Abstract
Abstract 2203
Thrombotic thrombocytopenic purpura (TTP) is frequently characterized by severe ADAMTS13 deficiency, the cause of which is unknown. An important exception is ticlopidine-associated TTP (tc-TTP), the most common drug-induced TTP syndrome. In 1998, a possible association of TTP with ticlopidine was reported. In 1999, two additional series reported this association. In 2000, a fourth study reported severe A DAMTS13 deficiency among six of seven tc-TTP persons- suggesting a causal pathway. All of these reports were from the United States. Recently, we reported characteristics of 186 acquired idiopathic (ai)- TTP patients in Japan with severe ADAMTS13 deficiency, noting that clinical and laboratory findings for ai-TTP patients in Japan differed from those for cohorts of ai-TTP patients in Europe and North America- raising concern that TTP findings vary by region of the world. (PLOS One 2011) We now on report clinical and laboratory characteristics of a cohort of TTP patients from Japan with tc-TTP, and compare these findings to three cohorts of tc-TTP in the United States and one cohort of ai-TTP patients from Japan.
We queried a database of thrombotic microangiopathy patients identified from a national TTP referral laboratory in Japan of cases identified between 1998 and 2008.
Severe ADAMTS13 deficiency was characterized by activity levels < 5%. All tc-TTP patients and 186 of 911 ai-TTP patients in the database had severe ADAMTS13 deficiency and first onset of TTP. Comparisons were made to tc-TTP patients reported previously from the United States.
Characteristics of ai- TTP with severe ADAMTS13 deficiency in Japan and tc-TTP in Japan and US
| . | Matsumoto (n= 186) . | Bennett (n=22) . | Bennett (n= 98) . | Tsai (n=7) . | Steinhubl (n=19) . |
|---|---|---|---|---|---|
| Source | PLOS One 2011 | This paper | Arch Int Med 1999 | Ann Int Med 2000 | JAMA 1999 |
| Country | Japan | Japan | US | US | US |
| Etiology | Idiopathic | Ticlopidine | Ticlopidine | Ticlopidine | Ticlopidine |
| % female | 55.1% | 45.5% | 46.6% | 70.0% | 30.0% |
| Median Age (yrs) | 54 (8 mos-87) | 69 (41-89) | 64.2 (11.1= SD) | 57 (42-89) | 62 (38-75) |
| Plt < 20k/mm3 | 100.0% | 96.0% | 71.9% | 100.0% | 89.4% |
| Hgb < 9 g/dl | NA | 72.7% | 26,9% | 42.3% | 66.7% |
| Cr > 2.0 mg/dl | 75.8% | 31.2% | 30.1% | NA | 47.0% |
| Neuro abn | 79.0% | 63.6% | 73.1% | 70.0% | 73.7% |
| Median days ticlopidine (range) | NA | 27.5 (14-36) | 21 (7-112) | 21 (14-56) | 21 (14-28) |
| % w/ coronary stent | Not applicable | 13.6% | 42.3% | 57.1% | 100.0% |
| % w/ other CAD indication | NA | 31.2% | 0.0% | 14.3% | 0.0% |
| % CVA prevention | Not applicable | 55.8% | 57.7% | 14.3% | 0.0% |
| Survival | 84.3% | 91.0% | 84.9% | 100.0% | 78.9% |
| % TPE | NA | 63.6% | 74.2% | 100.0% | 68.4% |
| Survival w/o TPE | Not available | 75.0% | 42.1% | NA | 33.3% |
| Survival w/ TPE | 83.9% | 100.0% | 81.7% | 100.0% | 100.0% |
| % w/ ADAMTS13:AC deficiency (<5%) | 100.0% | 100.0% | 100.0% | 83.3% | NA |
| % with ADAMTS13 inhibitors | 97.8% | 100.0% | 100.0% | 100.0% | NA |
| . | Matsumoto (n= 186) . | Bennett (n=22) . | Bennett (n= 98) . | Tsai (n=7) . | Steinhubl (n=19) . |
|---|---|---|---|---|---|
| Source | PLOS One 2011 | This paper | Arch Int Med 1999 | Ann Int Med 2000 | JAMA 1999 |
| Country | Japan | Japan | US | US | US |
| Etiology | Idiopathic | Ticlopidine | Ticlopidine | Ticlopidine | Ticlopidine |
| % female | 55.1% | 45.5% | 46.6% | 70.0% | 30.0% |
| Median Age (yrs) | 54 (8 mos-87) | 69 (41-89) | 64.2 (11.1= SD) | 57 (42-89) | 62 (38-75) |
| Plt < 20k/mm3 | 100.0% | 96.0% | 71.9% | 100.0% | 89.4% |
| Hgb < 9 g/dl | NA | 72.7% | 26,9% | 42.3% | 66.7% |
| Cr > 2.0 mg/dl | 75.8% | 31.2% | 30.1% | NA | 47.0% |
| Neuro abn | 79.0% | 63.6% | 73.1% | 70.0% | 73.7% |
| Median days ticlopidine (range) | NA | 27.5 (14-36) | 21 (7-112) | 21 (14-56) | 21 (14-28) |
| % w/ coronary stent | Not applicable | 13.6% | 42.3% | 57.1% | 100.0% |
| % w/ other CAD indication | NA | 31.2% | 0.0% | 14.3% | 0.0% |
| % CVA prevention | Not applicable | 55.8% | 57.7% | 14.3% | 0.0% |
| Survival | 84.3% | 91.0% | 84.9% | 100.0% | 78.9% |
| % TPE | NA | 63.6% | 74.2% | 100.0% | 68.4% |
| Survival w/o TPE | Not available | 75.0% | 42.1% | NA | 33.3% |
| Survival w/ TPE | 83.9% | 100.0% | 81.7% | 100.0% | 100.0% |
| % w/ ADAMTS13:AC deficiency (<5%) | 100.0% | 100.0% | 100.0% | 83.3% | NA |
| % with ADAMTS13 inhibitors | 97.8% | 100.0% | 100.0% | 100.0% | NA |
These data from Japan validate insights about tc-TTP initially proposed in 1998, 1999, and 2000 in the United States. Ticlopidine is a likely cause of TTP, the mechanism is via a cross-reactive antibody to ADAMTS13:AC resulting in formation of an ADAMTS13:INH, and therapeutic plasma exchange is necessary for treatment.
Ortel:Eisai: Research Funding; Glaxo SmithKline: Research Funding; Pfizer: Research Funding; Instrumentation Laboratory, Inc: Consultancy, Research Funding; Boehringer Ingelheim: Consultancy. Fujimura:Baxter BioScience: Membership on an entity's Board of Directors or advisory committees; Alexion Pharma: Membership on an entity's Board of Directors or advisory committees.
Author notes
Asterisk with author names denotes non-ASH members.
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