Your search keyword '"Goodship TH"' showing total 170 results

1. Association of a factor H mutation with hemolytic uremic syndrome following a diarrheal illness.

Author

Edey MM, Mead PA, Saunders RE, Strain L, Perkins SJ, Goodship TH, and Kanagasundaram NS

Abstract

Hemolytic uremic syndrome (HUS) takes 2 forms: diarrheal HUS and nondiarrheal HUS. As its name suggests, diarrheal HUS classically follows an enteric infection. The classic infective organism is the Escherichia coli O157 serotype, although other bacteria, including Shigella species, can produce the verocytotoxin required to cause HUS. The usual clinical course is an episode of bloody diarrhea followed by thrombotic microangiopathy and acute renal failure. Supportive treatment sees recovery of renal function in the vast majority of patients. Most cases occur in children, but all age groups can be affected. Conversely, nondiarrheal HUS may have one of a number of predisposing factors, including drugs, irradiation, and hypertension. It also is well established that mutations in the genes encoding the complement regulator proteins factor H, factor I, and membrane cofactor protein predispose to nondiarrheal HUS. In patients with nondiarrheal HUS, recovery of renal function is much less common. Here, we present a case of HUS after a diarrheal illness in which the patient did not recover renal function in the long term. A novel mutation in exon 23 of the factor H gene was discovered. This is clinically important. If this patient underwent transplantation, he would be expected to have an 80% risk of graft loss at 2 years because of recurrent HUS. We recommend consideration of complement gene mutations in any patient with HUS after a diarrheal episode in which there are unusual features. Copyright © 2008 National Kidney Foundation, Inc. [ABSTRACT FROM AUTHOR]

Published

2008

2. Urinary Tract Effects of HPSE2 Mutations

Author

Stuart, H. M., Roberts, N. A., Hilton, E. N., Mckenzie, E. A., Daly, S. B., Hadfield, K. D., Rahal, J. S., Gardiner, N. J., Tanley, S. W., Lewis, M. A., Sites, E., Angle, B., Alves, C., Lourenço, T., Rodrigues, M., Calado, A., Amado, M., Guerreiro, N., Serras, I., Beetz, C., Varga, R. -E., Silay, M. S., Darlow, J. M., Dobson, M. G., Barton, D. E., Hunziker, M., Puri, P., Feather, S. A., Goodship, J. A., Goodship, T. H. J., Lambert, H. J., Cordell, H. J., Saggar, A., Kinali, M., Lorenz, C, Moeller, K, Schaefer, F, Bayazit, Ak, Weber, S, Newman, Wg, Woolf, As, Beattie, J, Bradbuty, M, Coad, N, Coulthard, M, Cuckow, P, Dossetor, J, Dudley, J, Hughes, D, Feather, S, Fitzpatrick, M, Goodship, Ja, Goodship, Th, Griffin, N, Gullett, Am, Haycock, G, Hodes, D, Houtman, P, Hughes, A, Hulton, S, Hunter, E, Iqbal, J, Inward, C, Jackson, J, Jadresic, L, Jaswon, M, Jones, C, Jones, R, Judd, B, Kier, M, Kilby, A, Lambert, H, Lewis, M, Malcolm, S, Marks, S, Maxwell, H, Mcgraw, M, Milford, D, Moghal, N, O'Connor, M, O'Donoghue, Dj, Ognanovic, M, Plant, N, Postlethwaite, R, Rees, L, Reid, C, Rfidah, E, Rigdon, S, Sandford, R, Savage, M, Scanlan, J, Sinha, S, Stephens, S, Stewart, A, Storr, J, Taheri, S, Taylor, Cm, Tizard, J, Trompeter, R, Tullus, K, Verber, I, Van't Hoff, W, Vernon, S, Verrier-Jones, K, Watson, A, Webb, N, Wilcox, D, Aksu, N, Alpay, H, Anarat, A, Arbeiter, K, Ardissino, Gl, Balat, A, Baskin, E, Bayazit, A, Büscher, R, Cakar, N, Caldas Afonso, A, Caliskan, S, Candan, C, Canpolat, N, Donmez, O, Doyon, A, Drozdz, D, Dusek, J, Duzova, A, Emre, S, Erdogan, H, Feldkötter, M, Fischbach, M, Galiano, G, Haffner, D, Harambat, J, Jankauskiene, A, Jeck, N, John, U, Jungraithmair, T, Kemper, M, Kiyak, A, Kracht, D, Kranz, B, Laube, G, Litwin, M, Matteucci, Cm, Montini, G, Melk, A, Mir, S, Niemirska, A, Peco-Antic, A, Ozcelik, G, Pelan, E, Picca, S, Pohl, M, Querfeld, U, Ranchin, B, Shroff, R, Simonetti, G, Sözeri, B, Soylemezoglu, O, Tabel, Y, Testa, S, Trivelli, A, Vidal, E, Wigger, M, Wühl, E, Wygoda, S, Yalcinkaya, F, Yilmaz, E, Zeller, R, Zurowska, Am., and Çukurova Üniversitesi

Subjects

Proband, Male, Urologic Diseases, medicine.medical_specialty, Urinary system, Mutant, Medizin, HDE GEN, Biology, medicine.disease_cause, Brief Communication, Mice, Human genetics, Molecular genetics, medicine, Animals, Humans, Genetics and development, Heparanase, Urinary Tract, Glucuronidase, Genetics, Mutation, Urofacial syndrome, Facies, General Medicine, medicine.disease, 3. Good health, Mice, Inbred C57BL, Nephrology, Pediatric nephrology, Female

Abstract

PubMedID: 25145936 Urofacial syndrome (UFS) is an autosomal recessive congenital disease featuring grimacing and incomplete bladder emptying. Mutations of HPSE2, encoding heparanase 2, a heparanase 1 inhibitor, occur in UFS, but knowledge about the HPSE2 mutation spectrum is limited. Here, seven UFS kindreds with HPSE2 mutations are presented, including one with deleted asparagine 254, suggesting a role for this amino acid, which is conserved in vertebrate orthologs. HPSE2 mutations were absent in 23 non-neurogenic neurogenic bladder probands and, of 439 families with nonsyndromic vesicoureteric reflux, only one carried a putative pathogenic HPSE2 variant. Homozygous Hpse2 mutant mouse bladders contained urine more often than did wild-type organs, phenocopying human UFS. Pelvic ganglia neural cell bodies contained heparanase 1, heparanase 2, and leucine-rich repeats and immunoglobulin-like domains-2 (LRIG2), which is mutated in certain UFS families. In conclusion, heparanase 2 is an autonomic neural protein implicated in bladder emptying, but HPSE2 variants are uncommon in urinary diseases resembling UFS. Copyright © 2015 by the American Society of Nephrology. Kidney Research UK Wellcome Trust: 066647 Medical Research Council: G0600040 Medical Research Council: MR/L002744/1

3. Factor H genotype-phenotype correlations: lessons from aHUS, MPGN II, and AMD.

Author

Goodship TH

Published

2006

4. Factor H autoantibody is associated with atypical hemolytic uremic syndrome in children in the United Kingdom and Ireland.

Author

Brocklebank V, Johnson S, Sheerin TP, Marks SD, Gilbert RD, Tyerman K, Kinoshita M, Awan A, Kaur A, Webb N, Hegde S, Finlay E, Fitzpatrick M, Walsh PR, Wong EKS, Booth C, Kerecuk L, Salama AD, Almond M, Inward C, Goodship TH, Sheerin NS, Marchbank KJ, and Kavanagh D

Subjects

Adolescent, Antibodies, Monoclonal, Humanized therapeutic use, Atypical Hemolytic Uremic Syndrome blood, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome therapy, Child, Child, Preschool, Complement Factor H immunology, Complement System Proteins analysis, Complement System Proteins genetics, Female, Humans, Immunosuppression Therapy adverse effects, Immunosuppression Therapy methods, Infant, Ireland, Kidney Failure, Chronic blood, Kidney Failure, Chronic genetics, Kidney Failure, Chronic therapy, Male, Plasma Exchange, Recurrence, Renal Dialysis, Retrospective Studies, United Kingdom, Atypical Hemolytic Uremic Syndrome immunology, Autoantibodies blood, Kidney Failure, Chronic immunology, Kidney Transplantation

Abstract

Factor H autoantibodies can impair complement regulation, resulting in atypical hemolytic uremic syndrome, predominantly in childhood. There are no trials investigating treatment, and clinical practice is only informed by retrospective cohort analysis. Here we examined 175 children presenting with atypical hemolytic uremic syndrome in the United Kingdom and Ireland for factor H autoantibodies that included 17 children with titers above the international standard. Of the 17, seven had a concomitant rare genetic variant in a gene encoding a complement pathway component or regulator. Two children received supportive treatment; both developed established renal failure. Plasma exchange was associated with a poor rate of renal recovery in seven of 11 treated. Six patients treated with eculizumab recovered renal function. Contrary to global practice, immunosuppressive therapy to prevent relapse in plasma exchange-treated patients was not adopted due to concerns over treatment-associated complications. Without immunosuppression, the relapse rate was high (five of seven). However, reintroduction of treatment resulted in recovery of renal function. All patients treated with eculizumab achieved sustained remission. Five patients received renal transplants without specific factor H autoantibody-targeted treatment with recurrence in one who also had a functionally significant CFI mutation. Thus, our current practice is to initiate eculizumab therapy for treatment of factor H autoantibody-mediated atypical hemolytic uremic syndrome rather than plasma exchange with or without immunosuppression. Based on this retrospective analysis we see no suggestion of inferior treatment, albeit the strength of our conclusions is limited by the small sample size., (Copyright © 2017 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2017

5. Thrombotic Microangiopathy in Inverted Formin 2 - Mediated Renal Disease.

Author

Challis RC, Ring T, Xu Y, Wong EK, Flossmann O, Roberts IS, Ahmed S, Wetherall M, Salkus G, Brocklebank V, Fester J, Strain L, Wilson V, Wood KM, Marchbank KJ, Santibanez-Koref M, Goodship TH, and Kavanagh D

Subjects

Adolescent, Child, Female, Formins, Humans, Pedigree, Atypical Hemolytic Uremic Syndrome complications, Atypical Hemolytic Uremic Syndrome genetics, Microfilament Proteins genetics, Mutation, Thrombotic Microangiopathies etiology

Abstract

The demonstration of impaired C regulation in the thrombotic microangiopathy (TMA) atypical hemolytic uremic syndrome (aHUS) resulted in the successful introduction of the C inhibitor eculizumab into clinical practice. C abnormalities account for approximately 50% of aHUS cases; however, mutations in the non-C gene diacylglycerol kinase- ε have been described recently in individuals not responsive to eculizumab. We report here a family in which the proposita presented with aHUS but did not respond to eculizumab. Her mother had previously presented with a post-renal transplant TMA. Both the proposita and her mother also had Charcot-Marie-Tooth disease. Using whole-exome sequencing, we identified a mutation in the inverted formin 2 gene ( INF2 ) in the mutational hotspot for FSGS. Subsequent analysis of the Newcastle aHUS cohort identified another family with a functionally-significant mutation in INF2 In this family, renal transplantation was associated with post-transplant TMA. All individuals with INF2 mutations presenting with a TMA also had aHUS risk haplotypes, potentially accounting for the genetic pleiotropy. Identifying individuals with TMAs who may not respond to eculizumab will avoid prolonged exposure of such individuals to the infectious complications of terminal pathway C blockade., (Copyright © 2017 by the American Society of Nephrology.)

