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1. HLA-DR7 and HLA-DQ2: Transgenic mouse strains tested as a model system for ximelagatran hepatotoxicity.

Author

Hanna Lundgren, Klara Martinsson, Karin Cederbrant, Johan Jirholt, Daniel Mucs, Katja Madeyski-Bengtson, Said Havarinasab, and Per Hultman

Subjects
Medicine, Science
Abstract

The oral thrombin inhibitor ximelagatran was withdrawn in the late clinical trial phase because it adversely affected the liver. In approximately 8% of treated patients, drug-induced liver injury (DILI) was expressed as transient alanine transaminase (ALT) elevations. No evidence of DILI had been revealed in the pre-clinical in vivo studies. A whole genome scan study performed on the clinical study material identified a strong genetic association between the major histocompatibility complex alleles for human leucocyte antigens (HLA) (HLA-DR7 and HLA-DQ2) and elevated ALT levels in treated patients. An immune-mediated pathogenesis was suggested. Here, we evaluated whether HLA transgenic mice models could be used to investigate whether the expression of relevant HLA molecules was enough to reproduce the DILI effects in humans. In silico modelling performed in this study revealed association of both ximelagatran (pro-drug) and melagatran (active drug) to the antigen-presenting groove of the homology modelled HLA-DR7 molecule suggesting "altered repertoire" as a key initiating event driving development of DILI in humans. Transgenic mouse strains (tgms) expressing HLA of serotype HLA-DR7 (HLA-DRB1*0701, -DRA*0102), and HLA-DQ2 (HLA-DQB1*0202,-DQA1*0201) were created. These two lines were crossed with a human (h)CD4 transgenic line, generating the two tgms DR7xhCD4 and DQ2xhCD4. To investigate whether the DILI effects observed in humans could be reproduced in tgms, the mice were treated for 28 days with ximelagatran. Results revealed no signs of DILI when biomarkers for liver toxicity were measured and histopathology was evaluated. In the ximelagatran case, presence of relevant HLA-expression in a pre-clinical model did not fulfil the prerequisite for reproducing DILI observed in patients. Nonetheless, for the first time an HLA-transgenic mouse model has been investigated for use in HLA-associated DILI induced by a low molecular weight compound. This study shows that mimicking of genetic susceptibility, expressed as DILI-associated HLA-types in mice, is not sufficient for reproducing the complex pathogenesis leading to DILI in man.

Published
2017
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2. 4-aminobutyrate aminotransferase (ABAT): genetic and pharmacological evidence for an involvement in gastro esophageal reflux disease.

Author

Johan Jirholt, Bengt Asling, Paul Hammond, Geoffrey Davidson, Mikael Knutsson, Anna Walentinsson, Jörgen M Jensen, Anders Lehmann, Lars Agreus, and Maria Lagerström-Fermer

Subjects
Medicine, Science
Abstract

Gastro-esophageal reflux disease (GERD) is partly caused by genetic factors. The underlying susceptibility genes are currently unknown, with the exception of COL3A1. We used three independent GERD patient cohorts to identify GERD susceptibility genes. Thirty-six families, demonstrating dominant transmission of GERD were subjected to whole genome microsatellite genotyping and linkage analysis. Five linked regions were identified. Two families shared a linked region (LOD 3.9 and 2.0) on chromosome 16. We used two additional independent GERD patient cohorts, one consisting of 219 trios (affected child with parents) and the other an adult GERD case control cohort consisting of 256 cases and 485 controls, to validate individual genes in the linked region through association analysis. Sixty six single nucleotide polymorphism (SNP) markers distributed over the nine genes present in the linked region were genotyped in the independent GERD trio cohort. Transmission disequilibrium test analysis followed by multiple testing adjustments revealed a significant genetic association for one SNP located in an intron of the gene 4-aminobutyrate aminotransferase (ABAT) (P(adj) = 0.027). This association did not replicate in the adult case-control cohort, possibly due to the differences in ethnicity between the cohorts. Finally, using the selective ABAT inhibitor vigabatrin (γ-vinyl GABA) in a dog study, we were able to show a reduction of transient lower esophageal sphincter relaxations (TLESRs) by 57.3 ± 11.4 % (p = 0.007) and the reflux events from 3.1 ± 0.4 to 0.8 ± 0.4 (p = 0.007). Our results demonstrate the direct involvement of ABAT in pathways affecting lower esophageal sphincter (LES) control and identifies ABAT as a genetic risk factor for GERD.

Published
2011
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3. Late Breaking Abstract - The inflammasome cluster is linked with airway NETosis in COPD

Author

Lina Odqvist, Alix Berton, Thomas Southworth, Andrew Higham, Madeleine Ingelsten, Johan Jirholt, Sofia Lundin, Dave Singh, Magdalena Rhedin, Hoda Sharifian, Sofia Winslow, and Zala Jevnikar

Subjects
COPD, business.industry, Immunology, Medicine, Inflammasome, business, Airway, medicine.disease, Disease cluster, medicine.drug
Published
2021

4. AZD0284, a Potent, Selective, and Orally Bioavailable Inverse Agonist of Retinoic Acid Receptor-Related Orphan Receptor C2

