Your search keyword '"Stüve, Olaf"' showing total 7 results

1. A Single Amino Acid Substitution Prevents Recognition of a Dominant Human Aquaporin-4 Determinant in the Context of HLA-DRB1*03:01 by a Murine TCR.

Author

Arellano, Benjamine, Arellano, Benjamine, Hussain, Rehana, Miller-Little, William A, Herndon, Emily, Lambracht-Washington, Doris, Eagar, Todd N, Lewis, Robert, Healey, Don, Vernino, Steven, Greenberg, Benjamin M, Stüve, Olaf, Arellano, Benjamine, Arellano, Benjamine, Hussain, Rehana, Miller-Little, William A, Herndon, Emily, Lambracht-Washington, Doris, Eagar, Todd N, Lewis, Robert, Healey, Don, Vernino, Steven, Greenberg, Benjamin M, and Stüve, Olaf

Abstract

BackgroundAquaporin 4 (AQP4) is considered a putative autoantigen in patients with Neuromyelitis optica (NMO), an autoinflammatory disorder of the central nervous system (CNS). HLA haplotype analyses of patients with NMO suggest a positive association with HLA-DRB1* 03:01. We previously showed that the human (h) AQP4 peptide 281-300 is the dominant immunogenic determinant of hAQP4 in the context of HLA-DRB1*03:01. This immunogenic peptide stimulates a strong Th1 and Th17 immune response. AQP4281-300-specific encephalitogenic CD4+ T cells should initiate CNS inflammation that results in a clinical phenotype in HLA-DRB1*03:01 transgenic mice.MethodsControlled study with humanized experimental animals. HLA-DRB1*03:01 transgenic mice were immunized with hAQP4281-300, or whole-length hAQP4 protein emulsified in complete Freund's adjuvant. Humoral immune responses to both antigens were assessed longitudinally. In vivo T cell frequencies were assessed by tetramer staining. Mice were followed clinically, and the anterior visual pathway was tested by pupillometry. CNS tissue was examined histologically post-mortem. Flow cytometry was utilized for MHC binding assays and to immunophenotype T cells, and T cell frequencies were determined by ELISpot assay.ResultsImmunization with hAQP4281-300 resulted in an in vivo expansion of antigen-specific CD4+ T cells, and an immunoglobulin isotype switch. HLA-DRB1*03:01 TG mice actively immunized with hAQP4281-300, or with whole-length hAQP4 protein were resistant to developing a neurological disease that resembles NMO. Experimental mice show no histological evidence of CNS inflammation, nor change in pupillary responses. Subsequent analysis reveals that a single amino acid substitution from aspartic acid in hAQP4 to glutamic acid in murine (m)AQP4 at position 290 prevents the recognition of hAQP4281-300 by the murine T cell receptor (TCR).ConclusionInduction of a CNS inflammatory autoimmune disorder by active immunization of HLA-DRB1*03

Published

2016

2. A Single Amino Acid Substitution Prevents Recognition of a Dominant Human Aquaporin-4 Determinant in the Context of HLA-DRB1*03:01 by a Murine TCR.

Author

Arellano, Benjamine, Bradl, Monika1, Arellano, Benjamine, Hussain, Rehana, Miller-Little, William A, Herndon, Emily, Lambracht-Washington, Doris, Eagar, Todd N, Lewis, Robert, Healey, Don, Vernino, Steven, Greenberg, Benjamin M, Stüve, Olaf, Arellano, Benjamine, Bradl, Monika1, Arellano, Benjamine, Hussain, Rehana, Miller-Little, William A, Herndon, Emily, Lambracht-Washington, Doris, Eagar, Todd N, Lewis, Robert, Healey, Don, Vernino, Steven, Greenberg, Benjamin M, and Stüve, Olaf