Published

2017

6. Atypical hemolytic uremic syndrome and C3 glomerulopathy: conclusions from a "Kidney Disease: Improving Global Outcomes" (KDIGO) Controversies Conference.

Author

Goodship TH, Cook HT, Fakhouri F, Fervenza FC, Frémeaux-Bacchi V, Kavanagh D, Nester CM, Noris M, Pickering MC, Rodríguez de Córdoba S, Roumenina LT, Sethi S, and Smith RJ

Subjects

Animals, Atypical Hemolytic Uremic Syndrome drug therapy, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome pathology, Complement C3 genetics, Complement Inactivating Agents therapeutic use, Genetic Predisposition to Disease, Glomerulonephritis drug therapy, Glomerulonephritis genetics, Glomerulonephritis pathology, Humans, Kidney drug effects, Kidney pathology, Phenotype, Risk Factors, Treatment Outcome, Atypical Hemolytic Uremic Syndrome immunology, Complement Activation drug effects, Complement C3 immunology, Glomerulonephritis immunology, Kidney immunology

Abstract

In both atypical hemolytic uremic syndrome (aHUS) and C3 glomerulopathy (C3G) complement plays a primary role in disease pathogenesis. Herein we report the outcome of a 2015 Kidney Disease: Improving Global Outcomes (KDIGO) Controversies Conference where key issues in the management of these 2 diseases were considered by a global panel of experts. Areas addressed included renal pathology, clinical phenotype and assessment, genetic drivers of disease, acquired drivers of disease, and treatment strategies. In order to help guide clinicians who are caring for such patients, recommendations for best treatment strategies were discussed at length, providing the evidence base underpinning current treatment options. Knowledge gaps were identified and a prioritized research agenda was proposed to resolve outstanding controversial issues., (Copyright © 2016 International Society of Nephrology. Published by Elsevier Inc. All rights reserved.)

Published

2017

7. Chromosomal rearrangement-A rare cause of complement factor I associated atypical haemolytic uraemic syndrome.

Author

Gleeson PJ, Wilson V, Cox TE, Sharma SD, Smith-Jackson K, Strain L, Lappin D, McHale T, Kavanagh D, and Goodship TH

Subjects

Adult, Alleles, Atypical Hemolytic Uremic Syndrome blood, Atypical Hemolytic Uremic Syndrome diagnosis, Chromosome Breakpoints, Complement System Proteins genetics, DNA Mutational Analysis, Genotype, Humans, Male, Mutation, Polymorphism, Single Nucleotide, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome immunology, Complement Factor I genetics, Complement Factor I immunology, Genetic Predisposition to Disease, Translocation, Genetic

Abstract

Chromosomal rearrangements affecting the genes encoding complement factor H and the factor H related proteins have been described in aHUS patients. To date such disorders have not been described in other aHUS associated genes. We describe here a heterozygous 875,324bp deletion encompassing the gene (CFI) encoding complement factor I and ten other genes. The index case presented with aHUS and did not recover renal function. No abnormalities were detected on Sanger sequencing of CFI but a low factor I level led to a multiplex ligation-dependent probe amplification assay being undertaken. This showed a complete heterozygous deletion of CFI. The extent of the deletion and the breakpoint was defined. In the Newcastle aHUS cohort we have identified and report here 32 different CFI variants in 56 patients but to date this is the only deletion that we have identified. This finding although rare does suggest that screening for chromosomal rearrangements affecting CFI should be undertaken in all aHUS patients particularly if the factor I level is unexplainably low., (Copyright © 2016 Elsevier GmbH. All rights reserved.)

Published

2016

8. Patient stratification and therapy in atypical haemolytic uraemic syndrome (aHUS).

Author

Wong E, Challis R, Sheerin N, Johnson S, Kavanagh D, and Goodship TH

Subjects

Atypical Hemolytic Uremic Syndrome genetics, Clinical Trials as Topic, Cohort Studies, Complement Pathway, Alternative genetics, England, Humans, Monitoring, Physiologic, Patient Selection, Practice Guidelines as Topic, Risk, Transplant Recipients, Antibodies, Monoclonal, Humanized therapeutic use, Atypical Hemolytic Uremic Syndrome therapy, Complement Factor H genetics, Immunosuppressive Agents therapeutic use, Kidney Transplantation

Abstract

Approximately 50% of aHUS patients have an underlying inherited and/or acquired abnormality of complement which predisposes to excessive activation of the alternative pathway. Use of complement inhibitors such as eculizumab to treat aHUS is therefore logical. Anecdotal reports and subsequent open-label trials demonstrated the efficacy of eculizumab in aHUS leading to approval by both the FDA and EMA. NHS England established in 2013 an interim national service for aHUS including funding for eculizumab for both new patients and those undergoing transplantation. NICE guidance now also recommends eculizumab for funding within the NHS in England under the coordination of an expert centre. The investigation and response to treatment in this cohort provides a unique resource for patient stratification., (Copyright © 2015 Elsevier GmbH. All rights reserved.)

Published

2016

9. A De Novo Deletion in the Regulators of Complement Activation Cluster Producing a Hybrid Complement Factor H/Complement Factor H-Related 3 Gene in Atypical Hemolytic Uremic Syndrome.

Author

Challis RC, Araujo GS, Wong EK, Anderson HE, Awan A, Dorman AM, Waldron M, Wilson V, Brocklebank V, Strain L, Morgan BP, Harris CL, Marchbank KJ, Goodship TH, and Kavanagh D

Subjects

Animals, Cells, Cultured, Complement Factor H genetics, Humans, Sheep, Atypical Hemolytic Uremic Syndrome genetics, Blood Proteins genetics, Complement Activation genetics, Gene Deletion

Abstract

The regulators of complement activation cluster at chromosome 1q32 contains the complement factor H (CFH) and five complement factor H-related (CFHR) genes. This area of the genome arose from several large genomic duplications, and these low-copy repeats can cause genome instability in this region. Genomic disorders affecting these genes have been described in atypical hemolytic uremic syndrome, arising commonly through nonallelic homologous recombination. We describe a novel CFH/CFHR3 hybrid gene secondary to a de novo 6.3-kb deletion that arose through microhomology-mediated end joining rather than nonallelic homologous recombination. We confirmed a transcript from this hybrid gene and showed a secreted protein product that lacks the recognition domain of factor H and exhibits impaired cell surface complement regulation. The fact that the formation of this hybrid gene arose as a de novo event suggests that this cluster is a dynamic area of the genome in which additional genomic disorders may arise., (Copyright © 2016 by the American Society of Nephrology.)

Published

2016

10. A national specialized service in England for atypical haemolytic uraemic syndrome-the first year's experience.

Author

Sheerin NS, Kavanagh D, Goodship TH, and Johnson S

Subjects

Adolescent, Adult, Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal, Humanized adverse effects, Child, Child, Preschool, England, Female, Humans, Male, Meningococcal Infections prevention & control, Middle Aged, Renal Dialysis methods, Young Adult, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal, Humanized administration & dosage, Atypical Hemolytic Uremic Syndrome diagnosis, Atypical Hemolytic Uremic Syndrome drug therapy, Kidney physiopathology

Abstract

Background: In 2013 NHS England commissioned the use of eculizumab for both new patients with atypical haemolytic uraemic syndrome (aHUS) and those undergoing transplantation. This national service is delivered locally but coordinated by an expert centre at the Newcastle upon Tyne Hospitals NHS Foundation Trust., Results: In the first year of service, 43 aHUS patients received eculizumab, 15 children and 28 adults. Twenty-three were new patients and 20 prevalent. Fifteen of the 23 new patients required dialysis before eculizumab was started, 8 of these recovered renal function. Twelve of the 20 prevalent patients who received eculizumab were transplant patients, 8 with prophylactic use and 4 for recurrent disease; the outcome in all was good. Eculizumab was withdrawn in 14 patients, 5 were patients who had not recovered renal function. In 3 of the 14 patients, it was necessary to reintroduce eculizumab because of recurrent disease (2 extra-renal and 1 renal). There were 2 deaths in the 43 patients, and neither was associated with use of eculizumab. There were no episodes of meningococcal disease., Conclusions: The establishment of this national service has enabled aHUS patients in England to receive eculizumab when they need it for as long as they need it., (© The Author 2015. Published by Oxford University Press on behalf of the Association of Physicians. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2016

11. The role of ADAMTS-13 activity and complement mutational analysis in differentiating acute thrombotic microangiopathies.

Author

Phillips EH, Westwood JP, Brocklebank V, Wong EK, Tellez JO, Marchbank KJ, McGuckin S, Gale DP, Connolly J, Goodship TH, Kavanagh D, and Scully MA

Subjects

Acute Disease, Adolescent, Adult, Aged, Atypical Hemolytic Uremic Syndrome genetics, Child, Preschool, DNA Mutational Analysis, Female, Humans, Incidence, Infant, Kidney Function Tests, Male, Membrane Cofactor Protein genetics, Middle Aged, Mutation, Phenotype, Platelet Count, Purpura, Thrombotic Thrombocytopenic diagnosis, Purpura, Thrombotic Thrombocytopenic genetics, Retrospective Studies, Young Adult, ADAMTS13 Protein genetics, ADAMTS13 Protein metabolism, Complement C3 genetics, Complement Factor B genetics, Thrombotic Microangiopathies diagnosis, Thrombotic Microangiopathies genetics

Abstract

Unlabelled: ESSENTIALS: Molecular diagnostics has improved the differentiation of acute thrombotic microangiopathys (TMAs). Atypical hemolytic uremic syndrome may have features mimicking thrombotic thrombocytopenic purpura. We identified novel complement mutations and a high incidence of CD46, with favorable long term outcomes. Complement mutation analysis in TMA where the diagnosis is unclear and ADAMTS-13 activity is >10%., Background: Differentiation of acute thrombotic microangiopathy (TMA) at presentation has historically been dependent on clinical parameters. Confirmation of thrombotic thrombocytopenic purpura (TTP) is increasingly reliant on demonstrating deficient ADAMTS-13 activity. The identification of alternative complement pathway abnormalities in atypical hemolytic uremic syndrome (aHUS), along with the proven efficacy of terminal complement inhibitors in treatment, has increased the need for rapid differentiation of TTP from aHUS., Objectives: We describe the clinical phenotype and nature of complement mutations in a cohort of aHUS patients referred as acute TMAs., Patients/methods: Fourteen consecutive aHUS patients were screened for mutations in C3, CD46, CFH, CFI, and CFB, as well as factor H (FH) antibodies. All aHUS patients had ADAMTS-13 activity > 10%., Results: Of 14 aHUS patients, 11 (79%) had platelet counts < 30 × 10(9) /L during the acute phase. Median presenting creatinine level was 295 μmol L(-1) , while five (36%) of 14 presented with a serum creatinine level < 200 μmol L(-1) . Alternative complement pathway mutations were detected in 9 (64%) of 14 patients, including CD46 mutations in five (36%) of 14 patients. Patients were identified with novel mutations in CFB and C3 that have not been previously reported., Conclusions: We demonstrate that diagnostic differentiation based on platelet count and renal function is insufficient to predict an underlying complement mutation in some aHUS cases. Specifically, we demonstrate a high frequency of functionally significant CD46 mutations which may mimic TTP. ADAMTS-13 activity > 10% in a patient with a TMA should necessitate genetic screening for complement abnormalities., (© 2015 The Authors. Journal of Thrombosis and Haemostasis published by Wiley Periodicals, Inc. on behalf of International Society on Thrombosis and Haemostasis.)

