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1. Estradiol improves behavior in FAD transgenic mice that express APOE3 but not APOE4 after ovariectomy

Author

Deebika Balu, Ana C. Valencia-Olvera, Ashwini Deshpande, Saharsh Narayanam, Sravya Konasani, Shreya Pattisapu, Jason M. York, Gregory R. J. Thatcher, Mary Jo LaDu, and Leon M. Tai

Subjects
Alzheimer’s disease, ApoE4, female risk, transgenic mice, amyloid-beta, Diseases of the endocrine glands. Clinical endocrinology, RC648-665
Abstract

Increasing evidence suggests that female individuals have a higher Alzheimer’s disease (AD) risk associated with post-menopausal loss of circulating estradiol (E2). However, clinical data are conflicting on whether E2 lowers AD risk. One potential contributing factor is APOE. The greatest genetic risk factor for AD is APOE4, a factor that is pronounced in female individuals post-menopause. Clinical data suggests that APOE impacts the response of AD patients to E2 replacement therapy. However, whether APOE4 prevents, is neutral, or promotes any positive effects of E2 is unclear. Therefore, our goal was to determine whether APOE modulates the impact of E2 on behavior and AD pathology in vivo. To that end, mice that express human APOE3 (E3FAD) or APOE4 (E4FAD) and overproduce Aβ42 were ovariectomized at either 4 months (early) or 8 months (late) and treated with vehicle or E2 for 4 months. In E3FAD mice, we found that E2 mitigated the detrimental effect of ovariectomy on memory, with no effect on Aβ in the early paradigm and only improved learning in the late paradigm. Although E2 lowered Aβ in E4FAD mice in the early paradigm, there was no impact on learning or memory, possibly due to higher Aβ pathology compared to E3FAD mice. In the late paradigm, there was no effect on learning/memory and Aβ pathology in E4FAD mice. Collectively, these data support the idea that, in the presence of Aβ pathology, APOE impacts the response to E2 supplementation post-menopause.

Published
2024
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2. Non-covalent inhibitors of thioredoxin glutathione reductase with schistosomicidal activity in vivo

Author

Valentina Z. Petukhova, Sammy Y. Aboagye, Matteo Ardini, Rachel P. Lullo, Francesca Fata, Margaret E. Byrne, Federica Gabriele, Lucy M. Martin, Luke N. M. Harding, Vamshikrishna Gone, Bikash Dangi, Daniel D. Lantvit, Dejan Nikolic, Rodolfo Ippoliti, Grégory Effantin, Wai Li Ling, Jeremy J. Johnson, Gregory R. J. Thatcher, Francesco Angelucci, David L. Williams, and Pavel A. Petukhov

Subjects
Science
Abstract

Abstract Only praziquantel is available for treating schistosomiasis, a disease affecting more than 200 million people. Praziquantel-resistant worms have been selected for in the lab and low cure rates from mass drug administration programs suggest that resistance is evolving in the field. Thioredoxin glutathione reductase (TGR) is essential for schistosome survival and a validated drug target. TGR inhibitors identified to date are irreversible and/or covalent inhibitors with unacceptable off-target effects. In this work, we identify noncovalent TGR inhibitors with efficacy against schistosome infections in mice, meeting the criteria for lead progression indicated by WHO. Comparisons with previous in vivo studies with praziquantel suggests that these inhibitors outperform the drug of choice for schistosomiasis against juvenile worms.

Published
2023
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3. Systemic Candesartan Treatment Modulates Behavior, Synaptic Protein Levels, and Neuroinflammation in Female Mice That Express Human APOE4

Author

Sarah B. Scheinman, Steve Zaldua, Adedoyin Dada, Kateryna Krochmaliuk, Katherine Dye, Felecia M. Marottoli, Gregory R. J. Thatcher, and Leon M. Tai

Subjects
angiotensin receptor blocker, ApoE4, female sex, memory, inflammation, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Evidence suggests that angiotensin receptor blockers (ARBs) could be beneficial for Alzheimer’s disease (AD) patients independent of any effects on hypertension. However, studies in rodent models directly testing the activity of ARB treatment on behavior and AD-relevent pathology including neuroinflammation, Aβ levels, and cerebrovascular function, have produced mixed results. APOE4 is a major genetic risk factor for AD and has been linked to many of the same functions as those purported to be modulated by ARB treatment. Therefore, evaluating the effects of ARB treatment on behavior and AD-relevant pathology in mice that express human APOE4 could provide important information on whether to further develop ARBs for AD therapy. In this study, we treated female and male mice that express the human APOE4 gene in the absence (E4FAD−) or presence (E4FAD+) of high Aβ levels with the ARB prodrug candesartan cilexetil for a duration of 4 months. Compared to vehicle, candesartan treatment resulted in greater memory-relevant behavior and higher hippocampal presynaptic protein levels in female, but not male, E4FAD− and E4FAD+ mice. The beneficial effects of candesartan in female E4FAD− and E4FAD+ mice occurred in tandem with lower GFAP and Iba1 levels in the hippocampus, whereas there were no effects on markers of cerebrovascular function and Aβ levels. Collectively, these data imply that the effects of ARBs on AD-relevant pathology may be modulated in part by the interaction between APOE genotype and biological sex. Thus, the further development of ARBs could provide therapeutic options for targeting neuroinflammation in female APOE4 carriers.

Published
2021
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4. Structure–Activity Relationships and Transcriptomic Analysis of Hypoxia-Inducible Factor Prolyl Hydroxylase Inhibitors

Author

Andrey A. Poloznikov, Sergey V. Nikulin, Dmitry M. Hushpulian, Anna Yu. Khristichenko, Andrey I. Osipyants, Andrey F. Asachenko, Olga V. Shurupova, Svyatoslav S. Savin, Sue H. Lee, Irina N. Gaisina, Gregory R. J. Thatcher, Anthony Narciso, Eric P. Chang, Sergey V. Kazakov, Nancy Krucher, Vladimir I. Tishkov, Bobby Thomas, and Irina G. Gazaryan

Subjects
transcription factor, hypoxia, iron chelation, 2-oxoglutarate dioxygenase, adaptaquin, neuradapt, Therapeutics. Pharmacology, RM1-950
Abstract

To evaluate the differences in action of commercially available 2-oxoglutarate mimetics and “branched-tail” oxyquinoline inhibitors of hypoxia-inducible factor prolyl hydroxylase (HIF PHD), the inhibitors’ IC50 values in the activation of HIF1 ODD-luciferase reporter were selected for comparative transcriptomics. Structure–activity relationship and computer modeling for the oxyquinoline series of inhibitors led to the identification of novel inhibitors, which were an order of magnitude more active in the reporter assay than roxadustat and vadadustat. Unexpectedly, 2-methyl-substitution in the oxyquinoline core of the best HIF PHD inhibitor was found to be active in the reporter assay and almost equally effective in the pretreatment paradigm of the oxygen-glucose deprivation in vitro model. Comparative transcriptomic analysis of the signaling pathways induced by HIF PHD inhibitors showed high potency of the two novel oxyquinoline inhibitors (#4896-3249 and #5704-0720) at 2 μM concentrations matching the effect of 30 μM roxadustat and 500 μM dimethyl oxalyl glycine in inducing HIF1 and HIF2-linked pathways. The two oxyquinoline inhibitors exerted the same activation of HIF-triggered glycolytic pathways but opposite effects on signaling pathways linked to alternative substrates of HIF PHD 1 and 3, such as p53, NF-κB, and ATF4. This finding can be interpreted as the specificity of the 2-methyl-substitute variant for HIF PHD2.

Published
2022
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8. Inhibition of ACAT as a Therapeutic Target for Alzheimer’s Disease Is Independent of ApoE4 Lipidation

Author

Ana C. Valencia-Olvera, Deebika Balu, Naomi Faulk, Aspasia Amiridis, Yueting Wang, Christine Pham, Eva Avila-Munoz, Jason M. York, Gregory R. J. Thatcher, and Mary Jo LaDu

Subjects
Pharmacology, Pharmacology (medical), Neurology (clinical)
Abstract

APOE4, encoding apolipoprotein E4 (apoE4), is the greatest genetic risk factor for Alzheimer’s disease (AD), compared to the common APOE3. While the mechanism(s) underlying APOE4-induced AD risk remains unclear, increasing the lipidation of apoE4 is an important therapeutic target as apoE4-lipoproteins are poorly lipidated compared to apoE3-lipoproteins. ACAT (acyl-CoA: cholesterol-acyltransferase) catalyzes the formation of intracellular cholesteryl-ester droplets, reducing the intracellular free cholesterol (FC) pool. Thus, inhibiting ACAT increases the FC pool and facilitates lipid secretion to extracellular apoE-containing lipoproteins. Previous studies using commercial ACAT inhibitors, including avasimibe (AVAS), as well as ACAT-knock out (KO) mice, exhibit reduced AD-like pathology and amyloid precursor protein (APP) processing in familial AD (FAD)-transgenic (Tg) mice. However, the effects of AVAS with human apoE4 remain unknown. In vitro, AVAS induced apoE efflux at concentrations of AVAS measured in the brains of treated mice. AVAS treatment of male E4FAD-Tg mice (5xFAD+/-APOE4+/+) at 6–8 months had no effect on plasma cholesterol levels or distribution, the original mechanism for AVAS treatment of CVD. In the CNS, AVAS reduced intracellular lipid droplets, indirectly demonstrating target engagement. Surrogate efficacy was demonstrated by an increase in Morris water maze measures of memory and postsynaptic protein levels. Amyloid-beta peptide (Aβ) solubility/deposition and neuroinflammation were reduced, critical components of APOE4-modulated pathology. However, there was no increase in apoE4 levels or apoE4 lipidation, while amyloidogenic and non-amyloidogenic processing of APP were significantly reduced. This suggests that the AVAS-induced reduction in Aβ via reduced APP processing was sufficient to reduce AD pathology, as apoE4-lipoproteins remained poorly lipidated.

Published
2023

9. Effect of a brain‐penetrant selective estrogen receptor degrader ( <scp>SERD</scp> ) on binge drinking in female mice

Author

Hu Chen, Yunlong Lu, Rui Xiong, Carlo I. Rosales, Cassandre Coles, Kana Hamada, Nuria Asad, Gregory R. J. Thatcher, and Amy W. Lasek

Subjects
Male, Sucrose, Alcohol Drinking, Ethanol, Ventral Tegmental Area, Medicine (miscellaneous), Toxicology, Binge Drinking, Mice, Inbred C57BL, Mice, Psychiatry and Mental health, Receptors, Estrogen, Animals, Humans, Female
Abstract

Greater circulating levels of the steroid hormone 17β-estradiol (E2) are associated with higher levels of binge drinking in women. In female mice, estrogen receptors in the ventral tegmental area, a dopaminergic region of the brain involved in the motivation to consume ethanol, regulate binge-like ethanol intake. We recently developed a brain-penetrant selective estrogen receptor degrader (SERD), YL3-122, that could be used to test the behavioral role of brain estrogen receptors. We hypothesized that treating female mice with this compound would reduce binge-like ethanol drinking.Female C57BL/6J mice were treated systemically with YL3-122 and a related SERD with low brain penetrance, XR5-27, and tested for binge-like ethanol consumption in the drinking in the dark (DID) test. Mice were also tested for sucrose and water consumption and blood ethanol clearance after treatment with the SERDs. Finally, the effect of ethanol exposure on Esr1 gene expression was measured in the ventral tegmental area (VTA), prefrontal cortex (PFC), and ventral hippocampus (vHPC) of male and female mice by quantitative real-time PCR after 4 DID sessions.YL3-122 reduced ethanol consumption when mice were in diestrus but not estrus. YL3-122 also decreased sucrose consumption but did not alter water intake or blood ethanol clearance. XR5-27 did not affect any of these measures. Binge-like ethanol drinking resulted in increased Esr1 transcript in the VTA of both sexes, male vHPC, and female PFC.These results indicate that SERD treatment can decrease binge-like ethanol drinking in female mice. Thus, it could be a novel strategy to reduce binge drinking in women, with the caveat that effectiveness may depend on menstrual cycle phase. In addition, Esr1 transcript is increased by binge ethanol exposure in both sexes but in a brain region-specific manner.

Published
2022

10. MAP4K4 promotes pancreatic tumorigenesis via phosphorylation and activation of mixed lineage kinase 3

Author

Subhasis Das, Daniel R. Principe, Ajay Rana, Sandeep Kumar, Navin Viswakarma, Piush Srivastava, Paul J. Grippo, Gautam Sondarva, Gregory R. J. Thatcher, Rakesh Sathish Nair, Sunil Kumar Singh, Subhash C. Sinha, and Basabi Rana

Subjects
Threonine, Cancer Research, Programmed cell death, Protein Serine-Threonine Kinases, Biology, medicine.disease_cause, Article, Stress signalling, Mice, Cell Movement, Cell Line, Tumor, Pancreatic cancer, Genetics, medicine, Animals, Humans, Phosphorylation, Kinase activity, Molecular Biology, Cell Proliferation, Mechanism (biology), Intracellular Signaling Peptides and Proteins, Cancer, MAP Kinase Kinase Kinases, medicine.disease, Up-Regulation, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, HEK293 Cells, Disease Progression, Cancer research, Carcinogenesis, Neoplasm Transplantation, Function (biology)
Abstract

MAP4K4 is a Ste20 member and reported to play important roles in various pathologies, including in cancer. However, the mechanism by which MAP4K4 promotes pancreatic cancer is not fully understood. It is suggested that MAP4K4 might function as a cancer promoter via specific downstream target(s) in an organ-specific manner. Here we identified MLK3 as a direct downstream target of MAP4K4. The MAP4K4 and MLK3 associates with each other, and MAP4K4 phosphorylates MLK3 on Thr738 and increases MLK3 kinase activity and downstream signaling. The phosphorylation of MLK3 by MAP4K4 promotes pancreatic cancer cell proliferation, migration, and colony formation. Moreover, MAP4K4 is overexpressed in human pancreatic tumors and directly correlates with the disease progression. The MAP4K4-specific pharmacological inhibitor, GNE-495, impedes pancreatic cancer cell growth, migration, induces cell death, and arrests cell cycle progression. Additionally, the GNE-495 reduced the tumor burden and extended survival of the KPC mice with pancreatic cancer. The MAP4K4 inhibitor also reduced MAP4K4 protein expression, tumor stroma, and induced cell death in murine pancreatic tumors. These findings collectively suggest that MLK3 phosphorylation by MAP4K4 promotes pancreatic cancer, and therefore therapies targeting MAP4K4 might alleviate the pancreatic cancer tumor burden in patients.