Author

Roine I. Olsson, Rikard Pehrson, Rongfeng Chen, Jesper Malmberg, Anna Malmberg, Nafizal Hossain, Hanna Grindebacke, Mia Collins, Matti Lepistö, Yao Xiong, Nina Krutrök, Antonio Llinas, Thomas Hansson, Eva L. Hansson, Elisabeth Bäck, Anna Aagaard, Jane McPheat, Linda Thunberg, Sarah Lever, Agnes Leffler, Yafeng Xue, Stefan von Berg, Petter Svanberg, Frank Narjes, Marie Ramnegård, Glyn Hughes, and Johan Jirholt

Subjects
Male, Drug Inverse Agonism, Anti-Inflammatory Agents, Inflammation, Pharmacology, Isoindoles, chemistry.chemical_compound, Structure-Activity Relationship, Dogs, In vivo, Drug Discovery, medicine, Inverse agonist, Animals, Humans, Sulfones, Rats, Wistar, Orphan receptor, Imiquimod, Thymocytes, Molecular Structure, Chemistry, Isoindoline, Orphan Nuclear Receptors, Mice, Inbred C57BL, Retinoic acid receptor, Thymocyte, Nuclear receptor, Molecular Medicine, Th17 Cells, Female, medicine.symptom
Abstract

Inverse agonists of the nuclear receptor RORC2 have been widely pursued as a potential treatment for a variety of autoimmune diseases. We have discovered a novel series of isoindoline-based inverse agonists of the nuclear receptor RORC2, derived from our recently disclosed RORC2 inverse agonist 2. Extensive structure-activity relationship (SAR) studies resulted in AZD0284 (20), which combined potent inhibition of IL-17A secretion from primary human TH17 cells with excellent metabolic stability and good PK in preclinical species. In two preclinical in vivo studies, compound 20 reduced thymocyte numbers in mice and showed dose-dependent reduction of IL-17A containing γδ-T cells and of IL-17A and IL-22 RNA in the imiquimod induced inflammation model. Based on these data and a favorable safety profile, 20 was progressed to phase 1 clinical studies.

Published
2021

5. Potent and Orally Bioavailable Inverse Agonists of RORγt Resulting from Structure-Based Design

Author

Hanna Grindebacke, Frank Narjes, Eva L. Hansson, Yao Xiong, Antonio Llinas, Linda Thunberg, Jesper Malmberg, Stefan Tångefjord, Roine I. Olsson, Ge Hongbin, Rongfeng Chen, Yafeng Xue, Agnes Leffler, Hanna Leek, Thomas Hansson, Elisabeth Bäck, Jane McPheat, Nafizal Hossain, Matti Lepistö, Stefan von Berg, Johan Jirholt, and Anna Aagaard

Subjects
Models, Molecular, 0301 basic medicine, Drug Inverse Agonism, Protein Conformation, Stereochemistry, Administration, Oral, Biological Availability, Rodentia, Crystallography, X-Ray, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Amide, Acetamides, Drug Discovery, Animals, Humans, Inverse agonist, Structure–activity relationship, Tissue Distribution, Binding site, Cells, Cultured, Orphan receptor, Binding Sites, Molecular Structure, Interleukin-17, Nuclear Receptor Subfamily 1, Group F, Member 3, Retinoic acid receptor, 030104 developmental biology, chemistry, Drug Design, Th17 Cells, Molecular Medicine, Acetamide, Protein Binding
Abstract

Retinoic acid receptor related orphan receptor γt (RORγt), has been identified as the master regulator of TH17-cell function and development, making it an attractive target for the treatment of autoimmune diseases by a small-molecule approach. Herein, we describe our investigations on a series of 4-aryl-thienyl acetamides, which were guided by insights from X-ray cocrystal structures. Efforts in targeting the cofactor-recruitment site from the 4-aryl group on the thiophene led to a series of potent binders with nanomolar activity in a primary human-TH17-cell assay. The observation of a DMSO molecule binding in a subpocket outside the LBD inspired the introduction of an acetamide into the benzylic position of these compounds. Hereby, a hydrogen-bond interaction of the introduced acetamide oxygen with the backbone amide of Glu379 was established. This greatly enhanced the cellular activity of previously weakly cell-active compounds. The best compounds combined potent inhibition of IL-17 release with favorab...

Published
2018

6. Discovery of Potent and Orally Bioavailable Inverse Agonists of the Retinoic Acid Receptor-Related Orphan Receptor C2

Author

Stefan von Berg, Yafeng Xue, Mia Collins, Antonio Llinas, Roine I. Olsson, Torbjörn Halvarsson, Maria Lindskog, Jesper Malmberg, Johan Jirholt, Nina Krutrök, Marie Ramnegård, Marie Brännström, Anders Lundqvist, Matti Lepistö, Anna Aagaard, Jane McPheat, Eva L. Hansson, Rongfeng Chen, Yao Xiong, Thomas G. Hansson, and Frank Narjes

Subjects
Organic Chemistry, Drug Discovery, Biochemistry
Abstract

[Image: see text] The further optimization of a recently disclosed series of inverse agonists of the nuclear receptor RORC2 is described. Investigations into the left-hand side of compound 1, guided by X-ray crystal structures, led to the substitution of the 4-aryl-thiophenyl residue with the hexafluoro-2-phenyl-propan-2-ol moiety. This change resulted in to compound 28, which combined improved drug-like properties with good cell potency and a significantly lower dose, using an early dose to man prediction. Target engagement in vivo was demonstrated in the thymus of mice by a reduction in the number of double positive T cells after oral dosing.

