the local coordination of Eu(III). Electrochemical studies demonstrated that the redox reaction of Eu(III)/Eu(II) in DES displays quasi-reversible behavior. The reaction rate was observed to increase with higher temperatures. The findings of this study can contribute to the understanding of the fundamental properties and potential applications of this luminescent and electrochemically active complex and pave the way for further studies and the development of novel materials with enhanced luminescent and electrochemical properties.
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IMPORTANCE: The role of the upper respiratory tract (URT) microbiome in predicting lung health has been documented in several studies. The dysbiosis in COVID patients has been associated with disease outcomes by modulating the host immune system. However, although it has been known that different SARS-CoV-2 variants manifest distinct transmissibility and mortality rates in human populations, their effect on the composition and diversity of the URT microbiome has not been studied to date. Unlike the older variant (Delta), the newer variant (Omicron) have become more transmissible with lesser mortality and the symptoms have also changed significantly. Hence, in the present study, we have investigated the change in the URT microbiome associated with Delta and Omicron variants and identified variant-specific signatures that will be useful in the assessment of lung health and can be utilized for nasal probiotic therapy in the future.
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COVID-19 , Microbiota , Humanos , SARS-CoV-2/genética , Microbiota/genética , NarizRESUMO
Novel amide ligands in the ionic liquid (1-hexyl-3-methylimidazolium bis(trifluoromethylsulfonyl)imide) were utilized for the liquid-liquid biphasic mass transfer of Eu3+ ions from aqueous acidic waste solution. The cation exchange mechanism was found to be operative with the formation of [Eu(NO3)2L3]+ species (L = 4-chloro-N-(1-methyl-1H-pyrazol-3-yl)picolinamide). However, the presence of an inner-sphere water molecule was revealed by density functional theory (DFT) calculations. The viscosity-induced slower kinetics was evidenced during mass transfer, which was improved by increasing temperature. The process was exothermic in nature. The improvement in the kinetics of extractive mass transfer at higher temperatures is evinced by a reduction in the distribution ratio value. The spontaneity of the reaction was evidenced through the negative Gibbs free energy value, whereas the process enhances the entropy of the system, probably by releasing water molecules at least partially during complexation. The structures of bare ligands and complexes have been optimized by using DFT calculations. A high value of complexation energy, solvation energy, and associated enthalpy and free energy change reveal the efficacy in binding Eu with O and N donor atoms. In addition, natural population analysis, atoms-in-molecules analysis, and energy decomposition analysis have been employed to explore the nature of bonding existing in Eu-O and Eu-N bonds.
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Recent experimental detection of noble gas (Ng) inserted fluorocarbenes, viz., FKrCF and FXeCF, which were theoretically predicted by our group earlier and very recent experimental evidences on gold-halogen analogy motivated us to explore the possibility of the existence of noble gas inserted noble metal fluorocarbene, FNgCM (Ng = Kr, Xe, and Rn; M = Cu, Ag, and Au) molecules. Ab initio quantum chemical calculations have been performed to investigate structure, stability, vibrational frequency, charge distribution and bonding analysis of FNgCM molecules by employing DFT, MP2, and CCSD(T) methods. For the purpose of comparison FNgCH molecules have also been studied. One of the important outcomes of the study is that the predicted FNgCH, FNgCCu and FNgCAg molecules are more stable in their triplet electronic states, whereas the FNgCAu molecules are found to be more stable in their singlet potential energy surface, similar to the recently observed FNgCF (Ng = Kr and Xe) molecules, although the singlet state is the lowest energy state for all the precursor carbene molecules. The gold atom behaves as a better electron donor due to the pronounced relativistic effect as compared to hydrogen, copper and silver atoms, resulting in stabilization of the singlet carbene molecule indicating halogen like chemical behavior of gold. These molecules are found to be thermodynamically stable with respect to all plausible 2-body and 3-body dissociation channels, except the one that leads to the formation of the global minimum products. However, metastable nature of the predicted molecules has been proved by studying the saddle point corresponding to the transition from the minima to the global minimum products. Sufficient barrier heights provide the kinetic stability to the predicted FNgCM molecules, which prevent them from dissociating into their respective global minimum products. All the results clearly indicate that the F-Ng bond is mostly ionic in nature with certain amount of covalent character while Ng-C bond is found to be covalent in nature. Furthermore, atoms-in-molecule (AIM), energy decomposition analysis (EDA) and charge distribution analyses suggest that the predicted FNgCM molecules essentially exist in the form of [F]δ-[NgCM]δ+. The calculated results also indicate that it may be possible to prepare and characterize the predicted molecules by suitable experimental technique(s).
