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5. Structural basis of intron selection by U2 snRNP in the presence of covalent inhibitors.

Author

Cretu, Constantin, Gee, Patricia, Liu, Xiang, Agrawal, Anant, Nguyen, Tuong-Vi, Ghosh, Arun K, Cook, Andrew, Jurica, Melissa, Larsen, Nicholas A, and Pena, Vladimir

Subjects
Spliceosomes, Humans, Lactones, Pyrans, Pyrones, Spiro Compounds, Ribonucleoprotein, U2 Small Nuclear, DNA, Cryoelectron Microscopy, Crystallography, X-Ray, Nucleic Acid Conformation, Protein Conformation, Protein Binding, Introns, Models, Molecular
Abstract

Intron selection during the formation of prespliceosomes is a critical event in pre-mRNA splicing. Chemical modulation of intron selection has emerged as a route for cancer therapy. Splicing modulators alter the splicing patterns in cells by binding to the U2 snRNP (small nuclear ribonucleoprotein)-a complex chaperoning the selection of branch and 3' splice sites. Here we report crystal structures of the SF3B module of the U2 snRNP in complex with spliceostatin and sudemycin FR901464 analogs, and the cryo-electron microscopy structure of a cross-exon prespliceosome-like complex arrested with spliceostatin A. The structures reveal how modulators inactivate the branch site in a sequence-dependent manner and stall an E-to-A prespliceosome intermediate by covalent coupling to a nucleophilic zinc finger belonging to the SF3B subunit PHF5A. These findings support a mechanism of intron recognition by the U2 snRNP as a toehold-mediated strand invasion and advance an unanticipated drug targeting concept.

Published
2021

6. Spliceostatins and Derivatives: Chemical Syntheses and Biological Properties of Potent Splicing Inhibitors

Author

Ghosh, Arun K, Mishevich, Jennifer L, and Jurica, Melissa S

Subjects
Cancer, Underpinning research, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, 1.3 Chemical and physical sciences, Generic health relevance, Antineoplastic Agents, Biological Products, Humans, Molecular Structure, Pyrans, RNA Splicing, Spliceosomes, Chemical Sciences, Biological Sciences, Medical and Health Sciences, Medicinal & Biomolecular Chemistry
Abstract

Spliceostatins and thailanstatins are intriguing natural products due to their structural features as well as their biological significance. This family of natural products has been the subject of immense synthetic interest because they exhibit very potent cytotoxicity in representative human cancer cell lines. The cytotoxic properties of these natural products are related to their ability to inhibit spliceosomes. FR901564 and spliceostatins have been shown to inhibit spliceosomes by binding to their SF3B component. Structurally, these natural products contain two highly functionalized tetrahydropyran rings with multiple stereogenic centers joined by a diene moiety and an acyclic side chain linked with an amide bond. Total syntheses of this family of natural products led to the development of useful synthetic strategies, which enabled the synthesis of potent derivatives. The spliceosome modulating properties of spliceostatins and synthetic derivatives opened the door for understanding the underlying spliceosome mechanism as well as the development of new therapies based upon small-molecule splicing modulators. This review outlines the total synthesis of spliceostatins, synthetic studies of structural derivatives, and their bioactivity.

Published
2021

7. Herboxidiene Features That Mediate Conformation-Dependent SF3B1 Interactions to Inhibit Splicing

Author

Lopez, Adriana Gamboa, Allu, Srinivasa Rao, Mendez, Patricia, Reddy, Guddeti Chandrashekar, Maul-Newby, Hannah M, Ghosh, Arun K, and Jurica, Melissa S

Subjects
Medicinal and Biomolecular Chemistry, Chemical Sciences, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Adenosine Triphosphate, Base Sequence, Binding Sites, Fatty Alcohols, HeLa Cells, Humans, Models, Molecular, Phosphoproteins, Protein Binding, Protein Conformation, Pyrans, RNA Splicing, RNA Splicing Factors, RNA, Messenger, Ribonucleoprotein, U2 Small Nuclear, Spliceosomes, Structure-Activity Relationship, Temperature, Hela Cells, Biological Sciences, Organic Chemistry, Biological sciences, Chemical sciences
Abstract

