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1. Molecular Regulation of Bone Turnover in Juvenile Idiopathic Arthritis: Animal Models, Cellular Features and TNFα

Author

Harry C Blair, Jonathan Soboloff, Irina L Tourkova, Jamie L. McCall, Suravi Ray, Margalit E Rosenkranz, Cristina Sobacchi, Lisa J Robinson, and John B Barnett

Subjects
rheumatoid arthritis, juvenile idiopathic arthritis, macrophage, osteoclast, tnfα, interleukin 1, interleukin 6, Biochemistry, QD415-436, Biology (General), QH301-705.5
Abstract

We review the abnormal bone turnover that is the basis of idiopathic inflammatory or rheumatoid arthritis and bone loss, with emphasis on Tumor Necrosis Factor-alpha (TNFα)-related mechanisms. We review selected data on idiopathic arthritis in juvenile human disease, and discuss mouse models focusing on induction of bone resorbing cells by TNFα and Receptor Activator of Nuclear Factor kappa B Ligand (RANKL). In both humans and animal models, macrophage-derived cells in the joint, particularly in the synovium and periosteum, degrade bone and cartilage. Mouse models of rheumatoid arthritis share with human disease bone resorbing cells and strong relation to TNFα expression. In humans, differences in therapy and prognosis of arthritis vary with age, and results from early intervention for inflammatory cytokines in juvenile patients are particularly interesting. Mechanisms that contribute to inflammatory arthritis reflect, in large part, inflammatory cytokines that play minor roles in normal bone turnover. Changes in inflammatory cytokines, particularly TNFα, are many times larger, and presented in different locations, than cytokines that regulate normal bone turnover. Recent data from in vitro and mouse models include novel mechanisms described in differentiation of bone resorbing cells in inflammatory arthritis dependent on the Transient Receptor Potential Channel (TRPC) family of calcium channels. Low-molecular weight (MW) inhibitors of TRPC channels add to their potential importance. Associations with inflammatory arthritis unrelated to TNFα are briefly summarized as pointing to alternative mechanisms. We suggest that early detection and monoclonal antibodies targeting cytokines mediating disease progression deserves emphasis.

Published
2024
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2. Relentless placoid chorioretinitis: A review of four cases in pediatric and young adult patients with a discussion of therapeutic strategies

Author

Haniah A. Zaheer, Jamie Odden, Meghal Gagrani, Fatma Zaguia, Careen Lowder, Andreea Coca, Margalit E. Rosenkranz, Preeti Patil-Chhablani, Raphaelle Ores, Francois Boussion, Chad Indermill, José-Alain Sahel, Ken Nischal, Debra A. Goldstein, and Marie-Helene Errera

Subjects
relentless placoid chorioretinitis, uveitis, adalimumab, infliximab, interferon-alpha-2a, tocilizumab, Pediatrics, RJ1-570
Abstract

IntroductionRelentless placoid chorioretinitis (RPC) is a rare, bilateral disease of the retinal pigment epithelium. The clinical course is prolonged and relapsing. No standard treatment has been established to date. The purpose of this case series is to report four cases of RPC in pediatric and young adult patients in which varying treatments were used, comparing them to previously published cases.MethodsA literature review was conducted to investigate currently published presentations and treatment options for RPC. A multicenter retrospective chart review was also performed on four consecutive patients. These patients were diagnosed with RPC because of new chorioretinitis lesions continuing to appear without or despite therapy for 5–36 months (2 patients), with a clinical course prolonged and relapsing, or because of the atypical location of the multiple lesions (>50) extending from the posterior pole to the equator and mid-peripheral retina (all four patients), which were not consistent with other entities like acute posterior multifocal placoid pigment epitheliopathy and serpiginous choroiditis.ResultsAll four cases of RPC received oral or IV steroids acutely, and three of these patients were transitioned to a steroid-sparing agent and biologic therapy: anti-TNF alpha or anti-IL-6. Quiescence of the chorioretinitis lesions was obtained after 7 months, 1 month, and 36 months; however, the latter had issues with treatment adherence. Mycophenolate mofetil was insufficient to control the disease in one patient, but tocilizumab and infliximab thereafter were effective after cessation of adalimumab due to side effects. Adalimumab when started the first month after the presentation was effective in controlling the disease in one patient. After the failure of interferon-alpha-2a, one patient displayed long-term control with infliximab. One patient did not require a steroid-sparing agent after oral prednisone taper as there was no evidence of progression or recurrence.ConclusionThis case series adds to the current knowledge regarding potential treatments for RPC, specifically the use of anti-TNF-alpha treatment and anti-IL-6 tocilizumab. In this case study, relapses of RPC were found among patients on mycophenolate mofetil and interferon-alpha-2a, and one case did not relapse on oral steroids without a steroid-sparing agent. Our findings suggest that adalimumab, infliximab, and tocilizumab may be useful medications to obtain quiescence of RPC.