Published
2019

7. Retinoid-related orphan receptor γ (RORγ) adult induced knockout mice develop lymphoblastic lymphoma

Author

Camilla Johansson, Magnus Söderberg, Jenny Börjesson, Jorrit J. Hornberg, Marie Ramnegård, Maria Rehnberg, Maria Liljevald, Donatella Luciani, Johan Jirholt, Ulf Andersson, Lena Brändén, David J. Keeling, Anna-Karin Sjögren, Xiufeng Xu, Nina Krutrök, and Mikael Bjursell

Subjects
Male, Mice, Knockout, 0301 basic medicine, Immunology, Lymphoblastic lymphoma, Nuclear Receptor Subfamily 1, Group F, Member 3, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Biology, medicine.disease, Autoimmune Diseases, Lymphoma, Mice, 03 medical and health sciences, 030104 developmental biology, Immune system, Nuclear receptor, RAR-related orphan receptor gamma, Knockout mouse, medicine, Animals, Th17 Cells, Immunology and Allergy, CD8, Gene knockout
Abstract

RORγ is a nuclear hormone receptor which controls polarization of naive CD4+ T-cells into proinflammatory Th17 cells. Pharmacological antagonism of RORγ has therapeutic potential for autoimmune diseases; however, this mechanism may potentially carry target-related safety risks, as mice deficient in Rorc, the gene encoding RORγ, develop T-cell lymphoma with 50% frequency. Due to the requirement of RORγ during development, the Rorc knockout (KO) animals lack secondary lymphoid organs and have a dysregulation in the generation of CD4+ and CD8+ T cells. We wanted to extend the evaluation of RORγ deficiency to address the question whether lymphomas, similar to those observed in the Rorc KO, would develop in an animal with an otherwise intact adult immune system. Accordingly, we designed a conditional RORγ knockout mouse (Rorc CKO) where the Rorc locus could be deleted in adult animals. Based on these studies we can confirm that these animals also develop lymphoma in a similar time frame as embryonic Rorc knockouts. This study also suggests that in animals where the gene deletion is incomplete, the thymus undergoes a rapid selection process replacing Rorc deficient cells with remnant thymocytes carrying a functional Rorc locus and that subsequently, these animals do not develop lymphoblastic lymphoma.

Published
2016

9. Benzoxazepines Achieve Potent Suppression of IL-17 Release in Human T-Helper 17 (TH17) Cells through an Induced-Fit Binding Mode to the Nuclear Receptor RORγ

Author

Rongfeng Chen, Hanna Grindebacke, Pia Hansson, Agnes Leffler, Yafeng Xue, Stefan von Berg, Roine I. Olsson, Hongbin Ge, Eva L. Hansson, Thomas Hansson, Jane McPheat, Johan Jirholt, Yao Xiong, Jenny Bernström, Frank Narjes, and Anna Aagaard

Subjects
Models, Molecular, 0301 basic medicine, Agonist, Stereochemistry, medicine.drug_class, Biochemistry, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, RAR-related orphan receptor gamma, Drug Discovery, medicine, Humans, Inverse agonist, Structure–activity relationship, General Pharmacology, Toxicology and Pharmaceutics, Benzamide, Pharmacology, Orphan receptor, Binding Sites, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Interleukin-17, Organic Chemistry, Nuclear Receptor Subfamily 1, Group F, Member 3, Oxazepines, 030104 developmental biology, Mechanism of action, Nuclear receptor, Th17 Cells, Molecular Medicine, medicine.symptom, Protein Binding
Abstract

RORγt, an isoform of the retinoic acid-related orphan receptor gamma (RORc, RORγ), has been identified as the master regulator of T-helper 17 (TH 17) cell function and development, making it an attractive target for the treatment of autoimmune diseases. Validation for this target comes from antibodies targeting interleukin-17 (IL-17), the signature cytokine produced by TH 17 cells, which have shown impressive results in clinical trials. Through focused screening of our compound collection, we identified a series of N-sulfonylated benzoxazepines, which displayed micromolar affinity for the RORγ ligand-binding domain (LBD) in a radioligand binding assay. Optimization of these initial hits resulted in potent binders, which dose-dependently decreased the ability of the RORγ-LBD to interact with a peptide derived from steroid receptor coactivator 1, and inhibited the release of IL-17 secretion from isolated and cultured human TH 17 cells with nanomolar potency. A cocrystal structure of inverse agonist 15 (2-chloro-6-fluoro-N-(4-{[3-(trifluoromethyl)phenyl]sulfonyl}-2,3,4,5-tetrahydro-1,4-benzoxazepin-7-yl)benzamide) bound to the RORγ-LBD illustrated that both hydrophobic interactions, leading to an induced fit around the substituted benzamide moiety of 15, as well as a hydrogen bond from the amide NH to His479 seemed to be important for the mechanism of action. This structure is compared with the structure of agonist 25 (N-(2-fluorophenyl)-4-[(4-fluorophenyl)sulfonyl]-2,3,4,5-tetrahydro-1,4-benzoxazepin-6-amine ) and structures of other known RORγ modulators.