Published
2021

11. The mechanism of nicotinamide phosphoribosyltransferase whereby positive allosteric modulation elevates cellular NAD+

Author

Kiira M. Ratia, Zhengnan Shen, Jesse Gordon-Blake, Hyun Lee, Megan S. Laham, Isabella S. Krider, Nicholas Christie, Martha Ackerman-Berrier, Christopher Penton, Natalie G. Knowles, Soumya Reddy Musku, Jiqiang Fu, Ganga Reddy Velma, Rui Xiong, and Gregory R J Thatcher

Abstract

In aging and disease, cellular NAD+is depleted by catabolism to nicotinamide (NAM) and NAD+supple-mentation is being pursued to enhance human healthspan and lifespan. Activation of nicoti namide phosphoribosyl -transferase (NAMPT), the rate-limiting step in NAD+biosynthesis, has potential to increase salvage of NAM. Novel NAMPT positive allosteric modulators (N-PAMs) were discovered in addition to demonstration of NAMPT activati on by biogenic phenols. The mechanism of activation was revealed through synthesis of novel chemical probes, new NAMPT co-crystal structures, and enzyme kinetics. Binding to a rear channel in NAMPT regulates NAM binding and turnover, with biochemical observations being replicated by NAD+measurements in human cells. The mechanism of action of N-PAMs identifies, for the first time, the role of the rear channel in regulation of NAMPT turnover coupled to feedback inhibition by NAM. N-PAM inhibition of low affinity, non-productive NAM binding via the rear channel, causes a right-shif t in KI(NAM) that accompanies an increase in enzyme activity. Conversion of an N-PAM to a high-affinity l igand blocks both high and low affinity NAM binding, ablating enzyme activity. In the presence of an N-PAM, NAMPT boosts NAD+biosynthesis at higher NAM concentrations, in addition to relieving inhibition by NAD+. Since cellular stress often leads to enhanced catabolism of NAD+to NAM, this mechanism is relevant to supporting cellular N AD+levels in aging and disease. The tight regulation of cellular NAMPT is differentially regulated by N-PAMs and other activators, indicating that different classes of pharmacological activators may be engineered for cell and tissue selectivity.

Published
2022

12. Estrogen Receptor Modulators

Author

Gregory R. J. Thatcher, Lauren M. Gutgesell, Kiira Ratia, and Carlo I. Rosales

Subjects
Breast cancer, Nuclear receptor, business.industry, Estrogen, medicine.drug_class, medicine, Cancer research, Endocrine therapy, Estrogen Receptor Modulators, medicine.disease, business
Published
2021

13. Extending the Calpain–Cathepsin Hypothesis to the Neurovasculature: Protection of Brain Endothelial Cells and Mice from Neurotrauma

Author

Oleksii Dubrovskyi, Gregory R. J. Thatcher, Leon M. Tai, Ammar Jastaniah, Rachel C. Knopp, and Irina N. Gaisina

Subjects
Pharmacology, biology, Traumatic brain injury, business.industry, Neurodegeneration, Ischemia, Calpain, medicine.disease, medicine.disease_cause, Neuroprotection, Cathepsin B, medicine, biology.protein, Pharmacology (medical), Vascular dementia, business, Oxidative stress
Abstract

[Image: see text] The calpain–cathepsin hypothesis posits a key role for elevated calpain-1 and cathepsin-B activity in the neurodegeneration underlying neurotrauma and multiple disorders including Alzheimer’s disease (AD). AD clinical trials were recently halted on alicapistat, a selective calpain-1 inhibitor, because of insufficient exposure of neurons to the drug. In contrast to neuroprotection, the ability of calpain-1 and cathepsin-B inhibitors to protect the blood–brain barrier (BBB), is understudied. Since cerebrovascular dysfunction underlies vascular dementia, is caused by ischemic stroke, and is emerging as an early feature in the progression of AD, we studied protection of brain endothelial cells (BECs) by selective and nonselective calpain-1 and cathepsin-B inhibitors. We show these inhibitors protect both neurons and murine BECs from ischemia–reperfusion injury. Cultures of primary BECs from ALDH2(–/–) mice that manifest enhanced oxidative stress were sensitive to ischemia, leading to reduced cell viability and loss of tight junction proteins; this damage was rescued by calpain-1 and cathepsin-B inhibitors. In ALDH2(–/–) mice 24 h after mild traumatic brain injury (mTBI), BBB damage was reflected by significantly increased fluorescein extravasation and perturbation of tight junction proteins, eNOS, MMP-9, and GFAP. Both calpain and cathepsin-B inhibitors alleviated BBB dysfunction caused by mTBI. No clear advantage was shown by selective versus nonselective calpain inhibitors in these studies. The lack of recognition of the ability of calpain inhibitors to protect the BBB may have led to the premature abandonment of this therapeutic approach in AD clinical trials and requires further mechanistic studies of cerebrovascular protection by calpain-1 inhibitors.

Published
2021

14. Rapid Induction of the Unfolded Protein Response and Apoptosis by Estrogen Mimic TTC-352 for the Treatment of Endocrine-Resistant Breast Cancer

Author

Ramona Curpan, Balkees Abderrahman, Yue Chen, Debra A. Tonetti, Rui Xiong, Sean W. Fanning, Jay S. Hanspal, Charles E. Foulds, Ping Fan, Antrix Jain, Anna Malovannaya, Gregory R. J. Thatcher, V. Craig Jordan, Geoffrey L. Greene, and Philipp Y. Maximov

Subjects
X-Box Binding Protein 1, 0301 basic medicine, Cancer Research, Transcription, Genetic, Estrogen receptor, Apoptosis, Ligands, chemistry.chemical_compound, 0302 clinical medicine, Aromatase, biology, Chemistry, DNA, Neoplasm, Gene Expression Regulation, Neoplastic, Receptors, Estrogen, Oncology, 030220 oncology & carcinogenesis, MCF-7 Cells, Thermodynamics, Female, hormones, hormone substitutes, and hormone antagonists, Protein Binding, medicine.drug, Agonist, Cell Survival, medicine.drug_class, Breast Neoplasms, Molecular Dynamics Simulation, Protein Serine-Threonine Kinases, Models, Biological, Partial agonist, Fluorescence, Article, 03 medical and health sciences, Breast cancer, Protein Domains, Endoribonucleases, Biomarkers, Tumor, medicine, Humans, Benzothiazoles, Estrogens, medicine.disease, Hormones, 030104 developmental biology, Estetrol, Drug Resistance, Neoplasm, Estrogen, Unfolded Protein Response, biology.protein, Cancer research, Tamoxifen
Abstract

Patients with long-term estrogen-deprived breast cancer, after resistance to tamoxifen or aromatase inhibitors develops, can experience tumor regression when treated with estrogens. Estrogen's antitumor effect is attributed to apoptosis via the estrogen receptor (ER). Estrogen treatment can have unpleasant gynecologic and nongynecologic adverse events; thus, the development of safer estrogenic agents remains a clinical priority. Here, we study synthetic selective estrogen mimics (SEM) BMI-135 and TTC-352, and the naturally occurring estrogen estetrol (E4), which are proposed as safer estrogenic agents compared with 17β-estradiol (E2), for the treatment of endocrine-resistant breast cancer. TTC-352 and E4 are being evaluated in breast cancer clinical trials. Cell viability assays, real-time PCR, immunoblotting, ERE DNA pulldowns, mass spectrometry, X-ray crystallography, docking and molecular dynamic simulations, live cell imaging, and Annexin V staining were conducted in 11 biologically different breast cancer models. Results were compared with the potent full agonist E2, less potent full agonist E4, the benchmark partial agonist triphenylethylene bisphenol (BPTPE), and antagonists 4-hydroxytamoxifen and endoxifen. We report ERα's regulation and coregulators’ binding profiles with SEMs and E4. We describe TTC-352′s pharmacology as a weak full agonist and antitumor molecular mechanisms. This study highlights TTC-352′s benzothiophene scaffold that yields an H-bond with Glu353, which allows Asp351-to-helix 12 (H12) interaction, sealing ERα's ligand-binding domain, recruiting E2-enriched coactivators, and triggering rapid ERα-induced unfolded protein response (UPR) and apoptosis, as the basis of its anticancer properties. BPTPE's phenolic OH yields an H-Bond with Thr347, which disrupts Asp351-to-H12 interaction, delaying UPR and apoptosis and increasing clonal evolution risk.

Published
2021

15. Novel Pyrrolopyridone Bromodomain and Extra-Terminal Motif (BET) Inhibitors Effective in Endocrine-Resistant ER+ Breast Cancer with Acquired Resistance to Fulvestrant and Palbociclib

Author

Yangfeng Li, Katherine Dye, Fei Huang, Rui Xiong, Zhengnan Shen, Gregory R. J. Thatcher, Lauren M. Gutgesell, Oleksii Dubrovskyi, Jiong Zhao, Debra A. Tonetti, Huiping Zhao, and Kiira Ratia

Subjects
Models, Molecular, BRD4, Pyridines, Pyridones, Estrogen receptor, Breast Neoplasms, Palbociclib, 01 natural sciences, Piperazines, Article, Mice, 03 medical and health sciences, Breast cancer, Protein Domains, Downregulation and upregulation, Drug Discovery, medicine, Animals, Humans, Tissue Distribution, Fulvestrant, 030304 developmental biology, 0303 health sciences, Chemistry, medicine.disease, Xenograft Model Antitumor Assays, 0104 chemical sciences, Bromodomain, 010404 medicinal & biomolecular chemistry, Receptors, Estrogen, Drug Resistance, Neoplasm, MCF-7 Cells, Cancer research, Molecular Medicine, Estrogen receptor alpha, Transcription Factors, medicine.drug
Abstract

Acquired resistance to fulvestrant and palbociclib is a new challenge to treatment of estrogen receptor positive (ER+) breast cancer. ER is expressed in most resistance settings; thus, bromodomain and extra-terminal protein inhibitors (BETi) that target BET-amplified ER-mediated transcription have therapeutic potential. Novel pyrrolopyridone BETi leveraged novel interactions with L92/L94 confirmed by a cocrystal structure of 27 with BRD4. Optimization of BETi using growth inhibition in fulvestrant-resistant (MCF-7:CFR) cells was confirmed in endocrine-resistant, palbociclib-resistant, and ESR1 mutant cell lines. 27 was more potent in MCF-7:CFR cells than six BET inhibitors in clinical trials. Transcriptomic analysis differentiated 27 from the benchmark BETi, JQ-1, showing downregulation of oncogenes and upregulation of tumor suppressors and apoptosis. The therapeutic approach was validated by oral administration of 27 in orthotopic xenografts of endocrine-resistant breast cancer in monotherapy and in combination with fulvestrant. Importantly, at an equivalent dose in rats, thrombocytopenia was mitigated.

Published
2020

16. Mixed lineage kinase 3 inhibition induces T cell activation and cytotoxicity

Author

Rakesh Sathish Nair, Sandeep Kumar, Navin Viswakarma, Rajyasree Emmadi, Basabi Rana, Periannan Sethupathi, Oana Cristina Danciu, Ajay Rana, Sunil Kumar Singh, Gautam Sondarva, Gregory R. J. Thatcher, Subhash C. Sinha, and Kent Hoskins

Subjects
Isomerase activity, Pyridines, T cell, Primary Cell Culture, Breast Neoplasms, Lymphocyte Activation, Mice, Lymphocytes, Tumor-Infiltrating, Immune system, Cell Line, Tumor, medicine, Animals, Humans, Cytotoxic T cell, Pyrroles, Phosphorylation, Cytotoxicity, Protein Kinase Inhibitors, Multidisciplinary, NFATC Transcription Factors, biology, Chemistry, Mammary Neoplasms, Experimental, CD28, Biological Sciences, MAP Kinase Kinase Kinases, Cell biology, medicine.anatomical_structure, Granzyme, biology.protein, Female, Tumor Escape, Cyclophilin A, CD8, T-Lymphocytes, Cytotoxic
Abstract

Mixed lineage kinase 3 (MLK3), also known as MAP3K11, was initially identified in a megakaryocytic cell line and is an emerging therapeutic target in cancer, yet its role in immune cells is not known. Here, we report that loss or pharmacological inhibition of MLK3 promotes activation and cytotoxicity of T cells. MLK3 is abundantly expressed in T cells, and its loss alters serum chemokines, cytokines, and CD28 protein expression on T cells and its subsets. MLK3 loss or pharmacological inhibition induces activation of T cells in in vitro, ex vivo, and in vivo conditions, irrespective of T cell activating agents. Conversely, overexpression of MLK3 decreases T cell activation. Mechanistically, loss or inhibition of MLK3 down-regulates expression of a prolyl-isomerase, Ppia, which is directly phosphorylated by MLK3 to increase its isomerase activity. Moreover, MLK3 also phosphorylates nuclear factor of activated T cells 1 (NFATc1) and regulates its nuclear translocation via interaction with Ppia, and this regulates T cell effector function. In an immune-competent mouse model of breast cancer, MLK3 inhibitor increases Granzyme B-positive CD8(+) T cells and decreases MLK3 and Ppia gene expression in tumor-infiltrating T cells. Likewise, the MLK3 inhibitor in pan T cells, isolated from breast cancer patients, also increases cytotoxic CD8(+) T cells. These results collectively demonstrate that MLK3 plays an important role in T cell biology, and targeting MLK3 could serve as a potential therapeutic intervention via increasing T cell cytotoxicity in cancer.

