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1. Proteostasis Modulation in Germline Missense von Hippel Lindau Disease

Author

Prashant Chittiboina, Debjani Mandal, Alejandro Bugarini, David T. Asuzu, Dustin Mullaney, Panagiotis Mastorakos, Stefan Stoica, Reinier Alvarez, Gretchen Scott, Dragan Maric, Abdel Elkahloun, Zhengping Zhuang, Emily Y. Chew, Chunzhang Yang, Marston Linehan, and Russell R. Lonser

Subjects
Cancer Research, Oncology
Abstract

Purpose: Missense mutated von Hippel Lindau (VHL) protein (pVHL) maintains intrinsic function but undergoes proteasomal degradation and tumor initiation and/or progression in VHL disease. Vorinostat can rescue missense mutated pVHL and arrest tumor growth in preclinical models. We asked whether short-term oral vorinostat could rescue pVHL in central nervous system hemangioblastomas in patients with germline missense VHL. Patients and Methods: We administered oral vorinostat to 7 subjects (ages 46.0 ± 14.5 years) and then removed symptomatic hemangioblastomas surgically (ClinicalTrials.gov identifier NCT02108002). Results: Vorinostat was tolerated without serious adverse events by all patients. pVHL expression was elevated in neoplastic stromal cells compared with untreated hemangioblastomas from same patients. We found transcriptional suppression of downstream hypoxia-inducible factor (HIF) effectors. Mechanistically, vorinostat prevented Hsp90 recruitment to mutated pVHL in vitro. The effects of vorinostat on the Hsp90–pVHL interaction, pVHL rescue, and transcriptional repression of downstream HIF effectors was independent of the location of the missense mutation on the VHL locus. We confirmed a neoplastic stromal cell–specific effect in suppression of protumorigenic pathways with single-nucleus transcriptomic profiling. Conclusions: We found that oral vorinostat treatment in patients with germline missense VHL mutations has a potent biologic effect that warrants further clinical study. These results provide biologic evidence to support the use of proteostasis modulation for the treatment of syndromic solid tumors involving protein misfolding. Proteostasis modulation with vorinostat rescues missense mutated VHL protein. Further clinical trials are needed to demonstrate tumor growth arrest.

Published
2023
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3. ApoER2-Dab1 disruption as the origin of pTau-related neurodegeneration in sporadic Alzheimer’s disease

Author

Christopher E. Ramsden, Daisy Zamora, Mark S. Horowitz, Jahandar Jahanipour, Gregory S. Keyes, Xiufeng Li, Helen C. Murray, Maurice A. Curtis, Richard M. Faull, Andrea Sedlock, and Dragan Maric

Abstract

BACKGROUNDSporadic Alzheimer’s disease (sAD) is not a global brain disease. Specific regions, layers and neurons degenerate early while others remain untouched even in advanced disease. The prevailing model used to explain this selective neurodegeneration—prion-like Tau spread—has key limitations and is not easily integrated with other defining sAD features. Instead, we propose that in humans Tau hyperphosphorylation occurs locally via disruption in ApoER2-Dab1 signaling and thus the presence of ApoER2 in neuronal membranes confers vulnerability to degeneration. Further, we propose that disruption of the Reelin/ApoE/ApoJ-ApoER2-Dab1 P85α-LIMK1-Tau-PSD95 (RAAAD-P-LTP) pathway induces deficits in memory and cognition by impeding neuronal lipoprotein internalization and destabilizing actin, microtubules, and synapses. This new model is based in part on our recent finding that ApoER2-Dab1 disruption is evident in entorhinal-hippocampal terminal zones in sAD. Here, we hypothesized that neurons that degenerate in the earliest stages of sAD (1) strongly express ApoER2 and (2) show evidence of ApoER2-Dab1 disruption through co-accumulation of multiple RAAAD-P-LTP components.METHODSWe appliedin situhybridization and immunohistochemistry to characterize ApoER2 expression and accumulation of RAAAD-P-LTP components in five regions that are prone to early pTau pathology in 64 rapidly autopsied cases spanning the clinicopathological spectrum of sAD.RESULTSWe found that: (1) selectively vulnerable neuron populations strongly express ApoER2; (2) numerous RAAAD P-LTP pathway components accumulate in neuritic plaques and abnormal neurons; and (3) RAAAD-P-LTP components were higher in MCI and sAD cases and correlated with histological progression and cognitive deficits. Multiplex-IHC revealed that Dab1, pP85αTyr607, pLIMK1Thr508, pTau and pPSD95Thr19accumulated together within dystrophic dendrites and soma of ApoER2-expressing neurons in the vicinity of ApoE/ApoJ enriched extracellular plaques. These observations provide evidence for molecular derangements that can be traced back to ApoER2-Dab1 disruption, in each of the sampled regions, layers, and neuron populations that are prone to early pTau pathology.CONCLUSIONFindings support the RAAAD-P-LTP hypothesis, a unifying model that implicates dendritic ApoER2-Dab1 disruption as the major driver of both pTau accumulation and neurodegeneration in sAD. This model provides a new conceptual framework to explain why specific neurons degenerate and identifies RAAAD-P-LTP pathway components as potential mechanism-based biomarkers and therapeutic targets for sAD.

