Your search keyword '"Ellmerich S"' showing total 29 results

1. Dementia in the older population is associated with neocortex content of serum amyloid P component

Author

Ellmerich, S., Taylor, G.W., Richardson, C.D., Minett, T., Schmidt, A.F., Brayne, C., Matthews, F.E., Ince, P.G., Wharton, S.B., and Pepys, M.B.

Subjects

mental disorders

Abstract

Despite many reported associations, the direct cause of neurodegeneration responsible for cognitive loss in Alzheimer’s disease and some other common dementias is not known. The normal human plasma protein, serum amyloid P component, a constituent of all human fibrillar amyloid deposits and present on most neurofibrillary tangles, is cytotoxic for cerebral neurones in vitro and in experimental animals in vivo. The neocortical content of serum amyloid P component was immunoassayed in 157 subjects aged 65 or more with known dementia status at death, in the large scale, population-representative, brain donor cohort of the Cognitive Function and Ageing Study, which avoids the biases inherent in studies of predefined clinico-pathological groups. The serum amyloid P component values were significantly higher in individuals with dementia, independent of serum albumin content measured as a control for plasma in the cortex samples. The odds ratio for dementia at death in the high serum amyloid P component tertile was 5.24 (95% confidence interval 1.79–15.29) and was independent of Braak tangle stages and Thal amyloid-β phases of neuropathological severity. The strong and specific association of higher brain content of serum amyloid P component with dementia, independent of neuropathology, is consistent with a pathogenetic role in dementia.

Published

2021

2. A specific nanobody prevents amyloidogenesis of D76N β2-microglobulin in vitro and modifies its tissue distribution in vivo

Author

Raimondi, S., Porcari R., Pp, Mangione, ., Verona, G., Marcoux J., S, Giorgetti, ., Taylor, G. w., Ellmerich, S., Ballico, M., Zanini, S., Pardon, E., Al Shawi, R., Simons, J. p., Corazza, A., Fogolari, F., Leri, Manuela, Stefani, Massimo, Bucciantini, Monica, Gillmore, J. d., Hawkins, P. N., Valli, M., Stoppini, M., Robinson, C. v., Steyaert, J., Esposito, G, and Bellotti, V.

Subjects

nanobody, b2-microglobulina, amiloidosi

Published

2017

3. Promotion of intestinal carcinogenesis by Streptococcus bovis

Author

Ellmerich, S., primary, Scholler, M., additional, Duranton, B., additional, Gosse, F., additional, Galluser, M., additional, Klein, J.-P., additional, and Raul, F., additional

Published

2000

4. Increased surface toll-like receptor 2 expression in superantigen shock.

Author

Hopkins PA, Pridmore AC, Ellmerich S, Fraser JD, Russell HH, Read RC, and Sriskandan S

Published

2008

5. Sexual dimorphism in superantigen shock involves elevated TNF-alpha and TNF-alpha induced hepatic apoptosis.

Author

Faulkner L, Altmann DM, Ellmerich S, Huhtaniemi I, Stamp G, and Sriskandan S

Abstract

Rationale: There is conflicting evidence regarding sex differences in the outcome from severe sepsis and toxic shock. Superantigen-mediated toxic shock affects a higher proportion of female patients. Objectives: The objective of the current study was to investigate sexual dimorphism in superantigen-associated sepsis and in superantigen-mediated shock and to identify the key mechanisms responsible for this sex difference. Methods: We measured mortality and serum cytokines after induction of sepsis with isogenic superantigen-positive and superantigen-negative Streptococcus pyogenes in HLA class II transgenics. During superantigen-mediated toxic shock, we measured mortality, T-cell responses, systemic tumor necrosis factor (TNF)-alpha and TNF receptors, TNF-alpha-induced hepatocyte apoptosis, and conditioning of these responses by tamoxifen treatment. Measurements and Main Results: In both superantigen-associated sepsis and in superantigen-mediated shock, serum TNF-alpha was increased in females compared with males. This was not attributable to a detectable difference in splenic TNF-alpha transcription; rather, serum soluble TNF receptors were higher in males. Pretreatment of females with the estrogen receptor modulator tamoxifen increased serum soluble TNF receptors, reduced the early serum TNF-alpha response, and improved mortality in females challenged with staphylococcal enterotoxin B. Lethal superantigen shock was characterized by hepatocyte apoptosis, and was reproduced by injection of TNF-alpha. Females had enhanced susceptibility to TNF-alpha-mediated lethality. TNF-alpha-induced hepatocyte apoptosis was greater in females, and was reduced by tamoxifen pretreatment. Conclusions: Sexual dimorphism in experimental superantigen toxic shock results from increased systemic TNF-alpha in females, coupled with an increased susceptibility to TNF-alpha-induced hepatocyte apoptosis. Both processes are abrogated by estrogen receptor modulators. [ABSTRACT FROM AUTHOR]

Published

2007

6. C-reactive protein is essential for innate resistance to pneumococcal infection

Author

Simons, J P, Loeffler, J M, Al-Shawi, R, Ellmerich, S, Hutchinson, W L, Tennent, G A, Petrie, A, Raynes, J G, de Souza, J B, Lawrence, R A, Read, K D, Pepys, M B, Dundee, LSHTM, and UCL

7. Equilibrium contrast CMR for the detection of amyloidosis in mice

Author

Moon James C, Pepys Mark B, Ordidge Roger J, Hawkins Philip N, Al-Shawi Raya, Simons Paul, Ellmerich Stephan, Price Anthony N, Campbell Adrienne E, and Lythgoe Mark F

Subjects

Diseases of the circulatory (Cardiovascular) system, RC666-701

Published

2011

8. Genetic evidence for serum amyloid P component as a drug target in neurodegenerative disorders.

Author

Schmidt AF, Finan C, Chopade S, Ellmerich S, Rossor MN, Hingorani AD, and Pepys MB

Subjects

Humans, Alzheimer Disease genetics, Alzheimer Disease metabolism, Alzheimer Disease etiology, Polymorphism, Single Nucleotide, Genetic Predisposition to Disease, Mendelian Randomization Analysis, Biomarkers, tau Proteins metabolism, tau Proteins genetics, Lewy Body Disease genetics, Lewy Body Disease metabolism, Male, Female, Genome-Wide Association Study, Neurodegenerative Diseases genetics, Neurodegenerative Diseases etiology, Neurodegenerative Diseases metabolism, Serum Amyloid P-Component metabolism, Serum Amyloid P-Component genetics

