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1. Risk score for non-small cell lung cancer patients starting checkpoint inhibitor treatment

Author

Diem S, Fässler M, Hasan Ali O, Siano M, Niederer R, Berner F, Roux GA, Ackermann CJ, Schmid S, Güsewell S, Früh M, and Flatz L

Subjects
NSCLC, checkpoint inhibitor, biomarkers, risk score, response, survival, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Stefan Diem,1–3,* Mirjam Fässler,2,* Omar Hasan Ali,2,4 Marco Siano,1 Rebekka Niederer,2 Fiamma Berner,2 Guillaume-Alexandre Roux,2 Christoph Jakob Ackermann,1 Sabine Schmid,1 Sabine Güsewell,5 Martin Früh,1,6 Lukas Flatz1,2,4,7 1Department of Oncology/Haematology, Kantonsspital St. Gallen, St. Gallen, Switzerland; 2Department of Immunobiology, Kantonsspital St. Gallen, St. Gallen, Switzerland; 3Department of Oncology/Haematology, Spital Grabs, St. Gallen, Switzerland; 4Department of Dermatology, University Hospital Zürich, Zürich, Switzerland; 5Clinical Trial Unit, Kantonsspital St. Gallen, St. Gallen, Switzerland; 6University of Bern, Bern, Switzerland; 7Department of Dermatology/Allergology, Kantonsspital St. Gallen, St. Gallen, Switzerland *These authors contributed equally to this work Background: Prognosis of metastatic non-small cell lung cancer significantly improved with the availability of checkpoint inhibitors (anti-PD-1/PD-L1). Unfortunately, reliable biomarkers to predict treatment benefit are lacking.Patients and methods: We prospectively collected clinical and laboratory data of 56 non-small cell lung cancer patients treated with a checkpoint inhibitor. The aim was to identify baseline parameters correlating with worse outcome and to create a risk score that enabled to stratify patients into different risk groups. As inflammation is known to promote tumor growth, we focused on inflammation markers in the blood. Disease control (DC) was defined as complete response, partial response, and stable disease on CT scan according to RECIST 1.1.Results: Half of the patients achieved DC. Four parameters differed significantly between the DC group and the no disease control group: Eastern Cooperative Oncology Group performance status (P=0.009), number of organs with metastases (P=0.001), lactate dehydrogenase (P=0.029), and ferritin (P=0.005). A risk score defined as the number of these parameters (0= no risk factor) exceeding a threshold (Eastern Cooperative Oncology Group performance status ≥2, number of organs with metastases ≥4, lactate dehydrogenase ≥262U/L, and ferritin ≥241 µg/L) was associated with overall survival and progression-free survival. Overall survival at 6 and 12 months is as follows: Scores 0–1: 95% and 95%; Score 2: 67% and ≤33%; Scores 3–4: 15% and 0%. Progression-free survival at 6 and 12 months is as follows: Scores 0–1: 81% and 50%; Score 2: 25% and ≤25%; Scores 3–4: 0% and 0%.Conclusion: We propose an easy-to-apply risk score categorizing patients into different risk groups before treatment start with a PD-1/PD-L1 antibody. Keywords: NSCLC, checkpoint inhibitor, biomarkers, risk score, response, survival

Published
2018

3. Role of T-cell-mediated inflammation in psoriasis: pathogenesis and targeted therapy

Author

Flatz L and Conrad C

Subjects
Dermatology, RL1-803
Abstract

Lukas Flatz, Curdin ConradDepartment of Dermatology, University Hospital of Lausanne (CHUV), Lausanne, SwitzerlandAbstract: Psoriasis is one of the most common chronic, inflammatory, T-cell-mediated autoimmune diseases. Over the past decade, increased knowledge of disease pathogenesis has fundamentally changed psoriasis treatment, with the introduction of biologics, and this has led to a multitude of improved selective targets providing potential therapeutic options. Indeed, numerous pathogenesis-based treatments are currently in development, as psoriasis has also become increasingly relevant for proof-of-concept studies. The purpose of this review was to summarize current knowledge of psoriasis immunopathogenesis, focusing on the T-cell-mediated immune response and its initiation. The authors describe recent advances in psoriasis treatment and discuss pathogenesis-based therapies that are currently in development or which could be envisioned for the future. Although current biologics are well tolerated, several issues such as long-term efficacy, long-term safety, and high costs keep driving the search for new and better therapies. With further advances in understanding disease pathogenesis, more genomic data from psoriasis patients becoming available, and potentially the identification of autoantigens in psoriasis, current research should lead to the development of a growing arsenal of improved targeted treatments and to further breakthrough immunotherapies.Keywords: autoimmunity, autoimmune disease, immune response, immunopathogenesis

