Your search keyword '"Stüve, Olaf"' showing total 88 results

1. Systems Approaches to Unravel T Cell Function and Therapeutic Potential in Autoimmune Disease.

Author

Salinas, Victor H. and Stüve, Olaf

Subjects

*T cell receptors, *AUTOIMMUNE diseases, *T cells, *CELL physiology, *CYTOTOXIC T cells, *REGULATORY T cells, *T helper cells

Abstract

The article reports that Producing Ag-specific immune responses constrained to target tissues or cells that can be engaged or disengaged at will is predicated on understanding the network of genes governing immune cell function. Topics include successes and limitations of chimeric Ag receptor (CAR) T cells emphasize this goal, and advances in high-throughput sequencing; and generation of synthetic T cells informed by the principles learned from these systems approaches.

Published

2021

2. Extended-interval dosing of natalizumab in NOVA.

Author

Stüve, Olaf and Tugemann, Bastian

Subjects

*NATALIZUMAB

Published

2023

3. Natalizumab for Multiple Sclerosis: A Case in Point for the Impact of Translational Neuroimmunology.

Author

Shirani, Afsaneh and Stüve, Olaf

Subjects

*NATALIZUMAB, *MULTIPLE sclerosis treatment, *NEUROIMMUNOLOGY, *LEUCOCYTE motility, *PROGRESSIVE multifocal leukoencephalopathy, *THERAPEUTICS

Abstract

Advances in translational neuroimmunology over the last two decades have revolutionized the treatment of relapsing forms of multiple sclerosis. A pathological hallmark of multiple sclerosis is the presence of leukocytes in the areas of disease activity in the CNS.Natalizumab inhibits the trafficking of lymphocytes from the blood into the brain and spinal cord by blocking the adhesion molecule α4-integrin. Representing the enormous success of a molecular targeted approach, natalizumab was the first mAb approved for the treatment of relapsing--remitting multiple sclerosis. However, only a few months after its approval, natalizumab was withdrawn from the market because of an unanticipated life threatening adverse effect: progressive multifocal leukoencephalopathy. Natalizumab was later reintroduced with required adherence to a strict monitoring program. In this article, we review the bench-to-bedside journey of natalizumab, along with the lessons learned from postmarketing studies. [ABSTRACT FROM AUTHOR]

Published

2017

4. A critical appraisal of treatment decisions in multiple sclerosis--old versus new.

Author

Kieseier, Bernd C., Stüve, Olaf, and Stüve, Olaf

Subjects

*INTERFERONS, *MULTIPLE sclerosis treatment, *IMMUNE system, *IMMUNOTHERAPY, *QUALITY of life

Abstract

Interferon β and glatiramer acetate have been available for the treatment of multiple sclerosis (MS) for over a decade and their efficacy and safety are well established. These agents have detectable effects on the immune system, but have not been associated with a breakdown of immune surveillance. Novel MS therapies have been approved, or are awaiting approval, that differ from established immunotherapies with regard to their mechanisms of action, modes of administration, adverse-effect profiles and, possibly, the clinical and paraclinical benefits that they may provide for patients. Neurologists will soon be required to make complex treatment decisions with their patients on the basis of very limited clinical data and evidence. Under these circumstances, optimal assessment of risks and benefits will be challenging. In this Review, the anticipated benefits of novel therapies, including reduction in disease activity, possible prevention of disability, and improvement in quality of life, are outlined. In addition, the current acceptance of potential risks--including serious or even life-threatening adverse effects, the likelihood of which may rise with increased cumulative exposure to a particular agent--by patients with MS will be reviewed. [ABSTRACT FROM AUTHOR]

Published

2011

5. Immunomodulatory synergy by combination of atorvastatin and glatiramer acetate in treatment of CNS autoimmunity.

Author

Stüve, Olaf, Youssef, Sawsan, Weber, Martin S., Nessler, Stefan, von Budingen, Hans-Christian, Hemmer, Bernhard, Prod'homme, Thomas, Sobel, Raymond A., Steinman, Lawrence, Zamvil, Scott S., Stüve, Olaf, and von Büdingen, Hans-Christian

Subjects

*IMMUNOLOGICAL adjuvants, *CENTRAL nervous system, *AUTOIMMUNITY, *HYDROXYMETHYLGLUTARYL coenzyme A reductases, *TH2 cells, *CYTOKINES, *ANIMAL experimentation, *CELL culture, *COMBINATION drug therapy, *COMPARATIVE studies, *DEMYELINATION, *FATTY acids, *HETEROCYCLIC compounds, *MICE, *MONOCYTES, *MULTIPLE sclerosis, *PEPTIDES, *RESEARCH funding, *T cells, *PHARMACODYNAMICS, *THERAPEUTICS

Abstract

One approach to improving efficacy in MS therapy is to identify medications that provide additive or synergistic benefit in combination. Orally administered cholesterol-lowering HMG-CoA reductase inhibitors (known as statins), which exhibit immunomodulatory properties and are effective in treatment of the MS model EAE, are being tested in MS. As atorvastatin can enhance protective Th2 responses and has a different mechanism of action than glatiramer acetate (GA), a parenterally administered immunomodulatory agent approved for MS treatment, we tested whether the combination of these agents could be beneficial in EAE. Combination therapy using suboptimal doses of atorvastatin and GA prevented or reversed clinical and histologic EAE. Secretion of proinflammatory Th1 cytokines was reduced--and conversely Th2 cytokine secretion was increased--in these mice, but not in mice treated with each drug alone at the same doses. Monocytes treated with the combination of suboptimal doses of atorvastatin and GA secreted an antiinflammatory type II cytokine pattern and, when used as APCs, promoted Th2 differentiation of naive myelin-specific T cells. Our results demonstrate that agents with different mechanisms of immune modulation can combine in a synergistic manner for the treatment of CNS autoimmunity and provide rationale for testing the combination of atorvastatin and GA in MS. [ABSTRACT FROM AUTHOR]

Published

2006

6. Evaluation of HMG-CoA reductase inhibitors for multiple sclerosis: opportunities and obstacles.

Author

Neuhaus, Oliver, Stüve, Olaf, Zamvil, Scott S., Hartung, Hans-Peter, and Stüve, Olaf

Subjects

*HYDROXYMETHYLGLUTARYL coenzyme A reductases, *MULTIPLE sclerosis, *ENCEPHALOMYELITIS, *IMMUNOLOGICAL adjuvants, *MAGNETIC resonance, *DEMYELINATION, *ANTILIPEMIC agents, *CLINICAL trials, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *EVALUATION research

Abstract

The disease-modifying agents currently used in the treatment of multiple sclerosis (MS) are not completely effective and are associated with adverse effects and high costs. Thus, alternative treatment options are highly desirable. HMG-CoA reductase inhibitors (statins), widely prescribed as cholesterol-lowering agents, may be a future treatment option for MS--either in an add-on therapy regimen or alone--as they have been shown to exhibit potent immunomodulatory effects. Several recent reports have demonstrated that HMG-CoA reductase inhibitors prevent and reverse chronic and relapsing experimental autoimmune encephalomyelitis, an animal model of MS. Furthermore, in vitro experiments with human immune cells have shown an immunomodulatory mode of action of HMG-CoA reductase inhibitors that is comparable to that of interferon-beta, an established treatment for MS. An open-label clinical trial assessing simvastatin treatment in patients with MS revealed a significant decrease in the number and volume of new lesions, as assessed using magnetic resonance imaging, and a favourable safety profile. A large multicentre, placebo-controlled phase II clinical trial assessing atorvastatin in patients with a clinically isolated syndrome (i.e. a single clinical event that is indicative of demyelination, and that predisposes to the development MS) has recently been initiated. However, prospective placebo-controlled trials of HMG-CoA reductase inhibitors in definite MS are difficult to perform because of ethical and financial issues. Furthermore, overly optimistic reports in the popular media, as well as the often uncontrolled access to HMG-CoA reductase inhibitors by patients with MS, complicate the evaluation of HMG-CoA reductase inhibitors as a realistic future treatment option for MS. [ABSTRACT FROM AUTHOR]

Published

2005

7. Normal intrathecal leukocyte cell number and composition do not decrease the incidence of post–lumbar puncture headache.

Author

Stüve, Olaf, Cataldi, Fabio, Pradhan, Vivek, and Gorelick, Kenneth J.