Published
2023
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3. T Cell Receptor-Independent, CD31/IL-17A-Driven Inflammatory Axis Shapes Synovitis in Juvenile Idiopathic Arthritis

Author

Ian D. Ferguson, Patricia Griffin, Joshua J. Michel, Hiroshi Yano, Sarah L. Gaffen, Robert G. Mueller, Jeffrey A. Dvergsten, Jon D. Piganelli, Margalit E. Rosenkranz, Daniel A. Kietz, and Abbe N. Vallejo

Subjects
CD31, double negative alpha beta T cells, fibrocyte-like cells, IL-17, juvenile idiopathic arthritis, oxidoreductase, Immunologic diseases. Allergy, RC581-607
Abstract

T cells are considered autoimmune effectors in juvenile idiopathic arthritis (JIA), but the antigenic cause of arthritis remains elusive. Since T cells comprise a significant proportion of joint-infiltrating cells, we examined whether the environment in the joint could be shaped through the inflammatory activation by T cells that is independent of conventional TCR signaling. We focused on the analysis of synovial fluid (SF) collected from children with oligoarticular and rheumatoid factor-negative polyarticular JIA. Cytokine profiling of SF showed dominance of five molecules including IL-17A. Cytometric analysis of the same SF samples showed enrichment of αβT cells that lacked both CD4 and CD8 co-receptors [herein called double negative (DN) T cells] and also lacked the CD28 costimulatory receptor. However, these synovial αβT cells expressed high levels of CD31, an adhesion molecule that is normally employed by granulocytes when they transit to sites of injury. In receptor crosslinking assays, ligation of CD31 alone on synovial CD28nullCD31+ DN αβT cells effectively and sufficiently induced phosphorylation of signaling substrates and increased intracytoplasmic stores of cytokines including IL-17A. CD31 ligation was also sufficient to induce RORγT expression and trans-activation of the IL-17A promoter. In addition to T cells, SF contained fibrocyte-like cells (FLC) expressing IL-17 receptor A (IL-17RA) and CD38, a known ligand for CD31. Stimulation of FLC with IL-17A led to CD38 upregulation, and to production of cytokines and tissue-destructive molecules. Addition of an oxidoreductase analog to the bioassays suppressed the CD31-driven IL-17A production by T cells. It also suppressed the downstream IL-17A-mediated production of effectors by FLC. The levels of suppression of FLC effector activities by the oxidoreductase analog were comparable to those seen with corticosteroid and/or biologic inhibitors to IL-6 and TNFα. Collectively, our data suggest that activation of a CD31-driven, αβTCR-independent, IL-17A-mediated T cell-FLC inflammatory circuit drives and/or perpetuates synovitis. With the notable finding that the oxidoreductase mimic suppresses the effector activities of synovial CD31+CD28null αβT cells and IL-17RA+CD38+ FLC, this small molecule could be used to probe further the intricacies of this inflammatory circuit. Such bioactivities of this small molecule also provide rationale for new translational avenue(s) to potentially modulate JIA synovitis.

Published
2018
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6. Relentless placoid chorioretinitis: A review of four cases in pediatric and young adult patients with a discussion of therapeutic strategies

Author

Zaheer, Haniah A., primary, Odden, Jamie, additional, Gagrani, Meghal, additional, Zaguia, Fatma, additional, Lowder, Careen, additional, Coca, Andreea, additional, Rosenkranz, Margalit E., additional, Patil-Chhablani, Preeti, additional, Ores, Raphaelle, additional, Boussion, Francois, additional, Indermill, Chad, additional, Sahel, José-Alain, additional, Nischal, Ken, additional, Goldstein, Debra A., additional, and Errera, Marie-Helene, additional

Published
2023
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8. Experiences of Adults at 50% Risk of Inheriting a Genetic Mutation for Early-Onset Dementia

Author

Rosenblatt, Margalit E., Rosenblatt, Margalit E., Rosenblatt, Margalit E., and Rosenblatt, Margalit E.