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Designing heavy-atom-free triplet photosensitizers (PSs) is a challenge for the efficient photodynamic therapy (PDT) of cancer. Helicenes are twisted polycyclic aromatic hydrocarbons (PAHs) with an efficient intersystem crossing (ISC) that is proportional to their twisting angle. But their difficult syntheses and weak absorption profile in the visible spectral region restrict their use as heavy-atom-free triplet PSs for PDT. On the other hand, boron-containing PAHs, BODIPYs are highly recognized for their outstanding optical properties. However, planar BODIPY dyes has low ISC and thus they are not very effective as PDT agents. We have designed and synthesized fused compounds containing both BODIPY and hetero[5]helicene structures to develop red-shifted chromophores with efficient ISC. One of the pyrrole units of the BODIPY core was also replaced by a thiazole unit to further enhance the triplet conversion. All the fused compounds have helical structure, and their twisting angles are also increased by substitutions at the boron centre. The helical structures of the BODIPY-hetero[5]helicenes were confirmed by X-ray crystallography and DFT structure optimization. The designed BODIPY-hetero[5]helicenes showed superior optical properties and high ISC with respect to [5]helicene. Interestingly their ISC efficiencies increase proportionally with their twisting angles. This is the first report on the relationship between the twisting angle and the ISC efficiency in twisted BODIPY-based compounds. Theoretical calculations showed that energy gap of the S1 and T1 states decreases in BODIPY-hetero[5]helicene as compared to planar BODIPY. This enhances the ISC rate in BODIPY-hetero[5]helicene, which is responsible for their high generation of singlet oxygen. Finally, their potential applications as PDT agents were investigated, and one BODIPY-hetero[5]helicene showed efficient cancer cell killing upon photo-exposure. This new design strategy will be very useful for the future development of heavy-atom-free PDT agents.
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Host-derived cellular pathways can provide an unfavorable environment for virus replication. These pathways have been a subject of interest for herpesviruses, including the betaherpesvirus human cytomegalovirus (HCMV). Here, we demonstrate that a compound, ARP101, induces the noncanonical sequestosome 1 (SQSTM1)/p62-Keap1-Nrf2 pathway for HCMV suppression. ARP101 increased the levels of both LC3 II and SQSTM1/p62 and induced phosphorylation of p62 at the C-terminal domain, resulting in its increased affinity for Keap1. ARP101 treatment resulted in Nrf2 stabilization and translocation into the nucleus, binding to specific promoter sites and transcription of antioxidant enzymes under the antioxidant response element (ARE), and HCMV suppression. Knockdown of Nrf2 recovered HCMV replication following ARP101 treatment, indicating the role of the Keap1-Nrf2 axis in HCMV inhibition by ARP101. SQSTM1/p62 phosphorylation was not modulated by the mTOR kinase or casein kinase 1 or 2, indicating ARP101 engages other kinases. Together, the data uncover a novel antiviral strategy for SQSTM1/p62 through the noncanonical Keap1-Nrf2 axis. This pathway could be further exploited, including the identification of the responsible kinases, to define the biological events during HCMV replication. IMPORTANCE Antiviral treatment for human cytomegalovirus (HCMV) is limited and suffers from the selection of drug-resistant viruses. Several cellular pathways have been shown to modulate HCMV replication. The autophagy receptor sequestosome 1 (SQSTM1)/p62 has been reported to interact with several HCMV proteins, particularly with components of HCMV capsid, suggesting it plays a role in viral replication. Here, we report on a new and unexpected role for SQSTM1/p62, in HCMV suppression. Using a small-molecule probe, ARP101, we show SQSTM1/p62 phosphorylation at its C terminus domain initiates the noncanonical Keap1-Nrf2 axis, leading to transcription of genes under the antioxidant response element, resulting in HCMV inhibition in vitro. Our study highlights the dynamic nature of SQSTM1/p62 during HCMV infection and how its phosphorylation activates a new pathway that can be exploited for antiviral intervention.
