Your search keyword '"Anna Fogdell-Hahn"' showing total 10 results

1. COVID‐19 clinical outcomes and DMT of MS patients and population‐based controls

Author

Elisa Longinetti, Hannah Bower, Kyla A McKay, Simon Englund, Joachim Burman, Katharina Fink, Anna Fogdell‐Hahn, Martin Gunnarsson, Jan Hillert, Annette Langer‐Gould, Jan Lycke, Petra Nilsson, Jonatan Salzer, Anders Svenningsson, Johan Mellergård, Tomas Olsson, Fredrik Piehl, and Thomas Frisell

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective To estimate risks for all‐cause mortality and for severe COVID‐19 in multiple sclerosis patients and across relapsing–remitting multiple sclerosis patients exposed to disease‐modifying therapies. Methods We conducted a Swedish nationwide population‐based multi‐register linkage cohort study and followed all multiple sclerosis patients (n = 17,692 in March 2020), individually age‐, sex‐, and region‐matched to five population‐based controls (n = 86,176 in March 2020) during March 2020–June 2021. We compared annual all‐cause mortality within and across cohorts, and assessed incidence rates and relative risks for hospitalization, intensive care admission, and death due to COVID‐19 in relation to disease‐modifying therapy use, using Cox regression. Results Absolute all‐cause mortality among multiple sclerosis patients was higher from March to December 2020 than in previous years, but relative risks versus the population‐based controls were similar to preceding years. Incidence rates of hospitalization, intensive care admission, and death due to COVID‐19 remained in line with those for all‐cause hospitalization, intensive care admission, and mortality. Among relapsing–remitting patients on rituximab, trends for differences in risk of hospitalization due to COVID‐19 remained in the demographics‐, socioeconomic status‐, comorbidity‐, and multiple sclerosis severity‐adjusted model. Interpretation Risks of severe COVID‐19‐related outcomes were increased among multiple sclerosis patients as a whole compared to population controls, but risk increases were also seen for non‐COVID‐19 hospitalization, intensive care admission, and mortality, and did not significantly differ during the pandemic compared to pre‐pandemic years. The risk conveyed by disease‐modifying therapies was smaller than previously assumed, likely as a consequence of the possibility to better control for confounders.

Published

2022

2. Systematic evaluation of SARS‐CoV‐2 antigens enables a highly specific and sensitive multiplex serological COVID‐19 assay

Author

Sophia Hober, Cecilia Hellström, Jennie Olofsson, Eni Andersson, Sofia Bergström, August Jernbom Falk, Shaghayegh Bayati, Sara Mravinacova, Ronald Sjöberg, Jamil Yousef, Lovisa Skoglund, Sara Kanje, Anna Berling, Anne‐Sophie Svensson, Gabriella Jensen, Henric Enstedt, Delaram Afshari, Lan Lan Xu, Martin Zwahlen, Kalle vonFeilitzen, Leo Hanke, Ben Murrell, Gerald McInerney, Gunilla B Karlsson Hedestam, Christofer Lendel, Robert G Roth, Ingmar Skoog, Elisabet Svenungsson, Tomas Olsson, Anna Fogdell‐Hahn, Ylva Lindroth, Maria Lundgren, Kimia T Maleki, Nina Lagerqvist, Jonas Klingström, Rui Da Silva Rodrigues, Sandra Muschiol, Gordana Bogdanovic, Laila Sara Arroyo Mühr, Carina Eklund, Camilla Lagheden, Joakim Dillner, Åsa Sivertsson, Sebastian Havervall, Charlotte Thålin, Hanna Tegel, Elisa Pin, Anna Månberg, My Hedhammar, and Peter Nilsson

Subjects

COVID‐19, IgG, multiplex, SARS‐CoV‐2, serological assay, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Objective The COVID‐19 pandemic poses an immense need for accurate, sensitive and high‐throughput clinical tests, and serological assays are needed for both overarching epidemiological studies and evaluating vaccines. Here, we present the development and validation of a high‐throughput multiplex bead‐based serological assay. Methods More than 100 representations of SARS‐CoV‐2 proteins were included for initial evaluation, including antigens produced in bacterial and mammalian hosts as well as synthetic peptides. The five best‐performing antigens, three representing the spike glycoprotein and two representing the nucleocapsid protein, were further evaluated for detection of IgG antibodies in samples from 331 COVID‐19 patients and convalescents, and in 2090 negative controls sampled before 2020. Results Three antigens were finally selected, represented by a soluble trimeric form and the S1‐domain of the spike glycoprotein as well as by the C‐terminal domain of the nucleocapsid. The sensitivity for these three antigens individually was found to be 99.7%, 99.1% and 99.7%, and the specificity was found to be 98.1%, 98.7% and 95.7%. The best assay performance was although achieved when utilising two antigens in combination, enabling a sensitivity of up to 99.7% combined with a specificity of 100%. Requiring any two of the three antigens resulted in a sensitivity of 99.7% and a specificity of 99.4%. Conclusion These observations demonstrate that a serological test based on a combination of several SARS‐CoV‐2 antigens enables a highly specific and sensitive multiplex serological COVID‐19 assay.

