Your search keyword '"Rose, Kirsten L"' showing total 9 results

1. Factor I is required for the development of membranoproliferative glomerulonephritis in factor H--deficient mice

Author

Rose, Kirsten L., Paixao-Cavalcante, Danielle, Fish, Jennifer, Manderson, Anthony P., Malik, Talat H., Bygrave, Anne E., Lin, Tao, Sacks, Steven H., Walport, Mark J., Cook, H. Terence, Botto, Marina, and Pickering, Matthew C.

Subjects

Glomerulonephritis -- Risk factors, Glomerulonephritis -- Genetic aspects, Glomerulonephritis -- Research, Glycoproteins -- Health aspects, Glycoproteins -- Genetic aspects, Glycoproteins -- Structure, Glycoproteins -- Research, Enzyme-linked immunosorbent assay -- Usage, Enzyme-linked immunosorbent assay -- Research

Abstract

The inflammatory kidney disease membranoproliferative glomerulonephritis type II (MPGN2) is associated with dysregulation of the alternative pathway of complement activation. MPGN2 is characterized by the presence of complement C3 along the glomerular basement membrane (GBM). Spontaneous activation of C3 through the alternative pathway is regulated by 2 plasma proteins, factor H and factor I. Deficiency of either of these regulators results in uncontrolled C3 activation, although the breakdown of activated C3 is dependent on factor I. Deficiency of factor H, but not factor I, is associated with MPGN2 in humans, pigs, and mice. To explain this discordance, mice with single or combined deficiencies of these factors were studied. MPGN2 did not develop in mice with combined factor H and I deficiency or in mice deficient in factor I alone. However, administration of a source of factor I to mice with combined factor H and factor I deficiency triggered both activated C3 fragments in plasma and GBM C3 deposition. Mouse renal transplant studies demonstrated that C3 deposited along the GBM was derived from plasma. Together, these findings provide what we believe to be the first evidence that factor I--mediated generation of activated C3 fragments in the circulation is a critical determinant for the development of MPGN2 associated with factor H deficiency., Introduction The complement system is an important part of the innate immune system that is composed of a complex group of proteins whose main biological functions include host defense, the [...]

Published

2008

2. The Development of Atypical Hemolytic Uremic Syndrome Depends on Complement C5

Author

de Jorge, Elena Goicoechea, Macor, Paolo, Paixão-Cavalcante, Danielle, Rose, Kirsten L., Tedesco, Franco, Cook, H. Terence, Botto, Marina, and Pickering, Matthew C.

Published

2011

3. Relationship between complotype and reported severity of systemic allergic reactions to peanut

Author

Menikou, Stephanie, Patel, Mitali P., Rose, Kirsten L., Botto, Marina, Warner, John O., Pickering, Matthew C., and Boyle, Robert J.

Published

2012

4. Spontaneous Autoimmunity in 129 and C57BL/6 Mice—Implications for Autoimmunity Described in Gene-Targeted Mice

Author

Bygrave, Anne E, Rose, Kirsten L, Cortes-Hernandez, Josefina, Warren, Joanna, Rigby, Robert J, Cook, H. Terence, Walport, Mark J, Vyse, Timothy J, and Botto, Marina

Subjects

Cell Nucleus, Genome, Genotype, Models, Genetic, Genetic Linkage, Immunology, Quantitative Trait Loci, Chromosome Mapping, Autoimmunity, Epistasis, Genetic, Mice, Transgenic, Mus (Mouse), Genetics/Genomics/Gene Therapy, Cohort Studies, Mice, Inbred C57BL, Disease Models, Animal, Mice, Species Specificity, Gene Targeting, Animals, Lupus Erythematosus, Systemic, Female, Genetic Predisposition to Disease, Research Article, Microsatellite Repeats

Abstract

Systemic lupus erythematosus (SLE) is a multisystem autoimmune disorder in which complex genetic factors play an important role. Several strains of gene-targeted mice have been reported to develop SLE, implicating the null genes in the causation of disease. However, hybrid strains between 129 and C57BL/6 mice, widely used in the generation of gene-targeted mice, develop spontaneous autoimmunity. Furthermore, the genetic background markedly influences the autoimmune phenotype of SLE in gene-targeted mice. This suggests an important role in the expression of autoimmunity of as-yet-uncharacterised background genes originating from these parental mouse strains. Using genome-wide linkage analysis, we identified several susceptibility loci, derived from 129 and C57BL/6 mice, mapped in the lupus-prone hybrid (129 × C57BL/6) model. By creating a C57BL/6 congenic strain carrying a 129-derived Chromosome 1 segment, we found that this 129 interval was sufficient to mediate the loss of tolerance to nuclear antigens, which had previously been attributed to a disrupted gene. These results demonstrate important epistatic modifiers of autoimmunity in 129 and C57BL/6 mouse strains, widely used in gene targeting. These background gene influences may account for some, or even all, of the autoimmune traits described in some gene-targeted models of SLE., Several strains of gene-targeted mice develop systemic lupus erythematosus (SLE). Analysis of these strains demonstrates that the genetic background profoundly influences the development of autoimmunity