Abstract

BackgroundAquaporin 4 (AQP4) is considered a putative autoantigen in patients with Neuromyelitis optica (NMO), an autoinflammatory disorder of the central nervous system (CNS). HLA haplotype analyses of patients with NMO suggest a positive association with HLA-DRB1* 03:01. We previously showed that the human (h) AQP4 peptide 281-300 is the dominant immunogenic determinant of hAQP4 in the context of HLA-DRB1*03:01. This immunogenic peptide stimulates a strong Th1 and Th17 immune response. AQP4281-300-specific encephalitogenic CD4+ T cells should initiate CNS inflammation that results in a clinical phenotype in HLA-DRB1*03:01 transgenic mice.MethodsControlled study with humanized experimental animals. HLA-DRB1*03:01 transgenic mice were immunized with hAQP4281-300, or whole-length hAQP4 protein emulsified in complete Freund's adjuvant. Humoral immune responses to both antigens were assessed longitudinally. In vivo T cell frequencies were assessed by tetramer staining. Mice were followed clinically, and the anterior visual pathway was tested by pupillometry. CNS tissue was examined histologically post-mortem. Flow cytometry was utilized for MHC binding assays and to immunophenotype T cells, and T cell frequencies were determined by ELISpot assay.ResultsImmunization with hAQP4281-300 resulted in an in vivo expansion of antigen-specific CD4+ T cells, and an immunoglobulin isotype switch. HLA-DRB1*03:01 TG mice actively immunized with hAQP4281-300, or with whole-length hAQP4 protein were resistant to developing a neurological disease that resembles NMO. Experimental mice show no histological evidence of CNS inflammation, nor change in pupillary responses. Subsequent analysis reveals that a single amino acid substitution from aspartic acid in hAQP4 to glutamic acid in murine (m)AQP4 at position 290 prevents the recognition of hAQP4281-300 by the murine T cell receptor (TCR).ConclusionInduction of a CNS inflammatory autoimmune disorder by active immunization of HLA-DRB1*03

Published

2016

3. Use of Advanced Magnetic Resonance Imaging Techniques in Neuromyelitis Optica Spectrum Disorder.

Author

Kremer, Stephane, Kremer, Stephane, Renard, Felix, Achard, Sophie, Lana-Peixoto, Marco A, Palace, Jacqueline, Asgari, Nasrin, Klawiter, Eric C, Tenembaum, Silvia N, Banwell, Brenda, Greenberg, Benjamin M, Bennett, Jeffrey L, Levy, Michael, Villoslada, Pablo, Saiz, Albert, Fujihara, Kazuo, Chan, Koon Ho, Schippling, Sven, Paul, Friedemann, Kim, Ho Jin, de Seze, Jerome, Wuerfel, Jens T, Guthy-Jackson Charitable Foundation (GJCF) Neuromyelitis Optica (NMO) International Clinical Consortium and Biorepository, Cabre, Philippe, Marignier, Romain, Tedder, Thomas, van Pelt, Danielle, Broadley, Simon, Chitnis, Tanuja, Wingerchuk, Dean, Pandit, Lekha, Leite, Maria Isabel, Apiwattanakul, Metha, Kleiter, Ingo, Prayoonwiwat, Naraporn, Han, May, Hellwig, Kerstin, van Herle, Katja, John, Gareth, Hooper, D Craig, Nakashima, Ichiro, Sato, Douglas, Yeaman, Michael R, Waubant, Emmanuelle, Zamvil, Scott, Stüve, Olaf, Aktas, Orhan, Smith, Terry J, Jacob, Anu, O'Connor, Kevin, Kremer, Stephane, Kremer, Stephane, Renard, Felix, Achard, Sophie, Lana-Peixoto, Marco A, Palace, Jacqueline, Asgari, Nasrin, Klawiter, Eric C, Tenembaum, Silvia N, Banwell, Brenda, Greenberg, Benjamin M, Bennett, Jeffrey L, Levy, Michael, Villoslada, Pablo, Saiz, Albert, Fujihara, Kazuo, Chan, Koon Ho, Schippling, Sven, Paul, Friedemann, Kim, Ho Jin, de Seze, Jerome, Wuerfel, Jens T, Guthy-Jackson Charitable Foundation (GJCF) Neuromyelitis Optica (NMO) International Clinical Consortium and Biorepository, Cabre, Philippe, Marignier, Romain, Tedder, Thomas, van Pelt, Danielle, Broadley, Simon, Chitnis, Tanuja, Wingerchuk, Dean, Pandit, Lekha, Leite, Maria Isabel, Apiwattanakul, Metha, Kleiter, Ingo, Prayoonwiwat, Naraporn, Han, May, Hellwig, Kerstin, van Herle, Katja, John, Gareth, Hooper, D Craig, Nakashima, Ichiro, Sato, Douglas, Yeaman, Michael R, Waubant, Emmanuelle, Zamvil, Scott, Stüve, Olaf, Aktas, Orhan, Smith, Terry J, Jacob, Anu, and O'Connor, Kevin