Published
2013

4. Nomogram for predicting survival after first-line anti-PD-1-based immunotherapy in unresectable stage IV melanoma: a multicenter international study

Author

Chatziioannou, E., Higuita, L.M. Serna, Kreft, S., Kandolf, L., Dujovic, B., Reinhardt, L., Tamara, E., Marquez-Rodas, I., Fortuna, A.R.F.P., Nübling, A., Niessner, H., Forschner, A., Garbe, C., Popovic, A., Mirjana, B., Meier, F., Eigentler, T., Leiter, U., Flatz, L., Sinnberg, T., and Amaral, T.

Published
2024
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5. The KEYNOTE-630 Trial: A Phase 3 Study of Adjuvant Pembrolizumab in High-Risk Locally Advanced (LA) Cutaneous Squamous Cell Carcinoma (cSCC)

Author

Schenker, M., primary, Klochikhin, M., additional, Kirtbaya, D., additional, Mortier, L., additional, Gschnell, M., additional, Robert, C., additional, Meyer, N., additional, Flatz, L., additional, Dalle, S., additional, Beylot-Barry, M., additional, Eigentler, T., additional, Silverman, R. Kloss, additional, Gumuscu, B., additional, Yuan, J., additional, and Bratland, A., additional

Published
2024
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6. Identification of patients at high risk for relapse by Merlin Assay (CP-GEP) in an independent cohort of patients with melanoma who did not undergo sentinel lymph node biopsy: head and neck subgroup analysis

Author

Amaral, T., primary, Chatziioannou, E., additional, Nuebling, A., additional, Sinnberg, T., additional, Niessner, H., additional, Leiter, U., additional, Dwarkasing, J., additional, Arentsen, T., additional, Groß, C., additional, Eggermont, A., additional, Flatz, L., additional, and Forchhammer, S., additional

Published
2024
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8. STING activation of tumor endothelial cells initiates spontaneous and therapeutic antitumor immunity

Author

Demaria, O, De Gassart, A, Coso, S, Gestermann, N, Di Domizio, J, Flatz, L, Gaide, O, Michielin, O, Hwu, P, Petrova, TV, Martinon, F, Modlin, RL, Speiser, DE, and Gilliet, M

Abstract

Spontaneous CD8 T-cell responses occur in growing tumors but are usually poorly effective. Understanding the molecular and cellular mechanisms that drive these responses is of major interest as they could be exploited to generate a more efficacious antitumor immunity. As such, stimulator of IFN genes (STING), an adaptor molecule involved in cytosolic DNA sensing, is required for the induction of antitumor CD8 T responses in mouse models of cancer. Here, we find that enforced activation of STING by intratumoral injection of cyclic dinucleotide GMP-AMP (cGAMP), potently enhanced antitumor CD8 T responses leading to growth control of injected and contralateral tumors in mouse models of melanoma and colon cancer. The ability of cGAMP to trigger antitumor immunity was further enhanced by the blockade of both PD1 and CTLA4. The STING-dependent antitumor immunity, either induced spontaneously in growing tumors or induced by intratumoral cGAMP injection was dependent on type I IFNs produced in the tumor microenvironment. In response to cGAMP injection, both in the mouse melanoma model and an ex vivo model of cultured human melanoma explants, the principal source of type I IFN was not dendritic cells, but instead endothelial cells. Similarly, endothelial cells but not dendritic cells were found to be the principal source of spontaneously induced type I IFNs in growing tumors. These data identify an unexpected role of the tumor vasculature in the initiation of CD8 T-cell antitumor immunity and demonstrate that tumor endothelial cells can be targeted for immunotherapy of melanoma.

