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2. Insights into the role of the von Hippel-Lindau gene product. A key player in hypoxic regulation

Author

Maxwell, P. H., Pugh, C. W., and Peter Ratcliffe

Subjects
endocrine system diseases, cardiovascular diseases, urologic and male genital diseases, neoplasms, female genital diseases and pregnancy complications
Abstract

Many adaptive responses to hypoxia involve changes in gene transcription mediated by the hypoxia-inducible factor 1 complex. Central to this is oxygen-dependent proteolysis of the alpha subunit, which has recently been shown to require the von Hippel-Lindau tumour-suppressor protein. This observation provides one mechanism by which inherited defects in the von Hippel-Lindau gene could cause features of the clinical syndrome, and offers insight into the events leading to sporadic clear cell renal cancer. Furthermore, it clearly implicates the von Hippel-Lindau tumour-suppressor protein in the biochemistry of oxygen sensing.

Published
2016

3. Familial C3 Glomerulopathy Associated with CFHR5 Mutations

Author

Athanasiou, Yiannis, Voskarides, Konstantinos, Gale, D. P., Damianou, Loukas, Patsias, Charalambos, Zavros, Michalis, Maxwell, P. H., Cook, H. T., Demosthenous, Panayiota, Hadjisavvas, Andreas, Kyriacou, Kyriacos C., Zouvani, Ioanna, Pierides, Alkis M., Constantinou-Deltas, Constantinos D., and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
Male, Pathology, Time Factors, genetic association, creatinine blood level, Epidemiology, Biopsy, membranoproliferative glomerulonephritis, DNA Mutational Analysis, immunoglobulin A, Kidney, Critical Care and Intensive Care Medicine, Gastroenterology, immunoglobulin G, Glomerulonephritis, Focal segmental glomerulosclerosis, dipeptidyl carboxypeptidase inhibitor, London, Membranoproliferative glomerulonephritis, immunoglobulin M, Prospective Studies, gene mutation, Microscopic hematuria, familial disease, Aged, 80 and over, child, Proteinuria, adult, article, creatinine, complement factor H, Complement C3, Middle Aged, chronic kidney failure, Founder Effect, unclassified drug, Pedigree, aged, female, Phenotype, Nephrology, Disease Progression, histopathology, Female, medicine.symptom, Adult, mutational analysis, medicine.medical_specialty, Adolescent, kidney biopsy, omega 3 fatty acid, glomerulopathy, Nephropathy, complement component C3, Young Adult, complement component C4, mycophenolic acid 2 morpholinoethyl ester, pedigree analysis, Sex Factors, male, Glomerulopathy, Internal medicine, molecular diagnosis, medicine, Humans, follow up, Genetic Predisposition to Disease, human, Aged, Hematuria, Transplantation, business.industry, Original Articles, Complement System Proteins, school child, medicine.disease, major clinical study, heterozygote, methylprednisolone, complement factor H related protein 5, clinical feature, kidney failure, hematuria, angiotensin receptor antagonist, cell proliferation, Cyprus, Mutation, prednisone, glomerulus basement membrane, Kidney Failure, Chronic, cyclophosphamide, CFHR5 nephropathy, prognosis, proteinuria, business, CFHR5
Abstract

Background and objectives Complement factor H and related proteins (CFHR) are key regulators of the alternative complement pathway, where loss of function mutations lead to a glomerulopathy with isolated mesangial C3 deposits without immunoglobulins. Gale et al. (12) reported on 26 patients with the first familial, hematuric glomerulopathy caused by a founder mutation in the CFHR5 gene in patients of Cypriot descent living in the United Kingdom. CFHR5 nephropathy is clinically characterized by continuous microscopic hematuria whereas some patients present with additional episodes of synpharyngitic macrohematuria, associated with infection and pyrexia. A subgroup of patients, particularly men, develop additional proteinuria, hypertension, and chronic renal disease or ESRD. Design, setting, participants, & measurements We herewith expand significantly on the study by Gale et al., reporting on histologic, molecular, and clinical findings in 91 patients from 16 families with the same founder mutation. Results Eighty-two patients (90%) exhibited microscopic hematuria 51 (62%), exhibited only microscopic hematuria, whereas the remaining 31 additionally had proteinuria (38%) 28 proteinuric patients developed chronic renal failure (CRF). Among carriers of CFHR5 mutation aged >50 years, 80% of the men and 21% of the women developed CRF 18 developed ESRD (14 men [78%], 4 women [22%]). Conclusions The diagnosis of CFHR5-related, isolated C3 glomerulopathy was established in 2009 using newly described mutation analysis after decades of follow-up with unclear diagnoses, occasionally confused with IgA nephropathy. This larger patient cohort establishes the clinical course, significant variable expressivity, and marked gender difference regarding the development of CRF and ESRD. © 2011 by the American Society of Nephrology. 6 1436 1446 Cited By :75

