Your search keyword '"Alexandra E Gould"' showing total 22 results

1. Identification of Novel Carbocyclic Pyrimidine Cyclic Dinucleotide STING Agonists for Antitumor Immunotherapy Using Systemic Intravenous Route

Author

Alexandra E. Gould, Courtney Cullis, Lee Hong Myung, David Lok, Rachel E. Gershman, Scott R. Rowland, Miho Mizutani, Dave Janowick, Gipson Krista E, Vihren Kolev, Robert J. Griffin, Joe Conlon, Steve Stroud, Akito Hata, Jeffrey Ciavarri, Dylan Bradley England, Cardin David P, Sandeep Pusalkar, Paul D. Greenspan, Adnan O Abu-Yousif, Jenna Malley, Doanh Mai, Michael Shaw, Ji Zhang, Robert J. Skene, Hu Zhigen, Matthew A. Jones, Atsushi Matsuda, Shih-Chung Huang, Nina Molchanova, Xu Tianlin, Jian Huang, He Xu, Stepan Vyskocil, Nanda Gulavita, Francois Soucy, Gang Li, Yongbo Hu, Liting Ma, Steven P. Langston, Zhan Shi, Christelle C. Renou, Luhua Shen, Sean Harrison, Elise Nunes, Kenneth M. Gigstad, Yosuke Sato, and Hirotake Mizutani

Subjects

Transplantation, Heterologous, Inflammation, 01 natural sciences, Phosphates, Mice, Structure-Activity Relationship, 03 medical and health sciences, Cell Line, Tumor, Neoplasms, Drug Discovery, medicine, Animals, Humans, 030304 developmental biology, 0303 health sciences, Tumor microenvironment, Binding Sites, Innate immune system, Chemistry, Membrane Proteins, Type I interferon production, Acquired immune system, eye diseases, Rats, 0104 chemical sciences, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, Sting, Pyrimidines, Stimulator of interferon genes, Cancer research, Molecular Medicine, Administration, Intravenous, Cytokine secretion, Immunotherapy, Nucleotides, Cyclic, medicine.symptom, Half-Life

Abstract

Stimulator of Interferon Genes (STING) plays an important role in innate immunity by inducing type I interferon production upon infection with intracellular pathogens. STING activation can promote increased T-cell activation and inflammation in the tumor microenvironment, resulting in antitumor immunity. Natural and synthetic cyclic dinucleotides (CDNs) are known to activate STING, and several synthetic CDN molecules are being investigated in the clinic using an intratumoral administration route. Here, we describe the identification of STING agonist 15a, a cyclic dinucleotide structurally diversified from natural ligands with optimized properties for systemic intravenous (iv) administration. Our studies have shown that STING activation by 15a leads to an acute innate immune response as measured by cytokine secretion and adaptive immune response via activation of CD8+ cytotoxic T-cells, which ultimately provides robust antitumor efficacy.

Published

2021

2. Design of proteasome inhibitors with oral efficacy in vivo against Plasmodium falciparum and selectivity over the human proteasome

Author

Benigno F. Crespo-Fernandez, Eric Hanssen, Elizabeth A. Winzeler, Ioanna Deni, Lawrence Cohen, Du Yawei, Daniel C. Barry, Leann Tilley, Riley D. Metcalfe, David L. Gillett, Kurt E. Ward, Bei-Ching Chuang, Hirotake Mizutani, Lawrence R. Dick, Anna Caroline Campos Aguiar, David A. Fidock, Kirsten K. Hanson, Boyin Liu, Alexandra E. Gould, Stanley C. Xie, Rafael Victorio Carvalho Guido, Francisco-Javier Gamo, Tanya Puhalovich, Shih-Chung Huang, Daniel Ferguson, Paul Hales, Con Dogovski, Sabine Ottilie, Nimisha Mittal, Craig J. Morton, Sergio Wittlin, Robert J. Griffin, Delphine Baud, Tomas Yeo, Michael D. W. Griffin, Jake Baum, Stephen Brand, Alisje Churchyard, Jeffrey Ciavarri, and Michael W. Parker

Subjects

0303 health sciences, Multidisciplinary, biology, 010405 organic chemistry, Chemistry, Bortezomib, Plasmodium vivax, Active site, Plasmodium falciparum, QUÍMICA MÉDICA, Pharmacology, biology.organism_classification, 01 natural sciences, 3. Good health, 0104 chemical sciences, 03 medical and health sciences, Proteasome, In vivo, parasitic diseases, biology.protein, medicine, Potency, Selectivity, 030304 developmental biology, medicine.drug