Published
2023
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7. Supplementary Methods and Key Resources Table 1 from Proteostasis Modulation in Germline Missense von Hippel Lindau Disease

Author

Russell R. Lonser, Marston Linehan, Chunzhang Yang, Emily Y. Chew, Zhengping Zhuang, Abdel Elkahloun, Dragan Maric, Gretchen Scott, Reinier Alvarez, Stefan Stoica, Panagiotis Mastorakos, Dustin Mullaney, David T. Asuzu, Alejandro Bugarini, Debjani Mandal, and Prashant Chittiboina

Abstract

Supplementary Methods and Key Resources Table

Published
2023
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12. Data from Novel Targeting of Transcription and Metabolism in Glioblastoma

Author

Jing Wu, Mark R. Gilbert, Chunzhang Yang, Zhengping Zhuang, Mones Abu-Asab, Mioara Larion, Thomas Estok, Kristan Meetze, Wei Zhang, Orieta Celiku, Aiguo Li, Dragan Maric, Adrian Lita, Gabriel Vasconcelos, Hallie Lappin, Li-Yuan Chen, Qi Zhang, Hua Song, Herui Wang, Robert Chen, and Yu-Ting Su

Abstract

Purpose: Glioblastoma (GBM) is highly resistant to treatment, largely due to disease heterogeneity and resistance mechanisms. We sought to investigate a promising drug that can inhibit multiple aspects of cancer cell survival mechanisms and become an effective therapeutic for GBM patients.Experimental Design: To investigate TG02, an agent with known penetration of the blood–brain barrier, we examined the effects as single agent and in combination with temozolomide, a commonly used chemotherapy in GBM. We used human GBM cells and a syngeneic mouse orthotopic GBM model, evaluating survival and the pharmacodynamics of TG02. Mechanistic studies included TG02-induced transcriptional regulation, apoptosis, and RNA sequencing in treated GBM cells as well as the investigation of mitochondrial and glycolytic function assays.Results: We demonstrated that TG02 inhibited cell proliferation, induced cell death, and synergized with temozolomide in GBM cells with different genetic background but not in astrocytes. TG02-induced cytotoxicity was blocked by the overexpression of phosphorylated CDK9, suggesting a CDK9-dependent cell killing. TG02 suppressed transcriptional progression of antiapoptotic proteins and induced apoptosis in GBM cells. We further demonstrated that TG02 caused mitochondrial dysfunction and glycolytic suppression and ultimately ATP depletion in GBM. A prolonged survival was observed in GBM mice receiving combined treatment of TG02 and temozolomide. The TG02-induced decrease of CDK9 phosphorylation was confirmed in the brain tumor tissue.Conclusions: TG02 inhibits multiple survival mechanisms and synergistically decreases energy production with temozolomide, representing a promising therapeutic strategy in GBM, currently under investigation in an ongoing clinical trial. Clin Cancer Res; 24(5); 1124–37. ©2017 AACR.

Published
2023
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13. Supplementary Table 1 from Gliomagenesis Arising from Pten- and Ink4a/Arf-Deficient Neural Progenitor Cells Is Mediated by the p53-Fbxw7/Cdc4 Pathway, Which Controls c-Myc

Author

Howard A. Fine, Wei Zhang, Svetlana Kotliarova, Aiguo Li, Hua Song, Dragan Maric, Peter O. Bauer, Chen Lai, Kevin Woolard, and Hong Sug Kim

Abstract

PDF file, 322K, Pten-/-Ink4a/Arf-/-mNSCs induced gliomas. Intracranial Pten-/-Ink4a/Arf-/-mNSCs injected mice generated different tumor phenotypes with different survivals. II: WHO Grade II astrocytoma; III: WHO Grade III astrocytoma; IV: WHO Grade IV astrocytoma (GBM).

Published
2023
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15. Supplementary Materials and Methods, Figures 1 - 4, Table 1 from Tumor-Infiltrating Myeloid Cells Activate Dll4/Notch/TGF-β Signaling to Drive Malignant Progression

Author

Giovanna Tosato, Dragan Maric, David Sánchez-Martín, Hyeongil Kwak, Ombretta Salvucci, Dunrui Wang, Kan Jiang, and Hidetaka Ohnuki

Abstract

PDF file - 1522KB, Supplementary Figure S1: shows the kinetics of EL4, LLC1 and B16F10 tumor growth in WT and Gfi1-KO mice. Supplemental Figure S2: analysis of EL4 and LLC1 tumor vascularization (A); distribution and typical profiles of CD11b+Ly6C+Ly6G- and CD11b+Ly6C+Ly6G+ in spleen and bone marrow of naive and tumor-bearing mice (B-F). Supplementary Figure S3: typical sorting profiles of LLC1 tumorinfiltrating cell populations (A); expression profiles of Notch ligands and receptors in tumor cells and tumor-infiltrating populations (B); cartoon representation of interacting Notch ligands and receptors. Supplementary Figure S4: kinetic analysis of tumor growth with or without DAPT. Supplementary Table 1: Extensive gene expression profiling by qPCR.

Published
2023
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19. Supplementary Table 1 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Author

Howard A. Fine, Jeongwu Lee, Jean Claude Zenklusen, Dragan Maric, Rolanda Bailey, Wei Zhang, Hua Song, Yuri Kotliarov, Lara C. Kovell, Sandra Pastorino, and Svetlana Kotliarova

Abstract

Supplementary Table 1 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Published
2023
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23. Data from Tumor-Infiltrating Myeloid Cells Activate Dll4/Notch/TGF-β Signaling to Drive Malignant Progression

Author

Giovanna Tosato, Dragan Maric, David Sánchez-Martín, Hyeongil Kwak, Ombretta Salvucci, Dunrui Wang, Kan Jiang, and Hidetaka Ohnuki