Abstract

Brain parenchymal lesions are frequently observed on conventional magnetic resonance imaging (MRI) scans of patients with neuromyelitis optica (NMO) spectrum disorder, but the specific morphological and temporal patterns distinguishing them unequivocally from lesions caused by other disorders have not been identified. This literature review summarizes the literature on advanced quantitative imaging measures reported for patients with NMO spectrum disorder, including proton MR spectroscopy, diffusion tensor imaging, magnetization transfer imaging, quantitative MR volumetry, and ultrahigh-field strength MRI. It was undertaken to consider the advanced MRI techniques used for patients with NMO by different specialists in the field. Although quantitative measures such as proton MR spectroscopy or magnetization transfer imaging have not reproducibly revealed diffuse brain injury, preliminary data from diffusion-weighted imaging and brain tissue volumetry indicate greater white matter than gray matter degradation. These findings could be confirmed by ultrahigh-field MRI. The use of nonconventional MRI techniques may further our understanding of the pathogenic processes in NMO spectrum disorders and may help us identify the distinct radiographic features corresponding to specific phenotypic manifestations of this disease.

Published

2015

4. High-dose immunosuppressive therapy and autologous hematopoietic cell transplantation for relapsing-remitting multiple sclerosis (HALT-MS): a 3-year interim report.

Author

Nash, Richard A, Nash, Richard A, Hutton, George J, Racke, Michael K, Popat, Uday, Devine, Steven M, Griffith, Linda M, Muraro, Paolo A, Openshaw, Harry, Sayre, Peter H, Stüve, Olaf, Arnold, Douglas L, Spychala, Meagan E, McConville, Kaitlyn C, Harris, Kristina M, Phippard, Deborah, Georges, George E, Wundes, Annette, Kraft, George H, Bowen, James D, Nash, Richard A, Nash, Richard A, Hutton, George J, Racke, Michael K, Popat, Uday, Devine, Steven M, Griffith, Linda M, Muraro, Paolo A, Openshaw, Harry, Sayre, Peter H, Stüve, Olaf, Arnold, Douglas L, Spychala, Meagan E, McConville, Kaitlyn C, Harris, Kristina M, Phippard, Deborah, Georges, George E, Wundes, Annette, Kraft, George H, and Bowen, James D

Abstract

ImportanceMost patients with relapsing-remitting (RR) multiple sclerosis (MS) who receive approved disease-modifying therapies experience breakthrough disease and accumulate neurologic disability. High-dose immunosuppressive therapy (HDIT) with autologous hematopoietic cell transplant (HCT) may, in contrast, induce sustained remissions in early MS.ObjectiveTo evaluate the safety, efficacy, and durability of MS disease stabilization through 3 years after HDIT/HCT.Design, setting, and participantsHematopoietic Cell Transplantation for Relapsing-Remitting Multiple Sclerosis (HALT-MS) is an ongoing, multicenter, single-arm, phase 2 clinical trial of HDIT/HCT for patients with RRMS who experienced relapses with loss of neurologic function while receiving disease-modifying therapies during the 18 months before enrolling. Participants are evaluated through 5 years after HCT. This report is a prespecified, 3-year interim analysis of the trial. Thirty-six patients with RRMS from referral centers were screened; 25 were enrolled.InterventionsAutologous peripheral blood stem cell grafts were CD34+ selected; the participants then received high-dose treatment with carmustine, etoposide, cytarabine, and melphalan as well as rabbit antithymocyte globulin before autologous HCT.Main outcomes and measuresThe primary end point of HALT-MS is event-free survival defined as survival without death or disease activity from any one of the following outcomes: (1) confirmed loss of neurologic function, (2) clinical relapse, or (3) new lesions observed on magnetic resonance imaging. Toxic effects are reported using National Cancer Institute Common Terminology Criteria for Adverse Events.ResultsGrafts were collected from 25 patients, and 24 of these individuals received HDIT/HCT. The median follow-up period was 186 weeks (interquartile range, 176-250) weeks). Overall event-free survival was 78.4% (90% CI, 60.1%-89.0%) at 3 years. Progression-free survival and clinical relapse-free survival were