Published
2011
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5. A functional variant in NEPH3 gene confers high risk of renal failure in primary hematuric glomerulopathies. Evidence for predisposition to microalbuminuria in the general population

Author

Voskarides, Konstantinos, Stefanou, Charalambos, Pieri, Myrtani, Demosthenous, Panayiota, Felekkis, Kyriacos N., Arsali, Maria, Athanasiou, Yiannis, Xydakis, D., Stylianou, Konstantinos G., Daphnis, Eugenios K., Goulielmos, George N., Loizou, P., Savige, J., Höhne, M., Völker, L. A., Benzing, T., Maxwell, P. H., Gale, D. P., Gorski, M., Böger, C., Kollerits, B., Kronenberg, F., Paulweber, B., Zavros, Michalis, Pierides, Alkis M., Constantinou-Deltas, Constantinos D., Maxwell, Patrick [0000-0002-0338-2679], Apollo - University of Cambridge Repository, and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
Male, 0301 basic medicine, Oncology, Pathology, Heredity, 030232 urology & nephrology, lcsh:Medicine, Pathology and Laboratory Medicine, immunoprecipitation, Mathematical and Statistical Techniques, 0302 clinical medicine, Framingham Heart Study, single nucleotide polymorphism, Risk Factors, Chronic Kidney Disease, middle aged, Medicine and Health Sciences, Medicine, genetics, membrane protein, Renal Insufficiency, lcsh:Science, education.field_of_study, Multidisciplinary, Proteinuria, adult, chronic kidney failure, Middle Aged, Genetic Mapping, female, risk factor, Nephrology, HEK293 cell line, Physical Sciences, Cohort, Slit diaphragm, Female, medicine.symptom, immunoblotting, Statistics (Mathematics), Research Article, Adult, Genotyping, medicine.medical_specialty, Immunoblotting, Population, Immunoglobulins, Variant Genotypes, complication, Research and Analysis Methods, Polymorphism, Single Nucleotide, albuminuria, Nephropathy, 03 medical and health sciences, Signs and Symptoms, male, Diagnostic Medicine, Internal medicine, Genetics, Albuminuria, Humans, Immunoprecipitation, Genetic Predisposition to Disease, human, Statistical Methods, Allele, Molecular Biology Techniques, education, Molecular Biology, Hematuria, business.industry, lcsh:R, Biology and Life Sciences, Membrane Proteins, Human Genetics, medicine.disease, kidney failure, hematuria, HEK293 Cells, 030104 developmental biology, Genetics of Disease, physiology, Kidney Failure, Chronic, lcsh:Q, Microalbuminuria, KIRREL2 protein, human, business, immunoglobulin, genetic predisposition, Mathematics, Meta-Analysis
Abstract