Published

2016

12. Use of eculizumab in crescentic IgA nephropathy: proof of principle and conundrum?

Author

Ring T, Pedersen BB, Salkus G, and Goodship TH

Abstract

IgA nephropathy (IgAN) is characterized by a variable clinical course and multifaceted pathophysiology. There is substantial evidence to suggest that complement activation plays a pivotal role in the pathogenesis of the disease. Therefore, complement inhibition using the humanized anti-C5 monoclonal antibody eculizumab could be a rational treatment. We report here a 16-year-old male with the vasculitic form of IgAN who failed to respond to aggressive conventional therapy including high-dose steroids, cyclophosphamide and plasma exchange and who was treated with four weekly doses of 900 mg eculizumab followed by a single dose of 1200 mg. He responded rapidly to this treatment and has had a stable creatinine around 150 µmol/L (1.67 mg/dL) for >6 months. However, proteinuria was unabated on maximal conventional anti-proteinuric treatment, and a repeat renal biopsy 11 months after presentation revealed severe chronic changes. We believe this case provides proof of principle that complement inhibition may be beneficial in IgAN but also that development of chronicity may be independent of complement.

Published

2015

13. Thrombotic Microangiopathy as a Cause of Chronic Kidney Transplant Dysfunction: Case Report Demonstrating Successful Treatment with Eculizumab.

Author

Iqbal Z, Wood K, Carter V, Goodship TH, Brown AL, and Sheerin NS

Subjects

Chronic Disease, Female, Humans, Kidney pathology, Middle Aged, Primary Graft Dysfunction diagnosis, Primary Graft Dysfunction drug therapy, Recurrence, Thrombotic Microangiopathies etiology, Antibodies, Monoclonal, Humanized therapeutic use, Kidney Transplantation, Primary Graft Dysfunction etiology, Thrombotic Microangiopathies drug therapy

Abstract

Atypical hemolytic uremic syndrome is a rare disease associated with genetic or acquired defects in complement regulation which frequently leads to renal failure. Disease often recurs early after kidney transplantation, leading to a rapid irreversible loss of function. Extrarenal features, such as hemolysis and thrombocytopenia, may not always occur, and diagnosis is made by demonstrating the classic features of thrombotic microangiopathy on renal biopsy. Eculizumab, a terminal complement inhibitor, has been used successfully to treat fulminant early recurrent disease after transplantation. We describe a case of disease recurrence presenting in the second year after transplantation with a gradual decline in function and the first report of eculizumab treatment for chronic thrombotic microangiopathy in a transplanted kidney. The resultant diagnostic challenges and successful response to eculizumab in this setting are discussed., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

14. Atypical aHUS: State of the art.

Author

Nester CM, Barbour T, de Cordoba SR, Dragon-Durey MA, Fremeaux-Bacchi V, Goodship TH, Kavanagh D, Noris M, Pickering M, Sanchez-Corral P, Skerka C, Zipfel P, and Smith RJ

Subjects

Adult, Atypical Hemolytic Uremic Syndrome etiology, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome immunology, Autoantibodies biosynthesis, Child, Communicable Diseases complications, Communicable Diseases genetics, Communicable Diseases immunology, Complement Activation, Complement C3b genetics, Complement C3b immunology, Complement C3b Inactivator Proteins genetics, Complement C3b Inactivator Proteins immunology, Complement Factor H genetics, Complement Factor H immunology, Genetic Predisposition to Disease, Humans, Kidney immunology, Kidney Neoplasms complications, Kidney Neoplasms genetics, Kidney Neoplasms immunology, Kidney Transplantation, Atypical Hemolytic Uremic Syndrome pathology, Communicable Diseases pathology, Gene Expression Regulation immunology, Kidney pathology, Kidney Neoplasms pathology

Abstract

Tremendous advances in our understanding of the thrombotic microangiopathies (TMAs) have revealed distinct disease mechanisms within this heterogeneous group of diseases. As a direct result of this knowledge, both children and adults with complement-mediated TMA now enjoy higher expectations for long-term health. In this update on atypical hemolytic uremic syndrome, we review the clinical characteristics; the genetic and acquired drivers of disease; the broad spectrum of environmental triggers; and current diagnosis and treatment options. Many questions remain to be addressed if additional improvements in patient care and outcome are to be achieved in the coming decade., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

15. Mutations in TBX18 Cause Dominant Urinary Tract Malformations via Transcriptional Dysregulation of Ureter Development.

Author

Vivante A, Kleppa MJ, Schulz J, Kohl S, Sharma A, Chen J, Shril S, Hwang DY, Weiss AC, Kaminski MM, Shukrun R, Kemper MJ, Lehnhardt A, Beetz R, Sanna-Cherchi S, Verbitsky M, Gharavi AG, Stuart HM, Feather SA, Goodship JA, Goodship TH, Woolf AS, Westra SJ, Doody DP, Bauer SB, Lee RS, Adam RM, Lu W, Reutter HM, Kehinde EO, Mancini EJ, Lifton RP, Tasic V, Lienkamp SS, Jüppner H, Kispert A, and Hildebrandt F

Subjects

Base Sequence, Electrophoretic Mobility Shift Assay, Exome genetics, HEK293 Cells, Humans, Immunohistochemistry, Immunoprecipitation, Microscopy, Fluorescence, Molecular Sequence Data, Pedigree, Sequence Analysis, DNA, Gene Expression Regulation, Developmental genetics, Genes, Dominant genetics, Muscle, Smooth embryology, Mutation genetics, T-Box Domain Proteins genetics, Ureter embryology, Urinary Tract abnormalities

Abstract

Congenital anomalies of the kidneys and urinary tract (CAKUT) are the most common cause of chronic kidney disease in the first three decades of life. Identification of single-gene mutations that cause CAKUT permits the first insights into related disease mechanisms. However, for most cases the underlying defect remains elusive. We identified a kindred with an autosomal-dominant form of CAKUT with predominant ureteropelvic junction obstruction. By whole exome sequencing, we identified a heterozygous truncating mutation (c.1010delG) of T-Box transcription factor 18 (TBX18) in seven affected members of the large kindred. A screen of additional families with CAKUT identified three families harboring two heterozygous TBX18 mutations (c.1570C>T and c.487A>G). TBX18 is essential for developmental specification of the ureteric mesenchyme and ureteric smooth muscle cells. We found that all three TBX18 altered proteins still dimerized with the wild-type protein but had prolonged protein half life and exhibited reduced transcriptional repression activity compared to wild-type TBX18. The p.Lys163Glu substitution altered an amino acid residue critical for TBX18-DNA interaction, resulting in impaired TBX18-DNA binding. These data indicate that dominant-negative TBX18 mutations cause human CAKUT by interference with TBX18 transcriptional repression, thus implicating ureter smooth muscle cell development in the pathogenesis of human CAKUT., (Copyright © 2015 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2015

16. Case report: Benefits and challenges of long-term eculizumab in atypical hemolytic uremic syndrome.

Author

Cullinan N, Gorman KM, Riordan M, Waldron M, Goodship TH, and Awan A

Subjects

Female, Humans, Infant, Time Factors, Antibodies, Monoclonal, Humanized administration & dosage, Atypical Hemolytic Uremic Syndrome drug therapy

Abstract

Atypical hemolytic uremic syndrome (aHUS) is caused by dysregulation of the complement system, leading to complement overactivation. A humanized anti-C5 monoclonal antibody, eculizumab, has been available for the treatment of aHUS since 2011. The long-term safety and efficacy of this novel drug in the pediatric population remain under review. We present a child with a hybrid CFH/CFHR3 gene who, having had multiple disease relapses despite optimal treatment with plasma exchange, commenced eculizumab therapy in August 2010. She remains relapse free in follow-up at 52 months, and treatment has been well tolerated. The risk of meningococcal disease during this treatment is recognized. Despite vaccination against meningococcal disease and appropriate antibiotic prophylaxis, our patient developed meningococcal bacteremia 30 months into treatment. She presented with nonspecific symptoms but recovered without sequelae with appropriate treatment. We recommend that children be vaccinated against invasive meningococcal infection before beginning eculizumab therapy and take appropriate antibiotic prophylaxis during treatment, and we suggest that vaccine responses should be checked and followed annually. Clinicians need to maintain a high index of suspicion for invasive meningococcal disease. Neither vaccination nor antibiotic prophylaxis provides complete protection in patients on eculizumab therapy. The appropriate dosage of eculizumab needed to achieve remission in aHUS in the pediatric population is unknown. Having achieved remission in our patient, we monitor eculizumab and CH50 levels to evaluate ongoing blockade of the terminal complement cascade. Such information may help guide dosing intervals in the future., (Copyright © 2015 by the American Academy of Pediatrics.)

Published

2015

17. Plasma resistant atypical hemolytic uremic syndrome associated with a CFH mutation treated with eculizumab: a case report.

Author

Sevinc M, Basturk T, Sahutoglu T, Sakaci T, Koc Y, Ahbap E, Akgol C, Kara E, Brocklebank V, Goodship TH, Kavanagh D, and Unsal A

Subjects

Adult, Atypical Hemolytic Uremic Syndrome genetics, Atypical Hemolytic Uremic Syndrome therapy, Female, Humans, Male, Pedigree, Plasma Exchange, Renal Dialysis, Thrombotic Microangiopathies drug therapy, Antibodies, Monoclonal, Humanized therapeutic use, Atypical Hemolytic Uremic Syndrome drug therapy, Complement Factor H genetics, Complement Inactivating Agents therapeutic use, Mutation

Abstract

Introduction: Thrombotic microangiopathies are a group of diseases presenting as microangiopathic hemolytic anemia, thrombocytopenia and end-organ dysfunction. As the role of the complement system was elucidated in atypical hemolytic uremic syndrome pathogenesis, eculizumab was successfully introduced into clinical practice. We present a large pedigree with multiple individuals carrying a functionally significant novel factor H mutation. We describe the proband's presentation following a presumed infectious trigger requiring plasma exchange and hemodialysis., Case Presentation: A 32-year-old Caucasian woman presented with pyrexia and headache lasting one week to our Emergency Department. She gave no history of diarrhea or other symptoms to account for her high temperature. She was not taking any medication. She was pyrexial (38°C), tachycardic (110 bpm) and hypertensive (160/110 mmHg). Her fundoscopy revealed grade IV hypertensive retinopathy. She had mild pretibial and periorbital edema, with oliguria (450 mL/day). She had a pregnancy one year previously, during which she had hypertension, proteinuria and edema, with successful delivery at term. Her mother had died in her early 30s with a clinical picture consistent with thrombotic microangiopathy. Her laboratory evaluation showed microangiopathic hemolytic anemia. After 22 sessions of plasma exchange, her lactate dehydrogenase levels started to climb. As a result, she was classified as plasma resistant and eculizumab therapy was instituted. Her lactate dehydrogenase level and platelet count normalized, and her renal function recovered after three months of dialysis., Conclusions: We demonstrate that, even in patients with atypical hemolytic uremic syndrome and prolonged dialysis dependence, recovery of renal function can be seen with eculizumab treatment. We suggest a treatment regime of at least three months prior to evaluation of efficacy.

