Alkaloids from the Sponge Stylissa carteri Present Prospective Scaffolds for the Inhibition of Human Immunodeficiency Virus 1 (HIV-1).

The sponge Stylissa carteri is known to produce a number of secondary metabolites displaying anti-fouling, anti-inflammatory, and anti-cancer activity. However, the anti-viral potential of metabolites produced by S. carteri has not been extensively explored. In this study, an S. carteri extract was HPLC fractionated and a cell based assay was used to evaluate the effects of HPLC fractions on parameters of Human Immunodeficiency Virus (HIV-1) infection and cell viability. Candidate HIV-1 inhibitory fractions were then analyzed for the presence of potential HIV-1 inhibitory compounds by mass spectrometry, leading to the identification of three previously characterized compounds, i.e., debromohymenialdisine (DBH), hymenialdisine (HD), and oroidin. Commercially available purified versions of these molecules were re-tested to assess their antiviral potential in greater detail. Specifically, DBH and HD exhibit a 30%-40% inhibition of HIV-1 at 3.1 μM and 13 μM, respectively; however, both exhibited cytotoxicity. Conversely, oroidin displayed a 50% inhibition of viral replication at 50 μM with no associated toxicity. Additional experimentation using a biochemical assay revealed that oroidin inhibited the activity of the HIV-1 Reverse Transcriptase up to 90% at 25 μM. Taken together, the chemical search space was narrowed and previously isolated compounds with an unexplored anti-viral potential were found. Our results support exploration of marine natural products for anti-viral drug discovery

Diverse computational tools towards the understanding of HIV targets and design of potential drug candidates.

Ph. D. University of KwaZulu-Natal, Durban 2014.HIV/AIDS still remains to be a challenging epidemic infecting millions of individuals worldwide. The morbidity and mortality rates of HIV-infected patients has been well documented over the years. Despite on-going HIV/AIDS research and access to antiretroviral therapy, to date still no cure exists for this deliberating disease. In recent years, computational approaches have emerged as close counterparts to experiments in modern drug discovery process and in understanding complex biological phenomena. An array of in-silico computational techniques were implemented ranging from molecular dynamic (MD) simulations, de-novo design, hybrid structure-based and pharmacophore-based virtual screening, quantitative structure-activity relationship (QSAR), homology modeling, principle component analysis (PCA), residue interaction network analysis (RIN), substrate envelope analysis (SEA), to molecular mechanics and quantum mechanics. The first report (Chapter 4), demonstrated a unique strategy for developing dual acting inhibitors against HIV-1 protease (PR) and reverse transcriptase (RT). The designed targets exhibited binding affinities and dual inhibiting activity comparable to, and in some cases better than, known active reference drugs. The second study (Chapter 5), reported the activity of flexible hydroquinone-based compounds as non-nucleoside reverse transcriptase inhibitors (NNRTIs), as proposed by Bruccoleri, where no experimental or computational work supported his proposal. Results concluded that the novel flexible hydroquinone-based compounds showed improved binding affinity as compared to FDA-approved prototype drugs and more specifically potent potential mutant-resistant NNRT inhibitor activity. The third report (Chapter 6), explored the activity of novel CCR5 antagonists as potential HIV- 1 entry inhibitors. Ten scaffolds were identified as novel CCR5 antagonists or potential HIV-1 entry inhibitors. Furthermore, from the generated atom-based 3D-QSAR model, all of the parameters showed certain reliability and feasible predictability to help us design new and high selectivity CCR5 inhibitors. The fourth study (Chapter 7), explored the atomistic basis of why the M184I single mutation renders complete resistance of HIV-1 RT to lamivudine. Multiple molecular dynamics simulations, binding free energy calculations, principle component analysis (PCA) and residue interaction network (RIN) analyses adequately clarified the effect of the M184I mutation on drug resistance to lamvudine. Results presented in this study verified that M184I mutation decreased drug binding affinity, distorted ligand optimum orientation in RT active site and affected the overall protein conformational landscape. The results also provided some potential clues for further design of novel inhibitors that are less susceptible to drug resistance. In the fifth study (Chapter 8), we identified potential HIV-Nef inhibitors by exploiting the structural features of B9 using an integrated computational tools framework. The top identified hit compounds demonstrated comparatively better binding affinities and relatable binding modes compared to the prototype antagonist, B9. Top identified hits were proposed as new potential novel leads targeting HIV-Nef with a detailed analysis of their respective binding modes. The sixth report (Chapter 9), aimed to reveal the dimer packing and unpacking phenomena of HIV-Nef in its apo and inhibitor bound conformations using molecular dynamic simulations. Results verified a more conformational flexible nature of HIV-Nef dimer in the absence of an inhibitor.as compared to B9 bound conformation of HIV-Nef, which was found to be more conformationally rigid with a lesser inter-dimeric association. We believe that the results obtained from these several studies could be of great benefit in the development of more effective therapeutic interventions for the treatment and cure of HIV/AIDS

