Your search keyword '"G. R. Sitko"' showing total 14 results

1. Platelet transfusion reverses bleeding evoked by triple anti-platelet therapy including vorapaxar, a novel platelet thrombin receptor antagonist

Author

G. R. Sitko, Maria S. Michener, Dietmar Seiffert, Madhu Chintala, Michael J. Forrest, Richard Raubertas, L. Alexandra Wickham, Tian-Quan Cai, and Larry Handt

Subjects

Bleeding Time, Ticlopidine, Pyridines, Hemorrhage, Platelet Transfusion, Lactones, Bleeding time, medicine, Animals, Humans, Platelet, Platelet-poor plasma, Vorapaxar, Pharmacology, Aspirin, medicine.diagnostic_test, business.industry, Clopidogrel, Macaca fascicularis, Platelet transfusion, Hemostasis, Anesthesia, Drug Therapy, Combination, Receptors, Thrombin, business, Platelet Aggregation Inhibitors, medicine.drug

Abstract

Vorapaxar is a novel protease-activated receptor-1 (PAR-1) antagonist recently approved for the reduction of thrombotic cardiovascular events in patients with a history of myocardial infarction or with peripheral arterial disease. Patients who received vorapaxar in addition to standard of care antiplatelet therapy had an increased incidence of major bleeding events compared with placebo. To assess whether platelet transfusion can restore hemostasis in primates on triple antiplatelet therapy, template bleeding times were assessed concurrently in the buccal mucosa, finger pad, and distolateral tail of anesthetized cynomolgus macaques to evaluate bleeding with vorapaxar as either monotherapy or in combination with aspirin or aspirin and clopidogrel. Aspirin (5mg/kg, IV) or vorapaxar (1mg/kg, PO) alone had no significant effect on bleeding times in the three vascular beds examined. A modest (

Published

2015

2. α-Hydroxy amides as a novel class of bradykinin B1 selective antagonists

Author

Jacquelynn J. Cook, Rodney A. Bednar, Thomayant Prueksaritanont, Yvonne M. Leonard, Michael R. Wood, Qin Mei, Richard W. Ransom, Ronald K. Chang, Emily D. Adarayn, Robert M. DiPardo, Jian Yu, Audrey A. Wallace, Wei Lemaire, Scott D. Kuduk, Kathy L. Murphy, G. R. Sitko, Scott D. Mosser, Christina N. Di Marco, Mark G. Bock, Frank C. Clayton, Bang-Lin Wan, Kathy M. Schirripa, Marie A. Holahan, Roger M. Freidinger, Dennis L. Bohn, Douglas J. Pettibone, Raymond S.L. Chang, Cuyue Tang, and June J. Kim

Subjects

medicine.drug_class, Clinical Biochemistry, Biological Availability, Pharmaceutical Science, Bradykinin, Inflammation, Carboxamide, Biochemistry, Rats, Sprague-Dawley, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Drug Discovery, medicine, Animals, Cytochrome P-450 Enzyme Inhibitors, Humans, Bradykinin receptor, Receptor, Molecular Biology, Organic Chemistry, Antagonist, Amides, Rats, Bradykinin B1 Receptor Antagonists, chemistry, Blood-Brain Barrier, Molecular Medicine, Efflux, medicine.symptom, Antagonism, Half-Life

Abstract

Antagonism of the bradykinin B1 receptor represents a potential treatment for chronic pain and inflammation. Novel antagonists incorporating α-hydroxy amides were designed that display low-nanomolar affinity for the human bradykinin B1 receptor and good bioavailability in the rat and dog. In addition, these functionally active compounds show high passive permeability and low susceptibility to phosphoglycoprotein mediated efflux, predictive of good CNS exposure.

