Your search keyword '"Lidia Yshii"' showing total 4 results

1. Immunological Bases of Paraneoplastic Cerebellar Degeneration and Therapeutic Implications

Author

Lidia Yshii, Chloé Bost, and Roland Liblau

Subjects

paraneoplastic cerebellar degeneration, anti-neuronal antibodies, T cell, autoimmunity, immunotherapy, animal model, Immunologic diseases. Allergy, RC581-607

Abstract

Paraneoplastic cerebellar degeneration (PCD) is a rare immune-mediated disease that develops mostly in the setting of neoplasia and offers a unique prospect to explore the interplay between tumor immunity and autoimmunity. In PCD, the deleterious adaptive immune response targets self-antigens aberrantly expressed by tumor cells, mostly gynecological cancers, and physiologically expressed by the Purkinje neurons of the cerebellum. Highly specific anti-neuronal antibodies in the serum and cerebrospinal fluid represent key diagnostic biomarkers of PCD. Some anti-neuronal antibodies such as anti-Yo autoantibodies (recognizing the CDR2/CDR2L proteins) are only associated with PCD. Other anti-neuronal antibodies, such as anti-Hu, anti-Ri, and anti-Ma2, are detected in patients with PCD or other types of paraneoplastic neurological manifestations. Importantly, these autoantibodies cannot transfer disease and evidence for a pathogenic role of autoreactive T cells is accumulating. However, the precise mechanisms responsible for disruption of self-tolerance to neuronal self-antigens in the cancer setting and the pathways involved in pathogenesis within the cerebellum remain to be fully deciphered. Although the occurrence of PCD is rare, the risk for such severe complication may increase with wider use of cancer immunotherapy, notably immune checkpoint blockade. Here, we review recent literature pertaining to the pathophysiology of PCD and propose an immune scheme underlying this disabling disease. Additionally, based on observations from patients' samples and on the pre-clinical model we recently developed, we discuss potential therapeutic strategies that could blunt this cerebellum-specific autoimmune disease.

Published

2020

2. CD4+ and CD8+ T cells are both needed to induce paraneoplastic neurological disease in a mouse model

Author

Christina Gebauer, Béatrice Pignolet, Lidia Yshii, Emilie Mauré, Jan Bauer, and Roland Liblau

Subjects

autoimmunity, central nervous system, paraneoplastic neurological disease, t cells, tumor immunity, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Paraneoplastic neurological disorders (PNDs) are rare human autoimmune diseases that mostly affect the central nervous system (CNS). They are triggered by an efficient immune response against a neural self-antigen that is ectopically expressed in neoplastic tumors. Due to this shared antigenic expression, the immune system reacts not only to tumor cells but also to neural cells resulting in neurological damage. Growing data point to a major role of cell-mediated immunity in PNDs associated to autoantibodies against intracellular proteins. However, its precise contribution in the pathogenesis remains unclear. In this context, our study aimed at investigating the impact of anti-tumor cellular immune responses in the development of PND. To this end, we developed an animal model mimicking PND. We used a tumor cell line expressing the hemagglutinin (HA) of influenza virus to induce an anti-tumor response in CamK-HA mice, which express HA in CNS neurons. To promote and track the T cell response against the HA antigen, naïve HA-specific CD8+ and/or CD4+ T cells, originating from TCR-transgenic animals, were transferred into these mice. We demonstrate that HA-expressing tumors, but not control tumors, induce in vivo activation, proliferation and differentiation of naïve HA-specific CD4+ and CD8+ T cells into effector cells. Moreover, both T cell subsets were needed to control tumor growth and induce CNS inflammation in CamK-HA mice. Thus, this new mouse model provides further insight into the cellular mechanisms whereby a potent anti-tumor immunity triggers a cancer-associated autoimmune disease, and may therefore help to develop new therapeutic strategies against PND.