Published
2020

17. Optimization of 4-Aminopiperidines as Inhibitors of Influenza A Viral Entry That Are Synergistic with Oseltamivir

Author

Lijun Rong, Gregory R. J. Thatcher, Kevin Furlong, Norton P. Peet, Han Cheng, Ruikun Du, Balaji Manicassamy, Irina N. Gaisina, Qinghua Cui, Michael Caffrey, and Ping Li

Subjects
Oseltamivir, viruses, Hemagglutinins, Viral, Microbial Sensitivity Tests, Antiviral Agents, 01 natural sciences, Article, Madin Darby Canine Kidney Cells, Small Molecule Libraries, Seasonal influenza, Mice, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Influenza A Virus, H1N1 Subtype, Piperidines, Viral entry, Drug Discovery, Animals, Humans, 030304 developmental biology, 0303 health sciences, Binding Sites, Influenza A Virus, H5N1 Subtype, Molecular Structure, Chemistry, virus diseases, Drug Synergism, Influenza a, Virus Internalization, Virology, 0104 chemical sciences, Molecular Docking Simulation, Vaccination, 010404 medicinal & biomolecular chemistry, Microsomes, Liver, Molecular Medicine, Protein Binding
Abstract

Vaccination is the most prevalent prophylactic means for controlling seasonal influenza infections. However, an effective vaccine usually takes at least 6 months to develop for the circulating strains. Therefore, new therapeutic options are needed for the acute treatment of influenza infections to control this virus and prevent epidemics/pandemics from developing. We have discovered fast-acting, orally bioavailable acylated 4-aminopiperidines with an effective mechanism of action targeting viral hemagglutinin (HA). Our data show that these compounds are potent entry inhibitors of influenza A viruses. We present docking studies that suggest an HA binding site for these inhibitors on H5N1. Compound 16 displayed a significant decrease of viral titer when evaluated in the infectious assays with influenza virus H1N1 (A/Puerto Rico/8/1934) or H5N1 (A/Vietnam/1203/2004) strains and the oseltamivir-resistant strain with the most common H274Y mutation. In addition, compound 16 showed significant synergistic activity with oseltamivir in vitro.

Published
2020

18. Abstract P5-11-06: Phase 1 study of TTC-352 in patients with metastatic breast cancer progressing on endocrine therapy

Author

Robert P. Venuti, Jonathan Bleeker, Jasgit C. Sachdev, Debra A. Tonetti, Ruth O'Regan, Gregory R. J. Thatcher, Randolph Hurley, and Arkadiusz Z. Dudek

Subjects
Cancer Research, medicine.medical_specialty, Side effect, business.industry, Breast pain, Cancer, medicine.disease, Gastroenterology, Metastatic breast cancer, Breast cancer, Oncology, Tolerability, Internal medicine, medicine, medicine.symptom, business, Adverse effect, Progressive disease
Abstract

Background: TTC-352 is a selective human ER partial agonist (ShERPA) developed for treatment of ER+ breast cancer (BC). ShERPAs mimic the effects of estradiol (E2) in hormone-independent, endocrine-resistant BC cells, but since it has only partial agonist activity in ER+ cells, it could have an improved side effect profile. Thus, TTC-352 could be a promising option for endocrine-resistant BC. Methods: This is an open-label, accelerated dose escalation study with primary endpoint of maximum tolerated dose (MTD) that is evaluating up to five dose levels of TTC-352 in patients with ER+ endocrine-resistant metastatic BC (NCT03201913). The MTD of TTC-352 is determined using initial single-patient cohort escalations until grade 2 toxicity, then expansion to a modified-Fibonacci dose-escalation 3+3 design. The secondary objectives are: best response (BR), progression-free survival, overall survival, treatment tolerability, and pharmacokinetics (PK) of TTC-352. Patient population: patients with metastatic ER+ BC who received and progressed on at least two lines of endocrine therapy, with one that included a CDK4/CDK6 inhibitor, and with adequate hepatic, renal, and bone marrow function at screening. Results: This study completed enrollment of a total of 15 patients on June 5, 2019. Dose LevelTTC-352 Dose Level (mg)Number of SubjectsTwice-Daily (BID) DoseTotal Daily Dose115302230601360120141202401518036010 No dose limiting toxicity has been seen to date with any of the tested dose levels. There was one treatment-related grade 3 event of asymptomatic pulmonary embolism (30mg BID). The number and percentage (n, %) of patients with treatment-related grade 1 and grade 2 adverse events reported in two or more patients across all dose levels were diarrhea (9, 60), hot flush (4, 26), headache (3, 20), nausea (3, 20), abdominal pain (3, 20), rash (3, 20), blurred vision (2, 13) vomiting (2, 13), dizziness (2, 13), peripheral neuropathy (2, 13), breast pain (2, 13), uterine/vaginal hemorrhage (2, 13) and vaginal discharge (2, 13). BR in the 7 evaluable patients (patients with at least two 28-day cycles of treatment) showed that 3 patients had stable disease (SD) for 4, and 10 months, respectively; 1 patient continues study treatment with SD after 9 months; and 4 patients had progressive disease (PD) after completing two cycles of treatment. All 5 non-evaluable patients had PD prior to completing two cycles of treatment. PK: The intra- and inter-individual variability for AUC0-∞ hampered assessment of the relationship between dose and AUC0-∞., Half-life was 7.6-14.3 hrs. Trough TTC-352 plasma concentrations at steady-state (SS) remained well above the plasma concentrations associated with efficacy in animal models. PKC alpha expression in tumor tissue did not correlate with length of disease control with TTC-352 therapy, though the numbers are small and not all of the available specimens were metastatic. Conclusions: TTC 352 demonstrates manageable safety and early clinical evidence of antitumor activity in patients with BC progressing on endocrine therapy. Based upon SS TTC-352 plasma concentrations and tolerability, the 180mg BID dose is recommended for further testing. Citation Format: Ruth O'Regan, Randolph Hurley, Jasgit Sachdev, Jonathan Bleeker, Debra Tonetti, Gregory Thatcher, Robert Venuti, Arkadiusz Dudek. Phase 1 study of TTC-352 in patients with metastatic breast cancer progressing on endocrine therapy [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P5-11-06.

Published
2020

19. Dual Inhibition of Cathepsin L and 3CL-Pro by GC-376 Constrains SARS Cov2 Infection Including Omicron Variant

Author

Prabhakaran Kumar, Kiira M Ratia, Justin M Richner, Gregory R J Thatcher, Rashmi Kadam, Sandra P Smieszek, Bartlomiej P Przychodzen, Vuk Koprivica, Gunther Birznieks, Mihael H Polymeropoulos, and Bellur S Prabhakar

Abstract

Recurrent waves of SARS CoV2 infections remain a major global health concern. Emergence of highly infectious variants with reduced sensitivity to neutralization by vaccines and monoclonal antibodies (mAb) necessitates a deeper understanding of factors involved in SARS CoV2 infections and identification of drug candidates to halt infection. Here, we determined the primacy of endosomal protease cathepsin-L in mediating SARS CoV2 entry and screened a library of well-annotated bioactive compounds for potent cathepsin-L inhibitory activity. Whilst the potent cathepsin-L inhibitors were capable of inhibiting SARS CoV2 entry and cytopathic effect (CPE) in less susceptible cell lines such as human ACE2 expressing 293T cells, these drugs failed to inhibit SARS CoV2 in highly susceptible cell lines such as human TMPRSS2 or human-ACE2-TMPRSS2 overexpressing Vero E6 cells. Only drugs with dual inhibitory effect on both host cathepsin-L and virus 3CL-Protease enzymes such as Z-FA-FMK and GC-376 were capable of inhibiting prototypic (USA-WA1/2020, Lineage A) SARS CoV2 induced CPE in highly susceptible cell lines. Moreover, these drugs inhibited delta (Lineage-B.1.617.2) and omicron (Lineage-B.1.1.529) infection with equal potency showing that the newer mutations harbored in these variants did not affect the mechanism of action of these drugs such as cathepsin-L or 3CL-Pro inhibition. Moreover, our early evidence that 3CL-Pro inhibition can effectively inhibit omicron-induced CPE in highly susceptible cell lines suggests that the recently FDA-approved oral drug, a 3CL-Pro inhibitor which is a combination of nirmatrelvir/ritonavir (Paxlovid) could be effective against omicron variant which shows reduced sensitivity to vaccines and mAb.ImportanceWe report that cathepsin-L and 3CL-Pro as major targets for designing antivirals against SARS CoV2. Dual inhibition of cathepsin-L and 3CL-Pro by GC-376 renders it effective in inhibiting SARS CoV2-induced cytopathic effect in highly susceptible cell lines. Moreover, this candidate drug is equally effective against prototypic SARS CoV2 lineage A and emerging variants such as delta and omicron which show reduced sensitivity to vaccines and monoclonal antibodies. Given the recent wave of SARS CoV2 omicron variant infection around the world, and 3CL-Pro inhibitor nirmatrelvir is one of the components of the FDA-approved Paxlovid, our findings are timely, important and should be of broad interest.

Published
2022

20. Design of SARS-CoV-2 PLpro Inhibitors for COVID-19 Antiviral Therapy Leveraging Binding Cooperativity

Author

Saad Alqarni, Lijun Rong, Yangfeng Li, Hyun Lee, Fei Huang, Youngjin Kwon, Rui Xiong, Zhengnan Shen, Deyu Kong, Oleksii Dubrovskyi, Laura Cooper, Kiira Ratia, and Gregory R. J. Thatcher

Subjects
Models, Molecular, Proteases, medicine.medical_treatment, Coronavirus Papain-Like Proteases, Cooperativity, Microbial Sensitivity Tests, Cysteine Proteinase Inhibitors, Crystallography, X-Ray, Antiviral Agents, Article, Ubiquitin, Drug Discovery, medicine, Tumor Cells, Cultured, Humans, Binding site, Pandemics, Protease, Binding Sites, biology, Chemistry, COVID-19, Surface Plasmon Resonance, Cell biology, COVID-19 Drug Treatment, Viral replication, biology.protein, Microsomes, Liver, Molecular Medicine, Cysteine, Deubiquitination
Abstract

Antiviral agents blocking SARS-CoV-2 viral replication are desperately needed to complement vaccination to end the COVID-19 pandemic. Viral replication and assembly are entirely dependent on two viral cysteine proteases: 3C-like protease (3CLpro) and the papain-like protease (PLpro). PLpro also has deubiquitinase (DUB) activity, removing ubiquitin (Ub) and Ub-like modifications from host proteins, disrupting the host immune response. 3CLpro is inhibited by many known cysteine protease inhibitors, whereas PLpro is a relatively unusual cysteine protease, being resistant to blockade by such inhibitors. A high-throughput screen of biased and unbiased libraries gave a low hit rate, identifying only CPI-169 and the positive control, GRL0617, as inhibitors with good potency (IC50 < 10 lower case Greek μM). Analogues of both inhibitors were designed to develop structure-activity relationships; however, without a co-crystal structure of the CPI-169 series, we focused on GRL0617 as a starting point for structure-based drug design, obtaining several co-crystal structures to guide optimization. A series of novel 2-phenylthiophene-based non-covalent SARS-CoV-2 PLpro inhibitors were obtained, culminating in low nanomolar potency. The high potency and slow inhibitor off-rate were rationalized by newly identified ligand interactions with a 'BL2 groove' that is distal from the active site cysteine. Trapping of the conformationally flexible BL2 loop by these inhibitors blocks binding of viral and host protein substrates; however, until now it has not been demonstrated that this mechanism can induce potent and efficacious antiviral activity. In this study, we report that novel PLpro inhibitors have excellent antiviral efficacy and potency against infectious SARS-CoV-2 replication in cell cultures. Together, our data provide structural insights into the design of potent PLpro inhibitors and the first validation that non-covalent inhibitors of SARS-CoV-2 PLpro can block infection of human cells with low micromolar potency.

Published
2021

21. Probing the Surface of a Parasite Drug Target Thioredoxin Glutathione Reductase Using Small Molecule Fragments

Author

F. Fata, Gregory R. J. Thatcher, Nicola Demitri, Haining Lyu, Francesco Angelucci, Maurizio Polentarutti, Luana Di Leandro, Pavel A. Petukhov, David L. Williams, Matteo Ardini, I. Silvestri, Rodolfo Ippoliti, and Adele Di Matteo

Subjects
0301 basic medicine, NADPH:disulfide oxidoreductase, 030106 microbiology, Allosteric regulation, Druggability, enzyme inhibitor, fragment, NADPH Oxidoreductases, Article, 03 medical and health sciences, Multienzyme Complexes, schistosomiasis, Animals, NADH, NADPH Oxidoreductases, Binding site, allosteric effect, Antiparasitic Agents, Chemistry, Drug discovery, secondary site, Schistosoma mansoni, Small molecule, 030104 developmental biology, Infectious Diseases, Biochemistry, NADH, NADPH binding, Target protein, Thioredoxin
Abstract

Fragment screening is a powerful drug discovery approach particularly useful for enzymes difficult to inhibit selectively such as the thiol/selenol-dependent thioredoxin reductases (TrxRs), which are essential and druggable in several infectious diseases. Several known inhibitors are reactive electrophiles targeting the selenocysteine-containing C-terminus and thus often suffering from off-target reactivity in vivo. The lack of structural information on the interaction modalities of the C-terminus-targeting inhibitors, due to the high mobility of this domain, and the lack of alternative druggable sites prevents the development of selective inhibitors for TrxRs. In this work, fragments selected from actives identified in a large screen carried out against Thioredoxin Glutathione Reductase from Schistosoma mansoni (SmTGR), were probed by X-ray crystallography. SmTGR is one of the most promising drug targets for schistosomiasis, a devastating, neglected disease. Utilizing a multi-crystal method to analyze electron density maps, structural analysis, and functional studies, three binding sites were characterized in SmTGR: two sites are close to or partially superposable with the NADPH binding site, while the third one is found between two symmetry related SmTGR subunits of the crystal lattice. Surprisingly, one compound bound to this latter site stabilizes, through allosteric effects mediated by the so-called guiding bar residues, the crucial redox active C-terminus of SmTGR, making it finally visible at high resolution. These results further promote fragments as small molecule probes for investigating functional aspects of the target protein, exemplified by the allosteric effect on the C-terminus, and providing fundamental chemical information exploitable in drug discovery.