Published
2015

10. 170 A shared set of autoantigens is recognized in anti-tumor immunity and autoimmune diseases of the skin

Author

Walter, V., primary, Balciunaite, B., additional, Thomä, S., additional, Hofmeister, S., additional, Mroz, G., additional, Wolfsperger, F., additional, Knoll, M., additional, Amaral, T., additional, Leiter-Stöppke, U., additional, Aebischer, V., additional, Forchhammer, S., additional, Schaller, M., additional, and Flatz, L., additional

Published
2023
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12. The impact of the COVID-19 pandemic on the diagnosis of cutaneous melanomas: A retrospective cohort study from five European skin cancer reference centres

Author

Troesch, A., Magdalena, H., Forchhammer, S., Delregno, L., Lodde, G., Turko, P., Cheng, P. F., Levesque, M. L., Hadaschik, E., Livingstone, E., Peris, Ketty, Flatz, L., Peter, K., Dummer, R., Dimitriou, F., Peris K. (ORCID:0000-0002-5237-0463), Troesch, A., Magdalena, H., Forchhammer, S., Delregno, L., Lodde, G., Turko, P., Cheng, P. F., Levesque, M. L., Hadaschik, E., Livingstone, E., Peris, Ketty, Flatz, L., Peter, K., Dummer, R., Dimitriou, F., and Peris K. (ORCID:0000-0002-5237-0463)

Abstract

Background: The COVID-19 lockdown had a dramatic impact on primary care access and resulted in postponed skin cancer screenings. This raises concerns for a diagnostic delay on primary cutaneous melanomas, which can subsequently increase morbidity and mortality. Objectives: The aim of the study was to investigate the impact of the COVID-19-related restrictions on the melanoma diagnosis in five European skin cancer reference centres in Switzerland, Germany, Austria and Italy. Methods: A total of 7865 cutaneous melanoma cases were collected between 01 September 2018 and 31 August 2021. The time period was stratified into pre-COVID (pre-lockdown) and post-COVID (lockdown and post-lockdown) according to the established restrictions in each country. The data collection included demographic, clinical and histopathological data from histologically confirmed cutaneous melanomas. Personal and family history of melanoma, and presence of immunosuppression were used to assess the diagnosis delay in high-risk individuals. Results: There was an overall increase of the Breslow tumour thickness (mean 1.25 mm vs. 1.02 mm) during the post-COVID period, as well as an increase in the proportion of T3-T4 melanomas, rates of ulceration and the number of mitotic rates ≥2 (all, p < 0.001). Patients with immunosuppression and personal history of melanoma showed a decrease in the mean log10-transformed Breslow during lockdown and post-COVID. In the multivariate analysis, age at melanoma diagnosis (p < 0.01) and personal history of melanoma (p < 0.01) showed significant differences in the mean Breslow thickness. Conclusions: The study confirms the diagnostic delay in cutaneous melanomas due to the COVID-19 lockdown. High-risk individuals, such as patients with personal history of melanoma and elderly individuals, were more hesitant to restart their regular skin cancer screenings post-COVID. Further studies with longer follow-up are required to evaluate the consequences of this diagnos

Published
2023

16. 194P Thermal ablation followed by intratumoral injection of a novel immune stimulant IP-001 in patients with advanced solid tumors: Phase IB part of study SAKK 66/17

Author

Joerger, M., primary, Knüsel, P., additional, Alejandre-Lafont, E., additional, Metaxas, Y., additional, Mark, M.T., additional, von Moos, R.A.F., additional, Gysel, K., additional, Eckhardt, K., additional, Glaus Garzon, J., additional, Koster, K-L., additional, Wittwer, Y., additional, Tissot, S., additional, Flatz, L., additional, Alleruzzo, L., additional, Lam, S.K., additional, Anderson, D., additional, Chen, W., additional, Baskin-Bey, E., additional, and Hode, T., additional

Published
2022
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17. 814P Phase II study of cemiplimab in patients with advanced cutaneous squamous cell carcinoma (CSCC): Final analysis from EMPOWER-CSCC-1 groups 1, 2 and 3

Author

Migden, M.R., primary, Schmults, C., additional, Khushanlani, N., additional, Guminski, A., additional, Chang, A.L., additional, Lewis, K., additional, Ansstas, G., additional, Bowyer, S.E., additional, Hughes, B.G.M., additional, Schadendorf, D., additional, Modi, B., additional, Dunn, L., additional, Flatz, L., additional, Hauschild, A., additional, Yoo, S-Y., additional, Booth, J., additional, Seebach, F., additional, Lowy, I., additional, Fury, M.G., additional, and Rischin, D., additional