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Infecções por Citomegalovirus , Citomegalovirus , Replicação Viral , Citomegalovirus/efeitos dos fármacos , Citomegalovirus/fisiologia , Infecções por Citomegalovirus/prevenção & controle , Infecções por Citomegalovirus/virologia , Antivirais/farmacologia , Transcrição Gênica/efeitos dos fármacos , Fosforilação/efeitos dos fármacos , Elementos de Resposta Antioxidante/efeitos dos fármacos , Linhagem Celular , HumanosRESUMO
Closed-shell noble gas (Ng) compounds in the singlet electronic state have been extensively studied in the past two decades after the revolutionary discovery of 1HArF molecule. Motivated by the experimental identification of very strong donor-acceptor-type singlet-state Ng complex 1ArOH+, in the present article, for the first time, we report new donor-acceptor-type noble gas complexes in the triplet electronic state (3NgBeN+ (Ng = He-Rn)), where most of the Ng-Be bond lengths are smaller than the corresponding covalent limits. The newly proposed complexes are predicted to be stable by various computational tools, including coupled-cluster and multireference-based methods, with strong Ng-Be bonding (40.4-196.2 kJ mol-1). We have also investigated 3NgBeP+ (Ng = He-Rn) complexes for the purpose of comparison. Various computational results, including the structural parameters, bonding energies, vibrational frequencies, and atoms-in-molecule properties suggest that it may be possible to prepare and characterize these triplet state complexes through suitable experimental technique(s).
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Inosine pranobex (IP), an immunomodulatory agent, is used in the treatment of various viral infections. The results of a phase 3 randomized controlled trial are reported, evaluating the efficacy and safety of IP in the treatment of mild to moderate COVID-19. It includes 416 symptomatic patients with confirmed SARS-CoV-2 infection. In addition to a defined standard of care, patients randomly (1:1) receive either IP 500 mg tablet (IP group) or a matching placebo (placebo group) at 50 mg kg-1 body weight/day rounded to the nearest 500 mg dose (maximum 4 g day-1) administered in 3-4 divided doses for 10 days. Compared to the placebo group, IP group shows significantly higher rates of clinical response (CR) and clinical cure (CC) on Day-6 for both non-hospitalized patients and the total population. IP group shows significantly earlier CR and CC with fewer adverse events and no mortality. Based on these findings and the fact that IP increases natural killer cell-mediated cytotoxicity of virus-infected cells as an early immune response to viral infection and enhances NKG2D ligand expression, it is concluded that IP should be started early to maximize the benefit in mild to moderate COVID-19 patients. (Trial registration number: CTRI/2021/02/030892).
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Inspired by the overwhelming exploration of noble gas-boron (Ng-B) bond containing chemical compounds, the stability of the Ng bound BY+ and AlY+ (Y = O and S) has been investigated by using various ab initio based quantum chemical methods. Ng atoms are found to form exceptionally strong bonds with BO+ species in the predicted NgBO+ (Ng = He-Rn) complexes with remarkably high Ng-B dissociation energies ranging from 138.0 to 462.2 kJ mol-1 for the He-Rn series. It is the highest ever Ng-B binding energy in conjunction with the smallest Ng-B bond length for any of the cationic species involving a Ng-B bond as reported until today. More importantly, the calculated Ng-B bond lengths have been found to be much lower than the respective covalent limits in both NgBO+ and NgBS+ ions. The electronegativity difference between O and S atoms has been reflected nicely in the Ng-B and Ng-Al binding energies, which are found to be 91.9-346.5, 9.6-169.2, and 6.8-142.1 kJ mol-1 in NgBS+, NgAlO+, and NgAlS+, respectively. The strong covalent bonding between Ng and B/Al atoms in the predicted chemical systems has also been supported by the natural bonding orbital (NBO) and electron density based atoms-in-molecule (AIM) analysis. In addition, the energy decomposition analysis (EDA) in combination with the natural bond orbital for chemical valence (NOCV) indicates that the orbital interaction term is the prime contributor to the total attraction energy in the Ng-B and Ng-Al bonds. Furthermore, Ng-B and Ng-Al bonding can be assessed using the donor-acceptor model where the σ-electron donation that takes place from Ng (HOMO) â XY+ (LUMO) (X = B and Al; Y = O and S) is the major contributor to the orbital interaction energy. All the computational results along with the very recent experimental observation of ArOH+ and NgMX (Ng = Ar-Xe; M = Cu, Ag, Au; X = F, Cl) clearly indicate that it might be possible to synthesize and characterize these superstrong complexes, NgXY+ (Ng = He-Rn; X = B and Al; Y = O and S), under suitable experimental technique(s).