Published

2015

18. Urinary tract effects of HPSE2 mutations.

Author

Stuart HM, Roberts NA, Hilton EN, McKenzie EA, Daly SB, Hadfield KD, Rahal JS, Gardiner NJ, Tanley SW, Lewis MA, Sites E, Angle B, Alves C, Lourenço T, Rodrigues M, Calado A, Amado M, Guerreiro N, Serras I, Beetz C, Varga RE, Silay MS, Darlow JM, Dobson MG, Barton DE, Hunziker M, Puri P, Feather SA, Goodship JA, Goodship TH, Lambert HJ, Cordell HJ, Saggar A, Kinali M, Lorenz C, Moeller K, Schaefer F, Bayazit AK, Weber S, Newman WG, and Woolf AS

Subjects

Animals, Facies, Female, Humans, Male, Mice, Mice, Inbred C57BL, Mutation, Urologic Diseases physiopathology, Glucuronidase genetics, Urinary Tract physiopathology, Urologic Diseases genetics

Abstract

Urofacial syndrome (UFS) is an autosomal recessive congenital disease featuring grimacing and incomplete bladder emptying. Mutations of HPSE2, encoding heparanase 2, a heparanase 1 inhibitor, occur in UFS, but knowledge about the HPSE2 mutation spectrum is limited. Here, seven UFS kindreds with HPSE2 mutations are presented, including one with deleted asparagine 254, suggesting a role for this amino acid, which is conserved in vertebrate orthologs. HPSE2 mutations were absent in 23 non-neurogenic neurogenic bladder probands and, of 439 families with nonsyndromic vesicoureteric reflux, only one carried a putative pathogenic HPSE2 variant. Homozygous Hpse2 mutant mouse bladders contained urine more often than did wild-type organs, phenocopying human UFS. Pelvic ganglia neural cell bodies contained heparanase 1, heparanase 2, and leucine-rich repeats and immunoglobulin-like domains-2 (LRIG2), which is mutated in certain UFS families. In conclusion, heparanase 2 is an autonomic neural protein implicated in bladder emptying, but HPSE2 variants are uncommon in urinary diseases resembling UFS., (Copyright © 2015 by the American Society of Nephrology.)

Published

2015

19. Autoantibodies to CD59, CD55, CD46 or CD35 are not associated with atypical haemolytic uraemic syndrome (aHUS).

Author

Watson R, Wearmouth E, McLoughlin AC, Jackson A, Ward S, Bertram P, Bennaceur K, Barker CE, Pappworth IY, Kavanagh D, Lea SM, Atkinson JP, Goodship TH, and Marchbank KJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Antibody Formation immunology, Atypical Hemolytic Uremic Syndrome blood, Autoantibodies blood, Blood Donors, Case-Control Studies, Child, Child, Preschool, Escherichia coli metabolism, Female, Humans, Male, Middle Aged, Recombinant Proteins isolation & purification, Young Adult, Antigens, CD immunology, Atypical Hemolytic Uremic Syndrome immunology, Autoantibodies immunology

Abstract

Autoantibody formation against Factor H (FH) is found in 7-10% of patients who are diagnosed with atypical haemolytic uraemic syndrome (aHUS). These autoantibodies predominately target the C-terminal cell binding recognition domain of FH and are associated with absence of FHR1. Additional autoantibodies have also been identified in association with aHUS, for example autoantibodies to Factor I. Based on this, and that there are genetic mutations in other complement regulators and activators associated with aHUS, we hypothesised that other complement regulator proteins, particularly surface bound regulators in the kidney, might be the target for autoantibody formation in aHUS. Therefore, we assayed serum derived from 89 patients in the Newcastle aHUS cohort for the presence of autoantibodies to CD46 (membrane cofactor protein, MCP), CD55 (decay accelerating factor, DAF), CD35 (complement receptor type 1, CR1; TP10) and CD59. We also assayed 100 healthy blood donors to establish the normal levels of reactivity towards these proteins in the general population. Recombinant proteins CD46 and CD55 (purified from Escherichia coli) as well as soluble CR1 (CD35) and oligomeric C4BP-CD59 (purified from eukaryotic cell media) were used in ELISA to detect high responders. False positive results were established though Western blot and flow cytometric analysis. After excluding false positive responders to bacterial proteins in the CD46 and CD55 preparations, and responses to blood group antigens in CD35, we found no significant level of patient serum IgG reactivity with CD46, CD55, CD35 or CD59 above that detected in the normal population. These results suggest that membrane anchored complement regulators are not a target for autoantibody generation in aHUS., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

20. Characterization of a factor H mutation that perturbs the alternative pathway of complement in a family with membranoproliferative GN.

Author

Wong EK, Anderson HE, Herbert AP, Challis RC, Brown P, Reis GS, Tellez JO, Strain L, Fluck N, Humphrey A, Macleod A, Richards A, Ahlert D, Santibanez-Koref M, Barlow PN, Marchbank KJ, Harris CL, Goodship TH, and Kavanagh D

Subjects

Animals, Complement Factor H chemistry, Complement Factor H immunology, Complement Pathway, Alternative immunology, Crystallography, X-Ray, Erythrocytes cytology, Family Health, Female, Haplotypes, Hereditary Complement Deficiency Diseases, Heterozygote, Humans, Kidney Diseases immunology, Male, Pedigree, Polymorphism, Genetic, Protein Structure, Tertiary, Sheep, Structure-Activity Relationship, Complement Factor H deficiency, Complement Factor H genetics, Complement Pathway, Alternative genetics, Erythrocytes immunology, Glomerulonephritis, Membranoproliferative genetics, Glomerulonephritis, Membranoproliferative immunology, Kidney Diseases genetics

Abstract

Complement C3 activation is a characteristic finding in membranoproliferative GN (MPGN). This activation can be caused by immune complex deposition or an acquired or inherited defect in complement regulation. Deficiency of complement factor H has long been associated with MPGN. More recently, heterozygous genetic variants have been reported in sporadic cases of MPGN, although their functional significance has not been assessed. We describe a family with MPGN and acquired partial lipodystrophy. Although C3 nephritic factor was shown in family members with acquired partial lipodystrophy, it did not segregate with the renal phenotype. Genetic analysis revealed a novel heterozygous mutation in complement factor H (R83S) in addition to known risk polymorphisms carried by individuals with MPGN. Patients with MPGN had normal levels of factor H, and structural analysis of the mutant revealed only subtle alterations. However, functional analysis revealed profoundly reduced C3b binding, cofactor activity, and decay accelerating activity leading to loss of regulation of the alternative pathway. In summary, this family showed a confluence of common and rare functionally significant genetic risk factors causing disease. Data from our analysis of these factors highlight the role of the alternative pathway of complement in MPGN., (Copyright © 2014 by the American Society of Nephrology.)

Published

2014

21. Factors determining penetrance in familial atypical haemolytic uraemic syndrome.

Author

Sansbury FH, Cordell HJ, Bingham C, Bromilow G, Nicholls A, Powell R, Shields B, Smyth L, Warwicker P, Strain L, Wilson V, Goodship JA, Goodship TH, and Turnpenny PD

Subjects

Adult, Aged, Child, Preschool, Complement Factor H genetics, Female, Humans, Male, Middle Aged, Pedigree, Atypical Hemolytic Uremic Syndrome genetics, Penetrance

Abstract

Background: Inherited abnormalities of complement are found in ∼60% of patients with atypical haemolytic uraemic syndrome (aHUS). Such abnormalities are not fully penetrant. In this study, we have estimated the penetrance of the disease in three families with a CFH mutation (c.3643C>G; p. Arg1215Gly) in whom a common lineage is probable. 25 individuals have been affected with aHUS with three peaks of incidence-early childhood (n=6), early adulthood (n=11) and late adulthood (n=8). Eighteen individuals who have not developed aHUS carry the mutation., Methods: We estimated penetrance at the ages of 4, 27, 60 and 70 years as both a binary and a survival trait using MLINK and Mendel. We genotyped susceptibility factors in CFH, CD46 and CFHR1 in affected and unaffected carriers., Results and Conclusions: We found that the estimates of penetrance at the age of 4 years ranged from <0.01 to 0.10, at the age of 27 years from 0.16 to 0.29, at the age of 60 years from 0.39 to 0.51 and at the age of 70 years from 0.44 to 0.64. We found that the CFH haplotype on the allele not carrying the CFH mutation had a significant effect on disease penetrance. In this family, we did not find that the CD46 haplotypes had a significant effect on penetrance., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions.)

Published

2014

22. A novel method for direct measurement of complement convertases activity in human serum.

Author

Blom AM, Volokhina EB, Fransson V, Strömberg P, Berghard L, Viktorelius M, Mollnes TE, López-Trascasa M, van den Heuvel LP, Goodship TH, Marchbank KJ, and Okroj M

Subjects

Animals, Autoantibodies immunology, Complement C3 Nephritic Factor immunology, Complement C3-C5 Convertases immunology, Complement Pathway, Alternative immunology, Complement System Proteins immunology, Erythrocytes immunology, Guinea Pigs, Half-Life, Humans, Rabbits, Sheep, Complement C3-C5 Convertases analysis, Erythrocytes enzymology, Immunoassay methods

Abstract

Complement convertases are enzymatic complexes that play a central role in sustaining and amplification of the complement cascade. Impairment of complement function leads directly or indirectly to pathological conditions, including higher infection rate, kidney diseases, autoimmune- or neurodegenerative diseases and ischaemia-reperfusion injury. An assay for direct measurement of activity of the convertases in patient sera is not available. Existing assays testing convertase function are based on purified complement components and, thus, convertase formation occurs under non-physiological conditions. We designed a new assay, in which C5 blocking compounds enabled separation of the complement cascade into two phases: the first ending at the stage of C5 convertases and the second ending with membrane attack complex formation. The use of rabbit erythrocytes or antibody-sensitized sheep erythrocytes as the platforms for convertase formation enabled easy readout based on measurement of haemolysis. Thus, properties of patient sera could be studied directly regarding convertase activity and membrane attack complex formation. Another advantage of this assay was the possibility to screen for host factors such as C3 nephritic factor and other anti-complement autoantibodies, or gain-of-function mutations, which prolong the half-life of complement convertases. Herein, we present proof of concept, detailed description and validation of this novel assay., (© 2014 British Society for Immunology.)

Published

2014

23. Atypical haemolytic uraemic syndrome associated with a CD46 mutation triggered by Shigella flexneri.

Author

Brocklebank V, Wong EK, Fielding R, Goodship TH, and Kavanagh D

Abstract

We present a case of haemolytic uraemic syndrome (HUS) triggered by Shigella flexneri . Of the Shigella species, only S. dysenteriae type 1 is said to produce Shiga toxin and consequently cause HUS. Investigation of the complement system in this patient revealed a CD46 mutation. In individuals with mutations in complement genes incomplete penetrance of atypical HUS (aHUS) is seen, suggesting that a trigger, such as infection, is required for disease to manifest. In an era of complement modulatory therapy for aHUS it is important to be alert to unusual presentations of diarrhoeal-associated disease.