In silico screening for human norovirus antivirals reveals a novel non-nucleoside inhibitor of the viral polymerase

Human norovirus causes approximately 219,000 deaths annually, yet there are currently no antivirals available. A virtual screening of commercially available drug-like compounds (~300,000) was performed on the suramin and PPNDS binding-sites of the norovirus RNA-dependent RNA polymerase (RdRp). Selected compounds (n = 62) were examined for inhibition of norovirus RdRp activity using an in vitro transcription assay. Eight candidates demonstrated RdRp inhibition (>25% inhibition at 10 μM), which was confirmed using a gel-shift RdRp assay for two of them. The two molecules were identified as initial hits and selected for structure-activity relationship studies, which resulted in the synthesis of novel compounds that were examined for inhibitory activity. Five compounds inhibited human norovirus RdRp activity (>50% at 10 μM), with the best candidate, 54, demonstrating an IC50 of 5.6 μM against the RdRp and a CC50 of 62.8 μM. Combinational treatment of 54 and the known RdRp site-B inhibitor PPNDS revealed antagonism, indicating that 54 binds in the same binding pocket. Two RdRps with mutations (Q414A and R419A) previously shown to be critical for the binding of site-B compounds had no effect on inhibition, suggesting 54 interacts with distinct site-B residues. This study revealed the novel scaffold 54 for further development as a norovirus antiviral

Focus on chirality of HIV-​1 non-​nucleoside reverse transcriptase inhibitors

Chiral HIV-1 non-nucleoside reverse transcriptase inhibitors (NNRTIs) are of great interest since one enantiomer is often more potent than the corresponding counterpart against the HIV-1 wild type (WT) and the HIV-1 drug resistant mutant strains. This review exemplifies the various studies made to investigate the effect of chirality on the antiretroviral activity of top HIV-1 NNRTI compounds, such as nevirapine (NVP), efavirenz (EFV), alkynyl- and alkenylquinazolinone DuPont compounds (DPC), diarylpyrimidine (DAPY), dihydroalkyloxybenzyloxopyrimidine (DABO), phenethylthiazolylthiourea (PETT), indolylarylsulfone (IAS), arylphosphoindole (API) and trifluoromethylated indole (TFMI) The chiral separation, the enantiosynthesis, along with the biological properties of these HIV-1 NNRTIs, are discussed

Molecular modeling studies on HIV-1 Reverse Transcriptase (RT) and Heat shock protein (Hsp) 90 as a potential anti-HIV-1 target.

Masters Degree. University of KwaZulu-Natal, Durban.Human immunodeficiency virus (HIV) infection is the leading cause of death globally. This dissertation addresses two HIV-1 target proteins namely, HIV-1 Reverse Transcriptase (RT) and Heat shock protein (Hsp) 90. More specifically for HIV-1 RT, a case study for the identification of potential inhibitors as anti-HIV agents was carried out. A more refined virtual screening (VS) approach was implemented, which was an improvement on work previously published by our group- “target-bound pharmacophore modeling approach”. This study generated a pharmacophore library based only on highly contributing amino acid residues (HCAAR), instead of arbitrary pharmacophores, most commonly used in the conventional approaches in literature. HCAAR were distinguished based on free binding energy (FBE) contributions, obtained using calculation from molecular dynamics (MD) simulations. Previous approaches have relied on the docking score (DS) to generate energy-based pharmacophore models. However, DS are reportedly unreliable. Thus we present a model for a per-residue energy decomposition (PRED), constructed from MD simulation ensembles generating a more trustworthy pharmacophore model which can be applied in drug discovery workflow. This approach was employed in screening for potential HIV-1 RT inhibitors using the pharmacophoric features of the compound GSK952. The complex was subjected to docking and thereafter MD simulations confirmed the stability of the system. Experimentally determined inhibitors with known HIV-RT inhibitory activity were used to validate the proposed protocol. Two potential hits ZINC46849657 and ZINC54359621 showed a significant potential with regards to FBE. Reported results obtained from this work confirm that this new approach is favourable to the future of drug design process. Hsp90 was recently discovered to play a vital role in HIV-1 replication. Thus has emerged, as a promising target for anti-HIV-1 drugs. The molecular mechanism of Hsp90 is poorly understood, thus the second study was aimed to address this issue and provide a clear insight to the inhibition mechanism of Hsp90. Reasonable continuous MD simulations were employed for both unbound and bound Hsp90 conformations, to understand the dimerization and inhibition mechanisms. Results demonstrated that coumermycin A1 (C-A1), a newly discovered Hsp90 inhibitor, binds at the CTD dimer of Hsp90 and lead to a significant separation between orthogonally opposed residues, such as Arg591.B, Lys594.A, Ser663.A, Thr653.B, Ala665.A, Thr649.B, Leu646.B and Asn669A. A Large difference in magnitudes was observed in the radius of gyration (Rg), per-residue fluctuation, root-mean-square deviation (RMSD) and root-mean-square fluctuation (RMSF) confirming a completely more flexible state for the unbound conformation associated with dimerization. Whereas, a less globally correlated motion in the case of the bound conformer of Hsp90 approved a reduction of the dimeric process. This undoubtedly underlines the inhibition process due to ligand binding. The detailed dynamic analyses of Hsp90 presented herein are believed to give a greater insight and understanding to the function and mechanisms of inhibition of Hsp90. The report on the inhibitor-binding mode would also be of great assistance in the design of prospective inhibitors against Hsp90 as potential HIV target