Subjects
Genetics
Abstract

Background: An extensive body of scientific research on biomarkers associated with early-onset Alzheimer disease (EOAD) and familial frontotemporal dementia (FTD) has emerged from the Dominantly Inherited Alzheimer’s Network (DIAN) and Longitudinal Evaluation of Familial Frontotemporal Dementia Subjects (LEFFTDS) studies. Yet, little of that research has focused on the participants’ lived experiences. Therefore, it is not well understood how to best support these individuals as they face futures that may resemble their parents’ pasts. Methods: Semi-structured interviews with 6 informants (1 male, 5 females, age 30s-60s). Half of the participants chose not to know their genetic status, two knew they carried a pathogenic mutation associated with FTD, and one knew she did not have the pathogenic variant for EOAD that runs in her family. Results: Analysis of the interviews yielded four overarching themes: family disease, influence on family relationships, personal reactions, and research participation. Conclusion: The participants were aware from an early age of a debilitating medical condition occurring in multiple close relatives, even if they did not know or understand what the condition was. This fact, influenced by varying family dynamics, encouraged participants to take control of their situation by seeking out information and planning for the future, which in turn motivated them to partake in longitudinal, observational research.

Published
2019

9. Preserving a family’s photographic history: the private collection of Michina Pope

Author

Margalit E. Slovin

Abstract

Photographs can provide a pictorial testimony of a familial history; yet, each time objects are moved and handled the risk of loss and deterioration increases. However, to date, little guidance has been available to private collectors on how to organize and preserve their photographic collections. My practical thesis focuses on the unique challenges of organizing, preserving and digitizing a private collection of approximately 250 glass plate negatives and four corresponding albums, belonging to Michina Pope in Toronto, Canada. Using this specific collection, I have summarized my research with the intention of creating an illustrated manual with clear guidelines as a resource to help guide private collectors in caring for their photographic collection. In lieu of a specifically purposed manual, this thesis paper an act, in the time being, as a guide for collectors and/or those working with private collections of photographic materials.

Published
2021
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22. T Cell Receptor-Independent, CD31/IL-17A-Driven Inflammatory Axis Shapes Synovitis in Juvenile Idiopathic Arthritis

Author

Ferguson, Ian D., primary, Griffin, Patricia, additional, Michel, Joshua J., additional, Yano, Hiroshi, additional, Gaffen, Sarah L., additional, Mueller, Robert G., additional, Dvergsten, Jeffrey A., additional, Piganelli, Jon D., additional, Rosenkranz, Margalit E., additional, Kietz, Daniel A., additional, and Vallejo, Abbe N., additional

Published
2018
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24. Systemic and Localized Scleroderma in Children

Author

Petros Efthimiou, Thomas J. A. Lehman, Margalit E Rosenkranz, and Lucila M. A. Agle

Subjects
medicine.medical_specialty, Pathology, Scleroderma, Systemic, integumentary system, business.industry, Interstitial lung disease, Disease, medicine.disease, Systemic scleroderma, Dermatology, Scleroderma, Scleroderma, Localized, Fibrosis, Localized disease, Pediatrics, Perinatology and Child Health, medicine, Vitamin D and neurology, Humans, Pharmacology (medical), Child, business, Localized Scleroderma, Skin
Abstract