Abstract

The Plasmodium falciparum proteasome is a potential antimalarial drug target. We have identified a series of amino-amide boronates that are potent and specific inhibitors of the P. falciparum 20S proteasome (Pf20S) beta5 active site and that exhibit fast-acting antimalarial activity. They selectively inhibit the growth of P. falciparum compared with a human cell line and exhibit high potency against field isolates of P. falciparum and Plasmodium vivax They have a low propensity for development of resistance and possess liver stage and transmission-blocking activity. Exemplar compounds, MPI-5 and MPI-13, show potent activity against P. falciparum infections in a SCID mouse model with an oral dosing regimen that is well tolerated. We show that MPI-5 binds more strongly to Pf20S than to human constitutive 20S (Hs20Sc). Comparison of the cryo-electron microscopy (EM) structures of Pf20S and Hs20Sc in complex with MPI-5 and Pf20S in complex with the clinically used anti-cancer agent, bortezomib, reveal differences in binding modes that help to explain the selectivity. Together, this work provides insights into the 20S proteasome in P. falciparum, underpinning the design of potent and selective antimalarial proteasome inhibitors.

Published

2021

3. Discovery and optimization of pyrazolopyrimidine sulfamates as ATG7 inhibitors

Author

Natalie Roy D’Amore, Shih-Chung Huang, Sharmila Adhikari, Dylan England, David Lok, Anna Lublinsky, Jouhara Chouitar, Klaudia Foley, Patrick J. LeRoy, Emily F. Calderwood, Ji Zhang, Alexandra E. Gould, James E. Brownell, Sean J. Harrison, Li-Ting Ma, Yu Yang, and Saurabh Menon

Subjects

Clinical Biochemistry, Pharmaceutical Science, 01 natural sciences, Biochemistry, Autophagy-Related Protein 7, Pyrazolopyrimidine, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Autophagy, Humans, Molecular Biology, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Organic Chemistry, Autophagosome formation, 0104 chemical sciences, Cell biology, 010404 medicinal & biomolecular chemistry, Enzyme, HEK293 Cells, Pyrimidines, chemistry, Cancer cell, Molecular Medicine, Pyrazoles, Sulfonic Acids, Hypoxic stress

Abstract

Autophagy is postulated to be required by cancer cells to survive periods of metabolic and/or hypoxic stress. ATG7 is the E1 enzyme that is required for activation of Ubl conjugation pathways involved in autophagosome formation. This article describes the design and optimization of pyrazolopyrimidine sulfamate compounds as potent and selective inhibitors of ATG7. Cellular levels of the autophagy markers, LC3B and NBR1, are regulated following treatment with these compounds.

Published

2020

4. Optimization of tetrahydronaphthalene inhibitors of Raf with selectivity over hERG

Author

Mi-Sook Kim, Mansoureh Rezaei, Jouhara Chouitar, Katherine Brewer, Michael D. Smith, Alexandra E. Gould, Katherine Galvin, Shih-Chung Huang, Dong Mei Zhang, Sharmila Adhikari, Hirotake Mizutani, Steven P. Langston, Dylan England, Paul D. Greenspan, Emily F. Calderwood, Craig Fisher, Sean J. Harrison, Li-Ting Ma, Saurabh Menon, Roushan Afroze, and Jeffery Gaulin

Subjects

Male, Proto-Oncogene Proteins B-raf, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Tetrahydronaphthalenes, Stereochemistry, Transplantation, Heterologous, Clinical Biochemistry, hERG, Pharmaceutical Science, Ether, Biochemistry, Rats, Sprague-Dawley, Inhibitory Concentration 50, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, In vivo, Cell Line, Tumor, Neoplasms, Amide, Drug Discovery, Animals, Humans, Structure–activity relationship, cardiovascular diseases, Protein Kinase Inhibitors, Molecular Biology, biology, Chemistry, Organic Chemistry, Ether-A-Go-Go Potassium Channels, Potassium channel, Rats, 030104 developmental biology, Mutagenesis, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Selectivity, Protein Binding

Abstract

Investigations of a biaryl ether scaffold identified tetrahydronaphthalene Raf inhibitors with good in vivo activity; however these compounds had affinity toward the hERG potassium channel. Herein we describe our work to eliminate this hERG activity via alteration of the substituents on the benzoic amide functionality. The resulting compounds have improved selectivity against the hERG channel, good pharmacokinetic properties and potently inhibit the Raf pathway in vivo.

