Your search keyword '"de Vera, Ian Mitchelle S."' showing total 8 results

1. International Union of Basic and Clinical Pharmacology CXIII: Nuclear Receptor Superfamily—Update 2023

Author

Burris, Thomas P., de Vera, Ian Mitchelle S., Cote, Isabelle, Flaveny, Colin A., Wanninayake, Udayanga S., Chatterjee, Arindam, Walker, John K., Steinauer, Nickolas, Zhang, Jinsong, Coons, Laurel A., Korach, Kenneth S., Cain, Derek W., Hollenberg, Anthony N., Webb, Paul, Forrest, Douglas, Jetten, Anton M., Edwards, Dean P., Grimm, Sandra L., Hartig, Sean, Lange, Carol A., Richer, Jennifer K., Sartorius, Carol A., Tetel, Marc, Billon, Cyrielle, Elgendy, Bahaa, Hegazy, Lamees, Griffett, Kristine, Peinetti, Nahuel, Burnstein, Kerry L., Hughes, Travis S., Sitaula, Sadichha, Stayrook, Keitch R., Culver, Alexander, Murray, Meghan H., Finck, Brian N., and Cidlowski, John A.

Abstract

The NR superfamily comprises 48 transcription factors in humans that control a plethora of gene network programs involved in a wide range of physiologic processes. This review will summarize and discuss recent progress in NR biology and drug development derived from integrating various approaches, including biophysical techniques, structural studies, and translational investigation. We also highlight how defective NR signaling results in various diseases and disorders and how NRs can be targeted for therapeutic intervention via modulation via binding to synthetic lipophilic ligands. Furthermore, we also review recent studies that improved our understanding of NR structure and signaling.

Published

2023

2. International Union of Basic and Clinical Pharmacology CXIII: Nuclear Receptor Superfamily—Update 2023

Author

Burris, Thomas P., de Vera, Ian Mitchelle S., Cote, Isabelle, Flaveny, Colin A., Wanninayake, Udayanga S., Chatterjee, Arindam, Walker, John K., Steinauer, Nickolas, Zhang, Jinsong, Coons, Laurel A., Korach, Kenneth S., Cain, Derek W., Hollenberg, Anthony N., Webb, Paul, Forrest, Douglas, Jetten, Anton M., Edwards, Dean P., Grimm, Sandra L., Hartig, Sean, Lange, Carol A., Richer, Jennifer K., Sartorius, Carol A., Tetel, Marc, Billon, Cyrielle, Elgendy, Bahaa, Hegazy, Lamees, Griffett, Kristine, Peinetti, Nahuel, Burnstein, Kerry L., Hughes, Travis S., Sitaula, Sadichha, Stayrook, Keitch R., Culver, Alexander, Murray, Meghan H., Finck, Brian N., and Cidlowski, John A.

Abstract

The NR superfamily comprises 48 transcription factors in humans that control a plethora of gene network programs involved in a wide range of physiologic processes. This review will summarize and discuss recent progress in NR biology and drug development derived from integrating various approaches, including biophysical techniques, structural studies, and translational investigation. We also highlight how defective NR signaling results in various diseases and disorders and how NRs can be targeted for therapeutic intervention via modulation via binding to synthetic lipophilic ligands. Furthermore, we also review recent studies that improved our understanding of NR structure and signaling.Significance StatementNuclear receptors (NRs) are ligand-regulated transcription factors that are critical regulators of myriad physiological processes. NRs serve as receptors for an array of drugs, and in this review, we provide an update on recent research into the roles of these drug targets.

Published

2023

3. Identification of potent small molecule inhibitors of SARS-CoV-2 entry

Author

Mediouni, Sonia, Mou, Huihui, Otsuka, Yuka, Jablonski, Joseph Anthony, Adcock, Robert Scott, Batra, Lalit, Chung, Dong-Hoon, Rood, Christopher, de Vera, Ian Mitchelle S., Rahaim Jr., Ronald, Ullah, Sultan, Yu, Xuerong, Getmanenko, Yulia A., Kennedy, Nicole M., Wang, Chao, Nguyen, Tu-Trinh, Hull, Mitchell, Chen, Emily, Bannister, Thomas D., Baillargeon, Pierre, Scampavia, Louis, Farzan, Michael, Valente, Susana T., and Spicer, Timothy P.