Background Recent data emphasize that thin basement membrane nephropathy (TBMN) should not be viewed as a form of benign familial hematuria since chronic renal failure (CRF) and even end-stage renal disease (ESRD), is a possible development for a subset of patients on longterm follow-up, through the onset of focal and segmental glomerulosclerosis (FSGS). We hypothesize that genetic modifiers may explain this variability of symptoms. Methods We looked in silico for potentially deleterious functional SNPs, using very strict criteria, in all the genes significantly expressed in the slit diaphragm (SD). Two variants were genotyped in a cohort of well-studied adult TBMN patients from 19 Greek-Cypriot families, with a homogeneous genetic background. Patients were categorized as 'Severe' or 'Mild', based on the presence or not of proteinuria, CRF and ESRD. A larger pooled cohort (HEMATURIA) of 524 patients, including IgA nephropathy patients, was used for verification. Additionally, three large general population cohorts [Framingham Heart Study (FHS), KORAF4 and SAPHIR] were used to investigate if the NEPH3-V353M variant has any renal effect in the general population. Results and conclusions Genotyping for two high-scored variants in 103 TBMN adult patients with founder mutations who were classified as mildly or severely affected, pointed to an association with variant NEPH3-V353M (filtrin). This promising result prompted testing in the larger pooled cohort (HEMATURIA), indicating an association of the 353M variant with disease severity under the dominant model (p = 3.0×103, OR = 6.64 adjusting for gender/age allelic association: P = 4.2×103 adjusting for patients' kinships). Subsequently, genotyping 6,531 subjects of the Framingham Heart Study (FHS) revealed an association of the homozygous 353M/M genotype with microalbuminuria (p = 1.0×103). Two further general population cohorts, KORAF4 and SAPHIR confirmed the association, and a meta-analysis of all three cohorts (11,258 individuals) was highly significant (p = 1.3×105, OR = 7.46). Functional studies showed that Neph3 homodimerization and Neph3-Nephrin heterodimerization are disturbed by variant 353M. Additionally, 353M was associated with differential activation of the unfolded protein response pathway, when overexpressed in stressed cultured undifferentiated podocyte cells, thus attesting to its functional significance. Genetics and functional studies support a 'rare variant-strong effect' role for NEPH3-V353M, by e×erting a negative modifier effect on primary glomerular hematuria. Additionally, genetics studies provide evidence for a role in predisposing homozygous subjects of the general population to microalbuminuria. © 2017 Voskarides et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. 12

Published
2017
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6. Epistatic role of the MYH9/APOL1 region on familial hematuria genes

Author

Voskarides, Konstantinos, Demosthenous, Panayiota, Papazachariou, Louiza, Arsali, Maria, Athanasiou, Yiannis, Zavros, Michalis, Stylianou, Konstantinos G., Xydakis, D., Daphnis, Eugenios K., Gale, D. P., Maxwell, P. H., Elia, Avraam, Pattaro, C., Pierides, Alkis M., Constantinou-Deltas, Constantinos D., and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
Male, Pathology, genetic association, kidney disease, genetic risk, urologic and male genital diseases, Gastroenterology, Linkage Disequilibrium, lcsh:Science, quantitative analysis, adult, thin basement membrane nephropathy, Molecular Motor Proteins, allele, Apolipoprotein L1, Proteinuria, real time polymerase chain reaction, Nephrology, Cohort, Disease Progression, Medicine, disease severity, Lipoproteins, HDL, marker gene, medicine.medical_specialty, phenotype, Single-nucleotide polymorphism, glomerulopathy, Nephropathy, complement component C3, Molecular Genetics, Genetic Mutation, Genetics, Humans, human, Renal Insufficiency, Chronic, genetic epistasis, Biology, COL4A3 gene, Alleles, Aged, Hematuria, Myosin Heavy Chains, lcsh:R, medicine.disease, major clinical study, gene linkage disequilibrium, gene function, Apolipoproteins, lcsh:Q, Dialysis, haplotype, lcsh:Medicine, Epigenesis, Genetic, hereditary hematuria, APOL1 gene, single nucleotide polymorphism, genetic variability, Molecular Cell Biology, Chronic Kidney Disease, gene mutation, Multidisciplinary, messenger RNA, article, COL4A4 gene, Exons, Middle Aged, biological marker, female, CFHR5 gene, Female, Research Article, Clinical Pathology, sex difference, Polymorphism, Single Nucleotide, male, Glomerulopathy, Diagnostic Medicine, Internal medicine, medicine, controlled study, complement component C3 gene, Alport syndrome, Genetic Association Studies, Clinical Genetics, business.industry, Mutation Types, Human Genetics, gene structure, myosin heavy chain 9 gene, hematuria, Haplotypes, Genetics of Disease, CFHR5 nephropathy, business, CFHR5, Kidney disease
Abstract