Abstract

The mechanisms responsible for neuronal death causing cognitive loss in Alzheimer's disease (AD) and many other dementias are not known. Serum amyloid P component (SAP) is a constitutive plasma protein, which is cytotoxic for cerebral neurones and also promotes formation and persistence of cerebral A β amyloid and neurofibrillary tangles. Circulating SAP, which is produced exclusively by the liver, is normally almost completely excluded from the brain. Conditions increasing brain exposure to SAP increase dementia risk, consistent with a causative role in neurodegeneration. Furthermore, neocortex content of SAP is strongly and independently associated with dementia at death. Here, seeking genomic evidence for a causal link of SAP with neurodegeneration, we meta-analysed three genome-wide association studies of 44 288 participants, then conducted cis -Mendelian randomization assessment of associations with neurodegenerative diseases. Higher genetically instrumented plasma SAP concentrations were associated with AD (odds ratio 1.07, 95% confidence interval (CI) 1.02; 1.11, p = 1.8 × 10 -3 ), Lewy body dementia (odds ratio 1.37, 95%CI 1.19; 1.59, p = 1.5 × 10 -5 ) and plasma tau concentration (0.06 log 2 (ng l -1 ) 95%CI 0.03; 0.08, p = 4.55 × 10 -6 ). These genetic findings are consistent with neuropathogenicity of SAP. Depletion of SAP from the blood and the brain, by the safe, well tolerated, experimental drug miridesap may thus be neuroprotective.

Published

2024

9. Genetic evidence for serum amyloid P component as a drug target for treatment of neurodegenerative disorders.

Author

Schmidt AF, Finan C, Chopade S, Ellmerich S, Rossor MN, Hingorani AD, and Pepys MB

Abstract

The direct causes of neurodegeneration underlying Alzheimer's disease (AD) and many other dementias, are not known. Here we identify serum amyloid P component (SAP), a constitutive plasma protein normally excluded from the brain, as a potential drug target. After meta-analysis of three genome-wide association studies, comprising 44,288 participants, cis -Mendelian randomization showed that genes responsible for higher plasma SAP values are significantly associated with AD, Lewy body dementia and plasma tau concentration. These genetic findings are consistent with experimental evidence of SAP neurotoxicity and the strong, independent association of neocortex SAP content with dementia at death. Depletion of SAP from the blood and from the brain, as is provided by the safe, well tolerated, experimental drug, miridesap, may therefore contribute to treatment of neurodegeneration., Competing Interests: Competing interests: AFS and CF have received funding from NewAmsterdam Pharma for unrelated work. MBP is the inventor on expired patents on SAP depletion by miridesap (CPHPC). GlaxoSmithKline’s abandoned patents on an experimental miridesap prodrug are assigned to UCL spinout company, Pentraxin Therapeutics Ltd, founded and directed by MBP. The other authors have no competing interests.

Published

2023

10. Antibody-Associated Reversal of ATTR Amyloidosis-Related Cardiomyopathy.

Author

Fontana M, Gilbertson J, Verona G, Riefolo M, Slamova I, Leone O, Rowczenio D, Botcher N, Ioannou A, Patel RK, Razvi Y, Martinez-Naharro A, Whelan CJ, Venneri L, Duhlin A, Canetti D, Ellmerich S, Moon JC, Kellman P, Al-Shawi R, McCoy L, Simons JP, Hawkins PN, and Gillmore JD

Subjects

Humans, Antibodies immunology, Antibodies therapeutic use, Prealbumin, Amyloid Neuropathies, Familial complications, Amyloid Neuropathies, Familial drug therapy, Amyloidosis, Cardiomyopathies drug therapy, Cardiomyopathies etiology, Cardiomyopathies immunology

Published

2023

11. Plasmin activity promotes amyloid deposition in a transgenic model of human transthyretin amyloidosis.

Author

Slamova I, Adib R, Ellmerich S, Golos MR, Gilbertson JA, Botcher N, Canetti D, Taylor GW, Rendell N, Tennent GA, Verona G, Porcari R, Mangione PP, Gillmore JD, Pepys MB, Bellotti V, Hawkins PN, Al-Shawi R, and Simons JP

Subjects

Animals, Cardiomyopathies, Humans, Mice, Transgenic, Prealbumin metabolism, Protein Folding, Proteolysis, Amyloid metabolism, Amyloid Neuropathies, Familial metabolism, Fibrinolysin genetics, Fibrinolysin metabolism, Plaque, Amyloid metabolism

Abstract

Cardiac ATTR amyloidosis, a serious but much under-diagnosed form of cardiomyopathy, is caused by deposition of amyloid fibrils derived from the plasma protein transthyretin (TTR), but its pathogenesis is poorly understood and informative in vivo models have proved elusive. Here we report the generation of a mouse model of cardiac ATTR amyloidosis with transgenic expression of human TTR S52P . The model is characterised by substantial ATTR amyloid deposits in the heart and tongue. The amyloid fibrils contain both full-length human TTR protomers and the residue 49-127 cleavage fragment which are present in ATTR amyloidosis patients. Urokinase-type plasminogen activator (uPA) and plasmin are abundant within the cardiac and lingual amyloid deposits, which contain marked serine protease activity; knockout of α 2 -antiplasmin, the physiological inhibitor of plasmin, enhances amyloid formation. Together, these findings indicate that cardiac ATTR amyloid deposition involves local uPA-mediated generation of plasmin and cleavage of TTR, consistent with the previously described mechano-enzymatic hypothesis for cardiac ATTR amyloid formation. This experimental model of ATTR cardiomyopathy has potential to allow further investigations of the factors that influence human ATTR amyloid deposition and the development of new treatments., (© 2021. The Author(s).)

Published

2021

12. Dementia in the older population is associated with neocortex content of serum amyloid P component.

Author

Ellmerich S, Taylor GW, Richardson CD, Minett T, Schmidt AF, Brayne C, Matthews FE, Ince PG, Wharton SB, and Pepys MB

Abstract

Despite many reported associations, the direct cause of neurodegeneration responsible for cognitive loss in Alzheimer's disease and some other common dementias is not known. The normal human plasma protein, serum amyloid P component, a constituent of all human fibrillar amyloid deposits and present on most neurofibrillary tangles, is cytotoxic for cerebral neurones in vitro and in experimental animals in vivo . The neocortical content of serum amyloid P component was immunoassayed in 157 subjects aged 65 or more with known dementia status at death, in the large scale, population-representative, brain donor cohort of the Cognitive Function and Ageing Study, which avoids the biases inherent in studies of predefined clinico-pathological groups. The serum amyloid P component values were significantly higher in individuals with dementia, independent of serum albumin content measured as a control for plasma in the cortex samples. The odds ratio for dementia at death in the high serum amyloid P component tertile was 5.24 (95% confidence interval 1.79-15.29) and was independent of Braak tangle stages and Thal amyloid-β phases of neuropathological severity. The strong and specific association of higher brain content of serum amyloid P component with dementia, independent of neuropathology, is consistent with a pathogenetic role in dementia., (© The Author(s) (2021). Published by Oxford University Press on behalf of the Guarantors of Brain.)

