Successful treatment of a large intracoronary thrombus with urokinase and a chimerical monoclonal platelet aggregation inhibitor

被引:4
作者
Eick, B
Haude, M
Altmann, C
Liu, F
Caspari, G
Leischik, R
Erbel, R
机构
关键词
D O I
10.1055/s-2008-1047678
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
History and clinical findings: 7 days after an operation for intervertebral disc prolapse a 43-year-old man was referred with the clinical and ECG signs of an acute posterior wall myocardial infarction. Investigations: Creatine kinase (CK) activity was raised to 204 U/l (myocardial-specific isoenzyme CKMB of 23.6 U/l, 11.6% of total) and glutamatic-oxalate transferase (GOT) activity to 37 U/l. Emergency cardiac catheterisation, performed 4 hours after renewed onset of precordial pain showed no abnormal findings in the right coronary artery, despite the ECG signs, but a definite filling defect in the anterior interventricular branch which on intravascular ultrasound was an echo-dense noncalcified structure. Treatment and course: After percutaneous transluminal coronary angioplasty in the area of the obstructing structure al free-floating mass was identified in the proximal part of the anterior interventricular branch, most likely a thrombus. Intercoronary thrombolysis was therefore undertaken with urokinase (bolus of 1 mill. IU) together with the chimerical mono-clonal antibody c7E3, which inhibits platelet aggregation by blocking the platelet glycoprotein surface receptor IIb/IIIa. Coronary angiography 12 hours later revealed almost complete dissolution of the previously obstructing mass. Conclusion: Combining the platelet aggregation inhibitor c7E3 with a thrombolytic agent is an alternative treatment to the current management of intracoronary thrombi. Intravascular ultrasound is a suitable method for demonstrating angiographically inconspicious or unclear but pathogenetically significant vessel changes.
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页码:709 / 715
页数:7
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