Published

2016

5. Histone deacetylase inhibitors derived from 1,2,3,4-tetrahydropyrrolo[1,2-a]pyrazine and related heterocycles selective for the HDAC6 isoform

Author

Cynthia Barrett, Alexandra E. Gould, Janice Chin, Mable Brunson, John Ringeling, Christopher Tsu, R. Scott Rowland, Krista Wager, Kara Hoar, Juan Gutierrez, He Xu, Dylan England, Kris Garcia, Christopher Blackburn, and Kenneth Gigstad

Subjects

Gene isoform, Hydroxamic acid, Pyrazine, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Pharmaceutical Science, HDAC6, Hydroxamic Acids, Biochemistry, Histone Deacetylase Inhibitors, chemistry.chemical_compound, Pyrazines, Drug Discovery, Protein Isoforms, Molecular Medicine, Histone deacetylase, Selectivity, Molecular Biology

Abstract

Acyl derivatives of 4-(aminomethyl)-N-hydroxybenzamide are potent sub-type selective HDAC6 inhibitors. Constrained heterocyclic analogs based on 1,2,3,4-tetrahydropyrrolo[1,2-a]pyrazine show further enhanced HDAC6 selectivity and inhibitory activity in cells. Homology models suggest that the heterocyclic spacer can more effectively access the wider catalytic channel of HDAC6 compared to other HDAC sub-types.

Published

2014

6. Mechanistic Study of Uba5 Enzyme and the Ufm1 Conjugation Pathway

Author

Kara Hoar, Jiejin Chen, Sean J. Harrison, Jingya Ma, James M. Gavin, Neil F. Bence, Wei Chen, Ping Li, Michael Sintchak, Nancy J. Bump, Qing Xu, Lawrence R. Dick, William D. Mallender, Jesse J. Chen, Alexandra E. Gould, Frank Bruzzese, and Yafang Lin

Subjects

Stereochemistry, Ubiquitin-activating enzyme, Adenylate kinase, Ubiquitin-Activating Enzymes, Ubiquitin-conjugating enzyme, Thioester, Biochemistry, Cell Line, Enzyme activator, chemistry.chemical_compound, Adenosine Triphosphate, Catalytic Domain, Humans, Protein Structure, Quaternary, Molecular Biology, Ternary complex, chemistry.chemical_classification, biology, Chemistry, Proteins, Active site, Cell Biology, Enzyme Activation, Models, Chemical, Multiprotein Complexes, Ubiquitin-Conjugating Enzymes, Enzymology, biology.protein, Adenosine triphosphate, Protein Binding

Abstract

E1 enzymes activate ubiquitin or ubiquitin-like proteins (Ubl) via an adenylate intermediate and initiate the enzymatic cascade of Ubl conjugation to target proteins or lipids. Ubiquitin-fold modifier 1 (Ufm1) is activated by the E1 enzyme Uba5, and this pathway is proposed to play an important role in the endoplasmic reticulum (ER) stress response. However, the mechanisms of Ufm1 activation by Uba5 and subsequent transfer to the conjugating enzyme (E2), Ufc1, have not been studied in detail. In this work, we found that Uba5 activated Ufm1 via a two-step mechanism and formed a binary covalent complex of Uba5∼Ufm1 thioester. This feature contrasts with the three-step mechanism and ternary complex formation in ubiquitin-activating enzyme Uba1. Uba5 displayed random ordered binding with Ufm1 and ATP, and its ATP-pyrophosphate (PPi) exchange activity was inhibited by both AMP and PPi. Ufm1 activation and Uba5∼Ufm1 thioester formation were stimulated in the presence of Ufc1. Furthermore, binding of ATP to Uba5∼Ufm1 thioester was required for efficient transfer of Ufm1 from Uba5 to Ufc1 via transthiolation. Consistent with the two-step activation mechanism, the mechanism-based pan-E1 inhibitor, adenosine 5'-sulfamate (ADS), reacted with the Uba5∼Ufm1 thioester and formed a covalent, tight-binding Ufm1-ADS adduct in the active site of Uba5, which prevented further substrate binding or catalysis. ADS was also shown to inhibit the Uba5 conjugation pathway in the HCT116 cells through formation of the Ufm1-ADS adduct. This suggests that further development of more selective Uba5 inhibitors could be useful in interrogating the roles of the Uba5 pathway in cells.