Published
2021

22. The Anomeric Effect and Associated Stereoelectronic Effects

Author

GREGORY R. J. THATCHER, WALTER A. SZAREK, John T. Edward, Gregory R. J. Thatcher, P. Deslongchamps, Anthony J. Kirby, Nicholas H. Williams, Charles L. Perrin, Michael L. Sinnott, C. Webster Andrews, Bert Fraser-Reid, J. Phillip Bowen, B. Mario Pinto, Ronald Y. N. Leung, Peter A. Petillo, Laura E. Le

Published
1993

23. Potent, Novel SARS-CoV-2 PLpro Inhibitors Block Viral Replication in Monkey and Human Cell Cultures

Author

Lijun Rong, Alqarni S, Kiira Ratia, Yangfeng Li, Oleksii Dubrovskyi, Fei Huang, Kong D, Youjeong Kwon, Rui Xiong, Zhengnan Shen, Lisa Noelle Cooper, Gregory R. J. Thatcher, and Hyun Lee

Subjects
Proteases, Protease, biology, Chemistry, medicine.medical_treatment, Ligand (biochemistry), Cysteine protease, Virology, Deubiquitinating enzyme, Viral replication, Ubiquitin, medicine, biology.protein, Potency
Abstract

Antiviral agents blocking SARS-CoV-2 viral replication are desperately needed to complement vaccination to end the COVID-19 pandemic. Viral replication and assembly are entirely dependent on two viral cysteine proteases: 3C-like protease (3CLpro) and the papain-like protease (PLpro). PLpro also has deubiquitinase (DUB) activity, removing ubiquitin (Ub) and Ub-like modifications from host proteins, disrupting the host immune response. 3CLpro is inhibited by many known cysteine protease inhibitors, whereas PLpro is a relatively unusual cysteine protease, being resistant to blockade by such inhibitors. A high-throughput screen of biased and unbiased libraries gave a low hit rate, identifying only CPI-169 and the positive control, GRL0617, as inhibitors with good potency (IC50 < 10 µM). Analogues of both inhibitors were designed to develop structure-activity relationships; however, without a co-crystal structure of the CPI-169 series, we focused on GRL0617 as a starting point for structure-based drug design, obtaining several co-crystal structures to guide optimization. A series of novel 2-phenylthiophene-based non-covalent SARS-CoV-2 PLpro inhibitors were obtained, culminating in low nanomolar potency. The high potency and slow inhibitor off-rate were rationalized by newly identified ligand interactions with a “BL2 groove” that is distal from the active site cysteine. Trapping of the conformationally flexible BL2 loop by these inhibitors blocks binding of viral and host protein substrates; however, until now it has not been demonstrated that this mechanism can induce potent and efficacious antiviral activity. In this study, we report that novel PLpro inhibitors have excellent antiviral efficacy and potency against infectious SARS-CoV-2 replication in cell cultures. Together, our data provide structural insights into the design of potent PLpro inhibitors and the first validation that non-covalent inhibitors of SARS-CoV-2 PLpro can block infection of human cells with low micromolar potency.

Published
2021

24. Systemic Candesartan Treatment Modulates Behavior, Synaptic Protein Levels, and Neuroinflammation in Female Mice That Express Human APOE4

Author

Steve Zaldua, Adedoyin Dada, Gregory R. J. Thatcher, Kateryna Krochmaliuk, Katherine Dye, Felecia M. Marottoli, Leon M. Tai, and Sarah B. Scheinman

Subjects
Apolipoprotein E, business.industry, General Neuroscience, Hippocampus, Inflammation, Disease, Pharmacology, Hippocampal formation, Prodrug, lcsh:RC321-571, ApoE4, memory, Candesartan, inflammation, Medicine, cardiovascular diseases, angiotensin receptor blocker, medicine.symptom, business, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, female sex, Neuroinflammation, medicine.drug
Abstract

Evidence suggests that angiotensin receptor blockers (ARBs) could be beneficial for Alzheimer’s disease (AD) patients independent of any effects on hypertension. However, studies in rodent models directly testing the activity of ARB treatment on behavior and AD-relevent pathology including neuroinflammation, Aβ levels, and cerebrovascular function, have produced mixed results. APOE4 is a major genetic risk factor for AD and has been linked to many of the same functions as those purported to be modulated by ARB treatment. Therefore, evaluating the effects of ARB treatment on behavior and AD-relevant pathology in mice that express human APOE4 could provide important information on whether to further develop ARBs for AD therapy. In this study, we treated female and male mice that express the human APOE4 gene in the absence (E4FAD−) or presence (E4FAD+) of high Aβ levels with the ARB prodrug candesartan cilexetil for a duration of 4 months. Compared to vehicle, candesartan treatment resulted in greater memory-relevant behavior and higher hippocampal presynaptic protein levels in female, but not male, E4FAD− and E4FAD+ mice. The beneficial effects of candesartan in female E4FAD− and E4FAD+ mice occurred in tandem with lower GFAP and Iba1 levels in the hippocampus, whereas there were no effects on markers of cerebrovascular function and Aβ levels. Collectively, these data imply that the effects of ARBs on AD-relevant pathology may be modulated in part by the interaction between APOE genotype and biological sex. Thus, the further development of ARBs could provide therapeutic options for targeting neuroinflammation in female APOE4 carriers.

Published
2021

25. Evidence for distinct mechanisms of small molecule inhibitors of filovirus entry

Author

Hyun Lee, Adam Schafer, Lijun Rong, Norton P. Peet, Yangfeng Li, Raghad Nowar, Rui Xiong, Erica Ollmann Saphire, Han Cheng, Michael Caffrey, Laura Cooper, Benjamin E. Ramirez, and Gregory R. J. Thatcher

Subjects
RNA viruses, Glycobiology, Pathology and Laboratory Medicine, medicine.disease_cause, Biochemistry, Binding Analysis, 0302 clinical medicine, Viral Envelope Proteins, Chlorocebus aethiops, Medicine and Health Sciences, Biology (General), chemistry.chemical_classification, 0303 health sciences, Organic Compounds, Ebolavirus, Small molecule, Cell biology, Chemistry, medicine.anatomical_structure, Medical Microbiology, Filoviruses, Viral Pathogens, Viruses, Physical Sciences, Host-Pathogen Interactions, Engineering and Technology, Marburg Virus, Pathogens, Cellular Structures and Organelles, medicine.symptom, Ebola Virus, Research Article, Biotechnology, Viral Entry, QH301-705.5, Immunology, Drug design, Bioengineering, Research and Analysis Methods, Antiviral Agents, Microbiology, Small Molecule Libraries, 03 medical and health sciences, Viral entry, Virology, Lysosome, Genetics, medicine, Animals, Humans, Binding site, Microbial Pathogens, Vero Cells, Molecular Biology, Chemical Characterization, Glycoproteins, 030304 developmental biology, Virus Glycoproteins, Ebola virus, Biology and life sciences, Hemorrhagic Fever Viruses, Organic Chemistry, Organisms, Chemical Compounds, Cell Biology, Hemorrhagic Fever, Ebola, Virus Internalization, RC581-607, chemistry, Mechanism of action, Small Molecules, A549 Cells, Parasitology, Immunologic diseases. Allergy, Lysosomes, Glycoprotein, Viral Transmission and Infection, 030217 neurology & neurosurgery
Abstract

Many small molecules have been identified as entry inhibitors of filoviruses. However, a lack of understanding of the mechanism of action for these molecules limits further their development as anti-filoviral agents. Here we provide evidence that toremifene and other small molecule entry inhibitors have at least three distinctive mechanisms of action and lay the groundwork for future development of anti-filoviral agents. The three mechanisms identified here include: (1) direct binding to the internal fusion loop region of Ebola virus glycoprotein (GP); (2) the HR2 domain is likely the main binding site for Marburg virus GP inhibitors and a secondary binding site for some EBOV GP inhibitors; (3) lysosome trapping of GP inhibitors increases drug exposure in the lysosome and further improves the viral inhibition. Importantly, small molecules targeting different domains on GP are synergistic in inhibiting EBOV entry suggesting these two mechanisms of action are distinct. Our findings provide important mechanistic insights into filovirus entry and rational drug design for future antiviral development., Author summary Filoviruses are among the deadliest pathogens known to mankind with case-fatality rates ranging from 25–90%. New outbreaks in central Africa and the identification of novel filoviruses in other regions highlight the urgent need to develop novel therapeutics. Although many novel anti-filovirus compounds have been reported as entry inhibitors, to date, none have made to market. This high rate of failure is in part due to a lack of knowledge of the mechanisms of action. In this report, we provide a molecular basis for the multiple mechanisms of action by which small molecule inhibitors of Ebola virus and Marburg virus block virus entry, which provides new mechanistic insight to guide design for next-generation viral entry inhibitors.

Published
2021

26. Abstract 15297: Discovery and Preclinical Optimization of Selective ABCA1 Inducers as Multifunctional Therapeutic Candidates

Author

Brian T. Layden, Md. Wasim Khan, Manel Ben Aissa, Cutler T. Lewandowski, and Gregory R. J. Thatcher

Subjects
biology, Cholesterol, business.industry, Transporter, Type 2 diabetes, Disease, Pharmacology, medicine.disease, Pathogenesis, chemistry.chemical_compound, Metabolomics, chemistry, Physiology (medical), ABCA1, biology.protein, medicine, lipids (amino acids, peptides, and proteins), Inducer, Cardiology and Cardiovascular Medicine, business
Abstract

Introduction: Reduced expression of cholesterol transporter ABCA1 is critical in pathogenesis of type 2 diabetes (T2D) and related conditions, such as cardiovascular disease (CVD) and Alzheimer’s disease (AD). Thus, increasing ABCA1 represents a novel therapeutic strategy for these conditions. However, prior drug development efforts have achieved limited success at increasing ABCA1 (controlled by liver X receptor [LXR] β) while avoiding unwanted liver triglyceride production (through LXRα via transcription factor SREBP1c). Hypothesis: We hypothesized that phenotypic screening for selective ABCA1 inducers followed by medicinal chemistry optimization would bypass the isoform selectivity issues encountered in traditional target-based drug discovery and enable development of lead therapeutic candidates with preclinical efficacy and safety. Methods/Results: We screened 20k compounds for ABCA1 and SREBP1c-linked luciferase activity, followed by qPCR to validate and prioritize selective ABCA1-inducing hits. We synthesized ~70 structural analogs of the best hit, achieving substantial EC 50 (4.5 μM to 270 nM) and E max (3.5-fold to 6.0-fold vs. vehicle) improvements in ABCA1 luciferase assay while maintaining selectivity against SREBP1c. Direct binding assays confirmed selectivity for LXRβ vs. LXRα, corroborating cell-based data. Lead compounds enhanced cellular cholesterol efflux, reduced inflammation in vitro , and attenuated high-fat diet (HFD) induced weight gain, insulin resistance, and inflammation in mice. Metabolomics analysis revealed that our lead compound corrected HFD-induced perturbations in liver glucose and fatty acid synthesis. Finally, side effects associated with published LXR agonists - liver steatosis and neutropenia - were not observed with our compound. Conclusions: We established a platform to develop selective ABCA1 inducers as drug candidates. Via this platform, we identified a safe and efficacious lead compound for T2D. Our study also represents the first report of an LXR agonist characterized by metabolomics - a powerful tool to complement biochemical readouts. Continued optimization to improve pharmacokinetic parameters, plus evaluation in CVD and AD models, is ongoing.

Published
2020

27. Discovery of Nonlipogenic ABCA1 Inducing Compounds with Potential in Alzheimer's Disease and Type 2 Diabetes

Author

Mary Jo LaDu, Brian T. Layden, Sue H. Lee, Kiira Ratia, Cutler T. Lewandowski, Manel Ben Aissa, and Gregory R. J. Thatcher

Subjects
Pharmacology, biology, business.industry, Phospholipid efflux, nutritional and metabolic diseases, Type 2 diabetes, medicine.disease, Insulin receptor, Downregulation and upregulation, Diabetes mellitus, ABCA1, Lipogenesis, biology.protein, medicine, Pharmacology (medical), lipids (amino acids, peptides, and proteins), Liver X receptor, business, Uncategorized
Abstract

[Image: see text] Selective liver X receptor (LXR) agonists have been extensively pursued as therapeutics for Alzheimer’s disease and related dementia (ADRD) and, for comorbidities such as type 2 diabetes (T2D) and cerebrovascular disease (CVD), disorders with underlying impaired insulin signaling, glucose metabolism, and cholesterol mobilization. The failure of the LXR-focused approach led us to pursue a novel strategy to discover nonlipogenic ATP-binding cassette transporter A1 (ABCA1) inducers (NLAIs): screening for ABCA1-luciferase activation in astrocytoma cells and counterscreening against lipogenic gene upregulation in hepatocarcinoma cells. Beneficial effects of LXRβ agonists mediated by ABCA1 include the following: control of cholesterol and phospholipid efflux to lipid-poor apolipoproteins forming beneficial peripheral HDL and HDL-like particles in the brain and attenuation of inflammation. While rare, ABCA1 variants reduce plasma HDL and correlate with an increased risk of ADRD and CVD. In secondary assays, NLAI hits enhanced cholesterol mobilization and positively impacted in vitro biomarkers associated with insulin signaling, inflammatory response, and biogenic properties. In vivo target engagement was demonstrated after oral administration of NLAIs in (i) mice fed a high-fat diet, a model for obesity-linked T2D, (ii) mice administered LPS, and (iii) mice with accelerated oxidative stress. The lack of adverse effects on lipogenesis and positive effects on multiple biomarkers associated with T2D and ADRD supports this novel phenotypic approach to NLAIs as a platform for T2D and ADRD drug discovery.