Subjects

*LEUCOCYTES, *HEADACHE, *HEAD diseases, *LUMBAR puncture, *SPINAL anesthesia

Abstract

The pathogenesis of post–lumbar puncture headache (PLPH) has remained unclear. A beneficial role of CSF cells in the repair of a post-traumatic dural CSF leak has been suggested. The primary purpose of this study was to investigate the effects of 8 weeks of induction therapy with high-dose PF-00547659 on the cellular elements of CNS immune surveillance in patients with active Crohn's Disease and a history of immunosuppressive therapy ( Clinicaltrials.gov NCT01387594 ). PF-00547659 is a human monoclonal antibody that binds to mucosal addressin–cell adhesion molecule 1 (MAdCAM-1) on endothelial cells and blocks its interaction with beta7-integrin expressing lymphocytes. The study was executed in three parts or cohorts under two protocols. The incidence of a PLPH was 35% after the initial lumbar puncture, and 26% following the second lumbar puncture. After initiation of PF-00547659 anti-MAdCAM-1 therapy, there was a small and non-significant increase in the numbers of overall CSF leukocytes, and in lymphocyte subsets (CD3 +, CD4 +, and CD8 + T cells). The lymphocyte composition was unaltered by PF-00547659 anti-MAdCAM-1 therapy. Our observations suggest that normal numbers and composition of intrathecal leukocytes do not decrease the incidence of PLPH. [ABSTRACT FROM AUTHOR]

Published

2017

8. CD19 as a molecular target in CNS autoimmunity.

Author

Stüve, Olaf, Warnke, Clemens, Deason, Krystin, Stangel, Martin, Kieseier, Bernd, Hartung, Hans-Peter, Büdingen, Hans-Christian, Centonze, Diego, Forsthuber, Thomas, and Knappertz, Volker

Subjects

*MULTIPLE sclerosis, *CD19 antigen, *CENTRAL nervous system, *AUTOIMMUNITY, *HUMORAL immunity, *AQUAPORINS

Abstract

Multiple sclerosis (MS) and neuromyelitis optica (NMO) are the most prevalent neuroinflammatory diseases of the central nervous system (CNS). The immunological cascade of these disorders is complex, and the exact spatial and temporal role of different immune cells is not fully understood. Although MS has been considered for many years to be primarily T cell driven, it is well established that B cells and the humoral immune response play an important role in its pathogenesis. This has long been evident from laboratory findings that include the presence of oligoclonal bands in the CSF. In NMO, the importance of the humoral immune system appears even more obvious as evidenced by pathogenic antibodies against aquaporin 4 (AQP4). Besides their capacity to mature into antibody-producing plasma cells, B cells are potent antigen-presenting cells to T lymphocytes and they can provide soluble factors for cell activation and differentiation to other immune-competent cells. In MS and NMO, there are substantial data from clinical trials that B cell depletion with CD20-directed agents is effective and relatively safe. Plasma cells, which produce antibodies against molecular targets expressed by the host, but which also provide humoral immune responses against pathogens, are not targeted by anti-CD20 therapies. Therefore, the depletion of CD19-expressing cells would offer potential advantages with regard to efficacy, but potentially higher risks with regard to infectious complications. This review will outline the rationale for CD19 as a molecular target in CNS autoimmunity. The current stage of drug development is illustrated. Potential safety concerns will be discussed. [ABSTRACT FROM AUTHOR]

Published

2014

9. 200 years after Darwin.

Author

Rosenberg, Roger N., Stüve, Olaf, Eagar, Todd, and Stüve, Olaf

Subjects

*GENETIC polymorphism research, *NATURAL selection, *GENOMICS, *GENETICS, *AMYOTROPHIC lateral sclerosis, *ALZHEIMER'S disease, *ALZHEIMER'S disease research

Abstract

The authors discuss research which investigates the genetic basis for natural selection, noting that February 12, 2009 marks the 200th anniversary of the birth of naturalist Charles Darwin. They explain that molecular genomic analysis provides information regarding biological fitness and the risk of developing disease. They comment on genome-wide association studies which look at gene variations for several diseases, including amyotrophic lateral sclerosis and Alzheimer disease.

Published

2009

10. Immune-mediated CNS diseases: A review on nosological classification and clinical features

Author

Zettl, Uwe K., Stüve, Olaf, and Patejdl, Robert

Subjects

*CENTRAL nervous system diseases, *PATHOLOGICAL physiology, *MULTIPLE sclerosis, *POSTVACCINAL encephalitis, *DIFFUSE cerebral sclerosis, *OPTIC neuritis, *MYELIN sheath diseases

Abstract

Abstract: The immune-mediated diseases of the central nervous system (CNS) cover a wide range of clinical manifestations. Over the last years, considerable efforts have been made to establish a nosologic concept based upon distinctive pathophysiological characteristics of the single diseases. We describe the historically defined entities of immune-mediated diseases that primarily, but not exclusively, are affecting myelin structures. These include very rare entities as Schilder''s, Balo''s and Marburg''s disease or the chronic and relapsing types of optic neuritis, for which evidence based paradigms still are virtually missing. In other, slightly more frequent diseases as neuromyelitis optica (NMO), advances in the concepts of specific biological features have been achieved and are beginning to transform into changes in clinical concepts. Acute disseminated encephalomyelitis (ADEM) and multiple sclerosis (MS) are by far the most frequent entities in this group and thus the only ones for which extensive empirical data on disease biology and evidence based clinical management strategies exist by now. For the most important entities, clinical features and therapeutic approaches are reviewed on the basis of current evidence. The results of basic science studies are assessed for their implications in nosological classification. [Copyright &y& Elsevier]

Published

2012

11. Multiple Sclerosis in the Elderly Patient.

Author

Awad, Amer and Stüve, Olaf

Subjects

*MULTIPLE sclerosis, *DISEASES in older people, *MEDICAL care, *LIFE expectancy, *AGE factors in disease, *DIAGNOSIS

Abstract

Multiple sclerosis (MS) is an acquired inflammatory demyelinating disease of the CNS that is typically diagnosed in the second or third decade of life. It is generally believed that over the last few decades the life expectancy of patients with adult onset MS (AOMS) has approached that of the general population as a result of better medical and nursing care. Thus, an increasing number of MS patients are entering or have reached senescence. A second group of elderly patients with MS that may be very different in terms of disease pathogenesis are patients with late onset MS (LOMS). The diagnosis in LOMS patients can be challenging because of a large number of ageassociated MS differential diagnoses, atypical presentations, a low index of suspicion and the lack of diagnostic criteria specific to this age group. Also, specific problems these patients encounter have only recently become a focus of attention. Changes in renal and hepatic function with age, in addition to the coexistence of medical co–morbidities, require special attention in the management of elderly patients with MS. In this review we outline the characteristics of senescent AOMS and LOMS patients. In addition, we discuss therapeutic strategies in elderly patients with MS based on our knowledge of immunosenescence and age–associated characteristics of this disorder. Given the overall aging of the population, focusing on these two patient groups appears highly relevant. [ABSTRACT FROM AUTHOR]

Published

2010

12. Primary progressive multiple sclerosis--why we are failing.

Author

Segal, Benjamin M. and Stüve, Olaf

Subjects

*FINGOLIMOD, *MULTIPLE sclerosis, *MYELIN sheath diseases, *NEURODEGENERATION

Abstract

The author discusses the negative results of a randomised trial which evaluates the efficacy of fingolimod in patients with primary progressive multiple sclerosis. He states that the result is disappointing because of the lack of a U.S. Food and Drug Administration-approved disease-modifying therapies for primary progressive multiple sclerosis. Also discussed is the significance of inflammatory versus neurodegenerative processes in progressive forms of multiple sclerosis.

Published

2016

13. α4-Integrin antagonism with natalizumab.

