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Sep 10, 2018 (publication date) through Oct 29, 2025
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World Journal of Transplantation
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2220-3230
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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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Copyright ©The Author(s) 2018.
World J Transplantation. Sep 10, 2018; 8(5): 122-141
Published online Sep 10, 2018. doi: 10.5500/wjt.v8.i5.122
Table 1 Morphological features in microangiopathy
Active lesionsChronic lesions
Glomeruli: Thrombi - Endothelial swelling or denudation - Fragmented RBCs - Subendothelial flocculent material. EM: Mesangiolysis - MicroaneurysmsGlomeruli: LM: Double contours of peripheral capillary walls, with variable mesangial interposition - EM: New subendothelial basement membrane - Widening of the subendothelial zone
Arterioles: Thrombi - Endothelial swelling or denudation-Intramural fibrin-Fragmented red blood cells-Intimal swelling-Myocyte necrosisArterioles: Hyaline deposits Arteries: Fibrous intimal thickening with concentric lamination (onion skin)
Arteries: Thrombi - Myxoid intimal swelling -Intramural fibrin- Fragmented red blood cells
Adapted from: Goodship et al[58]. EM: Electron microscopy; LM: Light microscopy.
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Table 2 Risk of atypical hemolytic uremic syndrome recurrence according to the implicated genetic abnormality
GenemutationLocationFunctionalimpactMutation frequencyin aHUS (%)Recurrence after transplantation (%)
CFHPlasmaLoss20-3075-90
CFIPlasmaLoss2-1245-80
CFBPlasmaGain1-2100
C3PlasmaGain5-1040-70
MCPMembraneLoss10-1515-20
THBDMembraneLoss5One case
HomozygousCFHR1 del (3%-8%)CirculatingUndetermined14-23 (> 90% with anti-CHF AB)NA
Adapted from Salvadori et al[74]. NA: Not available; CFH: Complement factor H; CFI: Complement factor I; CFB: Complement factor B; C3: Complement component 3; MCP: Membrane cofactor protein; THBD: Thrombomodulin.
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Table 3 Complement studies for atypical hemolytic uremic syndrome (aHUS)
Complement testaHUS
Complement protein levelsC3, C4, FB1, C51
Complement regulatory protein levelsFH, FI, Properdin1, CD462
Complement split productsC3c1, C3d1, Bb1, sC5b-91
Complement functional assaysCH50, AH50, hemolytic assays, FH assays1
AutoantibodiesAnti-FH
Genetic screeningCFH, CFI, C3, CD46, CFB Genomic rearrangements across the FH-FHR locus (e.g., by MLPA) Sequencing of coding regions and assessment of CNV Non-complement genetic screening includes THBD and DGKE
1Currently available only at specific laboratories; they are research and not clinically validated assays;
2CD46 is also known as MCP. Adapted from: Goodship et al[58]. AH50: Alternative pathway hemolytic assay; C3: Complement component 3; C4: Complement component 4; C5: Complement component 5; CFB: Complement factor B gene; CFH: Complement factor H gene; CFHR: Complement factor H related genes; CFI: Complement factor I gene; CH50: Classical pathway hemolytic assay; CNV: Copy number variation; DGKE gene: Diacylglycerol kinase epsilon gene; FB: Complement factor B; FH: Complement factor H; FI: Complement factor I; MLPA: Multiplex ligation-dependent probe amplification; sC5b-9: Soluble C5b-9; THBD: Thrombomodulin; aHUS: Atypical hemolytic uremic syndrome.
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Table 4 Genotype-phenotype correlations in atypical hemolytic uremic syndrome (data refer to the period before introduction of eculizumab)
GeneRisk of death or ESRD at onset or first yrRisk ofrecurrenceRisk of death or ESRDafter 3-5 yrRisk of recurrencein allograft
CFH or CFH-CFHR1/3 hybrid genes50%-70%50%75%75%-90%
CFI50%10%-30%50%-60%45%-80%
MCP single0%-6%70%-90%6%-38%< 20%
MCP combined130%-40%50%50%50%-60%
C360%50%75%40%-70%
CFB50%100%75%100%
THBD50%30%54%?
Anti-FH30%-40%40%-60%35%-60%Depends on antibody titers
1Combined with CFH or CFI or C3 mutations. Adapted from: Goodship et al[58]. CFB: Complement factor B gene; CFH: Complement factor H gene; CFHR: Complement factor H-related genes; CFI: Complement factor I gene; FH: Factor H protein; THBD: Thrombomodulin gene.
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Table 5 Eculizumab dosing in atypical hemolytic uremic syndrome based on dosing goal, one additional monitoring may be required during intercurrent events (e.g., infection, surgery, vaccination) to detect unblocked complement activity
Minimal doseDesire to continue dosing with the minimal dose required to achieve a pre-identified level of complement blockade 1
Dose reduction or interval extension
Goal CH50 < 10% (recommended)
Goal AH50 < 10% (recommended)
Goal eculizumab trough > 100 μg/mL
DiscontinuationDesire to discontinue complement blockade: No consensus exists regarding tapering of dose
Adapted from: Goodship et al[58]. AH50: Alternative pathway hemolytic activity; CH50: Total complement activity.
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Table 6 Monitoring eculizumab therapy
Description
CH50 (total complement activity)Measures the combined activity of all of the complement pathways Tests the functional capability of serum complement components to lyse 50% of sheep erythrocytes in a reaction mixture Low in congenital complement deficiency (C1-8) or during complement blockade Normal range is assay dependent Recommended goal during therapeutic complement blockade: < 10% of normal
AH50 (alternative pathway hemolytic activity)Measures combined activity of alternative and terminal complement pathways Tests the functional capability of alternate or terminal pathway complement components to lyse 50% of rabbit erythrocytes in a Mg2+-EGTA buffer Will be low in congenital C3, FI, FB, properdin, FH, and FD deficiencies or during terminal complement blockade Normal range is assay dependent Recommended goal during complement blockade: < 10% of normal
Eculizumab troughMay be a free or bound level ELISA: Using C5 coated plates, patient sera, and an anti-human IgG detection system Not affected by complement deficiencies Recommended trough level during complement blockade: 50-100 μg/mL
Alternative assaysThe following assays are under investigation (or awaiting to be replicated in different laboratories)[83] as a means to monitor therapeutic complement blockade Free C5 In vitro human microvascular endothelial cell test sC5b -9 (also referred to as sMAC and TCC) may remain detectable in aHUS patients in remission and therefore is not recommended as a monitoring tool
Adapted from: Goodship et al[58]. aHUS: Atypical hemolytic uremic syndrome; C3: Complement component 3; C5: Complement component 5; EGTA: Ethyleneglycol tetraacetic acid; ELISA: Enzyme-linked immunosorbent assay; FB: Complement factor B; FD: Complement factor D; FH: Complement factor H; FI: Complement factor I; sC5b-9: Soluble C5b-9; sMAC: Soluble membrane attack complex; TCC: Terminal complement complex.
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