Small molecules that target the spliceosome SF3B complex are potent inhibitors of cancer cell growth. The compounds affect an early stage of spliceosome assembly when U2 snRNP first engages the branch point sequence of an intron. Employing an inactive herboxidiene analog (iHB) as a competitor, we investigated factors that influence inhibitor interactions with SF3B to interfere with pre-mRNA splicing in vitro. Order-of-addition experiments show that inhibitor interactions are long lasting and affected by both temperature and the presence of ATP. Our data are also consistent with the model that not all SF3B conformations observed in structural studies are conducive to productive inhibitor interactions. Notably, SF3B inhibitors do not impact an ATP-dependent rearrangement in U2 snRNP that exposes the branch binding sequence for base pairing. We also report extended structure-activity relationship analysis of the splicing inhibitor herboxidiene. We identified features of the tetrahydropyran ring that mediate its interactions with SF3B and its ability to interfere with splicing. In the context of recent structures of SF3B bound to inhibitor, our results lead us to extend the model for early spliceosome assembly and inhibitor mechanism. We postulate that interactions between a carboxylic acid substituent of herboxidiene and positively charged SF3B1 side chains in the inhibitor binding channel are needed to maintain inhibitor occupancy while counteracting the SF3B transition to a closed state that is required for stable U2 snRNP interactions with the intron.

Published
2021

8. Design and synthesis of herboxidiene derivatives that potently inhibit in vitro splicing

Author

Ghosh, Arun K, Allu, Srinivasa Rao, Reddy, Guddeti Chandrashekar, Lopez, Adriana Gamboa, Mendez, Patricia, and Jurica, Melissa S

Subjects
Antineoplastic Agents, Fatty Alcohols, HeLa Cells, Humans, Pyrans, RNA Splicing, Spliceosomes, Stereoisomerism, Hela Cells, Medicinal and Biomolecular Chemistry, Organic Chemistry
Abstract

Herboxidiene is a potent antitumor agent that targets the SF3B subunit of the spliceosome. Herboxidiene possesses a complex structural architecture with nine stereocenters and design of potent less complex structures would be of interest as a drug lead as well as a tool for studying SF3B1 function in splicing. We investigated a number of C-6 modified herboxidiene derivatives in an effort to eliminate this stereocenter and, also to understand the importance of this functionality. The syntheses of structural variants involved a Suzuki-Miyaura cross-coupling reaction as the key step. The functionalized tetrahydrofuran core has been constructed from commercially available optically active tri-O-acetyl-d-glucal. We investigated the effect of these derivatives on splicing chemistry. The C-6 alkene derivative showed very potent splicing inhibitory activity similar to herboxidiene. Furthermore, the C-6 gem-dimethyl derivative also exhibited very potent in vitro splicing inhibitory activity comparable to herboxidiene.

Published
2021

9. U2 snRNA structure is influenced by SF3A and SF3B proteins but not by SF3B inhibitors

Author

Urabe, Veronica K, Stevers, Meredith, Ghosh, Arun K, and Jurica, Melissa S

Subjects
Biochemistry and Cell Biology, Biological Sciences, Generic health relevance, HeLa Cells, Humans, Nucleic Acid Conformation, Protein Structure, Secondary, Protein Subunits, RNA, Small Nuclear, Ribonucleoprotein, U2 Small Nuclear, Spliceosomes, Hela Cells, General Science & Technology
Abstract

U2 snRNP is an essential component of the spliceosome. It is responsible for branch point recognition in the spliceosome A-complex via base-pairing of U2 snRNA with an intron to form the branch helix. Small molecule inhibitors target the SF3B component of the U2 snRNP and interfere with A-complex formation during spliceosome assembly. We previously found that the first SF3B inhibited-complex is less stable than A-complex and hypothesized that SF3B inhibitors interfere with U2 snRNA secondary structure changes required to form the branch helix. Using RNA chemical modifiers, we probed U2 snRNA structure in A-complex and SF3B inhibited splicing complexes. The reactivity pattern for U2 snRNA in the SF3B inhibited-complex is indistinguishable from that of A-complex, suggesting that they have the same secondary structure conformation, including the branch helix. This observation suggests SF3B inhibited-complex instability does not stem from an alternate RNA conformation and instead points to the inhibitors interfering with protein component interactions that normally stabilize U2 snRNP's association with an intron. In addition, we probed U2 snRNA in the free U2 snRNP in the presence of SF3B inhibitor and again saw no differences. However, increased protection of nucleotides upstream of Stem I in the absence of SF3A and SF3B proteins suggests a change of secondary structure at the very 5' end of U2 snRNA. Chemical probing of synthetic U2 snRNA in the absence of proteins results in similar protections and predicts a previously uncharacterized extension of Stem I. Because this stem must be disrupted for SF3A and SF3B proteins to stably join the snRNP, the structure has the potential to influence snRNP assembly and recycling after spliceosome disassembly.