Author

Stüve, Olaf, Gold, Ralf, Chan, Andrew, Mix, Eilhard, Zettl, Uwe, and Kieseier, Bernd

Subjects

*MULTIPLE sclerosis, *MONOCLONAL antibodies, *T cells, *DENDRITIC cells, *CEREBROSPINAL fluid, *IMMUNOSUPPRESSION, *CLINICAL trials

Abstract

Based on the results of two phase III clinical trials, the humanized recombinant monoclonal antibody natalizumab was approved for the treatment of relapsing forms of multiple sclerosis (MS). Since its initial approval in November 2004, it has been announced that six patients who received natalizumab in the context of clinical studies acquired an infection with the human polyoma virus JC and were diagnosed with progressive multifocal leukoencephalopathy (PML). Two of these individuals had a fatal outcome. Our groups recently showed that natalizumab therapy results in a reduction of CD4+ T cells within the cerebrospinal fluid (CSF) that is ten-fold more pronounced than the reduction in the number of CD8+ T lymphocytes. Interestingly, it appears that the effect of natalizumab on cell numbers in the CSF persists for at least 6 months after cessation of treatment. More recently, we studied the expression of major histocompatibility complex (MHC) I and II, and the number and phenotypes of leukocytes in cerebral perivascular spaces (CPVS). We observed that natalizumab therapy was associated with a significant decrease in the cell surface expression of MHC class II molecules, and the numbers of dendritic cells in CPVS. In addition, no CD4+ T cells were detectable in this compartment. Our observations may explain the differential and prolonged effects of natalizumab therapy on different leukocyte subsets in the central nervous system. They also suggest that natalizumab treatment may result in prolonged immunosuppression in peripheral organs, and the delayed onset of adverse events. [ABSTRACT FROM AUTHOR]

Published

2008

14. Immunosuppression in clinical practice.

Author

Chan, Andrew, Stüve, Olaf, and von Ahsen, Nicolas

Subjects

*IMMUNOSUPPRESSION, *IMMUNOSUPPRESSIVE agents, *DRUG side effects, *PATIENTS, *PHARMACOGENOMICS

Abstract

Despite novel immunoactive agents, immunosuppressants still play a considerable role in the treatment of MS, especially in rapidly progressive cases. Given the limited tolerability and potentially severe side effects of most immunosuppressive drugs, identification of patients with a favorable benefit-risk profile is essential. A narrow therapeutic index, with sometimes high interindividual variability in terms of response and side effects may partially be explained by genetic factors affecting different metabolic pathways. Here, we will review practical aspects in the clinical use of immunosuppressants in MS and discuss approaches to individualized treatment schemes, including novel pharmacogenetic strategies. [ABSTRACT FROM AUTHOR]

Published

2008

15. Pharmacological Treatment of Early Multiple Sclerosis.

Author

Stüve, Olaf, Bennett, Jeffrey L., Hemmer, Bernhard, Wiendl, Heinz, Racke, Michael K., Bar-Or, Amit, Wei Hu, Zivadinov, Robert, Weber, Martin S., Zamvil, Scott S., Pacheco, Maria F., Menge, Til, Hartung, Hans-Peter, Kieseier, Bernd C., and Frohman, Elliot M.

Subjects

*MULTIPLE sclerosis treatment, *DRUG utilization, *TREATMENT programs, *CLINICAL medicine, DISEASE relapse prevention

Abstract

Currently, six medications are approved by the US FDA for the treatment of relapsing forms of multiple sclerosis (MS). In contrast, no pharmacological agent has proved to be effective in patients with secondary-progressive MS without relapses, or in patients with primary-progressive MS. One of the principal issues concerning an optimal pharmacotherapy for relapsing forms of MS is the optimal time of treatment initiation. There is now an almost universal consensus among MS experts that many patients will benefit from early therapy. However, several formidable challenges exist in identifying individuals who will benefit versus those who will do well without intervention. How do we define early MS and what clinical and paraclinical markers may be useful in defining the timing and nature of therapy? Do patients with a benign form of MS require therapy or are they exposed unnecessarily to adverse effects of our currently available medications? How do we identify disease progression and treatment failures? This review discusses these issues and outlines the evidence for application of 'early' treatment in patients with relapsing forms of MS. [ABSTRACT FROM AUTHOR]

Published

2008

16. Pharmacological Properties, Toxicology and Scientific Rationale for the use of Natalizumab (Tysabri®) in Inflammatory Diseases.

Author

Stüve, Olaf and Bennett, Jeffrey L.

Subjects

*CELL adhesion molecules, *MULTIPLE sclerosis, *MONOCLONAL antibodies, *ENCEPHALOMYELITIS, *T cells, *TOXICOLOGY

Abstract

Natalizumab (Tysabri®) was the first adhesion molecule antagonist to make it into clinical trial for patients with multiple sclerosis (MS) and other inflammatory disorders. Natalizumab is a humanized recombinant monoclonal antibody (MAb) that binds to the alpha (α)4 chain of the α4 beta (β)1 (very late activating antigen 4; VLA-4) and α4β7 integrins. The scientific rationale for natalizumab therapy is the reduction of leukocyte extravasation into peripheral tissues. Natalizumab, like other VLA-4 antagonists, may also interfere with the activation of T lymphocytes in secondary lymphoid organs and their reactivation in the central nervous system (CNS). Shortly after its approval for the treatment of relapsing-remitting MS (RR-MS), three patients who were treated with natalizumab in the setting of clinical trials developed progressive multifocal leukoencephalopathy (PML), an opportunistic infection of the brain with the polyoma virus JC. It remains to be elucidated why the use of this VLA-4 antagonist is associated with an increased incidence of PML. Natalizumab was recently reapproved for the treatment of relapsing forms of MS. In this review, we outline the scientific rationale for using natalizumab in MS and other inflammatory disorders. In addition, an overview of pharmacological properties, clinical efficacy, safety, and toxicology of natalizumab is provided. [ABSTRACT FROM AUTHOR]

Published

2007

17. Immune response to immunotherapy: the role of neutralising antibodies to interferon beta in the treatment of multiple sclerosis

Author

Hemmer, Bernhard, Stüve, Olaf, Kieseier, Bernd, Schellekens, Huub, and Hartung, Hans-Peter

Subjects

*IMMUNE response, *INTERFERONS, *IMMUNOGLOBULINS, *MULTIPLE sclerosis, *IMMUNOLOGY

Abstract

Summary: Interferon beta was the first therapy to be approved for the treatment of relapsing-remitting multiple sclerosis (MS) more than 10 years ago. Interferon beta reduces relapse rates and disease burden and activity, and it may have beneficial effects on the progression of long-term disease disability. The occurrence of neutralising interferon-beta antibodies has been postulated as a possible cause of the failure of interferon beta in some patients with MS. Here we discuss the basic mechanisms that may account for the generation of an interferon-beta antibody response and its biological implications. We review the evidence for neutralising antibodies as a consequence of interferon-beta treatment, and discuss the implications for the treatment of MS. Strategies to assess and manage the long-term impact of neutralising antibodies will be outlined. [Copyright &y& Elsevier]

Published

2005

18. Putative mechanisms of action of statins in multiple sclerosis – comparison to interferon-β and glatiramer acetate

Author

Neuhaus, Oliver, Stüve, Olaf, Archelos, Juan J., and Hartung, Hans-Peter

Subjects

*ANTICHOLESTEREMIC agents, *MULTIPLE sclerosis, *STATINS (Cardiovascular agents), *ISOPENTENOIDS

Abstract

Abstract: Statins are inhibitors of 3-hydroxy-3-methylglutaryl coenzyme A reductase and are widely prescribed as cholesterol-lowering agents. They are promising candidates for future treatment in multiple sclerosis (MS) as they have been shown to exhibit immunomodulatory effects. Recent reports have demonstrated that statins are effective in preventing and reversing chronic and relapsing experimental autoimmune encephalomyelitis (EAE), an animal model of MS. Furthermore, in vitro experiments with human immune cells have documented an immunomodulatory mode of action of statins comparable to that of interferon (IFN)-β. An open label clinical trial assessing simvastatin in MS revealed a significant decrease in the number and volume of new MRI lesions and a favourable safety profile. This article reviews data thus far present on the putative mechanisms of action of statins in the immunopathogenesis of MS. Furthermore, the role of statins as potential pharmacotherapy for MS is discussed in the context of the mechanisms of approved immunotherapies in MS, namely IFN-β and glatiramer acetate (GA). [Copyright &y& Elsevier]

Published

2005

19. Mitoxantrone as a potential therapy for primary progressive multiple sclerosis.

Author

Stüve, Olaf, Kita, Mariko, Pelletier, Daniel, Fox, Robert J., Stone, Jerome, Goodkin, Donald E., and Zamvil, Scott S.

