Complement Mutation‐Associated De Novo Thrombotic Microangiopathy Following Kidney Transplantation

Complement Mutation‐Associated De Novo Thrombotic Microangiopathy Following Kidney Transplantation

Mutations in one or more genes encoding complement‐regulatory proteins predispose to atypical hemolytic uremic syndrome (aHUS) and its recurrence following kidney transplantation. We evaluated plasma complement level and performed a screening for mutations in genes encoding complement Factors H and...

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Veröffentlicht in:American journal of transplantation 2008-08, Vol.8 (8), p.1694-1701
Hauptverfasser: Le Quintrec, M., Lionet, A., Kamar, N., Karras, A., Barbier, S., Buchler, M., Fakhouri, F., Provost, F., Fridman, W. H., Thervet, E., Legendre, C., Zuber, J., Frémeaux‐Bacchi, V.
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Sprache:eng
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Adult
Complement
complement Factor H
Complement Factor H - genetics
complement Factor I
Complement Factor I - genetics
Female
hemolytic uremic syndrome
Humans
Kidney - blood supply
kidney transplantation
Kidney Transplantation - adverse effects
Male
Membrane Cofactor Protein - genetics
Microcirculation
Middle Aged
Mutation
Retrospective Studies
Risk Factors
Thrombosis
thrombotic microangiopathy
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container_end_page 1701
container_issue 8
container_start_page 1694
container_title American journal of transplantation
container_volume 8
creator Le Quintrec, M.
Lionet, A.
Kamar, N.
Karras, A.
Barbier, S.
Buchler, M.
Fakhouri, F.
Provost, F.
Fridman, W. H.
Thervet, E.
Legendre, C.
Zuber, J.
Frémeaux‐Bacchi, V.
description Mutations in one or more genes encoding complement‐regulatory proteins predispose to atypical hemolytic uremic syndrome (aHUS) and its recurrence following kidney transplantation. We evaluated plasma complement level and performed a screening for mutations in genes encoding complement Factors H and I (CFH, CFI) and membrane cofactor protein (MCP) in 24 kidney transplant recipients experiencing de novo thrombotic microangiopathy (TMA). Six patients presented with low C3 and/or low Factor B levels suggestive complement alternative pathway. A mutation in the CFH or CFI gene was found in 7/24 patients (29%), two of whom had a mutation in both genes. On the contrary, no mutation was identified in a control kidney transplant patients group (n = 25) without TMA. Patients with or without mutations were similar with regard to clinical features. Eight out of 24 patients lost their graft within 1 year of posttransplantation including six patients with a CFH mutation or a decrease of C3 or CFB in plasma. To conclude, kidney transplant patients with de novo TMA exhibit an unexpectedly high frequency of CFH and CFI mutations. These results suggest that genetic abnormalities may represent risk factors for de novo TMA after kidney transplantation and raise the question of the best therapeutic strategy. Kidney transplant patients with de novo TMA exhibit an unexpectedly high frequency of mutations in genes encoding for complement regulatory proteins (Factor H and Factor I).
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H.</au><au>Thervet, E.</au><au>Legendre, C.</au><au>Zuber, J.</au><au>Frémeaux‐Bacchi, V.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Complement Mutation‐Associated De Novo Thrombotic Microangiopathy Following Kidney Transplantation</atitle><jtitle>American journal of transplantation</jtitle><addtitle>Am J Transplant</addtitle><date>2008-08</date><risdate>2008</risdate><volume>8</volume><issue>8</issue><spage>1694</spage><epage>1701</epage><pages>1694-1701</pages><issn>1600-6135</issn><eissn>1600-6143</eissn><abstract>Mutations in one or more genes encoding complement‐regulatory proteins predispose to atypical hemolytic uremic syndrome (aHUS) and its recurrence following kidney transplantation. We evaluated plasma complement level and performed a screening for mutations in genes encoding complement Factors H and I (CFH, CFI) and membrane cofactor protein (MCP) in 24 kidney transplant recipients experiencing de novo thrombotic microangiopathy (TMA). Six patients presented with low C3 and/or low Factor B levels suggestive complement alternative pathway. A mutation in the CFH or CFI gene was found in 7/24 patients (29%), two of whom had a mutation in both genes. On the contrary, no mutation was identified in a control kidney transplant patients group (n = 25) without TMA. Patients with or without mutations were similar with regard to clinical features. Eight out of 24 patients lost their graft within 1 year of posttransplantation including six patients with a CFH mutation or a decrease of C3 or CFB in plasma. To conclude, kidney transplant patients with de novo TMA exhibit an unexpectedly high frequency of CFH and CFI mutations. These results suggest that genetic abnormalities may represent risk factors for de novo TMA after kidney transplantation and raise the question of the best therapeutic strategy. Kidney transplant patients with de novo TMA exhibit an unexpectedly high frequency of mutations in genes encoding for complement regulatory proteins (Factor H and Factor I).</abstract><cop>Oxford, UK</cop><pub>Blackwell Publishing Ltd</pub><pmid>18557729</pmid><doi>10.1111/j.1600-6143.2008.02297.x</doi><tpages>8</tpages></addata></record>
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subjects Adult
Complement
complement Factor H
Complement Factor H - genetics
complement Factor I
Complement Factor I - genetics
Female
hemolytic uremic syndrome
Humans
Kidney - blood supply
kidney transplantation
Kidney Transplantation - adverse effects
Male
Membrane Cofactor Protein - genetics
Microcirculation
Middle Aged
Mutation
Retrospective Studies
Risk Factors
Thrombosis
thrombotic microangiopathy
title Complement Mutation‐Associated De Novo Thrombotic Microangiopathy Following Kidney Transplantation
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