Published

2015

5. Defining the clinical course of multiple sclerosis:The 2013 revisions

Author

Lublin, Fred D, Reingold, Stephen C, Cohen, Jeffrey A, Cutter, Gary R, Sørensen, Per Soelberg, Thompson, Alan J, Wolinsky, Jerry S, Balcer, Laura J, Banwell, Brenda, Barkhof, Frederik, Bebo, Bruce, Calabresi, Peter A, Clanet, Michel, Comi, Giancarlo, Fox, Robert J, Freedman, Mark S, Goodman, Andrew D, Inglese, Matilde, Kappos, Ludwig, Kieseier, Bernd C, Lincoln, John A, Lubetzki, Catherine, Miller, Aaron E, Montalban, Xavier, O'Connor, Paul W, Petkau, John, Pozzilli, Carlo, Rudick, Richard A, Sormani, Maria Pia, Stüve, Olaf, Waubant, Emmanuelle, Polman, Chris H, Lublin, Fred D, Reingold, Stephen C, Cohen, Jeffrey A, Cutter, Gary R, Sørensen, Per Soelberg, Thompson, Alan J, Wolinsky, Jerry S, Balcer, Laura J, Banwell, Brenda, Barkhof, Frederik, Bebo, Bruce, Calabresi, Peter A, Clanet, Michel, Comi, Giancarlo, Fox, Robert J, Freedman, Mark S, Goodman, Andrew D, Inglese, Matilde, Kappos, Ludwig, Kieseier, Bernd C, Lincoln, John A, Lubetzki, Catherine, Miller, Aaron E, Montalban, Xavier, O'Connor, Paul W, Petkau, John, Pozzilli, Carlo, Rudick, Richard A, Sormani, Maria Pia, Stüve, Olaf, Waubant, Emmanuelle, and Polman, Chris H

Abstract

Accurate clinical course descriptions (phenotypes) of multiple sclerosis (MS) are important for communication, prognostication, design and recruitment of clinical trials, and treatment decision-making. Standardized descriptions published in 1996 based on a survey of international MS experts provided purely clinical phenotypes based on data and consensus at that time, but imaging and biological correlates were lacking. Increased understanding of MS and its pathology, coupled with general concern that the original descriptors may not adequately reflect more recently identified clinical aspects of the disease, prompted a re-examination of MS disease phenotypes by the International Advisory Committee on Clinical Trials of MS. While imaging and biological markers that might provide objective criteria for separating clinical phenotypes are lacking, we propose refined descriptors that include consideration of disease activity (based on clinical relapse rate and imaging findings) and disease progression. Strategies for future research to better define phenotypes are also outlined.