Subjects

*MULTIPLE sclerosis, *MITOXANTRONE hydrochloride, *CLINICAL trials, *GENETICS, *IMMUNOLOGY, *MAGNETIC resonance imaging, *PATHOLOGY, *NEUROLOGY

Abstract

Mitoxantrone (Novantrone®) was the first drug approved in western Europe and North America for treatment of secondary progressive multiple sclerosis (SPMS) and progressive relapsing MS (PRMS). Pharmacological properties of mitoxantrone, its role in SPMS, the study rational and design of an ongoing multi-centre, double blind, randomized, placebo-controlled phase 2 trial will be outlined in this article. [ABSTRACT FROM AUTHOR]

Published

2004

20. The HMG-CoA reductase inhibitor, atorvastatin, promotes a Th2 bias and reverses paralysis in central nervous system autoimmune disease.

Author

Youssef, Sawsan, Stüve, Olaf, Patarroyo, Juan C., Ruiz, Pedro J., Radosevich, Jennifer L., Hur, Eun Mi, Bravo, Manuel, Mitchell, Dennis J., Sobel, Raymond A., Steinman, Lawrence, and Zamvil, Scott S.

Subjects

*HYDROXYMETHYLGLUTARYL coenzyme A reductases, *AUTOIMMUNE diseases, *CENTRAL nervous system diseases

Abstract

Statins, 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase inhibitors, which are approved for cholesterol reduction, may also be beneficial in the treatment of inflammatory diseases. Atorvastatin (Lipitor) was tested in chronic and relapsing experimental autoimmune encephalomyelitis, a CD4[sup +] Th1-mediated central nervous system (CNS) demyelinating disease model of multiple sclerosis. Here we show that oral atorvastatin prevented or reversed chronic and relapsing paralysis. Atorvastatin induced STAT6 phosphorylation and secretion of Th2 cytokines (interleukin (IL)-4, IL-5 and IL-10) and transforming growth factor (TGF)-β. Conversely, STAT4 phosphorylation was inhibited and secretion of Th1 cytokines (IL-2, IL-12, interferon (IFN)-γ and tumour necrosis factor (TNF)-α) was suppressed. Atorvastatin promoted differentiation of Th0 cells into Th2 cells. In adoptive transfer, these Th2 cells protected recipient mice from EAE induction. Atorvastatin reduced CNS infiltration and major histocompatibility complex (MHC) class II expression. Treatment of microglia inhibited IFN-γ-inducible transcription at multiple MHC class II transactivator (CIITA) promoters and suppressed class II upregulation. Atorvastatin suppressed IFN-γ-inducible expression of CD40, CD80 and CD86 co-stimulatory molecules. L-Mevalonate, the product of HMG-CoA reductase, reversed atorvastatin's effects on antigenpresenting cells (APC) and T cells. Atorvastatin treatment of either APC or T cells suppressed antigen-specific T-cell activation. Thus, atorvastatin has pleiotropic immunomodulatory effects involving both APC and T-cell compartments. Statins may be beneficial for multiple sclerosis and other Th1-mediated autoimmune diseases. [ABSTRACT FROM AUTHOR]

Published

2002

21. The major histocompatibility complex and antibody-mediated limbic encephalitis.

Author

Stüve, Olaf, Vernino, Steven, and Stüve, Olaf

Abstract

In this article, the author discusses association of antileucine- rich glioma-inactivated1 (anti-LGI1) encephalitis with the major histocompatibility complex (MHC) II haplotype human leukocyte antigen (HLA). Topics discussed include observation of human leukocyte antigen (HLA) in several human immunemediated disorders; expression of MHC II on all nucleated cells; and therapeutic interventions in patients with anti-LGI1 encephalitis.

Published

2017

22. Multiple sclerosis: Natalizumab to fingolimod--the washout whitewash.

Author

Stangel, Martin and Stüve, Olaf

Published

2014

23. Trials and therapies in secondary progressive MS, simplified.

Author

Manouchehri, Navid and Stüve, Olaf

Subjects

*NOSOLOGY, *MULTIPLE sclerosis, *CLINICAL trials

Abstract

The FDA approvals of siponimod and cladribine for secondary progressive multiple sclerosis raise questions about the diagnostic criteria for multiple sclerosis phenotypes and their applicability to clinical trials. A simpler classification for the disease could be the answer. [ABSTRACT FROM AUTHOR]

Published

2019

24. Time to talk about timing – when to start, stop and change anti-migratory drugs in MS.

Author

Stüve, Olaf and Hemmer, Bernhard

Subjects

*MULTIPLE sclerosis treatment, *NATALIZUMAB, *AUTOIMMUNE diseases, *IMMUNOLOGIC diseases, *ALTERNATIVE medicine, *DRUG therapy

Abstract

The authors reflect on the right time to discuss anti-migratory drugs in multiple sclerosis (MS). They note that neither natalizumab nor fingolimod change the autoimmune response underlying MS. They point out that stopping either or both drugs is unreasonable without alternative therapies. They add that sequential pharmacotherapies involving fingolimod and natalizumab become a significant issue since they are widely used.

Published

2012

25. Is 1+1 0, 1, 2, or 11? Arithmetics of antiinflammatory agents in autoimmunity

Author

Hofstetter, Harald H., Stüve, Olaf, and Hartung, Hans-Peter

Published

2009

26. The effects of natalizumab on the innate and adaptive immune system in the central nervous system

Author

Stüve, Olaf

Subjects

*MONOCLONAL antibodies, *MULTIPLE sclerosis, *CENTRAL nervous system diseases, *IMMUNE system

Abstract

Abstract: Multiple sclerosis (MS) is an inflammatory demyelinating disorder of the central nervous system (CNS). Natalizumab (®Tysabri) is a humanized recombinant monoclonal antibody that binds to the alpha (α)4 chain of the α4 beta (β)1 integrin (very late activation antigen 4; VLA-4), and α4β7 integrin. Recently, two patients with MS and one patient with Crohn’s disease who were treated with natalizumab in the setting of clinical trials developed progressive multifocal leukoencephalopathy (PML), an opportunistic infection of the brain with the polyoma virus JC. We recently showed that natalizumab decreases the numbers of CD4+ and CD8+ T lymphocytes, CD19+ B cells, and CD138+ plasma cells in the cerebrospinal fluid (CSF) of patients with MS on natalizumab therapy. In addition, we demonstrated that the cell numbers in CSF remained unchanged even 6 months after cessation of natalizumab treatment. [Copyright &y& Elsevier]

Published

2008

27. Temporary leukocyte effects in temporal lobe epilepsy?

Author

Hofstetter, Harald H., Stüve, Olaf, and Hartung, Hans-Peter

Published

2008

28. Are statins a treatment option for multiple sclerosis?

Author

Neuhaus, Oliver, Stüve, Olaf, Zamvil, Scott S, and Hartung, Hans-Peter

Subjects

*MULTIPLE sclerosis, *INTERFERONS, *DRUGS, *ACETATES, *IMMUNOSUPPRESSION, *AUTOIMMUNE diseases, *ENCEPHALOMYELITIS

Abstract

Background Treatment options for multiple sclerosis (MS) are limited. The immunomodulatory drugs interferon beta and glatiramer acetate are only partly effective in reducing the relapse rate, slowing disease progression, and diminishing the number and volume of lesions on MRI. Mitoxantrone is an immunosuppressant approved for the treatment of active forms of relapsing-remitting or secondary progressive MS, but is dose-limited owing to its potential cardiotoxicity. Thus, identifying new effective therapeutic options with few side-effects is highly desirable.Recent developments Evidence has emerged that statins, which are inhibitors of 3-hydroxy-3-methylglutaryl coenzyme A reductase, have immunomodulatory effects. Recent reports showed that statins prevent and reverse chronic and relapsing experimental autoimmune encephalomyelitis, an animal model of MS. Furthermore, in vitro experiments with human immune cells have shown an immunomodulatory profile of statins comparable to that of interferon beta. An open label clinical trial of simvastatin for MS revealed a significant decrease in the number and volume of new MRI lesions and a favourable safety profile.Where next? The obvious advantage of statins over existing MS therapies is their oral route of dosing. Statins might be beneficial for MS patients as monotherapy or as an add-on to established disease modifying drugs. As the evidence of the benefit of statins in MS is currently insufficient, large controlled clinical trials are needed. The first of these trials is about to start. [Copyright &y& Elsevier]

Published

2004

29. Multiple sclerosis: combination therapy in MS--still a valid strategy.

Author

Kieseier, Bernd C., Stüve, Olaf, and Stüve, Olaf

Subjects

*MULTIPLE sclerosis treatment, *SIMVASTATIN, *INTERFERONS, *DRUG efficacy, *CLINICAL drug trials

Abstract

The article discusses a recent study published in "The Lancet Neurology," which reported negative results of combination therapy in multiple sclerosis (MS). The study has demonstrated that simvastatin as an add-on therapy has no beneficial clinical or paraclinical effect on the treatment of MS. It presents an overview of the simvastatin as add-on therapy to interferon (IFN) β-1ba for relapsing-remitting MS (RRMS) (SIMCOMBIN) trial.