Published
2015

10. HLA-DR7 and HLA-DQ2 : Transgenic mouse strains tested as a model system for ximelagatran hepatotoxicity

Author

Klara Martinsson, Hanna Lundgren, Daniel Mucs, Per Hultman, Johan Jirholt, Said Havarinasab, Karin Cederbrant, and Katja Madeyski-Bengtson

Subjects
0301 basic medicine, Male, Benzylamines, Ximelagatran, Physiology, HLA-DR7 Antigen, lcsh:Medicine, Pharmacology, Biochemistry, Pathogenesis, Major Histocompatibility Complex, White Blood Cells, 0302 clinical medicine, Animal Cells, Immune Physiology, Medicine and Health Sciences, Lymphocytes, lcsh:Science, Immune Response, Multidisciplinary, biology, T Cells, HLA-DQ2, Animal Models, Farmakologi och toxikologi, Body Fluids, Molecular Docking Simulation, Phenotype, Blood, Experimental Organism Systems, 030220 oncology & carcinogenesis, Female, Chemical and Drug Induced Liver Injury, Cellular Types, Anatomy, medicine.drug, Research Article, Genetically modified mouse, Drug Research and Development, Immune Cells, Immunology, Mice, Transgenic, Mouse Models, Human leukocyte antigen, Pharmacology and Toxicology, Major histocompatibility complex, Research and Analysis Methods, Blood Plasma, Cell Line, 03 medical and health sciences, Model Organisms, HLA-DQ Antigens, Genetic predisposition, medicine, Animals, Humans, Blood Cells, lcsh:R, Biology and Life Sciences, Cell Biology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Alanine transaminase, biology.protein, Azetidines, lcsh:Q, Clinical Immunology, Clinical Medicine, Spleen, Biomarkers
Abstract

The oral thrombin inhibitor ximelagatran was withdrawn in the late clinical trial phase because it adversely affected the liver. In approximately 8% of treated patients, drug-induced liver injury (DILI) was expressed as transient alanine transaminase (ALT) elevations. No evidence of DILI had been revealed in the pre-clinical in vivo studies. A whole genome scan study performed on the clinical study material identified a strong genetic association between the major histocompatibility complex alleles for human leucocyte antigens (HLA) (HLA-DR7 and HLA-DQ2) and elevated ALT levels in treated patients. An immunemediated pathogenesis was suggested. Here, we evaluated whether HLA transgenic mice models could be used to investigate whether the expression of relevant HLA molecules was enough to reproduce the DILI effects in humans. In silico modelling performed in this study revealed association of both ximelagatran (pro-drug) and melagatran (active drug) to the antigen-presenting groove of the homology modelled HLA-DR7 molecule suggesting "altered repertoire" as a key initiating event driving development of DILI in humans. Transgenic mouse strains (tgms) expressing HLA of serotype HLA-DR7 (HLA-DRB1*0701, -DRA*0102), and HLA-DQ2 (HLA-DQB1*0202, -DQA1*0201) were created. These two lines were crossed with a human (h) CD4 transgenic line, generating the two tgms DR7xhCD4 and DQ2xhCD4. To investigate whether the DILI effects observed in humans could be reproduced in tgms, the mice were treated for 28 days with ximelagatran. Results revealed no signs of DILI when biomarkers for liver toxicity were measured and histopathology was evaluated. In the ximelagatran case, presence of relevant HLA-expression in a preclinical model did not fulfil the prerequisite for reproducing DILI observed in patients. Nonetheless, for the first time an HLA-transgenic mouse model has been investigated for use in HLA-associated DILI induced by a low molecular weight compound. This study shows that mimicking of genetic susceptibility, expressed as DILI-associated HLA-types in mice, is not sufficient for reproducing the complex pathogenesis leading to DILI in man. Funding Agencies|AstraZeneca; AstraZeneca R&D as part of safety problem-solving activities initiated for ximelagatran (Exanta(R))

Published
2017

11. The role of lL-17 in the OVA-LPS driven model of lung inflammation

Author

Maria Rehnberg, Linda Yrlid, Johan Jirholt, Nina Krutrök, and Marie Ramnegård

Subjects
education.field_of_study, Lung, biology, business.industry, T cell, Population, Inflammation, respiratory system, medicine.disease, Staining, Ovalbumin, medicine.anatomical_structure, Immunology, biology.protein, medicine, medicine.symptom, Antibody, education, business, Asthma
Abstract