Published

2014

7. Mechanistic Studies on Activation of Ubiquitin and Di-ubiquitin-like Protein, FAT10, by Ubiquitin-like Modifier Activating Enzyme 6, Uba6

Author

Lawrence R. Dick, Hua Liao, Neil Rollins, Xiaofeng Yang, William D. Mallender, Qing Xu, James E. Brownell, James M. Gavin, Jingyang Chen, Alexandra E. Gould, Huay-Keng Loke, Jingya Ma, Trupti Lingaraj, and Benjamin S. Amidon

Subjects

Ubiquitin-activating enzyme, Blotting, Western, Molecular Sequence Data, Ubiquitin-Activating Enzymes, Plasma protein binding, Spodoptera, Biochemistry, Mass Spectrometry, Cell Line, Substrate Specificity, Interferon-gamma, Enzyme activator, Adenosine Triphosphate, Ubiquitin, Animals, Humans, Amino Acid Sequence, Sulfhydryl Compounds, Ubiquitins, Molecular Biology, Ternary complex, Molecular Structure, biology, Tumor Necrosis Factor-alpha, Chemistry, Cell Biology, UBA1, Surface Plasmon Resonance, Adenosine Monophosphate, Ubiquitin ligase, Diphosphates, Enzyme Activation, Kinetics, Enzymology, biology.protein, Protein Binding

Abstract

Uba6 is a homolog of the ubiquitin-activating enzyme, Uba1, and activates two ubiquitin-like proteins (UBLs), ubiquitin and FAT10. In this study, biochemical and biophysical experiments were performed to understand the mechanisms of how Uba6 recognizes two distinct UBLs and catalyzes their activation and transfer. Uba6 is shown to undergo a three-step activation process and form a ternary complex with both UBLs, similar to what has been observed for Uba1. The catalytic mechanism of Uba6 is further supported by inhibition studies using a mechanism-based E1 inhibitor, Compound 1, which forms covalent adducts with both ubiquitin and FAT10. In addition, pre-steady state kinetic analysis revealed that the rates of UBL-adenylate (step 1) and thioester (step 2) formation are similar between ubiquitin and FAT10. However, distinct kinetic behaviors were also observed for ubiquitin and FAT10. FAT10 binds Uba6 with much higher affinity than ubiquitin while demonstrating lower catalytic activity in both ATP-PP(i) exchange and E1-E2 transthiolation assays. Also, Compound 1 is less potent with FAT10 as the UBL compared with ubiquitin in ATP-PP(i) exchange assays, and both a slow rate of covalent adduct formation and weak adduct binding to Uba6 contribute to the diminished potency observed for FAT10. Together with expression level analysis in IM-9 cells, this study sheds light on the potential role of cytokine-induced FAT10 expression in regulating Uba6 pathways.

Published

2012

8. Design and Optimization of Potent and Orally Bioavailable Tetrahydronaphthalene Raf Inhibitors

Author

Emily F. Calderwood, Kathleen Aertgeerts, Michael D. Smith, Dylan Bradley England, Roushan Afroze, Ryan Chau, Stepan Vyskocil, Nancy E. Forsyth, Dong Mei Zhang, Ruth Adams, Stephen G. Stroud, O. P. Veiby, Christelle C. Renou, R. Scott Rowland, Erin Paske, Jane X. Liu, Ming Tregay, Michael D. Sintchak, Juliet A Williams, Shih-Chung Huang, Xu Tianlin, Bheemashankar Kulkarni, Sharmila Adhikari, Yuan Tian, Jason Yano, Christopher Blackburn, Paul D. Greenspan, Cheryl A. Farrer, Matthew O. Duffey, Liting Ma, Mi-Sook Kim, Qin Zhang, Sean Harrison, Hirotake Mizutani, Katherine M. Galvin, Alexandra E. Gould, Johnny J. Yang, Steven P. Langston, Dave Janowick, Natalia Iartchouk, Mansoureh Rezaei, Jeffery Gaulin, Khristofer Garcia, Hongbo Zeng, Ribo Guo, Tricia J. Vos, Jouhara Chouitar, and Saurabh Menon

