Your search keyword '"Beat M. Jucker"' showing total 76 results

1. MRI/PET multimodal imaging of the innate immune response in skeletal muscle and draining lymph node post vaccination in rats

Author

Saaussan Madi, Fang Xie, Kamyar Farhangi, Chih-Yang Hsu, Shih-Hsun Cheng, Tolulope Aweda, Bhasker Radaram, Stephanie Slania, Tammy Lambert, Mary Rambo, Tina Skedzielewski, Austin Cole, Valeriia Sherina, Shannon McKearnan, Hoang Tran, Hasan Alsaid, Minh Doan, Alan H. Stokes, Derek T. O’Hagan, Giulietta Maruggi, Sylvie Bertholet, Stéphane T. Temmerman, Russell Johnson, and Beat M. Jucker

Subjects

innate immune activation, magnetic resonance imaging, positron emission tomography, self-amplifying mRNA, lipid nanoparticle, AS01, Immunologic diseases. Allergy, RC581-607

Abstract

The goal of this study was to utilize a multimodal magnetic resonance imaging (MRI) and positron emission tomography (PET) imaging approach to assess the local innate immune response in skeletal muscle and draining lymph node following vaccination in rats using two different vaccine platforms (AS01 adjuvanted protein and lipid nanoparticle (LNP) encapsulated Self-Amplifying mRNA (SAM)). MRI and 18FDG PET imaging were performed temporally at baseline, 4, 24, 48, and 72 hr post Prime and Prime-Boost vaccination in hindlimb with Cytomegalovirus (CMV) gB and pentamer proteins formulated with AS01, LNP encapsulated CMV gB protein-encoding SAM (CMV SAM), AS01 or with LNP carrier controls. Both CMV AS01 and CMV SAM resulted in a rapid MRI and PET signal enhancement in hindlimb muscles and draining popliteal lymph node reflecting innate and possibly adaptive immune response. MRI signal enhancement and total 18FDG uptake observed in the hindlimb was greater in the CMV SAM vs CMV AS01 group (↑2.3 – 4.3-fold in AUC) and the MRI signal enhancement peak and duration were temporally shifted right in the CMV SAM group following both Prime and Prime-Boost administration. While cytokine profiles were similar among groups, there was good temporal correlation only between IL-6, IL-13, and MRI/PET endpoints. Imaging mass cytometry was performed on lymph node sections at 72 hr post Prime and Prime-Boost vaccination to characterize the innate and adaptive immune cell signatures. Cell proximity analysis indicated that each follicular dendritic cell interacted with more follicular B cells in the CMV AS01 than in the CMV SAM group, supporting the stronger humoral immune response observed in the CMV AS01 group. A strong correlation between lymph node MRI T2 value and nearest-neighbor analysis of follicular dendritic cell and follicular B cells was observed (r=0.808, P

Published

2023

2. Assessing the effects of LXR agonists on cellular cholesterol handling: a stable isotope tracer study

Author

Karpagam Aravindhan, Christine L. Webb, Michael Jaye, Avijit Ghosh, Robert N. Willette, N. John DiNardo, and Beat M. Jucker

Subjects

liver X receptor, HepG2, turnover, compartmental, mass isotopomer distribution analysis, Biochemistry, QD415-436

Abstract

The liver X receptors (LXRs) α and β are responsible for the transcriptional regulation of a number of genes involved in cholesterol efflux from cells and therefore may be molecular targets for the treatment of cardiovascular disease. However, the effects of LXR ligands on cholesterol turnover in cells has not been examined comprehensively. In this study, cellular cholesterol handling (e.g., synthesis, catabolism, influx, and efflux) was examined using a stable isotope labeling study and a two-compartment modeling scheme. In HepG2 cells, the incorporation of 13C into cholesterol from [1-13C]acetate was analyzed by mass isotopomer distribution analysis in conjunction with nonsteady state, multicompartment kinetic analysis to calculate the cholesterol fluxes. Incubation with synthetic, nonsteroidal LXR agonists (GW3965, T0901317, and SB742881) increased cholesterol synthesis (∼10-fold), decreased cellular cholesterol influx (71–82%), and increased cellular cholesterol efflux (1.7- to 1.9-fold) by 96 h. As a consequence of these altered cholesterol fluxes, cellular cholesterol decreased (36–39%) by 96 h. The increased cellular cholesterol turnover was associated with increased expression of the LXR-activated genes ABCA1, ABCG1, FAS, and sterol-regulatory element binding protein 1c. In summary, the mathematical model presented allows time-dependent calculations of cellular cholesterol fluxes. These data demonstrate that all of the cellular cholesterol fluxes were altered by LXR activation and that the increase in cholesterol synthesis did not compensate for the increased cellular cholesterol efflux, resulting in a net cellular cholesterol loss.

Published

2006

3. Comparison of soluble guanylate cyclase stimulators and activators in models of cardiovascular disease associated with oxidative stress

Author

Melissa H Costell, Nicolas eAncellin, Roberta E Bernard, Shufang eZhao, John J Upson, Lisa A Morgan, Kristeen eHauk, Alan R Olzinski, Victoria L T Ballard, Kenny eHerry, Pascal eGrondin, Nerina eDodic, Olivier eMirguet, Anne eBouillot, Francoise eGellibert, Robert W Coatney, John J Lepore, Beat M. Jucker, Larry J Jolivette, Robert N Willette, Christine G Schnackenberg, and David J Behm

Subjects

cGMP, soluble guanylate cyclase, BAY 60-4552, GSK2181236A, SHR-SP, VASP, Therapeutics. Pharmacology, RM1-950

Abstract

Soluble guanylate cyclase (sGC), the primary mediator of nitric oxide (NO) bioactivity, exists as reduced (NO-sensitive) and oxidized (NO-insensitive) forms. We tested the hypothesis that the cardiovascular protective effects of NO-insensitive sGC activation would be potentiated under conditions of oxidative stress compared to NO-sensitive sGC stimulation. The cardiovascular effects of the NO-insensitive sGC activator GSK2181236A (a non-depressor dose and a higher dose which lowered mean arterial pressure [MAP] by 5-10mmHg) and equi-efficacious doses of the NO-sensitive sGC stimulator BAY 60-4552 were assessed in Sprague Dawley rats during coronary artery ischemia/reperfusion (I/R) and spontaneously hypertensive stroke prone rats (SHR-SP) on a high salt/fat diet (HSFD). In I/R, neither compound reduced infarct size. In SHR-SP, HSFD increased MAP, urine output, microalbuminuria and mortality, caused left ventricular hypertrophy and impaired endothelium-dependent vasorelaxation. The low dose of BAY 60-4552 but not GSK2181236A decreased urine output and mortality. Conversely, the low dose of GSK2181236A attenuated cardiac hypertrophy. The high doses of both compounds similarly attenuated cardiac hypertrophy and mortality. In addition, the high dose of BAY 60-4552 reduced urine output, microalbuminuria and MAP. Neither compound improved endothelium-dependent vasorelaxation. In SHR-SP aorta, the vasodilatory responses to the NO-dependent compounds carbachol and sodium nitroprusside were attenuated by HSFD. In contrast, the vasodilatory responses to GSK2181236A and BAY 60-4552 were unaltered by HSFD, indicating that reduced NO-bioavailability and not changes in the sGC oxidative state is responsible for the vascular dysfunction. In summary, GSK2181236A and BAY 60-4552 provide partial benefit against hypertension-induced end organ damage. The differential beneficial effects observed between these compounds could reflect tissue-specific changes in the sGC oxidative state.

Published

2012

4. Multimodal imaging distribution assessment of a liposomal antibiotic in an infectious disease model

Author

Shih-Hsun Cheng, M. Reid Groseclose, Cindy Mininger, Mats Bergstrom, Lily Zhang, Stephen C. Lenhard, Tinamarie Skedzielewski, Zachary D. Kelley, Debra Comroe, Hyundae Hong, Haifeng Cui, Jennifer L. Hoover, Steve Rittenhouse, Stephen Castellino, Beat M. Jucker, and Hasan Alsaid

Subjects

Mice, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Positron-Emission Tomography, Liposomes, Animals, Humans, Pharmaceutical Science, Tissue Distribution, Multimodal Imaging, Lipids, Communicable Diseases, Anti-Bacterial Agents

Abstract

Liposomes are promising targeted drug delivery systems with the potential to improve the efficacy and safety profile of certain classes of drugs. Though attractive, there are unique analytical challenges associated with the development of liposomal drugs including human dose prediction given these are multi-component drug delivery systems. In this study, we developed a multimodal imaging approach to provide a comprehensive distribution assessment for an antibacterial drug, GSK2485680, delivered as a liposomal formulation (Lipo680) in a mouse thigh model of bacterial infection to support human dose prediction. Positron emission tomography (PET) imaging was used to track the in vivo biodistribution of Lipo680 over 48 h post-injection providing a clear assessment of the uptake in various tissues and, importantly, the selective accumulation at the site of infection. In addition, a pharmacokinetic model was created to evaluate the kinetics of Lipo680 in different tissues. Matrix-assisted laser desorption/ionization (MALDI) imaging mass spectrometry (IMS) was then used to quantify the distribution of GSK2485680 and to qualitatively assess the distribution of a liposomal lipid throughout sections of infected and non-infected hindlimb tissues at high spatial resolution. Through the combination of both PET and MALDI IMS, we observed excellent correlation between the Lipo680-radionuclide signal detected by PET with the GSK2485680 and lipid component signals detected by MALDI IMS. This multimodal translational method can reduce drug attrition by generating comprehensive biodistribution profiles of drug delivery systems to provide mechanistic insight and elucidate safety concerns. Liposomal formulations have potential to deliver therapeutics across a broad array of different indications, and this work serves as a template to aid in delivering future liposomal drugs to the clinic.

Published

2022

5. Immuno-PET Monitoring of CD8+ T Cell Infiltration Post ICOS Agonist Antibody Treatment Alone and in Combination with PD-1 Blocking Antibody Using a 89Zr Anti-CD8+ Mouse Minibody in EMT6 Syngeneic Tumor Mouse

Author

Hasan Alsaid, Shih-Hsun Cheng, Meixia Bi, Fang Xie, Mary Rambo, Tinamarie Skedzielewski, Bao Hoang, Sunish Mohanan, Debra Comroe, Andrew Gehman, Chih-Yang Hsu, Kamyar Farhangi, Hoang Tran, Valeriia Sherina, Minh Doan, M. Reid Groseclose, Christopher B. Hopson, Sara Brett, Ian A. Wilson, Andrew Nicholls, Marc Ballas, Jeremy D. Waight, and Beat M. Jucker

Subjects

Cancer Research, Oncology, Radiology, Nuclear Medicine and imaging

Abstract

Purpose The presence and functional competence of intratumoral CD8+ T cells is often a barometer for successful immunotherapeutic responses in cancer. Despite this understanding and the extensive number of clinical-stage immunotherapies focused on potentiation (co-stimulation) or rescue (checkpoint blockade) of CD8+ T cell antitumor activity, dynamic biomarker strategies are often lacking. To help fill this gap, immuno-PET nuclear imaging has emerged as a powerful tool for in vivo molecular imaging of antibody targeting. Here, we took advantage of immuno-PET imaging using 89Zr-IAB42M1-14, anti-mouse CD8 minibody, to characterize CD8+ T-cell tumor infiltration dynamics following ICOS (inducible T-cell co-stimulator) agonist antibody treatment alone and in combination with PD-1 blocking antibody in a model of mammary carcinoma. Procedures. Female BALB/c mice with established EMT6 tumors received 10 µg, IP of either IgG control antibodies, ICOS agonist monotherapy, or ICOS/PD-1 combination therapy on days 0, 3, 5, 7, 9, 10, or 14. Imaging was performed at 24 and 48 h post IV dose of 89Zr IAB42M1-14. In addition to 89Zr-IAB42M1-14 uptake in tumor and tumor-draining lymph node (TDLN), 3D radiomic features were extracted from PET/CT images to identify treatment effects. Imaging mass cytometry (IMC) and immunohistochemistry (IHC) was performed at end of study. Results 89Zr-IAB42M1-14 uptake in the tumor was observed by day 11 and was preceded by an increase in the TDLN as early as day 4. The spatial distribution of 89Zr-IAB42M1-14 was more uniform in the drug treated vs. control tumors, which had spatially distinct tracer uptake in the periphery relative to the core of the tumor. IMC analysis showed an increased percentage of cytotoxic T cells in the ICOS monotherapy and ICOS/PD-1 combination group compared to IgG controls. Additionally, temporal radiomics analysis demonstrated early predictiveness of imaging features. Conclusion To our knowledge, this is the first detailed description of the use of a novel immune-PET imaging technique to assess the kinetics of CD8+ T-cell infiltration into tumor and lymphoid tissues following ICOS agonist and PD-1 blocking antibody therapy. By demonstrating the capacity for increased spatial and temporal resolution of CD8+ T-cell infiltration across tumors and lymphoid tissues, these observations underscore the widespread potential clinical utility of non-invasive PET imaging for T-cell-based immunotherapy in cancer.

Published

2022

6. Concordance between alizarin red stained skeleton and <scp>micro‐CT</scp> skeleton evaluation methods: A case study in New Zealand White rabbits

Author

Howard M. Solomon, Stacia Murzyn, Joyce Rendemonti, Sharon Chapman, Shih‐Hsun Cheng, Beat M. Jucker, Dinesh Stanislaus, Andrew Gehman, and Hasan Alsaid

Subjects

Embryology, Health, Toxicology and Mutagenesis, Pediatrics, Perinatology and Child Health, Toxicology, Developmental Biology

Published

2023

7. Supplementary Material from Characterization of a Novel PERK Kinase Inhibitor with Antitumor and Antiangiogenic Activity

Author

Rakesh Kumar, Jeffrey M. Axten, Beat M. Jucker, Hasan Alsaid, Anthony E. Choudhry, Nathan Gaul, Aaron Goetz, Brent Sanders, Thomas B. Stanley, Katherine Moss, David J. Figueroa, Shu-Yun Zhang, Elisabeth Minthorn, Qi Liu, and Charity Atkins

Abstract

Supplementary Material PDF file - 147K, Supplementary Methods: Immunohistochemistry and magnetic resonance imaging. Supplementary Table 1: Kinase selectivity profiling of GSK2656157. Supplementary Table 2: Gene list for Human UPR array

Published

2023

8. Supplementary Figures 1-3 from Characterization of a Novel PERK Kinase Inhibitor with Antitumor and Antiangiogenic Activity

Author

Rakesh Kumar, Jeffrey M. Axten, Beat M. Jucker, Hasan Alsaid, Anthony E. Choudhry, Nathan Gaul, Aaron Goetz, Brent Sanders, Thomas B. Stanley, Katherine Moss, David J. Figueroa, Shu-Yun Zhang, Elisabeth Minthorn, Qi Liu, and Charity Atkins

Abstract

Supplementary Figures 1-3 PDF file - 245K, Supplementary Figure 1: Dose-dependent pharmacodynamic effect of GSK2656157 on PERK in mouse pancreas. Supplementary Figure 2: Specificity of phospho-PERK antibody in mouse cells. Supplementary Figure 3: Effect of PERK inhibitor on RNA expression in tumor xenografts.