Published
2021

11. Fluorescent Probes for Monitoring Serine Ubiquitination

Author

Puvar, Kedar, Saleh, Aya M, Curtis, Ryan W, Zhou, Yiyang, Nyalapatla, Prasanth R, Fu, Jiaqi, Rovira, Alexander R, Tor, Yitzhak, Luo, Zhao-Qing, Ghosh, Arun K, Wirth, Mary J, Chmielewski, Jean, Kinzer-Ursem, Tamara L, and Das, Chittaranjan

Subjects
5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Adenosine Diphosphate, Amino Acid Motifs, Bacterial Proteins, Biochemistry, Fluorescent Dyes, Legionella pneumophila, NAD, Serine, Ubiquitination, Medicinal and Biomolecular Chemistry, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology
Abstract

In a radical departure from the classical E1-E2-E3 three-enzyme mediated ubiquitination of eukaryotes, the recently described bacterial enzymes of the SidE family of Legionella pneumophila effectors utilize NAD+ to ligate ubiquitin onto target substrate proteins. This outcome is achieved via a two-step mechanism involving (1) ADP ribosylation of ubiquitin followed by (2) phosphotransfer to a target serine residue. Here, using fluorescent NAD+ analogues as well as synthetic substrate mimics, we have developed continuous assays enabling real-time monitoring of both steps of this mechanism. These assays are amenable to biochemical studies and high-throughput screening of inhibitors of these effectors, and the discovery and characterization of putative enzymes similar to members of the SidE family in other organisms. We also show their utility in studying enzymes that can reverse and inhibit this post-translational modification.

Published
2020

15. Enantioselective Synthesis of a Cyclopropane Derivative of Spliceostatin A and Evaluation of Bioactivity

Author

Ghosh, Arun K, Reddy, Guddeti Chandrashekar, Kovela, Satish, Relitti, Nicola, Urabe, Veronica K, Prichard, Beth E, and Jurica, Melissa S

Subjects
Cancer, Antineoplastic Agents, Cyclopropanes, HeLa Cells, Humans, Molecular Structure, Pyrans, Spiro Compounds, Stereoisomerism, Hela Cells, Chemical Sciences, Organic Chemistry
Abstract

Spliceostatin A is a potent inhibitor of spliceosomes and exhibits excellent anticancer activity against multiple human cancer cell lines. We describe here the design and synthesis of a stable cyclopropane derivative of spliceostatin A. The synthesis involved a cross-metathesis or a Suzuki cross-coupling reaction as the key step. The functionalized epoxy alcohol ring was constructed from commercially available optically active tri- O-acetyl-d-glucal. The biological properties of the cyclopropyl derivative revealed that it is active in human cells and inhibits splicing in vitro comparable to spliceostatin A.

Published
2018

16. Enantioselective Synthesis of Thailanstatin A Methyl Ester and Evaluation of in Vitro Splicing Inhibition

Author

Ghosh, Arun K, Veitschegger, Anne M, Nie, Shenyou, Relitti, Nicola, MacRae, Andrew J, and Jurica, Melissa S

Subjects
Medicinal and Biomolecular Chemistry, Organic Chemistry, Chemical Sciences, Chemistry Techniques, Synthetic, Esters, Pyrans, RNA Splicing, Stereoisomerism, Medicinal and biomolecular chemistry, Organic chemistry
Abstract