Published
2020

28. Metabolomic analysis of a selective ABCA1 inducer in obesogenic challenge provides a rationale for therapeutic development

Author

Manel BenAissa, Md. Wasim Khan, Brian T. Layden, Martha Ackerman-Berrier, Cutler T. Lewandowski, Oleksii Dubrovskyi, Mary Jo LaDu, and Gregory R. J. Thatcher

Subjects
0301 basic medicine, Male, Medicine (General), Peroxisome Proliferator-Activated Receptors, Peroxisome proliferator-activated receptor, ABCA1, Pharmacology, Mice, 0302 clinical medicine, Medicine, Molecular Targeted Therapy, RNA, Small Interfering, Uncategorized, Adiposity, Liver X Receptors, chemistry.chemical_classification, biology, Drug discovery, Type 2 diabetes, General Medicine, Lipids, High-fat diet, 030220 oncology & carcinogenesis, Lipogenesis, Metabolome, Cytokines, lipids (amino acids, peptides, and proteins), Disease Susceptibility, Inflammation Mediators, ATP Binding Cassette Transporter 1, Side effect, Retinoid X receptor, Diet, High-Fat, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Metabolomics, R5-920, Drug Development, Glucose Intolerance, Animals, Obesity, Liver X receptor, business.industry, Insulin receptor, Disease Models, Animal, 030104 developmental biology, Retinoid X Receptors, chemistry, biology.protein, Commentary, Anti-inflammatory, Insulin Resistance, business, Biomarkers
Abstract

Background Therapeutic agents with novel mechanisms of action are needed to combat the growing epidemic of type 2 diabetes (T2D) and related metabolic syndromes. Liver X receptor (LXR) agonists possess preclinical efficacy yet produce side effects due to excessive lipogenesis. Anticipating that many beneficial and detrimental effects of LXR agonists are mediated by ABCA1 and SREPB1c expression, respectively, we hypothesized that a phenotypic optimization strategy prioritizing selective ABCA1 induction would identify an efficacious lead compound with an improved side effect profile over existing LXRβ agonists. Methods We synthesized and characterized a novel small molecule for selective induction of ABCA1 vs. SREBP1c in vitro. This compound was evaluated in both wild-type mice and a high-fat diet (HFD) mouse model of obesity-driven diabetes through functional, biochemical, and metabolomic analysis. Findings Six weeks of oral administration of our lead compound attenuated weight gain, glucose intolerance, insulin signaling deficits, and adiposity. Global metabolomics revealed suppression of gluconeogenesis, free fatty acids, and pro-inflammatory metabolites. Target identification linked these beneficial effects to selective LXRβ agonism and PPAR/RXR antagonism. Interpretation Our observations in the HFD model, combined with the absence of lipogenesis and neutropenia in WT mice, support this novel approach to therapeutic development for T2D and related conditions.

Published
2020

29. Screening and Reverse-Engineering of Estrogen Receptor Ligands as Potent Pan-Filovirus Inhibitors

Author

Katherine Dye, Yangfeng Li, Adam Schafer, Lijun Rong, Raghad Nowar, Rui Xiong, Zhengnan Shen, Han Cheng, Manu Anantpadma, Robert A. Davey, Bani Medegan Fagla, Gregory R. J. Thatcher, and Laura Cooper

Subjects
Drug Evaluation, Preclinical, Mutagenesis (molecular biology technique), Estrogen receptor, Filoviridae, Ligands, 01 natural sciences, Antiviral Agents, Membrane Fusion, Models, Biological, Article, 03 medical and health sciences, Structure-Activity Relationship, Viral entry, Cell Line, Tumor, Drug Discovery, medicine, Humans, Toremifene, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, Dual inhibitor, biology.organism_classification, Virology, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Receptors, Estrogen, Selective estrogen receptor modulator, Molecular Medicine, Glycoprotein, medicine.drug
Abstract

Filoviridae, including Ebola (EBOV) and Marburg (MARV) viruses, are emerging pathogens that pose a serious threat to public health. No agents have been approved to treat filovirus infections, representing a major unmet medical need. The selective estrogen receptor modulator (SERM) toremifene was previously identified from a screen of FDA-approved drugs as a potent EBOV viral entry inhibitor, via binding to EBOV glycoprotein (GP). A focused screen of ER ligands identified ridaifen-B as a potent dual inhibitor of EBOV and MARV. Optimization and reverse-engineering to remove ER activity led to a novel compound 30 (XL-147) showing potent inhibition against infectious EBOV Zaire (0.09 μM) and MARV (0.64 μM). Mutagenesis studies confirmed that inhibition of EBOV viral entry is mediated by the direct interaction with GP. Importantly, compound 30 displayed a broad-spectrum antifilovirus activity against Bundibugyo, Tai Forest, Reston, and Měngla viruses and is the first submicromolar antiviral agent reported for some of these strains, therefore warranting further development as a pan-filovirus inhibitor.

Published
2020

30. Discovery and Structural Optimization of 4-(Aminomethyl)benzamides as Potent Entry Inhibitors of Ebola and Marburg Virus Infections

Author

Han Cheng, Lijun Rong, Norton P. Peet, Adam Schafer, Letitia Wong, Manu Anantpadma, Irina N. Gaisina, Robert A. Davey, and Gregory R. J. Thatcher

Subjects
viruses, Drug Evaluation, Preclinical, medicine.disease_cause, 01 natural sciences, Antiviral Agents, Article, West africa, Marburg virus, 03 medical and health sciences, Structure-Activity Relationship, Viral Envelope Proteins, Marburg virus disease, Drug Discovery, Chlorocebus aethiops, medicine, Animals, Humans, Marburg Virus Disease, Liver microsomes, Vero Cells, 030304 developmental biology, 0303 health sciences, Ebola virus, Chemistry, virus diseases, Hemorrhagic Fever, Ebola, Virus Internalization, Virology, 0104 chemical sciences, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, A549 Cells, Benzamides, Microsomes, Liver, Molecular Medicine, Cytochrome P-450 CYP3A Inhibitors, Toremifene
Abstract

The recent Ebola epidemics in West Africa underscore the great need for effective and practical therapies for future Ebola virus outbreaks. We have discovered a new series of remarkably potent small molecule inhibitors of Ebola virus entry. These 4-(aminomethyl)benzamide-based inhibitors are also effective against Marburg virus. Synthetic routes to these compounds allowed for the preparation of a wide variety of structures, including a conformationally restrained subset of indolines (compounds 41–50). Compounds 20, 23, 32, 33, and 35 are superior inhibitors of Ebola (Mayinga) and Marburg (Angola) infectious viruses. Representative compounds (20, 32 and 35) have shown good metabolic stability in plasma and liver microsomes (rat and human), and 32 did not inhibit CYP3A4 nor CYP2C9. These 4-(aminomethyl)benzamides are suitable for further optimization as inhibitors of filovirus entry, with potential to be developed as therapeutic agents for the treatment and control of Ebola virus infections.

Published
2020

31. Rationalized inhibition of mixed lineage kinase 3 and CD70 enhances life span and antitumor efficacy of CD8

Author

Sunil Kumar Singh, Ajay Rana, Matthew J. Dorman, Navin Viswakarma, Rakesh Sathish Nair, Basabi Rana, Subhash C. Sinha, Kent Hoskins, Sandeep Kumar, Gautam Sondarva, Gregory R. J. Thatcher, and Periannan Sethupathi

Subjects
0301 basic medicine, Cancer Research, medicine.medical_treatment, T cell, Immunology, Longevity, lymphocytes, tumor-infiltrating, CD38, CD8-Positive T-Lymphocytes, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Line, Tumor, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Humans, tumor microenvironment, RC254-282, Pharmacology, Clinical/Translational Cancer Immunotherapy, cytotoxicity, immunologic, Tumor microenvironment, Chemistry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, adaptive immunity, Acquired immune system, MAP Kinase Kinase Kinases, Molecular biology, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Oncology, Molecular Medicine, Tumor necrosis factor alpha, Female, 030217 neurology & neurosurgery, CD8, CD27 Ligand
Abstract

BackgroundThe mitogen-activated protein kinases (MAPKs) are important for T cell survival and their effector function. Mixed lineage kinase 3 (MLK3) (MAP3K11) is an upstream regulator of MAP kinases and emerging as a potential candidate for targeted cancer therapy; yet, its role in T cell survival and effector function is not known.MethodsT cell phenotypes, apoptosis and intracellular cytokine expressions were analyzed by flow cytometry. The apoptosis-associated gene expressions in CD8+CD38+ T cells were measured using RT2 PCR array. In vivo effect of combined blockade of MLK3 and CD70 was analyzed in 4T1 tumor model in immunocompetent mice. The serum level of tumor necrosis factor-α (TNFα) was quantified by enzyme-linked immunosorbent assay.ResultsWe report that genetic loss or pharmacological inhibition of MLK3 induces CD70-TNFα-TNFRSF1a axis-mediated apoptosis in CD8+ T cells. The genetic loss of MLK3 decreases CD8+ T cell population, whereas CD4+ T cells are partially increased under basal condition. Moreover, the loss of MLK3 induces CD70-mediated apoptosis in CD8+ T cells but not in CD4+ T cells. Among the activated CD8+ T cell phenotypes, CD8+CD38+ T cell population shows more than five fold increase in apoptosis due to loss of MLK3, and the expression of TNFRSF1a is significantly higher in CD8+CD38+ T cells. In addition, we observed that CD70 is an upstream regulator of TNFα-TNFRSF1a axis and necessary for induction of apoptosis in CD8+ T cells. Importantly, blockade of CD70 attenuates apoptosis and enhances effector function of CD8+ T cells from MLK3−/− mice. In immune-competent breast cancer mouse model, pharmacological inhibition of MLK3 along with CD70 increased tumor infiltration of cytotoxic CD8+ T cells, leading to reduction in tumor burden largely via mitochondrial apoptosis.ConclusionTogether, these results demonstrate that MLK3 plays an important role in CD8+ T cell survival and effector function and MLK3-CD70 axis could serve as a potential target in cancer.

Published
2020

32. Phase 1 study of TTC-352 in patients with metastatic breast cancer progressing on endocrine and CDK4/6 inhibitor therapy

Author

Arkadiusz Z. Dudek, James H. Fischer, Debra A. Tonetti, Jasgit C. Sachdev, Ruth O'Regan, Elizabeth L. Wiley, Robert P. Venuti, Jonathan Bleeker, Gregory R. J. Thatcher, Randolph Hurley, and Li C Liu

Subjects
0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Estrogen receptor, Breast Neoplasms, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Internal medicine, Clinical endpoint, Medicine, Humans, business.industry, Cancer, Cyclin-Dependent Kinase 4, medicine.disease, Metastatic breast cancer, Progression-Free Survival, 030104 developmental biology, Treatment Outcome, Tolerability, 030220 oncology & carcinogenesis, Toxicity, Hormonal therapy, Female, business
Abstract

TTC-352 is a selective human estrogen receptor (ER) partial agonist developed for treatment of hormone-refractory ER + breast cancer. This was an accelerated dose escalation study with the primary endpoint of maximum tolerated dose that evaluated five dose levels of TTC-352 in breast cancer progressing after at least two lines of hormonal therapy including one in combination with a CDK4/6 inhibitor. The secondary objectives were to determine treatment tolerability, pharmacokinetics of TTC-352, best response, progression-free survival (PFS), and PKCα expression in tumors. The study enrolled 15 patients. No dose-limiting toxicity was observed. Patients experienced the following grade 3 toxicities: asymptomatic pulmonary embolism, diarrhea, aspartate transaminase elevation, and myalgia, and one grade 4 toxicity of gamma glutamyltransferase elevation. Pharmacokinetic half-life was 7.6–14.3 h. The intra- and inter-individual variability for AUC0-∞ hampered assessment of the relationship between dose and AUC0-∞. Median PFS was 58 days (95% CI = 28,112). Higher PKCα expression in tumor stroma was associated with a trend toward longer PFS. TTC-352 demonstrates safety and early clinical evidence of antitumor activity against heavily pretreated hormone-refractory breast cancer. Based upon TTC-352 plasma concentrations and tolerability, the 180 mg twice a day is recommended for further testing. (ClinicalTrials.gov Identifier: NCT03201913)

Published
2020

33. Pharmacology and Molecular Mechanisms of Clinically Relevant Estrogen Estetrol and Estrogen Mimic BMI-135 for the Treatment of Endocrine-Resistant Breast Cancer

Author

Rui Xiong, Gregory R. J. Thatcher, Jay S. Hanspal, V. Craig Jordan, Balkees Abderrahman, Debra A. Tonetti, Philipp Y. Maximov, Ramona Curpan, and Ping Fan

Subjects
0301 basic medicine, Agonist, medicine.drug_class, Cell Survival, Estrogen receptor, Breast Neoplasms, Pharmacology, Partial agonist, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Medicine, Humans, Gene Regulatory Networks, Aromatase, Cell Proliferation, biology, Molecular Structure, business.industry, Estetrol, Molecular Mimicry, Estrogen Receptor alpha, Estriol, Estrogens, Articles, Gene Expression Regulation, Neoplastic, 030104 developmental biology, chemistry, Estrogen, Drug Resistance, Neoplasm, biology.protein, MCF-7 Cells, Unfolded Protein Response, Molecular Medicine, Female, business, 030217 neurology & neurosurgery, Tamoxifen, hormones, hormone substitutes, and hormone antagonists, medicine.drug
Abstract