Abstract

The severe acute respiratory syndrome coronavirus 2 responsible for COVID-19 remains a persistent threat to mankind, especially for the immunocompromised and elderly for which the vaccine may have limited effectiveness. Entry of SARS-CoV-2 requires a high affinity interaction of the viral spike protein with the cellular receptor angiotensin-converting enzyme 2. Novel mutations on the spike protein correlate with the high transmissibility of new variants of SARS-CoV-2, highlighting the need for small molecule inhibitors of virus entry into target cells. We report the identification of such inhibitors through a robust high-throughput screen testing 15,000 small molecules from unique libraries. Several leads were validated in a suite of mechanistic assays, including whole cell SARS-CoV-2 infectivity assays. The main lead compound, calpeptin, was further characterized using SARS-CoV-1 and the novel SARS-CoV-2 variant entry assays, SARS-CoV-2 protease assays and molecular docking. This study reveals calpeptin as a potent and specific inhibitor of SARS-CoV-2 and some variants.

Published

2022

4. Assessment of NR4A Ligands That Directly Bind and Modulate the Orphan Nuclear Receptor Nurr1

Author

Munoz-Tello, Paola, Lin, Hua, Khan, Pasha, de Vera, Ian Mitchelle S., Kamenecka, Theodore M., and Kojetin, Douglas J.

Abstract

Nurr1/NR4A2 is an orphan nuclear receptor transcription factor implicated as a drug target for neurological disorders including Alzheimer’s and Parkinson’s diseases. Previous studies identified small-molecule NR4A nuclear receptor modulators, but it remains unclear if these ligands affect transcription via direct binding to Nurr1. We assessed 12 ligands reported to affect NR4A activity for Nurr1-dependent and Nurr1-independent transcriptional effects and the ability to bind the Nurr1 ligand-binding domain (LBD). Protein NMR structural footprinting data show that amodiaquine, chloroquine, and cytosporone B bind the Nurr1 LBD; ligands that do not bind include C-DIM12, celastrol, camptothecin, IP7e, isoalantolactone, ethyl 2-[2,3,4-trimethoxy-6-(1-octanoyl)phenyl]acetate (TMPA), and three high-throughput screening hit derivatives. Importantly, ligands that modulate Nurr1 transcription also show Nurr1-independent effects on transcription in a cell type-specific manner, indicating that care should be taken when interpreting the functional response of these ligands in transcriptional assays. These findings should help focus medicinal chemistry efforts that desire to optimize Nurr1-binding ligands.

Published

2020

5. Identification of a Binding Site for Unsaturated Fatty Acids in the Orphan Nuclear Receptor Nurr1

Author

de Vera, Ian Mitchelle S., Giri, Pankaj K., Munoz-Tello, Paola, Brust, Richard, Fuhrmann, Jakob, Matta-Camacho, Edna, Shang, Jinsai, Campbell, Sean, Wilson, Henry D., Granados, Juan, Gardner, William J., Creamer, Trevor P., Solt, Laura. A., and Kojetin, Douglas J.

Abstract

Nurr1/NR4A2 is an orphan nuclear receptor, and currently there are no known natural ligands that bind Nurr1. A recent metabolomics study identified unsaturated fatty acids, including arachidonic acid and docosahexaenoic acid (DHA), that interact with the ligand-binding domain (LBD) of a related orphan receptor, Nur77/NR4A1. However, the binding location and whether these ligands bind other NR4A receptors were not defined. Here, we show that unsaturated fatty acids also interact with the Nurr1 LBD, and solution NMR spectroscopy reveals the binding epitope of DHA at its putative ligand-binding pocket. Biochemical assays reveal that DHA-bound Nurr1 interacts with high affinity with a peptide derived from PIASγ, a protein that interacts with Nurr1 in cellular extracts, and DHA also affects cellular Nurr1 transactivation. This work is the first structural report of a natural ligand binding to a canonical NR4A ligand-binding pocket and indicates a natural ligand can bind and affect Nurr1 function.