Scleroderma is a group of rare and complex diseases with varied clinical manifestations. The most obvious manifestation of the diseases is skin hardening and sclerosis. Scleroderma can be divided into two main subgroups: systemic and localized. The systemic form, also known as systemic sclerosis, involves diffuse skin involvement and potentially severe visceral involvement. Localized scleroderma on the other hand is more common in children and usually confined to a specific region of the body with no internal organ involvement. The juvenile forms of systemic sclerosis and localized scleroderma are important conditions in children because of the clinical severity and substantial mortality of systemic scleroderma and the major growth defects associated with childhood-onset localized disease even if the active disease itself is self-limited. The pathogenic pathways of the various forms of scleroderma are only partially defined, but the main defect in scleroderma is abnormal collagen deposition leading to eventual fibrosis in the skin as well as multiple organ systems such as the heart and lungs in juvenile systemic sclerosis. Therapeutics are divided into three main subgroups for systemic sclerosis: antifibrotics, anti-inflammatories, and vasodilators. For localized disease, anti-inflammatories, vitamin D analogs, and UV irradiation have been investigated. However, the infrequency of scleroderma in the pediatric population plus the fact that this disease is very often self-limiting makes randomized controlled trials very difficult. It is for this reason that most data on treatment modalities for this disease have been extrapolated from studies in adult patients. There is no one therapy for systemic sclerosis or localized scleroderma that has proven to be very effective or significantly disease modifying. However, current therapeutic strategies must be initiated early in the disease course for maximum beneficial clinical effects. New interventions such as autologous stem cell transplant and cytokine-directed therapies are under investigation as potential treatments for this complex disease.

Published
2006
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25. Premature cell senescence and T cell receptor-independent activation of CD8T cells in Juvenile Idiopathic Arthritis*

Author

Dvergsten, Jeffrey A., Mueller, Robert G., Griffin, Patricia, Abedin, Sameem, Pishko, Allyson, Michel, Joshua J., Rosenkranz, Margalit E., Reed, Ann M., Kietz, Daniel A., and Vallejo, Abbe N.

Subjects
CD4-Positive T-Lymphocytes, Male, Time Factors, Adolescent, Receptors, Antigen, T-Cell, CD8-Positive T-Lymphocytes, Telomere, Fetal Blood, Lymphocyte Activation, Article, Arthritis, Juvenile, Histones, Platelet Endothelial Cell Adhesion Molecule-1, CD28 Antigens, T-Lymphocyte Subsets, Synovial Fluid, Humans, Female, Child, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor p16, Cell Proliferation
Abstract

CD8+ T cells lacking CD28 were originally reported to be a characteristic feature of juvenile idiopathic arthritis (JIA), but the relevance of these unusual cells to this disease remains to be elucidated. Because of recent evidence that loss of CD28 cells is typical of terminally differentiated lymphocytes, the aim of this study was to examine functional subsets of CD8+ T cells in patients with JIA.Blood and/or waste synovial fluid samples were collected from children with a definite diagnosis of JIA (n = 98). Deidentified peripheral blood (n = 33) and cord blood (n = 13) samples from healthy donors were also collected. CD8+ and CD4+ T cells were screened for novel receptors, and where indicated, bioassays were performed to determine the functional relevance of the identified receptor.JIA patients had a naive T cell compartment with shortened telomeres, and their entire T cell pool had reduced proliferative capacity. They had an overabundance of CD31+CD28(null) CD8+ T cells, which was a significant feature of oligoarticular JIA (n = 62) as compared to polyarticular JIA (n = 36). CD31+ CD28(null) CD8+ T cells had limited mitotic capacity and expressed high levels of the senescence antigens histone γH2AX and/or p16. Ligation of CD31, which was independent of the T cell receptor (TCR), sufficiently induced tyrosine phosphorylation, vesicle exocytosis, and production of interferon-γ and interleukin-10.These data provide the first evidence of cell senescence, as represented by CD31+CD28(null) CD8+ T cells, in the pathophysiology of JIA. Activation of these unusual cells in a TCR-independent manner suggests that they are maladaptive and could be potential targets for immunotherapy.

Published
2013

26. TLR2 and MyD88 contribute to Lactobacillus casei extract-induced focal coronary arteritis in a mouse model of Kawasaki disease

Author

Wenxuan Zhang, Michael C. Fishbein, Danica J. Schulte, Michelle H. Wong, Moshe Arditi, Margalit E. Rosenkranz, Lionel B. Ivashkiv, Thomas J. A. Lehman, Lucila M. A. Agle, Kathrin S. Michelsen, and Terence M. Doherty

Subjects
Cell Extracts, Pathology, medicine.medical_specialty, Inflammation, Coronary Disease, Mucocutaneous Lymph Node Syndrome, Pathogenesis, Mice, Cell Wall, Physiology (medical), medicine, Animals, Humans, Arteritis, Receptor, Child, Adaptor Proteins, Signal Transducing, business.industry, medicine.disease, Toll-Like Receptor 2, Coronary arteries, Disease Models, Animal, Lacticaseibacillus casei, medicine.anatomical_structure, Myeloid Differentiation Factor 88, TLR4, medicine.symptom, Cardiology and Cardiovascular Medicine, Vasculitis, business
Abstract