Long-term estrogen deprivation (LTED) with tamoxifen (TAM) or aromatase inhibitors leads to endocrine-resistance, whereby physiologic levels of estrogen kill breast cancer (BC). Estrogen therapy is effective in treating patients with advanced BC after resistance to TAM and aromatase inhibitors develops. This therapeutic effect is attributed to estrogen-induced apoptosis via the estrogen receptor (ER). Estrogen therapy can have unpleasant gynecologic and nongynecologic adverse events. Here, we study estetrol (E4) and a model Selective Human ER Partial Agonist (ShERPA) BMI-135. Estetrol and ShERPA TTC-352 are being evaluated in clinical trials. These agents are proposed as safer estrogenic candidates compared with 17β-estradiol (E2) for the treatment of endocrine-resistant BC. Cell viability assays, real-time polymerase chain reaction, luciferase reporter assays, chromatin immunoprecipitation, docking and molecular dynamics simulations, human unfolded protein response (UPR) RT2 PCR profiler arrays, live cell microscopic imaging and analysis, and annexin V staining assays were conducted. Our work was done in eight biologically different human BC cell lines and one human endometrial cancer cell line, and results were compared with full agonists estrone, E2, and estriol, a benchmark partial agonist triphenylethylene bisphenol (BPTPE), and antagonists 4-hydroxytamoxifen and endoxifen. Our study shows the pharmacology of E4 and BMI-135 as less-potent full-estrogen agonists as well as their molecular mechanisms of tumor regression in LTED BC through triggering a rapid UPR and apoptosis. Our work concludes that the use of a full agonist to treat BC is potentially superior to a partial agonist given BPTPE's delayed induction of UPR and apoptosis, with a higher probability of tumor clonal evolution and resistance. SIGNIFICANCE STATEMENT: Given the unpleasant gynecologic and nongynecologic adverse effects of estrogen treatment, the development of safer estrogens for endocrine-resistant breast cancer (BC) treatment and hormone replacement therapy remains a priority. The naturally occurring estrogen estetrol and Selective Human Estrogen-Receptor Partial Agonists are being evaluated in endocrine-resistant BC clinical trials. This work provides a comprehensive evaluation of their pharmacology in numerous endocrine-resistant BC models and an endometrial cancer model and their molecular mechanisms of tumor regression through the unfolded protein response and apoptosis.

Published
2020

34. Interaction of oxidative stress and neurotrauma in ALDH2

Author

Rachel C, Knopp, Sue H, Lee, Michael, Hollas, Emily, Nepomuceno, David, Gonzalez, Kevin, Tam, Daniyal, Aamir, Yueting, Wang, Emily, Pierce, Manel, BenAissa, and Gregory R J, Thatcher

Subjects
Disease Models, Animal, Mice, Oxidative Stress, Neuroprotective Agents, Neuroinflammation, Drug discovery, Aldehyde Dehydrogenase, Mitochondrial, Lipid peroxidation, Animals, Mild traumatic brain injury, Brain Concussion, Research Paper
Abstract

Oxidative stress induced by lipid peroxidation products (LPP) accompanies aging and has been hypothesized to exacerbate the secondary cascade in traumatic brain injury (TBI). Increased oxidative stress is a contributor to loss of neural reserve that defines the ability to maintain healthy cognitive function despite the accumulation of neuropathology. ALDH2−/− mice are unable to clear aldehyde LPP by mitochondrial aldehyde dehydrogenase-2 (Aldh2) detoxification and provide a model to study mild TBI (mTBI), therapeutic interventions, and underlying mechanisms. The ALDH2−/− mouse model presents with elevated LPP-mediated protein modification, lowered levels of PSD-95, PGC1-α, and SOD-1, and mild cognitive deficits from 4 months of age. LPP scavengers are neuroprotective in vitro and in ALDH2−/− mice restore cognitive performance. A single-hit, closed skull mTBI failed to elicit significant effects in WT mice; however, ALDH2−/− mice showed a significant inflammatory cytokine surge in the ipsilateral hemisphere 24 h post-mTBI, and increased GFAP cleavage, a biomarker for TBI. Known neuroprotective agents, were able to reverse the effects of mTBI. This new preclinical model of mTBI, incorporating significant perturbations in behavior, inflammation, and clinically relevant biomarkers, allows mechanistic study of the interaction of LPP and neurotrauma in loss of neural reserve., Graphical abstract Image 1, Highlights • ALDH2−/− mice have elevated brain LPP adducts and mild cognitive impairment. • The effects of a “2nd hit” via LPS are exacerbated by LPP in vitro and in vivo. • ALDH2−/− mice + mTBI show amplified/prolonged cognitive deficits and neuroinflammation. • This new preclinical model for mTBI supports a role for LPP in reduced neural reserve.

Published
2020

35. Characterization of lead compounds targeting the selenoprotein thioredoxin glutathione reductase for treatment of schistosomiasis

Author

David L. Williams, Elias S.J. Arnér, Francesco Angelucci, Paul R. Banta, Haining Lyu, Pavel A. Petukhov, Anton Simeonov, Gregory R. J. Thatcher, Wendy A. Lea, Ajit Jadhav, and Qing Cheng

Subjects
0301 basic medicine, 030106 microbiology, Schistosomiasis, Article, Inhibitory Concentration 50, Mice, Schistosomicides, 03 medical and health sciences, chemistry.chemical_compound, Multienzyme Complexes, Drug Discovery, medicine, Animals, Helminths, NADH, NADPH Oxidoreductases, Enzyme Inhibitors, chemistry.chemical_classification, Oxidase test, biology, Superoxide, fungi, Schistosoma mansoni, medicine.disease, biology.organism_classification, High-Throughput Screening Assays, Praziquantel, 030104 developmental biology, Infectious Diseases, Biochemistry, chemistry, Selenoprotein, Oxidation-Reduction, NADP, Nicotinamide adenine dinucleotide phosphate, medicine.drug
Abstract

Schistosomiasis is a widespread human parasitic disease currently affecting over 200 million people. Chemotherapy for schistosomiasis relies exclusively on praziquantel. Although significant advances have been made in recent years to reduce the incidence and intensity of schistosome infections, these gains will be at risk should drug resistance parasites evolve. Thioredoxin glutathione reductase (TGR) is a selenoprotein of the parasite essential for the survival of schistosomes in the mammalian host. Several high-throughput screening campaigns have identified inhibitors of Schistosoma mansoni TGR. Follow up analyses of select active compounds form the basis of the present study. We identified eight compounds effective against ex vivo worms. Compounds 1 – 5 are active against all major species and development stages. Ability of these compounds to target immature worms is especially critical because praziquantel is poorly active against this stage. Compounds 1 – 5, 7, and 8 displayed schistosomicidal activity even after only one-hour incubation with the worms. Compounds 1 – 4 meet or exceed standards set by the World Health Organization for leads for schistosomiasis therapy activity. The mechanism of TGR inhibition was studied further with wild type and mutant TGR proteins. Compounds 4 – 6 were found to induce an nicotinamide adenine dinucleotide phosphate (NADPH) oxidase activity in TGR, leading to the production of superoxide and hydrogen peroxide. Collectively, this effort has identified several active compound series that may serve as the basis for the development of new schistosomicidal compounds.

Published
2020

36. Repurposing potential of 1st generation H1-specific antihistamines as anti-filovirus therapeutics

Author

Adam Schafer, Veronica Soloveva, Feiyan Mo, Sina Bavari, Lijun Rong, Gregory R. J. Thatcher, Cary Retterer, Rui Xiong, and Han Cheng

Subjects
0301 basic medicine, Drug, media_common.quotation_subject, medicine.medical_treatment, Drug Evaluation, Preclinical, Histamine Antagonists, Microbial Sensitivity Tests, Pharmacology, Antiviral Agents, Article, Piperazines, Inhibitory Concentration 50, 03 medical and health sciences, chemistry.chemical_compound, Chlorcyclizine, Virology, medicine, Humans, Receptor, Repurposing, media_common, business.industry, Drug Repositioning, Virus Internalization, Filoviridae, Molecular Docking Simulation, Drug repositioning, Hemorrhagic Fevers, Diphenhydramine, HEK293 Cells, 030104 developmental biology, chemistry, A549 Cells, Antihistamine, business, Histamine, medicine.drug
Abstract

Ebola and Marburg are filoviruses and biosafety level 4 pathogens responsible for causing severe hemorrhagic fevers in humans with mortality rates up to 90%. The most recent outbreak in West Africa resulted in approximately 11,310 deaths in 28,616 reported cases. Currently there are no FDA-approved vaccines or therapeutics to treat infections of these deadly viruses. Recently we screened an FDA-approved drug library and identified numerous G protein-coupled receptor (GPCR) antagonists including antihistamines possessing anti-filovirus properties. Antihistamines are attractive targets for drug repurposing because of their low cost and ease of access due to wide use. In this report we identify common over the counter antihistamines, such as diphenhydramine (Benadryl) and chlorcyclizine (Ahist) as potential candidates for repurposing as anti-filovirus agents. Furthermore, we demonstrate that this potential is wide-spread through the 1(st) generation of H(1)-specific antihistamines but is not present in newer drugs or drugs targeting H(2), H(3) and H(4) receptors. We showed that the filovirus entry inhibition is not dependent on the classical antagonism of cell surface histamine or muscarinic acetylcholine receptors but occurs in the endosome, like the cathepsin inhibitor CA-074. Finally, using extensive docking studies we showed the potential for these drugs to bind directly to the EBOV-GP at the same site as toremifene. These findings suggest that the 1(st) generation antihistamines are excellent candidates for repurposing as anti-filovirus therapeutics and can be further optimized for removal of unwanted histamine or muscarinic receptor interactions without loss of anti-filovirus efficacy.

Published
2018

37. 2-Arylidene Hydrazinecarbodithioates as Potent, Selective Inhibitors of Cystathionine γ-Lyase (CSE)

Author

Duncan J. Wardrop, Pavel A. Petukhov, Liang Yin, Abir Bhattacharjee, Gregory R. J. Thatcher, Antara Sinha, Loruhama Delgado-Rivera, and Kiira Ratia

Subjects
0301 basic medicine, biology, Chemistry, Hydrogen sulfide, Organic Chemistry, High selectivity, Cystathionine γ lyase, Hydrogen sulfide biosynthesis, Ischemic injury, 010402 general chemistry, 01 natural sciences, Biochemistry, Cystathionine beta synthase, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Downregulation and upregulation, FOS: Chemical sciences, parasitic diseases, Drug Discovery, biology.protein
Abstract

Hydrogen sulfide is produced from l-cysteine by the action of both cystathionine γ-lyase (CSE) and cystathionine β-synthase (CBS) and increasingly has been found to play a profound regulatory role in a range of physiological processes. Mounting evidence suggests that upregulation of hydrogen sulfide biosynthesis occurs in several disease states, including rheumatoid arthritis, hypertension, ischemic injury, and sleep-disordered breathing. In addition to being critical tools in our understanding of hydrogen sulfide biology, inhibitors of CSE hold therapeutic potential for the treatment of diseases in which increased levels of this gasotransmitter play a role. We describe the discovery and development of a novel series of potent CSE inhibitors that show increased activity over the benchmark inhibitor and, importantly, display high selectivity for CSE versus CBS.

Published
2017

38. Identification of a potent Nrf2 displacement activator among aspirin-containing prodrugs

Author

Dmitry M. Hushpulian, Eliot H. Kazakov, Bobby Thomas, Irina N. Gaisina, Irina G. Gazaryan, Manuj Ahuja, Arsen Gaisin, Navneet Ammal Kaidery, Andrey A. Poloznikov, and Gregory R. J. Thatcher

Subjects
Reporter gene, Aspirin, Dose-Response Relationship, Drug, NF-E2-Related Factor 2, Chemistry, Activator (genetics), Anti-Inflammatory Agents, Non-Steroidal, Leaving group, Cell Biology, Prodrug, Combinatorial chemistry, Article, Protein Structure, Tertiary, Cellular and Molecular Neuroscience, Acetylation, Cell Line, Tumor, Humans, Moiety, Prodrugs, Intracellular, Cysteine
Abstract

Aspirin is a desired leaving group in prodrugs aimed at treatment of neurodegeneration and other conditions. A library of aspirin derivatives of various scaffolds potentially activating Nrf2 has been tested in Neh2-luc reporter assay which screens for direct Nrf2 protein stabilizers working via disruption of Nrf2-Keap1 interaction. Most aspirin prodrugs had a pro-alkylating or pro-oxidant motif in the structure and, therefore, were toxic at high concentrations. However, among the active compounds, we identified a molecule resembling a well-known Nrf2 displacement activator, bis-1,4-(4-methoxybenzenesulfonamidyl) naphthalene (NMBSA). The direct comparison of the newly identified compound with NMBSA and its improved analog in the reporter assay showed no quenching with N-acetyl cysteine, thus pointing to Nrf2 stabilization mechanism without cysteine alkylation. The potency of the newly identified compound in the reporter assay was much stronger than NMBSA, despite its inhibitory action in the commercial fluorescence polarization assay was observed only in the millimolar range. Molecular docking predicted that mono-deacetylation of the novel prodrug should generate a potent displacement activator. The time-course of reporter activation with the novel prodrug had a pronounced lag-period pointing to a plausible intracellular transformation leading to an active product. Treatment of the novel prodrug with blood plasma or cell lysate demonstrated stepwise deacetylation as judge by liquid chromatography-mass spectrometry (LC-MS). Hence, the esterase-catalyzed hydrolysis of the prodrug liberates only acetyl groups from aspirin moiety and generates a potent Nrf2 activator. The discovered mechanism of prodrug activation makes the newly identified compound a promising lead for future optimization studies.