Published

2023

9. A multi-center preclinical study of gadoxetate DCE-MRI in rats as a biomarker of drug induced inhibition of liver transporter function.

Author

Anastassia Karageorgis, Stephen C Lenhard, Brittany Yerby, Mikael F Forsgren, Serguei Liachenko, Edvin Johansson, Mark A Pilling, Richard A Peterson, Xi Yang, Dominic P Williams, Sharon E Ungersma, Ryan E Morgan, Kim L R Brouwer, Beat M Jucker, and Paul D Hockings

Subjects

Medicine, Science

Abstract

Drug-induced liver injury (DILI) is a leading cause of acute liver failure and transplantation. DILI can be the result of impaired hepatobiliary transporters, with altered bile formation, flow, and subsequent cholestasis. We used gadoxetate dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI), combined with pharmacokinetic modelling, to measure hepatobiliary transporter function in vivo in rats. The sensitivity and robustness of the method was tested by evaluating the effect of a clinical dose of the antibiotic rifampicin in four different preclinical imaging centers. The mean gadoxetate uptake rate constant for the vehicle groups at all centers was 39.3 +/- 3.4 s-1 (n = 23) and 11.7 +/- 1.3 s-1 (n = 20) for the rifampicin groups. The mean gadoxetate efflux rate constant for the vehicle groups was 1.53 +/- 0.08 s-1 (n = 23) and for the rifampicin treated groups was 0.94 +/- 0.08 s-1 (n = 20). Both the uptake and excretion transporters of gadoxetate were statistically significantly inhibited by the clinical dose of rifampicin at all centers and the size of this treatment group effect was consistent across the centers. Gadoxetate is a clinically approved MRI contrast agent, so this method is readily transferable to the clinic. CONCLUSION:Rate constants of gadoxetate uptake and excretion are sensitive and robust biomarkers to detect early changes in hepatobiliary transporter function in vivo in rats prior to established biomarkers of liver toxicity.

Published

2018

10. Non invasive imaging assessment of the biodistribution of GSK2849330, an ADCC and CDC optimized anti HER3 mAb, and its role in tumor macrophage recruitment in human tumor-bearing mice.

Author

Hasan Alsaid, Tinamarie Skedzielewski, Mary V Rambo, Kristen Hunsinger, Bao Hoang, William Fieles, Edward R Long, James Tunstead, Danielle J Vugts, Matthew Cleveland, Neil Clarke, Christopher Matheny, and Beat M Jucker

Subjects

Medicine, Science

Abstract

The purpose of this work was to use various molecular imaging techniques to non-invasively assess GSK2849330 (anti HER3 ADCC and CDC enhanced 'AccretaMab' monoclonal antibody) pharmacokinetics and pharmacodynamics in human xenograft tumor-bearing mice. Immuno-PET biodistribution imaging of radiolabeled 89Zr-GSK2849330 was assessed in mice with HER3 negative (MIA-PaCa-2) and positive (CHL-1) human xenograft tumors. Dose dependency of GSK2849330 disposition was assessed using varying doses of unlabeled GSK2849330 co-injected with 89Zr-GSK2849330. In-vivo NIRF optical imaging and ex-vivo confocal microscopy were used to assess the biodistribution of GSK2849330 and the HER3 receptor occupancy in HER3 positive xenograft tumors (BxPC3, and CHL-1). Ferumoxytol (USPIO) contrast-enhanced MRI was used to investigate the effects of GSK2849330 on tumor macrophage content in CHL-1 xenograft bearing mice. Immuno-PET imaging was used to monitor the whole body drug biodistribution and CHL-1 xenograft tumor uptake up to 144 hours post injection of 89Zr-GSK2849330. Both hepatic and tumor uptake were dose dependent and saturable. The optical imaging data in the BxPC3 xenograft tumor confirmed the tumor dose response finding in the Immuno-PET study. Confocal microscopy showed a distinguished cytoplasmic punctate staining pattern within individual CHL-1 cells. GSK2849330 inhibited tumor growth and this was associated with a significant decrease in MRI signal to noise ratio after USPIO injection and with a significant increase in tumor macrophages as confirmed by a quantitative immunohistochemistry analysis. By providing both dose response and time course data from both 89Zr and fluorescently labeled GSK2849330, complementary imaging studies were used to characterize GSK2849330 biodistribution and tumor uptake in vivo. Ferumoxytol-enhanced MRI was used to monitor aspects of the immune system response to GSK2849330. Together these approaches potentially provide clinically translatable, non-invasive techniques to support dose optimization, and assess immune activation and anti-tumor responses.

Published

2017

11. Apoptosis signal-regulating kinase 1 inhibition attenuates cardiac hypertrophy and cardiorenal fibrosis induced by uremic toxins: Implications for cardiorenal syndrome.

Author

Feby Savira, Longxing Cao, Ian Wang, Wendi Yang, Kevin Huang, Yue Hua, Beat M Jucker, Robert N Willette, Li Huang, Henry Krum, Zhiliang Li, Qiang Fu, and Bing Hui Wang

Subjects

Medicine, Science

Abstract

Intracellular accumulation of protein-bound uremic toxins in the setting of cardiorenal syndrome leads to adverse effects on cardiorenal cellular functions, where cardiac hypertrophy and cardiorenal fibrosis are the hallmarks. In this study, we sought to determine if Apoptosis Signal-Regulated Kinase 1 (ASK1), an upstream regulator of cellular stress response, mediates cardiac hypertrophy and cardiorenal fibrosis induced by indoxyl sulfate (IS) and p-cresol sulfate (PCS) in vitro, and whether ASK1 inhibition is beneficial to ameliorate these cellular effects. PCS augmented cardiac myocyte hypertrophy and fibroblast collagen synthesis (as determined by 3H-leucine and 3H-proline incorporation, respectively), similar to our previous finding with IS. IS and PCS also increased collagen synthesis of proximal tubular cells and renal mesangial cells. Pro-hypertrophic (α-skeletal muscle actin and β-MHC) and pro-fibrotic genes (TGF-β1 and ctgf) were induced by both IS and PCS. Western blot analyses revealed the activation of ASK1 and downstream mitogen activated protein kinases (MAPKs) (p38MAPK and ERK1/2) as well as nuclear factor-kappa B (NF-κB) by IS and PCS. ASK1, OAT1/3, ERK1/2 and p38MAPK inhibitors suppressed all these effects. In summary, IS and PCS exhibit pro-hypertrophic and pro-fibrotic properties, at least in part, via the activation of ASK1 and its downstream pathways. ASK1 inhibitor is an effective therapeutic agent to alleviate protein-bound uremic toxin-induced cardiac hypertrophy and cardiorenal fibrosis in vitro, and may be translated further for cardiorenal syndrome therapy.

Published

2017

12. A Multimodal Imaging Approach to Assess the Quantitative Biodistribution of a Liposomal Nanoformulation with the antibiotic GSK2485680 (Lipo680)

Author

Shih-Hsun Cheng, Reid Groseclose, Cindy Mininger, Mats Bergstrom, Lily Zhang, Steve C. Lenhard, Tinamarie Skedzielewski, Debra Comroe, Hyundae Hong, Haifeng Cui, Jennifer L. Hoover, Steve Rittenhouse, Stephen Castellino, Beat M. Jucker, and Hasan Alsaid

Abstract

Liposomes are promising targeted drug delivery systems with the potential to improve the efficacy and safety profile of certain classes of drugs. Though attractive, there are unique analytical challenges associated with the development of liposomal drugs including human dose prediction given these are multi-component drug delivery systems. In this study, we developed a multimodal imaging approach to provide a comprehensive distribution assessment for an antibacterial drug, GSK2485680, delivered as a liposomal formulation (Lipo680) in a mouse thigh model of bacterial infection to support human dose prediction. Positron emission tomography (PET) imaging was used to track the in vivo biodistribution of Lipo680 over 48h post-injection providing a clear assessment of the uptake in various tissues and, importantly, the selective accumulation at the site of infection. In addition, a pharmacokinetic model was created to evaluate the kinetics of Lipo680 in different tissues. Matrix-assisted laser desorption/ionization (MALDI) imaging mass spectrometry (IMS) was then used to analyze and quantify the distribution of GSK2485680 and a liposomal lipid throughout sections of infected and non-infected thigh tissues at high spatial resolution. Through the combination of both PET and MALDI images, we observed an excellent correlation between the Lipo680-radionuclide signal from PET with GSK2485680 and lipid component signals from MALDI IMS. This multimodal translational method can reduce drug attrition by providing comprehensive biodistribution profiles of drug delivery systems to provide mechanistic insight and elucidate safety concerns. Liposomal formulations have broad potential to deliver therapeutics for other indications, and this work serves as a template to aid in delivering future liposomal drugs to the clinic.

Published

2022

13. Inhibition of apoptosis signal-regulating kinase 1 ameliorates left ventricular dysfunction by reducing hypertrophy and fibrosis in a rat model of cardiorenal syndrome

Author

Bing Hui Wang, Amanda J. Edgley, Robert N. Willette, Feby Savira, Andrew R Kompa, Beat M. Jucker, Henry Krum, and Darren J. Kelly

Subjects

medicine.medical_specialty, business.industry, Renal function, Cardiorenal syndrome, 030204 cardiovascular system & hematology, medicine.disease, Muscle hypertrophy, 03 medical and health sciences, Preload, 0302 clinical medicine, Fibrosis, Cardio-Renal Syndrome, Internal medicine, medicine, Cardiology, Myocyte, 030212 general & internal medicine, Myocardial infarction, Cardiology and Cardiovascular Medicine, business

Abstract

Background Cardiorenal syndrome (CRS) is a major health burden worldwide in need of novel therapies, as current treatments remain suboptimal. The present study assessed the therapeutic potential of apoptosis signal-regulating kinase 1 (ASK1) inhibition in a rat model of CRS. Methods Adult male Sprague-Dawley rats underwent surgery for myocardial infarction (MI) (week 0) followed by 5/6 subtotal nephrectomy (STNx) at week 4 to induce to induce a combined model of heart and kidney dysfunction. At week 6, MI + STNx animals were randomized to receive either 0.5% carboxymethyl cellulose (Vehicle, n = 15, Sham = 10) or G226 (15 mg/kg daily, n = 11). Cardiac and renal function was assessed by echocardiography and glomerular filtration rate (GFR) respectively, prior to treatment at week 6 and endpoint (week 14). Haemodynamic measurements were determined at endpoint prior to tissue analysis. Results G226 treatment attenuated the absolute change in left ventricular (LV) fractional shortening and posterior wall thickness compared to Vehicle. G226 also attenuated the reduction in preload recruitable stroke work. Increased myocyte cross sectional area, cardiac interstitial fibrosis, immunoreactivity of cardiac collagen-I and III and cardiac TIMP-2 activation, were significantly reduced following G226 treatment. Although we did not observe improvement in GFR, G226 significantly reduced renal interstitial fibrosis, diminished renal collagen-I and -IV, kidney injury molecule-1 immunoreactivity as well as macrophage infiltration and SMAD2 phosphorylation. Conclusion Inhibition of ASK1 ameliorated LV dysfunction and diminished cardiac hypertrophy and cardiorenal fibrosis in a rat model of CRS. This suggests that ASK1 is a critical pathway with therapeutic potential in the CRS setting.

Published

2020

14. Cardioprotection Resulting from Glucagon-Like Peptide-1 Administration Involves Shifting Metabolic Substrate Utilization to Increase Energy Efficiency in the Rat Heart.