Abstract

Myeloid cells that orchestrate malignant progression in the tumor microenvironment offer targets for a generalized strategy to attack solid tumors. Through an analysis of tumor microenvironments, we explored an experimental model of lung cancer that uncovered a network of Dll4/Notch/TGF-β1 signals that links myeloid cells to cancer progression. Myeloid cells attracted to the tumor microenvironment by the tumor-derived cytokines CCL2 and M-CSF expressed increased levels of the Notch ligand Dll4, thereby activating Notch signaling in the tumor cells and amplifying tumor-intrinsic Notch activation. Heightened Dll4/Notch signaling in tumor cells magnified TGF-β–induced pSMAD2/3 signaling and was required to sustain TGF-β–induced tumor cell growth. Conversely, Notch blockade reduced TGF-β signaling and limited lung carcinoma tumor progression. Corroborating these findings, by interrogating RNAseq results from tumor and adjacent normal tissue in clinical specimens of human head and neck squamous carcinoma, we found evidence that TGF-β/Notch crosstalk contributed to progression. In summary, the myeloid cell-carcinoma signaling network we describe uncovers novel mechanistic links between the tumor microenvironment and tumor growth, highlighting new opportunities to target tumors where this network is active. Cancer Res; 74(7); 2038–49. ©2014 AACR.

Published
2023
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25. Supplementary Table 3 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Author

Howard A. Fine, Jeongwu Lee, Jean Claude Zenklusen, Dragan Maric, Rolanda Bailey, Wei Zhang, Hua Song, Yuri Kotliarov, Lara C. Kovell, Sandra Pastorino, and Svetlana Kotliarova

Abstract

Supplementary Table 3 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Published
2023
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26. Supplementary Figures 1-12 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Author

Howard A. Fine, Jeongwu Lee, Jean Claude Zenklusen, Dragan Maric, Rolanda Bailey, Wei Zhang, Hua Song, Yuri Kotliarov, Lara C. Kovell, Sandra Pastorino, and Svetlana Kotliarova

Abstract

Supplementary Figures 1-12 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Published
2023
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27. Supplementary Table 2 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Author

Howard A. Fine, Jeongwu Lee, Jean Claude Zenklusen, Dragan Maric, Rolanda Bailey, Wei Zhang, Hua Song, Yuri Kotliarov, Lara C. Kovell, Sandra Pastorino, and Svetlana Kotliarova

Abstract

Supplementary Table 2 from Glycogen Synthase Kinase-3 Inhibition Induces Glioma Cell Death through c-MYC, Nuclear Factor-κB, and Glucose Regulation

Published
2023
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28. Data from Kaposi Sarcoma Herpesvirus Promotes Endothelial-to-Mesenchymal Transition through Notch-Dependent Signaling

Author

Giovanna Tosato, Robert Yarchoan, Mark N. Polizzotto, Thomas S. Uldrick, Dragan Maric, Ombretta Salvucci, Peter J. McCormick, Georgina Espigol-Frigole, and Paola Gasperini

Abstract

Endothelial-to-mesenchymal transition (EndMT) is now widely considered a pivotal contributor to cancer progression. In this study, we show that the Kaposi's sarcoma (KS)–associated herpesvirus (KSHV) is a sufficient cause of EndMT, potentially helping to explain the aggressiveness of KS that occurs commonly in AIDS patients. Upon KSHV infection, primary dermal microvascular endothelial cells lost expression of endothelial markers and acquired expression of mesenchymal markers, displaying new invasive and migratory properties along with increased survival. KSHV activated Notch-induced transcription factors Slug and ZEB1, and canonical Notch signaling was required for KSHV-induced EndMT. In contrast, KSHV did not utilize the TGFβ signaling pathway, which has also been linked to EndMT. Within KS lesions, KSHV-infected spindle cells displayed features compatible with KSHV-induced EndMT including a complex phenotype of endothelial and mesenchymal properties, Notch activity, and nuclear ZEB1 expression. Our results show that KSHV engages the EndMT program to increase the invasiveness and survival of infected endothelial cells, traits that likely contribute to viral persistence and malignant progression. One important implication of our findings is that therapeutic approaches to disrupt the Notch pathway may offer novel approaches for KS treatment. Cancer Res; 72(5); 1157–69. ©2012 AACR.

Published
2023
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29. Supplementary Table 2 from Gliomagenesis Arising from Pten- and Ink4a/Arf-Deficient Neural Progenitor Cells Is Mediated by the p53-Fbxw7/Cdc4 Pathway, Which Controls c-Myc

Author

Howard A. Fine, Wei Zhang, Svetlana Kotliarova, Aiguo Li, Hua Song, Dragan Maric, Peter O. Bauer, Chen Lai, Kevin Woolard, and Hong Sug Kim

Abstract

PDF file, 345K, Tumors and p53 mutations. All tumors contained one of two different types of p53 mutations (Cys132Trp and Arg270Cys).

Published
2023
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30. Lipid Peroxidation Induced ApoE Receptor-Ligand Disruption as a Unifying Hypothesis Underlying Sporadic Alzheimer’s Disease in Humans

Author

Christopher E. Ramsden, Gregory S. Keyes, Elizabeth Calzada, Mark S. Horowitz, Daisy Zamora, Jahandar Jahanipour, Andrea Sedlock, Fred E. Indig, Ruin Moaddel, Dimitrios Kapogiannis, and Dragan Maric

Subjects
Aldehydes, Extracellular Matrix Proteins, Cell Adhesion Molecules, Neuronal, General Neuroscience, Serine Endopeptidases, Nerve Tissue Proteins, Plaque, Amyloid, General Medicine, Ligands, Article, Reelin Protein, Psychiatry and Mental health, Clinical Psychology, Apolipoproteins E, Receptors, LDL, Alzheimer Disease, Humans, lipids (amino acids, peptides, and proteins), Lipid Peroxidation, Geriatrics and Gerontology, LDL-Receptor Related Proteins, Low Density Lipoprotein Receptor-Related Protein-1
Abstract

