Abstract
Abstract 892
The thienopyridines, ticlopidine and clopidogrel, have been associated with thrombotic thrombocytopenia purpura (TTP). However, few studies have reported information on antibodies to ADAMTS13 among patients with thienopyridine-associated TTP. We previously reported on two mechanistic pathways of thienopyridine-associated TTP with some overlapping features. Evaluation of ADAMTS13 autoantibodies was undertaken to improve understanding of these syndromes.
Clinical and laboratory findings were evaluated for 30 ticlopidine-, 10 clopidogrel-associated TTP cases, and 54 cases of idiopathic TTP.
Among patients with thienopyridine-induced TTP, those with a history of ticlopidine versus clopidogrel use were more likely to present with severe thrombocytopenia (platelet < 20,000) (90% versus 13%), severe ADAMTS13-deficiency (80% versus 0%), and neutralizing antibodies to ADAMTS13 (100% versus 0%), and were less likely to have less than a two week history of thienopyridine exposure (0% versus 50%) (p<0.05 for each comparison). They were also more likely to survive following therapeutic plasma exchange (TPE) (85% versus 50%). 2 patients exposed to clopidogrel later relapsed and had similar characteristics to idiopathic TTP patients with non-deficient ADAMTS13 activity.
Ticlopidine causes TTP by a pathway involving a neutralizing autoantibody to ADAMTS13 while clopidogrel causes TTP by an ADAMTS13-independent pathway. Although ADAMTS13 autoantibodies are present in both idiopathic and ticlopidine-associated TTP, spontaneous relapses are not seen in ticlopidine-associaated TTP, suggesting that drug-dependent antibodies are present. Clopidogrel associated TTP is distinct from idiopathic TTP in that ADAMTS13 autoantibodies are absent and response to TPE is poor.
. | Ticlopidine (n=30) . | Clopidogrel (n=8) . | Idiopathic ADAMTS13 deficient (≤10%) (n=30) . | Idiopathic ADAMTS13 non-deficient (>10%) (n=24) . | Idiopathic TTP with clopidogrel exposure (n=2) . |
---|---|---|---|---|---|
Age (years) | 68 | 58 | 40 | 46 | 55 |
Sex (%female) | 57% | 38% | 83% | 96% | 0% |
Platelet count <20,000/mm3 | 90%** | 13%** | 60%* | 29%* | 100% |
Creatinine >2.5 mg/dl | 20% | 50% | 7%* | 48%* | 0% |
Neurologic Dysfunction | 60% | 50% | 53% | 52% | 50% |
Neutralizing autoantibodies to ADAMTS 13 (at presentation) | 100%** | 0%** | 79%* | 39%* | 100% |
ADAMTS13 ≤10% | 80%** | 0%** | 100% | 0% | 100% |
ADAMTS13 level 11-50% | 20%* | 63%* | 0% | 100% | 0% |
Thienopyridine exposure < 2 weeks (%) | 0%** | 50%** | N/A | N/A | 100% |
Thienopyridine exposure 2-12 weeks (%) | 100%** | 25%** | N/A | N/A | 0% |
Thienopyridine exposure > 12 weeks (%) | 0%* | 25%* | N/A | N/A | 0% |
Treatment with TPE | 83% | 100% | 100% | 100% | 100% |
Survival after TPE | 85% (n=26) | 50% (n=8) | 97% | 96% | 100% |
30-day survival | 80% | 50% | 97% | 96% | 100% |
1-year relapse | 0% | 0% | 33% | 13% | 100% |
. | Ticlopidine (n=30) . | Clopidogrel (n=8) . | Idiopathic ADAMTS13 deficient (≤10%) (n=30) . | Idiopathic ADAMTS13 non-deficient (>10%) (n=24) . | Idiopathic TTP with clopidogrel exposure (n=2) . |
---|---|---|---|---|---|
Age (years) | 68 | 58 | 40 | 46 | 55 |
Sex (%female) | 57% | 38% | 83% | 96% | 0% |
Platelet count <20,000/mm3 | 90%** | 13%** | 60%* | 29%* | 100% |
Creatinine >2.5 mg/dl | 20% | 50% | 7%* | 48%* | 0% |
Neurologic Dysfunction | 60% | 50% | 53% | 52% | 50% |
Neutralizing autoantibodies to ADAMTS 13 (at presentation) | 100%** | 0%** | 79%* | 39%* | 100% |
ADAMTS13 ≤10% | 80%** | 0%** | 100% | 0% | 100% |
ADAMTS13 level 11-50% | 20%* | 63%* | 0% | 100% | 0% |
Thienopyridine exposure < 2 weeks (%) | 0%** | 50%** | N/A | N/A | 100% |
Thienopyridine exposure 2-12 weeks (%) | 100%** | 25%** | N/A | N/A | 0% |
Thienopyridine exposure > 12 weeks (%) | 0%* | 25%* | N/A | N/A | 0% |
Treatment with TPE | 83% | 100% | 100% | 100% | 100% |
Survival after TPE | 85% (n=26) | 50% (n=8) | 97% | 96% | 100% |
30-day survival | 80% | 50% | 97% | 96% | 100% |
1-year relapse | 0% | 0% | 33% | 13% | 100% |
p<0.05;
≤0.001; comparisons are made between ticlopidine versus clopidogrel associated TTP cases that did not experience relapse and deficient versus non-deficient idiopathic TTP.
No relevant conflicts of interest to declare.
Author notes
Asterisk with author names denotes non-ASH members.