Published

2004

5. Spontaneous hemolytic uremic syndrome triggered by complement factor H lacking surface recognition domains

Author

Pickering, Matthew C., Goicoechea de Jorge, Elena, Martínez-Barricarte, Rubén, Recalde, Sergio, García-Layana, Alfredo, Rose, Kirsten L., Moss, Jill, Walport, Mark J., Cook, H. Terence, Rodríguez de Córdoba, Santiago, Botto, Marina, Pickering, Matthew C., Goicoechea de Jorge, Elena, Martínez-Barricarte, Rubén, Recalde, Sergio, García-Layana, Alfredo, Rose, Kirsten L., Moss, Jill, Walport, Mark J., Cook, H. Terence, Rodríguez de Córdoba, Santiago, and Botto, Marina

Abstract

Factor H (FH) is an abundant serum glycoprotein that regulates the alternative pathway of complement-preventing uncontrolled plasma C3 activation and nonspecific damage to host tissues. Age-related macular degeneration (AMD), atypical hemolytic uremic syndrome (aHUS), and membranoproliferative glomerulonephritis type II (MPGN2) are associated with polymorphisms or mutations in the FH gene (Cfh), suggesting the existence of a genotype–phenotype relationship. Although AMD and MPGN2 share pathological similarities with the accumulation of complement-containing debris within the eye and kidney, respectively, aHUS is characterized by renal endothelial injury. This pathological distinction was reflected in our Cfh association analysis, which demonstrated that although AMD and MPGN2 share a Cfh at-risk haplotype, the haplotype for aHUS was unique. FH-deficient mice have uncontrolled plasma C3 activation and spontaneously develop MPGN2 but not aHUS. We show that these mice, transgenically expressing a mouse FH protein functionally equivalent to aHUS-associated human FH mutants, regulate C3 activation in plasma and spontaneously develop aHUS but not MPGN2. These animals represent the first model of aHUS and provide in vivo evidence that effective plasma C3 regulation and the defective control of complement activation on renal endothelium are the critical events in the molecular pathogenesis of FH-associated aHUS.

Published

2007

6. A Hybrid CFHR3-1 Gene Causes Familial C3 Glomerulopathy

Author

Malik, Talat H., primary, Lavin, Peter J., additional, Goicoechea de Jorge, Elena, additional, Vernon, Katherine A., additional, Rose, Kirsten L., additional, Patel, Mitali P., additional, de Leeuw, Marcel, additional, Neary, John J., additional, Conlon, Peter J., additional, Winn, Michelle P., additional, and Pickering, Matthew C., additional

Published

2012

7. C5 activation is required for the development of atypical haemolytic uraemic syndrome in Cfh−/−·FHΔ16–20 mice

Author

de Jorge, Elena Goicoechea, primary, Paixao-Cavalcante, Danielle, additional, Rose, Kirsten L., additional, Cook, H. Terence, additional, Botto, Marina, additional, and Pickering, Matthew C., additional

Published

2008

8. Factor I is required for the development of membranoproliferative glomerulonephritis in factor H-deficient mice

Author

Rose, Kirsten L., primary, Paixao-Cavalcante, Danielle, additional, Fish, Jennifer, additional, Manderson, Anthony P., additional, Malik, Talat, additional, Bygrave, Anne E., additional, Lin, Tao, additional, Sacks, Steven H., additional, Walport, Mark J., additional, Cook, H. Terence, additional, Botto, Marina, additional, and Pickering, Matthew C., additional

Published

2007

9. Spontaneous hemolytic uremic syndrome triggered by complement factor H lacking surface recognition domains

Author

Pickering, Matthew C., primary, de Jorge, Elena Goicoechea, additional, Martinez-Barricarte, Rubén, additional, Recalde, Sergio, additional, Garcia-Layana, Alfredo, additional, Rose, Kirsten L., additional, Moss, Jill, additional, Walport, Mark J., additional, Cook, H. Terence, additional, de Córdoba, Santiago Rodriguez, additional, and Botto, Marina, additional

Published

2007