Subjects

Models, Molecular, Proto-Oncogene Proteins B-raf, Tetrahydronaphthalenes, Mutant, Melanoma, Experimental, Administration, Oral, Biological Availability, Mice, Nude, Antineoplastic Agents, Pharmacology, Crystallography, X-Ray, Mice, Structure-Activity Relationship, Pharmacokinetics, Mouse xenograft, In vivo, Drug Discovery, medicine, Animals, chemistry.chemical_classification, Chemistry, Melanoma, Stereoisomerism, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Bioavailability, Enzyme, Drug Design, Mutation, Molecular Medicine

Abstract

Inhibition of mutant B-Raf signaling, through either direct inhibition of the enzyme or inhibition of MEK, the direct substrate of Raf, has been demonstrated preclinically to inhibit tumor growth. Very recently, treatment of B-Raf mutant melanoma patients with a selective B-Raf inhibitor has resulted in promising preliminary evidence of antitumor activity. This article describes the design and optimization of tetrahydronaphthalene-derived compounds as potent inhibitors of the Raf pathway in vitro and in vivo. These compounds possess good pharmacokinetic properties in rodents and inhibit B-Raf mutant tumor growth in mouse xenograft models.

Published

2011

9. Discovery and optimization of N-acyl and N-aroylpyrazolines as B-Raf kinase inhibitors

Author

Christopher Blackburn, Tricia J. Vos, Jane X. Liu, Masayuki Nagayoshi, Bheemashankar Kulkarni, Juliet A Williams, Saurabh Menon, Alexandra E. Gould, and Matthew O. Duffey

Subjects

Proto-Oncogene Proteins B-raf, chemistry.chemical_classification, Sulfonyl, Pyridines, Stereochemistry, Kinase, Organic Chemistry, Clinical Biochemistry, Mutant, Drug Evaluation, Preclinical, Pharmaceutical Science, Raf kinase, Biochemistry, Recombinant Proteins, High-Throughput Screening Assays, Structure-Activity Relationship, Enzyme, Amino Acid Substitution, chemistry, Drug Discovery, Pyrazoles, Molecular Medicine, Protein Kinase Inhibitors, Molecular Biology

Abstract

A high throughput screen identified N-aroylpyrazoline 1 as a selective inhibitor of the V600E mutant of B-Raf kinase. Parallel synthesis of acyl, aroyl, and sulfonyl derivatives led to the identification of several potent inhibitors in both enzymatic and cellular (pERK) assays such as compound 42.

Published

2010

10. Selective Tolyl Carbon Alkylation Mediated by Imidazoline‐Directed Lithiation

Author

Emily F. Calderwood, Alexandra E. Gould, and Nancy E. Forsyth

Subjects

chemistry.chemical_classification, chemistry, Organic Chemistry, Electrophile, Organic chemistry, Imidazoline receptor, chemistry.chemical_element, Alkylation, Protecting group, Nitrogen, Carbon, Alkyl

Abstract

Imidazoline‐directed lithiation of 2‐o‐tolyl‐4,5‐dihydro‐1H‐imidazole and its subsequent treatment with electrophiles yields C‐alkylated products, without the need for a nitrogen protecting group. A variety of electrophiles were used to install aromatic, heteroaromatic, and alkyl substituted moieties.

Published

2004

11. Novel Small-Molecule Inhibitors of RNA Polymerase III

Author

Deborah R. Wysong, Tony Wood, Patrick R. Errada, Tanya Parkinson, Karen J. McGovern, Ian M. Willis, Ronald K. Blackman, Liping Wu, Alexandra E. Gould, Vala Thoroddsen, Timothy D. Ocain, Daniel Kornitzer, Lawrence R. Dick, Patrick Dorr, Christine E. Bulawa, Jing Pan, and Ziva Weissman

Subjects

Antifungal Agents, Transcription, Genetic, Molecular Sequence Data, RNA-dependent RNA polymerase, Saccharomyces cerevisiae, Biology, Microbiology, RNA polymerase III, chemistry.chemical_compound, RNA, Transfer, Drug Resistance, Fungal, Transcription (biology), RNA polymerase, Candida albicans, Reaction Time, Transcriptional regulation, Humans, Enzyme Inhibitors, Molecular Biology, Cells, Cultured, Dose-Response Relationship, Drug, Sequence Homology, Amino Acid, RNA Polymerase III, RNA, Articles, General Medicine, Processivity, Molecular biology, Molecular Weight, Protein Subunits, Biochemistry, chemistry, Mutation, Transfer RNA