Published

2011

30. Multiple sclerosis drugs: how much bang for the buck?

Author

Stüve, Olaf and Cutter, Gary R

Published

2015

31. Does risk stratification decrease the risk of natalizumab-associated PML? Where is the evidence?

Author

Cutter, Gary R and Stüve, Olaf

Subjects

*NATALIZUMAB, *PROGRESSIVE multifocal leukoencephalopathy, *IMMUNOGLOBULINS, *IMMUNOSUPPRESSIVE agents, *DISEASE risk factors, *THERAPEUTICS

Abstract

The use of natalizumab has likely been limited by its association with progressive multifocal leukoencephalopathy (PML), an infection caused by the human polyomavirus John Cunningham (JC). Three factors were recently identified that contribute to the overall risk of natalizumab-associated PML: (1) Positive serostatus for anti-JCV antibodies, (2) prior use of immunosuppressants, and (3) duration of natalizumab therapy. This risk stratification algorithm has not led to a reduction in the incidence of PML in natalizumab-treated patients with multiple sclerosis between April 2010 and February 2014. This observation may appear perplexing, as treatment duration and JCV serostatus are modifiable risk factors. Potential reasons for the lack of success of companion diagnostics that determine the overall risk of natalizumab-associated PML are discussed. [ABSTRACT FROM AUTHOR]

Published

2014

32. The role of B cells in multiple sclerosis: Current and future therapies.

Author

Negron, Austin, Robinson, Rachel R., Stüve, Olaf, and Forsthuber, Thomas G.

Subjects

*B cells, *MULTIPLE sclerosis, *T cells, *CELL physiology, *MONOCLONAL antibodies

Abstract

• Peripheral B cell tolerance mechanisms are defective in multiple sclerosis (MS). • Multiple B cell effector functions can contribute to MS pathology. • B cell-depleting monoclonal antibody therapies are effective in MS. • Current disease-modifying therapies in MS have appreciable effects on B cells. • Future B cell targets include pathogenic subsets, signaling, and survival factors. While it was long held that T cells were the primary mediators of multiple sclerosis (MS) pathogenesis, the beneficial effects observed in response to treatment with Rituximab (RTX), a monoclonal antibody (mAb) targeting CD20, shed light on a key contributor to MS that had been previously underappreciated: B cells. This has been reaffirmed by results from clinical trials testing the efficacy of subsequently developed B cell-depleting mAbs targeting CD20 as well as studies revisiting the effects of previous disease-modifying therapies (DMTs) on B cell subsets thought to modulate disease severity. In this review, we summarize current knowledge regarding the complex roles of B cells in MS pathogenesis and current and potential future B cell-directed therapies. [ABSTRACT FROM AUTHOR]

Published

2019

33. Firategrast—natalizumab in a pill?

Author

Prat, Alexandre, Stüve, Olaf, Miller, David H, Weber, Thomas, Grove, Richard, Wardell, Claire, Horrigan, Joseph, Graff, Ole, Atkinson, Gillian, Dua, Pinky, Yousry, Tarek, Macmanus, David, and Montalban, Xavier

Subjects

*CELL receptors, *CHEMICAL elements, *CLINICAL trials, *COMPARATIVE studies, *DOSE-effect relationship in pharmacology, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *MONOCLONAL antibodies, *MULTIPLE sclerosis, *PLACEBOS, *RESEARCH, *EVALUATION research, *RANDOMIZED controlled trials, *TREATMENT effectiveness, *BLIND experiment

Abstract

Background: Monoclonal antibody therapy against α4β-integrin is efficacious in patients with multiple sclerosis (MS) with some safety concerns. We assessed the safety and efficacy of firategrast, a small oral anti-α4β-integrin molecule, in patients with relapsing remitting MS.Methods: We did a multicentre, phase 2, randomised, double-blind, placebo-controlled, dose-ranging study in participants with clinically definite relapsing-remitting MS. A 24-week treatment period was followed by 12 weeks of core follow-up and 40 weeks of extended follow-up. Participants were randomly assigned, via computer-generated block randomisation in a 1:2:2:2 ratio, to receive one of four treatments twice a day: firategrast 150 mg, firategrast 600 mg, or firategrast 900 mg (women) or 1200 mg (men), or placebo. Brain scans were obtained at 4-week intervals to the end of core follow-up. The primary outcome was cumulative number of new gadolinium-enhancing brain lesions during the treatment phase and was analysed using a generalised linear model with an underlying negative binomial distribution, adjusted for sex, baseline number of new gadolinium-enhancing lesions, and country. This study is registered with ClinicalTrials.gov, NCT00395317.Findings: Of 343 individuals enrolled, 49 received firategrast 150 mg, 95 received firategrast 600 mg, 100 received firategrast 900 mg or 1200 mg, and 99 received placebo. A 49% reduction (95% CI 21·2-67·6; p=0·0026) in the cumulative number of new gadolinium-enhancing lesions was seen for the 900 mg or 1200 mg firategrast group (n=92, mean number of lesions 2·69 [SE 1·18]) versus the placebo group (90, 5·31 [1·18]). In the 600 mg group (86, 4·12 [SE 1·19]), a non-significant 22% reduction (95% CI -21·3 to 49·7; p=0·2657) occurred in mean number of new gadolinium-enhanced lesions relative to placebo; for the 150 mg group (47, 9·51 [SE 1·24]), a 79% increase (95% CI 4·1-308·1; p=0·0353) occurred relative to placebo. Firategrast was generally well tolerated at all doses. The frequency of all adverse events was similar across all treatment groups except for an increased rate of urinary tract infections in the high-dose firategrast group. No cases of progressive multifocal leukoencephalopathy or evidence of reactivation of JC virus were identified.Interpretation: This study showed efficacy on imaging endpoints for firategrast at the highest dose tested, and suggests that further investigation of oral short-acting α4β integrin blockade therapies is warranted.Funding: GlaxoSmithKline. [ABSTRACT FROM AUTHOR]