Thailanstatin A has been isolated recently from the fermentation broth of B. thailandensis MSMB43. We describe here an enantioselective convergent synthesis of thailanstatin A methyl ester and evaluation of its splicing activity. Synthesis of both highly functionalized tetrahydropyran rings were carried out from commercially available tri- O-acetyl-d-glucal as the key starting material. Our convergent synthesis involved the synthesis of both tetrahydropyran fragments in a highly stereoselective manner. The fragments were then coupled using cross-metathesis as the key step. The synthesis of the diene subunit included a highly stereoselective Claisen rearrangement, a Cu(I)-mediated conjugate addition of MeLi to set the C-14 methyl stereochemistry, a reductive amination reaction to install the C16-amine functionality, and a Wittig olefination reaction to incorporate the diene unit. The epoxy alcohol subunit was synthesized by a highly selective anomeric allylation, a Peterson olefination, and a vanadium catalyzed epoxidation that installed the epoxide stereoselectively. Cross-metathesis of the olefins provided the methyl ester derivative of thailanstatin A. We have carried out in vitro splicing studies of the methyl ester derivative, which proved to be a potent inhibitor of the spliceosome.

Published
2018

17. Enantioselective Synthesis of Spliceostatin G and Evaluation of Bioactivity of Spliceostatin G and Its Methyl Ester

Author

Ghosh, Arun K, Reddy, Guddeti Chandrashekar, MacRae, Andrew J, and Jurica, Melissa S

Subjects
Organic Chemistry, Chemical Sciences, Amination, Esters, Molecular Structure, RNA Splicing, Spiro Compounds, Stereoisomerism, Chemical sciences
Abstract

An enantioselective total synthesis of spliceostatin G has been accomplished. The synthesis involved a Suzuki cross-coupling reaction as a key step. The functionalized tetrahydropyran ring was constructed from commercially available optically active tri-O-acetyl-d-glucal. Other key reactions include a highly stereoselective Claisen rearrangement, a Cu(I)-mediated 1,4 addition of MeLi to install the C8 methyl group, and a reductive amination to incorporate the C10 amine functionality of spliceostatin G. Biological evaluation of synthetic spliceostatin G and its methyl ester revealed that it does not inhibit splicing in vitro.

Published
2018

20. Control of biofilm formation by an Agrobacterium tumefaciens pterin-binding periplasmic protein conserved among diverse Proteobacteria.

Author

Greenwich, Jennifer L., Eagan, Justin L., Feirer, Nathan, Boswinkle, Kaleb, Minasov, George, Shuvalova, Ludmilla, Inniss, Nicole L., Raghavaiah, Jakka, Ghosh, Arun K., Satchell, Karla J. F., Allen, Kylie D., and Fuqua, Clay

Subjects
AGROBACTERIUM tumefaciens, BIOFILMS, PROTEOBACTERIA, BICYCLIC compounds, PROTEINS
Abstract

Biofilm formation and surface attachment in multiple Alphaproteobacteria is driven by unipolar polysaccharide (UPP) adhesins. The pathogen Agrobacterium tumefaciens produces a UPP adhesin, which is regulated by the intracellular second messenger cyclic diguanylate monophosphate (c-di-GMP). Prior studies revealed that DcpA, a diguanylate cyclase-phosphodiesterase, is crucial in control of UPP production and surface attachment. DcpA is regulated by PruR, a protein with distant similarity to enzymatic domains known to coordinate the molybdopterin cofactor (MoCo). Pterins are bicyclic nitrogen-rich compounds, several of which are produced via a nonessential branch of the folate biosynthesis pathway, distinct from MoCo. The pterin-binding protein PruR controls DcpA activity, fostering c-di-GMP breakdown and dampening its synthesis. Pterins are excreted, and we report here that PruR associates with these metabolites in the periplasm, promoting interaction with the DcpA periplasmic domain. The pteridine reductase PruA, which reduces specific dihydro-pterin molecules to their tetrahydro forms, imparts control over DcpA activity through PruR. Tetrahydromonapterin preferentially associates with PruR relative to other related pterins, and the PruR-DcpA interaction is decreased in a pruA mutant. PruR and DcpA are encoded in an operon with wide conservation among diverse Proteobacteria including mammalian pathogens. Crystal structures reveal that PruR and several orthologs adopt a conserved fold, with a pterin-specific binding cleft that coordinates the bicyclic pterin ring. These findings define a pterin-responsive regulatory mechanism that controls biofilm formation and related c-di-GMP-dependent phenotypes in A. tumefaciens and potentially acts more widely in multiple proteobacterial lineages. [ABSTRACT FROM AUTHOR]