Background— Kawasaki disease is the most common cause of acquired cardiac disease and acute vasculitis in children, targets the coronary arteries, and can occasionally be fatal. The pathogenesis and the molecular mechanisms remain unknown. After injection of Lactobacillus casei cell-wall extract (LCCWE), mice develop a focal coronary arteritis that histopathologically resembles Kawasaki disease, but the mechanism remains unclear. Here, we tested the hypothesis that signaling by Toll-like receptors (TLRs) through their key downstream adaptor molecule myeloid differentiation factor 88 (MyD88) is required for the cellular activation and coronary arteritis produced by LCCWE. Methods and Results— Bone marrow–derived macrophages from TLR2- or MyD88-deficient mice were unresponsive to LCCWE-induced stimulation. In contrast, macrophages obtained from TLR4-deficient mice produced the same amount of interleukin-6 as macrophages from wild-type mice after stimulation with LCCWE. Intraperitoneal injection of LCCWE produced severe focal coronary arteritis in TLR4 −/− and C57BL/6 control mice but not in TLR2 −/− or MyD88 −/− mice. Collectively, these results indicate that LCCWE is a potent inducer of nuclear factor-κB via TLR2 but not TLR4 and that this activation proceeds via the MyD88-dependent signaling pathway. In vivo studies suggest that TLR2 −/− mice are protected from LCCWE-induced coronary arteritis and that this protection is mediated through the adaptor molecule MyD88. Conclusions— Our results provide important insights into the molecular signaling in this mouse model of coronary arteritis. We show here that LCCWE-induced coronary arteritis is dependent on intact TLR2 and MyD88 signaling.

Published
2005

27. Novel therapies for the treatment of juvenile rheumatoid arthritis (juvenile idiopathic arthritis)

Author

Thomas J. A. Lehman, Margalit E Rosenkranz, and Lucila M. A. Agle

Subjects
Anti-Inflammatory Agents, Arthritis, Inflammation, Aggressive disease, medicine, Juvenile, Animals, Humans, Technology, Pharmaceutical, Pharmacology (medical), Pharmacology, business.industry, Tumor Necrosis Factor-alpha, Anti-Inflammatory Agents, Non-Steroidal, General Medicine, medicine.disease, Systemic-onset juvenile idiopathic arthritis, Arthritis, Juvenile, Thalidomide, Antirheumatic Agents, Immunology, medicine.symptom, Antirheumatic drugs, business, Juvenile rheumatoid arthritis, medicine.drug
Abstract

The majority of children with juvenile idiopathic arthritis respond well to conventional treatment. However, some children will have a more aggressive disease course and will be resistant to standard management. Over the past 20 years, growth in our understanding of the immunopathogenesis of juvenile idiopathic arthritis and related diseases has facilitated significant therapeutic advances. In this report, recently released antirheumatic drugs, as well as some treatments currently in development, will be discussed. Biological agents, such as antiTNF and other cytokines inhibitors, and unique drugs, such as thalidomide, provide new opportunities to suppress the inflammation found in severe cases of systemic onset juvenile idiopathic arthritis and can obtain a satisfactory outcome.

Published
2003

28. Clinical trials for pediatric scleroderma

Author

Margalit E Rosenkranz and Thomas J. A. Lehman

Subjects
musculoskeletal diseases, medicine.medical_specialty, MEDLINE, Scleroderma, stomatognathic system, Rheumatology, Internal medicine, medicine, Humans, Intensive care medicine, Child, Cyclophosphamide, Clinical Trials as Topic, Scleroderma, Systemic, business.industry, Penicillamine, Progressive systemic sclerosis, medicine.disease, eye diseases, Thalidomide, Clinical trial, stomatognathic diseases, Methotrexate, Antirheumatic Agents, Physical therapy, business, Rare disease, Pediatric population, medicine.drug
Abstract

Progressive systemic sclerosis (PSS), or scleroderma, is a rare disease in the pediatric population. Many children with PSS have significant involvement of their internal organs, which leads to decreased survival. Because of the infrequency of the condition and delayed diagnosis, there are no large studies to evaluate therapy for PSS in children. Treatment is controversial in the adult literature, and its applicability to children is unclear. Only through collaborative efforts will researchers be able to clearly delineate the etiopathogenesis of PSS, and gather information from multicenter studies to ultimately provide appropriate and effective care for children with PSS.