Published

2008

3. Metabolism-Directed Optimization of 3-Aminopyrazinone Acetamide Thrombin Inhibitors. Development of an Orally Bioavailable Series Containing P1 and P3 Pyridines

Author

Bobby J. Lucas, Franklin C. Clayton, Daniel R. McMasters, James C. Barrow, Peter D. Williams, Robinson Kyle A, Theodore J. Detwiler, Yvonne M. Leonard, Sanderson Philip E, Julie A. Krueger, S. Dale Lewis, Rebecca B. White, Elizabeth A. Lyle, Cynthia Miller-Stein, William M. Sanders, Marie A. Holahan, Colleen M. McDonough, Youwei Yan, Jacquelynn J. Cook, Maria T. Stranieri, Joseph J. Lynch, Rominder Singh, G. R. Sitko, Lawrence Kuo, Terry A. Lyle, Craig A. Coburn, Zhongguo Chen, Dennis L. Bohn, Jules A. Shafer, Joseph P. Vacca, Audrey A. Wallace, Bruce D. Dorsey, Bradley K. Wong, Christopher S. Burgey, and Stephen J. Gardell

Subjects

Models, Molecular, Pyridines, medicine.drug_class, Administration, Oral, Biological Availability, Carboxamide, Crystallography, X-Ray, Structure-Activity Relationship, chemistry.chemical_compound, Dogs, Thrombin, Pharmacokinetics, Oral administration, Acetamides, Drug Discovery, medicine, Animals, Protease Inhibitors, biology, Anticoagulants, Macaca mulatta, Rats, Bioavailability, chemistry, Biochemistry, Enzyme inhibitor, Pyrazines, biology.protein, Molecular Medicine, Acetamide, medicine.drug, Discovery and development of direct thrombin inhibitors

Abstract

Recent efforts in the field of thrombin inhibitor research have focused on the identification of compounds with good oral bioavailability and pharmacokinetics. In this manuscript we describe a metabolism-based approach to the optimization of the 3-(2-phenethylamino)-6-methylpyrazinone acetamide template (e.g., 1) which resulted in the modification of each of the three principal components (i.e., P1, P2, P3) comprising this series. As a result of these studies, several potent thrombin inhibitors (e.g., 20, 24, 25) were identified which exhibit high levels of oral bioavailability and long plasma half-lives.

Published

2003

4. Effects of pentobarbital on pharmacokinetics and pharmacodynamics of a potent fibrinogen receptor antagonist, L-734 217, in dogs

Author

Marie A. Holahan, Thomayant Prueksaritanont, E. L. Hand, Maria T. Stranieri, Jacquelynn J. Cook, G. R. Sitko, and Joan D. Ellis

Subjects

Pharmacology, Pentobarbital, Chemistry, Fibrinogen receptor, Antagonist, Pharmaceutical Science, General Medicine, Blood proteins, Pharmacokinetics, Pharmacodynamics, Anesthetic, medicine, Pharmacology (medical), Ex vivo, medicine.drug

Abstract

Effects of pentobarbital on pharmacokinetics and pharmacodynamics of L-734,217, a potent fibrinogen receptor antagonist, were studied in male dogs. L-734,217 was given intravenously at 0.01 mg kg-1, in a cross-over fashion, to conscious dogs or to dogs anesthetized with pentobarbital. Plasma concentrations of L-734,217 were measured using a radioimmunoassay and inhibitory effects on ex vivo platelet aggregation induced by ADP or collagen were determined. In pentobarbital-treated dogs, L-734,217 plasma concentrations during the first 3 h collection period were significantly higher than those in the control animals. Corresponding to the increased plasma levels, the mean ex vivo inhibitory effects on ADP- or collagen-induced platelet aggregation in dogs under anesthesia appeared greater than in those without the anesthetic treatment. Pharmacokinetic analysis revealed a modest, but significant (up to 40%) elevation in the area under the plasma concentration-time curve during 6 h of the drug administration, and a reduction in L-734,217 plasma clearance and volumes of distribution, in the anesthetized dogs. Analysis of pharmacodynamic data indicated that the EC50 and the Hill coefficient of the platelet aggregation response-plasma concentration curve were not altered by pentobarbital treatment. The results are in agreement with the findings that the administration of pentobarbital alone (in the absence of L-734,217) did not affect appreciably the ex vivo platelet aggregatory responses. In a separate group of dogs, L-734,217 was found to be metabolically stable, and was eliminated unchanged renally (64 +/- 4%) and hepatically (32 +/- 6%). In addition, L-734,217 did not bind substantially to canine plasma proteins or blood cellular components. It is possible that alterations of regional hemodynamics, reportedly mediated by pentobarbital, contributed to changes observed in the present study. That is, alterations occurred in L-734,217 elimination and distribution processes which resulted in an increase in drug plasma levels. Since pentobarbital anesthesia influenced only the pharmacokinetics, and not the pharmacodynamics, of L-734,217, the apparent increases in the inhibition of platelet aggregation responses observed following L-734,217 administration to the anesthetized dogs were probably sequential effects of the pharmacokinetic interactions.