Published
2022
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21. Prognosis of Patients With Primary Melanoma Stage I and II According to American Joint Committee on Cancer Version 8 Validated in Two Independent Cohorts: Implications for Adjuvant Treatment

Author

Garbe, C., Keim, U., Amaral, T., Berking, C., Eigentler, T. K., Flatz, L., Gesierich, A., Leiter, U., Stadler, R., Sunderkotter, C., Tuting, T., Utikal, J., Wollina, U., Zimmer, L., Zouboulis, C. C., Ascierto, P. A., Eggermont, A. M. M., Grob, J. -J., Hauschild, A., Sekulovic, L. K., Long, G. V., Luke, J. J., Michielin, O., Peris, Ketty, Schadendorf, D., Kirkwood, J. M., Lorigan, P. C., Peris K. (ORCID:0000-0002-5237-0463), Garbe, C., Keim, U., Amaral, T., Berking, C., Eigentler, T. K., Flatz, L., Gesierich, A., Leiter, U., Stadler, R., Sunderkotter, C., Tuting, T., Utikal, J., Wollina, U., Zimmer, L., Zouboulis, C. C., Ascierto, P. A., Eggermont, A. M. M., Grob, J. -J., Hauschild, A., Sekulovic, L. K., Long, G. V., Luke, J. J., Michielin, O., Peris, Ketty, Schadendorf, D., Kirkwood, J. M., Lorigan, P. C., and Peris K. (ORCID:0000-0002-5237-0463)

Abstract

PURPOSEThe first randomized trial of adjuvant treatment with checkpoint inhibitor in stage II melanoma reported a significant reduction in risk of tumor recurrence. This study evaluates two independent data sets to further document survival probabilities for patients with primary stage I and II melanoma.PATIENTS AND METHODSThe Central Malignant Melanoma Registry (CMMR) in Germany evaluated 17,544 patients with a primary diagnosis of stage I and II melanoma from 2000 to 2015. The exploratory cohort consisted of 6,725 patients from the Center for Dermato-Oncology at the University of Tübingen, and the confirmatory cohort consisted of 10,819 patients from 11 other German centers. Survival outcomes were compared with published American Joint Committee on Cancer version 8 (AJCCv8) stage I and II survival data.RESULTSFor the two CMMR cohorts in stage IA compared with the AJCCv8 cohort, melanoma-specific survival rates at 10 years were 95.1%-95.6% versus 98%; 89.7%-90.9% versus 94% in stage IB; 80.7%-83.1% versus 88% in stage IIA; 72.0%-79.9% versus 82% in stage IIB; and 57.6%-64.7% versus 75% in stage IIC, respectively. Recurrence rates were approximately twice as high as melanoma-specific mortality rates in stages IA-IIA.CONCLUSIONThe melanoma-specific survival rates in the two CMMR cohorts across stages I and II are less favorable than published in AJCCv8. This has important implications for the consideration of adjuvant treatment in this population.

Published
2022

23. Genomic profiling of late-onset basal cell carcinomas from two brothers with nevoid basal cell carcinoma syndrome

Author

Hasan Ali, O, Yurchenko, A A, Pavlova, O, Sartori, A, Bomze, D, Higgins, R, Ring, S S, Hartmann, F, Bühler, D, Fritzsche, F R, Jochum, W, Navarini, A A, Kim, A, French, L E, Dermitzakis, E, Christiano, A M, Hohl, D, Bickers, D R, Nikolaev, S I, Flatz, L, University of Zurich, Nikolaev, S I, and Flatz, L

Subjects
2708 Dermatology, 10177 Dermatology Clinic, 610 Medicine & health, 2725 Infectious Diseases
Published
2021

25. 1044P Sequential targeted and immunotherapies in stage IV melanoma

Author

Amaral, T.M.S., primary, Nolinski, J., additional, Niessner, H., additional, Sinnberg, T., additional, Seeber, O., additional, Sanchez, S., additional, Keim, U., additional, Thomas, I., additional, Meiwes, A., additional, Koechel, A., additional, Forschner, A., additional, Leiter, U., additional, Flatz, L., additional, Eigentler, T., additional, and Garbe, C., additional

Published
2021
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26. Étude de phase 3 (PIVOTAL) sur le daromun intralésionnel néoadjuvant comparé à une chirurgie immédiate dans le mélanome entièrement résécable avec métastases cutanées régionales et/ou ganglionnaires

Author

Robert, C., Hassel, J.C., Ziemer, M., Rutkowski, P., Meier, F.E., Flatz, L., Gaudy-Marqueste, C., Santinami, M., Russano, F., Von, W.I., Eigentler, T., Maio, M., Zalaudek, I., Haferkamp, S., Quaglino, P., Ascierto, P.A., Garbe, C., Schadendorf, D., Kaehler, K.C., and Hauschild, A.