Published

2021

3. Cancer Risk for Fingolimod, Natalizumab, and Rituximab in Multiple Sclerosis Patients

Author

Katharina Fink, Joachim Burman, Anna Fogdell-Hahn, Petra Nilsson, Thomas Frisell, Peter Alping, Tomas Olsson, Jonatan Salzer, Martin Gunnarsson, Jan Lycke, Annette Langer-Gould, Johan Askling, Jan Hillert, Anders Svenningsson, Magnus Vrethem, and Fredrik Piehl

Subjects

Adult, Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Multiple Sclerosis, Neurology, Neurologi, MEDLINE, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Natalizumab, Neoplasms, Internal medicine, Humans, Immunologic Factors, Medicine, Sweden, Fingolimod Hydrochloride, business.industry, Incidence, Kirurgi, Multiple sclerosis, Incidence (epidemiology), Middle Aged, medicine.disease, Fingolimod, 030104 developmental biology, Female, Surgery, Rituximab, Neurology (clinical), business, 030217 neurology & neurosurgery, medicine.drug, Cohort study

Abstract

Objective: Novel, highly effective disease-modifying therapies have revolutionized multiple sclerosis (MS) care. However, evidence from large comparative studies on important safety outcomes, such as cancer, is still lacking. Methods: In this nationwide register-based cohort study, we linked data from the Swedish MS register to the Swedish Cancer Register and other national health care and census registers. We included 4,187 first-ever initiations of rituximab, 1,620 of fingolimod, and 1,670 of natalizumab in 6,136 MS patients matched for age, sex, and location to 37,801 non-MS general population subjects. Primary outcome was time to first invasive cancer. Results: We identified 78 invasive cancers among treated patients: rituximab 33 (incidence rate [IR] per 10,000 person-years = 34.4, 95% confidence interval [CI] = 23.7–48.3), fingolimod 28 (IR = 44.0, 95% CI = 29.2–63.5), and natalizumab 17 (IR = 26.0, 95% CI = 15.1–41.6). The general population IR was 31.0 (95% CI = 27.8–34.4). Adjusting for baseline characteristics, we found no difference in risk of invasive cancer between rituximab, natalizumab, and the general population but a possibly higher risk with fingolimod compared to the general population (hazard ratio [HR] = 1.53, 95% CI = 0.98–2.38) and rituximab (HR = 1.68, 95% CI = 1.00–2.84). Interpretation: In this first large comparative study of 3 highly effective MS disease-modifying therapies, no increased risk of invasive cancer was seen with rituximab and natalizumab, compared to the general population. However, there was a borderline-significant increased risk with fingolimod, compared to both the general population and rituximab. It was not possible to attribute this increased risk to any specific type of cancer, and further studies are warranted to validate these findings.

Published

2020

4. Men and women in immunology: Closing the gap on gender parity?

Author

Catherine Williamson, Anna Fogdell-Hahn, Christina Helbig, Jesper Fundberg, Peter J. M. Openshaw, and Landsteiner Laboratory

Subjects

0301 basic medicine, Science & Technology, media_common.quotation_subject, Closing (real estate), Immunology, Biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 1107 Immunology, Immunology and Allergy, 030212 general & internal medicine, Parity (mathematics), Life Sciences & Biomedicine, media_common, Demography

Published

2018

5. Antidrug Antibodies: B Cell Immunity Against Therapy

Author

Anna Fogdell-Hahn

Subjects

Drug, Multiple Sclerosis, media_common.quotation_subject, Immunology, Antibodies, Monoclonal, Humanized, Hemophilia A, Haemophilia, Antibodies, Arthritis, Rheumatoid, Immune system, Natalizumab, Immune Tolerance, medicine, Humans, Treatment Failure, media_common, B-Lymphocytes, Factor VIII, biology, business.industry, Multiple sclerosis, Interferon-beta, General Medicine, medicine.disease, Biopharmaceutical, Pharmaceutical Preparations, Drug development, Antirheumatic Agents, biology.protein, Antibody, business, medicine.drug

Abstract

Chronic inflammatory diseases are now treated with a range of different biopharmaceuticals, often requiring lifelong parenteral administrations. This exposure to drugs is unnatural and can trigger the immune system and result in the formation of antidrug antibodies. Drug-specific antibodies will, if of sufficiently high titre and affinity, block the intended effect of the drug, increase its clearance and make continued treatment worthless. We expect the immune system to react towards therapies against which tolerance has never been established, which is the case for factor VIII treatment in patients with haemophilia A. However, even biopharmaceutical molecules that we should be tolerant against can elicit antidrug antibodies, for instance in treatment of multiple sclerosis patients with recombinant human interferon-beta. Possible immunological mechanisms behind the breaking of tolerance against drugs, the impact this has on continuous treatment success, clinical practice and drug development, will be discussed in this review.