Background: Sporadic Alzheimer’s disease (sAD) lacks a unifying hypothesis that can account for the lipid peroxidation observed early in the disease, enrichment of ApoE in the core of neuritic plaques, hallmark plaques and tangles, and selective vulnerability of entorhinal-hippocampal structures. Objective: We hypothesized that 1) high expression of ApoER2 (receptor for ApoE and Reelin) helps explain this anatomical vulnerability; 2) lipid peroxidation of ApoE and ApoER2 contributes to sAD pathogenesis, by disrupting neuronal ApoE delivery and Reelin-ApoER2-Dab1 signaling cascades. Methods: In vitro biochemical experiments; Single-marker and multiplex fluorescence-immunohistochemistry (IHC) in postmortem specimens from 26 individuals who died cognitively normal, with mild cognitive impairment or with sAD. Results: ApoE and ApoER2 peptides and proteins were susceptible to attack by reactive lipid aldehydes, generating lipid-protein adducts and crosslinked ApoE-ApoER2 complexes. Using in situ hybridization alongside IHC, we observed that: 1) ApoER2 is strongly expressed in terminal zones of the entorhinal-hippocampal ‘perforant path’ projections that underlie memory; 2) ApoE, lipid aldehyde-modified ApoE, Reelin, ApoER2, and the downstream Reelin-ApoER2 cascade components Dab1 and Thr19-phosphorylated PSD95 accumulated in the vicinity of neuritic plaques in perforant path terminal zones in sAD cases; 3) several ApoE/Reelin-ApoER2-Dab1 pathway markers were higher in sAD cases and positively correlated with histological progression and cognitive deficits. Conclusion: Results demonstrate derangements in multiple ApoE/Reelin-ApoER2-Dab1 axis components in perforant path terminal zones in sAD and provide proof-of-concept that ApoE and ApoER2 are vulnerable to aldehyde-induced adduction and crosslinking. Findings provide the foundation for a unifying hypothesis implicating lipid peroxidation of ApoE and ApoE receptors in sAD.

Published
2022
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31. IDH-mutated gliomas promote epileptogenesis through d-2-hydroxyglutarate-dependent mTOR hyperactivation

Author

Armin Mortazavi, Islam Fayed, Muzna Bachani, Tyrone Dowdy, Jahandar Jahanipour, Anas Khan, Jemima Owotade, Stuart Walbridge, Sara K Inati, Joseph Steiner, Jing Wu, Mark Gilbert, Chun Zhang Yang, Mioara Larion, Dragan Maric, Alexander Ksendzovsky, and Kareem A Zaghloul

Subjects
Cancer Research, Epilepsy, Brain Neoplasms, TOR Serine-Threonine Kinases, Glioma, Isocitrate Dehydrogenase, Glutarates, Oncology, Seizures, Mutation, Basic and Translational Investigations, Quality of Life, Humans, Neurology (clinical)
Abstract

Background Uncontrolled seizures in patients with gliomas have a significant impact on quality of life and morbidity, yet the mechanisms through which these tumors cause seizures remain unknown. Here, we hypothesize that the active metabolite d-2-hydroxyglutarate (d-2-HG) produced by the IDH-mutant enzyme leads to metabolic disruptions in surrounding cortical neurons that consequently promote seizures. Methods We use a complementary study of in vitro neuron-glial cultures and electrographically sorted human cortical tissue from patients with IDH-mutant gliomas to test this hypothesis. We utilize micro-electrode arrays for in vitro electrophysiological studies in combination with pharmacological manipulations and biochemical studies to better elucidate the impact of d-2-HG on cortical metabolism and neuronal spiking activity. Results We demonstrate that d-2-HG leads to increased neuronal spiking activity and promotes a distinct metabolic profile in surrounding neurons, evidenced by distinct metabolomic shifts and increased LDHA expression, as well as upregulation of mTOR signaling. The increases in neuronal activity are induced by mTOR activation and reversed with mTOR inhibition. Conclusion Together, our data suggest that metabolic disruptions in the surrounding cortex due to d-2-HG may be a driving event for epileptogenesis in patients with IDH-mutant gliomas.

Published
2023

32. Chronic neuronal activation leads to elevated lactate dehydrogenase A through the AMP-activated protein kinase/hypoxia-inducible factor-1α hypoxia pathway

Author

Alexander Ksendzovsky, Muznabanu Bachani, Marcelle Altshuler, Stuart Walbridge, Armin Mortazavi, Mitchell Moyer, Chixiang Chen, Islam Fayed, Joseph Steiner, Nancy Edwards, Sara K Inati, Jahandar Jahanipour, Dragan Maric, John D Heiss, Jaideep Kapur, and Kareem A Zaghloul

Subjects
Cellular and Molecular Neuroscience, Psychiatry and Mental health, Neurology, Original Article, Biological Psychiatry
Abstract

Recent studies suggest that changes in neuronal metabolism are associated with epilepsy. High rates of ATP depletion, lactate dehydrogenase A and lactate production have all been found in epilepsy patients, animal and tissue culture models. As such, it can be hypothesized that chronic seizures lead to continuing elevations in neuronal energy demand which may lead to an adapted metabolic response and elevations of lactate dehydrogenase A. In this study, we examine elevations in the lactate dehydrogenase A protein as a long-term cellular adaptation to elevated metabolic demand from chronic neuronal activation. We investigate this cellular adaptation in human tissue samples and explore the mechanisms of lactate dehydrogenase A upregulation using cultured neurones treated with low Mg2+, a manipulation that leads to NMDA-mediated neuronal activation. We demonstrate that human epileptic tissue preferentially upregulates neuronal lactate dehydrogenase A, and that in neuronal cultures chronic and repeated elevations in neural activity lead to upregulation of neuronal lactate dehydrogenase A. Similar to states of hypoxia, this metabolic change occurs through the AMP-activated protein kinase/hypoxia-inducible factor-1α pathway. Our data therefore reveal a novel long-term bioenergetic adaptation that occurs in chronically activated neurones and provide a basis for understanding the interplay between metabolism and neural activity during epilepsy.