Introduction: Classical theory suggests that asthma is driven by a Th2 inflammatory response in the lung. Although this is true for many asthmatics it is becoming clear that in others, disease is driven by more diverse T cell subsets. Aim: To develop and characterise a model of ovalbumin (OVA) and LPS induced inflammation that may mimic processes involved in driving disease in Th2 low asthmatics. Methods: Female C57BL/6 mice were sensitized intratracheally with 100µg OVA with 1µg LPS in 50µl saline at day 0 and day 6. At day 13 the animals were challenged with an aerosol of 1% OVA in PBS for one hour. Animals were terminated at day 15 and BALF and lung were collected and prepared for flow cytometric staining. In a separate experiment an anti-IL-17 antibody was dosed subcutaneously at day 0, 4, 8 and 12. Results: Infiltrating cells in the lung tissue were composed of TCRb+ cells (45%, mainly CD4+ cells) and non-T-non-B cells. Within the CD4+ population the biggest difference was found in the RORgt and the T-bet expressing population. Very few GATA-3+ cells were found. Total cell numbers as well as neutrophil counts were significantly increased in BALF whereas the number of eosinophils was unchanged. Given the increased RORgt+ cells we investigated the effect of an anti-IL-17 antibody. In BALF, total cell count and neutrophils were reduced. In lung tissue, we observed a reduction of TCRb+ cells, a slight reduction of CD4+ cells, RORgt+ cells and IL-17 (50%). Conclusions We describe the development of an OVA LPS driven model of airway inflammation which demonstrates a mixed Th1/Th17 driven lung inflammation. We believe this model could be useful to examine the effects of therapies targeting Th17 driven inflammation in asthma.

Published
2015

12. Genetic linkage analysis of collagen-induced arthritis in the mouse

Author

Johan Jirholt, Andrew D. Cook, Tesfai Emahazion, Liselotte Jansson, Mats Sundvall, Ulf Pettersson, Niklas Nordquist, and Rikard Holmdahl

Subjects
Male, musculoskeletal diseases, Genetic Linkage, Immunology, Arthritis, Locus (genetics), Major histocompatibility complex, Arthritis, Rheumatoid, Mice, medicine, Animals, Immunology and Allergy, Genetic Predisposition to Disease, Genetic Testing, Chromosome 13, Genetics, biology, Chromosome Mapping, medicine.disease, Chromosome 17 (human), Disease Models, Animal, Chromosome 3, biology.protein, Microsatellite, Female, Collagen, Gene polymorphism, Microsatellite Repeats
Abstract

The genetic susceptibility to collagen-induced arthritis (CIA) in mice, the most commonly used model for rheumatoid arthritis, has been analyzed. The highly susceptible B10.RIII strain was crossed with the resistant RIIIS/J strain and the F2 intercross mice were subjected to genomic screening using microsatellite markers. These strains share the MHC region on chromosome 17, known to be of importance in CIA (this locus is named Mcia1). The same cross has earlier been used to map the major genes outside the MHC controlling chronic relapsing experimental allergic encephalomyelitis (EAE). It was found that the major locus controlling CIA (Mcia2; lod 4.12) was located on chromosome 3 in the same region as one of the major loci controlling EAE (Eae3). The linkage was reproduced in a mouse strain in which the locus was isolated on the B10.RIII background at the N4I2 generation. A second putative locus was identified on chromosome 13 (lod 3.13). The present finding identifies new loci outside the MHC controlling CIA and provides evidence that mouse CIA is controlled by polymorphic genes.

Published
1998

13. B cell-deficient mice do not develop type II collagen-induced arthritis (CIA)

Author

Liselotte Jansson, Rikard Holmdahl, Johan Jirholt, and Lars Svensson

Subjects
Male, musculoskeletal diseases, Ratón, T-Lymphocytes, Immunology, Type II collagen, Arthritis, chemical and pharmacologic phenomena, macromolecular substances, Lymphocyte Activation, medicine.disease_cause, Autoimmunity, Pathogenesis, Mice, Animals, Immunology and Allergy, Medicine, skin and connective tissue diseases, Gene, B cell, Autoimmune disease, B-Lymphocytes, business.industry, medicine.disease, Arthritis, Experimental, Rats, Mice, Inbred C57BL, medicine.anatomical_structure, Original Article, Cattle, Collagen, business
Abstract

SUMMARYTo investigate the role of B cells in the development of CIA, a model for rheumatoid arthritis, we investigated susceptibility to CIA in mice lacking B cells due to the deletion of the IgM heavy chain gene (μMT). The μMT deletion was backcrossed into two different CIA-susceptible strains, B10.Q and B10.RIII. Two different variants of the CIA model are inducible in these strains: in B10.Q with rat type II collagen (CII) and in B10.RIII with bovine CII. Homozygous deletion of the IgM gene led to the absence of B cells and dramatically reduced immunoglobulin levels compared with wild-type mice. The deletion of IgM totally abrogated development of CIA in both strains, although the anti-CII T cell response did not differ between the μMT and wild-type controls. We conclude that B cells play a crucial role in the development of CIA.

Published
1998

14. Back Cover: Benzoxazepines Achieve Potent Suppression of IL-17 Release in Human T-Helper 17 (TH17) Cells through an Induced-Fit Binding Mode to the Nuclear Receptor RORγ (ChemMedChem 2/2016)

Author

Eva L. Hansson, Johan Jirholt, Yao Xiong, Jenny Bernström, Roine I. Olsson, Hongbin Ge, Rongfeng Chen, Hanna Grindebacke, Frank Narjes, Anna Aagaard, Thomas Hansson, Stefan von Berg, Pia Hansson, Agnes Leffler, Yafeng Xue, and Jane McPheat

Subjects
Pharmacology, Nuclear receptor, Chemistry, Stereochemistry, Organic Chemistry, Drug Discovery, Molecular Medicine, Inverse agonist, Cover (algebra), Interleukin 17, General Pharmacology, Toxicology and Pharmaceutics, Biochemistry
Published
2016