Published

2021

13. Systemic Exosomal Delivery of shRNA Minicircles Prevents Parkinsonian Pathology.

Author

Izco M, Blesa J, Schleef M, Schmeer M, Porcari R, Al-Shawi R, Ellmerich S, de Toro M, Gardiner C, Seow Y, Reinares-Sebastian A, Forcen R, Simons JP, Bellotti V, Cooper JM, and Alvarez-Erviti L

Subjects

Animals, Gene Expression Regulation, Genetic Therapy, Humans, Male, Mice, Mice, Inbred C3H, Mice, Inbred C57BL, Mice, Transgenic, Parkinson Disease genetics, Parkinson Disease pathology, alpha-Synuclein antagonists & inhibitors, alpha-Synuclein genetics, Brain metabolism, Disease Models, Animal, Drug Delivery Systems, Exosomes genetics, Parkinson Disease therapy, RNA, Small Interfering genetics, alpha-Synuclein administration & dosage

Abstract

The development of new therapies to slow down or halt the progression of Parkinson's disease is a health care priority. A key pathological feature is the presence of alpha-synuclein aggregates, and there is increasing evidence that alpha-synuclein propagation plays a central role in disease progression. Consequently, the downregulation of alpha-synuclein is a potential therapeutic target. As a chronic disease, the ideal treatment will be minimally invasive and effective in the long-term. Knockdown of gene expression has clear potential, and siRNAs specific to alpha-synuclein have been designed; however, the efficacy of siRNA treatment is limited by its short-term efficacy. To combat this, we designed shRNA minicircles (shRNA-MCs), with the potential for prolonged effectiveness, and used RVG-exosomes as the vehicle for specific delivery into the brain. We optimized this system using transgenic mice expressing GFP and demonstrated its ability to downregulate GFP protein expression in the brain for up to 6 weeks. RVG-exosomes were used to deliver anti-alpha-synuclein shRNA-MC therapy to the alpha-synuclein preformed-fibril-induced model of parkinsonism. This therapy decreased alpha-synuclein aggregation, reduced the loss of dopaminergic neurons, and improved the clinical symptoms. Our results confirm the therapeutic potential of shRNA-MCs delivered by RVG-exosomes for long-term treatment of neurodegenerative diseases., (Copyright © 2019 The American Society of Gene and Cell Therapy. Published by Elsevier Inc. All rights reserved.)

Published

2019

14. A specific nanobody prevents amyloidogenesis of D76N β 2 -microglobulin in vitro and modifies its tissue distribution in vivo.

Author

Raimondi S, Porcari R, Mangione PP, Verona G, Marcoux J, Giorgetti S, Taylor GW, Ellmerich S, Ballico M, Zanini S, Pardon E, Al-Shawi R, Simons JP, Corazza A, Fogolari F, Leri M, Stefani M, Bucciantini M, Gillmore JD, Hawkins PN, Valli M, Stoppini M, Robinson CV, Steyaert J, Esposito G, and Bellotti V

Subjects

Amyloid drug effects, Amyloid immunology, Amyloid metabolism, Amyloidosis metabolism, Amyloidosis prevention & control, Animals, Cell Line, Tumor, Doxycycline pharmacokinetics, Doxycycline pharmacology, Humans, Mice, 129 Strain, Mice, Knockout, Mutation, Missense, Protein Aggregates drug effects, Protein Aggregation, Pathological prevention & control, Single-Domain Antibodies metabolism, Single-Domain Antibodies pharmacology, Tissue Distribution drug effects, beta 2-Microglobulin genetics, beta 2-Microglobulin metabolism, Amyloidosis immunology, Single-Domain Antibodies immunology, beta 2-Microglobulin immunology

Abstract

Systemic amyloidosis is caused by misfolding and aggregation of globular proteins in vivo for which effective treatments are urgently needed. Inhibition of protein self-aggregation represents an attractive therapeutic strategy. Studies on the amyloidogenic variant of β 2 -microglobulin, D76N, causing hereditary systemic amyloidosis, have become particularly relevant since fibrils are formed in vitro in physiologically relevant conditions. Here we compare the potency of two previously described inhibitors of wild type β 2 -microglobulin fibrillogenesis, doxycycline and single domain antibodies (nanobodies). The β 2 -microglobulin -binding nanobody, Nb24, more potently inhibits D76N β 2 -microglobulin fibrillogenesis than doxycycline with complete abrogation of fibril formation. In β 2 -microglobulin knock out mice, the D76N β 2 -microglobulin/ Nb24 pre-formed complex, is cleared from the circulation at the same rate as the uncomplexed protein; however, the analysis of tissue distribution reveals that the interaction with the antibody reduces the concentration of the variant protein in the heart but does not modify the tissue distribution of wild type β 2 -microglobulin. These findings strongly support the potential therapeutic use of this antibody in the treatment of systemic amyloidosis.

Published

2017

15. Amyloid persistence in decellularized liver: biochemical and histopathological characterization.

Author

Mazza G, Simons JP, Al-Shawi R, Ellmerich S, Urbani L, Giorgetti S, Taylor GW, Gilbertson JA, Hall AR, Al-Akkad W, Dhar D, Hawkins PN, De Coppi P, Pinzani M, Bellotti V, and Mangione PP

Subjects

Amino Acid Sequence, Amyloid chemistry, Animals, Extracellular Matrix physiology, Female, Immunoglobulin Light-chain Amyloidosis, Liver chemistry, Mice, Inbred C57BL, Mice, Transgenic, Molecular Sequence Data, Serum Amyloid A Protein chemistry, Amyloid physiology, Amyloidosis pathology, Liver pathology, Liver Diseases pathology

Abstract

Systemic amyloidoses are a group of debilitating and often fatal diseases in which fibrillar protein aggregates are deposited in the extracellular spaces of a range of tissues. The molecular basis of amyloid formation and tissue localization is still unclear. Although it is likely that the extracellular matrix (ECM) plays an important role in amyloid deposition, this interaction is largely unexplored, mostly because current analytical approaches may alter the delicate and complicated three-dimensional architecture of both ECM and amyloid. We describe here a decellularization procedure for the amyloidotic mouse liver which allows high-resolution visualization of the interactions between amyloid and the constitutive fibers of the extracellular matrix. The primary structure of the fibrillar proteins remains intact and the amyloid fibrils retain their amyloid enhancing factor activity.