Published
2022
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34. 379 Human Endogenous Retrovirus-K (HML-2) Contributes to a Unique Stem-Cell Niche in Glioblastoma

Author

Ashish Harish Shah, Sarah Rivas, Tara Doucet-Ohare, Vaidya Govindarajan, Catherine DeMarino, Leonel Ampie, Yeshavanath Banasavadi-Siddegowda, Dragan Maric, Rob Suter, Myoung-hwa Lee, Kareem A. Zaghloul, Stuart Walbridge, Marta Garcia-Montojo, Joe Steiner, Kory Johnson, Mark R. Gilbert, John D. Heiss, and Avindra Nath

Subjects
Surgery, Neurology (clinical)
Published
2023
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35. Assessing organ-level immunoreactivity in a rat model of sepsis using TSPO PET imaging

Author

Neysha, Martinez-Orengo, Sarine, Tahmazian, Jianhao, Lai, Zeping, Wang, Sanhita, Sinharay, William, Schreiber-Stainthorp, Falguni, Basuli, Dragan, Maric, William, Reid, Swati, Shah, and Dima A, Hammoud

Subjects
Lipopolysaccharides, Fluorine Radioisotopes, Positron Emission Tomography Computed Tomography, Positron-Emission Tomography, Sepsis, Immunology, Animals, Immunology and Allergy, Carrier Proteins, Receptors, GABA-A, Systemic Inflammatory Response Syndrome, Rats
Abstract

There is current need for new approaches to assess/measure organ-level immunoreactivity and ensuing dysfunction in systemic inflammatory response syndrome (SIRS) and sepsis, in order to protect or recover organ function. Using a rat model of systemic sterile inflammatory shock (intravenous LPS administration), we performed PET imaging with a translocator protein (TSPO) tracer, [18F]DPA-714, as a biomarker for reactive immunoreactive changes in the brain and peripheral organs. In vivo dynamic PET/CT scans showed increased [18F]DPA-714 binding in the brain, lungs, liver and bone marrow, 4 hours after LPS injection. Post-LPS mean standard uptake values (SUVmean) at equilibrium were significantly higher in those organs compared to baseline. Changes in spleen [18F]DPA-714 binding were variable but generally decreased after LPS. SUVmean values in all organs, except the spleen, positively correlated with several serum cytokines/chemokines. In vitro measures of TSPO expression and immunofluorescent staining validated the imaging results. Noninvasive molecular imaging with [18F]DPA-714 PET in a rat model of systemic sterile inflammatory shock, along with in vitro measures of TSPO expression, showed brain, liver and lung inflammation, spleen monocytic efflux/lymphocytic activation and suggested increased bone marrow hematopoiesis. TSPO PET imaging can potentially be used to quantify SIRS and sepsis-associated organ-level immunoreactivity and assess the effectiveness of therapeutic and preventative approaches for associated organ failures, in vivo.

Published
2022
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36. Widespread subclinical cellular changes revealed across a neural-epithelial-vascular complex in choroideremia using adaptive optics

Author

Nancy Aguilera, Tao Liu, Andrew J. Bower, Joanne Li, Sarah Abouassali, Rongwen Lu, John Giannini, Maximilian Pfau, Chelsea Bender, Margery G. Smelkinson, Amelia Naik, Bin Guan, Owen Schwartz, Andrei Volkov, Alfredo Dubra, Zhuolin Liu, Daniel X. Hammer, Dragan Maric, Robert Fariss, Robert B. Hufnagel, Brett G. Jeffrey, Brian P. Brooks, Wadih M. Zein, Laryssa A. Huryn, and Johnny Tam

Subjects
Male, Optics and Photonics, Choroid, Retinal Degeneration, Retinal Cone Photoreceptor Cells, Humans, Medicine (miscellaneous), Female, General Agricultural and Biological Sciences, Choroideremia, General Biochemistry, Genetics and Molecular Biology
Abstract

Choroideremia is an X-linked, blinding retinal degeneration with progressive loss of photoreceptors, retinal pigment epithelial (RPE) cells, and choriocapillaris. To study the extent to which these layers are disrupted in affected males and female carriers, we performed multimodal adaptive optics imaging to better visualize the in vivo pathogenesis of choroideremia in the living human eye. We demonstrate the presence of subclinical, widespread enlarged RPE cells present in all subjects imaged. In the fovea, the last area to be affected in choroideremia, we found greater disruption to the RPE than to either the photoreceptor or choriocapillaris layers. The unexpected finding of patches of photoreceptors that were fluorescently-labeled, but structurally and functionally normal, suggests that the RPE blood barrier function may be altered in choroideremia. Finally, we introduce a strategy for detecting enlarged cells using conventional ophthalmic imaging instrumentation. These findings establish that there is subclinical polymegathism of RPE cells in choroideremia.