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The scarce literature on noble gas (Ng)-phosphorous chemical bonding and our recent theoretical prediction of the FNgP molecule motivate us to explore a unique novel class of neutral noble gas-inserted phosphorus trifluoride and pentafluoride molecules, i.e., FNgPF2 and FNgPF4 (Ng = Ar, Kr, Xe, and Rn). The predicted molecules have been designed by inserting an Ng atom between the F and P atoms in the PF3 and PF5 molecules. The minima and saddle point geometries of all the FNgPFn (n = 2 and 4) molecules have been optimized using density functional theory (DFT) and second-order Møller-Plesset perturbation theory (MP2). The coupled cluster theory (CCSD(T)) method is also used to optimize the FNgPF2 molecules to test the performance of the above-mentioned methods. The predicted FNgPF2 and FNgPF4 molecules are found to be energetically stable with respect to all the probable 2-body and 3-body dissociation channels, except for the one leading to the global minimum products (Ng + PF3 and Ng + PF5). The existence of large barrier heights corresponding to the saddle point geometries is responsible for the kinetic stability of the metastable FNgPFn (n = 2 and 4) molecules, which prevents them from dissociating into their global minima products. The optimized structural parameters, energetics and harmonic vibrational frequency analysis suggest that the Ng-P bond is covalent in nature, while the F-Ng bond is mostly ionic in nature with some degree of covalency in the predicted molecules. In fact, the Ng-P bond length in the experimentally observed Ng-PF3 van der Waals complex is reduced significantly in the isomeric FNgPF2 molecule, almost leading to a conventional covalent Ng-P bond (cf. 4.152 vs. 2.413 Å for the Kr-P bond). Furthermore, the charge distribution and the AIM analysis also confirm the above-mentioned conclusion and indicate that the predicted FNgPF2 and FNgPF4 molecules can be represented as [F]δ-[NgPF2]δ+ and [F]δ-[NgPF4]δ+, respectively. All the computational results strongly reinforce the possible existence of these predicted FNgPFn (n = 2 and 4) molecules and clearly indicate that it may be possible to synthesize and characterize these molecules under suitable experimental technique(s).
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Treatment options for human cytomegalovirus (CMV) remain limited and are associated with significant adverse effects and the selection of resistant CMV strains in transplant recipients and congenitally infected infants. Although most approved drugs target and inhibit the CMV DNA polymerase, additional agents with distinct mechanisms of action are needed for the treatment and prevention of CMV. In a large high throughput screen using our CMV-luciferase reporter Towne, we identified several unique inhibitors of CMV replication. Here, we synthesize and test in vitro 13 analogs of the original NCGC2955 hit (1). Analogs with no activity against the CMV-luciferase at 10 µM and 30 µM (2-6, 10-14) were removed from further analysis. Three analogs (7-9) inhibited CMV replication in infected human foreskin fibroblasts. The EC50 of (1) was 1.7 ± 0.6 µM and 1.99 ± 0.15 µM, based on luciferase and plaque assay, respectively. Compounds 7, 8, and 9 showed similar activities: the EC50 values of 7 were 0.21 ± 0.06 µM (luciferase) and 0.55 ± 0.06 (plaque), of 8: 0.28 ± 0.06 µM and 0.42 ± 0.07, and of 9: 0.30 ± 0.05 µM (luciferase) and 0.35 ± 0.07 (plaque). The CC50 for 7, 8, and 9 in non-infected human foreskin fibroblasts was > 500µM, yielding a selectivity index of >1500. Compounds 1, 7, and 8 were also tested in CMV-infected primary human hepatocytes and showed a dose-response against CMV by luciferase activity and viral protein expression. None of the active compounds inhibited herpes simplex virus 1 or 2. Compounds 7 and 8 inhibited mouse CMV replication in vitro. Both inhibited CMV at late stages of replication; 7 reduced virus yield at all late time points, although not to the same degree as letermovir. Finally, the activity of analog 8 was additive with newly identified CMV inhibitors (MLS8969, NFU1827, MSL8554, and MSL8091) and with ganciclovir. Further structural activity development should provide promising anti-CMV agents for use in clinical studies.