Abstract

A genetic approach utilizing the yeast Saccharomyces cerevisiae was used to identify the target of antifungal compounds. This analysis led to the identification of small molecule inhibitors of RNA polymerase (Pol) III from Saccharomyces cerevisiae . Three lines of evidence show that UK-118005 inhibits cell growth by targeting RNA Pol III in yeast. First, a dominant mutation in the g domain of Rpo31p, the largest subunit of RNA Pol III, confers resistance to the compound. Second, UK-118005 rapidly inhibits tRNA synthesis in wild-type cells but not in UK-118005 resistant mutants. Third, in biochemical assays, UK-118005 inhibits tRNA gene transcription in vitro by the wild-type but not the mutant Pol III enzyme. By testing analogs of UK-118005 in a template-specific RNA Pol III transcription assay, an inhibitor with significantly higher potency, ML-60218, was identified. Further examination showed that both compounds are broad-spectrum inhibitors, displaying activity against RNA Pol III transcription systems derived from Candida albicans and human cells. The identification of these inhibitors demonstrates that RNA Pol III can be targeted by small synthetic molecules.

Published

2003

12. Potent histone deacetylase inhibitors derived from 4-(aminomethyl)-N-hydroxybenzamide with high selectivity for the HDAC6 isoform

Author

R. Scott Rowland, Juan A Gutierrez, Alexandra E. Gould, John Ringeling, Chris Tsu, Christopher Blackburn, Chrissie Lynch, Kenneth M. Gigstad, Sean Harrison, Janice Chin, He Xu, Kris Garcia, Kara Hoar, and Cynthia Barrett

Subjects

Gene isoform, biology, Chemistry, Stereochemistry, High selectivity, Active site, HDAC6, Histone Deacetylase 6, Hydroxamic Acids, Histone Deacetylases, Substrate Specificity, Histone Deacetylase Inhibitors, Biochemistry, Drug Discovery, Benzamides, biology.protein, Molecular Medicine, Substrate specificity, Humans, Histone deacetylase, Surface protein, Selectivity

Abstract

A screen for HDAC6 inhibitors identified acyl derivatives of 4-(aminomethyl)-N-hydroxybenzamide as potent leads with unexpected selectivity over the other subtypes. We designed and synthesized constrained heterocyclic analogues such as tetrahydroisoquinolines that show further enhanced HDAC6 selectivity and inhibitory activity in cellular assays. Selectivity may be attributed to the benzylic spacer more effectively accessing the wider channel of HDAC6 compared to other HDAC subtypes as well as hydrophobic capping groups interacting with the protein surface near the rim of the active site.

Published

2013

13. (+)-Trienomycins A, B, C, and F and (+)-Mycotrienins I and II: Relative and Absolute Stereochemistry

Author

Joseph Barbosa, Satoshi Ōmura, John L. Wood, and Kanki Komiyama, Alexandra E. Gould, W. Wong, Amos B. Smith, Iii,†, and Carmelo J. Rizzo

Subjects

Antifungal, Colloid and Surface Chemistry, medicine.drug_class, Stereochemistry, Chemistry, medicine, Ansamycin Antibiotics, General Chemistry, Biochemistry, Catalysis

Abstract

The complete relative and absolute stereochemistries have been elucidated for the ansamycin antibiotics (+)-trienomycins A, B, and C and their potent antifungal congeners, the (+)-mycotrienins I and II. A new species, (+)-trienomycin F, has also been isolated and characterized. In addition, an end-game synthetic strategy for the trienomycins and mycotrienins has been developed.

Published

1996

14. ChemInform Abstract: (+)-Trienomycins A, B, and C: Relative and Absolute Stereochemistry

Author

John L. Wood, Amos B. Smith, Shinji Funayama, W. Wong, Carmelo J. Rizzo, Satoshi Omura, and Alexandra E. Gould

Subjects

Absolute (philosophy), Chemistry, Stereochemistry, General Medicine

Published

2010

15. ChemInform Abstract: (+)-Trienomycins A (Ia), B (Ib), C (Ic), and F (Id) and (+)- Mycotrienins I (II) and II (Ie): Relative and Absolute Stereochemistry