Published
2024
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22. Design, synthesis and in vitro splicing inhibition of desmethyl and carba-derivatives of herboxidiene

Author

Ghosh, Arun K, Lv, Kai, Ma, Nianchun, Cárdenas, Emilio L, Effenberger, Kerstin A, and Jurica, Melissa S

Subjects
Organic Chemistry, Chemical Sciences, Cancer, Boronic Acids, Chemistry Techniques, Synthetic, Drug Design, Fatty Alcohols, Inhibitory Concentration 50, Pyrans, RNA Splicing, Stereoisomerism, Medicinal and Biomolecular Chemistry, Medicinal and biomolecular chemistry, Organic chemistry
Abstract

Herboxidiene is a potent inhibitor of spliceosomes. It exhibits excellent anticancer activity against multiple human cancer cell lines. Herein, we describe an enantioselective synthesis of a desmethyl derivative and the corresponding carba-derivatives of herboxidiene. The synthesis involved Suzuki coupling of a vinyl iodide with boronate as the key reaction. For the synthesis of carba-derivatives, the corresponding optically active cyclohexane-1,3-dicarbonyl derivatives were synthesized using an enantioselective desymmetrization of meso-anhydride. The biological properties of these derivatives were evaluated in an in vitro splicing assay.

Published
2016

23. Interchangeable SF3B1 inhibitors interfere with pre-mRNA splicing at multiple stages

Author

Effenberger, Kerstin A, Urabe, Veronica K, Prichard, Beth E, Ghosh, Arun K, and Jurica, Melissa S

Subjects
Biochemistry and Cell Biology, Biological Sciences, Cancer, Genetics, Underpinning research, 1.1 Normal biological development and functioning, Adenosine Triphosphate, Binding Sites, Exons, Humans, Phosphoproteins, RNA Precursors, RNA Splicing, RNA Splicing Factors, RNA, Messenger, Ribonucleoprotein, U2 Small Nuclear, SF3B1, spliceosome, pre-mRNA splicing, inhibitor, Developmental Biology, Biochemistry and cell biology
Abstract

The protein SF3B1 is a core component of the spliceosome, the large ribonucleoprotein complex responsible for pre-mRNA splicing. Interest in SF3B1 intensified when tumor exome sequencing revealed frequent specific SF3B1 mutations in a variety of neoplasia and when SF3B1 was identified as the target of three different cancer cell growth inhibitors. A better mechanistic understanding of SF3B1's role in splicing is required to capitalize on these discoveries. Using the inhibitor compounds, we probed SF3B1 function in the spliceosome in an in vitro splicing system. Formerly, the inhibitors were shown to block early steps of spliceosome assembly, consistent with a previously determined role of SF3B1 in intron recognition. We now report that SF3B1 inhibitors also interfere with later events in the spliceosome cycle, including exon ligation. These observations are consistent with a requirement for SF3B1 throughout the splicing process. Additional experiments aimed at understanding how three structurally distinct molecules produce nearly identical effects on splicing revealed that inactive analogs of each compound interchangeably compete with the active inhibitors to restore splicing. The competition indicates that all three types of compounds interact with the same site on SF3B1 and likely interfere with its function by the same mechanism, supporting a shared pharmacophore model. It also suggests that SF3B1 inhibition does not result from binding alone, but is consistent with a model in which the compounds affect a conformational change in the protein. Together, our studies reveal new mechanistic insight into SF3B1 as a principal player in the spliceosome and as a target of inhibitor compounds.