Published

2015

6. Complete replication cycle and acquisition of tegument in nucleus of human herpesvirus 6A in astrocytes and in T-cells

Author

Steven Jacobson, Nahid Akhyani, Anna Fogdell-Hahn, Eugene O. Major, Donatella Donati, Jenny Ahlqvist, Jean Hou, and Elena Martinelli

Subjects

Herpesvirus 6, Human, T-Lymphocytes, viruses, Biology, Virus Replication, Cytopathogenic Effect, Viral, Microscopy, Electron, Transmission, Viral life cycle, Virology, medicine, Humans, Cells, Cultured, Tropism, Nucleoplasm, Virion, virus diseases, Viral tegument, biochemical phenomena, metabolism, and nutrition, Cell Nucleus Structures, Cell biology, Infectious Diseases, medicine.anatomical_structure, Viral replication, Cytoplasm, Astrocytes, Neuroglia, Astrocyte

Abstract

The ultrastructural replication cycle of human herpesvirus 6A and 6B, both T-lymphotropic viruses, with tropism for the central nervous system, was compared by electron microscopy in the same cells, that is, in the T-lymphoblastoid cell line SupT-1 and in human astrocytes. Both HHV-6A and HHV-6B replicated efficiently in SupT-1 and formed viral particles. The tegument is the least characterized structure of the herpesviral particle and both variants were able to form intranuclear membrane compartments called tegusomes in SupT-1 where tegumentation occurred. Also, tegumentation occurred in HHV-6A infected cells in the nucleoplasm without the presence of a tegusome. This suggests that there is more than one possible route of tegumentation. Differences in the replication cycles between HHV-6A and HHV-6B were also observed in the cytoplasm. One such difference was that prominent annulate lamellae were only found in the cytoplasm of HHV-6A infected cells. In astrocytes a successful formation of viral particles was only seen with the HHV-6A variant. The HHV-6A virus life cycle in astrocytes resembled the life cycle in the T-cell line SupT-1, except that no annulate lamellae were found. Complete viral particles were found extracellularly around the astrocytes and the supernatant of infected astrocytes were able to re-infect SupT-1 cells. This suggests that HHV-6A infection in astrocytes can generate complete, viable, and infectious viral particles. The HHV-6 variants behave differently in the same type of cells and have different tropisms for astrocytes, supporting the notion that the variants might induce different diseases.

Published

2006

7. A NOTCH4 association with multiple sclerosis is secondary to HLA-DR*1501

Author

M Anderson, Jan Hillert, Kristina Duvefelt, and Anna Fogdell-Hahn

Subjects

Central Nervous System, Linkage disequilibrium, Multiple Sclerosis, Immunology, Receptors, Cell Surface, Single-nucleotide polymorphism, Human leukocyte antigen, Biology, Polymorphism, Single Nucleotide, Biochemistry, Linkage Disequilibrium, Proto-Oncogene Proteins, Genetics, Genetic predisposition, HLA-DR, Humans, Immunology and Allergy, Allele, Receptor, Notch4, Alleles, HLA-A Antigens, Receptors, Notch, Tumor Necrosis Factor-alpha, Haplotype, HLA-DR Antigens, General Medicine, Haplotypes, Trinucleotide repeat expansion, HLA-DRB1 Chains