Published

1997

5. Non-Peptide Glycoprotein IIb/IIIa Inhibitors. 17. Design and Synthesis of Orally Active, Long-Acting Non-Peptide Fibrinogen Receptor Antagonists

Author

B. C. Askew, Thomayant Prueksaritanont, Joseph J. Lynch, Charles J. Mcintyre, Terrence G. Hamill, Rodney A. Bednar, Marie A. Holahan, Stanley L. Gaul, R. J. Lynch, G. R. Sitko, Robert J. Gould, Joan D. Glass, Cecila A. Hunt, John J. Baldwin, Jacquelynn J. Cook, Lynn M. Gorham, George D. Hartman, David A. Claremon, Maria T. Stranieri, and Bohumil Bednar

Subjects

Blood Platelets, Fibrinogen receptor, Platelet Glycoprotein GPIIb-IIIa Complex, Pharmacology, Fibrinogen, Structure-Activity Relationship, Dogs, Fibrinolytic Agents, Drug Discovery, medicine, Animals, Humans, Platelet, Vitronectin, IC50, Sulfonamides, Molecular Structure, biology, Chemistry, Biological activity, Azepines, Fibronectins, Adenosine Diphosphate, Biochemistry, Glycoprotein IIb/IIIa inhibitors, biology.protein, Molecular Medicine, Collagen, Endothelium, Vascular, Platelet Aggregation Inhibitors, Ex vivo, medicine.drug

Abstract

The synthesis and pharmacological evaluation of 5 (L-738, 167), a potent, selective non-peptide fibrinogen receptor antagonist is reported. Compound 5 inhibited the aggregation of human gel-filtered platelets with an IC50 value of 8 nM and was found to be33000-fold less effective at inhibiting the attachment of human endothelial cells to fibrinogen, fibronectin, and vitronectin than it was at inhibiting platelet aggregation. Ex vivo platelet aggregation was inhibited by85% 24 h after the oral administration of 5 to dogs at 100 micrograms/kg. The extended pharmacodynamic profile exhibited by 5 appears to be a consequence of its high-affinity binding to GPIIb/IIIa on circulating platelets and suggests that 5 is suitable for once-a-day dosing.

Published

1997

6. Nonpeptide GPIIB/IIIA inhibitors. 16. Thieno[2,3-b]thiophene α-sulfonamides are potent inhibitors of platelet aggregation

Author

G. R. Sitko, Robert J. Gould, S. Lee Gaul, Guixiang Zhang, John D. Prugh, Bohumil Bednar, Maria T. Stranieri, Rodney A. Bednar, Marie A. Holahan, Jacquelynn J. Cook, George D. Hartman, and R. J. Lynch

Subjects

Bicyclic molecule, Chemistry, Stereochemistry, Organic Chemistry, Clinical Biochemistry, Sulfonamide (medicine), Pharmaceutical Science, Biochemistry, Chemical synthesis, In vitro, chemistry.chemical_compound, Oral administration, In vivo, Drug Discovery, medicine, Thiophene, Molecular Medicine, Platelet aggregation inhibitor, Molecular Biology, medicine.drug

Abstract

Centrally constrained thieno[2,3- b ]thiophene sulfonamides have provided a potent, selective, orally active series of platelet aggregation inhibitors. Compound 21 showed excellent activity in the dog after a single oral dose of 200 μg/kg.