Author

Karpagam Aravindhan, Weike Bao, Mark R Harpel, Robert N Willette, John J Lepore, and Beat M Jucker

Subjects

Medicine, Science

Abstract

Previous studies have shown that glucagon-like peptide-1 (GLP-1) provides cardiovascular benefits independent of its role on peripheral glycemic control. However, the precise mechanism(s) by which GLP-1 treatment renders cardioprotection during myocardial ischemia remain unresolved. Here we examined the role for GLP-1 treatment on glucose and fatty acid metabolism in normal and ischemic rat hearts following a 30 min ischemia and 24 h reperfusion injury, and in isolated cardiomyocytes (CM). Relative carbohydrate and fat oxidation levels were measured in both normal and ischemic hearts using a 1-13C glucose clamp coupled with NMR-based isotopomer analysis, as well as in adult rat CMs by monitoring pH and O2 consumption in the presence of glucose or palmitate. In normal heart, GLP-1 increased glucose uptake (↑64%, p

Published

2015

15. Multiparametric magnetic resonance imaging to characterize cabotegravir long-acting formulation depot kinetics in healthy adult volunteers

Author

Jafar Sadik Shaik, Valeriu Damian, Katarzyna J. Macura, Susan L. Ford, Paul Galette, Kalpana Bakshi, Craig W. Hendrix, Michael A. Jacobs, Meiyappan Solaiyappan, Robert L. Janiczek, Sarah Lee, Manish Gupta, William Spreen, Beat M. Jucker, Edward J. Fuchs, Kelong Han, Ethel D. Weld, Parul Patel, Ronald D'Amico, and David A. Margolis

Subjects

Adult, Male, Volunteers, Depot, Anti-HIV Agents, Pyridones, Cmax, Adipose tissue, HIV Infections, Diketopiperazines, Injections, Intramuscular, chemistry.chemical_compound, Cabotegravir, Pharmacokinetics, medicine, Distribution (pharmacology), Humans, Pharmacology (medical), Multiparametric Magnetic Resonance Imaging, Gluteal muscles, Compartment (pharmacokinetics), Pharmacology, business.industry, Kinetics, medicine.anatomical_structure, chemistry, Female, business, Nuclear medicine

Abstract

Aim Cabotegravir long-acting (LA) intramuscular (IM) injection is being investigated for HIV preexposure prophylaxis due to its potent antiretroviral activity and infrequent dosing requirement. A subset of healthy adult volunteers participating in a phase I study assessing cabotegravir tissue pharmacokinetics underwent serial magnetic resonance imaging (MRI) to assess drug depot localization and kinetics following a single cabotegravir LA IM targeted injection. Methods Eight participants (four men, four women) were administered cabotegravir LA 600 mg under ultrasonographic-guided injection targeting the gluteal muscles. MRI was performed to determine injection-site location in gluteal muscle (IM), subcutaneous (SC) adipose tissue, and combined IM/SC compartments and to quantify drug depot characteristics, including volume and surface area, on Days 1 (≤2 hours postinjection), 3, and 8. Linear regression analysis examined correlations between MRI-derived parameters and plasma cabotegravir exposure metrics, including maximum observed concentration (Cmax ) and partial area under the concentration-time curve (AUC) through Weeks 4 and 8. Results Cabotegravir LA depot locations varied by participant and were identified in the IM compartment (n=2), combined IM/SC compartments (n=4), SC compartment (n=1), and retroperitoneal cavity (n=1). Although several MRI parameter and exposure metric correlations were determined, total depot surface area on Day 1 strongly correlated with plasma cabotegravir concentration at Days 3 and 8, Cmax , and partial AUC through Weeks 4 and 8. Conclusion MRI clearly delineated cabotegravir LA injection-site location and depot kinetics in healthy adults. Although injection-site variability was observed, drug depot surface area correlated with both plasma Cmax and partial AUC independently of anatomical distribution.

Published

2021

16. RE: Inhibition of apoptosis signal-regulating kinase 1 might be a novel therapeutic target in the treatment of cardiorenal syndrome

Author

Beat M. Jucker, Darren J. Kelly, Henry Krum, Robert N. Willette, Feby Savira, Bing Hui Wang, Andrew R Kompa, and Amanda J. Edgley

Subjects

Cardio-Renal Syndrome, Kinase, business.industry, Cardiorenal syndrome, medicine.disease, MAP Kinase Kinase Kinase 5, Fibrosis, Muscle hypertrophy, Text mining, Apoptosis, medicine, Cancer research, Humans, Cardiology and Cardiovascular Medicine, business

Published

2020

17. Abstract 2816: Immuno-PET monitoring of CD8+ T cell infiltration post anti-ICOS agonist antibody treatment alone and in combination with PD-1 blocking antibody using a 89Zr anti-CD8+ mouse minibody in EMT 6 syngeneic tumor mouse

Author

Chih-Yang Hsu, Fang Xie, Sunish Mohanan, Sara Brett, Axel Hoos, Bao Hoang, Tinamarie Skedzielewski, Jeremy D. Waight, Hasan Alsaid, Meixia Bi, Minh Doan, M. Reid Groseclose, Andrew Gehman, Shih-Hsun Cheng, Mary V. Rambo, Marc S. Ballas, Christopher B. Hopson, Andrew Nicholls, Ian A. Wilson, and Beat M. Jucker

Subjects

Agonist, Cancer Research, biology, Chemistry, medicine.drug_class, Syngeneic tumor, medicine.disease, Oncology, Blocking antibody, Cancer research, medicine, biology.protein, Cytotoxic T cell, Antibody, Infiltration (medical), CD8, Immuno pet

Abstract

Introduction Inducible T cell co-stimulator (ICOS) is a co-stimulatory receptor that is important for promoting immune activation and function. Despite reported clinical activity and a wide range of non-clinical studies supporting a role for ICOS in lymphocyte activation, proliferation and pro-inflammatory cytokine secretion, little is known regarding the potential of monoclonal agonist antibody-mediated ICOS signaling to drive cytotoxic T cell infiltration into tumors. Feladilimab (GSK3359609) is a non-depleting IgG4 ICOS agonist antibody currently being evaluated in pivotal clinical trials. Here, we used PET/CT imaging to evaluate CD8+ T cell infiltration following treatment with a rodent surrogate of feladilimab (7E.17G9 mouse [m] IgG1) alone or in combination with anti-PD-1 mAb (RMP-14 rat IgG2a) in a syngeneic model of breast cancer (EMT6). Method Female BALB/c mice with established tumors (~150 mm3) received 10µg, IP of either IgG control mAbs, ICOS mAb, or ICOS + PD-1 mAbs on day 0, 3, 5, 7, 9, 10, or 14. Imaging was performed at 24 & 48 hrs post IV dose of 89Zr labeled CD8 minibody (IAB42M1-14, ImaginAb, CA) on day 0, 3, 5, 9, or 14. In addition to the CD8 minibody uptake in tumor & tumor-draining lymph node (TDLN), 3D radiomic features were extracted from PET/CT images. Top ranked features were used for hierarchical clustering to identify treatment effects. Results Tumor size regressed in all treated groups relative to IgG control, with a number of mice clearing tumors (ICOS: 4 mice, ICOS + PD-1: 9 mice). The in vivo uptake of CD8 minibody in TDLN was significantly higher in the ICOS + PD-1 group on day 4, 6, & 7 relative to IgG control P Conclusions Herein, we demonstrated for the first time that treatment of tumor-bearing mice with ICOS agonist mAb alone or in combination with PD-1 blockade can increase CD8+ T cell infiltration into tumors & TDLN, and is correlated with reduced tumor burden. Notably, radiomics features predicted an effect of treatment on CD8+ T cell infiltration earlier than the detection of absolute changes in the CD8 minibody uptake in tumor & TDLN. Overall, these data support the ongoing pivotal investigation of feladilimab. Moreover, this translational imaging method may be a useful tool to non-invasively monitor CD8+ T cell in response to immunotherapies and understand the temporal relationship between CD8+ T cell flux in tumor and in TDLN. Citation Format: Hasan Alsaid, Shih-Hsun Cheng, Meixia Bi, Mary V. Rambo, Tinamarie Skedzielewski, Bao Hoang, Sunish Mohanan, Andrew Gehman, Chih-Yang Hsu, Minh Doan, Fang Xie, M. Reid Groseclose, Christopher Hopson, Sara Brett, Ian A. Wilson, Andrew Nicholls, Marc Ballas, Jeremy D. Waight, Beat M. Jucker, Axel Hoos. Immuno-PET monitoring of CD8+ T cell infiltration post anti-ICOS agonist antibody treatment alone and in combination with PD-1 blocking antibody using a 89Zr anti-CD8+ mouse minibody in EMT 6 syngeneic tumor mouse [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 2816.

Published

2021

18. The use of micro-CT imaging to examine and illustrate fetal skeletal abnormalities in Dutch Belted rabbits and to prove concordance with Alizarin Red stained skeletal examination

Author

Howard M. Solomon, Joyce Rendemonti, Tinamarie Skedzielewski, Beat M. Jucker, Dinesh Stanislaus, Stacia F Murzyn, Hasan Alsaid, and Sharon P Chapman

Subjects

0301 basic medicine, Embryology, Pathology, medicine.medical_specialty, Health, Toxicology and Mutagenesis, ALIZARIN RED, Anthraquinones, Biology, Toxicology, Stain, Bone and Bones, 03 medical and health sciences, Fetus, medicine, Animals, Craniofacial, Skeletal Examination, Staining and Labeling, Ossification, 030111 toxicology, X-Ray Microtomography, Skeleton (computer programming), Staining, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Unossified, Rabbits, medicine.symptom, Developmental Biology

Abstract

Objectives In our laboratory we evaluated the use of micro-computed tomography (micro-CT) using a high resolution acquisition protocol and fetuses obtained on Gestation Day (GD) 29 (mating = GD 0). Methods To show concordance between traditional Alizarin Red S stain and micro-CT skeletal examination methods, 103 fetuses from 19 untreated Dutch belted rabbits were obtained by cesarean section and stored frozen. The fetuses were thawed, imaged and examined digitally by micro-CT, then stained and re-examined using traditional methods. Results A total of 12 individual malformations and 35 unique variations were detected by both methods. Differences in the extent of ossification were found in only 51 of 26,196 bones while 99.8% of the observations were identical. Of the 51 differences, 31 were an unossified fifth medial phalanx of the forepaw indicating that very low-density skeletal bones may be visible by Alizarin Red stain but not by micro-CT scan. To establish this methodology under pharmaceutical testing conditions, we obtained and imaged by micro-CT Alizarin Red S stained abnormal fetal rabbit skeletons previously exposed to a drug candidate associated with craniofacial malformations in humans. All of the types of skeletal abnormalities first identified by staining were also detected by micro-CT examination. Representative images of these 66 different fetal skeletal abnormalities were characterized, and compiled to illustrate visual concordance between micro-CT scanned and traditional Alizarin Red S stained skeletons. Conclusion Micro-CT imaging is an accurate, reliable and robust method that can be used as an alternative to stain when examining fetal rabbit skeletons in developmental toxicity studies.

Published

2017

19. Apoptosis signal-regulating kinase 1 inhibition reverses deleterious indoxyl sulfate-mediated endothelial effects

Author

Andrew R Kompa, Robert N. Willette, Li Huang, Darren J. Kelly, Ruth Magaye, Xin Xiong, Bing Hui Wang, Feby Savira, and Beat M. Jucker

Subjects

Male, 0301 basic medicine, Nitric Oxide Synthase Type III, Endothelium, Apoptosis, Pharmacology, MAP Kinase Kinase Kinase 5, medicine.disease_cause, 030226 pharmacology & pharmacy, General Biochemistry, Genetics and Molecular Biology, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, ASK1, Interleukin 8, General Pharmacology, Toxicology and Pharmaceutics, Endothelial dysfunction, Autocrine signalling, Cells, Cultured, Chemistry, Endothelial Cells, NADPH Oxidases, General Medicine, medicine.disease, Rats, Vasodilation, Endothelial stem cell, Oxidative Stress, 030104 developmental biology, medicine.anatomical_structure, Endothelium, Vascular, Signal transduction, Reactive Oxygen Species, Indican, Oxidative stress, Signal Transduction

Abstract

Aims Indoxyl sulfate (IS), a protein-bound uremic toxin, is implicated in endothelial dysfunction, which contributes to adverse cardiovascular events in chronic kidney disease. Apoptosis signal regulating kinase 1 (ASK1) is a reactive oxygen species-driven kinase involved in IS-mediated adverse effects. This study assessed the therapeutic potential of ASK1 inhibition in alleviating endothelial effects induced by IS. Main methods IS, in the presence and absence of a selective ASK1 inhibitor (GSK2261818A), was assessed for its effect on vascular reactivity in rat aortic rings, and cultured human aortic endothelial cells where we evaluated phenotypic and mechanistic changes. Key findings IS directly impairs endothelium-dependent vasorelaxation and endothelial cell migration. Mechanistic studies revealed increased production of reactive oxygen species-related markers, reduction of endothelial nitric oxide synthase and increased protein expression of tissue inhibitor of matrix metalloproteinase 1 (TIMP1). IS also increases angiopoietin-2 and tumour necrosis factor α gene expression and promotes transforming growth factor β receptor abundance. Inhibition of ASK1 ameliorated the increase in oxidative stress markers, promoted autocrine interleukin 8 pro-angiogenic signalling and decreased anti-angiogenic responses at least in part via reducing TIMP1 protein expression. Significance ASK1 inhibition attenuated vasorelaxation and endothelial cell migration impaired by IS. Therefore, ASK1 is a viable intracellular target to alleviate uremic toxin-induced impairment in the vasculature.

Published

2021

20. RE: Blockade of apoptosis signal-regulating kinase 1 ameliorates cardiac dysfunction in cardiorenal syndrome via enhancing angiogenesis

Author

Beat M. Jucker, Andrew R Kompa, Bing Hui Wang, Robert N. Willette, Amanda J. Edgley, Darren J. Kelly, and Feby Savira

Subjects

Cardio-Renal Syndrome, Heart Diseases, business.industry, Angiogenesis, Kinase, Cardiorenal syndrome, MAP Kinase Kinase Kinase 5, medicine.disease, Fibrosis, Blockade, Cardiac dysfunction, Apoptosis, Cancer research, Humans, Medicine, Cardiology and Cardiovascular Medicine, business

Published

2021

21. RE: ASK1, a new target in treating cardiorenal syndrome (CRS)

Author

Robert N. Willette, Andrew R Kompa, Amanda J. Edgley, Feby Savira, Bing Hui Wang, Darren J. Kelly, and Beat M. Jucker

Subjects

medicine.medical_specialty, Cardio-Renal Syndrome, business.industry, MEDLINE, Hypertrophy, Cardiorenal syndrome, MAP Kinase Kinase Kinase 5, medicine.disease, Fibrosis, Rats, Muscle hypertrophy, Ventricular Dysfunction, Left, Internal medicine, Cardiology, Animals, Medicine, Cardiology and Cardiovascular Medicine, business

Published

2020

22. A multi-center preclinical study of gadoxetate DCE-MRI in rats as a biomarker of drug induced inhibition of liver transporter function

Author

Kim L. R. Brouwer, Dominic P. Williams, Mark Pilling, Beat M. Jucker, Xi Yang, Ryan E. Morgan, Brittany Yerby, Sharon E. Ungersma, Edvin Johansson, Richard A. Peterson, Mikael Forsgren, Serguei Liachenko, Stephen C. Lenhard, Anastassia Karageorgis, Paul D. Hockings, Karageorgis, Anastassia [0000-0003-1348-5580], and Apollo - University of Cambridge Repository