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Antivirais/síntese química , Antivirais/farmacologia , Citomegalovirus/efeitos dos fármacos , Animais , Células Cultivadas , Citomegalovirus/fisiologia , Ganciclovir/farmacologia , Hepatócitos/virologia , Herpesvirus Humano 1/efeitos dos fármacos , Herpesvirus Humano 2/efeitos dos fármacos , Humanos , Camundongos , Testes de Sensibilidade Microbiana , Estrutura Molecular , Muromegalovirus/efeitos dos fármacos , Relação Estrutura-Atividade , Carga Viral , Replicação Viral/efeitos dos fármacosRESUMO
Recent theoretical prediction and experimental identification of fluorinated noble gas cyanides and isocyanides motivate us to explore a unique novel series of neutral noble gas-inserted heavier cyanofluoride isomers, FNgYSi and FNgSiY (Ng = Kr, Xe, and Rn; Y = N and P), theoretically using quantum chemical calculations. The concerned minima and saddle point geometries have been optimized using DFT, MP2, and CCSD(T) methods. The precursor molecule FSiY is more stable than its isomer FYSi, and the stability order is found to be reversed after the insertion of a noble gas (Ng) atom into them which is in contrast to the previously reported FCN/FNC systems where the stability order in the precursors remains intact after the insertion of a Ng atom into them. The predicted FNgYSi molecules are metastable in nature as they are kinetically stable but thermodynamically unstable with respect to the global minima products (FYSi and Ng). All the calculations for the corresponding FNgSiY molecules clearly indicate that the less stable FNgSiY behaves similarly to the FNgYSi in all respects. The energetics, force constant, and spectroscopic data strongly reinforce the possibility of occurrence of these predicted FNgYSi and FNgSiY molecules which might be experimentally realized under suitable cryogenic condition(s).
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As the toll of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic continues, efforts are ongoing to identify new agents and repurpose safe drugs for its treatment. Antimalarial peroxides have reported antiviral and anticancer activities. Here, we evaluated the in vitro activities of artesunate (AS) and two ozonides (OZ418 and OZ277) against human α-coronavirus NL63 and ß-coronaviruses OC43 and SARS-CoV-2 in several cell lines. OZ418 had the best selectivity index (SI) in NL63-infected Vero cells and MK2 cells. The overall SI of the tested compounds was cell-type dependent. In OC43-infected human foreskin fibroblasts, AS had the best cell-associated SI, ≥17 µM, while the SI of OZ418 and OZ277 was ≥12 µM and ≥7 µM, respectively. AS did not inhibit SARS-CoV-2 in either Vero or Calu-3 cells. A comparison of OZ418 and OZ277 activity in SARS-CoV2-infected Calu-3 cells revealed similar EC50 (5.3 µM and 11.6 µM, respectively), higher than the EC50 of remdesivir (1.0 ± 0.1 µM), but the SI of OZ418 was higher than OZ277. A third ozonide, OZ439, inhibited SARS-CoV-2 efficiently in Vero cells, but compared to OZ418 in Calu-3 cells, it showed higher toxicity. Improved inhibition of SARS-CoV-2 was observed when OZ418 was used together with remdesivir. Although the EC50 of ozonides might be clinically achieved in plasma after intravenous administration, sustained virus suppression in tissues will require further considerations, including drug combination. Our work supports the potential repurposing of ozonides and calls for future in vivo models.
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Antimaláricos , COVID-19 , Animais , Antimaláricos/farmacologia , Chlorocebus aethiops , Humanos , Peróxidos/farmacologia , RNA Viral , SARS-CoV-2 , Células VeroRESUMO
The antimalarial agents artemisinins inhibit cytomegalovirus (CMV) in vitro and in vivo, but their target(s) has been elusive. Using a biotin-labeled artemisinin, we identified the intermediate filament protein vimentin as an artemisinin target, validated by detailed biochemical and biological assays. We provide insights into the dynamic and unique modulation of vimentin, depending on the stage of human CMV (HCMV) replication. In vitro, HCMV entry and viral progeny are reduced in vimentin-deficient fibroblasts, compared with control cells. Similarly, mouse CMV (MCMV) replication in vimentin knockout mice is significantly reduced compared with controls in vivo, confirming the requirement of vimentin for establishment of infection. Early after HCMV infection of human foreskin fibroblasts vimentin level is stable, but as infection proceeds, vimentin is destabilized, concurrent with its phosphorylation and virus-induced calpain activity. Intriguingly, in vimentin-overexpressing cells, HCMV infection is reduced compared with control cells. Binding of artesunate, an artemisinin monomer, to vimentin prevents virus-induced vimentin degradation, decreasing vimentin phosphorylation at Ser-55 and Ser-83 and resisting calpain digestion. In vimentin-deficient fibroblasts, the anti-HCMV activity of artesunate is reduced compared with controls. In summary, an intact and stable vimentin network is important for the initiation of HCMV replication but hinders its completion. Artesunate binding to vimentin early during infection stabilizes it and antagonizes subsequent HCMV-mediated vimentin destabilization, thus suppressing HCMV replication. Our target discovery should enable the identification of vimentin-binding sites and compound moieties for binding.