Published

2014

6. Defining the clinical course of multiple sclerosis:The 2013 revisions

Author

Lublin, Fred D, Reingold, Stephen C, Cohen, Jeffrey A, Cutter, Gary R, Sørensen, Per Soelberg, Thompson, Alan J, Wolinsky, Jerry S, Balcer, Laura J, Banwell, Brenda, Barkhof, Frederik, Bebo, Bruce, Calabresi, Peter A, Clanet, Michel, Comi, Giancarlo, Fox, Robert J, Freedman, Mark S, Goodman, Andrew D, Inglese, Matilde, Kappos, Ludwig, Kieseier, Bernd C, Lincoln, John A, Lubetzki, Catherine, Miller, Aaron E, Montalban, Xavier, O'Connor, Paul W, Petkau, John, Pozzilli, Carlo, Rudick, Richard A, Sormani, Maria Pia, Stüve, Olaf, Waubant, Emmanuelle, Polman, Chris H, Lublin, Fred D, Reingold, Stephen C, Cohen, Jeffrey A, Cutter, Gary R, Sørensen, Per Soelberg, Thompson, Alan J, Wolinsky, Jerry S, Balcer, Laura J, Banwell, Brenda, Barkhof, Frederik, Bebo, Bruce, Calabresi, Peter A, Clanet, Michel, Comi, Giancarlo, Fox, Robert J, Freedman, Mark S, Goodman, Andrew D, Inglese, Matilde, Kappos, Ludwig, Kieseier, Bernd C, Lincoln, John A, Lubetzki, Catherine, Miller, Aaron E, Montalban, Xavier, O'Connor, Paul W, Petkau, John, Pozzilli, Carlo, Rudick, Richard A, Sormani, Maria Pia, Stüve, Olaf, Waubant, Emmanuelle, and Polman, Chris H

Abstract

Accurate clinical course descriptions (phenotypes) of multiple sclerosis (MS) are important for communication, prognostication, design and recruitment of clinical trials, and treatment decision-making. Standardized descriptions published in 1996 based on a survey of international MS experts provided purely clinical phenotypes based on data and consensus at that time, but imaging and biological correlates were lacking. Increased understanding of MS and its pathology, coupled with general concern that the original descriptors may not adequately reflect more recently identified clinical aspects of the disease, prompted a re-examination of MS disease phenotypes by the International Advisory Committee on Clinical Trials of MS. While imaging and biological markers that might provide objective criteria for separating clinical phenotypes are lacking, we propose refined descriptors that include consideration of disease activity (based on clinical relapse rate and imaging findings) and disease progression. Strategies for future research to better define phenotypes are also outlined.

Published

2014

7. Developmental maturation of innate immune cell function correlates with susceptibility to central nervous system autoimmunity.

Author

Hertzenberg, Deetje, Hertzenberg, Deetje, Lehmann-Horn, Klaus, Kinzel, Silke, Husterer, Veronika, Cravens, Petra D, Kieseier, Bernd C, Hemmer, Bernhard, Brück, Wolfgang, Zamvil, Scott S, Stüve, Olaf, Weber, Martin S, Hertzenberg, Deetje, Hertzenberg, Deetje, Lehmann-Horn, Klaus, Kinzel, Silke, Husterer, Veronika, Cravens, Petra D, Kieseier, Bernd C, Hemmer, Bernhard, Brück, Wolfgang, Zamvil, Scott S, Stüve, Olaf, and Weber, Martin S

Abstract

MS is an inflammatory CNS disorder, which typically occurs in early adulthood and rarely in children. Here we tested whether functional maturation of innate immune cells may determine susceptibility to CNS autoimmune disease in EAE. Two-week-old mice were resistant to active EAE, which causes fulminant paralysis in adult mice; this resistance was associated with an impaired development of Th1 and Th17 cells. Resistant, young mice had higher frequencies of myeloid-derived suppressor cells and plasma-cytoid DCs. Furthermore, myeloid APCs and B cells from young mice expressed lower levels of MHC class II and CD40, produced decreased amounts of proinflammatory cytokines, and released enhanced levels of anti-inflammatory IL-10. When used as APCs, splenocytes from 2-week-old mice failed to differentiate naive T cells into Th1 and Th17 cells irrespective of the T-cell donor's age, and promoted development of Treg cells and Th2 cells instead. Adoptive transfer of adult APCs restored the ability of 2-week-old mice to generate encephalitogenic T cells and develop EAE. Collectively, these findings indicate that the innate immune compartment functionally matures during development, which may be a prerequisite for development of T-cell-mediated CNS autoimmune disease.

Published

2013