Subjects

Gadolinium DTPA, Male, Physiology, medicine.medical_treatment, Drug Evaluation, Preclinical, lcsh:Medicine, Contrast Media, Aminotransferases, Liver transplantation, Pharmacology, Toxicology, Pathology and Laboratory Medicine, Biochemistry, 030218 nuclear medicine & medical imaging, Diagnostic Radiology, 0302 clinical medicine, Animal Cells, Immune Physiology, Medicine and Health Sciences, lcsh:Science, Liver injury, Multidisciplinary, medicine.diagnostic_test, Radiology and Imaging, Magnetic Resonance Imaging, 3. Good health, Enzymes, Liver, 030220 oncology & carcinogenesis, Toxicity, Cellular Types, Anatomy, Research Article, Radiology, Nuclear Medicine and Medical Imaging, Drug Research and Development, Imaging Techniques, Biological Transport, Active, Surgical and Invasive Medical Procedures, Research and Analysis Methods, 03 medical and health sciences, Digestive System Procedures, Cholestasis, Pharmacokinetics, In vivo, Diagnostic Medicine, Transferases, medicine, Animals, Rats, Wistar, Transplantation, business.industry, lcsh:R, Biology and Life Sciences, Proteins, Magnetic resonance imaging, Cell Biology, Organ Transplantation, medicine.disease, Liver Transplantation, Rats, Hepatocytes, Enzymology, lcsh:Q, Radiologi och bildbehandling, business, Spleen, Biomarkers

Abstract

Drug-induced liver injury (DILI) is a leading cause of acute liver failure and transplantation. DILI can be the result of impaired hepatobiliary transporters, with altered bile formation, flow, and subsequent cholestasis. We used gadoxetate dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI), combined with pharmacokinetic modelling, to measure hepatobiliary transporter function in vivo in rats. The sensitivity and robustness of the method was tested by evaluating the effect of a clinical dose of the antibiotic rifampicin in four different preclinical imaging centers. The mean gadoxetate uptake rate constant for the vehicle groups at all centers was 39.3 +/- 3.4 s-1 (n = 23) and 11.7 +/- 1.3 s-1 (n = 20) for the rifampicin groups. The mean gadoxetate efflux rate constant for the vehicle groups was 1.53 +/- 0.08 s-1 (n = 23) and for the rifampicin treated groups was 0.94 +/- 0.08 s-1 (n = 20). Both the uptake and excretion transporters of gadoxetate were statistically significantly inhibited by the clinical dose of rifampicin at all centers and the size of this treatment group effect was consistent across the centers. Gadoxetate is a clinically approved MRI contrast agent, so this method is readily transferable to the clinic.less thanbr /greater thanConclusion: Rate constants of gadoxetate uptake and excretion are sensitive and robust biomarkers to detect early changes in hepatobiliary transporter function in vivo in rats prior to established biomarkers of liver toxicity. Funding agencies: HESI; National Center for Toxicological Research (NCTR)/U.S. Food and Drug Administration (FDA) [P00800]; National Institutes of Health from the National Institute of General Medical Sciences [R01 GM041935, R35 GM122576]

Published

2018

23. Inhibition of Apoptosis Signal-Regulating Kinase 1 Attenuates Myocyte Hypertrophy and Fibroblast Collagen Synthesis

Author

Beat M. Jucker, Wendi Yang, Andrew R Kompa, Darren J. Kelly, Henry Krum, Zhiliang Li, Qian Fu, Robert N. Willette, Bing Hui Wang, Feby Savira, Ian Wang, and Li Huang

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, MAPK/ERK pathway, Inflammation, Cardiomegaly, 030204 cardiovascular system & hematology, MAP Kinase Kinase Kinase 5, Polymerase Chain Reaction, Muscle hypertrophy, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, ASK1, Myocytes, Cardiac, Cells, Cultured, business.industry, Gene Expression Regulation, Developmental, Fibroblasts, Angiotensin II, Rats, Disease Models, Animal, 030104 developmental biology, Animals, Newborn, Cancer research, RNA, Tumor necrosis factor alpha, Collagen, medicine.symptom, Signal transduction, Cardiology and Cardiovascular Medicine, business, Transforming growth factor, Signal Transduction

Abstract

Background Cardiac remodelling is a dynamic process whereby structural and functional changes occur within the heart in response to injury or inflammation. Recent studies have demonstrated reactive oxygen species sensitive MAPK, apoptosis signal-regulating kinase 1 (ASK1) plays a critical role in cardiac remodelling. This study aims to determine the effectiveness of small molecule ASK1 inhibitors on these processes and their therapeutic potential. Methods Neonatal rat cardiac fibroblasts (NCF) were pre-treated with ASK1 inhibitors, G2261818A (G226) and G2358939A (G235), for 2 hours before stimulated with 100 nM angiotensin II (AngII), 10 μM indoxyl sulphate (IS) or 10 ng/ml transforming growth factor β1 (TGFβ1) for 48 hours. Neonatal rat cardiac myocytes (NCM) were pre-treated with G226 and G235 for 2 hours before being stimulated with 100 nM AngII for 60 hours, 10 μM IS, 10 ng/ml interleukin 1β (IL-1β) or tumour necrosis factor α (TNFα) for 48 hours. 3H-proline and 3H-leucine incorporation was used to assess collagen turnover and hypertrophy, respectively. Pro-fibrotic, pro-hypertrophic and THP-1 inflammatory cytokine gene expressions were determined by RT-PCR. Results Both G226 and G235 dose-dependently attenuated AngII-, IS-, IL-1β- and TNFα-stimulated NCM hypertrophy and hypertrophic gene expression, IS-, AngII- and TGFβ1-stimulated NCF collagen synthesis and AngII- and TGFβ1-stimulated pro-fibrotic gene expression. Inhibition of ASK1 by G226 and G235 inhibited lipopolysaccharides-stimulated inflammatory cytokine gene expression in THP-1 cells. Conclusions Selective ASK1 inhibition confers anti-hypertrophic and anti-fibrotic effects in cardiac cells, and anti-inflammation in monocytic cells. ASK1 inhibitors may represent novel therapeutic agents to alleviate cardiac remodelling post cardiac injury where hypertrophy, fibrosis and inflammation play critical roles.

Published

2017

24. Multimodal imaging approach to examine biodistribution kinetics of Cabotegravir (GSK1265744) long acting parenteral formulation in rat

Author

Bao Hoang, Stephen C. Lenhard, Valeriu Damian, Hasan Alsaid, M. Reid Groseclose, Stephen Castellino, Beat M. Jucker, Gary D. Bowers, Mary V. Rambo, Manish Gupta, and Fang Xie

Subjects

Drug, Male, medicine.medical_specialty, Biodistribution, Depot, Pyridones, media_common.quotation_subject, MRI contrast agent, Injections, Subcutaneous, Pharmaceutical Science, Contrast Media, 02 engineering and technology, Pharmacology, 030226 pharmacology & pharmacy, Injections, Intramuscular, Multimodal Imaging, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cabotegravir, Pharmacokinetics, Edema, medicine, Distribution (pharmacology), Animals, Tissue Distribution, media_common, business.industry, Macrophages, 021001 nanoscience & nanotechnology, Magnetic Resonance Imaging, Ferrosoferric Oxide, Surgery, chemistry, Delayed-Action Preparations, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, medicine.symptom, 0210 nano-technology, business

Abstract

Long-Acting Parenterals (LAPs) have been used in the clinic to provide sustained therapeutic drug levels at a target site, and thereby reducing the frequency of dosing required. In an effort to understand the factors associated with long-acting cabotegravir (GSK1265744 LAP) pharmacokinetic variability, the current study was designed to investigate the temporal relationship between intramuscular (IM) or subcutaneous (SC) drug depot morphology and distribution kinetics with plasma pharmacokinetics. Therefore, a multi-modal molecular imaging (MRI & MALDI IMS) approach was employed to examine the temporal GSK1265744 LAP biodistribution in rat following either IM or SC administration. Serial MRI was performed immediately post drug administration, and then at day 1 (24h post), 2, 3, 4, 7, and 14. In a separate cohort of rats, an MRI contrast agent, Feraheme® (USPIO), was administered 2days post IM drug injection in order to investigate the potential involvement of macrophages trafficking to the GSK1265744 LAP and Vehicle depot sites. The GSK1265744 LAP depot volume increased rapidly by day 2 in the IM injected rats (~3-7 fold) compared with a ~1 fold increase in the SC injected rats. In addition, the USPIO contrast agent labeled macrophages were shown to be present in the depot region of the GSK1265744 LAP injected gastrocnemius while the Vehicle injected gastrocnemius appeared to show reduced uptake. Matrix-assisted laser desorption ionization (MALDI) imaging mass spectrometry (IMS) of muscle and abdominal tissue sections identified the drug content primarily within the depot. Co-registration of the GSK1265744 ion images with immunohistochemical images established that the drug was taken up by macrophages associated with the depot. Linear regression analysis demonstrated that the drug depot characteristics including volume, surface area, and perimeter assessed by MRI at day 2 correlated with early time point plasma drug concentrations. In summary, a multimodal molecular imaging approach was used to identify the drug depot location and volumetric/physiologic changes in both IM and SC locations following GSK1265744 LAP administration. The IM depot volume increased rapidly to a maximum volume at 2days post-GSK1265744 LAP administration, while the Vehicle depot did not suggesting that the active drug substance and/or related particle was a key driver for drug depot evolution. The depot expansion was associated with an increase in macrophage infiltration and edema in and around the depot region and was correlated to plasma drug concentration at early time points (0-4days). Consequently, molecular imaging approaches may be used in patients to help understand the biodistribution of GSK1265744 LAP and its associated pharmacokinetics.

Published

2017

25. Non invasive imaging assessment of the biodistribution of GSK2849330, an ADCC and CDC optimized anti HER3 mAb, and its role in tumor macrophage recruitment in human tumor-bearing mice

Author

Danielle J. Vugts, Mary V. Rambo, Matthew Cleveland, Bao Hoang, Hasan Alsaid, Edward Long, Tinamarie Skedzielewski, James Tunstead, Neil J. Clarke, Kristen Hunsinger, William E. Fieles, Beat M. Jucker, Christopher Matheny, Radiology and nuclear medicine, and CCA - Imaging and biomarkers

Subjects

0301 basic medicine, Fluorescence-lifetime imaging microscopy, Pathology, Confocal Microscopy, Receptor, ErbB-3, Physiology, Cancer Treatment, lcsh:Medicine, Biochemistry, Diagnostic Radiology, law.invention, White Blood Cells, Mice, 0302 clinical medicine, Animal Cells, law, Immune Physiology, Neoplasms, Medicine and Health Sciences, Medicine, Tissue Distribution, lcsh:Science, Antibody-dependent cell-mediated cytotoxicity, Microscopy, Immune System Proteins, Multidisciplinary, Radiology and Imaging, Light Microscopy, Antibodies, Monoclonal, Magnetic Resonance Imaging, Immunohistochemistry, Body Fluids, Blood, In Vivo Imaging, Oncology, Isotope Labeling, 030220 oncology & carcinogenesis, Female, Cellular Types, Anatomy, Preclinical imaging, Research Article, medicine.medical_specialty, Biodistribution, Imaging Techniques, Immune Cells, Immunology, Transplantation, Heterologous, Mice, Nude, Research and Analysis Methods, Antibodies, Monoclonal, Humanized, Antibodies, 03 medical and health sciences, Diagnostic Medicine, In vivo, Confocal microscopy, Cell Line, Tumor, Fluorescence Imaging, Animals, Humans, Radioisotopes, Blood Cells, business.industry, Macrophages, lcsh:R, Biology and Life Sciences, Proteins, Cell Biology, Ferrosoferric Oxide, Monoclonal Antibodies, Transplantation, 030104 developmental biology, lcsh:Q, Zirconium, Radiopharmaceuticals, Molecular imaging, business

Abstract

The purpose of this work was to use various molecular imaging techniques to non-invasively assess GSK2849330 (anti HER3 ADCC and CDC enhanced 'AccretaMab' monoclonal antibody) pharmacokinetics and pharmacodynamics in human xenograft tumor-bearing mice. Immuno-PET biodistribution imaging of radiolabeled 89Zr-GSK2849330 was assessed in mice with HER3 negative (MIA-PaCa-2) and positive (CHL-1) human xenograft tumors. Dose dependency of GSK2849330 disposition was assessed using varying doses of unlabeled GSK2849330 co-injected with 89Zr-GSK2849330. In-vivo NIRF optical imaging and ex-vivo confocal microscopy were used to assess the biodistribution of GSK2849330 and the HER3 receptor occupancy in HER3 positive xenograft tumors (BxPC3, and CHL-1). Ferumoxytol (USPIO) contrast-enhanced MRI was used to investigate the effects of GSK2849330 on tumor macrophage content in CHL-1 xenograft bearing mice. Immuno-PET imaging was used to monitor the whole body drug biodistribution and CHL-1 xenograft tumor uptake up to 144 hours post injection of 89Zr-GSK2849330. Both hepatic and tumor uptake were dose dependent and saturable. The optical imaging data in the BxPC3 xenograft tumor confirmed the tumor dose response finding in the Immuno-PET study. Confocal microscopy showed a distinguished cytoplasmic punctate staining pattern within individual CHL-1 cells. GSK2849330 inhibited tumor growth and this was associated with a significant decrease in MRI signal to noise ratio after USPIO injection and with a significant increase in tumor macrophages as confirmed by a quantitative immunohistochemistry analysis. By providing both dose response and time course data from both 89Zr and fluorescently labeled GSK2849330, complementary imaging studies were used to characterize GSK2849330 biodistribution and tumor uptake in vivo. Ferumoxytol-enhanced MRI was used to monitor aspects of the immune system response to GSK2849330. Together these approaches potentially provide clinically translatable, non-invasive techniques to support dose optimization, and assess immune activation and anti-tumor responses.