Published

2016

16. Bifunctional crosslinking ligands for transthyretin.

Author

Mangione PP, Deroo S, Ellmerich S, Bellotti V, Kolstoe S, Wood SP, Robinson CV, Smith MD, Tennent GA, Broadbridge RJ, Council CE, Thurston JR, Steadman VA, Vong AK, Swain CJ, Pepys MB, and Taylor GW

Subjects

Animals, Binding Sites, Humans, Mice, Mice, Inbred C57BL, Models, Molecular, Piperidines chemistry, Prealbumin chemistry, Protein Structure, Quaternary, Thyroxine chemistry, Thyroxine metabolism, Cross-Linking Reagents chemistry, Ligands, Prealbumin metabolism

Abstract

Wild-type and variant forms of transthyretin (TTR), a normal plasma protein, are amyloidogenic and can be deposited in the tissues as amyloid fibrils causing acquired and hereditary systemic TTR amyloidosis, a debilitating and usually fatal disease. Reduction in the abundance of amyloid fibril precursor proteins arrests amyloid deposition and halts disease progression in all forms of amyloidosis including TTR type. Our previous demonstration that circulating serum amyloid P component (SAP) is efficiently depleted by administration of a specific small molecule ligand compound, that non-covalently crosslinks pairs of SAP molecules, suggested that TTR may be also amenable to this approach. We first confirmed that chemically crosslinked human TTR is rapidly cleared from the circulation in mice. In order to crosslink pairs of TTR molecules, promote their accelerated clearance and thus therapeutically deplete plasma TTR, we prepared a range of bivalent specific ligands for the thyroxine binding sites of TTR. Non-covalently bound human TTR-ligand complexes were formed that were stable in vitro and in vivo, but they were not cleared from the plasma of mice in vivo more rapidly than native uncomplexed TTR. Therapeutic depletion of circulating TTR will require additional mechanisms., (© 2015 The Authors.)

Published

2015

17. C-reactive protein is essential for innate resistance to pneumococcal infection.

Author

Simons JP, Loeffler JM, Al-Shawi R, Ellmerich S, Hutchinson WL, Tennent GA, Petrie A, Raynes JG, de Souza JB, Lawrence RA, Read KD, and Pepys MB

Subjects

Animals, C-Reactive Protein deficiency, C-Reactive Protein genetics, Humans, Mice, Mice, Knockout, Phenotype, C-Reactive Protein immunology, Immunity, Innate, Pneumococcal Infections immunology, Streptococcus pneumoniae immunology

Abstract

No deficiency of human C-reactive protein (CRP), or even structural polymorphism of the protein, has yet been reported so its physiological role is not known. Here we show for the first time that CRP-deficient mice are remarkably susceptible to Streptococcus pneumoniae infection and are protected by reconstitution with isolated pure human CRP, or by anti-pneumococcal antibodies. Autologous mouse CRP is evidently essential for innate resistance to pneumococcal infection before antibodies are produced. Our findings are consistent with the significant association between clinical pneumococcal infection and non-coding human CRP gene polymorphisms which affect CRP expression. Deficiency or loss of function variation in CRP may therefore be lethal at the first early-life encounter with this ubiquitous virulent pathogen, explaining the invariant presence and structure of CRP in human adults., (© 2014 The Authors. Immunology published by John Wiley & Sons Ltd.)

Published

2014

18. Pathogenetic mechanisms of amyloid A amyloidosis.

Author

Simons JP, Al-Shawi R, Ellmerich S, Speck I, Aslam S, Hutchinson WL, Mangione PP, Disterer P, Gilbertson JA, Hunt T, Millar DJ, Minogue S, Bodin K, Pepys MB, and Hawkins PN

Subjects

Amyloidosis etiology, Animals, Congo Red, DNA Primers genetics, Doxycycline pharmacology, Female, Gene Expression Regulation drug effects, Mice, Mice, Transgenic, Real-Time Polymerase Chain Reaction, Amyloid metabolism, Amyloidosis physiopathology, Inflammation complications, Serum Amyloid A Protein metabolism

Abstract

Systemic amyloid A (AA) amyloidosis is a serious complication of chronic inflammation. Serum AA protein (SAA), an acute phase plasma protein, is deposited extracellularly as insoluble amyloid fibrils that damage tissue structure and function. Clinical AA amyloidosis is typically preceded by many years of active inflammation before presenting, most commonly with renal involvement. Using dose-dependent, doxycycline-inducible transgenic expression of SAA in mice, we show that AA amyloid deposition can occur independently of inflammation and that the time before amyloid deposition is determined by the circulating SAA concentration. High level SAA expression induced amyloidosis in all mice after a short, slightly variable delay. SAA was rapidly incorporated into amyloid, acutely reducing circulating SAA concentrations by up to 90%. Prolonged modest SAA overexpression occasionally produced amyloidosis after long delays and primed most mice for explosive amyloidosis when SAA production subsequently increased. Endogenous priming and bulk amyloid deposition are thus separable events, each sensitive to plasma SAA concentration. Amyloid deposits slowly regressed with restoration of normal SAA production after doxycycline withdrawal. Reinduction of SAA overproduction revealed that, following amyloid regression, all mice were primed, especially for rapid glomerular amyloid deposition leading to renal failure, closely resembling the rapid onset of renal failure in clinical AA amyloidosis following acute exacerbation of inflammation. Clinical AA amyloidosis rarely involves the heart, but amyloidotic SAA transgenic mice consistently had minor cardiac amyloid deposits, enabling us to extend to the heart the demonstrable efficacy of our unique antibody therapy for elimination of visceral amyloid.