15. Collagen type III alpha I is a gastro-oesophageal reflux disease susceptibility gene and a male risk factor for hiatus hernia

Author

Lars Agréus, Johan Jirholt, Bengt Åsling, Anders Lehmann, Maria Lagerström-Fermér, Mikael Knutsson, Geoff Davidson, Paul Hammond, and Anna Walentinsson

Subjects
Male, medicine.medical_specialty, Candidate gene, Collagen, type III, alpha 1, Adolescent, Genotype, DNA Mutational Analysis, Single-nucleotide polymorphism, Gastroenterology, Polymorphism, Single Nucleotide, Hiatal hernia, Esophagus, Sex Factors, Risk Factors, Internal medicine, medicine, otorhinolaryngologic diseases, Humans, Genetic Predisposition to Disease, Child, Genetic association, business.industry, digestive, oral, and skin physiology, Case-control study, Chromosome Mapping, Infant, medicine.disease, digestive system diseases, Oesophagus, Collagen Type III, Hernia, Hiatal, Gastrointestinal disorder, Case-Control Studies, Child, Preschool, Cohort, Gastroesophageal Reflux, Female, business
Abstract

Background and objectives: Gastro-oesophageal reflux disease (GORD) is a common gastrointestinal disorder with a genetic component. Our aim was to identify genetic factors associated with GORD. Patients and methods: Four separate patient cohorts were analysed using a step-wise approach. (1) Whole genome linkage analysis was performed in 36 families. (2) Candidate genes were tested for GORD association in a trio cohort. (3) Genetic association was replicated in a case–control cohort. We also investigated genetic association to hiatus hernia (HH). (4) Protein expression was analysed in oesophageal biopsies. Results: A region on chromosome 2, containing collagen type III alpha 1 (COL3A1), was identified (LOD = 3.3) in families with dominant transmission of GORD, stratified for hiatus hernia (HH). COL3A1 showed significant association with GORD in an independent paediatric trio cohort (p corr = 0.003). The association was male specific (p corr = 0.018). The COL3A1 association was replicated in an independent adult case control cohort (p corr = 0.022). Moreover, male specific association to HH (p corr = 0.019) was found for a SNP not associated to GORD. Collagen type III protein was more abundant in oesophageal biopsies from male patients with GORD (p = 0.03). Conclusion: COL3A1 is a disease-associated gene in both paediatric and adult GORD. Furthermore, we show that COL3A1 is genetically associated with HH in adult males. The GORD- and HH-associated alleles are different, indicating two separate mechanisms leading to disease. Our data provides new insight into GORD aetiology, identifying a connective tissue component and indicating a tissue remodelling mechanism in GORD. Our results implicate gender differences in the genetic risk for both for GORD and HH.

Published
2009

16. Identification of susceptibility genes for experimental autoimmune encephalomyelitis that overcome the effect of protective alleles at the eae2 locus

Author

Anna-Karin B. Lindqvist, Jenny C Karlsson, Rikard Holmdahl, Johan Jirholt, and Åsa Andersson

Subjects
Genetics, Encephalomyelitis, Autoimmune, Experimental, Genetic Linkage, Immunology, Congenic, Chromosome Mapping, Locus (genetics), Mice, Inbred Strains, General Medicine, Biology, Quantitative trait locus, Chromosome 15, Mice, Genetic linkage, Multigene Family, Genotype, Immunology and Allergy, Animals, Female, Genetic Predisposition to Disease, Allele, Gene
Abstract

We have previously identified a locus on mouse chromosome 15 (eae2) that regulates susceptibility to experimental autoimmune encephalomyelitis in a cross between the susceptible strain B10.RIII and the resistant strain RIIIS/J. In an effort to verify the protective effect from having two RIIIS/J alleles at eae2, the resistant locus was bred into the susceptible strain in homozygous form. However, the expected effect was not as clear as in the original study. This might be due to an epistatic effect conferred by several unidentified genes in the genome of the resistant strain or due to the environment by genotype interactions, possibly overcoming the effect of protective alleles at eae2. To further the genetic understanding in this disease, a genome-wide linkage screening approach was employed on an F(2) intercross that carried the protective allele at eae2in homozygous form while the rest of the genome segregated between the B10.RIII and RIIIS/J strains as in the original investigation. In the present study we find one region on chromosome 7, not previously identified in this strain combination, that affects the disease at significant logarithm of the odds score and six regions showing suggestive evidence for linkage to disease phenotypes.

