Inhibition of Factor XIIIa in a Canine Model of Coronary Thrombosis: Effect on Reperfusion and Acute Reocclusion After Recombinant Tissue-Type Plasminogen Activator

The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5-methylthiazolo[2,3-b]1,3,4-thiadiazolium perchlorate (L-722,151) on coronary thrombolysis and reocclusion was studied in an acute dog model of electrically induced coronary thrombosis. L-722, 151 (0.1 mg/kg/min intravenously [IV] or...

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Published in	Blood Vol. 75; no. 7; pp. 1455 - 1459
Main Authors	Shebuski, Ronald J., Sitko, Gary R., Claremon, David A., Baldwin, Jack J., Remy, David C., Stern, Andrew M.
Format	Journal Article
Language	English
Published	United States Elsevier Inc 01.04.1990
Subjects	Animals Blood Pressure - drug effects Coronary Circulation - drug effects Coronary Disease - drug therapy Coronary Thrombosis - drug therapy Coronary Thrombosis - physiopathology Coronary Vessels - physiology Disease Models, Animal Dogs Electric Stimulation Female Male Myocardial Reperfusion Recombinant Proteins - therapeutic use Thiadiazoles - blood Thiadiazoles - pharmacokinetics Thiadiazoles - therapeutic use Tissue Plasminogen Activator - therapeutic use Transglutaminases - antagonists & inhibitors
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Abstract	The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5-methylthiazolo[2,3-b]1,3,4-thiadiazolium perchlorate (L-722,151) on coronary thrombolysis and reocclusion was studied in an acute dog model of electrically induced coronary thrombosis. L-722, 151 (0.1 mg/kg/min intravenously [IV] or placebo was administered 15 minutes before current initiation (150 μA) and for the duration of the experiment (270 minutes). Fifteen minutes after thrombus formation, heparin (300 U/kg, IV) was administered, followed 45 minutes later by recombinant tissue-type plasminogen activator (tPA) (10 μg/kg/min, IV for 90 minutes). Placebo-treated animals thrombosed at 48.9 ±8.1 minutes (mean ± SEM) and reperfused in response to tPA at 49.1 ± 9.3 minutes. L-722, 151 pretreated animals thrombosed at 44.4 ± 9.7 minutes and reperfused in response to tPA at 16.4 ± 2.8 minutes (P < .05 v vehicle). Furthermore, residual thrombus mass was reduced by L-722, 151 from 6.9 ± 1.9 mg in placebo-treated animals to 1.7 ± 0.6 mg (P < .05 v vehicle). Acute reocclusion occurred in 86% of placebo and in 75% of L-722, 151-treated animals. The incidence of tPA-induced reperfusion in L-722, 151-treated dogs was 100% (8 of 8), whereas only 70% (7 of 10) of placebo-treated dogs reperfused. These results demonstrate that pretreatment with L-722, 151 hastens reperfusion time threefold and reduces residual thrombus mass. These effects occurred with no change in systemic blood pressure in response to L-722,151. When L-722,151 was administered 15 minutes after thrombus formation in a separate group of dogs (n = 5), no beneficial effect on thrombolysis time or thrombus mass was observed. Thus, the specific factor XIIIa catalyzed crosslinking reaction(s), which may determine(s) resistance to plasmin-mediated fibrin degradation, occur(s) rapidly. Inhibition of this cross-linking by pretreatment with L-722,151 promotes tPA-induced thrombolysis.
AbstractList	Abstract The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5- methylthiazolo[2,3-b]1,3,4-thiadiazo lium perchlorate (L-722,151) on coronary thrombolysis and reocclusion was studied in an acute dog model of electrically induced coronary thrombosis. L-722,151 (0.1 mg/kg/min intravenously [IV] or placebo was administered 15 minutes before current initiation (150 microA) and for the duration of the experiment (270 minutes). Fifteen minutes after thrombus formation, heparin (300 U/kg, IV) was administered, followed 45 minutes later by recombinant tissue-type plasminogen activator (tPA) (10 micrograms/kg/min, IV for 90 minutes). Placebo-treated animals thrombosed at 48.9 +/- 8.1 minutes (mean +/- SEM) and reperfused in response to tPA at 49.1 +/- 9.3 minutes. L-722,151 pretreated animals thrombosed at 44.4 +/- 9.7 minutes and reperfused in response to tPA at 16.4 +/- 2.8 minutes (P less than .05 v vehicle). Furthermore, residual thrombus mass was reduced by L-722,151 from 6.9 +/- 1.9 mg in placebo-treated animals to 1.7 +/- 0.6 mg (P less than .05 v vehicle). Acute reocclusion occurred in 86% of placebo and in 75% of L-722,151-treated animals. The incidence of tPA-induced reperfusion in L-722,151-treated dogs was 100% (8 of 8), whereas only 70% (7 of 10) of placebo-treated dogs reperfused. These results demonstrate that pretreatment with L-722,151 hastens reperfusion time threefold and reduces residual thrombus mass. These effects occurred with no change in systemic blood pressure in response to L-722,151. When L-722,151 was administered 15 minutes after thrombus formation in a separate group of dogs (n = 5), no beneficial effect on thrombolysis time or thrombus mass was observed. Thus, the specific factor XIIIa catalyzed crosslinking reaction(s), which may determine(s) resistance to plasmin-mediated fibrin degradation, occur(s) rapidly. Inhibition of this crosslinking by pretreatment with L-722,151 promotes tPA-induced thrombolysis. The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5-methylthiazolo[2,3-b]1,3,4-thiadiazolium perchlorate (L-722,151) on coronary thrombolysis and reocclusion was studied in an acute dog model of electrically induced coronary thrombosis. L-722, 151 (0.1 mg/kg/min