Published

2013

19. Monitoring systemic amyloidosis using MRI measurements of the extracellular volume fraction.

Author

Campbell-Washburn AE, Price AN, Ellmerich S, Simons JP, Al-Shawi R, Kalber TL, Ghatrora R, Hawkins PN, Moon JC, Ordidge RJ, Pepys MB, and Lythgoe MF

Subjects

Amyloidosis metabolism, Amyloidosis pathology, Animals, Female, Humans, Liver diagnostic imaging, Liver metabolism, Male, Mice, Mice, Transgenic, Myocardium metabolism, Radiography, Serum Amyloid A Protein metabolism, Serum Amyloid P-Component immunology, Serum Amyloid P-Component metabolism, Spleen diagnostic imaging, Spleen metabolism, Amyloid metabolism, Amyloidosis diagnosis, Extracellular Fluid metabolism, Liver pathology, Magnetic Resonance Imaging, Myocardium pathology, Spleen pathology

Abstract

We report the in vivo evaluation, in a murine model, of MRI measurements of the extracellular volume fraction (ECV) for the detection and monitoring of systemic amyloidosis. A new inducible transgenic model was used, with increased production of mouse serum amyloid A protein controlled by oral administration of doxycycline, that causes both the usual hepatic and splenic amyloidosis and also cardiac deposits. ECV was measured in vivo by equilibrium contrast MRI in the heart and liver of 11 amyloidotic and 10 control mice. There was no difference in the cardiac function between groups, but ECV was significantly increased in the heart, mean (standard deviation) 0.20 (0.05) versus 0.14 (0.04), p < 0.005, and liver, 0.27 (0.04) versus 0.15 (0.04), p < 0.0005, of amyloidotic animals and was strongly correlated with the histological amyloid score, myocardium, ρ = 0.67, p < 0.01; liver, ρ = 0.87, p < 0.01. In a further four mice that received human serum amyloid P component (SAP) followed by anti-human SAP antibody, a treatment to eliminate visceral amyloid deposits, ECV in the liver and spleen returned to baseline after therapy (p < 0.01). MRI measurement of ECV is a sensitive marker of amyloid deposits with potential application for early detection and monitoring therapies promoting their clearance.

Published

2013

20. Exon skipping of hepatic APOB pre-mRNA with splice-switching oligonucleotides reduces LDL cholesterol in vivo.

Author

Disterer P, Al-Shawi R, Ellmerich S, Waddington SN, Owen JS, Simons JP, and Khoo B

Subjects

Animals, Apolipoproteins B metabolism, Caco-2 Cells, Genetic Therapy methods, Hep G2 Cells, Homozygote, Humans, Hyperlipoproteinemia Type II blood, Hyperlipoproteinemia Type II genetics, Hyperlipoproteinemia Type II therapy, Lipoproteins, VLDL antagonists & inhibitors, Lipoproteins, VLDL blood, Liver metabolism, Mice, Mice, Transgenic, Oligonucleotides metabolism, RNA Precursors metabolism, Rabbits, Receptors, Lipoprotein genetics, Receptors, Lipoprotein metabolism, Sequence Analysis, RNA, Apolipoproteins B genetics, Cholesterol, LDL blood, Exons, Oligonucleotides genetics, RNA Precursors genetics, RNA Splicing

Abstract

Familial hypercholesterolemia (FH) is a genetic disorder characterized by extremely high levels of plasma low-density lipoprotein (LDL), due to defective LDL receptor-apolipoprotein B (APOB) binding. Current therapies such as statins or LDL apheresis for homozygous FH are insufficiently efficacious at lowering LDL cholesterol or are expensive. Treatments that target APOB100, the structural protein of LDL particles, are potential therapies for FH. We have developed a series of APOB-directed splice-switching oligonucleotides (SSOs) that cause the expression of APOB87, a truncated isoform of APOB100. APOB87, like similarly truncated isoforms expressed in patients with a different condition, familial hypobetalipoproteinemia, lowers LDL cholesterol by inhibiting very low-density lipoprotein (VLDL) assembly and increasing LDL clearance. We demonstrate that these "APO-skip " SSOs induce high levels of exon skipping and expression of the APOB87 isoform, but do not substantially inhibit APOB48 expression in cell lines. A single injection of an optimized APO-skip SSO into mice transgenic for human APOB resulted in abundant exon skipping that persists for >6 days. Weekly treatments generated a sustained reduction in LDL cholesterol levels of 34-51% in these mice, superior to pravastatin in a head-to-head comparison. These results validate APO-skip SSOs as a candidate therapy for FH.

Published

2013

21. Isolation and characterization of pharmaceutical grade human pentraxins, serum amyloid P component and C-reactive protein, for clinical use.

Author

Pepys MB, Gallimore JR, Lloyd J, Li Z, Graham D, Taylor GW, Ellmerich S, Mangione PP, Tennent GA, Hutchinson WL, Millar DJ, Bennett G, More J, Evans D, Mistry Y, Poole S, and Hawkins PN

Subjects

Acute-Phase Proteins analysis, Acute-Phase Proteins isolation & purification, Acute-Phase Proteins pharmacology, Amyloidosis blood, Animals, C-Reactive Protein isolation & purification, C-Reactive Protein pharmacology, Cells, Cultured, Chromatography, Gel, Electrophoresis, Polyacrylamide Gel, Enzyme-Linked Immunosorbent Assay, Female, Humans, Interleukin-10 metabolism, Interleukin-1beta metabolism, Interleukin-6 metabolism, Interleukin-8 metabolism, Leukocytes, Mononuclear drug effects, Mice, Mice, Inbred C57BL, Serum Amyloid P-Component isolation & purification, Serum Amyloid P-Component pharmacology, Spectrometry, Mass, Electrospray Ionization, Tumor Necrosis Factor-alpha metabolism, C-Reactive Protein analysis, Cytokines metabolism, Leukocytes, Mononuclear metabolism, Serum Amyloid P-Component analysis

Abstract

The human pentraxin proteins, serum amyloid P component (SAP) and C-reactive protein (CRP) are important in routine clinical diagnosis, SAP for systemic amyloidosis and CRP for monitoring the non-specific acute phase response. They are also targets for novel therapies currently in development but their roles in health and disease are controversial. Thus, both for clinical use and to rigorously elucidate their functions, structurally and functionally intact, pharmaceutical grade preparations of the natural, authentic proteins are required. We report here the production from normal human donor plasma and the characterization of the first such preparations. Importantly, we demonstrate that, contrary to reports using recombinant proteins and less well characterized preparations, neither CRP nor SAP stimulate the release by human peripheral blood mononuclear cells in vitro of any TNFα, IL-6 or IL-8, nor does SAP cause release of IL-1β or IL-10. Furthermore neither of our preparations was pro-inflammatory in mice in vivo., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

22. Protein engineered variants of hepatocyte growth factor/scatter factor promote proliferation of primary human hepatocytes and in rodent liver.