Author

J. Barbosa, Amos B. Smith, Kanki Komiyama, Alexandra E. Gould, John L. Wood, Carmelo J. Rizzo, S. Omura, and W. Wong

Subjects

Chemistry, Stereochemistry, General Medicine

Published

2010

16. ChemInform Abstract: Highly Selective Hydrolytic Kinetic Resolution of Terminal Epoxides Catalyzed by Chiral (Salen)CoIII Complexes. Practical Synthesis of Enantioenriched Terminal Epoxides and 1,2-Diols

Author

Bridget D. Brandes, Jay F. Larrow, Makoto Tokunaga, Alexandra E. Gould, Michael E. Furrow, Karl B. Hansen, Eric N. Jacobsen, and Scott E. Schaus

Subjects

Steric effects, chemistry.chemical_compound, Hydrolysis, Chemistry, Epoxide, General Medicine, Highly selective, Selectivity, Enantiomeric excess, Combinatorial chemistry, Kinetic resolution, Catalysis

Abstract

The hydrolytic kinetic resolution (HKR) of terminal epoxides catalyzed by chiral (salen)CoIII complex 1·OAc affords both recovered unreacted epoxide and 1,2-diol product in highly enantioenriched form. As such, the HKR provides general access to useful, highly enantioenriched chiral building blocks that are otherwise difficult to access, from inexpensive racemic materials. The reaction has several appealing features from a practical standpoint, including the use of H2O as a reactant and low loadings (0.2−2.0 mol %) of a recyclable, commercially available catalyst. In addition, the HKR displays extraordinary scope, as a wide assortment of sterically and electronically varied epoxides can be resolved to ≥99% ee. The corresponding 1,2-diols were produced in good-to-high enantiomeric excess using 0.45 equiv of H2O. Useful and general protocols are provided for the isolation of highly enantioenriched epoxides and diols, as well as for catalyst recovery and recycling. Selectivity factors (krel) were determined ...

Published

2010

17. Discovery and optimization of pyrazoline compounds as B-Raf inhibitors

Author

Paul D. Greenspan, Susan Chen, Liting Ma, Jane X. Liu, Johnny J. Yang, Qin Zhang, Ruth Adams, Shih-Chung Huang, Bheemashankar Kulkarni, Ryan W. Chau, Masayuki Nagayoshi, Matthew O. Duffey, Shaoxia Yu, Christopher Blackburn, Khristofer Garcia, Katherine M. Galvin, Tricia J. Vos, Sean Harrison, R. Scott Rowland, Xu Tianlin, Steven P. Langston, Mi-Sook Kim, Saurabh Menon, and Alexandra E. Gould

Subjects

Proto-Oncogene Proteins B-raf, Stereochemistry, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Pyrazoline, Pyrazoline derivatives, Non-specific serine/threonine protein kinase, Biochemistry, Chemical synthesis, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Computer Simulation, Molecular Biology, Protein Kinase Inhibitors, chemistry.chemical_classification, Binding Sites, biology, Organic Chemistry, Chemical modification, Thiophene derivatives, Recombinant Proteins, Enzyme, chemistry, Amino Acid Substitution, Enzyme inhibitor, biology.protein, Molecular Medicine, Pyrazoles

Abstract

The discovery of novel pyrazoline derivatives as B-Raf (V600E) inhibitors is described in this report. Chemical modification of the pyrazoline scaffold led to the development of SAR and identified potent and selective inhibitors of B-Raf (V600E). Determination of the pharmacokinetic properties of selected inhibitors is also reported.

Published

2010

18. Selective Tolyl Carbon Alkylation Mediated by Imidazoline-Directed Lithiation

Author

Nancy E. Forsyth, Alexandra E. Gould, and Emily F. Calderwood

Subjects

chemistry.chemical_classification, chemistry, Electrophile, Imidazoline receptor, chemistry.chemical_element, Organic chemistry, General Medicine, Alkylation, Protecting group, Carbon, Alkyl

Abstract

Imidazoline‐directed lithiation of 2‐o‐tolyl‐4,5‐dihydro‐1H‐imidazole and its subsequent treatment with electrophiles yields C‐alkylated products, without the need for a nitrogen protecting group. A variety of electrophiles were used to install aromatic, heteroaromatic, and alkyl substituted moieties.