Published

2017

26. Soluble Epoxide Hydrolase Inhibition Does Not Prevent Cardiac Remodeling and Dysfunction After Aortic Constriction in Rats and Mice

Author

Bao Hoang, Stephen H. Eisennagel, James Tunstead, Shufang Zhao, Alan R. Olzinski, Beat M. Jucker, David J. Behm, Tao Wang, John J. Upson, Joseph P. Marino, Lisa A. Morgan, and Robert N. Willette

Subjects

Male, Epoxide hydrolase 2, medicine.medical_specialty, Cardiomegaly, Vasodilation, Constriction, Pathologic, Muscle hypertrophy, Rats, Sprague-Dawley, Mice, Piperidines, Species Specificity, Fibrosis, Internal medicine, medicine.artery, medicine, Animals, Enzyme Inhibitors, Aorta, Epoxide Hydrolases, Pharmacology, Pressure overload, Cyclohexylamines, Ventricular Remodeling, Triazines, business.industry, Anatomy, medicine.disease, Rats, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, Ventricle, Heart failure, cardiovascular system, Cardiology and Cardiovascular Medicine, business

Abstract

Epoxyeicosatrienoic acids, substrates for soluble epoxide hydrolase (sEH), exhibit vasodilatory and antihypertrophic activities. Inhibitors of sEH might therefore hold promise as heart failure therapeutics. We examined the ability of sEH inhibitors GSK2188931 and GSK2256294 to modulate cardiac hypertrophy, fibrosis, and function after transverse aortic constriction (TAC) in rats and mice. GSK2188931 administration was initiated in rats 1 day before TAC, whereas GSK2256294 treatment was initiated in mice 2 weeks after TAC. Four weeks later, cardiovascular function was assessed, plasma was collected for drug and sEH biomarker concentrations, and left ventricle was isolated for messenger RNA and histological analyses. In rats, although GSK2188931 prevented TAC-mediated increases in certain genes associated with hypertrophy and fibrosis (α-skeletal actin and connective tissue growth factor), the compound failed to attenuate TAC-induced increases in left ventricle mass, posterior wall thickness, end-diastolic volume and pressure, and perivascular fibrosis. Similarly, in mice, GSK2256294 did not reverse cardiac remodeling or systolic dysfunction induced by TAC. Both compounds increased the sEH substrate/product (leukotoxin/leukotoxin diol) ratio, indicating sEH inhibition. In summary, sEH inhibition does not prevent cardiac remodeling or dysfunction after TAC. Thus, targeting sEH seems to be insufficient for reducing pressure overload hypertrophy.

Published

2013

27. Chronic Inhibition of Hypoxia-inducible Factor Prolyl 4-hydroxylase Improves Ventricular Performance, Remodeling, and Vascularity After Myocardial Infarction in the Rat

Author

Beat M. Jucker, Connie L. Erickson-Miller, Weike Bao, Saul Needle, G. C. Teg Pipes, Jennifer L. Ariazi, Robert N. Willette, Alan R. Olzinski, Erding Hu, John J. Lepore, David J. Behm, Shufang Zhao, Kevin J. Duffy, and Pu Qin

Subjects

Male, medicine.medical_specialty, Angiogenesis, Glycine, Myocardial Infarction, Procollagen-Proline Dioxygenase, Inflammation, Quinolones, Cell Line, Rats, Sprague-Dawley, Vascularity, Internal medicine, medicine, Animals, Transcription factor, Pharmacology, Ventricular Remodeling, business.industry, Hemodynamics, Hypoxia-Inducible Factor 1, alpha Subunit, Coronary Vessels, Rats, Oxygen tension, Endocrinology, Hypoxia-inducible factors, Rats, Inbred Lew, Erythropoietin, Erythropoiesis, Hypoxia-Inducible Factor 1, medicine.symptom, Cardiology and Cardiovascular Medicine, business, medicine.drug

Abstract

Hypoxia inducible factors (HIFs) are transcription factors that are regulated by HIF-prolyl 4-hydroxylases (PHDs) in response to changes in oxygen tension. Once activated, HIFs play an important role in angiogenesis, erythropoiesis, proliferation, cell survival, inflammation, and energy metabolism. We hypothesized that GSK360A, a novel orally active HIF-PHD inhibitor, could facilitate local and systemic HIF-1 alpha signaling and protect the failing heart after myocardial infarction (MI).GSK360A is a potent (nanomolar) inhibitor of HIF-PHDs (PHD1PHD2 = PHD3) capable of activating the HIF-1 alpha pathway in a variety of cell types including neonatal rat ventricular myocytes and H9C2 cells. Male rats treated orally with GSK360A (30 mg x kg x d) had a sustained elevation in circulating levels of erythropoietin and hemoglobin and increased hemoxygenase-1 expression in the heart and skeletal muscle. In a rat model of established heart failure with systolic dysfunction induced by ligation of left anterior descending coronary artery, chronic treatment with GSK360A for 28 days prevented the progressive reduction in ejection fraction, ventricular dilation, and increased lung weight, which were observed in the vehicle-treated animals, for up to 3 months. In addition, the microvascular density in the periinfarct region was increased (2-fold) in GSK360A-treated animals. Treatment was well tolerated (survival was 89% in the GSK360A group vs. 82% in the placebo group).Chronic post-myocardial infarction treatment with a selective HIF PHD inhibitor (GSK360A) exerts systemic and local effects by stabilizing HIF-1 alpha signaling and improves long-term ventricular function, remodeling, and vascularity in a model of established ventricular dysfunction. These results suggest that HIF-PHD inhibitors may be suitable for the treatment of post-MI remodeling and heart failure.

Published

2010

28. Pharmacological Inhibition of C-C Chemokine Receptor 2 Decreases Macrophage Infiltration in the Aortic Root of the Human C-C Chemokine Receptor 2/Apolipoprotein E −/− Mouse: Magnetic Resonance Imaging Assessment

Author

Colin H. Macphee, Gregory H. Turner, Michael A. Ringenberg, Carla A. Cornejo, Robert N. Willette, Alan R. Olzinski, Pu Qin, Clark A. Sehon, Karpagam Aravindhan, Bao Hoang, Roberta E. Bernard, Heather Karr, Krista B. Goodman, Beat M. Jucker, and Peter J. Gough

Subjects

Apolipoprotein E, CCR2, Pathology, medicine.medical_specialty, Time Factors, Receptors, CCR2, MRI contrast agent, Anti-Inflammatory Agents, Aortic Diseases, Contrast Media, Mice, Transgenic, Peritonitis, Biology, Mice, Chemokine receptor, Apolipoproteins E, In vivo, medicine, Animals, Humans, Naphthyridines, Magnetite Nanoparticles, Mice, Knockout, medicine.diagnostic_test, Angiotensin II, Macrophages, Dextrans, Magnetic resonance imaging, Infusion Pumps, Implantable, Atherosclerosis, Dietary Fats, Immunohistochemistry, Magnetic Resonance Imaging, Ferrosoferric Oxide, Disease Models, Animal, Cardiology and Cardiovascular Medicine, Ex vivo

Abstract

Purpose— This study assessed the pharmacological effect of a novel selective C-C chemokine receptor (CCR) 2 antagonist (GSK1344386B) on monocyte/macrophage infiltration into atherosclerotic plaque using magnetic resonance imaging (MRI) in an atherosclerotic mouse model. Methods and Results— Apolipoprotein E −/− mice expressing human CCR2 were fed a Western diet (vehicle group) or a Western diet plus10 mg/kg per day of GSK1344386B (GSK1344386B group). After the baseline MRI, mice were implanted with osmotic pumps containing angiotensin II, 1000 ng/kg per minute, to accelerate lesion formation. After five weeks of angiotensin II administration, mice received ultrasmall superparamagnetic iron oxide, an MRI contrast agent for the assessment of monocyte/macrophage infiltration to the plaque, and underwent imaging. After imaging, mice were euthanized, and the heart and aorta were harvested for ex vivo MRI and histopathological examination. After 5 weeks of dietary dosing, there were no significant differences between groups in body or liver weight or plasma cholesterol concentrations. An in vivo MRI reflected a decrease in ultrasmall superparamagnetic iron oxide contrast agent uptake in the aortic arch of the GSK1344386B group ( P P P Conclusion— An MRI was used to noninvasively assess the decreased macrophage content in the atherosclerotic plaque after selective CCR2 inhibition.

Published

2010

29. Inhibition of FGF/FGFR autocrine signaling in mesothelioma with the FGF ligand trap, FP-1039/GSK3052230

Author

Hasan Alsaid, M. Phillip DeYoung, Tina Skedzielewski, Bao Hoang, Mary S. Barnette, James Tunstead, Gopinath Ganji, Christian S. Sherk, Elisabeth A. Minthorn, Rakesh Kumar, Beat M. Jucker, Maggie Fricko, and Christina Blackwell

Subjects

0301 basic medicine, Mesothelioma, ligand trap, Pathology, medicine.medical_specialty, Oncogene Proteins, Fusion, Angiogenesis, Recombinant Fusion Proteins, Mice, SCID, Fibroblast growth factor, Ligands, Cell Line, 03 medical and health sciences, Mice, angiogenesis, 0302 clinical medicine, fibroblast growth factor, medicine, Animals, Humans, Receptor, Fibroblast Growth Factor, Type 1, Autocrine signalling, Cell Proliferation, Neovascularization, Pathologic, Chemistry, Cell growth, Fibroblast growth factor receptor 1, medicine.disease, Magnetic Resonance Imaging, Fibroblast Growth Factors, Gene Expression Regulation, Neoplastic, Autocrine Communication, 030104 developmental biology, Oncology, Fibroblast growth factor receptor, 030220 oncology & carcinogenesis, Immunoglobulin G, Cancer research, Female, Signal transduction, signaling, Neoplasm Transplantation, Signal Transduction, Research Paper

Abstract

Fibroblast growth factor (FGF) ligand-dependent signaling has a fundamental role in cancer development and tumor maintenance. GSK3052230 (also known as FP-1039) is a soluble decoy receptor that sequesters FGFs and inhibits FGFR signaling. Herein, the efficacy of this molecule was tested in models of mesothelioma, a tumor type shown to express high levels of FGF2 and FGFR1. GSK3052230 demonstrated antiproliferative activity across a panel of mesothelioma cell lines and inhibited growth of tumor xenografts in mice. High expression of FGF2 and FGFR1 correlated well with response to FGF pathway inhibition. GSK3052230 inhibited MAPK signaling as evidenced by decreased phospho-ERK and phospho-S6 levels in vitro and in vivo. Additionally, dose-dependent and statistically-significant reductions in tumor vessel density were observed in GSK3052230-treated tumors compared to vehicle-treated tumors. These data support the role of GSK3052230 in effectively targeting FGF-FGFR autocrine signaling in mesothelioma, demonstrate its impact on tumor growth and angiogenesis, and provide a rationale for the current clinical evaluation of this molecule in mesothelioma patients.

Published

2015

30. Atherosclerotic Plaque Inflammation Varies Between Vascular Sites and Correlates With Response to Inhibition of Lipoprotein‐Associated Phospholipase A 2

Author

Beat M. Jucker, Robert L. Wilensky, Eliot G Peyster, Robert S. Fenning, Mark E. Burgert, Stephen C. Lenhard, Emile R. Mohler, Colin H. Macphee, Damir Hamamdzic, and Shreya Kangovi

Subjects

Male, Pathology, medicine.medical_specialty, Phospholipase A2 Inhibitors, Swine, Hypercholesterolemia, Gene Expression, Inflammation, Lesion, Phospholipase A2, Darapladib, Diabetes mellitus, Oximes, Diabetes Mellitus, medicine, Animals, Aorta, Abdominal, biology, lipoprotein‐associated phospholipase A2, business.industry, Macrophages, Lipoprotein-associated phospholipase A2, Editorials, coronary atherosclerosis, Arteriosclerosis, Atherosclerosis, medicine.disease, Coronary Vessels, Plaque, Atherosclerotic, Disease Models, Animal, Benzaldehydes, 1-Alkyl-2-acetylglycerophosphocholine Esterase, Circulatory system, biology.protein, medicine.symptom, Cardiology and Cardiovascular Medicine, business

Abstract

Background Despite systemic exposure to risk factors, the circulatory system develops varying patterns of atherosclerosis for unclear reasons. In a porcine model, we investigated the relationship between site‐specific lesion development and inflammatory pathways involved in the coronary arteries ( COR s) and distal abdominal aortas ( AA s). Methods and Results Diabetes mellitus ( DM ) and hypercholesterolemia ( HC ) were induced in 37 pigs with 3 healthy controls. Site‐specific plaque development was studied by comparing plaque severity, macrophage infiltration, and inflammatory gene expression between COR s and AA s of 17 DM / HC pigs. To assess the role of lipoprotein‐associated phospholipase A 2 (Lp‐ PLA 2 ) in plaque development, 20 DM / HC pigs were treated with the Lp‐ PLA 2 inhibitor darapladib and compared with the 17 DM / HC untreated pigs. DM / HC caused site‐specific differences in plaque severity. In the AA s, normalized plaque area was 4.4‐fold higher ( P AA and not the COR , P =0.004), while normalized macrophage staining area was 1.5‐fold higher ( P =0.011) compared with COR s. DM / HC caused differential expression of 8 of 87 atherosclerotic genes studied, including 3 important in inflammation with higher expression in the COR s. Darapladib‐induced attenuation of normalized plaque area was site‐specific, as COR s responded 2.9‐fold more than AA s ( P =0.045). Conclusions While plaque severity was worse in the AA s, inflammatory genes and inflammatory pathways that use Lp‐ PLA 2 were more important in the COR s. Our results suggest fundamental differences in inflammation between vascular sites, an important finding for the development of novel anti‐inflammatory therapeutics.

Published

2015

31. Preservation of Cardiac Function and Attenuation of Remodelling in Transient Receptor Potential Vanilloid 4 Knockout Mice Following Myocardial Infarctionnd Medical Center

Author

Weike Bao, Kevin S. Thorneloe, John J. Lepore, Robert N. Willette, Beat M. Jucker, and Gregory H. Turner

Subjects

Cardiac function curve, medicine.medical_specialty, Ejection fraction, business.industry, Ischemia, Diastole, Pulmonary edema, medicine.disease, Internal medicine, Heart failure, cardiovascular system, medicine, Cardiology, cardiovascular diseases, Myocardial infarction, Cardiology and Cardiovascular Medicine, business, Reperfusion injury

Abstract

Transient receptor potential channel vanilloid 4 (TRPV4) is a non-selective Ca2+ permeable cation channel, recently implicated by computational methods as a key signalling component during myocardial infarction. We previously showed that pharmacological TRPV4 inhibition can prevent and resolve pulmonary edema in pre-clinical heart failure animal models. Here, we examined the impact of genetic deletion of TRPV4 (TRPV4-/-) on cardiac function, both basally and following myocardial infarction. Cardiac function was similar in wild type and TRPV4-/- mice under normal conditions. By contrast, following myocardial infarction induced by permanent ligation of the left anterior descending coronary artery, left ventricular systolic and diastolic volumes were reduced and ejection fraction was significantly improved in TRPV4-/- when compared to wild type mice. Consistent with the differences in chamber volumes between TRPV4-/- and wild type mice, myocardial infarction induced a significant increase in heart weight and left ventricular mass index in wild type, but not in TRPV4-/- mice. In a separate cohort of mice, we also investigated the effect of genetic deletion of TRPV4 on infarct size after a 30 min myocardial ischemia and 24 hours reperfusion. There were no differences in myocardial infarct size or area at risk in TRPV4-/- and wild type mice after ischemia/reperfusion injury. These results suggest that TRPV4 does not mediate acute myocardial ischemic injury, but does play an important role in ventricular remodelling known to correlate with poor outcomes following acute myocardial infarction.