Author

Ross J, Gherardi E, Mallorqui-Fernandez N, Bocci M, Sobkowicz A, Rees M, Rowe A, Ellmerich S, Massie I, Soeda J, Selden C, and Hodgson H

Subjects

Animals, Apoptosis, Binding Sites, Carbon Tetrachloride, Caspase 3 metabolism, Caspase 7 metabolism, Cells, Cultured, DNA Replication, Disease Models, Animal, Dose-Response Relationship, Drug, Fas Ligand Protein metabolism, Heparan Sulfate Proteoglycans metabolism, Hepatectomy, Hepatocyte Growth Factor chemistry, Hepatocyte Growth Factor genetics, Hepatocyte Growth Factor metabolism, Hepatocytes metabolism, Hepatocytes pathology, Humans, Liver metabolism, Liver pathology, Liver surgery, Liver Cirrhosis chemically induced, Liver Cirrhosis metabolism, Liver Cirrhosis pathology, Male, Mice, Mice, Inbred BALB C, Models, Molecular, Peptide Fragments chemistry, Peptide Fragments genetics, Peptide Fragments metabolism, Poly(ADP-ribose) Polymerases metabolism, Protein Conformation, Protein Stability, Rats, Rats, Sprague-Dawley, Recombinant Proteins metabolism, Time Factors, Ultracentrifugation, Cell Proliferation drug effects, Hepatocyte Growth Factor pharmacology, Hepatocytes drug effects, Liver drug effects, Liver Cirrhosis prevention & control, Liver Regeneration drug effects, Peptide Fragments pharmacology, Protein Engineering

Abstract

Background & Aims: Hepatocyte growth factor/scatter factor (HGF/SF) stimulates hepatocyte DNA synthesis and protects against apoptosis; in vivo it promotes liver regeneration and reduces fibrosis. However, its therapeutic value is limited by its complex domain structure, high cost of production, instability, and poor tissue penetration due to sequestration by heparin sulfate proteoglycans (HSPGs)., Methods: Using protein engineering techniques, we created a full-length form of HGF/SF (called HP21) and a form of the small, naturally occurring HGF/SF fragment, NK1 (called 1K1), which have reduced affinity for HSPG. We characterized the stability and proliferative and anti-apoptotic effects of these variants in primary human hepatocytes and in rodents., Results: Analytical ultracentrifugation showed that 1K1 and NK1 were more stable than the native, full-length protein. All 4 forms of HGF/SF induced similar levels of DNA synthesis in human hepatocytes; 1K1 and NK1 required heparin, an HSPG analogue, for full agonistic activity. All the proteins reduced levels of Fas ligand-mediated apoptosis, reducing the activity of caspase-3/7 and cleavage of poly(adenosine diphosphate-ribose) polymerase. 1K1 was more active than NK1 in rodents; in healthy mice, 1K1 significantly increased hepatocyte DNA synthesis, and in mice receiving carbon tetrachloride, it reduced fibrosis. In rats, after 70% partial hepatectomy, daily administration of 1K1 for 5 days significantly increased liver mass and the bromodeoxyuridine labeling index compared with mice given NK1., Conclusions: 1K1, an engineered form of the small, naturally occurring HGF/SF fragment NK1, has reduced affinity for HSPG and exerts proliferative and antiapoptotic effects in cultured hepatocytes. In rodents, 1K1 has antifibrotic effects and promotes liver regeneration. The protein has better stability and is easier to produce than HGF/SF and might be developed as a therapeutic for acute and chronic liver disease., (Copyright © 2012 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2012

23. Requirement for complement in antibody responses is not explained by the classic pathway activator IgM.

Author

Rutemark C, Alicot E, Bergman A, Ma M, Getahun A, Ellmerich S, Carroll MC, and Heyman B

Subjects

Animals, Antibodies, Monoclonal immunology, C-Reactive Protein immunology, Chromatography, Agarose, DNA Primers genetics, Enzyme-Linked Immunosorbent Assay, Enzyme-Linked Immunospot Assay, Flow Cytometry, Gene Knock-In Techniques, Immunoglobulin mu-Chains genetics, Mice, Mice, Inbred BALB C, Microscopy, Confocal, Mutation, Missense genetics, Polymerase Chain Reaction, Serum Amyloid P-Component immunology, Antibody Formation immunology, Complement Pathway, Classical immunology, Complement System Proteins immunology, Immunoglobulin mu-Chains immunology

Abstract

Animals lacking complement factors C1q, C2, C3, or C4 have severely impaired Ab responses, suggesting a major role for the classic pathway. The classic pathway is primarily initiated by antigen-Ab complexes. Therefore, its role for primary Ab responses seems paradoxical because only low amounts of specific Abs are present in naive animals. A possible explanation could be that the classic pathway is initiated by IgM from naive mice, binding with sufficient avidity to the antigen. To test this hypothesis, a knock-in mouse strain, Cμ13, with a point mutation in the gene encoding the third constant domain of the μ-heavy chain was constructed. These mice produce IgM in which proline in position 436 is substituted with serine, a mutation previously shown to abrogate the ability of mouse IgM to activate complement. Unexpectedly, the Ab response to sheep erythrocytes and keyhole limpet hemocyanin in Cμ13 mice was similar to that in WT mice. Thus, although secreted IgM and the classic pathway activation are both required for the normal primary Ab response, this does not require that IgM activate C. This led us to test Ab responses in animals lacking one of three other endogenous activators of the classic pathway: specific intracellular adhesion molecule-grabbing nonintegrin R1, serum amyloid P component, and C-reactive protein. Ab responses were also normal in these animals.