Published
2022
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37. Targeting protein arginine methyltransferase 5 sensitizes glioblastoma to trametinib

Author

Yeshavanth Kumar Banasavadi-Siddegowda, Sriya Namagiri, Yoshihiro Otani, Hannah Sur, Sarah Rivas, Jean-Paul Bryant, Allison Shellbourn, Mitchell Rock, Ashis Chowdhury, Cole T Lewis, Toshihiko Shimizu, Stuart Walbridge, Sivarajan Kumarasamy, Ashish H Shah, Tae Jin Lee, Dragan Maric, Yuanqing Yan, Ji Young Yoo, Sangamesh G Kumbar, John D Heiss, and Balveen Kaur

Subjects
Basic and Translational Investigations, General Medicine
Abstract

Background The prognosis of glioblastoma (GBM) remains dismal because therapeutic approaches have limited effectiveness. A new targeted treatment using MEK inhibitors, including trametinib, has been proposed to improve GBM therapy. Trametinib had a promising preclinical effect against several cancers, but its adaptive treatment resistance precluded its clinical translation in GBM. Previously, we have demonstrated that protein arginine methyltransferase 5 (PRMT5) is upregulated in GBM and its inhibition promotes apoptosis and senescence in differentiated and stem-like tumor cells, respectively. We tested whether inhibition of PRMT5 can enhance the efficacy of trametinib against GBM. Methods Patient-derived primary GBM neurospheres (GBMNS) with transient PRMT5 knockdown were treated with trametinib and cell viability, proliferation, cell cycle progression, ELISA, and western blot were analyzed. In vivo, NSG mice were intracranially implanted with PRMT5-intact and -depleted GBMNS, treated with trametinib by daily oral gavage, and observed for tumor progression and mice survival rate. Results PRMT5 depletion enhanced trametinib-induced cytotoxicity in GBMNS. PRMT5 knockdown significantly decreased trametinib-induced AKT and ERBB3 escape pathways. However, ERBB3 inhibition alone failed to block trametinib-induced AKT activity suggesting that the enhanced antitumor effect imparted by PRMT5 knockdown in trametinib-treated GBMNS resulted from AKT inhibition and not ERBB3 inhibition. In orthotopic murine xenograft models, PRMT5-depletion extended the survival of tumor-bearing mice, and combination with trametinib further increased survival. Conclusion Combined PRMT5/MEK inhibition synergistically inhibited GBM in animal models and is a promising strategy for GBM therapy.

Published
2022

38. Anatomical Analysis of Transient Potential Vanilloid Receptor 1 (Trpv1+) and Mu-Opioid Receptor (Oprm1+) Co-expression in Rat Dorsal Root Ganglion Neurons

Author

Wenting Ma, Matthew R. Sapio, Allison P. Manalo, Dragan Maric, Mary Kate Dougherty, Taichi Goto, Andrew J. Mannes, and Michael J. Iadarola

Subjects
Cellular and Molecular Neuroscience, Molecular Biology
Abstract

Primary afferent neurons of the dorsal root ganglia (DRG) transduce peripheral nociceptive signals and transmit them to the spinal cord. These neurons also mediate analgesic control of the nociceptive inputs, particularly through the μ-opioid receptor (encoded by Oprm1). While opioid receptors are found throughout the neuraxis and in the spinal cord tissue itself, intrathecal administration of μ-opioid agonists also acts directly on nociceptive nerve terminals in the dorsal spinal cord resulting in marked analgesia. Additionally, selective chemoaxotomy of cells expressing the TRPV1 channel, a nonselective calcium-permeable ion channel that transduces thermal and inflammatory pain, yields profound pain relief in rats, canines, and humans. However, the relationship between Oprm1 and Trpv1 expressing DRG neurons has not been precisely determined. The present study examines rat DRG neurons using high resolution multiplex fluorescent in situ hybridization to visualize molecular co-expression. Neurons positive for Trpv1 exhibited varying levels of expression for Trpv1 and co-expression of other excitatory and inhibitory ion channels or receptors. A subpopulation of densely labeled Trpv1+ neurons did not co-express Oprm1. In contrast, a population of less densely labeled Trpv1+ neurons did co-express Oprm1. This finding suggests that the medium/low Trpv1 expressing neurons represent a specific set of DRG neurons subserving the opponent processes of both transducing and inhibiting nociceptive inputs. Additionally, the medium/low Trpv1 expressing neurons co-expressed other markers implicated in pathological pain states, such as Trpa1 and Trpm8, which are involved in chemical nociception and cold allodynia, respectively, as well as Scn11a, whose mutations are implicated in familial episodic pain. Conversely, none of the Trpv1+ neurons co-expressed Spp1, which codes for osteopontin, a marker for large diameter proprioceptive neurons, validating that nociception and proprioception are governed by separate neuronal populations. Our findings support the hypothesis that the population of Trpv1 and Oprm1 coexpressing neurons may explain the remarkable efficacy of opioid drugs administered at the level of the DRG-spinal synapse, and that this subpopulation of Trpv1+ neurons is responsible for registering tissue damage.

Published
2022
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39. Longitudinal Transcriptomic Profiling in Carrageenan-Induced Rat Hind Paw Peripheral Inflammation and Hyperalgesia Reveals Progressive Recruitment of Innate Immune System Components

Author

Andrew J. Mannes, Dragan Maric, Jeffrey Robinson, Matthew R. Sapio, Michael J. Iadarola, Taichi Goto, and Leorey N. Saligan

Subjects
Male, Chemokine, medicine.medical_treatment, Inflammation, Carrageenan, Article, Nociceptive Pain, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, 030202 anesthesiology, medicine, Animals, Secretome, Innate immune system, biology, Foot, Sequence Analysis, RNA, business.industry, Gene Expression Profiling, Immunity, Innate, Rats, Gene expression profiling, CXCL1, Disease Models, Animal, Anesthesiology and Pain Medicine, Cytokine, Neurology, Hyperalgesia, Immunology, biology.protein, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