Abstract

Multiple sclerosis (MS) is a chronic inflammatory disease of the central nervous system (CNS) with supposedly autoimmune features known to be associated with a specific HLA DR-DQ haplotype (DR15, DQ6, or HLDRB1*1501,DRB5*0101,DQA1*0102,DQB1*0602). We have previously reported that the associated haplotype extends to HLA-B and described an independent association with HLA-A alleles in MS. Owing to a complex situation with extensive linkage disequilibria, it is still unclear whether classical HLA genes are responsible or whether associations may be due to other genes in this region. Here, we analyzed an association in MS with the NOTCH4 and TNFalpha (tumor necrosis factor-alpha) genes, located between the HLA-DRB1 gene and the HLA-A gene. For NOTCH4, located 0.4 Mb telomeric to HLA-DRB1, an SNP at position -25 and a trinucleotide repeat were investigated in 181 MS patients, and 180 controls also typed P = 0.027 for HLA-DRB and HLA-A. A modest association was observed (OR = 3.44) with the C-25 allele. However, two-locus analysis revealed that this association was secondary to the classical association with HLA-DRB1. For TNF, located 0.7 Mb telomeric of NOTCH4, SNPs at positions -308 and -238 were studied in the same dataset. We found no association between these TNFalpha gene polymorphisms and MS in this dataset, although there was linkage disequilibrium (LD) between DRB1 and TNF and between HLA-A and TNF. We conclude that alleles of the NOTCH4 and TNFalpha genes are unlikely to be of importance for the susceptibility to MS, although specific alleles of these genes are often carried on the same haplotype as DR15, DQ6.

Published

2004

8. Multiple sclerosis: a modifying influence of HLA class I genes in an HLA class II associated autoimmune disease

Author

Arturs Ligers, M. Grønning, Olle Olerup, Anna Fogdell-Hahn, and Jan Hillert

Subjects

Genetics, Autoimmune disease, Multiple sclerosis, Immunology, Haplotype, General Medicine, Odds ratio, Human leukocyte antigen, Biology, medicine.disease_cause, medicine.disease, Biochemistry, Autoimmunity, medicine, Genetic predisposition, Immunology and Allergy, Allele

Abstract

Acknowledgments: This study was supported by grants from the Swedish Medical Research Council, the Childrens’ Cancer Foundation, the Tobias Foundation and the Swedish association of the Neurologically Disabled. Abstract: Multiple sclerosis (MS) is a presumed autoimmune disease of the central nervous system, shown to be associated with the HLA class II haplotype DRB1*15,DQB1*06. Carrying the HLA class II haplotype DRB1*15,DQB1*06 increases the risk of MS by 3.6. By adopting a polymerase chain reaction (PCR)-based typing technique for HLA class I and class II genes, 200 Swedish MS patients and 210 Swedish healthy controls were analysed for their HLA alleles. Additional HLA class I alleles that increase and decrease the genetic susceptibility to MS were identified. The HLA-A*0301 allele increases the risk of MS (odds ratio=2.1) independently of DRB1*15,DQB1*06. HLA-A*0201 decreases the overall risk (odds ratio=0.52) and the presence of A*0201 reduces the risk of MS for DRB1*15,DQB1*06 carriers from 3.6 to 1.5. Our findings are the first to identify a major modulating effect of HLA class I alleles on the susceptibility to a human autoimmune disease; a phenomenon that has previously only been observed in animal models.

Published

2000

9. DQB1*0202and the newDQB1*0203allele: a fourth pair ofDQB1alleles differing only at codon 57

Author

A. Aldener-Cannavá, Anna Fogdell-Hahn, D. R. Wagenknecht, Olle Olerup, R. R. Getty, and John A. McIntyre

Subjects

DNA, Complementary, endocrine system diseases, Molecular Sequence Data, Immunology, Fixed allele, Peptide binding, Human leukocyte antigen, Biology, Balancing selection, Biochemistry, HLA-DQ Antigens, Sequence Homology, Nucleic Acid, Genetics, HLA-DQ beta-Chains, Humans, Immunology and Allergy, Allele, Codon, Gene, Alleles, HLA-DQB1, Base Sequence, Haplotype, nutritional and metabolic diseases, Exons, General Medicine, Molecular biology

Abstract

Amino acid 57 of DQ β chains is of functional importance as it influences peptide binding, is part of B and T cell epitopes, and is associated with susceptibility and resistance to insulin-dependent diabetes mellitus and humoral immunodeficiencies. Polymorphism of codon 57 is conserved in primates and in HLA class II B genes implying that balancing selection operates on this residue. Previously, three DQB1 allele pairs have been described, that only differ at residue 57. In an African-American Black individual with the HLA pheno-type A23, 30; B58, 63; Cw6; DR18, 12; DR52; DQ5, 2, we found a fourth example of this dimorphism; the new DQB1*0203 allele, that was identical to DQB1*0202 except for codon 57, which encodes aspartic acid and alanine respectively in the two alleles. The class II haplotype carrying the new allele was deduced to be DRB1*0302, DRB3*0101, DQA1*05011, DQB1*0203

Published

1997

10. 3rd Nordic Meeting on Genetics and Pathogenesis of Inflammatory Diseases

Author

Anna Fogdell-Hahn and Marie Wahren-Herlenius

Subjects

Pathogenesis, business.industry, Immunology, Medicine, General Medicine, business

Published

2012