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Antivirais/farmacologia , Artemisininas/farmacologia , Citomegalovirus/efeitos dos fármacos , Vimentina/antagonistas & inibidores , Antivirais/química , Antivirais/metabolismo , Artemisininas/química , Artemisininas/metabolismo , Artesunato/farmacologia , Sítios de Ligação , Calpaína/metabolismo , Ciclo Celular/efeitos dos fármacos , Células Cultivadas , Citomegalovirus/fisiologia , Infecções por Citomegalovirus/metabolismo , Reposicionamento de Medicamentos , Humanos , Espectrometria de Massas , Fosforilação , Complexo de Endopeptidases do Proteassoma/metabolismo , Vimentina/genética , Vimentina/metabolismo , Replicação Viral/efeitos dos fármacos , Vitanolídeos/farmacologiaRESUMO
Motivated by the discovery of neutral noble gas hydrides, herein, we have explored the possibility of the existence of a novel class of neutral noble gas compounds, HNgBO, HNgOB, HNgAlO and HNgOAl (Ng = Xe and Rn), through the insertion of a Ng atom into the hydroxides of icosagens and their isomers, namely, HBO, HOB, HAlO and HOAl. Second-order Møller-Plesset perturbation theory (MP2), density functional theory (DFT), and coupled-cluster theory (CCSD(T))-based methods have been employed to investigate the structures, stabilities, energetics, harmonic vibrational frequencies, and charge distribution of the predicted molecules. The HXeBO, HXeOAl, HRnBO, HRnAlO and HRnOAl molecules are found to be thermodynamically stable with respect to all plausible 2-body and 3-body dissociation channels except the 2-body dissociation pathway, leading to the formation of global minimum products (Ng + HBO), (Ng + HOAl) and (Ng + HAlO). However, the very large activation energy barrier heights provide enough kinetic stability to the predicted metastable molecules, which in turn can prevent them from dissociating into the global minimum products. Between the HNgBO-HNgOB isomers, HNgBO is found to be more stable, where both HNgBO and the precursor molecule HBO are linear. On the other hand, HNgOAl is more stable between the HNgAlO-HNgOAl isomers, where the precursor molecule HOAl is bent and HNgOAl is linear in contradiction and in agreement with Walsh's rule, respectively. Moreover, in contrast to the more stable HNgBO case, where the Ng atom is bonded with the icosagen atom, in the more stable HNgOAl, the Ng atom is connected to the chalcogen atom. All the detailed aforementioned analyses concerning the predicted molecules clearly indicate that a strong covalent bond exists between the H and Ng atoms, while an ionic interaction is found between the Ng and B atoms in HNgBO and Ng and O atoms in the HNgOAl molecules. In addition, the charge distribution and atoms-in-molecules (AIM) analyses are in agreement with the above-mentioned conclusion and also suggest that the predicted metastable HNgBO and HNgOAl molecules should essentially exist in the form of [HNg]+[BO]- and [HNg]+[OAl]-, respectively. All the calculated results reported in this work indicate that it might be possible to prepare and characterize the predicted molecules via suitable experimental technique(s) under cryogenic conditions.
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The critical consequences of human cytomegalovirus (HCMV) infection in the transplant population and in congenitally infected infants, the limited treatment options for HCMV, and the rise of resistant mutants toward existing therapies has fueled the search for new anti-HCMV agents. A pp28-luciferase recombinant HCMV was used as a reporter system for high-throughput screening of HCMV inhibitors. Approximately 400â¯000 compounds from existing libraries were screened. Subsequent validation assays using resynthesized compounds, several virus strains, and detailed virology assays resulted in the identification of five structurally unique and selective HCMV inhibitors, active at sub to low micromolar concentrations. Further characterization revealed that each compound inhibited a specific stage of HCMV replication. One compound was also active against herpes simplex virus (HSV1 and HSV2), and another compound was active against Epstein-Barr virus (EBV). Drug combination studies revealed that all five compounds were additive with ganciclovir or letermovir. Future studies will focus on optimization of these new anti-HCMV compounds along with mechanistic studies.