Abstract

PIVOTAL (NCT02938299) est un essai ouvert, randomisé, multicentrique de phase 3 évaluant le daromun comme traitement (Tx) intralésionnel néoadjuvant pour le mélanome localement avancé, résécable, de stade III. Le daromun, une combinaison de deux fusions anticorps-cytokines (L19IL2, L19TNF) a montré son efficacité dans une étude de phase 2 (NCT02076633) chez des patients (pts) atteints de mélanome non résécable.

Published
2024
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33. Genomic profiling of late‐onset basal cell carcinomas from two brothers with nevoid basal cell carcinoma syndrome

Author

Hasan Ali, O., primary, Yurchenko, A.A., additional, Pavlova, O., additional, Sartori, A., additional, Bomze, D., additional, Higgins, R., additional, Ring, S.S., additional, Hartmann, F., additional, Bühler, D., additional, Fritzsche, F.R., additional, Jochum, W., additional, Navarini, A.A., additional, Kim, A., additional, French, L.E., additional, Dermitzakis, E., additional, Christiano, A.M., additional, Hohl, D., additional, Bickers, D.R., additional, Nikolaev, S.I., additional, and Flatz, L., additional

Published
2020
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34. Viral infection overcomes ineffectiveness of anti-tumoral CD8+ T cell mediated cytotoxicity

Author

Duhan, Judith Bezgovsek, Kardash J, Flatz L, Karl S. Lang, Pa Lang, Hilal Bhat, Sarah-Kim Friedrich, Halime Kalkavan, Krolik M, Yara Maria Machlah, Fan Zhou, Michael Bergerhausen, Cornelia Hardt, Tim Brandenburg, and Maximilian Schiller

Subjects
Immune system, medicine.anatomical_structure, biology, Tumor progression, T cell, MHC class I, biology.protein, medicine, Cancer research, Cytotoxic T cell, T cell mediated cytotoxicity, Immune checkpoint, CD8
Abstract

With the integration of PD-1 and CTLA-4 targeting immune checkpoint blockade into cancer treatment regimes, the anti-tumoral cytotoxicity of tumor-specific CD8+T cells is well established. However, while the unresponsiveness of CD8+T cells against big tumors is mainly explained by T cell exhaustion, other factors contributing to CD8+T cell failure remain not well studied. Here we used a mouse melanoma model to study the interaction of growing tumor cells, innate immunity and CD8+T cell responses induced by viral replication. Mouse model of melanoma (B16F10-OVA) and infections with arenaviruses. Growing B16F10-OVA cells did not induce systemic ablation of tumor specific CD8+T cells. However, despite the presence of tumor-infiltrating CD8+T cells, the anti-tumoral immune response was very limited. T cell anergy against the tumor was accompanied with a strong down-regulation of MHC-I on advanced tumors. LCMV infection restored the MHC class I expression, enhanced T cell function and lead to tumor regression. This study shows that tumor progression does not necessary lead to systemic exhaustion of the anti-tumoral CD8+T cell response. Lack of innate signals is an additional reason for limited CD8+T cell mediated cytotoxicity against the tumor.