Published
2002

30. Erratum: Synovial fluid proteins differentiate between the subtypes of juvenile idiopathic arthritis

Author

Rosenkranz, Margalit E., primary, Wilson, David C., additional, Marinov, Anthony D., additional, Decewicz, Alisha, additional, Grof-Tisza, Patrick, additional, Kirchner, David, additional, Giles, Brendan, additional, Reynolds, Paul R., additional, Liebman, Michael N., additional, Kolli, V. S. Kumar, additional, Thompson, Susan D., additional, and Hirsch, Raphael, additional

Published
2011
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32. Neural interactions in the frontal cortex of a behaving monkey: signs of dependence on stimulus context and behavioral state

Author

Aertsen A, Vaadia E, Abeles M, Ahissar E, Bergman H, Karmon B, Lavner Y, Margalit E, Israel Nelken, and Rotter S

Subjects
Cerebral Cortex, Neurons, nervous system, Behavior, Animal, Animals, Macaca mulatta, Frontal Lobe
Abstract

In order to gain an understanding of the processes taking place within and between neuronal assemblies, we made simultaneous recordings of spike trains from groups of up to 11 neurons in the frontal cortex of a rhesus monkey, that was trained to perform a sensorimotor behavioral task. We report here on preliminary results from correlation analysis of these neuronal activities, with special emphasis on signs of behaviorally induced modifications of neural interaction, possibly due to rapid modulations of discharge synchronization among the neurons. Our findings suggest that different functional groups of neurons may co-exist within each small volume of cortex, and that neurons may be dynamically recruited into such a group to fulfil a specific function.

Published
1991

34. TLR2 and MyD88 Contribute to Lactobacillus casei Extract–Induced Focal Coronary Arteritis in a Mouse Model of Kawasaki Disease

Author

Rosenkranz, Margalit E., primary, Schulte, Danica J., additional, Agle, Lucila M.A., additional, Wong, Michelle H., additional, Zhang, Wenxuan, additional, Ivashkiv, Lionel, additional, Doherty, Terence M., additional, Fishbein, Michael C., additional, Lehman, Thomas J.A., additional, Michelsen, Kathrin S., additional, and Arditi, Moshe, additional

Published
2005
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35. Visual and electrical evoked response recorded from subdural electrodes implanted above the visual cortex in normal dogs under two methods of anesthesia

Author

Margalit, E, primary, Weiland, J.D, additional, Clatterbuck, R.E, additional, Fujii, G.Y, additional, Maia, M, additional, Tameesh, M, additional, Torres, G, additional, D'Anna, S.A, additional, Desai, S, additional, Piyathaisere, D.V, additional, Olivi, A, additional, de Juan, E, additional, and Humayun, Mark S, additional

Published
2003
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36. RIG-1-Like Receptor Activation Synergizes With Intratumoral Alpha Radiation to Induce Pancreatic Tumor Rejection, Triple-Negative Breast Metastases Clearance, and Antitumor Immune Memory in Mice

Author

Vered Domankevich, Margalit Efrati, Michael Schmidt, Eran Glikson, Fairuz Mansour, Amit Shai, Adi Cohen, Yael Zilberstein, Elad Flaisher, Razvan Galalae, Itzhak Kelson, and Yona Keisari