Published

2015

32. Differential uptake of ferumoxtran-10 and ferumoxytol, ultrasmall superparamagnetic iron oxide contrast agents in rabbit: Critical determinants of atherosclerotic plaque labeling

Author

Alan R. Olzinski, Paula M. Jacobs, Karpagam Aravindhan, Robert N. Willette, Beat M. Jucker, Susan M. Gruver, Tom C.-C. Hu, April D. Yancy, and Stephen C. Lenhard

Subjects

Male, Pathology, medicine.medical_specialty, Arteriosclerosis, Iron, Contrast Media, chemistry.chemical_compound, Pharmacokinetics, In vivo, medicine.artery, Ferumoxtran-10, medicine, Animals, Radiology, Nuclear Medicine and imaging, Magnetite Nanoparticles, medicine.diagnostic_test, business.industry, Cholesterol, Macrophages, Abdominal aorta, Dextrans, Oxides, Magnetic resonance imaging, Magnetic Resonance Imaging, Ferrosoferric Oxide, Ferumoxytol, chemistry, Rabbits, Nuclear medicine, business, Ex vivo

Abstract

Purpose To compare atherosclerotic plaque uptake of a first (ferumoxtran-10) and second generation (ferumoxytol) ultrasmall superparamagnetic iron oxide (USPIO) contrast agent with different pharmacokinetic/pharmacodynamic properties. Materials and Methods New Zealand White rabbits maintained on a high cholesterol/fat diet were subjected to balloon injury to the abdominal aorta. Ferumoxtran-10 or ferumoxytol (500 μmol/kg) was administered at 2, 4, and 8 weeks following injury. In vivo magnetic resonance imaging (MRI) was performed immediately prior to, immediately after, and 6 days post-contrast administration. Ex vivo MRI, histologic, and inductively coupled plasma-mass spectrometry (ICP-MS) iron analyses were performed on the excised vessels. Results The blood pool clearance of ferumoxytol (t½ ≤ 6 hours) was more rapid than that of ferumoxtran-10 (t½ ≤ 48 hours). Decreased in vivo MRI signal intensity in the abdominal aorta was observed at 2, 4, and 8 weeks following injury with ferumoxtran-10, but not with ferumoxytol. Consistent with these observations, ex vivo MRI signal intensity was decreased in the ferumoxtran-10 vessels, and to a lesser degree in the ferumoxytol vs. control vessels (− contrast agent). In contrast, in vitro macrophage phagocytosis of USPIO was four to six fold greater with ferumoxytol than with ferumoxtran-10. Additionally, the absolute iron content correlated with ex vivo MRI signal intensity in all vessels (r = −0.86, P < 0.0001). Conclusions These data suggest that the exposure period of atherosclerotic plaque to USPIO rather than the kinetics of the USPIO uptake by plaque alone is a critical criterion for experimental design of in vivo studies. J. Magn. Reson. Imaging 2005;21:432–442. © 2005 Wiley-Liss, Inc.

Published

2005

33. Activation of Peroxisome Proliferator–Activated Receptor-α Protects the Heart From Ischemia/Reperfusion Injury

Author

Weike Bao, Juan-Li Gu, Eliot H. Ohlstein, Tian-Li Yue, Douglas T. Thudium, Anne M. Romanic, Cynthia L. Burns-Kurtis, Beat M. Jucker, Jianqi Cui, Rogely W. Boyce, Karpagam Aravindhan, Peter Brown, and Rosanna C. Mirabile

Subjects

Male, Agonist, medicine.medical_specialty, medicine.drug_class, Premedication, Drug Evaluation, Preclinical, Myocardial Infarction, Myocardial Ischemia, Ischemia, Down-Regulation, Receptors, Cytoplasmic and Nuclear, Peroxisome proliferator-activated receptor, Myocardial Reperfusion Injury, Mice, NF-KappaB Inhibitor alpha, Physiology (medical), Internal medicine, Animals, Medicine, RNA, Messenger, Myocardial infarction, Receptor, Ligation, Beta oxidation, Mice, Knockout, Cardioprotection, chemistry.chemical_classification, business.industry, Myocardium, Phenylurea Compounds, Fatty Acids, NF-kappa B, medicine.disease, Matrix Metalloproteinases, Butyrates, Chemotaxis, Leukocyte, Endocrinology, chemistry, Cytokines, I-kappa B Proteins, Cardiology and Cardiovascular Medicine, business, Oxidation-Reduction, Reperfusion injury, Transcription Factors

Abstract

Background— Peroxisome proliferator–activated receptor-α (PPAR-α) is expressed in the heart and regulates genes involved in myocardial fatty acid oxidation (FAO). The role of PPAR-α in acute ischemia/reperfusion myocardial injury remains unclear. Methods and Results— The coronary arteries of male mice were ligated for 30 minutes. After reperfusion for 24 hours, ischemic and infarct sizes were determined. A highly selective and potent PPAR-α agonist, GW7647, was administered by mouth for 2 days, and the third dose was given 1 hour before ischemia. GW7647 at 1 and 3 mg · kg −1 · d −1 reduced infarct size by 28% and 35%, respectively ( P Conclusions— Activation of PPAR-α protected the heart from reperfusion injury. This cardioprotection might be mediated through metabolic and antiinflammatory mechanisms. This novel effect of the PPAR-α agonist could provide an added benefit to patients treated with PPAR-α activators for dyslipidemia.

Published

2003

34. p38 MAPK Inhibitors Ameliorate Target Organ Damage in Hypertension: Part 2. Improved Renal Function as Assessed by Dynamic Contrast-Enhanced Magnetic Resonance Imaging

Author

Rogely W. Boyce, Thomas R. Schaeffer, Rosanna C. Mirabile, Robert N. Willette, Beat M. Jucker, David F. Adams, Stephen C. Lenhard, and Sandhya S. Nerurkar

Subjects

Gadolinium DTPA, MAPK/ERK pathway, medicine.medical_specialty, p38 mitogen-activated protein kinases, Contrast Media, Renal function, In Vitro Techniques, Kidney, Kidney Function Tests, p38 Mitogen-Activated Protein Kinases, Pathogenesis, In vivo, Rats, Inbred SHR, Internal medicine, medicine, Albuminuria, Animals, Enzyme Inhibitors, Pharmacology, medicine.diagnostic_test, business.industry, Imidazoles, Sodium, Dietary, Magnetic resonance imaging, Dietary Fats, Magnetic Resonance Imaging, Rats, Stroke, Pyrimidines, Blood pressure, Endocrinology, Creatinine, Hypertension, Molecular Medicine, Endothelium, Vascular, Mitogen-Activated Protein Kinases, medicine.symptom, business, Glomerular Filtration Rate

Abstract

Recent evidence suggests p38 mitogen-activated protein kinase (MAPK) signal transduction plays an important role in the pathogenesis of progressive renal disease. Using dynamic contrast enhanced magnetic resonance imaging (MRI), we evaluated chronic treatment with a p38 MAPK inhibitor, trans-1-(4-hydroxycyclohexyl)-4-(4-fluorophenyl-methoxypyridimidin-4-yl)imidazole (SB-239063), on renal function in a hypertension model of progressing renal dysfunction. Spontaneously hypertensive-stroke prone rats were placed on a high salt/fat diet (SFD) or maintained on normal chow diet (ND). SFD animals with albuminuria at 4 to 8 weeks (or =10 mg/day inclusion criteria), were randomized into p38 MAPK inhibitor treatment (SB-239063, 1200 ppm in diet) or vehicle groups. The progression of blood pressure and albuminuria during the treatment period (approximately 6 weeks) was decreased by 12 and 60%, respectively, in the SFD + SB-239063 versus SFD control group. Renal perfusion and filtration were assessed by in vivo MRI at the end of the study. Relative cortical perfusion was increased in the SFD + SB-239063 group compared with the SFD control group as reflected by a 29% decrease in time to peak of contrast agent in the cortex. Additionally, the regional renal glomerular filtration rate index (Kcl) was increased by 39% in the SFD + SB-239063 versus SFD control group and was normalized to the ND control group. Greater functional heterogeneity was observed in the SFD control versus SFD + SB-239063 or ND control group. All alterations of renal function were supported by histopathological findings. In conclusion, chronic treatment with a p38 MAPK inhibitor, SB-239063, attenuates functional and structural renal degeneration in a hypertensive model of established renal dysfunction.

Published

2003

35. Carbon-13 NMR assignments of the bases in oligodeoxynucleotides: an automated procedure using Bayesian statistics.

Author

Timothy J. Hyman, Eilis A. Boudreau, Gilles G. Martin, Beat M. Jucker, Philip N. Borer, and George C. Levy

Published

1988

36. Normalization of Skeletal Muscle Glycogen Synthesis and Glycolysis in Rosiglitazone-Treated Zucker Fatty Rats

Author

Stephen A. Smith, Robin E. Haimbach, Derek H. Ohlstein, Thomas S. McIntosh, Daniel Chun, Beat M. Jucker, Matthew E. Mayer, Thomas R. Schaeffer, Susanta K. Sarkar, Alexander R. Cobitz, and Hugh M. Davis

Subjects

medicine.medical_specialty, Glycogen, Endocrinology, Diabetes and Metabolism, Glucose uptake, Glucose transporter, Metabolism, Biology, Carbohydrate metabolism, chemistry.chemical_compound, Endocrinology, Nuclear magnetic resonance, Gluconeogenesis, chemistry, Internal medicine, Internal Medicine, medicine, biology.protein, Glycolysis, Glycogen synthase

Abstract

The aim of this study was to characterize insulin-stimulated skeletal muscle glucose metabolism in Zucker fatty rats and to provide insight into the therapeutic mechanism by which rosiglitazone increases insulin-stimulated glucose disposal in these rats. Metabolic parameters were measured using combined in vivo (13)C nuclear magnetic resonance (NMR) spectroscopy to measure skeletal muscle glucose uptake and its distributed fluxes (glycogen synthesis and glycolysis), and (31)P NMR was used to measure simultaneous changes in glucose-6-phosphate (G-6-P) during a euglycemic-hyperinsulinemic clamp in awake Zucker fatty rats. Three groups of Zucker fatty rats (fatty rosiglitazone [FRSG], fatty control [FC], lean control [LC]) were treated for 7 days before the experiment (3 mg/kg rosiglitazone or vehicle via oral gavage). Rates of glycolysis and glycogen synthesis were assessed after treatment by monitoring 1,6-(13)C(2) glucose label incorporation into 1-(13)C glycogen, 3-(13)C lactate, and 3-(13)C alanine during a euglycemic ( approximately 7-8 mmol/l)-hyperinsulinemic (10 mU. kg(-1). min(-1)) clamp. The FRSG group exhibited a significant increase in insulin sensitivity, reflected by an increased whole-body glucose disposal rate during the clamp (24.4 +/- 1.9 vs. 17.6 +/- 1.4 and 33.2 +/- 2.0 mg. kg(-1). min(-1) in FRSG vs. FC [P < 0.05] and LC [P < 0.01] groups, respectively). The increased insulin-stimulated glucose disposal in the FRSG group was associated with a normalization of the glycolytic flux (52.9 +/- 9.1) to LC (56.2 +/- 16.6) versus FC (18.8 +/- 8.6 nmol. g(-1). min(-1), P < 0.02) and glycogen synthesis flux (56.3 +/- 11.5) to LC (75.2 +/- 15.3) versus FC (16.6 +/- 12.8 nmol. g(-1). min(-1), P < 0.05). [G-6-P] increased in the FRSG and LC groups versus baseline during the clamp (13.0 +/- 11.1 and 16.9 +/- 5.8%, respectively), whereas [G-6-P] in the FC group decreased (-23.3 +/- 13.4%, P < 0.05). There were no differences between groups in intramyocellular glucose, as measured by biochemical assay. These data suggest that the increased insulin-stimulated glucose disposal in muscle after rosiglitazone treatment can be attributed to a normalization of glucose transport and metabolism.

Published

2002

37. Effect of triiodothyronine on mitochondrial energy coupling in human skeletal muscle

Author

Vincent Lebon, Sylvie Dufour, Kitt Falk Petersen, Jianming Ren, Beat M. Jucker, Lori A. Slezak, Gary W. Cline, Douglas L. Rothman, and Gerald I. Shulman

Subjects

Adult, Male, Magnetic Resonance Spectroscopy, Citric Acid Cycle, Glutamic Acid, General Medicine, Article, Oxidative Phosphorylation, Mitochondria, Adenosine Triphosphate, Humans, Triiodothyronine, Female, Muscle, Skeletal

Abstract

The mechanism underlying the regulation of basal metabolic rate by thyroid hormone remains unclear. Although it has been suggested that thyroid hormone might uncouple substrate oxidation from ATP synthesis, there are no data from studies on humans to support this hypothesis. To examine this possibility, we used a novel combined (13)C/(31)P nuclear magnetic resonance (NMR) approach to assess mitochondrial energy coupling in skeletal muscle of seven healthy adults before and after three days of triiodothyronine (T(3)) treatment. Rates of ATP synthesis and tricarboxylic acid (TCA) cycle fluxes were measured by (31)P and (13)C NMR spectroscopy, respectively, and mitochondrial energy coupling was assessed as the ratio. Muscle TCA cycle flux increased by approximately 70% following T(3) treatment. In contrast, the rate of ATP synthesis remained unchanged. Given the disproportionate increase in TCA cycle flux compared with ATP synthesis, these data suggest that T(3) promotes increased thermogenesis in part by promoting mitochondrial energy uncoupling in skeletal muscle.