intravenously [IV] or placebo was administered 15 minutes before current initiation (150 μA) and for the duration of the experiment (270 minutes). Fifteen minutes after thrombus formation, heparin (300 U/kg, IV) was administered, followed 45 minutes later by recombinant tissue-type plasminogen activator (tPA) (10 μg/kg/min, IV for 90 minutes). Placebo-treated animals thrombosed at 48.9 ±8.1 minutes (mean ± SEM) and reperfused in response to tPA at 49.1 ± 9.3 minutes. L-722, 151 pretreated animals thrombosed at 44.4 ± 9.7 minutes and reperfused in response to tPA at 16.4 ± 2.8 minutes (P < .05 v vehicle). Furthermore, residual thrombus mass was reduced by L-722, 151 from 6.9 ± 1.9 mg in placebo-treated animals to 1.7 ± 0.6 mg (P < .05 v vehicle). Acute reocclusion occurred in 86% of placebo and in 75% of L-722, 151-treated animals. The incidence of tPA-induced reperfusion in L-722, 151-treated dogs was 100% (8 of 8), whereas only 70% (7 of 10) of placebo-treated dogs reperfused. These results demonstrate that pretreatment with L-722, 151 hastens reperfusion time threefold and reduces residual thrombus mass. These effects occurred with no change in systemic blood pressure in response to L-722,151. When L-722,151 was administered 15 minutes after thrombus formation in a separate group of dogs (n = 5), no beneficial effect on thrombolysis time or thrombus mass was observed. Thus, the specific factor XIIIa catalyzed crosslinking reaction(s), which may determine(s) resistance to plasmin-mediated fibrin degradation, occur(s) rapidly. Inhibition of this cross-linking by pretreatment with L-722,151 promotes tPA-induced thrombolysis. The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5-methylthiazolo[2,3-b]1,3,4-thiadiazo lium perchlorate (L-722,151) on coronary thrombolysis and reocclusion was studied in an acute dog model of electrically induced coronary thrombosis. L-722,151 (0.1 mg/kg/min intravenously [IV] or placebo was administered 15 minutes before current initiation (150 microA) and for the duration of the experiment (270 minutes). Fifteen minutes after thrombus formation, heparin (300 U/kg, IV) was administered, followed 45 minutes later by recombinant tissue-type plasminogen activator (tPA) (10 micrograms/kg/min, IV for 90 minutes). Placebo-treated animals thrombosed at 48.9 +/- 8.1 minutes (mean +/- SEM) and reperfused in response to tPA at 49.1 +/- 9.3 minutes. L-722,151 pretreated animals thrombosed at 44.4 +/- 9.7 minutes and reperfused in response to tPA at 16.4 +/- 2.8 minutes (P less than .05 v vehicle). Furthermore, residual thrombus mass was reduced by L-722,151 from 6.9 +/- 1.9 mg in placebo-treated animals to 1.7 +/- 0.6 mg (P less than .05 v vehicle). Acute reocclusion occurred in 86% of placebo and in 75% of L-722,151-treated animals. The incidence of tPA-induced reperfusion in L-722,151-treated dogs was 100% (8 of 8), whereas only 70% (7 of 10) of placebo-treated dogs reperfused. These results demonstrate that pretreatment with L-722,151 hastens reperfusion time threefold and reduces residual thrombus mass. These effects occurred with no change in systemic blood pressure in response to L-722,151. When L-722,151 was administered 15 minutes after thrombus formation in a separate group of dogs (n = 5), no beneficial effect on thrombolysis time or thrombus mass was observed. Thus, the specific factor XIIIa catalyzed crosslinking reaction(s), which may determine(s) resistance to plasmin-mediated fibrin degradation, occur(s) rapidly. Inhibition of this crosslinking by pretreatment with L-722,151 promotes tPA-induced thrombolysis.
Author	Baldwin, Jack J. Stern, Andrew M. Remy, David C. Claremon, David A. Shebuski, Ronald J. Sitko, Gary R.
Author_xml	– sequence: 1 givenname: Ronald J. surname: Shebuski fullname: Shebuski, Ronald J. – sequence: 2 givenname: Gary R. surname: Sitko fullname: Sitko, Gary R. – sequence: 3 givenname: David A. surname: Claremon fullname: Claremon, David A. – sequence: 4 givenname: Jack J. surname: Baldwin fullname: Baldwin, Jack J. – sequence: 5 givenname: David C. surname: Remy fullname: Remy, David C. – sequence: 6 givenname: Andrew M. surname: Stern fullname: Stern, Andrew M.
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Snippet	The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5-methylthiazolo[2,3-b]1,3,4-thiadiazolium perchlorate (L-722,151) on coronary thrombolysis... The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5-methylthiazolo[2,3-b]1,3,4-thiadiazo lium perchlorate (L-722,151) on coronary thrombolysis... Abstract The effect of inhibition of factor XIIIa with 2-(l-acetonylthio)-5- methylthiazolo[2,3-b]1,3,4-thiadiazo lium perchlorate (L-722,151) on coronary...
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SubjectTerms	Animals Blood Pressure - drug effects Coronary Circulation - drug effects Coronary Disease - drug therapy Coronary Thrombosis - drug therapy Coronary Thrombosis - physiopathology Coronary Vessels - physiology Disease Models, Animal Dogs Electric Stimulation Female Male Myocardial Reperfusion Recombinant Proteins - therapeutic use Thiadiazoles - blood Thiadiazoles - pharmacokinetics Thiadiazoles - therapeutic use Tissue Plasminogen Activator - therapeutic use Transglutaminases - antagonists & inhibitors
Title	Inhibition of Factor XIIIa in a Canine Model of Coronary Thrombosis: Effect on Reperfusion and Acute Reocclusion After Recombinant Tissue-Type Plasminogen Activator
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