Familial hematuria (FH) is explained by at least four different genes (see below). About 50% of patients develop late proteinuria and chronic kidney disease (CKD). We hypothesized that MYH9/APOL1, two closely linked genes associated with CKD, may be associated with adverse progression in FH. Our study included 102 thin basement membrane nephropathy (TBMN) patients with three known COL4A3/COL4A4 mutations (cohort A), 83 CFHR5/C3 glomerulopathy patients (cohort B) with a single CFHR5 mutation and 15 Alport syndrome patients (cohort C) with two known COL4A5 mild mutations, who were categorized as "Mild" (controls) or "Severe" (cases), based on renal manifestations. E1 and S1 MYH9 haplotypes and variant rs11089788 were analyzed for association with disease phenotype. Evidence for association with "Severe" progression in CFHR5 nephropathy was found with MYH9 variant rs11089788 and was confirmed in an independent FH cohort, D (cumulative p value = 0.001, odds ratio = 3.06, recessive model). No association was found with APOL1 gene. Quantitative Real time PCR did not reveal any functional significance for the rs11089788 risk allele. Our results derive additional evidence supporting previous reports according to which MYH9 is an important gene per se, predisposing to CKD, suggesting its usefulness as a prognostic marker for young hematuric patients. © 2013 Voskarides et al. 8 Cited By :3

Published
2012

7. Identification of a mutation in complement factor H-related protein 5 in patients of Cypriot origin with glomerulonephritis

Author

Gale, D. P., De Jorge, E. G., Cook, H. T., Martinez-Barricarte, R., Hadjisavvas, Andreas, McLean, A. G., Pusey, C. D., Pierides, Alkis M., Kyriacou, Kyriacos C., Athanasiou, Yiannis, Voskarides, Konstantinos, Constantinou-Deltas, Constantinos D., Palmer, A., De Cordoba, S. R., Maxwell, P. H., Pickering, M. C., Frémeaux-Bacchi, V., and Constantinou-Deltas, Constantinos D. [0000-0001-5549-9169]

Subjects
Male, Endemic Diseases, Genetic Linkage, Biopsy, kidney disease, polymerase chain reaction, 030232 urology & nephrology, genetic identification, Genome-wide association study, Disease, genetic analysis, high risk patient, urologic and male genital diseases, Western blotting, Glomerulonephritis, 0302 clinical medicine, genetic linkage, single nucleotide polymorphism, gene mutation, Respiratory Tract Infections, 0303 health sciences, education.field_of_study, medicine.diagnostic_test, adult, article, complement factor H, Antibodies, Monoclonal, Complement C5, Articles, General Medicine, Blood Proteins, Middle Aged, 3. Good health, unclassified drug, Pedigree, aged, female, priority journal, Chromosomes, Human, Pair 1, diagnostic test, Complement Factor H, Factor H, Disease Progression, Female, Renal biopsy, Adult, Population, kidney biopsy, Antibodies, Monoclonal, Humanized, Polymorphism, Single Nucleotide, Diagnosis, Differential, 03 medical and health sciences, male, medicine, Humans, human, education, multigene family, Aged, Hematuria, 030304 developmental biology, business.industry, Glomerulonephritis, IGA, Complement System Proteins, medicine.disease, major clinical study, heterozygote, United Kingdom, complement factor H related protein 5, kidney failure, hematuria, Immunology, Cyprus, Mutation, Kidney Failure, Chronic, CFHR5 nephropathy, business, CFHR5, glomerulonephritis, Kidney disease, Genome-Wide Association Study
Abstract