Published

2011

24. Antibodies to human serum amyloid P component eliminate visceral amyloid deposits.

Author

Bodin K, Ellmerich S, Kahan MC, Tennent GA, Loesch A, Gilbertson JA, Hutchinson WL, Mangione PP, Gallimore JR, Millar DJ, Minogue S, Dhillon AP, Taylor GW, Bradwell AR, Petrie A, Gillmore JD, Bellotti V, Botto M, Hawkins PN, and Pepys MB

Subjects

Amyloidosis therapy, Animals, Antibodies therapeutic use, Disease Models, Animal, Humans, Mice, Mice, Inbred C57BL, Mice, Transgenic, Serum Amyloid P-Component genetics, Amyloid drug effects, Amyloidosis prevention & control, Antibodies immunology, Antibodies pharmacology, Serum Amyloid P-Component antagonists & inhibitors, Serum Amyloid P-Component immunology

Abstract

Accumulation of amyloid fibrils in the viscera and connective tissues causes systemic amyloidosis, which is responsible for about one in a thousand deaths in developed countries. Localized amyloid can also have serious consequences; for example, cerebral amyloid angiopathy is an important cause of haemorrhagic stroke. The clinical presentations of amyloidosis are extremely diverse and the diagnosis is rarely made before significant organ damage is present. There is therefore a major unmet need for therapy that safely promotes the clearance of established amyloid deposits. Over 20 different amyloid fibril proteins are responsible for different forms of clinically significant amyloidosis and treatments that substantially reduce the abundance of the respective amyloid fibril precursor proteins can arrest amyloid accumulation. Unfortunately, control of fibril-protein production is not possible in some forms of amyloidosis and in others it is often slow and hazardous. There is no therapy that directly targets amyloid deposits for enhanced clearance. However, all amyloid deposits contain the normal, non-fibrillar plasma glycoprotein, serum amyloid P component (SAP). Here we show that administration of anti-human-SAP antibodies to mice with amyloid deposits containing human SAP triggers a potent, complement-dependent, macrophage-derived giant cell reaction that swiftly removes massive visceral amyloid deposits without adverse effects. Anti-SAP-antibody treatment is clinically feasible because circulating human SAP can be depleted in patients by the bis-d-proline compound CPHPC, thereby enabling injected anti-SAP antibodies to reach residual SAP in the amyloid deposits. The unprecedented capacity of this novel combined therapy to eliminate amyloid deposits should be applicable to all forms of systemic and local amyloidosis.

Published

2010

25. High incidence of spontaneous disease in an HLA-DR15 and TCR transgenic multiple sclerosis model.

Author

Ellmerich S, Mycko M, Takacs K, Waldner H, Wahid FN, Boyton RJ, King RH, Smith PA, Amor S, Herlihy AH, Hewitt RE, Jutton M, Price DA, Hafler DA, Kuchroo VK, and Altmann DM

Subjects

Animals, Antigen Presentation genetics, Antigen Presentation immunology, Cell Movement genetics, Cell Movement immunology, Central Nervous System immunology, Central Nervous System pathology, DNA-Binding Proteins deficiency, DNA-Binding Proteins genetics, Disease Models, Animal, Disease Progression, Epitopes, T-Lymphocyte immunology, Epitopes, T-Lymphocyte metabolism, HLA-DR Antigens biosynthesis, HLA-DR Antigens physiology, HLA-DR Serological Subtypes, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Multiple Sclerosis pathology, Myelin Basic Protein immunology, Myelin Basic Protein metabolism, Paralysis genetics, Paralysis immunology, Peptide Fragments immunology, Peptide Fragments metabolism, Receptors, Antigen, T-Cell, alpha-beta biosynthesis, Receptors, Antigen, T-Cell, alpha-beta physiology, T-Lymphocyte Subsets pathology, HLA-DR Antigens genetics, Multiple Sclerosis genetics, Multiple Sclerosis immunology, Receptors, Antigen, T-Cell, alpha-beta genetics, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets metabolism

Abstract

Multiple sclerosis (MS) is thought to involve CD4 T cell recognition of self myelin, many studies focusing on a pathogenic role for anti-myelin, HLA-DR15-restricted T cells. In experimental allergic encephalomyelitis, it is known which epitopes trigger disease and that disease is associated with determinant spread of T cell reactivity. Characterization of these events in human MS is critical for the development of peptide immunotherapies, but it has been difficult to define the role of determinant spread or define which epitopes might be involved. In this study, we report humanized transgenic mice, strongly expressing HLA-DR15 with an MS-derived TCR; even on a RAG-2 wild-type background, mice spontaneously develop paralysis. Disease, involving demyelination and axonal degeneration, correlates with inter- and intramolecular spread of the T cell response to HLA-DR15-restricted epitopes of myelin basic protein, myelin oligodendrocyte glycoprotein, and alphaB-crystallin. Spread is reproducible and progressive, with two of the epitopes commonly described in responses of HLA-DR15 patients. The fact that this pattern is reiterated as a consequence of CNS tissue damage in mice demonstrates the value of the transgenic model in supplying an in vivo disease context for the human responses. This model, encompassing pathologically relevant, spontaneous disease with the presentation of myelin epitopes in the context of HLA-DR15, should offer new insights and predictions about T cell responses during MS as well as a more stringent test bed for immunotherapies.

Published

2005

26. Modified amino acid copolymers suppress myelin basic protein 85-99-induced encephalomyelitis in humanized mice through different effects on T cells.

Author

Illés Z, Stern JN, Reddy J, Waldner H, Mycko MP, Brosnan CF, Ellmerich S, Altmann DM, Santambrogio L, Strominger JL, and Kuchroo VK

Subjects

Amino Acid Sequence, Animals, Cytokines drug effects, Cytokines metabolism, Drug Therapy, Combination, Encephalomyelitis, Autoimmune, Experimental chemically induced, Encephalomyelitis, Autoimmune, Experimental prevention & control, Glatiramer Acetate, HLA-DR2 Antigen, Humans, Mice, Mice, Transgenic, Myelin Basic Protein pharmacology, Peptide Fragments administration & dosage, Peptide Fragments pharmacology, Peptides administration & dosage, Receptors, Antigen, T-Cell immunology, T-Lymphocytes drug effects, T-Lymphocytes immunology, Treatment Outcome, Vaccination, Encephalomyelitis, Autoimmune, Experimental drug therapy, Peptide Fragments therapeutic use, Peptides therapeutic use

Abstract

A humanized mouse bearing the HLA-DR2 (DRA/DRB1*1501) protein associated with multiple sclerosis (MS) and the myelin basic protein (MBP) 85-99-specific HLA-DR2-restricted T cell receptor from an MS patient has been used to examine the effectiveness of modified amino acid copolymers poly(F,Y,A,K)n and poly-(V,W,A,K)n in therapy of MBP 85-99-induced experimental autoimmune encephalomyelitis (EAE) in comparison to Copolymer 1 [Copaxone, poly(Y,E,A,K)n]. The copolymers were designed to optimize binding to HLA-DR2. Vaccination, prevention, and treatment of MBP-induced EAE in the humanized mice with copolymers FYAK and VWAK ameliorated EAE more effectively than Copolymer 1, reduced the number of pathological lesions, and prevented the up-regulation of human HLA-DR on CNS microglia. Moreover, VWAK inhibited MBP 85-99-specific T cell proliferation more efficiently than either FYAK or Copolymer 1 and induced anergy of HLA-DR2-restricted transgenic T cells as its principle mechanism. In contrast, FYAK induced proliferation and a pronounced production of the antiinflammatory T helper 2 cytokines IL-4 and IL-10 from nontransgenic T cells as its principle mechanism of immunosuppression. Thus, copolymers generated by using different amino acids inhibited disease using different mechanisms to regulate T cell responses.