A Brief Review of the Medicinally Important Indole Derivatives

Indole is an exceptional heterocyclic molecule with a broad spectrum of pharmacological activity owing to various modes of action. It is also a versatile pharmacophore and a favored scaffold. For drug development, it is an excellent moiety whose only characteristic is that it resembles many protein structures. Plenty of research has been taking place in recent years to synthesize and explore the various therapeutic prospective of this moiety. This review summarizes some of the recent effective chemical synthesis (2014-2018) for indole ring. Some of the most recent efficient chemical synthesis for the indole ring (from 2014 to 2018) is compiled in this review. The structure-activity relationship (SAR) was also given a lot of weight in this review in order to pinpoint the active pharmacophores of different indole analogues that have been the subject of studies for the past five years and are responsible for a variety of effects, including antiviral, antitubercular, anticancer, and anticonvulsant ones. The goals and framework of every research issue are explained in detail to help medicinal chemists have a deeper understanding of the circumstances contextually. Researchers will undoubtedly use this review as a platform to strategically design a variety of novel indole derivatives with lower toxicity and side effects and a range of intriguing pharmacological activit

Chemical Similarity Networks for Drug Discovery

Chemical similarity networks are an emerging area of interest in medicinal chemistry, chemical biology, and systems chemoinformatics that are currently being applied to drug target prediction, drug repurposing, and drug discovery in the new paradigm of poly-pharmacology and systems biology. In this chapter, we discuss the network-based drug target identification and discovery framework called chemical similarity network analysis pull-down (CSNAP) and its applications. We highlight the utility of CSNAP in identifying novel antimitotic drugs and their targets through practical case studies

Screening of the Pan-African Natural Product Library Identifies Ixoratannin A-2 and Boldine as Novel HIV-1 Inhibitors

The continued burden of HIV in resource-limited regions such as parts of sub-Saharan Africa, combined with adverse effects and potential risks of resistance to existing antiretroviral therapies, emphasize the need to identify new HIV inhibitors. Here we performed a virtual screen of molecules from the pan-African Natural Product Library, the largest collection of medicinal plant-derived pure compounds on the African continent. We identified eight molecules with structural similarity to reported interactors of Vpu, an HIV-1 accessory protein with reported ion channel activity. Using in vitro HIV-1 replication assays with a CD4+ T cell line and peripheral blood mononuclear cells, we confirmed antiviral activity and minimal cytotoxicity for two compounds, ixoratannin A-2 and boldine. Notably, ixoratannin A-2 retained inhibitory activity against recombinant HIV-1 strains encoding patient-derived mutations that confer resistance to protease, non-nucleoside reverse transcriptase, or integrase inhibitors. Moreover, ixoratannin A-2 was less effective at inhibiting replication of HIV-1 lacking Vpu, supporting this protein as a possible direct or indirect target. In contrast, boldine was less effective against a protease inhibitor-resistant HIV-1 strain. Both ixoratannin A-2 and boldine also inhibited in vitro replication of hepatitis C virus (HCV). However, BIT-225, a previously-reported Vpu inhibitor, demonstrated antiviral activity but also cytotoxicity in HIV-1 and HCV replication assays. Our work identifies pure compounds derived from African plants with potential novel activities against viruses that disproportionately afflict resource-limited regions of the world