Published

2005

19. Highly selective hydrolytic kinetic resolution of terminal epoxides catalyzed by chiral (salen)Co(III) complexes. Practical synthesis of enantioenriched terminal epoxides and 1,2-diols

Author

Bridget D. Brandes, Eric N. Jacobsen, Scott E. Schaus, Jay F. Larrow, Alexandra E. Gould, Karl B. Hansen, Makoto Tokunaga, and Michael E. Furrow

Subjects

Steric effects, Reaction mechanism, Hydrolysis, Epoxide, Stereoisomerism, General Chemistry, Cobalt, Ethylenediamines, Biochemistry, Catalysis, Kinetic resolution, Substrate Specificity, chemistry.chemical_compound, Kinetics, Colloid and Surface Chemistry, chemistry, Alcohols, Organic chemistry, Epoxy Compounds, Enantiomeric excess, Selectivity, Chelating Agents

Abstract

The hydrolytic kinetic resolution (HKR) of terminal epoxides catalyzed by chiral (salen)Co(III) complex 1 x OAc affords both recovered unreacted epoxide and 1,2-diol product in highly enantioenriched form. As such, the HKR provides general access to useful, highly enantioenriched chiral building blocks that are otherwise difficult to access, from inexpensive racemic materials. The reaction has several appealing features from a practical standpoint, including the use of H(2)O as a reactant and low loadings (0.2-2.0 mol %) of a recyclable, commercially available catalyst. In addition, the HKR displays extraordinary scope, as a wide assortment of sterically and electronically varied epoxides can be resolved toor = 99% ee. The corresponding 1,2-diols were produced in good-to-high enantiomeric excess using 0.45 equiv of H(2)O. Useful and general protocols are provided for the isolation of highly enantioenriched epoxides and diols, as well as for catalyst recovery and recycling. Selectivity factors (k(rel)) were determined for the HKR reactions by measuring the product ee at ca. 20% conversion. In nearly all cases, k(rel) values for the HKR exceed 50, and in several cases are well in excess of 200.

Published

2002

20. Substrate-Based Design of the First Class of Angiotensin-Converting Enzyme-Related Carboxypeptidase (ACE2) Inhibitors

Author

Timothy D. Ocain, Alexandra E. Gould, Natalie A. Dales, James Brown, Emily F. Calderwood, James M. Gavin, Charles A. Minor, Bing Guan, Chad S Vickers, Virendar K. Kaushik, Paul Hales, Michael A. Patane, Peter J. Tummino, and Michael Stewart

Subjects

Stereochemistry, Angiotensin-Converting Enzyme Inhibitors, Carboxypeptidases, Peptidyl-Dipeptidase A, Biochemistry, Catalysis, Carboxypeptidase activity, Structure-Activity Relationship, Colloid and Surface Chemistry, Glutamate carboxypeptidase II, Structure–activity relationship, chemistry.chemical_classification, biology, Chemistry, Imidazoles, Rational design, Succinates, Angiotensin-converting enzyme, General Chemistry, Carboxypeptidase, Protein Structure, Tertiary, Enzyme, Drug Design, Angiotensin-converting enzyme 2, biology.protein, Angiotensin-Converting Enzyme 2, hormones, hormone substitutes, and hormone antagonists

Abstract

Angiotensin-converting enzyme-related carboxypeptidase (ACE2) is a recently identified zinc metalloprotease with carboxypeptidase activity that was identified using our genomics platform. We implemented a rational design approach to identify potent and selective ACE2 inhibitors. To this end, picomolar inhibitors of ACE2 were designed and synthesized.

Published

2002

21. Intramolecular [4+2] Cycloaddition Reactions of Conjugated Enynes

Author

Alexandra E. Gould, Anna L. Helgason, Rick L. Danheiser, and Roberto Fernández de la Pradilla

Subjects

Intramolecular reaction, Bicyclic molecule, Chemistry, Intramolecular force, Organic Chemistry, Conjugated system, Medicinal chemistry, Cycloaddition

Abstract

The intramolecular [4+2] cycloaddition of conjugated enynes provides an efficient and general route to aromatic and dihydroaromatic compounds

Published

1994

22. (+)-Trienomycins A, B, and C: relative and absolute stereochemistry

Author

Carmelo J. Rizzo, Satoshi Omura, Shinji Funayama, Alexandra E. Gould, John L. Wood, W. Wong, and Amos B. Smith

Subjects

chemistry.chemical_compound, Colloid and Surface Chemistry, Absolute (philosophy), chemistry, Stereochemistry, Lactam, Absolute configuration, General Chemistry, Enantiomer, Biochemistry, Catalysis, Cyclophane

Published

1990