Subjects
PolyIC, polyethylenimine, decitabine, radiotherapy, immunotherapy, alpha radiation, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Diffusing alpha-emitting radiation therapy (DaRT) employs intratumoral Ra-224-coated seeds that efficiently destroy solid tumors by slowly releasing alpha-emitting atoms inside the tumor. In immunogenic tumor models, DaRT was shown to activate systemic antitumor immunity. Agonists of the membrane-bound toll-like receptors (TLRs) enhanced these effects and led to tumor rejection. Here, we examined the combination of DaRT with agents that activate a different type of pattern recognition receptors, the cytoplasmatic RIG1-like receptors (RLRs). In response to cytoplasmatic viral dsRNA, RLRs activate an antiviral immune response that includes the elevation of antigen presentation. Thus, it was postulated that in low-immunogenic tumor models, RLR activation in tumor cells prior to the induction of their death by DaRT will be superior compared to TLR activation. Intratumoral cytoplasmatic delivery of the dsRNA mimic polyIC by polyethylenimine (PEI), was used to activate RLR, while polyIC without PEI was used to activate TLR. PolyIC(PEI) prior to DaRT synergistically retarded 4T1 triple-negative breast tumors and metastasis development more efficiently than polyIC and rejected panc02 pancreatic tumors in some of the treated mice. Splenocytes from treated mice, adoptively transferred to naive mice in combination with 4T1 tumor cells, delayed tumor development compared to naïve splenocytes. Low-dose cyclophosphamide, known to reduce T regulatory cell number, enhanced the effect of DaRT and polyIC(PEI) and led to high long-term survival rates under neoadjuvant settings, which confirmed metastasis clearance. The epigenetic drug decitabine, known to activate RLR in low doses, was given intraperitoneally prior to DaRT and caused tumor growth retardation, similar to local polyIC(PEI). The systemic and/or local administration of RLR activators was also tested in the squamous cell carcinoma (SCC) tumor model SQ2, in which a delay in tumor re-challenge development was demonstrated. We conclude that RIG-I-like activation prior to intratumoral alpha radiation may serve as a potent combination technique to reduce both tumor growth and the spread of distant metastases in low-immunogenic and metastatic tumor models.

Published
2020
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40. Quantification of Two Fluorophores’ Concentration Ratio in a Mice Model in Preparation for a Proposed Method for Early Detection of Alzheimer’s Disease

Author

Osnat Harbater, Margalit Efrati, and Israel Gannot

Subjects
fluorescence, disease markers, Alzheimer’s early diagnostics, CSF biomarkers, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999
Abstract

Many biomedical applications require concentration measurements of biological compounds, which may be achieved using targeted fluorescent probes. It has been shown that the ratio between amyloid-Beta and tau protein in the cerebrospinal fluid (CSF) is a good indicator of incipient Alzheimer’s disease (AD). We have previously proposed a method that can accurately estimate the concentration ratio of these two proteins without the need to collect CSF samples: Fluorescent probes are injected to the blood and bind to the CSF biomarkers. A miniature needle with an optical fiber excites the fluorescent probes and collects the fluorescence emission. The concentration ratio between the proteins is estimated, and used for diagnosis of incipient AD. We present here the results of the method’s concentration ratio estimation during trials performed on mice. Miniature tubes containing two fluorescent probes in several concentration ratios were implanted in two locations in the mice: subcutaneously, and deeper in the abdomen. The fluorescent probes were excited and the fluorescence intensity was measured. The concentration ratios were estimated from the fluorescence intensities with an average error of less than 20%. This study is a step towards the demonstration of the method in in vivo studies in mice with markers in the bloodstream/CSF.

Published
2018
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42. Retinal prosthesis

Author

Eong, K. -G A., Margalit, E., James Weiland, Juan, E., and Humayun, M. S.

43. Human apoE3 but not apoE4 rescues impaired astrocyte activation in apoE null mice

Author

Gal Ophir, Sigal Meilin, Margalit Efrati, Joab Chapman, Dimitri Karussis, Allen Roses, and Daniel M Michaelson

Subjects
Alzheimer’s disease, Apolipoprotein E, Astrocytes, Brain inflammation, Transgenic mice, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

The allele E4 of apolipoprotein E (apoE) is an important risk factor for Alzheimer’s disease (AD) and the chronic brain inflammation which is associated with AD is more pronounced in subjects who carry this allele. In the present study, we employed mice transgenic for the human apoE isoforms apoE3 or apoE4 on a null mouse apoE background and intracerebroventricular injection of LPS to investigate the possibility that the regulation of brain inflammation is affected by the apoE genotype. LPS treatment of control mice resulted in activation of brain astrocytes and microglia whose extent decreased with age. LPS treatment of 6-month-old apoE transgenic and control mice resulted in marked activation of brain astrocytes in the control and apoE3 transgenic mice but had no effect on astrogliosis of age-matched apoE-deficient and apoE4 transgenic mice. In contrast, there were no significant differences between the levels of activated microglia of the apoE3 and apoE4 transgenic mice following LPS treatment. Immunoblot assays revealed that the apoE4 and apoE3 transgenic mice had the same levels of brain apoE, which were similarly increased following LPS treatment. These results show that LPS-induced astrogliosis in apoE transgenic mice is regulated isoform-specifically by apoE3 and not by apoE4 and suggest that similar mechanisms may mediate the phenotypic expression of the apoE4 genotype in AD and in other neurodegenerative diseases.