Published

2001

38. 13C/31P NMR Assessment of Mitochondrial Energy Coupling in Skeletal Muscle of Awake Fed and Fasted Rats

Author

Kevin S. Cadman, Sylvie Dufour, Beat M. Jucker, Gerald I. Shulman, Xueying Cao, Jian-Ming Ren, and Stephen F. Previs

Subjects

Messenger RNA, medicine.medical_specialty, Skeletal muscle, Cell Biology, Hindlimb, Mitochondrion, Biology, Biochemistry, chemistry.chemical_compound, Endocrinology, medicine.anatomical_structure, chemistry, Internal medicine, medicine, Uncoupling protein, Carnitine O-palmitoyltransferase, Molecular Biology, Adenosine triphosphate, UCP3

Abstract

To examine the relationship between mitochondrial energy coupling in skeletal muscle and change in uncoupling protein 3 (UCP3) expression during the transition from the fed to fasted state, we used a novel noninvasive31P/13C NMR spectroscopic approach to measure the degree of mitochondrial energy coupling in the hind limb muscles of awake rats before and after a 48-h fast. Compared with fed levels, UCP3 mRNA and protein levels in the gastrocnemius increased 1.7- (p

Published

2000

39. Assessment of mitochondrial energy coupling in vivo by 13 C/ 31 P NMR

Author

Kevin S. Cadman, Xueying Cao, Jian-Ming Ren, Beat M. Jucker, Sylvie Dufour, Stephen F. Previs, Gerald I. Shulman, and Brian Underhill

Subjects

Magnetic Resonance Spectroscopy, Multidisciplinary, ATP synthase, biology, Citric Acid Cycle, Skeletal muscle, Nuclear magnetic resonance spectroscopy, Biological Sciences, Mitochondrion, Carbon-13 NMR, Mitochondria, Rats, Rats, Sprague-Dawley, Adenosine Triphosphate, medicine.anatomical_structure, Biochemistry, biology.protein, medicine, Animals, Uncoupling protein, Obesity, Energy Metabolism, Oxidation-Reduction, Flux (metabolism), UCP3

Abstract

The recently cloned uncoupling protein homolog UCP3 is expressed primarily in muscle and therefore may play a significant role in the regulation of energy expenditure and body weight. However, investigation into the regulation of uncoupling protein has been hampered by the inability to assess its activity in vivo . In this report, we demonstrate the use of a noninvasive NMR technique to assess mitochondrial energy uncoupling in skeletal muscle of awake rats by combining 13 C NMR to measure rates of mitochondrial substrate oxidation with 31 P NMR to assess unidirectional ATP synthesis flux. These combined 31 P/ 13 C NMR measurements were performed in control, 10-day triiodo- l -thyronine (T 3 )-treated (model of increased UCP3 expression), and acute 2,4-dinitrophenol (DNP)-treated (protonophore and mitochondrial uncoupler) rats. UCP3 mRNA and protein levels increased 8.1-fold (± 1.1) and 2.8-fold (± 0.8), respectively, in the T 3 -treated vs. control rat gastrocnemius muscle. 13 C NMR measurements of tricarboxylic acid cycle flux as an index of mitochondrial substrate oxidation were 61 ± 21, 148 ± 25, and 310 ± 48 nmol/g per min in the control, T 3 , and DNP groups, respectively. 31 P NMR saturation transfer measurements of unidirectional ATP synthesis flux were 83 ± 14, 84 ± 14, and 73 ± 7 nmol/g per s in the control, T 3 , and DNP groups, respectively. Together, these flux measurements, when normalized to the control group, suggest that acute administration of DNP (mitochondrial uncoupler) and chronic administration of T 3 decrease energy coupling by ≈80% and ≈60%, respectively, and that the latter treatment correlates with an increase in UCP3 mRNA and protein expression. This NMR approach could prove useful for exploring the regulation of uncoupling protein activity in vivo and elucidating its role in energy metabolism and obesity.

Published

2000

40. A novel13C NMR method to assess intracellular glucose concentration in muscle, in vivo

Author

Gerald I. Shulman, Alexander J. M. Rennings, Gary W. Cline, Beat M. Jucker, and Zlatko Trajanoski

Subjects

Blood Glucose, Intracellular Fluid, Male, medicine.medical_specialty, Magnetic Resonance Spectroscopy, Physiology, Endocrinology, Diabetes and Metabolism, Rats, Sprague-Dawley, In vivo, Physiology (medical), Internal medicine, medicine, Hyperinsulinemia, Animals, Insulin, Mannitol, Carbon Isotopes, Chemistry, Muscles, Skeletal muscle, Nuclear magnetic resonance spectroscopy, Carbon-13 NMR, medicine.disease, In vitro, Rats, Sprague dawley, Glucose, Endocrinology, medicine.anatomical_structure, Hyperglycemia, Glycogen, Intracellular

Abstract

Intracellular glucose concentration in skeletal muscle of awake rats was determined under conditions of hyperglycemic (10.2 ± 0.6 mM) hyperinsulinemia (∼1,200 pM) and hyperglycemic (20.8 ± 1.5 mM) hypoinsulinemia (13C nuclear magnetic resonance (NMR) spectroscopy during a prime-constant infusion of [1-13C]glucose and [1-13C]mannitol with either insulin (10 mU ⋅ kg−1⋅ min−1) or somatostatin (1.0 μg ⋅ kg−1⋅ min−1). Intracellular glucose was calculated as the difference between the concentrations of total tissue glucose (calculated from the in vivo13C NMR spectrum with mannitol as an internal concentration standard) and extracellular glucose, corrected by the ratio of intra- and extracellular water space. Extracellular concentration was corrected for an interstitial fluid-to-plasma glucose concentration gradient of 0.83 ± 0.07, determined by open-flow microperfusion. The mean ratio of intra- to extracellular glucose space, determined from the relative NMR signal intensities and concentrations of mannitol and total creatine, was 9.2 ± 1.1 (hyperglycemic hyperinsulinemia, n = 10), and 9.0 ± 1.7 (hyperglycemic hypoinsulinemia, n= 7). Mean muscle intracellular glucose concentration was

Published

1998

41. 13C and 31P NMR Studies on the Effects of Increased Plasma Free Fatty Acids on Intramuscular Glucose Metabolism in the Awake Rat

Author

Beat M. Jucker, Gary W. Cline, Gerald I. Shulman, and Alexander J. M. Rennings

Subjects

medicine.medical_specialty, Magnetic Resonance Spectroscopy, Glucose-6-Phosphate, Fatty Acids, Nonesterified, Carbohydrate metabolism, Models, Biological, Biochemistry, Rats, Sprague-Dawley, chemistry.chemical_compound, Hyperinsulinism, Internal medicine, medicine, Animals, Insulin, Glycolysis, Wakefulness, Infusions, Intravenous, Muscle, Skeletal, Pyruvates, Glycogen synthase, Molecular Biology, Carbon Isotopes, Alanine, Glycogen, biology, Skeletal muscle, Phosphorus, Cell Biology, Ketones, Glucose clamp technique, medicine.disease, Rats, Citric acid cycle, Kinetics, Glucose, Endocrinology, medicine.anatomical_structure, chemistry, Glucose Clamp Technique, Lactates, biology.protein

Abstract

The effects of increased plasma free fatty acids (FFA) on insulin-dependent whole body glucose disposal, skeletal muscle glycolysis, glycogen synthesis, pyruvate versus FFA/ketone oxidation, and glucose 6-phosphate (Glu-6-P) were investigated in the awake rat. A control group (glycerol-infused) and high plasma FFA group (Liposyn-infused) were clamped at euglycemia (approximately 6 mM)-hyperinsulinemia (10 milliunits/kg/min) throughout the experiment (180-240 min). In the initial experiment, 13C NMR was used to observe [1-13C]glucose incorporation into [1-13C]glycogen in the rat hindlimb for glycogen synthesis calculations and into [3-13C]lactate and [3-13C]alanine for glycolytic flux calculations. These experiments were followed by 31P NMR measurements of Glu-6-P changes under identical conditions of the initial experiment. Plasma FFA concentrations were 2.25 +/- 0.36 and 0.20 +/- 0.03 mM in the high plasma FFA and control groups respectively (p < 0.0005). Glucose infusion rates (Ginf) decreased significantly in the Liposyn-infused rats (29.5 +/- 0.7 and 27.2 +/- 1.2 mg/kg/min for control and high plasma FFA group, respectively, at 15 min to 30.7 +/- 2.3 and 17.7 +/- 1.3 mg/kg/min, respectively, at the end of the experiment, p < 0.002). Glycogen synthesis rates were 163 +/- 32 and 104 +/- 17 nmol/g/min, and glycolytic rates were 57.9 +/- 8.0 and 19. 5 +/- 3.6 nmol/g/min (p < 0.002) in the control and high plasma FFA groups, respectively. The relative flux of pyruvate versus free fatty acids and ketones entering the tricarboxylic acid cycle was greater in the control (57 +/- 9%) versus high plasma FFA group (25 +/- 4%) (p < 0.005) as assessed by [4-13C]glutamate/[3-13C]lactate steady state isotopic enrichment measurements. Finally, Glu-6-P concentrations increased by 29.8 +/- 7.0 and 52.8 +/- 12.3% (p < 0. 05) in the control and high plasma FFA groups, respectively, above their basal concentrations by 180 min. In conclusion, we have demonstrated the ability to use in vivo NMR to elucidate the metabolic fate of glucose within skeletal muscle of an awake rat during a euglycemic-hyperinsulinemic clamp and increased levels of plasma FFA. These data suggest that increased concentrations of plasma FFA inhibit insulin-stimulated muscle glucose metabolism in the rat through inhibition of glycolysis.

Published

1997

42. Technologies: preclinical imaging for drug development

Author

Robert W. Coatney, Hasan Alsaid, Paul M. Matthews, Beat M. Jucker, Kumar Changani, Christine A. Parker, and Sharon Ashworth

Subjects

Diagnostic Imaging, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Ultrasound, Drug Evaluation, Preclinical, Magnetic resonance imaging, Drug development, Drug Therapy, Positron emission tomography, Drug Discovery, medicine, Medical imaging, Molecular Medicine, Animals, Humans, Pharmacokinetics, Radiology, Tomography, business, Nuclear medicine, Preclinical imaging, Emission computed tomography

Abstract

Preclinical imaging with magnetic resonance imaging (MRI), computerised tomography (CT), ultrasound (US), positron emission tomography (PET) or single-photon emission computed tomography (SPECT) enable non-invasive measures of tissue structure, function or metabolism in vivo. The technologies can add value to preclinical studies by enabling dynamic pharmacological observations on the same animal and because of possibilities for relatively direct clinical translation. Potential benefits from the application of preclinical imaging should be considered routinely in drug development.

Published

2013

43. Cardiac fibrosis and diastolic dysfunction are highly correlated in a mouse chronic pressure‐overload model

Author

Weike Bao, Saul Needle, Fe Wright, Tao Wang, Drew DeLong, Beat M. Jucker, Alan R. Olzinski, Stephen H. Eisennagel, Christine G. Schnackenberg, Robert W. Coatney, and Steve Lenhard

Subjects

Pressure overload, medicine.medical_specialty, business.industry, Cardiac fibrosis, Aortic constriction, Diastole, medicine.disease, Biochemistry, Internal medicine, cardiovascular system, Genetics, medicine, Cardiology, business, Molecular Biology, Biotechnology

Abstract

The purpose of this study was to determine which measurements of diastolic dysfunction are most correlated with cardiac fibrosis. Mice were subjected to Sham (n=7) or transverse aortic constriction...

Published

2013

44. Longitudinal assessment of systolic and diastolic function using conventional and speckle tracking echocardiography following acute ischemia and prolonged reperfusion in the rat

Author

Christine G. Schnackenberg, Kendall S. Frazier, Weike Bao, Zhaohui Ao, Fe Wright, Robert W. Coatney, Rosanna C. Mirabile, and Beat M. Jucker

Subjects

medicine.medical_specialty, business.industry, Internal medicine, Genetics, medicine, Cardiology, Diastolic function, Speckle tracking echocardiography, business, Molecular Biology, Biochemistry, Biotechnology, Acute ischemia

Published

2013

45. Examining the relationship between exercise tolerance and isoproterenol-based cardiac reserve in murine models of heart failure

Author

Weike Bao, Daniel A. Richards, Mary V. Rambo, Stephen C. Lenhard, Mark E. Burgert, and Beat M. Jucker

Subjects

Male, medicine.medical_specialty, Cardiotonic Agents, Physiology, Physical Exertion, Myocardial Infarction, Exercise intolerance, Ventricular Function, Left, Mice, Oxygen Consumption, Physiology (medical), Internal medicine, medicine, Animals, Humans, Myocardial infarction, Treadmill, Heart Failure, Exercise Tolerance, medicine.diagnostic_test, business.industry, Isoproterenol, Cardiac reserve, Magnetic resonance imaging, Adrenergic beta-Agonists, medicine.disease, Magnetic Resonance Imaging, Mice, Inbred C57BL, Disease Models, Animal, Heart failure, Cardiology, Exercise Test, medicine.symptom, business

Abstract

The loss of cardiac reserve is, in part, responsible for exercise intolerance in late-stage heart failure (HF). Exercise tolerance testing (ETT) has been performed in mouse models of HF; however, treadmill performance and at-rest cardiac indexes determined by magnetic resonance imaging (MRI) rarely correlate. The present study adopted a stress-MRI technique for comparison with ETT in HF models, using isoproterenol (ISO) to evoke cardiac reserve responses. Male C57BL/6J mice were randomly subjected to myocardial infarction (MI), transverse aortic constriction (TAC), or sham surgery under general anesthesia. Mice underwent serial ETT on a graded treadmill with follow-up ISO stress-MRI. TAC mice showed consistent exercise intolerance, with a 16.2% reduction in peak oxygen consumption vs. sham at 15-wk postsurgery (WPS). MI and sham mice had similar peak oxygen consumption from 7 WPS onward. Time to a respiratory exchange ratio of 1.0 correlated with ETT distance ( r = 0.64; P < 0.001). The change in ejection fraction under ISO stress was reduced in HF mice at 4 WPS [10.1 ± 3.9% change (Δ) and 8.9 ± 3.5%Δ in MI and TAC, respectively, compared with 32.0 ± 3.5%Δ in sham; P < 0.001]. However, cardiac reserve differences between surgery groups were not observed at 16 WPS in terms of ejection fraction or cardiac output. In addition, ETT did not correlate with cardiac indexes under ISO stress. In conclusion, ISO stress was unable to reflect consistent differences in ETT between HF and healthy mice, suggesting cardiac-specific indexes are not the sole factors in defining exercise intolerance in mouse HF models.