Published

2004

27. Disease-related epitope spread in a humanized T cell receptor transgenic model of multiple sclerosis.

Author

Ellmerich S, Takacs K, Mycko M, Waldner H, Wahid F, Boyton RJ, Smith PA, Amor S, Baker D, Hafler DA, Kuchroo VK, and Altmann DM

Subjects

Animals, Cells, Cultured, Female, Humans, Male, Mice, Mice, Transgenic, Multiple Sclerosis genetics, Myelin Basic Protein chemistry, Myelin Basic Protein immunology, Phenotype, Receptors, Antigen, T-Cell genetics, T-Lymphocytes immunology, T-Lymphocytes metabolism, Disease Models, Animal, Epitopes immunology, Multiple Sclerosis immunology, Receptors, Antigen, T-Cell immunology

Abstract

While EAE has been an invaluable model for the immunopathogenesis of multiple sclerosis, it has sometimes been difficult to bridge the gap between findings and therapies in the rodent models and the cellular and molecular interactions that can be studied in the human disease. Humanized transgenic models offer a means of achieving this, through the expression of disease-implicated HLA class II molecules, co-expressed with a cognate HLA-class II-restricted, myelin-specific TCR derived from a human T cell clone implicated in disease. We have generated such a transgenic line, called line 8, that co-expresses a high level of HLA-DR15 and a human TCR specific for HLA-DR15/MBP 85-99. T cells from the transgenic line are skewed to the CD4 single-positive compartment and produce IFN-gamma in response to peptide from mylein basic protein. Mice develop a spontaneous disease phenotype, showing poverty of movement, although this rarely develops into paralysis except following immunization with peptide. On induction of paralysis by immunization with peptide, disease correlates with epitope spread to a number of additional, HLA-DR15-restricted myelin epitopes. This model should be valuable for analyzing epitope spread in a humanized immunogenetic environment and for the testing of specific immunotherapies.

Published

2004

28. Altered major histocompatibility complex class II peptide loading in H2-O-deficient mice.

Author

Perraudeau M, Taylor PR, Stauss HJ, Lindstedt R, Bygrave AE, Pappin DJ, Ellmerich S, Whitten A, Rahman D, Canas B, Walport MJ, Botto M, and Altmann DM

Subjects

Animals, Antigens immunology, Antigens metabolism, Antigens, Differentiation, B-Lymphocyte metabolism, CD4 Antigens immunology, CD8 Antigens immunology, Dimerization, Female, Genes, MHC Class II, Genotype, Histocompatibility Antigens Class II genetics, Histocompatibility Antigens Class II metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Peptide Fragments immunology, Protein Binding, Receptors, Antigen, T-Cell, alpha-beta genetics, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, T-Lymphocyte Subsets immunology, Antigen Presentation, Histocompatibility Antigens Class II immunology, Peptide Fragments metabolism

Abstract

The biosynthesis of MHC class II/peptide complexes involves classical, cell surface MHC products as well as the intracellular component H2-M, required for the removal of invariant chain-derived CLIP and for peptide loading. The function of another intracellular class II heterodimer, H2-O, is the matter of some controversy. The physical association of H2-O with H2-M and co-localization in class II+ vesicles suggest a related function in peptide exchange. Furthermore, the distinctive thymic distribution of H2-O raises the possibility of a specialized role in T cell thymic selection. To investigate the role of H2-O in vivo we generated mice carrying a targeted disruption in the H2-Oa gene. No evidence was obtained for a defect in removal of CLIP. However, the array of endogenous peptides bound by class II was altered and a defect in antigen presentation through H2-A to T cells was seen on the 129/Sv/ C57BL/6 mixed strain background but not in 129/Sv pure strain mice. Furthermore, H2-O-null mice showed enhanced selection of CD4+ single positive thymocytes. The findings indicate that H2-O interacts with H2-M in peptide editing but that the genetic background in which H2-O deficiency is manifest is also important. Overall, the experiments indicate that H2-O/HLA-DO should be regarded as neither up-regulating nor down-regulating the DM-dependent release of CLIP, but as a modulator of peptide editing, determining the presenting cell type specific peptide profile able to retain stability in the class II groove.

Published

2000

29. Production of cytokines by monocytes, epithelial and endothelial cells activated by Streptococcus bovis.

Author

Ellmerich S, Djouder N, Schöller M, and Klein JP

Subjects

Cells, Cultured, Endothelium, Vascular cytology, Humans, Intestines cytology, Mouth cytology, Saphenous Vein cytology, Endothelium, Vascular immunology, Epithelial Cells immunology, Extracellular Matrix immunology, Interleukin-8 biosynthesis, Monocytes immunology, Streptococcus bovis metabolism

Abstract

There are numerous reports documenting the correlation between Streptococcus bovis bacteraemia and endocarditis in conjunction with colonic diseases. The adherence of S. bovis to either buccal or intestinal epithelial cells seems to be the initial process in colonization and subsequent infection of the host, allowing further adhesion of S. bovis to either endothelial cells or extracellular matrix components which leads to infective endocarditis. Bacterial entry at tumour sites is further assisted by the local action of cytokines that promotes vasodilatation and increased capillary permeability. Thus the ability of S. bovis to adhere to and to stimulate human cells may contribute to the pathogenicity of this bacteria. In the present study, we have shown the ability of S. bovis and wall-extracted antigens (WEA) to adhere to human buccal (KB) or intestinal (Caco-2) epithelial cell lines, to human saphenous vein endothelial cells, to human monocytic cell line (THP-1) and to extracellular matrix components (ECM) (fibronectin, collagen and laminin). The fixation of S. bovis on cells was followed by the synthesis of IL-8 from all the cells except Caco-2, whereas S. bovis WEA was able to induce cytokine synthesis from all of them, showing the immunomodulatory effect of S. bovis and S. bovis WEA on different cells., (Copyright 2000 Academic Press.)

Published

2000