Published

2016

6. Ebselen, a Small-Molecule Capsid Inhibitor of HIV-1 Replication

Author

Thenin-Houssier, Suzie, de Vera, Ian Mitchelle S., Pedro-Rosa, Laura, Brady, Angela, Richard, Audrey, Konnick, Briana, Opp, Silvana, Buffone, Cindy, Fuhrmann, Jakob, Kota, Smitha, Billack, Blase, Pietka-Ottlik, Magdalena, Tellinghuisen, Timothy, Choe, Hyeryun, Spicer, Timothy, Scampavia, Louis, Diaz-Griffero, Felipe, Kojetin, Douglas J., and Valente, Susana T.

Abstract

ABSTRACTThe human immunodeficiency virus type 1 (HIV-1) capsid plays crucial roles in HIV-1 replication and thus represents an excellent drug target. We developed a high-throughput screening method based on a time-resolved fluorescence resonance energy transfer (HTS-TR-FRET) assay, using the C-terminal domain (CTD) of HIV-1 capsid to identify inhibitors of capsid dimerization. This assay was used to screen a library of pharmacologically active compounds, composed of 1,280 in vivo-active drugs, and identified ebselen [2-phenyl-1,2-benzisoselenazol-3(2H)-one], an organoselenium compound, as an inhibitor of HIV-1 capsid CTD dimerization. Nuclear magnetic resonance (NMR) spectroscopic analysis confirmed the direct interaction of ebselen with the HIV-1 capsid CTD and dimer dissociation when ebselen is in 2-fold molar excess. Electrospray ionization mass spectrometry revealed that ebselen covalently binds the HIV-1 capsid CTD, likely via a selenylsulfide linkage with Cys198 and Cys218. This compound presents anti-HIV activity in single and multiple rounds of infection in permissive cell lines as well as in primary peripheral blood mononuclear cells. Ebselen inhibits early viral postentry events of the HIV-1 life cycle by impairing the incoming capsid uncoating process. This compound also blocks infection of other retroviruses, such as Moloney murine leukemia virus and simian immunodeficiency virus, but displays no inhibitory activity against hepatitis C and influenza viruses. This study reports the use of TR-FRET screening to successfully identify a novel capsid inhibitor, ebselen, validating HIV-1 capsid as a promising target for drug development.

Published

2016

7. Correction to Assessment of NR4A Ligands That Directly Bind and Modulate the Orphan Nuclear Receptor Nurr1

Author

Munoz-Tello, Paola, Lin, Hua, Khan, Pasha, de Vera, Ian Mitchelle S., Kamenecka, Theodore M., and Kojetin, Douglas J.

Published

2021

8. Didehydro-Cortistatin A Inhibits HIV-1 by Specifically Binding to the Unstructured Basic Region of Tat

Author

Mediouni, Sonia, Chinthalapudi, Krishna, Ekka, Mary K., Usui, Ippei, Jablonski, Joseph A., Clementz, Mark A., Mousseau, Guillaume, Nowak, Jason, Macherla, Venkat R., Beverage, Jacob N., Esquenazi, Eduardo, Baran, Phil, de Vera, Ian Mitchelle S., Kojetin, Douglas, Loret, Erwann P., Nettles, Kendall, Maiti, Souvik, Izard, Tina, and Valente, Susana T.

Abstract

Tat activates virus production, and limited Tat transactivation correlates with HIV-1 latency. The Tat inhibitor dCA locks HIV in persistent latency. This drug class enables block-and-lock functional cure approaches, aimed at reducing residual viremia during therapy and limiting viral rebound. dCA may also have additional therapeutic benefits since Tat is also neurotoxic. Unfortunately, Tat inhibitors are not clinically available. We generated chemical derivatives and rationalized binding to an active and specific Tat conformer. dCA features required for Tat inhibition are distinct from features needed for inhibition of cyclin-dependent kinase 8 (CDK8), the only other known target of dCA. Furthermore, knockdown of CDK8 did not impact dCA’s activity on HIV-1 transcription. Binding of dCA to Tat’s basic domain altered the local protein environment and rendered Tat more resistant to proteolytic digestion. dCA locks a transient conformer of Tat, blocking functions dependent on its basic domain, namely its ability to amplify viral transcription. Our results define dCA’s mode of action, support structure-based-design strategies targeting Tat, and provide valuable information for drug development around the dCA pharmacophore.

Published

2019