Published
2019
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38. Protective Efficacy of Individual CD8+ T Cell Specificities in Chronic Viral Infection

Author

Johnson S Bergthaler A Graw F Flatz L Bonilla WV Siegrist C Lambert P Regoes RR Pinschewer D

Subjects
viruses, hemic and immune systems, chemical and pharmacologic phenomena
Abstract

Specific CD8+ T cells (CTLs) play an important role in resolving protracted infection with hepatitis B and C virus in humans and lymphocytic choriomeningitis virus (LCMV) in mice. The contribution of individual CTL specificities to chronic virus control as well as epitope specific patterns in timing and persistence of antiviral selection pressure remain however incompletely defined. To monitor and characterize the antiviral efficacy of individual CTL specificities throughout the course of chronic infection we coinoculated mice with a mixture of wild type LCMV and genetically engineered CTL epitope deficient mutant virus. A quantitative longitudinal assessment of viral competition revealed that mice continuously exerted CTL selection pressure on the persisting virus population. The timing of selection pressure characterized individual epitope specificities and its magnitude varied considerably between individual mice. This longitudinal assessment of “antiviral efficacy” provides a novel parameter to characterize CTL responses in chronic viral infection. It demonstrates remarkable perseverance of all antiviral CTL specificities studied thus raising hope for therapeutic vaccination in the treatment of persistent viral diseases.

Published
2015

39. Genomic profiling of late‐onset basal cell carcinomas from two brothers with nevoid basal cell carcinoma syndrome.

Author

Hasan Ali, O., Yurchenko, A.A., Pavlova, O., Sartori, A., Bomze, D., Higgins, R., Ring, S.S., Hartmann, F., Bühler, D., Fritzsche, F.R., Jochum, W., Navarini, A.A., Kim, A., French, L.E., Dermitzakis, E., Christiano, A.M., Hohl, D., Bickers, D.R., Nikolaev, S.I., and Flatz, L.

Subjects
BASAL cell nevus syndrome, BASAL cell carcinoma, BROTHERS, DNA analysis, RNA sequencing
Abstract

Background: Nevoid basal cell carcinoma syndrome (NBCCS) is an autosomal dominant genetic disorder. It is commonly caused by mutations in PTCH1 and chiefly characterized by multiple basal cell carcinomas (BCCs) developing prior to the age of 30 years. In rare cases, NBCCS presents with a late onset of BCC development. Objective: To investigate BCC tumorigenesis in two brothers, who showed characteristic features of NBCCS but developed their first BCCs only after the age of 40 years. Two other siblings did not show signs of NBCCS. Results: We obtained blood samples from four siblings and nine BCCs from the two brothers with NBCCS. Whole exome sequencing and RNA sequencing revealed loss of heterozygosity (LOH) of PTCH1 in eight out of nine tumours that consistently involved the same haplotype on chromosome 9. This haplotype contained a germinal splice site mutation in PTCH1 (NM_001083605:exon9:c.763‐6C>A). Analysis of germline DNA confirmed segregation of this mutation with the disease. All BCCs harboured additional somatic loss‐of‐function (LoF) mutations in the remaining PTCH1 allele which are not typically seen in other cases of NBCCS. This suggests a hypomorphic nature of the germinal PTCH1 mutation in this family. Furthermore, all BCCs had a similar tumour mutational burden compared to BCCs of unrelated NBCCS patients while harbouring a higher number of damaging PTCH1 mutations. Conclusions: Our data suggest that a sequence of three genetic hits leads to the late development of BCCs in two brothers with NBCCS: a hypomorphic germline mutation, followed by somatic LOH and additional mutations that complete PTCH1 inactivation. These genetic events are in line with the late occurrence of the first BCC and with the higher number of damaging PTCH1 mutations compared to usual cases of NBCCS. [ABSTRACT FROM AUTHOR]

Published
2021
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42. Vaccination Strategies against Highly Pathogenic Arenaviruses: The Next Steps toward Clinical Trials

Author

Olschläger, S. and Flatz, L.

Subjects
viruses, virus diseases
Abstract

Vaccination is one of the most valuable weapons against infectious diseases and has led to a significant reduction in mortality and morbidity. However, for most viral hemorrhagic fevers caused by arenaviruses, no prophylactic vaccine is available. This is particularly problematic as these diseases are notoriously difficult to diagnose and treat. Lassa fever is globally the most important of the fevers caused by arenaviruses, potentially affecting millions of people living in endemic areas, particularly in Nigeria. Annually, an estimated 300,000 humans are infected and several thousands succumb to the disease. The successful development of the vaccine "Candid#1" against Junin virus, the causative agent of Argentine hemorrhagic fever, proved that an effective arenavirus vaccine can be developed. Although several promising studies toward the development of a Lassa fever vaccine have been published, no vaccine candidate has been tested in human volunteers or patients. This review summarizes the immunology and other aspects of existing experimental arenavirus vaccine studies, discusses the reasons for the lack of a vaccine, and proposes a plan for overcoming the final hurdles toward clinical trials.