Published
2021

39. Design, Synthesis, Molecular Modeling, and Biological Evaluation of Novel Amine-based Histone Deacetylase Inhibitors

Author

Gregory R. J. Thatcher, Aditya S. Vaidya, Irida Kastrati, Antonett Madriaga, Taha Y. Taha, Hazem Abdelkarim, Raghupathi Neelarapu, Jonna Frasor, Pavel A. Petukhov, Bhargava Karumudi, and Yue-Ting Wang

Subjects
Models, Molecular, 0301 basic medicine, Stereochemistry, Antineoplastic Agents, Crystallography, X-Ray, Biochemistry, Histone Deacetylases, Article, Structure-Activity Relationship, 03 medical and health sciences, Cell Line, Tumor, Drug Discovery, Humans, Amines, General Pharmacology, Toxicology and Pharmaceutics, IC50, Cell Proliferation, Pharmacology, Dose-Response Relationship, Drug, Molecular Structure, biology, Chemistry, Histone deacetylase 2, Organic Chemistry, HDAC8, Histone Deacetylase Inhibitors, 030104 developmental biology, Histone, Acetylation, Docking (molecular), Drug Design, biology.protein, Molecular Medicine, Histone deacetylase, Drug Screening Assays, Antitumor, Drug metabolism
Abstract

Histone deacetylases (HDACs) are promising drug targets for a variety of therapeutic applications. Herein we describe the design, synthesis, biological evaluation in cellular models of cancer, and preliminary drug metabolism and pharmacokinetic studies (DMPK) of a series of secondary and tertiary N-substituted 7-aminoheptanohydroxamic acid-based HDAC inhibitors. Introduction of an amino group with one or two surface binding groups (SBGs) yielded a successful strategy to develop novel and potent HDAC inhibitors. The secondary amines were found to be generally more potent than the corresponding tertiary amines. Docking studies suggested that the SBGs of tertiary amines cannot be favorably accommodated at the gorge region of the binding site. The secondary amines with naphthalen-2-ylmethyl, 5-phenylthiophen-2-ylmethyl, and 1H-indol-2-ylmethyl (2 j) substituents exhibited the highest potency against class I HDACs: HDAC1 IC50 39-61 nm, HDAC2 IC50 260-690 nm, HDAC3 IC50 25-68 nm, and HDAC8 IC50 320-620 nm. The cytotoxicity of a representative set of secondary and tertiary N-substituted 7-aminoheptanoic acid hydroxyamide-based inhibitors against HT-29, SH-SY5Y, and MCF-7 cancer cells correlated with their inhibition of HDAC1, 2, and 3 and was found to be similar to or better than that of suberoylanilide hydroxamic acid (SAHA). Compounds in this series increased the acetylation of histones H3 and H4 in a time-dependent manner. DMPK studies indicated that secondary amine 2 j is metabolically stable and has plasma and brain concentrations >23- and >1.6-fold higher than the IC50 value for class I HDACs, respectively. Overall, the secondary and tertiary N-substituted 7-aminoheptanoic acid hydroxyamide-based inhibitors exhibit excellent lead- and drug-like properties and therapeutic capacity for cancer applications.

Published
2017

40. Design, Synthesis, and Biological Evaluation of Tetrahydroisoquinoline-Based Histone Deacetylase 8 Selective Inhibitors

Author

Raghupathi Neelarapu, Yunlong Lu, Naohiko Ikegaki, Taha Y. Taha, Pavel A. Petukhov, Gregory R. J. Thatcher, Jayaprakash Neerasa, Shaimaa M. Aboukhatwa, Rachel C. Knopp, Thomas W. Hanigan, and Hazem Abdelkarim

Subjects
0301 basic medicine, Tetrahydroisoquinoline, Stereochemistry, Organic Chemistry, HDAC8, HDAC6, Biology, Biochemistry, HDAC1, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Acetylation, 030220 oncology & carcinogenesis, Drug Discovery, Histone deacetylase, Binding site, Cytotoxicity
Abstract

Histone deacetylase 8 (HDAC8) is a promising drug target for multiple therapeutic applications. Here, we describe the modeling, design, synthesis, and biological evaluation of a novel series of C1-substituted tetrahydroisoquinoline (TIQ)-based HDAC8 inhibitors. Minimization of entropic loss upon ligand binding and use of the unique HDAC8 “open” conformation of the binding site yielded a successful strategy for improvement of both HDAC8 potency and selectivity. The TIQ-based 3g and 3n exhibited the highest 82 and 55 nM HDAC8 potency and 330- and 135-fold selectivity over HDAC1, respectively. Selectivity over other class I isoforms was comparable or better, whereas inhibition of HDAC6, a class II HDAC isoform, was below 50% at 10 μM. The cytotoxicity of 3g and 3n was evaluated in neuroblastoma cell lines, and 3n displayed concentration-dependent cytotoxicity similar to or better than that of PCI-34051. The selectivity of 3g and 3n was confirmed in SH-SY5Y cells as both did not increase the acetylation of hi...

Published
2017

41. A Novel Strategy to Co-target Estrogen Receptor and Nuclear Factor κB Pathways with Hybrid Drugs for Breast Cancer Therapy

Author

Gregory R. J. Thatcher, Irida Kastrati, Svitlana D. Brovkovych, Jonna Frasor, and Marton I. Siklos

Subjects
Selective Estrogen Receptor Modulators, 0301 basic medicine, Drug, Cancer Research, Antineoplastic Agents, Hormonal, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Estrogen receptor, Breast Neoplasms, Pharmacology, Article, 03 medical and health sciences, Endocrinology, Breast cancer, Fumarates, medicine, Humans, Raloxifene, Molecular Targeted Therapy, Aromatase, Clonogenic assay, media_common, biology, Endocrine and Autonomic Systems, business.industry, NF-kappa B, medicine.disease, Tamoxifen, 030104 developmental biology, Receptors, Estrogen, Oncology, Selective estrogen receptor modulator, Raloxifene Hydrochloride, MCF-7 Cells, biology.protein, Female, business, Signal Transduction, medicine.drug
Abstract

Nearly 75% of breast tumors express estrogen receptor (ER), and will be treated with endocrine therapy, such as selective estrogen receptor modulator (SERM), tamoxifen, or aromatase inhibitors. Despite their proven success, as many as 40-50% of ER+ tumors fail to respond to endocrine therapy and eventually recur as aggressive, metastatic cancers. Therefore, preventing and/or overcoming endocrine resistance in ER+ tumors remains a major clinical challenge. Deregulation or activation of the nuclear factor κB (NFκB) pathway has been implicated in endocrine resistance and poor patient outcome in ER+ tumors. As a consequence, one option to improve on existing anti-cancer treatment regimens may be to introduce additional anti-NFκB activity to endocrine therapy drugs. Our approach was to design and test SERM-fumarate co-targeting hybrid drugs capable of simultaneously inhibiting both ER, via the SERM, raloxifene, and the NFκB pathway, via fumarate, in breast cancer cells. We find that the hybrid drugs display improved anti-NFκB pathway inhibition compared to either raloxifene or fumarate. Despite some loss in potency against the ER pathway, these hybrid drugs maintain anti-proliferative activity in ER+ breast cancer cells. Furthermore, these drugs prevent clonogenic growth and mammosphere formation of ER+ breast cancer cells. As a proof-of-principle, the simultaneous inhibition of ER and NFκB via a single bifunctional hybrid drug may represent a viable approach to improve the anti-inflammatory activity and prevent therapy resistance of ER-targeted anti-cancer drugs.

Published
2017

42. Novel Selective Estrogen Receptor Downregulators (SERDs) Developed against Treatment-Resistant Breast Cancer

Author

Sue Lee, Gregory R. J. Thatcher, Yue-Ting Wang, Huiping Zhao, Rui Xiong, Jiong Zhao, Debra A. Tonetti, Yunlong Lu, Bhargava Karumudi, and Lauren M. Gutgesell

Subjects
Models, Molecular, Selective Estrogen Receptor Modulators, 0301 basic medicine, Neoplasms, Hormone-Dependent, Antineoplastic Agents, Hormonal, Mice, Nude, Estrogen receptor, Breast Neoplasms, Thiophenes, Pharmacology, Article, Arzoxifene, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Raloxifene, Breast, Viability assay, Aromatase, Fulvestrant, biology, 030104 developmental biology, Receptors, Estrogen, chemistry, Drug Resistance, Neoplasm, Selective estrogen receptor modulator, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, Female, Tamoxifen, medicine.drug
Abstract

Resistance to the selective estrogen receptor modulator (SERM) tamoxifen and to aromatase inhibitors that lower circulating estradiol occurs in up to 50% of patients, generally leading to an endocrine-independent ER+ phenotype. Selective ER downregulators (SERDs) are able to ablate ER and thus theoretically to prevent survival of both endocrine-dependent and independent ER+ tumors. The clinical SERD, fulvestrant, is hampered by intramuscular administration and undesirable pharmacokinetics. Novel SERDs were designed using the 6-OH-benzothiophene (BT) scaffold common to arzoxifene and raloxifene. Treatment-resistant (TR) ER+ cell lines (MCF-7:5C and MCF-7:TAM1) were used for optimization, followed by validation in the parent endocrine-dependent cell line (MCF-7:WS8), in 2D and 3D cultures, using ERα in-cell westerns, ERE-luciferase, and cell viability assays, with GDC-0810 (ARN-810) used for comparison. Two BT SERDs with superior in vitro activity to GDC-0810 were studied for bioavailability and shown to cause regression of a TR, endocrine-independent ER+ xenograft superior to GDC-0810.

Published
2017

43. Rexinoids as Therapeutics for Alzheimer's Disease: Role of APOE

Author

Kevin P. Koster, Ana Carolina Valencia-Olvera, Gregory R. J. Thatcher, Mary Jo LaDu, Conor Smith, and Leon M. Tai

Subjects
0301 basic medicine, Apolipoprotein E, Pathology, medicine.medical_specialty, Population, Disease, Retinoid X receptor, Biology, Bioinformatics, Pathogenesis, Retinoids, 03 medical and health sciences, Apolipoproteins E, 0302 clinical medicine, Alzheimer Disease, Drug Discovery, medicine, Humans, Allele, Adverse effect, education, Bexarotene, education.field_of_study, General Medicine, 030104 developmental biology, 030217 neurology & neurosurgery, medicine.drug
Abstract

Alzheimer's disease (AD) is a progressive neurodegenerative disease characterized by amyloid plaques, composed of amyloid-beta peptide (Aβ) and neurofibrillary tangles, composed of aberrantly phosphorylated tau. APOE4 is the greatest genetic risk factor for AD, increasing risk up to 12- fold with a double allele compared to APOE3. In contrast, APOE2 reduces AD risk ~2-fold per allele. Accumulating evidence demonstrates that apolipoprotein E4 (apoE4) plays a multifactorial role in AD pathogenesis, although the exact mechanisms remain unclear. Further data support roles for apoE4 as a toxic gain of function or loss of positive function in AD, a discrepancy that has significant implications for the future of apoE-directed therapeutics. However, recent evidence repurposing retinoid X receptor (RXR) agonists, or rexinoids, for the treatment of AD demonstrates conflicting, though potentially beneficial effects in familial AD-transgenic (FAD-Tg) mouse models. Of particular note is bexarotene (Targretin®), a selective rexinoid previously utilized in cancer treatment emerging as a viable candidate for AD clinical trials. However, the mechanism of action of bexarotene and similar rexinoids remains controversial, particularly in the context of human APOE. In addition, rexinoids demonstrate distinct adverse event profiles in humans that may have greater detrimental effects in an elderly AD population. Therefore, this special issue review discusses the implications for rexinoiddirected therapeutic strategies in AD, the potential mechanistic targets, and future directions for the improvement of rexinoid-based therapies in AD.

Published
2017

44. Design and Synthesis of Basic Selective Estrogen Receptor Degraders for Endocrine Therapy Resistant Breast Cancer

Author

Yunlong Lu, Donghong He, Fei Huang, Yangfeng Li, Jiong Zhao, Michael A. Hollas, Sue Lee, Huiping Zhao, Carlo I. Rosales, Jesse Gordon-Blake, Rui Xiong, Oleksii Dubrovyskyii, Zhengnan Shen, Yue-Ting Wang, Gregory R. J. Thatcher, Amy W. Lasek, Debra A. Tonetti, Katherine Dye, Hu Chen, and Lauren M. Gutgesell

Subjects
Selective Estrogen Receptor Modulators, Estrogen receptor, Mice, Nude, Apoptosis, Breast Neoplasms, Thiophenes, 01 natural sciences, Article, Rats, Sprague-Dawley, 03 medical and health sciences, Mice, Breast cancer, Drug Discovery, medicine, Tumor Cells, Cultured, Potency, Animals, Humans, Tissue Distribution, 030304 developmental biology, Cell Proliferation, 0303 health sciences, Fulvestrant, Cell growth, Chemistry, Aromatase Inhibitors, Estrogen Receptor alpha, medicine.disease, Metastatic breast cancer, Xenograft Model Antitumor Assays, 0104 chemical sciences, Rats, Mice, Inbred C57BL, 010404 medicinal & biomolecular chemistry, Drug Resistance, Neoplasm, Drug Design, Mutation, Proteolysis, Cancer research, Molecular Medicine, Female, Estrogen receptor alpha, medicine.drug
Abstract

The clinical steroidal selective estrogen receptor (ER) degrader (SERD), fulvestrant, is effective in metastatic breast cancer, but limited by poor pharmacokinetics, prompting the development of orally bioavailable, nonsteroidal SERDs, currently in clinical trials. These trials address local breast cancer as well as peripheral metastases, but patients with brain metastases are generally excluded because of the lack of blood-brain barrier penetration. A novel family of benzothiophene SERDs with a basic amino side arm (B-SERDs) was synthesized. Proteasomal degradation of ERα was induced by B-SERDs that achieved the objectives of oral and brain bioavailability, while maintaining high affinity binding to ERα and both potency and efficacy comparable to fulvestrant in cell lines resistant to endocrine therapy or bearing ESR1 mutations. A novel 3-oxyazetidine side chain was designed, leading to 37d, a B-SERD that caused endocrine-resistant ER+ tumors to regress in a mouse orthotopic xenograft model.