Published
2016

24. A small molecule compound with an indole moiety inhibits the main protease of SARS-CoV-2 and blocks virus replication

Author

Hattori, Shin-ichiro, Higashi-Kuwata, Nobuyo, Hayashi, Hironori, Allu, Srinivasa Rao, Raghavaiah, Jakka, Bulut, Haydar, Das, Debananda, Anson, Brandon J., Lendy, Emma K., Takamatsu, Yuki, Takamune, Nobutoki, Kishimoto, Naoki, Murayama, Kazutaka, Hasegawa, Kazuya, Li, Mi, Davis, David A., Kodama, Eiichi N., Yarchoan, Robert, Wlodawer, Alexander, Misumi, Shogo, Mesecar, Andrew D., Ghosh, Arun K., and Mitsuya, Hiroaki

Published
2021
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25. Enantioselective Synthesis of Spliceostatin E and Evaluation of Biological Activity

Author

Ghosh, Arun K, Veitschegger, Anne M, Sheri, Venkata Reddy, Effenberger, Kerstin A, Prichard, Beth E, and Jurica, Melissa S

Subjects
Antineoplastic Agents, Drug Screening Assays, Antitumor, HeLa Cells, Humans, Lactones, Molecular Structure, Pyrans, Pyrones, Spiro Compounds, Stereoisomerism, Hela Cells, Chemical Sciences, Organic Chemistry
Abstract

An enantioselective total synthesis of spliceostatin E has been accomplished. The δ-lactone unit A was constructed from readily available (R)-glycidyl alcohol using a ring-closing olefin metathesis as the key reaction. A cross-metathesis of ring A containing δ-lactone and the functionalized tetrahydropyran B-ring provided spliceostatin E. Our biological evaluation of synthetic spliceostatin E revealed that it does not inhibit splicing in vitro and does not impact speckle morphology in cells. Spliceostatin E was reported to possess potent antitumor activity.

Published
2014

27. Enantioselective Total Syntheses of FR901464 and Spliceostatin A and Evaluation of Splicing Activity of Key Derivatives

Author

Ghosh, Arun K, Chen, Zhi-Hua, Effenberger, Kerstin A, and Jurica, Melissa S

Subjects
Medicinal and Biomolecular Chemistry, Organic Chemistry, Chemical Sciences, Cancer, Alkenes, Catalysis, Cell Line, Tumor, Humans, Molecular Structure, Pyrans, RNA Splicing, Spiro Compounds, Stereoisomerism, Medicinal and biomolecular chemistry, Organic chemistry
Abstract

FR901464 (1) and spliceostatin A (2) are potent inhibitors of spliceosomes. These compounds have shown remarkable anticancer activity against multiple human cancer cell lines. Herein, we describe efficient, enantioselective syntheses of FR901464, spliceostatin A, six corresponding diastereomers and an evaluation of their splicing activity. Syntheses of spliceostatin A and FR901464 were carried out in the longest linear sequence of 9 and 10 steps, respectively. To construct the highly functionalized tetrahydropyran A-ring, we utilized CBS reduction, Achmatowicz rearrangement, Michael addition, and reductive amination as key steps. The remarkable diastereoselectivity of the Michael addition was specifically demonstrated with different substrates under various reaction conditions. The side chain B was prepared from an optically active alcohol, followed by acetylation and hydrogenation over Lindlar's catalyst. The other densely functionalized tetrahydropyran C-ring was derived from readily available (R)-isopropylidene glyceraldehyde through a route featuring 1,2-addition, cyclic ketalization, and regioselective epoxidation. These fragments were coupled together at a late stage through amidation and cross-metathesis in a convergent manner. Six key diastereomers were then synthesized to probe the importance of specific stereochemical features of FR901464 and spliceostatin A, with respect to their in vitro splicing activity.

Published
2014

28. Total Synthesis of GEX1Q1, Assignment of C‑5 Stereoconfiguration and Evaluation of Spliceosome Inhibitory Activity

Author

Ghosh, Arun K, Ma, Nianchun, Effenberger, Kerstin A, and Jurica, Melissa S

Subjects
Cycloaddition Reaction, Fatty Alcohols, Macrolides, Molecular Structure, Pyrans, Spliceosomes, Stereoisomerism, Chemical Sciences, Organic Chemistry
Abstract

An enantioselective total synthesis of GEX1Q1 has been accomplished in a convergent manner. The C-5 asymmetric center has now been assigned through synthesis. GEX1Q1 displayed slightly better spliceosome inhibitory activity over its C-5 epimer. The salient features of this synthesis include an asymmetric hetero-Diels-Alder reaction to construct the tetrahydropyran ring and a Suzuki cross-coupling to assemble the key segments.