Published
2013

44. Innate and adaptive immune control of genetically engineered live-attenuated arenavirus vaccine prototypes

Author

Pinschewer, D D, Flatz, L, Steinborn, R, Horvath, E, Fernandez, M, Lutz, H, Suter, M, Bergthaler, A, Pinschewer, D D, Flatz, L, Steinborn, R, Horvath, E, Fernandez, M, Lutz, H, Suter, M, and Bergthaler, A

Abstract

Arenaviruses such as Lassa virus (LASV) cause significant morbidity and mortality in endemic areas. Using a glycoprotein (GP) exchange strategy, we have recently developed live-attenuated arenavirus vaccine prototypes (rLCMV/VSVG) based on lymphocytic choriomeningitis virus (LCMV), a close relative of LASV. rLCMV/VSVG induced long-term CD8(+) T cell immunity against wild-type virus challenge and exhibited a stably attenuated phenotype in vivo. Here we elucidated the innate and adaptive immune requirements for the control of rLCMV/VSVG. Infection of RAG(-/-) mice resulted in persisting viral RNA in blood but not in overt viremia. The latter was only found in mice lacking both RAG and IFN type I receptor. Conversely, absence of IFN type II signaling or NK cells on an RAG-deficient background had only minor effects on vaccine virus load or none at all. rLCMV/VSVG infection of wild-type mice induced less type I IFN than did wild-type LCMV, and type I as well as type II IFNs were dispensable for the induction of virus-specific memory CD8 T cells and virus-neutralizing antibodies by rLCMV/VSVG. In conclusion, the adaptive immune systems are essential for elimination of rLCMV/VSVG, and type I but not type II IFN plays a major contributive role in lowering rLCMV/VSVG loads in vivo, attesting to the attenuation profile of the vaccine. Nevertheless, IFNs are not required for the induction of potent vaccine responses. These results provide a better understanding of the immunobiology of rLCMV/VSVG and will contribute to the further development of GP exchange vaccines for combating arenaviral hemorrhagic fevers.

Published
2010

45. T cell-dependence of Lassa fever pathogenesis

Author

Flatz, L, Rieger, T, Merkler, D, Bergthaler, A, Regen, T, Schedensack, M, Bestmann, L, Verschoor, A, Kreutzfeldt, M, Brück, W, Hanisch, U K, Günther, S, Pinschewer, D D, Flatz, L, Rieger, T, Merkler, D, Bergthaler, A, Regen, T, Schedensack, M, Bestmann, L, Verschoor, A, Kreutzfeldt, M, Brück, W, Hanisch, U K, Günther, S, and Pinschewer, D D

Abstract

Lassa virus (LASV), the causative agent of Lassa fever (LF), is endemic in West Africa, accounting for substantial morbidity and mortality. In spite of ongoing research efforts, LF pathogenesis and mechanisms of LASV immune control remain poorly understood. While normal laboratory mice are resistant to LASV, we report that mice expressing humanized instead of murine MHC class I (MHC-I) failed to control LASV infection and develop severe LF. Infection of MHC-I knockout mice confirmed a key role for MHC-I-restricted T cell responses in controlling LASV. Intriguingly we found that T cell depletion in LASV-infected HHD mice prevented disease, irrespective of high-level viremia. Widespread activation of monocyte/macrophage lineage cells, manifest through inducible NO synthase expression, and elevated IL-12p40 serum levels indicated a systemic inflammatory condition. The absence of extensive monocyte/macrophage activation in T cell-depleted mice suggested that T cell responses contribute to deleterious innate inflammatory reactions and LF pathogenesis. Our observations in mice indicate a dual role for T cells, not only protecting from LASV, but also enhancing LF pathogenesis. The possibility of T cell-driven enhancement and immunopathogenesis should be given consideration in future LF vaccine development.