Published
2003
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49. Intraocular pressure and aqueous humor flow during a euglycemic-hyperinsulinemic clamp in patients with type 1 diabetes and microvascular complications

Author

Lane James T, Larson LuAnn, Fan Shan, Stoner Julie A, Margalit Eyal, and Toris Carol B

Subjects
Ophthalmology, RE1-994
Abstract

Abstract Background Microvascular complications, including retinopathy and nephropathy are seen with type 1 diabetes. It is unknown whether functional changes in aqueous humor flow or intraocular pressure (IOP) develop in parallel with these complications. This study was designed to test the hypothesis that clinical markers of microvascular complications coexist with the alteration in aqueous humor flow and IOP. Methods Ten patients with type 1 diabetes and ten healthy age- and weight-matched controls were studied. Aqueous flow was measured by fluorophotometry during a hyperinsulinemic-euglycemic clamp (insulin 2 mU/kg/min). Intraocular pressure was measured by tonometry at -10, 90 and 240 minutes from the start of the clamp, and outflow facility was measured by tonography at 240 minutes. Results During conditions of identical glucose and insulin concentrations, mean aqueous flow was lower by 0.58 μl/min in the diabetes group compared to controls (2.58 ± 0.65 versus 3.16 ± 0.66 μl/min, respectively, mean ± SD, p = 0.07) but statistical significance was not reached. Before the clamp, IOP was higher in the diabetes group (22.6 ± 3.0 mm Hg) than in the control group (19.3 ± 1.8 mm Hg, p = 0.01) but at 90 minutes into the clamp, and for the remainder of the study, IOP was reduced in the diabetes group to the level of the control group. Ocular pulse amplitude and outflow facility were not different between groups. Systolic blood pressure was significantly higher in the diabetes group, but diastolic and mean arterial pressures were not different. Conclusions We conclude that compared to healthy participants, patients with type 1 diabetes having microalbuminuria and retinopathy have higher IOPs that are normalized by hyperinsulinemia. During the clamp, a reduction in aqueous flow was not statistically significant.

Published
2010
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50. Outcome of retinopathy of prematurity patients following adoption of revised indications for treatment

Author

Ingvoldstad David D, Qiu Fang, Meza Jane L, Hejkal Thomas W, Mulhern Michael L, Alme Aaron M, and Margalit Eyal

Subjects
Ophthalmology, RE1-994
Abstract

Abstract Background The Early Treatment for Retinopathy of Prematurity study (ETROP), published in 2003, established new guidelines for treatment of retinopathy of prematurity (ROP) and demonstrated improved outcomes compared to previous guidelines. We examined outcomes before and after implementing the ETROP recommendations. Methods A retrospective chart review was performed using records of infants who had laser ablations for ROP performed from January, 2000 through December, 2005. Data collected included date of birth; birth weight; estimated gestational age (EGA); grading of ROP; date of laser ablation; and outcome of laser surgery. Univariate association with threshold or prethreshold treatment (Pre-ETROP and Post-ETROP, respectively) were assessed using t-tests or Wilcoxon tests. Additional comparison between groups was performed using Fisher's exact tests. Results 581 patients were examined before and 464 after December 2003. Of these, 29/581 (5% – Pre-ETROP Group) and 53/464 (11% – Post-ETROP Group) patients advanced to criteria requiring laser treatment respectively (P = 0.0001). The average estimated gestational age (EGA) at birth was 26.3 and 25.2 weeks, with an average birth weight of 888 and 707 grams for Pre and Post-ETROP Groups, respectively. Stage 5 retinal detachment (RD) developed in 10.3% of eyes in the Pre-ETROP Group and 1.9% of eyes in the Post-ETROP Group (P = 0.02). Conclusion After the ETROP guidelines were implemented, there was a decrease from 10.3% to 1.9% of eyes developing Stage 5 retinal detachment, despite this group having a lower average EGA and lower average birth weight. These results underscore the importance of adoption of the Revised Indications.

Published
2008
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