Published
2001

17. Screening of several H-2 congenic mouse strains identified H-2(q) mice as highly susceptible to MOG-induced EAE with minimal adjuvant requirement

Author

Erik Wallström, Tomas Olsson, Peter Kjellén, Rikard Holmdahl, Johan Jirholt, Hans Lassmann, Khairul-Bariah Abdul-Majid, Robert A. Harris, Andreas Stefferl, and Christine Stadelmann

Subjects
Encephalomyelitis, Autoimmune, Experimental, Encephalomyelitis, Immunology, Congenic, Epitopes, T-Lymphocyte, Pertussis toxin, Epitope, Myelin oligodendrocyte glycoprotein, Mice, Mice, Congenic, Adjuvants, Immunologic, immune system diseases, Genotype, medicine, Immunology and Allergy, Animals, Virulence Factors, Bordetella, Autoantibodies, biology, Immunodominant Epitopes, Multiple sclerosis, Macrophages, hemic and immune systems, medicine.disease, Peptide Fragments, nervous system diseases, Mice, Inbred C57BL, Disease Models, Animal, Myelin-Associated Glycoprotein, nervous system, Neurology, Pertussis Toxin, Spinal Cord, Mice, Inbred DBA, biology.protein, Experimental pathology, Immunization, Myelin-Oligodendrocyte Glycoprotein, Neurology (clinical), Disease Susceptibility, Lymph Nodes, Cell Division, Myelin Proteins, Spleen
Abstract

We identified H-2(q) as a susceptible genotype for MOG-induced EAE by systematic screening of a series of H-2 congenic B10 mouse strains. A series of H-2(q)-bearing strains with divergent gene backgrounds were subsequently investigated. DBA/1 mice were highly susceptible to MOG(1-125)- and MOG(79-96)-induced EAE in the absence of pertussis toxin. Immunisation with MOG(1-125) and MOG(79-96) induced an autoreactive T-cell response in DBA/1 mice. Brain histopathology revealed T-cell and macrophage-infiltrated lesions with associated demyelination. The important features which make this an appropriate model of human disease are high sensitivity to MOG and dependence of an immunodominant peptide region homologous to that implicated in multiple sclerosis.

Published
2000

19. Identification of murine loci associated with susceptibility to chronic experimental autoimmune encephalomyelitis

Author

Mats Sundvall, Johan Jirholt, Ulf Pettersson, Hai Tao Yang, Rikard Holmdahl, Åke Engström, and Liselotte Jansson

Subjects
Genetic Markers, Male, Encephalomyelitis, Autoimmune, Experimental, Genotype, Genetic Linkage, Encephalomyelitis, Molecular Sequence Data, chemical and pharmacologic phenomena, Locus (genetics), DNA, Satellite, Major histocompatibility complex, Chromosome 15, Mice, Species Specificity, Genetic linkage, Genetics, medicine, Animals, Amino Acid Sequence, Crosses, Genetic, biology, Experimental autoimmune encephalomyelitis, Chromosome Mapping, Myelin Basic Protein, medicine.disease, Peptide Fragments, Myelin basic protein, Phenotype, Chromosome 3, Immunology, biology.protein, Female, Immunization
Abstract

B10.RIII mice develop chronic and relapsing experimental autoimmune encephalomyelitis (EAE) after immunization with the myelin basic protein (MBP) peptide 89-101. The disease is associated with the major histocompatibility complex (MHC) (eae1). We have now investigated the importance of non-MHC regions for the EAE susceptibility in a cross between RIIIS/J and B10.RIII mice which share the MHC region but differ in disease susceptibility. Linkage analysis using microsatellite markers spanning the genome identified a region (eae2) on chromosome 15 which showed linkage to disease (P = 0.0002). Our data also suggest linkage to a second region (eae3) on chromosome 3 (P = 0.0024), and provide evidence for locus interactions between eae2 and eae3. These results provide clues to the genetic basis of multiple sclerosis.

Published
1995

21. 4-Aminobutyrate Aminotransferase (ABAT): Genetic and Pharmacological Evidence for an Involvement in Gastro Esophageal Reflux Disease

Author

Mikael Knutsson, Bengt Åsling, Jörgen Jensen, Anna Walentinsson, Anders Lehmann, Lars Agréus, Johan Jirholt, Maria Lagerström-Fermér, Geoffrey P. Davidson, and Paul Hammond

Subjects
Male, Heredity, Genetic Linkage, Gastroenterology, Esophageal Sphincter, Lower, Genetics, Multidisciplinary, Linkage (Genetics), Genomics, Animal Models, Transmission disequilibrium test, Genome Scans, Cohort, Gastroesophageal Reflux, Medicine, Female, Pediatric Gastroenterology, Research Article, Adult, Drugs and Devices, medicine.medical_specialty, Adolescent, Science, Single-nucleotide polymorphism, Gastroenterology and Hepatology, Biology, Dogs, Model Organisms, Esophagus, Genome Analysis Tools, Genetic linkage, Internal medicine, medicine, Animals, Humans, SNP, Genetic Predisposition to Disease, Genetic Association Studies, Genetic association, Case-control study, Reproducibility of Results, Human Genetics, Sequence Analysis, DNA, medicine.disease, digestive system diseases, Pharmacogenetics, 4-Aminobutyrate Transaminase, Case-Control Studies, Genetics of Disease, Genetic Polymorphism, GERD, Pharmacogenomics, Population Genetics
Abstract