Published

2012

34. Anticipated benefits and surprising effects of daclizumab in multiple sclerosis

Author

Stüve, Olaf and Greenberg, Benjamin M

Published

2010

35. B cells, antibodies, and tertiary lymphoid tissue in MS brains

Author

Stüve, Olaf and Eagar, Todd N

Published

2008

36. Revised criteria for neuromyelitis optica—a new diagnostic standard?

Author

Hemmer, Bernhard and Stüve, Olaf

Subjects

*OPTIC neuritis, *MYELITIS, *DIAGNOSIS, *NEUROLOGY, *MAGNETIC resonance imaging

Abstract

BACKGROUND In 1999, Wingerchuk et a!. proposed the following diagnostic criteria for Devic's neuromyelitis optica (NMO): optic neuritis, acute myelitis, and no symptoms implicating CNS involvement beyond the optic nerves and spinal cord. In addition, fulfillment of one of the following supportive criteria was required: brain MRI nondiagnostic for multiple sclerosis (MS), MRI evidence of a spinal cord lesion extending over at least three vertebral segments, or elevated white blood cell count or neutrophil count in the cerebrospinal fluid. This diagnostic model has limitations, and since its development it has emerged that the serum autoantibody NMO-lgG is highly specific for NMO. OBJECTIVES To evaluate the diagnostic performance of the previously proposed diagnostic criteria for NMO, and to develop a new diagnostic model with improved predictive power. DESIGN AND INTERVENTION The investigators evaluated a cohort of 129 patients (96 NMO, 33 MS) with at least one attack of optic neuritis and myelitis. All patients were treated at a Mayo Clinic MS center in the US during 1999-2005. The diagnosis for NMO or MS was based on the available clinical, imaging and laboratory data and information for the subsequent disease course. Brain MRI scans were assessed using the Paty criteria for MS. In addition, serum samples were tested for NMO-IgG. NMO and MS patients were compared with regard to their frequency of meeting the 1999 diagnostic criteria for NMO. The investigators then constructed new diagnostic models, each including optic neuritis and acute myelitis as essential criteria, and two or three of the most accurate individual diagnostic variables as supportive criteria. OUTCOME MEASURES The sensitivity, specificity, positive likelihood ratio (PLR) and negative likelihood ratio (NLR) of individual and combined diagnostic variables. RESULTS The 1999 criteria were 85% sensitive but only 48% specific for NMO. Fourteen (14.6%) patients who were diagnosed with NMO had neurological symptoms that indicated disease outside the optic nerves and spinal cord. The individual variables that most accurately predicted NMO were NMO-IgG seropositivity (best rule-in criterion) and absence of a long spinal cord lesion (best rule-out criterion). A revised diagnostic model requiring fulfillment of the two MRI criteria had a sensitivity of 94% (95% CI 89-99%), a specificity of 96% (95% CI 89-100%), a PLR of 25.4 (95% CI 3.71-1 74), and an NLR of 0.06 (95% CI 0.03-0.15) for predicting NMO. A model requiring the presence of two out of three supportive criteria—long spinal cord lesion, nondiagnostic brain MRI or NMO-lgG seropositivity—had a sensitivity of 99% (95% CI 97-100%), a specificity of 90% (95% CI 80-100%), a PLR of 10.2 (95% CI 3.49-30.0) and an NLR of 0.01 (95% CI 0.002-0.09) for predicting NMO. CONCLUSION The authors propose a new model for the diagnosis of NMO, requiring the presence of optic neuritis and acute myelitis as well as fulfillment of two of the three following supportive criteria: long spinal cord lesion, nondiagnostic brain MRI and NMO-IgG seropositivity. [ABSTRACT FROM AUTHOR]

Published

2007

37. Knowns and unknowns in the future of multiple sclerosis treatment

Author

Stüve, Olaf

Subjects

*MULTIPLE sclerosis treatment, *INFLAMMATION, *MYELINATION, *NEURODEGENERATION, *AUTOIMMUNITY, *IMMUNOSUPPRESSION, *MONOCLONAL antibodies, *IMMUNOREGULATION

Abstract

Summary: Multiple sclerosis is a chronic disease confined to the central nervous system. Its pathological hallmarks are neuroinflammation, de- and re-myelination, neurodegeneration and astrogliosis. The aetiology of multiple sclerosis is unknown, although a growing body of evidence supports an autoimmune pathogenesis triggered by environmental factors in genetically susceptible individuals. It is therefore perhaps unsurprising that immunomodulatory therapies have now been the mainstay of pharmacotherapy and the focus for the search for a cure for many decades. Currently, clinicians have access to two distinct treatment strategies, namely general immunomodulation or immunosuppression. During the last two decades, several immunomodulatory agents and one immunosuppressant drug have been shown to be effective in clinical trials and have been approved on this basis for the treatment of multiple sclerosis. Current drugs offer well-established safe and effective therapeutic agents for multiple sclerosis in both the short and long term. More recently, growing knowledge of specific anatomical, cellular and molecular targets that play critical roles in the inflammatory cascade of multiple sclerosis have shifted the focus of drug development towards specific targets. Future multiple sclerosis therapies arising from this research may offer better suppression of disease activity, but may be associated with potentially severe side-effects in some patients that may be difficult to manage. In the near future, better understanding of the pathogenesis of multiple sclerosis will probably allow the development of even more effective agents for all clinical phenotypes of the disease. Future therapeutic agents will also have to be designed to address the neurodegenerative component of the physiopathology of multiple sclerosis. [Copyright &y& Elsevier]

Published

2009

38. Mitoxantrone as a potential therapy for primary progressive multiple sclerosis.

Author

Stüve, Olaf, Kita, Mariko, Pelletier, Daniel, Fox, Robert J, Stone, Jerome, Goodkin, Donald E, and Zamvil, Scott S

Abstract

Mitoxantrone (Novantrone®) was the first drug approved in western Europe and North America for treatment of secondary progressive multiple sclerosis (SPMS) and progressive relapsing MS (PRMS). Pharmacological properties of mitoxantrone, its role in SPMS, the study rational and design of an ongoing multi-centre, double blind, randomized, placebo-controlled phase 2 trial will be outlined in this article. Multiple Sclerosis (2004)10, S58-S61 [ABSTRACT FROM PUBLISHER]

Published

2004

39. Mitoxantrone as a potential therapy for primary progressive multiple sclerosis.

Author

Stüve, Olaf, Kita, Mariko, Pelletier, Daniel, Fox, Robert J, Stone, Jerome, Goodkin, Donald E, and Zamvil, Scott S

Abstract

Mitoxantrone (Novantrone®) was the first drug approved in western Europe and North A merica for treatment of secondary progressive multiple sclerosis (SPMS) and progressive relapsing MS (PRMS). Pharmacological properties of mitoxantrone, its role in SPMS, the study rational and design of an ongoing multi-centre, double blind, randomized, placebo -controlled phase 2 trial will be outlined in this article. [ABSTRACT FROM PUBLISHER]

Published

2004

40. Dimethyl Fumarate Delays Multiple Sclerosis in Radiologically Isolated Syndrome.

Author

Okuda, Darin T., Kantarci, Orhun, Lebrun‐Frénay, Christine, Sormani, Maria Pia, Azevedo, Christina J., Bovis, Francesca, Hua, Le H., Amezcua, Lilyana, Mowry, Ellen M., Hotermans, Christophe, Mendoza, Jason, Walsh, John S., von Hehn, Christian, Vargas, Wendy S., Donlon, Stacy, Naismith, Robert T., Okai, Annette, Pardo, Gabriel, Repovic, Pavle, and Stüve, Olaf

Subjects

*DIMETHYL fumarate, *MULTIPLE sclerosis, *CENTRAL nervous system, *CLINICAL trials, *MYELIN sheath diseases, *SYNDROMES

Abstract

Objective: The radiologically isolated syndrome (RIS) represents the earliest detectable pre‐clinical phase of multiple sclerosis (MS). This study evaluated the impact of therapeutic intervention in preventing first symptom manifestation at this stage in the disease spectrum. Methods: We conducted a multi‐center, randomized, double‐blinded, placebo‐controlled study involving people with RIS. Individuals without clinical symptoms typical of MS but with incidental brain MRI anomalies consistent with central nervous system (CNS) demyelination were included. Within 12 MS centers in the United States, participants were randomly assigned 1:1 to oral dimethyl fumarate (DMF) 240 mg twice daily or placebo. The primary endpoint was the time to onset of clinical symptoms attributable to a CNS demyelinating event within a follow‐up period of 96 weeks. An intention‐to‐treat analysis was applied to all participating individuals in the primary and safety investigations. The study is registered at ClinicalTrials.gov, NCT02739542 (ARISE). Results: Participants from 12 centers were recruited from March 9, 2016, to October 31, 2019, with 44 people randomized to dimethyl fumarate and 43 to placebo. Following DMF treatment, the risk of a first clinical demyelinating event during the 96‐week study period was highly reduced in the unadjusted Cox proportional‐hazards regression model (hazard ratio [HR] = 0.18, 95% confidence interval [CI] = 0.05–0.63, p = 0.007). More moderate adverse reactions were present in the DMF (34 [32%]) than placebo groups (19 [21%]) but severe events were similar (DMF, 3 [5%]; placebo, 4 [9%]). Interpretation: This is the first randomized clinical trial demonstrating the benefit of a disease‐modifying therapy in preventing a first acute clinical event in people with RIS. ANN NEUROL 2023;93:604–614 [ABSTRACT FROM AUTHOR]

Published

2023

41. Distinctive transcriptomic and epigenomic signatures of bone marrow-derived myeloid cells and microglia in CNS autoimmunity.