Pain is a common but potentially debilitating symptom, often requiring complex management strategies. To understand the molecular dynamics of peripheral inflammation and nociceptive pain, we investigated longitudinal changes in behavior, tissue structure, and transcriptomic profiles in the rat carrageenan-induced peripheral inflammation model. Sequential changes in the number of differentially expressed genes are consistent with temporal recruitment of key leukocyte populations, mainly neutrophils and macrophages with each wave being preceded by upregulation of the cell-specific chemoattractants, Cxcl1 and Cxcl2, and Ccl2 and Ccl7, respectively. We defined 12 temporal gene clusters based on expression pattern. Within the patterns we extracted genes comprising the inflammatory secretome and others related to nociceptive tissue remodeling and to sensory perception of pain. Structural tissue changes, involving upregulation of multiple collagens occurred as soon as 1-hour postinjection, consistent with inflammatory tissue remodeling. Inflammatory expression profiling revealed a broad-spectrum, temporally orchestrated molecular and cellular recruitment process. The results provide numerous potential targets for modulation of pain and inflammation. PERSPECTIVE: This study investigates the highly orchestrated biological response during tissue inflammation with precise assessment of molecular dynamics at the transcriptional level. The results identify transcriptional changes that define an evolving inflammatory state in rats. This study provides foundational data for identifying markers of, and potential treatments for, inflammation and pain in patients.

Published
2021
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45. Inhibiting protein phosphatase 2A increases the antitumor effect of protein arginine methyltransferase 5 inhibition in models of glioblastoma

Author

John D. Heiss, Sriya Namagiri, Guruprasad Rachaiah, Toshihiko Shimizu, Yuanqing Yan, Hannah Sur, Prashant Chittiboina, Leomar Y. Ballester, Balveen Kaur, Amelie Vezina, Zhuang Zhengping, Cole T. Lewis, Ashis Chowdhury, Xiang Wang, Ji Young Yoo, Dragan Maric, Yoshihiro Otani, Sadhana Jackson, Yeshavanth Kumar Banasavadi-Siddegowda, Arunakumar Gangaplara, Sachin Kumar, and Abhik Ray-Chaudhury

Subjects
Protein-Arginine N-Methyltransferases, Cancer Research, Combination therapy, Arginine, medicine.diagnostic_test, Chemistry, Necroptosis, Protein arginine methyltransferase 5, Phosphatase, Editorials, Protein phosphatase 2, Xenograft Model Antitumor Assays, Piperazines, Mice, Oncology, Western blot, In vivo, Cell Line, Tumor, medicine, Cancer research, Animals, Humans, Protein Phosphatase 2, Neurology (clinical), Glioblastoma
Abstract

Background Despite multi-model therapy of maximal surgical resection, radiation, chemotherapy, and tumor-treating fields, the median survival of glioblastoma (GBM) patients is less than 15 months. Protein arginine methyltransferase 5 (PRMT5) catalyzes the symmetric dimethylation of arginine residues and is overexpressed in GBM. Inhibition of PRMT5 causes senescence in stem-like GBM tumor cells. LB100, a first-in-class small molecular inhibitor of protein phosphatase 2A (PP2A), can sensitize therapy-resistant tumor cells. Here, we tested the anti-GBM effect of concurrent PRMT5 and PP2A inhibition. Methods Patient-derived primary GBM neurospheres (GBMNS), transfected with PRMT5 target-specific siRNA, were treated with LB100 and subjected to in vitro assays including PP2A activity and western blot. The intracranial mouse xenograft model was used to test the in vivo antitumor efficacy of combination treatment. Results We found that PRMT5 depletion increased PP2A activity in GBMNS. LB100 treatment significantly reduced the viability of PRMT5-depleted GBMNS compared to PRMT5-intact GBMNS. LB100 enhanced G1 cell cycle arrest induced by PRMT5 depletion. Combination therapy also increased the expression of phospho-MLKL. Necrostatin-1 rescued PRMT5-depleted cells from the cytotoxic effects of LB100, indicating that necroptosis caused the enhanced cytotoxicity of combination therapy. In the in vivo mouse tumor xenograft model, LB100 treatment combined with transient depletion of PRMT5 significantly decreased tumor size and prolonged survival, while LB100 treatment alone had no survival benefit. Conclusion Overall, combined PRMT5 and PP2A inhibition had significantly greater antitumor effects than PRMT5 inhibition alone.

Published
2021
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46. EXTH-76. PRMT5 INHIBITION SENSITIZES GLIOBLASTOMA NEUROSPHERES TO TEMOZOLOMIDE

Author

Sarah Rivas, Kimberly Rivera-Caraballo, Sara Murphy, Yoshihiro Otani, Allison Shelbourn, Leo Ampie, Dragan Maric, Stuart Walbridge, Ashish Shah, Yuanqing Yan, Ji young Yoo, John Heiss, Balveen Kaur, and Yeshavanath Banasavadi-Siddegowda

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

INTRODUCTION The median survival of Glioblastoma (GBM) patients is less than two years with the standard of care of maximal surgical resection, radiation, and temozolomide (TMZ) chemotherapy. Protein Arginine Methyltransferase 5 (PRMT5), which regulates cellular functions by symmetrically di-methylating arginine residues, is overexpressed in GBM. Inhibiting PRMT5 induces apoptosis in differentiated and senescence in stem-like GBM tumor cells. We inhibited PRMT5 in GBM neurospheres to determine if PRMT5 inhibition would enhance TMZ’s antitumor effect. METHODS We depleted PRMT5 activity, in vitro, using target-specific siRNA or LLY-283 and combined these with TMZ treatment. We evaluated the antitumor effect of this combination using cell viability assay, cell cycle analysis, apoptosis assay, and western blot. RESULTS TMZ reduced the viability of GBMNS with PRMT5 knockdown significantly more than the viability of PRMT5 intact GBMNS. The combination of TMZ and PRMT5 knockdown elevated the expression of cleaved caspase 3 and caspase3/7 indicating that PRMT5 knockdown enhanced the apoptotic effects of TMZ. Cell cycle analysis showed that depleting PRMT5 abrogated TMZ-induced G2/M cell cycle arrest. Further, treatment of PRMT5-depleted GBMNS with TMZ increased ɣ-H2AX expression compared PRMT5 intact GBMNS treated with TMZ, suggesting that PRMT5 depletion enhanced TMZ-induced DNA damage. PRMT5 knockdown also inhibited the symmetric di-methylation of RUVBL1 that is required for homologous recombination repair of TMZ treatment-related DNA damage. CONCLUSION Overall, PRMT5 inhibition sensitized GBMNS to TMZ and enhanced TMZ-related DNA damage and cytotoxicity. These findings support further development of this potential therapeutic combination.