Published
2010

46. Overexpression of lymphotoxin in T cells induces fulminant thymic involution

Author

Heikenwalder, M, Prinz, M, Zeller, N, Lang, K S, Junt, T, Rossi, S, Tumanov, A, Schmidt, H, Priller, J, Flatz, L, Rülicke, T, Macpherson, A J, Holländer, G A, Nedospasov, S A, Aguzzi, A; https://orcid.org/0000-0002-0344-6708, Heikenwalder, M, Prinz, M, Zeller, N, Lang, K S, Junt, T, Rossi, S, Tumanov, A, Schmidt, H, Priller, J, Flatz, L, Rülicke, T, Macpherson, A J, Holländer, G A, Nedospasov, S A, and Aguzzi, A; https://orcid.org/0000-0002-0344-6708

Abstract

Activated lymphocytes and lymphoid-tissue inducer cells express lymphotoxins (LTs), which are essential for the organogenesis and maintenance of lymphoreticular microenvironments. Here we describe that T-cell-restricted overexpression of LT induces fulminant thymic involution. This phenotype was prevented by ablation of the LT receptors tumor necrosis factor receptor (TNFR) 1 or LT beta receptor (LTbetaR), representing two non-redundant pathways. Multiple lines of transgenic Ltalphabeta and Ltalpha mice show such a phenotype, which was not observed on overexpression of LTbeta alone. Reciprocal bone marrow transfers between LT-overexpressing and receptor-ablated mice show that involution was not due to a T cell-autonomous defect but was triggered by TNFR1 and LTbetaR signaling to radioresistant stromal cells. Thymic involution was partially prevented by the removal of one allele of LTbetaR but not of TNFR1, establishing a hierarchy in these signaling events. Infection with the lymphocytic choriomeningitis virus triggered a similar thymic pathology in wt, but not in Tnfr1(-/-) mice. These mice displayed elevated TNFalpha in both thymus and plasma, as well as increased LTs on both CD8(+) and CD4(-)CD8(-) thymocytes. These findings suggest that enhanced T cell-derived LT expression helps to control the physiological size of the thymic stroma and accelerates its involution via TNFR1/LTbetaR signaling in pathological conditions and possibly also in normal aging.

Published
2008

49. T cell-dependence of Lassa fever pathogenesis

Author

Flatz, L, Rieger, T, Merkler, D, Bergthaler, A, Regen, T, Schedensack, M, Bestmann, L, Verschoor, A, Kreutzfeldt, M, Brück, W, Hanisch, U K, Günther, S, and Pinschewer, D D

Subjects
3. Good health

50. Meropenem Prevents Levofloxacin-Induced Resistance in Penicillin-Resistant Pneumococci and Acts Synergistically with Levofloxacin in Experimental Meningitis

Author

Cottagnoud, P., Cottagnoud, M., Acosta, F., Flatz, L., Kühn, F., Stucki, A., Entenza, J., Cottagnoud, P., Cottagnoud, M., Acosta, F., Flatz, L., Kühn, F., Stucki, A., and Entenza, J.

Abstract

The aim of the present study was to investigate the potential synergy between meropenem and levofloxacin in vitro and in experimental meningitis and to determine the effect of meropenem on levofloxacin-induced resistance in vitro. Meropenem increased the efficacy of levofloxacin against the penicillin-resistant pneumococcal strain KR4 in time-killing assays in vitro and acted synergistically against a second penicillin-resistant strain WB4. In the checkerboard, only an additive effect (FIC indices: 1.0) was observed for both strains. In cycling experiments in vitro, levofloxacin alone led to a 64-fold increase in the MIC for both strains after 12 cycles. Addition of meropenem in sub-MIC concentrations (0.25×MIC) completely inhibited the selection of levofloxacin-resistant mutants in WB4 after 12 cycles. In KR4, the addition of meropenem led to just a twofold increase in the MIC for levofloxacin after 12 cycles. Mutations detected in the genes encoding for topoisomerase IV (parC) and gyrase (gyrA) confirmed the levofloxacin-induced resistance in both strains. Addition of meropenem was able to completely suppress levofloxacin-induced mutations in WB4 and led to only one mutation in parE in KR4. In experimental meningitis, meropenem, given in two doses (2×125mg/kg), produced a good bactericidal activity (−0.45 Δlog10 cfu/ml·h) comparable to one dose (1×10mg/kg) of levofloxacin (−0.44 Δlog10 cfu/ml·h) against the penicillin-resistant strain WB4. Meropenem combined with levofloxacin acted synergistically (−0.93 Δlog10 cfu/ml·h), sterilizing the CSF of all rabbits

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