Published

2014

24. Complement therapy in atypical haemolytic uraemic syndrome (aHUS).

Author

Wong EK, Goodship TH, and Kavanagh D

Subjects

Antibodies, Monoclonal adverse effects, Antibodies, Monoclonal, Humanized adverse effects, Atypical Hemolytic Uremic Syndrome, Complement System Proteins immunology, Diacylglycerol Kinase genetics, Hemolytic-Uremic Syndrome diagnosis, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome immunology, Humans, Penetrance, Prognosis, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, Hemolytic-Uremic Syndrome therapy, Plasma Exchange

Abstract

Central to the pathogenesis of atypical haemolytic uraemic syndrome (aHUS) is over-activation of the alternative pathway of complement. Inherited defects in complement genes and autoantibodies against complement regulatory proteins have been described. The use of plasma exchange to replace non-functioning complement regulators and hyper-functional complement components in addition to the removal of CFH-autoantibodies made this the 'gold-standard' for management of aHUS. In the last 4 years the introduction of the complement inhibitor Eculizumab has revolutionised the management of aHUS. In this review we shall discuss the available literature on treatment strategies to date., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

25. Genotype/phenotype correlations in complement factor H deficiency arising from uniparental isodisomy.

Author

Wilson V, Darlay R, Wong W, Wood KM, McFarlane J, Schejbel L, Schmidt IM, Harris CL, Tellez J, Hunze EM, Marchbank K, Goodship JA, and Goodship TH

Subjects

Atypical Hemolytic Uremic Syndrome, Complement Factor H genetics, Haplotypes genetics, Hereditary Complement Deficiency Diseases, Homozygote, Humans, Infant, Male, Membrane Cofactor Protein genetics, Mutation genetics, Polymorphism, Single Nucleotide genetics, Complement Factor H deficiency, Genotype, Hemolytic-Uremic Syndrome genetics, Kidney Diseases genetics, Phenotype, Uniparental Disomy genetics

Abstract

We report a male infant who presented at 8 months of age with atypical hemolytic uremic syndrome (aHUS) responsive to plasma therapy. Investigation showed him to have complement factor H (CFH) deficiency associated with a homozygous CFH mutation (c.2880delT [p.Phe960fs]). Mutation screening of the child's parents revealed that the father was heterozygous for this change but that it was not present in his mother. Chromosome 1 uniparental isodisomy of paternal origin was confirmed by genotyping chromosome 1 SNPs. CD46 SNP genotyping was undertaken in this individual and another patient with CFH deficiency associated with chromosome 1 uniparental isodisomy. This showed a homozygous aHUS risk haplotype (CD46GGAAC) in the patient with aHUS and a homozygous glomerulonephritis risk haplotype (CD46AAGGT) in the patient with endocapillary glomerulonephritis. We also showed that FHL-1 (factor H-like protein 1) was present in the patient with aHUS and absent in the patient with glomerulonephritis. This study emphasizes that modifiers such as CD46 and FHL-1 may determine the kidney phenotype of patients who present with homozygous CFH deficiency., (Copyright © 2013 National Kidney Foundation, Inc. Published by Elsevier Inc. All rights reserved.)

Published

2013

26. Atypical hemolytic uremic syndrome.

Author

Kavanagh D, Goodship TH, and Richards A

Subjects

Antibodies, Monoclonal, Humanized therapeutic use, Atypical Hemolytic Uremic Syndrome, Autoantibodies, Complement Factor H genetics, Complement Factor H immunology, Complement System Proteins immunology, Complement System Proteins metabolism, Humans, Kidney Transplantation adverse effects, Kidney Transplantation mortality, Precipitating Factors, Complement Activation physiology, Complement System Proteins genetics, Hemolytic-Uremic Syndrome etiology, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome physiopathology

Abstract

Hemolytic uremic syndrome (HUS) is a triad of microangiopathic hemolytic anemia, thrombocytopenia, and acute renal failure. The atypical form of HUS is a disease characterized by complement overactivation. Inherited defects in complement genes and acquired autoantibodies against complement regulatory proteins have been described. Incomplete penetrance of mutations in all predisposing genes is reported, suggesting that a precipitating event or trigger is required to unmask the complement regulatory deficiency. The underlying genetic defect predicts the prognosis both in native kidneys and after renal transplantation. The successful trials of the complement inhibitor eculizumab in the treatment of atypical HUS will revolutionize disease management., (© 2013 Elsevier Inc. All rights reserved.)

Published

2013

27. Prevalence in the General Population of a CFH Sequence Variant Associated with Atypical Haemolytic Uraemic Syndrome in an Extensive Family from Southwest England.

Author

Hamilton AJ, Lyons CB, Goodship TH, and Bingham C

Abstract

Background/aims: Twenty-five members of a family from the county of Devon in England have been affected by atypical haemolytic uraemic syndrome (aHUS) associated with a CFH mutation (c.3643C>G; p.Arg1215Gly). A 65-year-old male was diagnosed with aHUS after losing a renal transplant to a thrombotic microangiopathy. Subsequent mutation screening revealed the same CFH mutation without him being knowingly related to the local kindred. We designed a study to investigate the prevalence of this mutation in the local area. In addition, we examined the diagnoses of pre-existing haemodialysis patients to determine whether other patients might unknowingly be at risk of carrying the same CFH mutation., Methods: The Exeter Ten Thousand (EXTEND) study aims to recruit 10,000 healthy volunteers over the age of 18 years living within 25 miles of Exeter in Devon. We genotyped DNA from 4,000 EXTEND subjects for CFH c.3643C>G; p.Arg1215Gly. We reviewed the diagnoses of 294 haemodialysis patients in the Devon area and genotyped 7 patients with either end-stage renal disease of unknown aetiology, malignant hypertension or renovascular disease., Results: CFH c.3643C>G; p.Arg1215Gly was not detected in any of the 7 haemodialysis patients or the 4,000 individuals within the EXTEND study., Conclusions: We conclude that CFH c.3643C>G; p.Arg1215Gly is not endemic in Devon. This reinforces our existing practice of genotyping only patients with kidney disease and evidence of a thrombotic microangiopathy for this mutation. This is the first study looking at the prevalence of CFH mutations in the general population.

Published

2013

28. Eculizumab therapy for atypical haemolytic uraemic syndrome due to a gain-of-function mutation of complement factor B.

Author

Gilbert RD, Fowler DJ, Angus E, Hardy SA, Stanley L, and Goodship TH

Subjects

Atypical Hemolytic Uremic Syndrome, Biomarkers blood, Biopsy, Complement Membrane Attack Complex metabolism, Female, Genetic Predisposition to Disease, Hemolytic-Uremic Syndrome diagnosis, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome immunology, Humans, Infant, L-Lactate Dehydrogenase blood, Phenotype, Treatment Outcome, Antibodies, Monoclonal, Humanized therapeutic use, Complement Factor B genetics, Hemolytic-Uremic Syndrome drug therapy, Immunologic Factors therapeutic use, Mutation

Abstract

Background: Atypical haemolytic uraemic syndrome (aHUS) is caused by dysregulated complement activation. A humanised anti-C5 monoclonal antibody has recently become available for treatment of this condition, Case-Diagnosis/treatment: We present the first description of an infant with an activating mutation of complement factor B successfully treated with eculizumab. On standard doses she had evidence of ongoing C5 cleavage despite a good clinical response., Conclusions: Eculizumab is effective therapy for aHUS associated with factor B mutations, but recommended doses may not be adequate for all patients.

Published

2013

29. Cisplatin-induced haemolytic uraemic syndrome associated with a novel intronic mutation of CD46 treated with eculizumab.

Author

Gilbert RD, Stanley LK, Fowler DJ, Angus EM, Hardy SA, and Goodship TH

Abstract

A 2-year-old patient with a neuroblastoma developed haemolytic uraemic syndrome (HUS) following treatment with cisplatin and carboplatin. Following treatment with eculizumab, there was a substantial improvement in renal function with the recovery of the platelet count and the cessation of haemolysis. Subsequent investigations showed a novel, heterozygous CD46 splice site mutation with reduced peripheral blood neutrophil CD46 expression. Withdrawal of eculizumab was followed by the recurrence of disease activity, which resolved with re-introduction of therapy. Abnormal regulation of complement may be associated with other cases of cisplatin-induced HUS and treatment with eculizumab may be appropriate for other affected individuals.

Published

2013

30. Changing strategies for organ transplantation in atypical haemolytic uraemic syndrome: a tertiary case series.

Author

Forbes TA, Bradbury MG, Goodship TH, McKiernan PJ, and Milford DV

Subjects

Antibodies, Monoclonal, Humanized therapeutic use, Anticoagulants therapeutic use, Atypical Hemolytic Uremic Syndrome, Child, Child, Preschool, Complement Factor H metabolism, Female, Humans, Male, Plasma Exchange, Quality of Life, Renal Insufficiency therapy, Risk, Treatment Outcome, Hemolytic-Uremic Syndrome therapy, Kidney Transplantation methods, Liver Transplantation methods

Abstract

We present three cases of organ transplantation for atypical haemolytic uraemic syndrome secondary to complement factor H mutation: one isolated renal transplant; one previously reported isolated liver transplant; and one combined liver and kidney transplant. All three patients were treated prior to the licensing of eculizumab for this condition, and all have had favourable outcomes with maintenance of graft function for years following transplantation. We discuss the evolution of transplantation therapy for aHUS over the last two decades. Transplantation decision-making in aHUS has evolved over this time with expanding knowledge of pathophysiology and genetics, alongside refined plasma exchange and anticoagulation protocols and improved centre experience. Our cases demonstrate how individual patient factors within this heterogeneous condition also underlie transplantation decisions and outcomes. Whilst our cases demonstrate that transplantation in aHUS can be a successful long-term treatment providing good quality of life, worldwide experience has proven that most curative treatment for aHUS strategies represents significant risks. Whether new pharmacotherapies such as eculizumab will alter this risk is yet to be determined., (© 2013 John Wiley & Sons A/S.)

Published

2013

31. Determining the population frequency of the CFHR3/CFHR1 deletion at 1q32.

Author

Holmes LV, Strain L, Staniforth SJ, Moore I, Marchbank K, Kavanagh D, Goodship JA, Cordell HJ, and Goodship TH

Subjects

Humans, Sequence Deletion genetics, Complement C3b Inactivator Proteins genetics, Gene Frequency genetics

Abstract

In this study we have used multiplex ligation-dependent probe amplification (MLPA) to measure the copy number of CFHR3 and CFHR1 in DNA samples from 238 individuals from the UK and 439 individuals from the HGDP-CEPH Human Genome Diversity Cell Line Panel. We have then calculated the allele frequency and frequency of homozygosity for the copy number polymorphism represented by the CFHR3/CFHR1 deletion. There was a highly significant difference between geographical locations in both the allele frequency (X(2)  = 127.7, DF = 11, P-value = 4.97x10(-22)) and frequency of homozygosity (X(2)  = 142.3, DF = 22, P-value = 1.33x10(-19)). The highest frequency for the deleted allele (54.7%) was seen in DNA samples from Nigeria and the lowest (0%) in samples from South America and Japan. The observed frequencies in conjunction with the known association of the deletion with AMD, SLE and IgA nephropathy is in keeping with differences in the prevalence of these diseases in African and European Americans. This emphasises the importance of identifying copy number polymorphism in disease.