Published

1997

7. Primary Prevention of Coronary Arterial Thrombosis with the Factor Xa Inhibitor rTAP in a Canine Electrolytic Injury Model

Author

G.P. Vlasuk, G. R. Sitko, Lehman Ed, and J.J. Lynch

Subjects

medicine.drug_class, business.industry, medicine.medical_treatment, Anticoagulant, Hematology, Heparin, medicine.disease, Thrombosis, Bolus (medicine), medicine.anatomical_structure, Anesthesia, Coronary vessel, medicine, Thrombus, business, Saline, medicine.drug, Artery

Abstract

SummaryThe antithrombotic efficacies of the coagulation factor Xa inhibitor recombinant tick anticoagulant peptide (rTAP) and heparin were compared in a canine model of left circumflex (LCX) coronary artery electrolytic lesion. Intravenous infusions of saline (controls), rTAP (50 μg/kg/min continuous infusion) or heparin (200 U/kg bolus followed by 2 U/kg/min continuous infusion) were started 60 min prior to the initiation of LCX coronary artery electrolytic injury (150 μA continuous anodal current). All 6/6 saline-treated control animals developed occlusive thrombi at 49.8 ± 13.6 min after the initiation of vessel injury, and possessed a residual thrombus mass of 20.7 ± 3.3 mg. In the rTAP treatment group, 4/6 preparations developed occlusive thrombi, but with times to thrombosis delayed significantly compared to both the saline control as well as to the heparin treatment group (202.7 ± 28.9 min; p

Published

1995

8. Enhancement of recombinant tissue plasminogen activator-induced reperfusion by recombinant tick anticoagulant peptide, a selective factor Xa inhibitor, in a canine model of femoral arterial thrombosis

Author

G. R. Sitko, G.P. Vlasuk, M J Mellott, Maria T. Stranieri, J.J. Lynch, and Inez I. Stabilito

Subjects

medicine.diagnostic_test, biology, business.industry, medicine.drug_class, medicine.medical_treatment, Anticoagulant, Hematology, Blood flow, Femoral artery, Pharmacology, medicine.disease, biology.organism_classification, Thrombosis, law.invention, law, Anesthesia, medicine.artery, Ornithodoros moubata, medicine, Recombinant DNA, business, Saline, Partial thromboplastin time

Abstract

Tick anticoagulant peptide (TAP) is a 60 amino acid protein originally isolated from the soft tick, Ornithodoros moubata, which exhibits potent anticoagulant properties due to its selective inhibition of blood coagulation factor Xa. We evaluated a recombinant version of TAP (rTAP) for its ability to accelerate recombinant tissue plasminogen activator (rt-PA) -mediated lysis of an occlusive thrombus and prevent acute reocclusion in a canine model of femoral artery thrombosis. An occlusive thrombus was formed by insertion of a thrombogenic copper coil into the femoral artery of anesthetized dogs. Blood flow velocity was monitored directly and continuously by Doppler flowmetry. 60 min after occlusion, dogs received an i.v. infusion of either saline or rTAP (0.5, 2.5 or 8.0 μg/kg/min), followed 45 min later by rt-PA (0.8 mg/kg, i.v. over 90 min; n=8/group). The saline and rTAP infusions were discontinued 1 h after stopping the rt-PA. All dogs achieved reperfusion, with a time to reperfusion in the saline-treated (vehicle) group (administered rt-PA alone) of 61 ±7 min. The time to reperfusion was slightly decreased in the 0.5ug/kg/min rTAP group (47±4min, p=NS). In the groups administered rTAP at 2.5 and 8.0 ug/kg/min, significant reductions in the time to reperfusion were observed (28±4 and 32±5mins, respectively, p

Published

1993

9. ChemInform Abstract: Nonpeptide Glycoprotein IIb/IIIa Inhibitors. Part 13. Design and Synthesis of an Orally Active Pyrazolopiperazinone Nonpeptide Fibrinogen Receptor Antagonist