Published
2014

29. Coherence between Cellular Responses and in Vitro Splicing Inhibition for the Anti-tumor Drug Pladienolide B and Its Analogs* * This work was supported, in whole or in part, by National Institutes of Health Grants R01CA136762 (to M. S. J.) and 1S10RR022455. This work was also supported by the University of California Cancer Research Coordinating Committee, the California Institute for Quantitative Biosciences (QB3), and the United States Department of State. This article contains supplemental materials.

Author

Effenberger, Kerstin A, Anderson, David D, Bray, Walter M, Prichard, Beth E, Ma, Nianchun, Adams, Matthew S, Ghosh, Arun K, and Jurica, Melissa S

Subjects
Medicinal and Biomolecular Chemistry, Chemical Sciences, Cancer, Antineoplastic Agents, Epoxy Compounds, HeLa Cells, Humans, Macrolides, Neoplasm Proteins, Neoplasms, Phosphoproteins, Pyrans, RNA Splicing, RNA Splicing Factors, Ribonucleoprotein, U2 Small Nuclear, Spiro Compounds, Alternative Splicing, Drug Action, Enzyme Inhibitors, Nucleus, Hela Cells, Biological Sciences, Medical and Health Sciences, Biochemistry & Molecular Biology, Biological sciences, Biomedical and clinical sciences, Chemical sciences
Abstract

Pladienolide B (PB) is a potent cancer cell growth inhibitor that targets the SF3B1 subunit of the spliceosome. There is considerable interest in the compound as a potential chemotherapeutic, as well as a tool to study SF3B1 function in splicing and cancer development. The molecular structure of PB, a bacterial natural product, contains a 12-member macrolide ring with an extended epoxide-containing side chain. Using a novel concise enantioselective synthesis, we created a series of PB structural analogs and the structurally related compound herboxidiene. We show that two methyl groups in the PB side chain, as well as a feature of the macrolide ring shared with herboxidiene, are required for splicing inhibition in vitro. Unexpectedly, we find that the epoxy group contributes only modestly to PB potency and is not absolutely necessary for activity. The orientations of at least two chiral centers off the macrolide ring have no effect on PB activity. Importantly, the ability of analogs to inhibit splicing in vitro directly correlated with their effects in a series of cellular assays. Those effects likely arise from inhibition of some, but not all, endogenous splicing events in cells, as previously reported for the structurally distinct SF3B1 inhibitor spliceostatin A. Together, our data support the idea that the impact of PB on cells is derived from its ability to impair the function of SF3B1 in splicing and also demonstrate that simplification of the PB scaffold is feasible.

Published
2014

30. Control of Biofilm Formation by anAgrobacterium tumefaciensPterin-Binding Periplasmic Protein Conserved Among Pathogenic Bacteria

Author

Greenwich, Jennifer L., primary, Eagan, Justin L., additional, Feirer, Nathan, additional, Boswinkle, Kaleb, additional, Minasov, George, additional, Shuvalova, Ludmilla, additional, Inniss, Nicole L., additional, Raghavaiah, Jakka, additional, Ghosh, Arun K., additional, Satchell, Karla J.F., additional, Allen, Kylie D., additional, and Fuqua, Clay, additional

Published
2023
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33. The Design, Development, and Evaluation of BACE1 Inhibitors for the Treatment of Alzheimer’s Disease

Author

Ghosh, Arun K., Cárdenas, Emilio L., Osswald, Heather L., Bernstein, Peter R., Series editor, Georg, Gunda I., Series editor, Keller, Thomas, Series editor, Lowe, John A., Series editor, Meanwell, Nicholas A., Series editor, Saxena, Anil Kumar, Series editor, Stilz, Ulrich, Series editor, Supuran, Claudiu T., Series editor, Zhang, Ao, Series editor, and Wolfe, Michael S., editor

Published
2017
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39. Delineation of the G Protein-Coupled Receptor Kinase Phosphorylation Sites Within the D1 Dopamine Receptor and Their Role in Regulating Receptor Function

Author

Madaras, Nora S., primary, Rankin, Michele L., additional, Free, R. Benjamin, additional, Haider, Raphael, additional, Drube, Julia, additional, Ghosh, Arun K., additional, Tesmer, John JG., additional, Hoffmann, Carsten, additional, Sibley, David R., additional, and Moritz, Amy E., additional

Published
2023
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