Author

Manouchehri, Navid, Salinas, Victor H., Hussain, Rehana Z., and Stüve, Olaf

Subjects

*MYELOID cells, *MICROGLIA, *AUTOIMMUNITY, *TRANSCRIPTOMES, *CENTRAL nervous system

Abstract

In the context of autoimmunity, myeloid cells of the central nervous system (CNS) constitute an ontogenically heterogeneous population that includes yolk sac-derived microglia and infiltrating bone marrow-derived cells (BMC). We previously identified a myeloid cell subset in the brain and spinal cord that expresses the surface markers CD88 and CD317 and is associated with the onset and persistence of clinical disease in the murine model of the human CNS autoimmune disorder, experimental autoimmune encephalomyelitis (EAE). We employed an experimental platform utilizing single-cell transcriptomic and epigenomic profiling of bone marrow-chimeric mice to categorically distinguish BMC from microglia during CNS autoimmunity. Analysis of gene expression and chromosomal accessibility identified CD88+CD317+ myeloid cells in the CNS of EAE mice as originating from BMC and microglia. Interestingly, each cell lineage exhibited overlapping and unique gene expression patterns and transcription factor motifs that allowed their segregation. Our observations will facilitate determining pathogenic contributions of BMC and microglia in CNS autoimmune disease. Ultimately, this agnostic characterization of myeloid cells will be required for devising disease stage-specific and tissue-specific interventions for CNS inflammatory and neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2023

42. Sodium Phenylbutyrate-Taurursodiol for ALS.

Author

Turnbull, John, Herz, Joachim, Stüve, Olaf, Paganoni, Sabrina, and Cudkowicz, Merit E.

Subjects

*SODIUM, *RNA replicase, *FRONTOTEMPORAL lobar degeneration, *AMYOTROPHIC lateral sclerosis, *CARBOCYCLIC acids

Published

2020

43. Opinion: Statins-a cure-all for the brain?

Author

Menge, Til, Hartung, Hans-Peter, and Stüve, Olaf

Subjects

*STATINS (Cardiovascular agents), *ANTICHOLESTEREMIC agents, *DRUGS, *HYPERCHOLESTEREMIA treatment, *NEUROLOGICAL disorders

Abstract

'Statins' are 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitors-oral cholesterol-lowering drugs that are used to treat hypercholesterolaemia. It is widely accepted that statins have anti-inflammatory effects that are independent of their ability to lower cholesterol. Animal studies and observational clinical studies have indicated that statins might also be effective in treating certain neurological diseases-in particular, multiple sclerosis, Alzheimer's disease and ischaemic stroke. At present, however, results from ongoing prospective, randomized clinical trials are not available. [ABSTRACT FROM AUTHOR]

Published

2005

44. CD11c+CD88+CD317+ myeloid cells are critical mediators of persistent CNS autoimmunity.

Author

Manouchehri, Navid, Hussain, Rehana Z., Cravens, Petra D., Esaulova, Ekaterina, Artyomov, Maxim N., Edelson, Brian T., Wu, Gregory F., Cross, Anne H., Doelger, Richard, Loof, Nicolas, Eagare, Todd N., Forsthuber, Thomas G., Calvier, Laurent, Herzg, Joachim, and Stüve, Olaf

Subjects

*DELAYED onset of disease, *CENTRAL nervous system, *CEREBROSPINAL fluid, *DENDRITIC cells, *AUTOIMMUNITY, *COMMERCIAL products, *MYELOID cells

Abstract

Natalizumab, a humanized monoclonal antibody (mAb) against a4- integrin, reduces the number of dendritic cells (DC) in cerebral perivascular spaces in multiple sclerosis (MS). Selective deletion of a4- integrin in CD11c+ cells should curtail their migration to the central nervous system (CNS) and ameliorate experimental autoimmune encephalomyelitis (EAE). We generated CD11c. Cre+/-ITGA4fl/fl C57BL/6 mice to selectively delete a4-integrin in CD11c+ cells. Active immunization and adoptive transfer EAE models were employed and compared with WT controls. Multiparameter flow cytometry was utilized to immunophenotype leukocyte subsets. Single-cell RNA sequencing was used to profile individual cells. a4-Integrin expression by CD11c+ cells was significantly reduced in primary and secondary lymphoid organs in CD11c.Cre+/-ITGA4fl/fl mice. In active EAE, a delayed disease onset was observed in CD11c.Cre+/-ITGA4fl/fl mice, during which CD11c+CD88+ cells were sequestered in the blood. Upon clinical EAE onset, CD11c+CD88+ cells appeared in the CNS and expressed CD317+. In adoptive transfer experiments, CD11c.Cre+/-ITGA4fl/fl mice had ameliorated clinical disease phenotype associated with significantly diminished numbers of CNS CD11c+CD88+CD317+ cells. In human cerebrospinal fluid from subjects with neuroinflammation, microglia-like cells display coincident expression of ITGAX (CD11c), C5AR1 (CD88), and BST2 (CD317). In mice, we show that only activated, but not naïve microglia expressed CD11c, CD88, and CD317. Finally, anti-CD317 treatment prior to clinical EAE substantially enhanced recovery in mice. [ABSTRACT FROM AUTHOR]

Published

2021

45. The temporal and causal relationship between inflammation and neurodegeneration in multiple sclerosis.

Author

Milo, Ron, Korczyn, Amos D, Manouchehri, Navid, and Stüve, Olaf

Subjects

*MULTIPLE sclerosis, *NEURODEGENERATION, *CENTRAL nervous system, *PATHOLOGY, *INFLAMMATION, *MYELIN sheath diseases

Abstract

It is currently incompletely understood whether inflammation and neurodegeneration are causally related in multiple sclerosis (MS). The sequence of a potential causal relationship is also unknown. Inflammation is present in rather all clinical stages of MS. Its role in the pathogenesis of MS is supported by histopathological analyses, genetic data, and numerous animal models of MS. All approved disease-modifying therapies that reduce clinical relapses and diminish the accumulation of lesions on neuroimaging are anti-inflammatory. Axonal loss and accelerated brain volume loss can also be detected from clinical disease onset throughout all stages. The expression of neurofilament light chain in cerebrospinal fluid and serum, a scaffolding protein in axons and dendrites, is a biomarker of neuronal injury associated with clinical relapses and reflects neuronal loss during episodes of acute inflammation. The recent association of human endogenous retrovirus (HERV) and its envelope proteins with MS illustrates a pathogenic pathway that causally links central nervous system (CNS)–intrinsic proinflammatory effects and inhibition of myelin repair and neuroregeneration. A review of current data on the causal relationship between inflammation and neurodegeneration in MS identified numerous plausible pathomechanisms that link the two events. Observations from most experimental models appear to favor a pathogenesis in which inflammation precedes neurodegeneration. [ABSTRACT FROM AUTHOR]

Published

2020

46. Simplification of combination antiretroviral therapy (cART) and the brain—a real-life experience.

Author

Arendt, Gabriele, Schlonies, Svenja, Orhan, Eser, and Stüve, Olaf

Subjects

*DRUG side effects, *CD4 lymphocyte count, *NEUROPSYCHOLOGICAL tests, *VIRAL load, *BIOMARKERS, *AIDS-related opportunistic infections

Abstract

Modern antiretroviral combination therapy (cART) has transformed HIV from a life-threatening infection into a chronic disease. However, the life-long treatment has side effects that frequently have a negative impact on patients' quality of life. Thus, there are some efforts to "simplify" therapy, i.e. apply regimens with three or fewer antiretroviral substances. However, neurologists are relatively sceptical towards this cART "simplification", because the capacity of simplified regimens to access the cerebrospinal fluid (CSF) might be too weak to effectively suppress viral load in this compartment. Thus, data of a big Neuro-AIDS cohort of 4992 HIV-positive patients consecutively recruited over three decades were retrospectively analysed in terms of neurocognitive performance of patients switched to simplified therapy regimens. To test whether simplified drug regimens result in new neuropsychological deficits or the worsening of pre-existing ones in HIV+ patients. Three groups of HIV+ patients were switched from triple therapy to three different two drug regimens (n = 177 to lamivudine/PI, n = 37 to INI/PI, and n = 303 to dual PI); three other groups of patients put from one to an alternative triple combination (n = 290 ABC/3TC/PI, n = 244 TDF/FTC/PI, and n = 158 TDF/FTC/NNRTI) for whatever reason served as controls. All patients were followed up over 4 years maximum. Every patient group improved immunologically and virologically after the switch. However, patients who switched to INI/PI combinations remained stable in neuropsychological tests, while a considerable percentage of patients who switched to other treatments demonstrated a decline. Remarkably, a high percentage of the patients switched to "simplified drug regimens" was not well-controlled virologically before the switch. HIV-positive patients with simplified therapy regimens show some benefit in terms of systemic infection surrogate markers (CD4 ± cell count and plasma viral load); however, neurocognitive deficits do not improve, but remain stable in most cases. [ABSTRACT FROM AUTHOR]

Published

2019

47. Vestibular hypofunction after monosodium glutamate ingestion: broadening the spectrum of 'Chinese restaurant syndrome'.