Published

2013

32. Combined complement gene mutations in atypical hemolytic uremic syndrome influence clinical phenotype.

Author

Bresin E, Rurali E, Caprioli J, Sanchez-Corral P, Fremeaux-Bacchi V, Rodriguez de Cordoba S, Pinto S, Goodship TH, Alberti M, Ribes D, Valoti E, Remuzzi G, and Noris M

Subjects

Adult, Atypical Hemolytic Uremic Syndrome, Child, Child, Preschool, Complement C3 genetics, Complement Factor B genetics, Complement Factor H genetics, Female, Fibrinogen genetics, Genetic Association Studies, Haplotypes, Humans, Infant, Male, Membrane Cofactor Protein genetics, Middle Aged, Pedigree, Penetrance, Risk Factors, Young Adult, Complement System Proteins genetics, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome immunology, Mutation

Abstract

Several abnormalities in complement genes reportedly contribute to atypical hemolytic uremic syndrome (aHUS), but incomplete penetrance suggests that additional factors are necessary for the disease to manifest. Here, we sought to describe genotype-phenotype correlations among patients with combined mutations, defined as mutations in more than one complement gene. We screened 795 patients with aHUS and identified single mutations in 41% and combined mutations in 3%. Only 8%-10% of patients with mutations in CFH, C3, or CFB had combined mutations, whereas approximately 25% of patients with mutations in MCP or CFI had combined mutations. The concomitant presence of CFH and MCP risk haplotypes significantly increased disease penetrance in combined mutated carriers, with 73% penetrance among carriers with two risk haplotypes compared with 36% penetrance among carriers with zero or one risk haplotype. Among patients with CFH or CFI mutations, the presence of mutations in other genes did not modify prognosis; in contrast, 50% of patients with combined MCP mutation developed end stage renal failure within 3 years from onset compared with 19% of patients with an isolated MCP mutation. Patients with combined mutations achieved remission with plasma treatment similar to patients with single mutations. Kidney transplant outcomes were worse, however, for patients with combined MCP mutation compared with an isolated MCP mutation. In summary, these data suggest that genotyping for the risk haplotypes in CFH and MCP may help predict the risk of developing aHUS in unaffected carriers of mutations. Furthermore, screening patients with aHUS for all known disease-associated genes may inform decisions about kidney transplantation.

Published

2013

33. Sensitive and specific assays for C3 nephritic factors clarify mechanisms underlying complement dysregulation.

Author

Paixão-Cavalcante D, López-Trascasa M, Skattum L, Giclas PC, Goodship TH, de Córdoba SR, Truedsson L, Morgan BP, and Harris CL

Subjects

Animals, Biomarkers blood, CD55 Antigens metabolism, Case-Control Studies, Complement C3 metabolism, Complement C3-C5 Convertases metabolism, Complement Factor D metabolism, Complement Factor H metabolism, Complement Hemolytic Activity Assay, Enzyme-Linked Immunosorbent Assay, Glomerulonephritis, Membranoproliferative blood, Glomerulonephritis, Membranoproliferative immunology, Humans, Predictive Value of Tests, Properdin metabolism, Protein Binding, Receptors, Complement metabolism, Reproducibility of Results, Sensitivity and Specificity, Sheep, Time Factors, Complement Activation, Complement C3 Nephritic Factor metabolism, Glomerulonephritis, Membranoproliferative diagnosis, Immunoassay methods

Abstract

C3 nephritic factors are autoantibodies that prolong the half-life or prevent regulation of the alternative pathway C3 convertase, resulting in uncontrolled complement activation. They are strongly associated with renal disease but their role in pathogenesis remains controversial. Here we optimized and compared a panel of assays to identify and interrogate nephritic factor activities. Of 101 patients with histologic or clinically evident disease, 48 were positive in some or all assays. In the presence of properdin, binding of autoantibody was detected in 39 samples and convertase stabilization was detected in 36. Forty-two of 48 nephritic factors tested prevented convertase decay by factor H, and most of these by decay accelerating factor (28) and complement receptor 1 (34). Representative properdin-independent nephritic factors had no effect on C5 cleavage and terminal pathway activity, while properdin-dependent nephritic factors enhanced activity. Biacore analysis of four purified IgG samples confirmed resistance to decay and showed that properdin-independent nephritic factors increased convertase half-life over 50-fold, whereas properdin-dependent nephritic factors increased the half-life 10- to 20-fold and also increased activity of the C3 convertase up to 10-fold. Thus, our study provides a rational approach to detect and characterize nephritic factors in patients.

Published

2012

34. Factor H autoantibodies in membranoproliferative glomerulonephritis.

Author

Goodship TH, Pappworth IY, Toth T, Denton M, Houlberg K, McCormick F, Warland D, Moore I, Hunze EM, Staniforth SJ, Hayes C, Cavalcante DP, Kavanagh D, Strain L, Herbert AP, Schmidt CQ, Barlow PN, Harris CL, and Marchbank KJ

Subjects

Adolescent, Adult, Aged, Binding Sites, Antibody, Complement C3, Complement C3 Nephritic Factor analysis, Complement Factor H chemistry, Female, Glomerulonephritis, Membranoproliferative genetics, Humans, Male, Middle Aged, Young Adult, Autoantibodies blood, Autoantibodies immunology, Complement Factor H immunology, Glomerulonephritis, Membranoproliferative immunology

Abstract

Factor H autoantibodies are found in ~10% of aHUS patients. Most are associated with complete deficiency of factor H related proteins 1/3 and bind to the C terminal recognition domain. MPGN, like aHUS, is characterised by complement activation. In this study we, therefore, examined the hypothesis that factor H autoantibodies are associated with MPGN. We screened sera from 16 MPGN patients and 100 normal controls using ELISA and detected strongly positive IgG factor H autoantibodies in 2 patients. One patient had type II (DDD) MPGN (male aged 24 yrs) with C3NeF and the other type I (female aged 26 yrs) with no detectable C3NeF. We identified the binding site of the autoantibodies using small SCR domain fragments in the ELISA and showed that the autoantibodies in both patients bound predominately to the N terminal complement regulatory domain of factor H. We measured CFHR 1/3 copy number using MLPA and showed that both patients had 2 copies of CFHR1 and 3. Finally, we examined the functionality of detected factor H autoantibodies using purified patient IgG and observed increased haemolysis when purified IgG from both patients was added to normal human sera prior to incubation with rabbit red blood cells. Thus, in a cohort of MPGN patients we have found a high titre of functionally significant factor H autoantibodies in two patients with MPGN. Antibody depleting therapy may have a role in such patients and we suggest that screening for factor H autoantibodies should be undertaken in all patients with MPGN., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

35. Postpartum aHUS secondary to a genetic abnormality in factor H acquired through liver transplantation.

Author

Brown JH, Tellez J, Wilson V, Mackie IJ, Scully M, Tredger MM, Moore I, McDougall NI, Strain L, Marchbank KJ, Sheerin NS, O'Grady J, Harris CL, and Goodship TH

Subjects

Adult, Budd-Chiari Syndrome surgery, Female, Homozygote, Humans, Complement Factor H genetics, Liver Transplantation, Postpartum Period

Abstract

We report here a young female who underwent a successful deceased donor liver transplant for hepatic vein thrombosis. Five years after transplantation she developed postpartum atypical hemolytic uremic syndrome (aHUS). She did not recover renal function. Mutation screening of complement genes in her DNA did not show any abnormality. Mutation screening of DNA available from the donor showed a nonsense CFH mutation leading to factor H deficiency. Genotyping of the patient showed that she was homozygous for an aHUS CD46 at-risk haplotype. In this individual, the development of aHUS has been facilitated by the combination of a trigger (pregnancy), an acquired rare genetic variant (CFH mutation) and a common susceptibility factor (CD46 haplotype)., (© Copyright 2012 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2012

36. Factor I autoantibodies in patients with atypical hemolytic uremic syndrome: disease-associated or an epiphenomenon?

Author

Kavanagh D, Pappworth IY, Anderson H, Hayes CM, Moore I, Hunze EM, Bennaceur K, Roversi P, Lea S, Strain L, Ward R, Plant N, Nailescu C, Goodship TH, and Marchbank KJ

Subjects

Adult, Atypical Hemolytic Uremic Syndrome, Blotting, Western, Case-Control Studies, Child, Preschool, Complement Factor H genetics, DNA Mutational Analysis, England, Enzyme-Linked Immunosorbent Assay, Female, Genetic Predisposition to Disease, Hemolytic-Uremic Syndrome blood, Hemolytic-Uremic Syndrome genetics, Humans, Infant, Male, Mutation, Prognosis, Risk Assessment, Risk Factors, Time Factors, Autoantibodies blood, Complement Factor I immunology, Hemolytic-Uremic Syndrome immunology

Abstract

Background and Objectives: Atypical hemolytic uremic syndrome is a disease associated with mutations in the genes encoding the complement regulators factors H and I. In addition, factor H autoantibodies have been reported in ∼10% of patients with atypical hemolytic uremic syndrome. This study searched for the presence of factor I autoantibodies in atypical hemolytic uremic syndrome., Design, Setting, Participants, & Measurements: This study screened 175 atypical hemolytic uremic syndrome patients for factor I autoantibodies using ELISA with confirmatory Western blotting. Functional studies using purified immunoglobulin from one patient were subsequently undertaken., Results: Factor I autoantibodies were detected in three patients. In one patient with a high titer of autoantibody, the titer was tracked over time and was found to have no association with disease activity. This study found evidence of an immune complex of antibody and factor I in this patient, but purified IgG, isolated from current serum samples, had only a minor effect on fluid phase and cell surface complement regulation. Genetic analysis of the three patients with factor I autoantibodies revealed that they had two copies of the genes encoding factor H-related proteins 1 and 3 and therefore, did not have a deletion commonly associated with factor H autoantibodies in atypical hemolytic uremic syndrome. Two patients, however, had functionally significant mutations in complement factor H., Conclusions: These findings reinforce the concept of multiple concurrent risk factors being associated with atypical hemolytic uremic syndrome but question whether autoantibodies per se predispose to atypical hemolytic uremic syndrome.

Published

2012

37. Complement polymorphisms: geographical distribution and relevance to disease.

Author

Ermini L, Wilson IJ, Goodship TH, and Sheerin NS

Subjects

Africa South of the Sahara, Complement System Proteins metabolism, Europe, Evolution, Molecular, Genetic Predisposition to Disease, Genotype, Geography, Humans, Macular Degeneration immunology, Polymorphism, Single Nucleotide, Selection, Genetic, Complement System Proteins genetics, Genetic Variation, Macular Degeneration genetics

Abstract

The evolution of man has been characterised by recurrent episodes of migration and settlement with infectious disease a constant threat. This long history of demographic change, together with the action of evolutionary forces such as natural selection and genetic drift, has shaped human genetic diversity. In particular, the interaction between humans, pathogens and the environment has played a crucial role in generating patterns of human genetic variation. The complement system plays a crucial role in the early protective immune response after exposure to a pathogen. Pathogens, over time, have developed mechanisms to circumvent the effects of complement which in turn has led to development of a more complex complement system. During the evolution of the complement system genes coding complement proteins have evolved polymorphisms, some of which have a functional effect, and this may reflect human-pathogen interaction and geographical origin. An example is the polymorphism Ile62Val (rs800292 (A>G)) in the complement regulator Factor H gene which alters the susceptibility to age-related macular degeneration (AMD), with the Ile62 polymorphism protecting against AMD. When sub-Saharan African and European populations are compared, the frequency of this polymorphism shows a very marked geographical distribution. Polymorphisms in other complement genes such as complement factor B show similar trends. This paper describes the geographical variation present in complement genes and discusses the implications of these observations. The analysis of genetic variation in complement genes is a promising tool to unravel mechanisms of host-pathogen interaction and can provide new insights into the evolution of the human immune system., (Copyright © 2011 Elsevier GmbH. All rights reserved.)

Published

2012

38. A novel hybrid CFH/CFHR3 gene generated by a microhomology-mediated deletion in familial atypical hemolytic uremic syndrome.

