To the editor:

The antiplatelet agent ticlopidine is associated with the rapid onset of a thrombotic microangiopathy (TMA) resembling thrombotic thrombocytopenic purpura (TTP) and atypical hemolytic-uremic syndrome (aHUS). These disorders occur in 0.06% of individuals exposed to ticlopidine, usually within 1.5 to 6 weeks of exposure.1,2  The vast majority of ticlopidine TMAs are accompanied by antibody-mediated inhibition of the protease ADAMTS13, making them similar to idiopathic TTP.3,4  However, ADAMTS13 deficiency alone is not sufficient for the development of TMAs. Our group has shown that exposure to both the pharmacologic levels of ticlopidine and plasma from patients with ticlopidine TMAs induces apoptosis in primary human microvascular endothelial cells, suggesting that ticlopidine-induced endothelial cell apoptosis is a provoking factor in ticlopidine TMAs.5  In other TMAs such as aHUS, complement regulatory protein mutations represent another provoking factor for the development of these diseases.6  Complement mutations have not been studied in ticlopidine TMAs.

We obtained plasma samples from 4 consecutive patients with TMAs that occurred within 2.5 to 4 weeks of ticlopidine exposure (Table 1).7  ADAMTS13 activity and inhibitor titers were determined, as previously described by Bennett et al.8  All patients had thrombocytopenia, schistocytosis, markedly elevated levels of lactate dehydrogenase (LDH), renal impairment, and significantly decreased ADAMTS13 activity. Three of 4 had ADAMTS13 inhibitors. Plasma levels of C5a and C5b-9 (membrane attack complex) were measured by enzyme-linked immunosorbent assay (Quidel). Genomic DNA was isolated from plasma using the QIAamp kit (Qiagen). To determine the presence of complement mutations, we selected primers to soluble complement factor H (CFH), complement factor I, and membrane-linked membrane cofactor protein, 3 complement regulatory factors with mutations that have been identified with high frequency in aHUS.4,5  We found substantially elevated levels of membrane attack complex despite normal C5a levels, and all 4 patients had CFH genetic abnormalities (Table 2). Two of the 3 polymorphisms are of known functional significance, and even heterozygous CFH mutations are sufficient to develop aHUS.7,9 

This is the first report of CFH mutations in ticlopidine TMAs. These mutations are otherwise uncommon in healthy individuals and have a background mutation rate of <5% in northern Europeans.10,11  ADAMTS13 deficiency has previously been considered to be pathognomonic of TTP. However, complement regulatory factor mutations represent another independent susceptibility factor in many types of TMAs, and their presence in addition to ADAMTS13 deficiency may be required for the onset of disease. If a complement mutation is required for TMA development after ticlopidine exposure, it could explain the rarity of ticlopidine TMAs despite the fact that the drug causes microvascular endothelial cell injury in vitro.5  Unlike idiopathic TTP, both aHUS and ticlopidine TMAs respond poorly to plasma exchange, even though hematologic parameters may normalize. Renal disease and overall mortality are not affected, and LDH levels do not return to normal, which suggests ongoing endothelial injury.9  We hypothesize that ticlopidine TMAs occur as a result of a failure to regulate complement on endothelial cell surfaces after cell injury, leading to ongoing microvascular damage. This defect may be present in other TMAs. We recently illustrated the role of complement in a patient with severe refractory idiopathic TTP with ADAMTS13 <5% and a high inhibitor titer. He rapidly responded to anti-C5 therapy after other treatment failures.12  No complement mutations were detected utilizing a commercially available platform. Subsequent analysis, however, did reveal a CFH mutation (unpublished data).12  In conclusion, complement regulatory protein mutations may form the basis for TMA susceptibility and should be further studied.

Contribution: J.C. performed DNA extraction and collected clinical information; H.-M.T. performed ADAMTS13 testing; S.E. and R.S. performed semi-nested PCR on all DNA samples; J.L. and J.C. analyzed the data and authored the manuscript; and all authors contributed equally to the editing and revision of this work.

Conflict-of-interest disclosure: The authors declare no competing financial interests.

H.-M.T. is not currently affiliated with any institution.

Correspondence: John Chapin, Division of Hematology-Oncology Payson 3, Weill Cornell Medical College, 525 E 68th St, New York, NY 10065; e-mail: joc9160@nyp.org.

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