Published
2019

45. G1T48, an oral selective estrogen receptor degrader, and the CDK4/6 inhibitor lerociclib inhibit tumor growth in animal models of endocrine-resistant breast cancer

Author

Lauren M. Gutgesell, Kendall A. Heetderks, Jay C. Strum, Delita A. Thompson, John D. Norris, Rui Xiong, Debra A. Tonetti, Christina A. Chao, John E. Bisi, Suzanne E. Wardell, Kaitlyn Andreano, Jennifer G. Baker, Robert Baldi, Taylor K. Desautels, Jessica A. Sorrentino, Jiong Zhao, Gregory R. J. Thatcher, and Yeeun Bae

Subjects
0301 basic medicine, Selective Estrogen Receptor Modulators, Cancer Research, Neoplasms, Hormone-Dependent, Estrogen receptor, Apoptosis, Breast Neoplasms, Palbociclib, HIV Antibodies, G1T48, Antibodies, Monoclonal, Humanized, CDK4/6 inhibitor, 03 medical and health sciences, Mice, 0302 clinical medicine, Breast cancer, Preclinical Study, In vivo, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, Selective estrogen receptor degrader, Medicine, Animals, Humans, Protein Kinase Inhibitors, Cell Proliferation, Fulvestrant, business.industry, Estrogen Antagonists, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, medicine.disease, Antiestrogen, Xenograft Model Antitumor Assays, Tamoxifen, 030104 developmental biology, Oncology, Mechanism of action, Receptors, Estrogen, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Female, Combination therapies, medicine.symptom, business, Endocrine-resistant breast cancer, medicine.drug
Abstract

Purpose The combination of targeting the CDK4/6 and estrogen receptor (ER) signaling pathways with palbociclib and fulvestrant is a proven therapeutic strategy for the treatment of ER-positive breast cancer. However, the poor physicochemical properties of fulvestrant require monthly intramuscular injections to patients, which limit the pharmacokinetic and pharmacodynamic activity of the compound. Therefore, an orally available compound that more rapidly reaches steady state may lead to a better clinical response in patients. Here, we report the identification of G1T48, a novel orally bioavailable, non-steroidal small molecule antagonist of ER. Methods The pharmacological effects and the antineoplastic mechanism of action of G1T48 on tumors was evaluated using human breast cancer cells (in vitro) and xenograft efficacy models (in vivo). Results G1T48 is a potent and efficacious inhibitor of estrogen-mediated transcription and proliferation in ER-positive breast cancer cells, similar to the pure antiestrogen fulvestrant. In addition, G1T48 can effectively suppress ER activity in multiple models of endocrine therapy resistance including those harboring ER mutations and growth factor activation. In vivo, G1T48 has robust antitumor activity in a model of estrogen-dependent breast cancer (MCF7) and significantly inhibited the growth of tamoxifen-resistant (TamR), long-term estrogen-deprived (LTED) and patient-derived xenograft tumors with an increased response being observed with the combination of G1T48 and the CDK4/6 inhibitor lerociclib. Conclusions These data show that G1T48 has the potential to be an efficacious oral antineoplastic agent in ER-positive breast cancer.

Published
2019

46. Time-Gated Detection of Cystathionine γ-Lyase Activity and Inhibition with a Selective, Luminogenic Hydrogen Sulfide Sensor

Author

Terry W. Moore, Tom G. Driver, Kiira Ratia, Gregory R. J. Thatcher, Chen Kong, Lawrence W. Miller, Liang Yin, Atul D. Jain, and Yao Yao

Subjects
Lanthanide, Magnetic Resonance Spectroscopy, Sulfide, Hydrogen sulfide, 010402 general chemistry, Photochemistry, Lanthanoid Series Elements, 01 natural sciences, Article, Catalysis, Hydrogen sulfide sensor, chemistry.chemical_compound, Europium, Selective reduction, Hydrogen Sulfide, chemistry.chemical_classification, Luminescent Agents, 010405 organic chemistry, Chemistry, Organic Chemistry, Cystathionine gamma-Lyase, General Chemistry, High-Throughput Screening Assays, 0104 chemical sciences, Luminescent Measurements, Amine gas treating, Azide, Luminescence
Abstract

Herein, we report the design, synthesis, and characterization of a lanthanideIII complex-based probe for the time-gated luminescence detection of hydrogen sulfide (H2 S) in aqueous media. The probe's unique sensing mechanism relies on the selective reduction of azide to amine by sulfide, followed by intramolecular cyclization to form a quinolinone. The quinolinone is a sensitizer that absorbs near-UV light and transfers excitation energy to coordinated TbIII or EuIII ions to trigger a strong "turn-on" luminescence response with ms-scale lifetimes characteristic of lanthanide complexes. Using this probe, we developed a robust, high throughput screening (HTS) assay for detecting H2 S generated by cystathionine γ-lyase (CSE), one of the main producers of H2 S in mammalian cells. In a 240-compound screen to identify potential CSE inhibitors, the EuIII analogue of the sensor showed a low false-positive rate and high Z'-factor (>0.7).

Published
2016

47. Targeting NO/cGMP Signaling in the CNS for Neurodegeneration and Alzheimer’s Disease

Author

Gregory R. J. Thatcher, Sue H. Lee, Brian M. Bennett, and Manel Ben Aissa

Subjects
Central Nervous System, 0301 basic medicine, MAPK/ERK pathway, Biology, Nitric Oxide, CREB, Biochemistry, Neuroprotection, 03 medical and health sciences, Soluble Guanylyl Cyclase, Alzheimer Disease, Ca2+/calmodulin-dependent protein kinase, Drug Discovery, medicine, Humans, Cyclic GMP, Pharmacology, Neuronal Plasticity, Phosphoric Diester Hydrolases, Organic Chemistry, Neurodegeneration, Neurodegenerative Diseases, medicine.disease, CREB-Binding Protein, 030104 developmental biology, Synapses, Immunology, Synaptic plasticity, biology.protein, Molecular Medicine, Signal transduction, Soluble guanylyl cyclase, Neuroscience, Signal Transduction
Abstract

cAMP-response element-binding protein (CREB) plays a central role in various aspects of central nervous system (CNS) function, ranging from the developmental stages to neuronal plasticity and survival in adult brain. Activation of CREB plays a crucial role in learning and memory and is at the convergence of multiple intracellular signaling cascades including CAMKII and MAPK. This review focuses on the important functions of nitric oxide (NO) in activating CREB via the NO receptor, soluble guanylyl cyclase (sGC), and production of the second messenger, cGMP. The involvement of the NO/cGMP signaling pathway in synaptic plasticity suggests several avenues for therapeutic intervention, and targeting early synaptic degeneration could be an attractive approach for the development of novel disease-modifying approaches to treat cognition and memory dysfunction in neurodegenerative diseases.

Published
2016

48. Cortical Proteins Associated With Cognitive Resilience in Community-Dwelling Older Persons

Author

Thomas S. Wingo, Shinya Tasaki, Gregory R. J. Thatcher, Lei Yu, Duc M. Duong, David A. Bennett, Julie A. Schneider, Aliza P. Wingo, Allan I. Levey, Nicholas T. Seyfried, Nicola Kearns, Konstantinos Arfanakis, and Philip L. De Jager

Subjects
Male, Gerontology, Vesicular Transport Proteins, Nerve Tissue Proteins, Ubiquitin-Activating Enzymes, GPI-Linked Proteins, 03 medical and health sciences, 0302 clinical medicine, Adaptation, Psychological, medicine, Humans, Dementia, Actinin, Cognitive Dysfunction, Cognitive decline, Prefrontal cortex, Adaptor Proteins, Signal Transducing, Aged, Original Investigation, Memory and aging, Aged, 80 and over, Epoxide Hydrolases, Hippocampal sclerosis, business.industry, Neuropeptides, Intracellular Signaling Peptides and Proteins, Proteins, Cognition, medicine.disease, 030227 psychiatry, Dorsolateral prefrontal cortex, Adaptor Proteins, Vesicular Transport, Psychiatry and Mental health, medicine.anatomical_structure, Female, Independent Living, Alzheimer's disease, business, 030217 neurology & neurosurgery, Molecular Chaperones
Abstract

IMPORTANCE: Identifying genes and proteins for cognitive resilience (ie, targets that may be associated with slowing or preventing cognitive decline regardless of the presence, number, or combination of common neuropathologic conditions) provides a complementary approach to developing novel therapeutics for the treatment and prevention of Alzheimer disease and related dementias. OBJECTIVE: To identify proteins associated with cognitive resilience via a proteome-wide association study of the human dorsolateral prefrontal cortex. DESIGN, SETTING, AND PARTICIPANTS: This study used data from 391 community-dwelling older persons who participated in the Religious Orders Study and the Rush Memory and Aging Project. The Religious Orders Study began enrollment January 1, 1994, and the Rush Memory and Aging Project began enrollment September 1, 1997, and data were collected and analyzed through October 23, 2019. EXPOSURES: Participants had undergone annual detailed clinical examinations, postmortem evaluations, and tandem mass tag proteomics analyses. MAIN OUTCOMES AND MEASURES: The outcome of cognitive resilience was defined as a longitudinal change in cognition over time after controlling for common age-related neuropathologic indices, including Alzheimer disease, Lewy bodies, transactive response DNA-binding protein 43, hippocampal sclerosis, infarcts, and vessel diseases. More than 8000 high abundance proteins were quantified from frozen dorsolateral prefrontal cortex tissue using tandem mass tag and liquid chromatography-mass spectrometry. RESULTS: There were 391 participants (273 women); their mean (SD) age was 79.7 (6.7) years at baseline and 89.2 (6.5) years at death. Eight cortical proteins were identified in association with cognitive resilience: a higher level of NRN1 (estimate, 0.140; SE, 0.024; P = 7.35 × 10(−9)), ACTN4 (estimate, 0.321; SE, 0.065; P = 9.94 × 10(−7)), EPHX4 (estimate, 0.198; SE, 0.042; P = 2.13 × 10(−6)), RPH3A (estimate, 0.148; SE, 0.031; P = 2.58 × 10(−6)), SGTB (estimate, 0.211; SE, 0.045; P = 3.28 × 10(−6)), CPLX1 (estimate, 0.136; SE, 0.029; P = 4.06 × 10(−6)), and SH3GL1 (estimate, 0.179; SE, 0.039; P = 4.21 × 10(−6)) and a lower level of UBA1 (estimate, −0.366; SE, 0.076; P = 1.43 × 10(−6)) were associated with greater resilience. CONCLUSIONS AND RELEVANCE: These protein signals may represent novel targets for the maintenance of cognition in old age.

Published
2020

49. Interaction of oxidative stress and neurotrauma in ALDH2 mice causes significant and persistent behavioral and pro-inflammatory effects in a tractable model of mild traumatic brain injury

Author

Sue H. Lee, Yue-Ting Wang, Kevin A. Tam, Rachel C. Knopp, Gregory R. J. Thatcher, Manel BenAissa, Emily C Pierce, Daniyal Aamir, David Gonzalez, Emily Nepomuceno, and Michael A. Hollas

Subjects
0301 basic medicine, medicine.medical_specialty, Traumatic brain injury, Lipid peroxidation, Clinical Biochemistry, Inflammation, Neuropathology, medicine.disease_cause, Biochemistry, Neuroprotection, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Neuroinflammation, Internal medicine, medicine, Mild traumatic brain injury, lcsh:QH301-705.5, Uncategorized, ALDH2, lcsh:R5-920, Drug discovery, business.industry, Organic Chemistry, medicine.disease, 030104 developmental biology, Endocrinology, lcsh:Biology (General), chemistry, Oxidative stress, medicine.symptom, lcsh:Medicine (General), business, 030217 neurology & neurosurgery
Abstract

Oxidative stress induced by lipid peroxidation products (LPP) accompanies aging and has been hypothesized to exacerbate the secondary cascade in traumatic brain injury (TBI). Increased oxidative stress is a contributor to loss of neural reserve that defines the ability to maintain healthy cognitive function despite the accumulation of neuropathology. ALDH2−/− mice are unable to clear aldehyde LPP by mitochondrial aldehyde dehydrogenase-2 (Aldh2) detoxification and provide a model to study mild TBI (mTBI), therapeutic interventions, and underlying mechanisms. The ALDH2−/− mouse model presents with elevated LPP-mediated protein modification, lowered levels of PSD-95, PGC1-α, and SOD-1, and mild cognitive deficits from 4 months of age. LPP scavengers are neuroprotective in vitro and in ALDH2−/− mice restore cognitive performance. A single-hit, closed skull mTBI failed to elicit significant effects in WT mice; however, ALDH2−/− mice showed a significant inflammatory cytokine surge in the ipsilateral hemisphere 24 h post-mTBI, and increased GFAP cleavage, a biomarker for TBI. Known neuroprotective agents, were able to reverse the effects of mTBI. This new preclinical model of mTBI, incorporating significant perturbations in behavior, inflammation, and clinically relevant biomarkers, allows mechanistic study of the interaction of LPP and neurotrauma in loss of neural reserve.

Published
2020

50. P1‐074: TISSUE‐SELECTIVE ABCA1 AGONISTS AS POTENTIAL ALZHEIMER'S DISEASE THERAPEUTICS: HIT‐TO‐LEAD OPTIMIZATION

Author

Cutler T. Lewandowski, Sue H. Lee, Manel Ben Aissa, Bhargava Karumudi, and Gregory R. J. Thatcher

Subjects
biology, Epidemiology, business.industry, Health Policy, Disease, Hit to lead, Bioinformatics, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, ABCA1, biology.protein, Medicine, Neurology (clinical), Geriatrics and Gerontology, business
Published
2018

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