Published

2013

46. Characterization of a novel PERK kinase inhibitor with antitumor and antiangiogenic activity

Author

Nathan Gaul, Rakesh Kumar, Hasan Alsaid, Charity Atkins, Beat M. Jucker, Elisabeth A. Minthorn, Jeffrey M. Axten, Qi Liu, Shu-Yun Zhang, David J. Figueroa, Katherine G. Moss, Thomas B. Stanley, Aaron S. Goetz, Anthony E. Choudhry, and Brent Sanders

Subjects

endocrine system, Cancer Research, Indoles, Kinase, Adenine, Gene Expression Profiling, ATF4, Autophosphorylation, Angiogenesis Inhibitors, Antineoplastic Agents, Biology, Pharmacology, Mice, eIF-2 Kinase, Oncology, Biochemistry, Enhancer binding, Eukaryotic initiation factor, Unfolded protein response, Animals, PERK inhibitors, Female, Signal transduction, Protein Kinase Inhibitors

Abstract

The unfolded protein response (UPR) is a signal transduction pathway that coordinates cellular adaptation to microenvironmental stresses that include hypoxia, nutrient deprivation, and change in redox status. These stress stimuli are common in many tumors and thus targeting components of the UPR signaling is an attractive therapeutic approach. We have identified a first-in-class, small molecule inhibitor of the eukaryotic initiation factor 2-alpha kinase 3 (EIF2AK3) or PERK, one of the three mediators of UPR signaling. GSK2656157 is an ATP-competitive inhibitor of PERK enzyme activity with an IC50 of 0.9 nmol/L. It is highly selective for PERK with IC50 values >100 nmol/L against a panel of 300 kinases. GSK2656157 inhibits PERK activity in cells with an IC50 in the range of 10–30 nmol/L as shown by inhibition of stress-induced PERK autophosphorylation, eIF2α substrate phosphorylation, together with corresponding decreases in ATF4 and CAAT/enhancer binding protein homologous protein (CHOP) in multiple cell lines. Oral administration of GSK2656157 to mice shows a dose- and time-dependent pharmacodynamic response in pancreas as measured by PERK autophosphorylation. Twice daily dosing of GSK2656157 results in dose-dependent inhibition of multiple human tumor xenografts growth in mice. Altered amino acid metabolism, decreased blood vessel density, and vascular perfusion are potential mechanisms for the observed antitumor effect. However, despite its antitumor activity, given the on-target pharmacologic effects of PERK inhibition on pancreatic function, development of any PERK inhibitor in human subjects would need to be cautiously pursued in cancer patients. Cancer Res; 73(6); 1993–2002. ©2012 AACR.

Published

2013

47. Cardioprotection by systemic dosing of thymosin beta four following ischemic myocardial injury

Author

James Tunstead, Weike Bao, Stephen C. Lenhard, Beat M. Jucker, Bao Hoang, G. C. Teg Pipes, Victoria L. T. Ballard, Saul Needle, and Robert N. Willette

Subjects

Cardiac function curve, medicine.medical_specialty, Hemodynamics, Infarction, Cardioprotection, angiogenesis, Internal medicine, Medicine, Pharmacology (medical), Original Research Article, Dosing, Pharmacology, Ejection fraction, business.industry, lcsh:RM1-950, medicine.disease, ischemia/reperfusion, Surgery, thymosin beta four, Thymosin beta-4, myocardial ischemia, lcsh:Therapeutics. Pharmacology, medicine.anatomical_structure, Cardiology, business, Blood vessel

Abstract

Thymosin beta 4 (Tβ4) was previously shown to reduce infarct size and improve contractile performance in chronic myocardial ischemic injury via two phases of action: an acute phase, just after injury, when Tβ4 preserves ischemic myocardium via anti-apoptotic or anti-inflammatory mechanisms; and a chronic phase, when Tβ4 activates the growth of vascular or cardiac progenitor cells. In order to differentiate between the effects of Tβ4 during the acute and during the chronic phases, and also in order to obtain detailed hemodynamic and biomarker data on the effects of Tβ4 treatment suitable for use in clinical studies, we tested Tβ4 in a rat model of chronic myocardial ischemia using two dosing regimens: short term dosing (Tβ4 administered only during the first three days following injury), and long term dosing (Tβ4 administered during the first three days following injury and also every third day until the end of the study). Tβ4 administered throughout the study reduced infarct size and resulted in significant improvements in hemodynamic performance; however, chamber volumes and ejection fractions were not significantly improved. Tβ4 administered only during the first three days following injury tended to reduce infarct size, chamber volumes and improve hemodynamic performance. Plasma biomarkers of myocyte injury were significantly reduced by Tβ4 treatment during the acute injury period, and plasma ANP levels were significantly reduced in both dosing groups. Surprisingly, neither acute nor chronic Tβ4 treatment significantly increased blood vessel density in peri-infarct regions. These results suggest the following: repeated dosing may be required to achieve clinically measureable improvements in cardiac function post-myocardial infarction; improvement in cardiac function may be observed in the absence of a high degree of angiogenesis; and that plasma biomarkers of cardiac function and myocardial injury are sensitive pharmacodynamic biomarkers of the effects of Tβ4.

Published

2013

48. An Orally Active TRPV4 Channel Blocker Prevents and Resolves Pulmonary Edema Induced by Heart Failure

Author

James Tunstead, Robert N. Willette, Linda N. Casillas, Mui Cheung, Guosen Ye, Ming-Yuan Jian, Hasan Alsaid, John J. Lepore, Earl Gordon, John R. Toomey, Daniel S Matasic, Kristeen Maniscalco-Hauk, Chris James, J. Larkin, Kevin S. Thorneloe, Eidam Hilary Schenck, Stephen C. Lenhard, Krista B. Goodman, Lorena A. Kallal, Brian Donovan, Alan R. Olzinski, Pu Qin, Mary I. Townsley, Christine G. Schnackenberg, Lou Elefante, Weike Bao, John A. Krawiec, Theresa J. Roethke, Irina M. Lozinskaya, Kalindi Vaidya, Elizabeth A. Davenport, Melissa H. Costell, Robert W. Marquis, Beat M. Jucker, Mark E. Burgert, and Anna Waszkiewicz

Subjects

medicine.medical_specialty, Endothelium, Administration, Oral, TRPV Cation Channels, Blood Pressure, Pulmonary Edema, Vascular permeability, In Vitro Techniques, Permeability, Mice, Heart Rate, Membrane Transport Modulators, Internal medicine, Edema, Animals, Humans, Medicine, Myocardial infarction, Diuretics, Lung, Heart Failure, Mice, Knockout, business.industry, General Medicine, Water-Electrolyte Balance, Pulmonary edema, medicine.disease, Rats, Disease Models, Animal, Protein Transport, medicine.anatomical_structure, Blood pressure, Anesthesia, Heart failure, Cardiology, Calcium, medicine.symptom, business, Ion Channel Gating

Abstract

Pulmonary edema resulting from high pulmonary venous pressure (PVP) is a major cause of morbidity and mortality in heart failure (HF) patients, but current treatment options demonstrate substantial limitations. Recent evidence from rodent lungs suggests that PVP-induced edema is driven by activation of pulmonary capillary endothelial transient receptor potential vanilloid 4 (TRPV4) channels. To examine the therapeutic potential of this mechanism, we evaluated TRPV4 expression in human congestive HF lungs and developed small-molecule TRPV4 channel blockers for testing in animal models of HF. TRPV4 immunolabeling of human lung sections demonstrated expression of TRPV4 in the pulmonary vasculature that was enhanced in sections from HF patients compared to controls. GSK2193874 was identified as a selective, orally active TRPV4 blocker that inhibits Ca(2+) influx through recombinant TRPV4 channels and native endothelial TRPV4 currents. In isolated rodent and canine lungs, TRPV4 blockade prevented the increased vascular permeability and resultant pulmonary edema associated with elevated PVP. Furthermore, in both acute and chronic HF models, GSK2193874 pretreatment inhibited the formation of pulmonary edema and enhanced arterial oxygenation. Finally, GSK2193874 treatment resolved pulmonary edema already established by myocardial infarction in mice. These findings identify a crucial role for TRPV4 in the formation of HF-induced pulmonary edema and suggest that TRPV4 blockade is a potential therapeutic strategy for HF patients.

Published

2012

49. Comparison of Soluble Guanylate Cyclase Stimulators and Activators in Models of Cardiovascular Disease Associated with Oxidative Stress

Author

John J. Lepore, Anne Marie Jeanne Bouillot, Kristeen Maniscalco, Olivier Mirguet, Alan R. Olzinski, Christine G. Schnackenberg, Larry J. Jolivette, John J. Upson, Nerina Dodic, Françoise Gellibert, Lisa A. Morgan, Shu Fang Zhao, Pascal Grondin, Robert W. Coatney, Beat M. Jucker, David J. Behm, Victoria L. T. Ballard, Robert N. Willette, Roberta E. Bernard, Nicolas Ancellin, Kenny Herry, and Melissa H. Costell

Subjects

soluble guanylate cyclase, SHR-SP, medicine.medical_specialty, Mean arterial pressure, End organ damage, Vasodilation, Left ventricular hypertrophy, medicine.disease_cause, Nitric oxide, BAY 60-4552, chemistry.chemical_compound, Internal medicine, Medicine, Pharmacology (medical), Original Research, GSK2181236A, Pharmacology, business.industry, lcsh:RM1-950, VASP, medicine.disease, cGMP, Endocrinology, lcsh:Therapeutics. Pharmacology, chemistry, cardiovascular system, Microalbuminuria, Sodium nitroprusside, business, Oxidative stress, medicine.drug

Abstract

Soluble guanylate cyclase (sGC), the primary mediator of nitric oxide (NO) bioactivity, exists as reduced (NO-sensitive) and oxidized (NO-insensitive) forms. We tested the hypothesis that the cardiovascular protective effects of NO-insensitive sGC activation would be potentiated under conditions of oxidative stress compared to those of NO-sensitive sGC stimulation. The cardiovascular effects of the NO-insensitive sGC activator GSK2181236A [a low, non-depressor dose, and a high dose which lowered mean arterial pressure (MAP) by 5-10 mmHg] and those of equi-efficacious doses of the NO-sensitive sGC stimulator BAY 60-4552 were assessed in (1) Sprague Dawley rats during coronary artery ischemia/reperfusion (I/R) and (2) spontaneously hypertensive stroke prone rats (SHR-SP) on a high salt/fat diet (HSFD). In I/R, neither compound reduced infarct size 24 h after reperfusion. In SHR-SP, HSFD increased MAP, urine output, microalbuminuria, and mortality, caused left ventricular hypertrophy with preserved ejection fraction, and impaired endothelium-dependent vasorelaxation. The low dose of BAY 60-4552, but not that of GSK2181236A, decreased urine output, and improved survival. Conversely, the low dose of GSK2181236A, but not that of BAY 60-4552, attenuated the development of cardiac hypertrophy. The high doses of both compounds similarly attenuated cardiac hypertrophy and improved survival. In addition to these effects, the high dose of BAY 60-4552 reduced urine output and microalbuminuria and attenuated the increase in MAP to a greater extent than did GSK2181236A. Neither compound improved endothelium-dependent vasorelaxation. In SHR-SP isolated aorta, the vasodilatory responses to the NO-dependent compounds carbachol and sodium nitroprusside were attenuated by HSFD. In contrast, the vasodilatory responses to both GSK2181236A and BAY 60-4552 were unaltered by HSFD, indicating that reduced NO-bioavailability and not changes in the oxidative state of sGC is responsible for the vascular dysfunction. In summary, GSK2181236A and BAY 60-4552 provide partial benefit against hypertension-induced end-organ damage. The differential beneficial effects observed between these compounds could reflect tissue-specific changes in the oxidative state of sGC and might help direct the clinical development of these novel classes of therapeutic agents.

Published

2012

50. Liver glycogen turnover in fed and fasted humans

Author

Robert G. Shulman, Inger Magnusson, Douglas L. Rothman, Beat M. Jucker, Gary W. Cline, and Gerald I. Shulman

Subjects

Adult, Blood Glucose, Male, Uridine Diphosphate Glucose, medicine.medical_specialty, Magnetic Resonance Spectroscopy, Glycogenolysis, Physiology, Endocrinology, Diabetes and Metabolism, Biology, Carbohydrate metabolism, Models, Biological, Eating, chemistry.chemical_compound, Physiology (medical), Internal medicine, medicine, Humans, Insulin, Glycogen synthase, Carbon Isotopes, Glycogen, Fasting, Metabolism, Glucose clamp technique, Liver Glycogen, Kinetics, Glucose, Endocrinology, chemistry, Turnover, Glycogenesis, Hyperglycemia, Glucose Clamp Technique, biology.protein, Mathematics

Abstract

Whether liver glycogen synthesis and breakdown occur simultaneously during net glycogen synthesis was assessed in fed and fasted healthy humans. The peak intensity of the carbon-1 (C1) resonance of the glycosyl units of glycogen was monitored with 13C nuclear magnetic resonance spectroscopy during [1-13C]glucose infusion followed by unlabeled glucose infusion. The C1 peak intensity increased almost linearly during the [1-13C]glucose infusion, reflecting a near linear rate of glycogen synthesis. When switched to unlabeled glucose, the C1 peak intensity reached a plateau in the fasted subjects and declined in the fed subjects, reflecting active glycogenolysis during a time of net glycogen synthesis. We conclude that liver glycogen synthesis and degradation occur simultaneously in humans under conditions of net glycogen synthesis. The relative turnover rate was significantly higher in the fed (57 +/- 3%) than in the fasted state (31 +/- 8%; P < 0.01). The results indicate that glycogen may regulate its rate of breakdown and that liver glycogen turnover may be an important factor in limiting the accumulation of liver glycogen in humans.

Published

1994