Gastro-esophageal reflux disease (GERD) is partly caused by genetic factors. The underlying susceptibility genes are currently unknown, with the exception of COL3A1. We used three independent GERD patient cohorts to identify GERD susceptibility genes. Thirty-six families, demonstrating dominant transmission of GERD were subjected to whole genome microsatellite genotyping and linkage analysis. Five linked regions were identified. Two families shared a linked region (LOD 3.9 and 2.0) on chromosome 16. We used two additional independent GERD patient cohorts, one consisting of 219 trios (affected child with parents) and the other an adult GERD case control cohort consisting of 256 cases and 485 controls, to validate individual genes in the linked region through association analysis. Sixty six single nucleotide polymorphism (SNP) markers distributed over the nine genes present in the linked region were genotyped in the independent GERD trio cohort. Transmission disequilibrium test analysis followed by multiple testing adjustments revealed a significant genetic association for one SNP located in an intron of the gene 4-aminobutyrate aminotransferase (ABAT) (P(adj) = 0.027). This association did not replicate in the adult case-control cohort, possibly due to the differences in ethnicity between the cohorts. Finally, using the selective ABAT inhibitor vigabatrin (γ-vinyl GABA) in a dog study, we were able to show a reduction of transient lower esophageal sphincter relaxations (TLESRs) by 57.3 ± 11.4 % (p = 0.007) and the reflux events from 3.1 ± 0.4 to 0.8 ± 0.4 (p = 0.007). Our results demonstrate the direct involvement of ABAT in pathways affecting lower esophageal sphincter (LES) control and identifies ABAT as a genetic risk factor for GERD.

Published
2011

22. [Untitled]

Author

Rikard Holmdahl, Anna-Karin B. Lindqvist, and Johan Jirholt

Subjects
Genetics, medicine.medical_specialty, business.industry, Experimental model, Multifactorial disease, Arthritis, Disease, Quantitative trait locus, medicine.disease, Rheumatology, Rheumatoid arthritis, Internal medicine, Medicine, business, Gene
Abstract

The causes of rheumatoid arthritis (RA) are largely unknown. However, RA is most probably a multifactorial disease with contributions from genetic and environmental factors. Searches for genes that influence RA have been conducted in both human and experimental model materials. Both types of study have confirmed the polygenic inheritance of the disease. It has become clear that the features of RA complicate the human genetic studies. Animal models are therefore valuable tools for identifying genes and determining their pathogenic role in the disease. This is probably the fastest route towards unravelling the pathogenesisis of RA and developing new therapies.

Published
2001

23. Suggestive evidence for association of human chromosome 18q12-q21 and its orthologue on rat and mouse chromosome 18 with several autoimmune diseases

Author

Iain A. Eaves, Fleming Pociot, Francesca Coraddu, C. Ionesco-Tirgoviste, John A. Todd, Stephen Sawcer, Johan Jirholt, Kjersti S. Rønningen, Alastair Compston, Francesco Cucca, Tony R. Merriman, Rikard Holmdahl, Argyrios N. Theofilopoulos, Dwight H. Kono, Dag E. Undlien, Maria Giovanna Marrosu, Steve Laval, Steve Bain, Simon Broadley, Patrick Danoy, Constantin Polychronakos, Heather J. Cordell, Julian P.H. Shield, Chaim O. Jacob, Raffaella Buzzetti, Rachael A. Barber, Eva Tuomilehto-Wolf, Jaakko Tuomilehto, Paul Wordsworth, Jørn Nerup, and Jane Shatford

Subjects
Candidate gene, Multiple Sclerosis, Genetic Linkage, Endocrinology, Diabetes and Metabolism, Sequence Homology, Locus (genetics), Biology, medicine.disease_cause, Autoimmunity, Autoimmune Diseases, Arthritis, Rheumatoid, Mice, Chromosome 18, Genetic linkage, Internal Medicine, medicine, Animals, Humans, Genetic association, Genetics, Autoimmune disease, Haplotype, Chromosome Mapping, medicine.disease, Rats, Diabetes Mellitus, Type 1, Genes, DCC, Phenotype, Haplotypes, Chromosomes, Human, Pair 18, Microsatellite Repeats
Abstract

Some immune system disorders, such as type 1 diabetes, multiple sclerosis (MS), and rheumatoid arthritis (RA), share common features: the presence of autoantibodies and self-reactive T-cells, and a genetic association with the major histocompatibility complex. We have previously published evidence, from 1,708 families, for linkage and association of a haplotype of three markers in the D18S487 region of chromosome 18q21 with type 1 diabetes. Here, the three markers were typed in an independent set of 627 families and, although there was evidence for linkage (maximum logarithm of odds score [MLS] = 1.2; P = 0.02), no association was detected. Further linkage analysis revealed suggestive evidence for linkage of chromosome 18q21 to type 1 diabetes in 882 multiplex families (MLS = 2.2; lambdas = 1.2; P = 0.001), and by meta-analysis the orthologous region (also on chromosome 18) is linked to diabetes in rodents (P = 9 x 10(-4)). By meta-analysis, both human chromosome 18q12-q21 and the rodent orthologous region show positive evidence for linkage to an autoimmune phenotype (P = 0.004 and 2 x 10(-8), respectively, empirical P = 0.01 and 2 x 10(-4), respectively). In the diabetes-linked region of chromosome 18q12-q21, a candidate gene, deleted in colorectal carcinoma (DCC), was tested for association with human autoimmunity in 3,380 families with type 1 diabetes, MS, and RA. A haplotype ("2-10") of two newly characterized microsatellite markers within DCC showed evidence for association with autoimmunity (P = 5 x 10(-6)). Collectively, these data suggest that a locus (or loci) exists on human chromosome 18q12-q21 that influences multiple autoimmune diseases and that this association might be conserved between species.

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