Mutations in complement C3 predispose to development of atypical hemolytic uremic syndrome

Frémeaux‐Bacchi, Véronique; Miller, Elizabeth C.; Liszewski, M. Kathryn; Strain, Lisa; Blouin, Jacques; Brown, Audrey E.; Moghal, Nadeem; Kaplan, Bernard S.; Weiss, Robert A; Lhotta, Karl; Kapur, Gaurav; Mattoo, Tej K.; Nivet, Hubert; Wong, William; Gié, Sophie; Ligny, Bruno Hurault de; Fischbach, Michel; Gupta, Ritu; Hauhart, Richard E.; Meunier, Vincent; Loirat, Chantal; Dragon-Durey, Marie-Agnès; Fridman, Wolf‐Herman; Janssen, B.J.C.; Goodship, Timothy H.J.; Atkinson, John P.

doi:10.1182/blood-2008-01-133702

Cited by 360 publications

(326 citation statements)

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“…Approximately 50% of patients with aHUS have mutations in one of the complement regulatory proteins: Factor H (CFH), factor I (CFI), or membrane co-factor protein (MCP) (3)(4)(5). More recently, mutations in factor B (CFB) and C3 have been associated with aHUS (6,7). The frequencies of homozygous deletions of CFH-related genes CFHR1/CFHR3 and of polymorphisms in CFH, MCP, and C4-binding protein are increased (8 -10).…”

Section: H Emolytic Uremic Syndrome (Hus) Is a Clinical Triad Ofmentioning

confidence: 99%

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Complement Inhibitor Eculizumab in Atypical Hemolytic Uremic Syndrome

Mache

Acham-Roschitz

Frémeaux‐Bacchi

et al. 2009

Clinical Journal of the American Society of Nephrology

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143

103

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Background and objectives: Atypical hemolytic uremic syndrome (aHUS) is associated with a congenital or acquired dysregulation of the complement alternative pathway that leads to continuous complement activation on host cells causing inflammation and damage. Eculizumab, a humanized mAb against complement protein C5, inhibits activation of the terminal complement pathway.Design, setting, participants, & measurements: We report an adolescent with relapsing unclassified aHUS. On admission, a high plasma creatinine level indicated a poor prognosis, and hemodialysis had to be started. Plasma exchanges were initially effective against the microangiopathic hemolytic activity and allowed a temporary improvement of renal function with termination of hemodialysis after 7 wk. Subsequently, plasma exchanges (three times per week) failed to prevent ongoing aHUS activity and progressive renal failure. After 12 wk, aHUS treatment was switched to eculizumab.Results: Eculizumab was effective in terminating the microangiopathic hemolytic process in two aHUS relapses; however, after normalization of complement activity, aHUS recurred and ultimately led to anuric end-stage renal failure.Conclusions: In this patient, complement inhibition by eculizumab temporarily terminated the microangiopathic hemolytic activity. Nevertheless, renal damage as a result of preceding and subsequent aHUS activity resulted in end-stage renal failure; therefore, therapeutic success may depend on early administration of eculizumab. The optimal duration of treatment may be variable and remains to be determined.

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Section: H Emolytic Uremic Syndrome (Hus) Is a Clinical Triad Ofmentioning

confidence: 99%

“…All exons of the complement regulatory genes were sequenced as described previously (7,(27)(28)(29). The primer sequences for CFH, CFI, MCP, CFB, C3, and C4BP gene screening are available from the authors on request.…”

Section: Genetic Analysesmentioning

confidence: 99%

Complement Inhibitor Eculizumab in Atypical Hemolytic Uremic Syndrome

Mache

Acham-Roschitz

Frémeaux‐Bacchi

et al. 2009

Clinical Journal of the American Society of Nephrology

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143

103

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“…by guest www.bloodjournal.org From previously. [13][14][15][16][17] Genotyping of the following SNPs was undertaken using direct sequencing:…”

Section: Mutation Screening and Genotypingmentioning

confidence: 99%

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

Francis

McNicholas

Awan

et al. 2012

Blood

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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 microhomologymediated 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. (Blood. 2012;119(2):591-601)

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“…Penetrance is also incomplete in aHUS, and seems to be 40%-50% among carriers of CFH, membrane cofactor protein (MCP), and CFI mutations [25]; healthy carriers of C3 and CFB mutations have also been described [26,27]. There are numerous reports describing the onset of aHUS symptoms in association with an environmental trigger.…”

Section: Epidemiology and Clinical Presentationmentioning

confidence: 99%

Atypical hemolytic uremic syndrome: from diagnosis to treatment

Franchini¹

2015

Clinical Chemistry and Laboratory Medicine (CCLM)

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Thrombotic microangiopathy (TMA) is a relatively rare condition but a medical urgency requiring immediate intervention to avoid irreversible organ damage or death. Symptoms on presentation include microangiopathic haemolytic anaemia, thrombocytopenia and organ damage. The most frequent direct causes of TMA are thrombotic thrombocytopenic purpura (TTP) and haemolytic uremic syndrome (HUS). The most common form of HUS is related to Shiga toxin producing Escherichia coli (STEC) infection while approximately 10% of cases are due to dysregulation of the complement pathway (atypical haemolytic uremic syndrome, aHUS). Optimal treatment regimens differ depending on the underlying cause; however, differential diagnosis may be difficult. The most accurate method of diagnosis is based on exclusion and should consider, beyond the symptoms common to TMA, ADAMTS13 activity levels and STEC infection status. For the management of TTP, plasma exchange (PE) is the most important acute intervention and is associated with lower mortality and better outcomes than plasma infusion. In most patients with STEC-HUS, the course of disease is selflimiting although management of acute kidney injury is often required. Until recently, the management of aHUS consisted of early and intensive PE, although this was mostly ineffective in protecting from subsequent organ damage. Eculizumab, an inhibitor of the alternative complement pathway, produces a rapid and sustained inhibition of the TMA process, with significant improvements in long-term clinical outcomes. Due to the significant improvement achieved, eculizumab has subsequently been approved as first-line therapy when an unequivocal diagnosis of aHUS has been made.

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Mutations in complement C3 predispose to development of atypical hemolytic uremic syndrome

Cited by 360 publications

References 24 publications

Complement Inhibitor Eculizumab in Atypical Hemolytic Uremic Syndrome

Complement Inhibitor Eculizumab in Atypical Hemolytic Uremic Syndrome

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

Atypical hemolytic uremic syndrome: from diagnosis to treatment

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