Author

Francis NJ, McNicholas B, Awan A, Waldron M, Reddan D, Sadlier D, Kavanagh D, Strain L, Marchbank KJ, Harris CL, and Goodship TH

Subjects

Animals, Apolipoproteins metabolism, Atypical Hemolytic Uremic Syndrome, Autoantibodies, Base Sequence, Blood Proteins metabolism, Blotting, Western, Complement Activation, Complement C3b Inactivator Proteins metabolism, Complement Factor H metabolism, Erythrocytes metabolism, Hemolysis, Hemolytic-Uremic Syndrome metabolism, Hemolytic-Uremic Syndrome pathology, Homologous Recombination, Humans, Molecular Sequence Data, Mutant Chimeric Proteins genetics, Mutant Chimeric Proteins metabolism, Mutation genetics, Pedigree, Sequence Homology, Nucleic Acid, Sheep, Surface Plasmon Resonance, Apolipoproteins genetics, Blood Proteins genetics, Complement C3b Inactivator Proteins genetics, Complement Factor H genetics, Gene Deletion, Genetic Predisposition to Disease, Hemolytic-Uremic Syndrome genetics

Abstract

Genomic disorders affecting the genes encoding factor H (fH) and the 5 factor H related proteins have been described in association with atypical hemolytic uremic syndrome. These include deletions of CFHR3, CFHR1, and CFHR4 in association with fH autoantibodies and the formation of a hybrid CFH/CFHR1 gene. These occur through nonallelic homologous recombination secondary to the presence of large segmental duplications (macrohomology) in this region. Using multiplex ligation-dependent probe amplification to screen for such genomic disorders, we have identified a large atypical hemolytic uremic syndrome family where a deletion has occurred through microhomology-mediated end joining rather than nonallelic homologous recombination. In the 3 affected persons of this family, we have shown that the deletion results in formation of a CFH/CFHR3 gene. We have shown that the protein product of this is a 24 SCR protein that is secreted with normal fluid-phase activity but marked loss of complement regulation at cell surfaces despite increased heparin binding. In this study, we have therefore shown that microhomology in this area of chromosome 1 predisposes to disease associated genomic disorders and that the complement regulatory function of fH at the cell surface is critically dependent on the structural integrity of the whole molecule.

Published

2012

39. Common genetic variants in complement genes other than CFH, CD46 and the CFHRs are not associated with aHUS.

Author

Ermini L, Goodship TH, Strain L, Weale ME, Sacks SH, Cordell HJ, Fremeaux-Bacchi V, and Sheerin NS

Subjects

Adult, Case-Control Studies, Cohort Studies, Complement C3 genetics, Complement Factor I genetics, Complement System Proteins genetics, Female, Genetic Predisposition to Disease, Genotype, Haplotypes genetics, Humans, Linkage Disequilibrium genetics, Male, Middle Aged, Mutation, Polymorphism, Single Nucleotide, Risk Factors, White People, Young Adult, Apolipoproteins genetics, Complement Factor H genetics, Hemolytic-Uremic Syndrome genetics, Membrane Cofactor Protein genetics

Abstract

It is well established that common genetic variants in CFH, CD46 and the CFHRs are additional risk factors for the development of aHUS. To examine the hypothesis that common variants in other complement genes have a similar effect we genotyped 501 SNPs in 47 complement genes in 94 aHUS patients from Newcastle, 126 aHUS patients from Paris, 374 UK controls and 165 French controls. We replicated the associations in CFH, CD46 and the CFHRs but found no association with any other complement gene. The strongest associations replicated in both cohorts were found for four SNPs within CD46 (p-value<10(-3)) and five SNPs within CFH (p-value<5×10(-3)). Significant replicable associations with single SNPs in CFHR2, CFHR4 and an intergenic SNP (CR1-CD46) were also found. Analysis of the Paris cohort showed that the association with CD46 SNPs was only present in those patients with complement mutations. Haplotype analysis showed at-risk and protective haplotypes in both CD46 and CFH. The CD46 haplotype was only disease-associated in those patients with mutations., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2012

40. Plasma therapy for atypical haemolytic uraemic syndrome associated with heterozygous factor H mutations.

Author

Kim JJ, Goodship TH, Tizard J, and Inward C

Subjects

Atypical Hemolytic Uremic Syndrome, DNA Mutational Analysis, Humans, Infant, Complement Factor H genetics, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome therapy, Mutation, Plasma Exchange, Plasmapheresis

Abstract

Atypical haemolytic uraemic syndrome (aHUS) is frequently associated with mutations in the gene encoding complement factor H (CFH). The clinical response to plasma therapy in aHUS is variable. We present here our experience of plasma therapy in three aHUS patients with CFH mutations. Three children presented aged 4, 22 and 6 months (patients 1-3 respectively) in acute kidney injury requiring dialysis. Plasma therapy consisting of plasma filtration (patient 1) or plasma exchange (PEX; patients 2 and 3) was commenced early following presentation. This resulted in aHUS remission and cessation of dialysis after 2 weeks, 9 days and 2 weeks respectively. Relapses were common and associated with increasing the interval between PEX, but all responded to intensification of PEX therapy. Patient 1 recovered 50% of renal function after first presentation. She had four relapses and started peritoneal dialysis 41 months after presentation. Mutation screening of CFH showed a missense mutation (c.3546 G > T, p.Arg1182Ser) in exon 23. PEX in patient 2 was slowly tapered over 4 months to fortnightly sessions, but she relapsed when PEX was extended to every 4 weeks. Renal function remained normal 12 months post-presentation. Mutation screening of CFH showed a mutation in exon 23 (c.3590 T > C, p.Val1197Ala) and two additional sequence variants in exons 3 and 4. Patient 3 had two relapses associated with intercurrent illnesses concurrent with reducing PEX to weekly doses. Renal function was normal 5 months post-presentation. All three patients showed a good response to PEX with improved renal function both initially and following a relapse. Further research is necessary to determine the best maintenance strategy to delay or prevent end-stage kidney disease.

Published

2011

41. Successful treatment of de novo posttransplant thrombotic microangiopathy with eculizumab.

Author

Wilson CH, Brown AL, White SA, Goodship TH, Sheerin NS, and Manas DM

Subjects

Hemolytic-Uremic Syndrome drug therapy, Humans, Male, Middle Aged, Plasmapheresis, Antibodies, Monoclonal, Humanized therapeutic use, Complement C5a antagonists & inhibitors, Diabetic Nephropathies surgery, Kidney Transplantation adverse effects, Pancreas Transplantation adverse effects, Postoperative Complications drug therapy, Thrombotic Microangiopathies drug therapy

Published

2011

42. Monogenic diabetes, renal dysplasia and hypopituitarism: a patient with a HNF1A mutation.

Author

Simms RJ, Sayer JA, Quinton R, Walker M, Ellard S, and Goodship TH

Subjects

Abnormalities, Multiple genetics, Adult, Female, Genitalia, Female abnormalities, Humans, Pedigree, Diabetes Mellitus, Type 2 genetics, Frameshift Mutation, Hepatocyte Nuclear Factor 1-alpha genetics, Hypopituitarism genetics, Kidney abnormalities

Published

2011

43. Association of genetic variants in complement factor H and factor H-related genes with systemic lupus erythematosus susceptibility.

Author

Zhao J, Wu H, Khosravi M, Cui H, Qian X, Kelly JA, Kaufman KM, Langefeld CD, Williams AH, Comeau ME, Ziegler JT, Marion MC, Adler A, Glenn SB, Alarcón-Riquelme ME, Pons-Estel BA, Harley JB, Bae SC, Bang SY, Cho SK, Jacob CO, Vyse TJ, Niewold TB, Gaffney PM, Moser KL, Kimberly RP, Edberg JC, Brown EE, Alarcon GS, Petri MA, Ramsey-Goldman R, Vilá LM, Reveille JD, James JA, Gilkeson GS, Kamen DL, Freedman BI, Anaya JM, Merrill JT, Criswell LA, Scofield RH, Stevens AM, Guthridge JM, Chang DM, Song YW, Park JA, Lee EY, Boackle SA, Grossman JM, Hahn BH, Goodship TH, Cantor RM, Yu CY, Shen N, and Tsao BP

Subjects

Black or African American genetics, Alleles, Asian People genetics, Case-Control Studies, Chromosomes, Human, Pair 1 genetics, Gene Deletion, Gene Frequency, Genotype, Hispanic or Latino genetics, Humans, Introns, Lupus Erythematosus, Systemic ethnology, White People genetics, Antigens, Neoplasm genetics, Biomarkers, Tumor genetics, Complement Factor H genetics, Genetic Predisposition to Disease, Lupus Erythematosus, Systemic genetics, Polymorphism, Single Nucleotide

Abstract

Systemic lupus erythematosus (SLE), a complex polygenic autoimmune disease, is associated with increased complement activation. Variants of genes encoding complement regulator factor H (CFH) and five CFH-related proteins (CFHR1-CFHR5) within the chromosome 1q32 locus linked to SLE, have been associated with multiple human diseases and may contribute to dysregulated complement activation predisposing to SLE. We assessed 60 SNPs covering the CFH-CFHRs region for association with SLE in 15,864 case-control subjects derived from four ethnic groups. Significant allelic associations with SLE were detected in European Americans (EA) and African Americans (AA), which could be attributed to an intronic CFH SNP (rs6677604, in intron 11, P(meta) = 6.6×10(-8), OR = 1.18) and an intergenic SNP between CFHR1 and CFHR4 (rs16840639, P(meta) = 2.9×10(-7), OR = 1.17) rather than to previously identified disease-associated CFH exonic SNPs, including I62V, Y402H, A474A, and D936E. In addition, allelic association of rs6677604 with SLE was subsequently confirmed in Asians (AS). Haplotype analysis revealed that the underlying causal variant, tagged by rs6677604 and rs16840639, was localized to a ~146 kb block extending from intron 9 of CFH to downstream of CFHR1. Within this block, the deletion of CFHR3 and CFHR1 (CFHR3-1Δ), a likely causal variant measured using multiplex ligation-dependent probe amplification, was tagged by rs6677604 in EA and AS and rs16840639 in AA, respectively. Deduced from genotypic associations of tag SNPs in EA, AA, and AS, homozygous deletion of CFHR3-1Δ (P(meta) = 3.2×10(-7), OR = 1.47) conferred a higher risk of SLE than heterozygous deletion (P(meta) = 3.5×10(-4), OR = 1.14). These results suggested that the CFHR3-1Δ deletion within the SLE-associated block, but not the previously described exonic SNPs of CFH, might contribute to the development of SLE in EA, AA, and AS, providing new insights into the role of complement regulators in the pathogenesis of SLE., Competing Interests: The authors have declared that no competing interests exist.

Published

2011

44. Primary, nonsyndromic vesicoureteric reflux and nephropathy in sibling pairs: a United Kingdom cohort for a DNA bank.