Published
2022
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47. Early detection of cerebrovascular pathology and protective antiviral immunity by MRI

Author

Li Liu, Steve Dodd, Ryan D Hunt, Nikorn Pothayee, Tatjana Atanasijevic, Nadia Bouraoud, Dragan Maric, E Ashley Moseman, Selamawit Gossa, Dorian B McGavern, and Alan P Koretsky

Subjects
Mice, Inbred C57BL, Mice, General Immunology and Microbiology, General Neuroscience, Animals, Brain, Endothelial Cells, Humans, General Medicine, Antiviral Agents, Magnetic Resonance Imaging, General Biochemistry, Genetics and Molecular Biology, Cerebral Hemorrhage
Abstract

Central nervous system (CNS) infections are a major cause of human morbidity and mortality worldwide. Even patients that survive, CNS infections can have lasting neurological dysfunction resulting from immune and pathogen induced pathology. Developing approaches to noninvasively track pathology and immunity in the infected CNS is crucial for patient management and development of new therapeutics. Here, we develop novel MRI-based approaches to monitor virus-specific CD8+ T cells and their relationship to cerebrovascular pathology in the living brain. We studied a relevant murine model in which a neurotropic virus (vesicular stomatitis virus) was introduced intranasally and then entered the brain via olfactory sensory neurons – a route exploited by many pathogens in humans. Using T2*-weighted high-resolution MRI, we identified small cerebral microbleeds as an early form of pathology associated with viral entry into the brain. Mechanistically, these microbleeds occurred in the absence of peripheral immune cells and were associated with infection of vascular endothelial cells. We monitored the adaptive response to this infection by developing methods to iron label and track individual virus specific CD8+ T cells by MRI. Transferred antiviral T cells were detected in the brain within a day of infection and were able to reduce cerebral microbleeds. These data demonstrate the utility of MRI in detecting the earliest pathological events in the virally infected CNS as well as the therapeutic potential of antiviral T cells in mitigating this pathology.

Published
2022
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48. Anatomical Analysis of Transient Potential Vanilloid Receptor 1 (

Author

Wenting, Ma, Matthew R, Sapio, Allison P, Manalo, Dragan, Maric, Mary Kate, Dougherty, Taichi, Goto, Andrew J, Mannes, and Michael J, Iadarola

Abstract

Primary afferent neurons of the dorsal root ganglia (DRG) transduce peripheral nociceptive signals and transmit them to the spinal cord. These neurons also mediate analgesic control of the nociceptive inputs, particularly through the μ-opioid receptor (encoded by

Published
2022

50. PET imaging of TSPO expression in immune cells can assess organ-level pathophysiology in high-consequence viral infections

Author

Swati Shah, Sanhita Sinharay, Reema Patel, Jeffrey Solomon, Ji Hyun Lee, William Schreiber-Stainthorp, Falguni Basuli, Xiang Zhang, Katie R. Hagen, Rebecca Reeder, Paul Wakim, Louis M. Huzella, Dragan Maric, Reed F. Johnson, and Dima A. Hammoud

Subjects
Disease Models, Animal, Multidisciplinary, Pyrimidines, Receptors, GABA, Positron-Emission Tomography, Animals, Pyrazoles, Hemorrhagic Fever, Ebola, Lung, Macaca mulatta, Biomarkers, Spleen
Abstract

Ebola virus (EBOV) disease is characterized by lymphopenia, breach in vascular integrity, cytokine storm, and multiorgan failure. The pathophysiology of organ involvement, however, is incompletely understood. Using [18F]-DPA-714 positron emission tomography (PET) imaging targeting the translocator protein (TSPO), an immune cell marker, we sought to characterize the progression of EBOV-associated organ-level pathophysiology in the EBOV Rhesus macaque model. Dynamic [18F]-DPA-714 PET/computed tomography imaging was performed longitudinally at baseline and at multiple time points after EBOV inoculation, and distribution volumes (Vt) were calculated as a measure of peripheral TSPO binding. Using a mixed-effect linear regression model, spleen and lung Vt decreased, while the bone marrow Vt increased over time after infection. No clear trend was found for liver Vt. Multiple plasma cytokines correlated negatively with lung/spleen Vt and positively with bone marrow Vt. Multiplex immunofluorescence staining in spleen and lung sections confirmed organ-level lymphoid and monocytic loss/apoptosis, thus validating the imaging results. Our findings are consistent with EBOV-induced progressive monocytic and lymphocytic depletion in the spleen, rather than immune activation, as well as depletion of alveolar macrophages in the lungs, with inefficient reactive neutrophilic activation. Increased bone marrow Vt, on the other hand, suggests hematopoietic activation in response to systemic immune cell depletion and leukocytosis and could have prognostic relevance. In vivo PET imaging provided better understanding of organ-level pathophysiology during EBOV infection. A similar approach can be used to delineate the pathophysiology of other systemic infections and to evaluate the effectiveness of newly developed treatment and vaccine strategies.

Published
2022

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