Published

2017

3. Brain-resident regulatory T cells and their role in health and disease

Author

Adrian Liston, James Dooley, and Lidia Yshii

Subjects

Neuroimmunology, Immunology, Tregs, Autoimmunity, Lymphocyte Activation, T-Lymphocytes, Regulatory, Multiple sclerosis, INFLAMMATION, Immunology and Allergy, Homeostasis, Humans, POPULATION, REQUIRES, REPAIR, Science & Technology, MEMORY, Brain, Forkhead Transcription Factors, Regulatory T cells, Alzheimer's disease, Stroke, B-CELLS, CNS, Life Sciences & Biomedicine, WHITE-MATTER, RESPONSES

Abstract

Regulatory T cells (Tregs) control inflammation and maintain immune homeostasis. The well-characterised circulatory population of CD4+Foxp3+ Tregs is effective at preventing autoimmunity and constraining the immune response, through direct and indirect restraint of conventional T cell activation. Recent advances in Treg cell biology have identified tissue-resident Tregs, with tissue-specific functions that contribute to the maintenance of tissue homeostasis and repair. A population of brain-resident Tregs, characterised as CD69+, has recently been identified in the healthy brain of mice and humans, with rapid population expansion observed under a number of neuroinflammatory conditions. During neuroinflammation, brain-resident Tregs have been proposed to control astrogliosis through the production of amphiregulin, polarize microglia into neuroprotective states, and restrain inflammatory responses by releasing IL-10. While protective effects for Tregs have been demonstrated in a number of neuroinflammatory pathologies, a clear demarcation between the role of circulatory and brain-resident Tregs has been difficult to achieve. Here we review the state-of-the-art for brain-resident Treg population, and describe their potential utilization as a therapeutic target across different neuroinflammatory conditions. ispartof: IMMUNOLOGY LETTERS vol:248 pages:26-30 ispartof: location:Netherlands status: published

Published

2022

4. CD8

Author

Catharina C, Gross, Céline, Meyer, Urvashi, Bhatia, Lidia, Yshii, Ilka, Kleffner, Jan, Bauer, Anna R, Tröscher, Andreas, Schulte-Mecklenbeck, Sebastian, Herich, Tilman, Schneider-Hohendorf, Henrike, Plate, Tanja, Kuhlmann, Markus, Schwaninger, Wolfgang, Brück, Marc, Pawlitzki, David-Axel, Laplaud, Delphine, Loussouarn, John, Parratt, Michael, Barnett, Michael E, Buckland, Todd A, Hardy, Stephen W, Reddel, Marius, Ringelstein, Jan, Dörr, Brigitte, Wildemann, Markus, Kraemer, Hans, Lassmann, Romana, Höftberger, Eduardo, Beltrán, Klaus, Dornmair, Nicholas, Schwab, Luisa, Klotz, Sven G, Meuth, Guillaume, Martin-Blondel, Heinz, Wiendl, and Roland, Liblau

Subjects

Adult, Central Nervous System, Male, Susac Syndrome, Integrin alpha4, Natalizumab, Neuroimmunology, Mice, Transgenic, Autoimmunity, Middle Aged, Article, Disease Models, Animal, Young Adult, Microvessels, Cell Adhesion, Animals, Humans, Female, Endothelium, Vascular, T-Lymphocytes, Cytotoxic

Abstract

Neuroinflammation is often associated with blood-brain-barrier dysfunction, which contributes to neurological tissue damage. Here, we reveal the pathophysiology of Susac syndrome (SuS), an enigmatic neuroinflammatory disease with central nervous system (CNS) endotheliopathy. By investigating immune cells from the blood, cerebrospinal fluid, and CNS of SuS patients, we demonstrate oligoclonal expansion of terminally differentiated activated cytotoxic CD8+ T cells (CTLs). Neuropathological data derived from both SuS patients and a newly-developed transgenic mouse model recapitulating the disease indicate that CTLs adhere to CNS microvessels in distinct areas and polarize granzyme B, which most likely results in the observed endothelial cell injury and microhemorrhages. Blocking T-cell adhesion by anti-α4 integrin-intervention ameliorates the disease in the preclinical model. Similarly, disease severity decreases in four SuS patients treated with natalizumab along with other therapy. Our study identifies CD8+ T-cell-mediated endotheliopathy as a key disease mechanism in SuS and highlights therapeutic opportunities., Susac syndrome is an inflammatory pathology of the brain endothelium. Here the authors show that the pathology is driven by CD8 T cells attacking the endothelium, and that blocking T cell-endothelial adhesion ameliorates the disease in a mouse model, and associates with improved clinical score in 4 patients.

Published

2019