Author

Lambert HJ, Stewart A, Gullett AM, Cordell HJ, Malcolm S, Feather SA, Goodship JA, Goodship TH, and Woolf AS

Subjects

Adolescent, Adult, Blood Pressure, Child, Child, Preschool, Cohort Studies, Databases, Nucleic Acid, Female, Glomerular Filtration Rate, Humans, Infant, Male, Middle Aged, Proteinuria genetics, Siblings, United Kingdom, Vesico-Ureteral Reflux ethnology, Kidney Diseases genetics, Vesico-Ureteral Reflux genetics

Abstract

Background and Objectives: Primary vesicoureteric reflux (VUR) can coexist with reflux nephropathy (RN) and impaired renal function. VUR appears to be an inherited condition and is reported in approximately one third of siblings of index cases. The objective was to establish a DNA collection and clinical database from U.K. families containing affected sibling pairs for future VUR genetics studies. The cohort's clinical characteristics have been described., Design, Setting, Participants, & Measurements: Most patients were identified from tertiary pediatric nephrology centers; each family had an index case with cystography-proven primary, nonsyndromic VUR. Affected siblings had radiologically proven VUR and/or radiographically proven RN., Results: One hundred eighty-nine index cases identified families with an additional 218 affected siblings. More than 90% were <20 years at the study's end. Blood was collected and leukocyte DNA extracted from all 407 patients and from 189 mothers and 183 fathers. Clinical presentation was established in 122; 92 had urinary tract infections and 16 had abnormal antenatal renal scans. RN was radiologically proven in 223 patients. Four patients had been transplanted; none were on dialysis. In 174 others aged >1 year, estimated GFR (eGFR) was calculated. Five had eGFR 15 to 59 and 48 had eGFR 60 to 89 ml/min per 1.73 m(2). Values were lower in bilateral RN patients than in those with either unilateral or absent RN., Conclusions: The large DNA collection from families with VUR and associated RN constitutes a resource for researchers exploring the most likely complex, genetic components predisposing to VUR and RN., (© 2011 by the American Society of Nephrology)

Published

2011

45. Prevention of large-vessel stenoses in atypical hemolytic uremic syndrome associated with complement dysregulation.

Author

Davin JC, Majoie C, Groothoff J, Gracchi V, Bouts A, Goodship TH, and Loirat C

Subjects

Adolescent, Atypical Hemolytic Uremic Syndrome, Child, Preschool, Complement System Proteins genetics, Female, Gene Expression Regulation, Hemolytic-Uremic Syndrome complications, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome immunology, Humans, Intracranial Arteriosclerosis prevention & control, Magnetic Resonance Angiography, Mutation, Pedigree, Plasma Exchange, Siblings, Intracranial Arteriosclerosis etiology

Published

2011

46. Atypical hemolytic uremic syndrome, genetic basis, and clinical manifestations.

Author

Kavanagh D and Goodship TH

Subjects

Atypical Hemolytic Uremic Syndrome, Hemolytic-Uremic Syndrome diagnosis, Hemolytic-Uremic Syndrome therapy, Humans, Membrane Cofactor Protein metabolism, Risk Factors, Genetic Predisposition to Disease, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome pathology

Abstract

Atypical hemolytic uremic syndrome (aHUS) is now well recognized to be a disease characterized by excessive complement activation in the microvasculature. In both the familial and sporadic forms, inherited and acquired abnormalities affecting components of the alternative complement pathway are found in ~ 60% of patients. These include mutations in the genes encoding both complement regulators (factor H, factor I, membrane cofactor protein, and thrombomodulin) and activators (factors B and C3) and autoantibodies against factor H. Multiple hits are necessary for the disease to manifest, including a trigger, mutations, and at-risk haplotypes in complement genes. The prognosis for aHUS is poor, with most patients developing end-stage renal failure. Renal transplantation in most patients also has a poor prognosis, with frequent loss of the allograft to recurrent disease. However, improving results with combined liver-kidney transplantation and the advent of complement inhibitors such as eculizumab offer hope that the prognosis for aHUS will improve in future years.

Published

2011

47. Complement factor h autoantibodies and age-related macular degeneration.

Author

Dhillon B, Wright AF, Tufail A, Pappworth I, Hayward C, Moore I, Strain L, Kavanagh D, Barlow PN, Herbert AP, Schmidt CQ, Armbrecht AM, Laude A, Deary IJ, Staniforth SJ, Holmes LV, Goodship TH, and Marchbank KJ

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Blood Donors, Blood Proteins genetics, Case-Control Studies, Complement C3b Inactivator Proteins genetics, Complement Factor H immunology, DNA Primers chemistry, DNA Probes chemistry, Enzyme-Linked Immunosorbent Assay, Female, Gene Dosage, Gene Frequency, Humans, Male, Middle Aged, Nucleic Acid Amplification Techniques, Polymerase Chain Reaction, Young Adult, Autoantibodies blood, Macular Degeneration immunology

Abstract

Purpose: In this case-control study, the hypothesis that factor H autoantibodies are associated with age-related macular degeneration (AMD) was examined., Methods: One hundred AMD patients (median age, 78 years), 98 age-matched control subjects (median age, 78 years) known not to have AMD, and 100 healthy blood donors (median age, 43 years) were enrolled. An enzyme-linked immunosorbent assay (ELISA) was used to screen for complement factor H autoantibodies and either quantitative polymerase chain reaction (qPCR) or multiplex ligation-dependent probe amplification (MLPA) were performed to measure the copy number of the gene encoding complement factor H-related protein 3 (CFHR3)., Results: There was a significant difference in the median complement factor H autoantibody titer between the three groups (AMD patients, 196 reference units [RU]]; age-match control subjects, 316 RU; and blood donor control subjects, 121 RU; Kruskal-Wallis test, P < 0.001). Pair-wise comparison (Mann-Whitney test) showed that all three groups were significantly different from each other. Two different thresholds were used in the healthy blood donors to identify individuals with complement factor H autoantibodies. Both suggested that the prevalence of factor H autoantibodies was decreased in AMD patients. The CFHR3 copy number was measured as a surrogate for the deletion of the genes encoding complement factor H-related proteins 3 and 1 (CFHR3/1). The allele frequency of the deletion was significantly higher in the age-matched control subjects than in the AMD patients (22.2% vs. 8.2%)., Conclusions: The level of factor H autoantibodies is lower in AMD patients than in age-matched control subjects.

Published

2010

48. Relative role of genetic complement abnormalities in sporadic and familial aHUS and their impact on clinical phenotype.

Author

Noris M, Caprioli J, Bresin E, Mossali C, Pianetti G, Gamba S, Daina E, Fenili C, Castelletti F, Sorosina A, Piras R, Donadelli R, Maranta R, van der Meer I, Conway EM, Zipfel PF, Goodship TH, and Remuzzi G

Subjects

Adolescent, Adult, Aged, 80 and over, Autoantibodies blood, Chi-Square Distribution, Complement C3 genetics, Complement Factor H genetics, Complement System Proteins immunology, DNA Mutational Analysis, Disease-Free Survival, Female, Gene Frequency, Genetic Predisposition to Disease, Genetic Testing, Hemolytic-Uremic Syndrome immunology, Hemolytic-Uremic Syndrome mortality, Hemolytic-Uremic Syndrome therapy, Humans, Infant, Infant, Newborn, Kaplan-Meier Estimate, Kidney Transplantation, Male, Membrane Cofactor Protein genetics, Pedigree, Phenotype, Proportional Hazards Models, Recurrence, Registries, Risk Assessment, Risk Factors, Thrombomodulin genetics, Time Factors, Treatment Outcome, Young Adult, Complement System Proteins genetics, Hemolytic-Uremic Syndrome genetics, Mutation, Polymorphism, Genetic

Abstract

Background and Objectives: Hemolytic uremic syndrome (HUS) is characterized by microangiopathic hemolytic anemia, thrombocytopenia, and renal impairment. Most childhood cases are caused by Shiga toxin-producing bacteria. The other form, atypical HUS (aHUS), accounts for 10% of cases and has a poor prognosis. Genetic complement abnormalities have been found in aHUS., Design, Setting, Participants, and Measurements: We screened 273 consecutive patients with aHUS for complement abnormalities and studied their role in predicting clinical phenotype and response to treatment. We compared mutation frequencies and localization and clinical outcome in familial (82) and sporadic (191) cases., Results: In >70% of sporadic and familial cases, gene mutations, disease-associated factor H (CFH) polymorphisms, or anti-CFH autoantibodies were found. Either mutations or CFH polymorphisms were also found in the majority of patients with secondary aHUS, suggesting a genetic predisposition. Familial cases showed a higher prevalence of mutations in SCR20 of CFH and more severe disease than sporadic cases. Patients with CFH or THBD (thrombomodulin) mutations had the earliest onset and highest mortality. Membrane-cofactor protein (MCP) mutations were associated with the best prognosis. Plasma therapy induced remission in 55 to 80% of episodes in patients with CFH, C3, or THBD mutations or autoantibodies, whereas patients with CFI (factor I) mutations were poor responders. aHUS recurred frequently after kidney transplantation except for patients with MCP mutations., Conclusions: Results underline the need of genetic screening for all susceptibility factors as part of clinical management of aHUS and for identification of patients who could safely benefit from kidney transplant.

Published

2010

49. Non-atheromatous arterial stenoses in atypical haemolytic uraemic syndrome associated with complement dysregulation.

Author

Loirat C, Macher MA, Elmaleh-Berges M, Kwon T, Deschênes G, Goodship TH, Majoie C, Davin JC, Blanc R, Savatovsky J, Moret J, and Fremeaux-Bacchi V

Subjects

Adolescent, Female, Humans, Renal Replacement Therapy adverse effects, Arterial Occlusive Diseases etiology, Complement Factor B genetics, Hemolytic-Uremic Syndrome complications, Mutation

Abstract

Background: A child, who presented atypical haemolytic uraemic syndrome (aHUS) at the age of 1 month, developed cerebral ischaemic events at the age of 10 years., Results: Stenoses of both carotid arteries, left subclavian and vertebral arteries, several intracranial, right humeral, several coronary, and all pulmonary arteries were demonstrated. At the age of 13 years, left subclavian and right cervical carotid arteries were occluded. Right carotid recanalization induced intracranial dissection and death. The child had a Lys350Asp factor B mutation., Conclusion: Arterial steno-occlusive lesions appear as potential complications of dysregulated complement activation in aHUS. Endovascular treatment should be considered cautiously in this setting.

Published

2010

50. Successful isolated liver transplantation in a child with atypical hemolytic uremic syndrome and a mutation in complement factor H.

Author

Haller W, Milford DV, Goodship TH, Sharif K, Mirza DF, and McKiernan PJ

Subjects

Caliciviridae Infections etiology, Gastroenteritis virology, Hemolytic-Uremic Syndrome physiopathology, Herpesvirus 4, Human, Heterozygote, Humans, Infant, Newborn, Kidney physiopathology, Male, Norovirus, Postoperative Complications, Risk Assessment, Secondary Prevention, Viremia etiology, Complement Factor H genetics, Hemolytic-Uremic Syndrome genetics, Hemolytic-Uremic Syndrome surgery, Liver Transplantation adverse effects, Mutation

Abstract

A male infant was diagnosed with atypical hemolytic uremic syndrome (aHUS) at the age of 5.5 months. Sequencing of the gene (CFH) encoding complement factor H revealed a heterozygous mutation (c.3644G>A, p.Arg1215Gln). Despite maintenance plasmapheresis he developed recurrent episodes of aHUS and vascular access complications while maintaining stable renal function. At the age of 5 years he received an isolated split liver graft following a previously established protocol using pretransplant plasma exchange (PE) and intratransplant plasma infusion. Graft function, renal function and disease remission are preserved 2 years after transplantation. Preemptive liver transplantation prior to the development of end stage renal disease is a valuable option in the management of aHUS associated with CFH mutations.

Published

2010