Author

Leussink, Verena, Hartung, Hans-Peter, Stüve, Olaf, and Kieseier, Bernd

Subjects

*VERTIGO, *PHYSIOLOGICAL effects of monosodium glutamate

Abstract

A letter to the editor is presented which discusses a case study of a 53-year-old man with vestibular hypofunction, and Chinese restaurant syndrome caused by the ingestion of monosodium glutamate.

Published

2016

48. TLR3 agonism re‐establishes CNS immune competence during α4‐integrin deficiency.

Author

Hussain, Rehana Z., Cravens, Petra C., Doelger, Richard, Dentel, Brianne, Herndon, Emily, Loof, Nicolas, Tsai, Peter, Okuda, Darin T., Racke, Michael K., and Stüve, Olaf

Subjects

*TYPE I interferons, *CENTRAL nervous system, *BLOOD-brain barrier, *SPINAL cord, *NATALIZUMAB

Abstract

Objective: Natalizumab blocks α4‐integrin‐mediated leukocyte migration into the central nervous system (CNS). It diminishes disease activity in multiple sclerosis (MS), but carries a high risk of progressive multifocal encephalopathy (PML), an opportunistic infection with JV virus that may be prompted by diminished CNS immune surveillance. The initial host response to viral infections entails the synthesis of type I interferons (IFN) upon engagement of TLR3 receptors. We hypothesized that TLR3 agonism reestablishes CNS immune competence in the setting of α4‐integrin deficiency. Method: We generated the conditional knock out mouse strain Mx1.Cre+α4‐integrinfl/fl, in which the α4‐integrin gene is ablated upon treatment with the TLR3 agonist poly I:C. Adoptive transfer of purified lymphocytes from poly I:C‐treated Mx1.Cre+α4‐integrinfl/fl donors into naive recipients recapitulates immunosuppression under natalizumab. Active experimental autoimmune encephalomyelitis (EAE) in Mx1.Cre+α4‐integrinfl/fl mice treated with poly I:C represents immune‐reconstitution. Results: Adoptive transfer of T cells from poly I:C treated Mx1.Cre+α4‐integrinfl/fl mice causes minimal EAE. The in vitro migratory capability of CD45+ splenocytes from these mice is reduced. In contrast, actively‐induced EAE after poly I:C treatment results in full disease susceptibility of Mx1.Cre+α4‐integrinfl/fl mice, and the number and composition of CNS leukocytes is similar to controls. Extravasation of Evans Blue indicates a compromised blood‐brain barrier. Poly I:C treatment results in a 2‐fold increase in IFNβ transcription in the spinal cord. Interpretation: Our data suggest that TLR3 agonism in the setting of relative α4‐integrin deficiency can reestablish CNS immune surveillance in an experimental model. This pathway may present a feasible treatment strategy to treat and prevent PML under natalizumab therapy and should be considered for further experimental evaluation in a controlled setting. [ABSTRACT FROM AUTHOR]

Published

2018

49. Laquinimod has no effects on brain volume or cellular CNS composition in the F1 3xTg-AD/C3H mouse model of Alzheimer's disease.

Author

Hussain, Rehana Z., Miller-Little, William A., Lambracht-Washington, Doris, Jaramillo, Tom C., Fu, Min, Powell, Craig M., Rosenberg, Roger N., Stüve, Olaf, Takahashi, Masaya, Zhang, Shanrong, Cutter, Gary R., and Hayardeny, Liat

Subjects

*ALZHEIMER'S disease research, *ANTI-inflammatory agents, *CENTRAL nervous system, *MULTIPLE sclerosis, *BIOAVAILABILITY

Abstract

Background Laquinimod is an anti-inflammatory agent with good central nervous system (CNS) bioavailability, and neuroprotective and myelorestorative properties. A clinical trial in patients with multiple sclerosis demonstrated that laquinimod significantly reduced loss of brain volume. The cellular substrate or molecular events underlying that treatment effect are unknown. In this study, we aimed to explore laquinimod's potential effects on brain volume, animal behavior, cellular numbers and composition of CNS-intrinsic cells and mononuclear cells within the CNS, amyloid beta (Aβ) accumulation and tau phosphorylation in the F1 3xTg-AD/C3H mouse model of Alzheimer's disease. Methods Utilizing a dose response study design, four months old F1 3xTg-AD/C3H mice were treated for 10 months between ages 4 and 14 months with laquinimod (5, 10, or 25 mg/kg), or PBS administered by oral gavage. Brain volumes were measured in a 7 Tesla magnetic resonance imager (MRI) at ages 4 and 14 months. Behavioral testing included locomotor and rearing activity and the Morris water maze task. Cell numbers and immunophenotypes were assessed by multiparameter flow cytometry. Aβ deposition and tau phosphorylation were determined by immunohistochemistry. Results In the F1 3xTg-AD/C3H animal model of AD, there was no detectable reduction of brain volume over a period of 10 months of treatment, as there was not brain atrophy in any of the placebo or treatment groups. Laquinimod had no detectable effects on most neurobehavioral outcomes. The number or composition of CNS intrinsic cells and mononuclear subsets isolated from the CNS were not altered by laquinimod. Conclusion This is the first demonstration that there are no age-associated brain volume changes in the F1 3xTg-AD/C3H mouse model of Alzheimer's disease. Consequently, laquinimod had no effect on that outcome of this study. Most secondary outcomes on the effects of laquinimod on behavior and the number and composition of CNS-intrinsic cells and mononuclear cells within the CNS were also negative. [ABSTRACT FROM AUTHOR]

Published

2017

50. IL-12/IL-23p40 Is Highly Expressed in Secondary Lymphoid Organs and the CNS during All Stages of EAE, but Its Deletion Does Not Affect Disease Perpetuation.

Author

Cravens, Petra D., Hussain, Rehana Z., Miller-Little, William A., Ben, Li-Hong, Segal, Benjamin M., Herndon, Emily, and Stüve, Olaf

Subjects

*INTERLEUKINS, *PROTEIN expression, *DELETION mutation, *HETERODIMERS, *T helper cells, *CELL differentiation

Abstract

Background: Interleukin (IL)-12 and IL-23 are heterodimers that share the p40 subunit, and both cytokines are critical in the differentiation of T helper (Th)1 and Th17 cells, respectively. Th1 and Th17 effector cells have been implicated in the pathogenesis of experimental autoimmune encephalitis (EAE), an animal model of the human central nervous system (CNS) autoimmune demyelinating disorder multiple sclerosis (MS). However, ustekinumab, a monoclonal antibody (mAb) against p40 failed to show efficacy over placebo in a phase II clinical trial in patients with MS. The role of p40 in initial T cell priming and maintenance in secondary lymphoid tissues is not yet well understood. Methods: Active EAE was induced in the B6.129-IL12b strain of p40eYFP reporter mice (yet40 mice), and Th1 and Th17 polarized cells were adoptively transferred into p40-deficient mice. Cellular subsets were phenotyped by multi-parameter flow cytometry, and p40 tissue expression was identified by confocal microscopy. Results: We show that yet40 mice are susceptible to EAE, and that p40 is highly expressed in secondary lymphoid organs and the CNS during all stages of the disease. Interestingly, p40 expression in the recipient is not required for EAE induction after adoptive transfer of activated and differentiated encephalitogenic Th1 and Th17 cells into p40-deficient mice. Peripheral antagonism of T helper cell trophic factors critical for the differentiation and maintenance of Th1 and Th17 cells ameliorates EAE, indicating that p40 may play a critical role in the induction of CNS autoimmunity but not in its perpetuation. Conclusion: Our data may explain why ustekinumab did not ameliorate paraclinical and clinical disease in patients with MS. In patients with already established disease, activated antigen-specific encephalitogenic CD4+ T cells are likely already differentiated, and are not dependent on p40 for maintenance. A clinical trial of longer duration with anti-p40 mAbs or other forms of pharmacological p40 antagonism, or sequential anti-p40 therapy following T cell depletion may show a benefit by affecting de novo generation of autoimmune T cells. [ABSTRACT FROM AUTHOR]

Published

2016