8 páginas, 8 figuras, 1 tabla -- PAGS nros. 794-801, Background Complement is a key component of the innate immune system, and variation in genes that regulate its activation is associated with renal and other disease. We aimed to establish the genetic basis for a familial disorder of complement regulation associated with persistent microscopic haematuria, recurrent macroscopic haematuria, glomerulonephritis, and progressive renal failure. Methods We sought patients from the West London Renal and Transplant Centre (London, UK) with unusual renal disease and affected family members as a method of identification of new genetic causes of kidney disease. Two families of Cypriot origin were identified in which renal disease was consistent with autosomal dominant transmission and renal biopsy of at least one individual showed C3 glomerulonephritis. A mutation was identified via a genome-wide linkage study and candidate gene analysis. A PCR-based diagnostic test was then developed and used to screen for the mutation in population-based samples and in individuals and families with renal disease. Findings Occurrence of familial renal disease cosegregated with the same mutation in the complement factor H-related protein 5 gene (CFHR5). In a cohort of 84 Cypriots with unexplained renal disease, four had mutation in CFHR5. Overall, we identified 26 individuals with the mutation and evidence of renal disease from 11 ostensibly unrelated kindreds, including the original two families. A mutant CFHR5 protein present in patient serum had reduced affinity for surface-bound complement. We term this renal disease CFHR5 nephropathy. Interpretation CFHR5 nephropathy accounts for a substantial burden of renal disease in patients of Cypriot origin and can be diagnosed with a specific molecular test. The high risk of progressive renal disease in carriers of the CFHR5 mutation implies that isolated microscopic haematuria or recurrent macroscopic haematuria should not be regarded as a benign finding in individuals of Cypriot descent, DPG is supported by the UK Medical Research Council and EGdJ and MCP are supported by the Wellcome Trust. Additional support was provided by the UK National Institute for Health Research Biomedical Research Centre Funding Scheme and the Cyprus Research Promotion MCP is a Wellcome Trust Senior Fellow in Clinical Science (WT082291MA) and GdJ is funded by this fellowship. CD is supported by the Cyprus Research Promotion Foundation through grants ENIΣX/0505/02 and ENIΣX/0308/08. Additional support was obtained from the UK National Institute for Health Research Biomedical Research Centre Funding Scheme. PHM is supported by the EU large scale collaborative project Metoxia, the St Peter’s Trust, and a Senior Investigator Award from the UK National Institute for Health Research

Published
2010

8. Hypoxia-inducible expression of tumor-associated carbonic anhydrases

Author

Wykoff, C. C., Beasley, N. J. P., Peter Watson, Turner, K. J., Pastorek, J., Sibtain, A., Wilson, G. D., Turley, H., Talks, K. L., Maxwell, P. H., Pugh, C. W., Ratcliffe, P. J., and Harris, A. L.

Subjects
urologic and male genital diseases
Abstract

The transcriptional complex hypoxia-inducible factor-1 (HIF-1) has emerged as an important mediator of gene expression patterns in tumors, although the range of responding genes is still incompletely defined. Here we show that the tumor-associated carbonic anhydrases (CAs) are tightly regulated by this system. Both CA9 and CA12 were strongly induced by hypoxia in a range of tumor cell lines. In renal carcinoma cells that are defective for the von Hippel-Lindau (VHL) tumor suppressor, up-regulation of these CAs is associated with loss of regulation by hypoxia, consistent with the critical function of pVHL in the regulation of HIF-1. Further studies of CA9 defined a HIF-1-dependent hypoxia response element in the minimal promoter and demonstrated that tight regulation by the HIF/pVHL system was reflected in the pattern of CA IX expression within tumors. Generalized up-regulation of CA IX in VHL-associated renal cell carcinoma contrasted with focal perinecrotic expression in a variety of non-VHL-associated tumors. In comparison with vascular endothelial growth factor mRNA, expression of CA IX demonstrated a similar, although more tightly circumscribed, pattern of expression around regions of necrosis and showed substantial although incomplete overlap with activation of the hypoxia marker pimonidazole. These studies define a new class of HIF-1-responsive gene, the activation of which has implications for the understanding of hypoxic tumor metabolism and which may provide endogenous markers for tumor hypoxia.

Published
2000

11. Hypoxia response elements

Author

O Rourke, J. F., Dachs, G. U., Gleadle, J. M., Maxwell, P. H., Pugh, C. W., and ian stratford

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