Author

David A. Claremon, G. R. Sitko, Jacquelynn J. Cook, Charles J. Mcintyre, Robert J. Gould, Maria T. Stranieri, J.J. Lynch, John J. Baldwin, R. J. Lynch, Marie A. Holahan, C. C.‐T. Chang, P. S. Anderson, Hunt Cecilia, and B. C. Askew

Subjects

Pyrazolopiperazinone, Orally active, Fibrinogen receptor, Chemistry, Glycoprotein IIb/IIIa inhibitors, medicine, Antagonist, General Medicine, Pharmacology, medicine.drug

Published

2010

10. Acceleration of recombinant tissue-type plasminogen activator-induced thrombolysis and prevention of reocclusion by the combination of heparin and the Arg-Gly-Asp-containing peptide bitistatin in a canine model of coronary thrombosis

Author

G R Sitko, R J Shebuski, I J Stabilito, and M H Polokoff

Subjects

Male, Platelet Aggregation, medicine.medical_treatment, Coronary Disease, Myocardial Reperfusion, Dogs, Fibrinolytic Agents, Coronary thrombosis, Recurrence, Coronary Circulation, Physiology (medical), medicine, Animals, Thromboplastin, Thrombus, biology, Heparin, business.industry, Coronary Thrombosis, Fissipedia, Hemodynamics, Thrombolysis, medicine.disease, biology.organism_classification, Thrombosis, Electric Stimulation, Recombinant Proteins, Drug Combinations, Tissue Plasminogen Activator, Anesthesia, Female, Partial Thromboplastin Time, Peptides, Cardiology and Cardiovascular Medicine, business, Plasminogen activator, Snake Venoms, medicine.drug

Abstract

The effect of tissue-type plasminogen activator (t-PA) alone or in combination with heparin, the Arg-Gly-Asp-containing peptide bitistatin, or both heparin and bitistatin was evaluated on thrombolysis time and acute reocclusion in a canine model of coronary thrombosis. Thrombus formation was elicited by electrolytic injury with a needle electrode to the endothelial surface of the circumflex coronary artery in the open-chest, anesthetized dog in the presence of a flow-limiting critical stenosis. Thirty minutes after spontaneous coronary artery occlusion, t-PA (1 mg/kg i.v. over 90 minutes) was administered. Group 1 was given t-PA alone; reperfusion occurred at 78.2 +/- 5.6 minutes with a reperfusion incidence of 60% (6/10). Group 2 received t-PA plus heparin (100 units/kg plus 50 units/kg/hr); reperfusion occurred at 61.9 +/- 9.1 minutes with a reperfusion incidence of 90% (9/10). Group 3 received t-PA plus heparin plus bitistatin (30 micrograms/kg plus 3 micrograms/kg/min); reperfusion occurred at 47.3 +/- 7.6 minutes (p less than 0.05 versus group 1) with a reperfusion incidence of 90% (9/10). Group 4 received t-PA plus bitistatin, and reperfusion occurred at 51.8 +/- 8.5 minutes; however, the reperfusion incidence was only 60% (6/10). In groups 1, 2, and 4, acute reocclusion occurred in more than 80% of the reperfused dogs, whereas in group 3 reocclusion occurred in 22% (2/9) of the reperfused dogs (p less than 0.05 versus group 1). The dose of heparin used in this study increased activated partial thromboplastin times 1.5-2.0-fold over control.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1990

11. 9-hydroxyazafluorenes and their use in thrombin inhibitors

Author

Rominder Singh, K.J. Stauffer, S. Dale Lewis, Marie A. Holahan, Daniel R. McMasters, Youwei Yan, Harold G. Selnick, Rebecca B. White, Matthew M. Zrada, Peter D. Williams, Audrey A. Wallace, Joseph J. Lynch, Maria Stranieri-Michener, Beth Pietrak, Cynthia Miller-Stein, Bradley K. Wong, Yvonne M. Leonard, Julie A. Krueger, G. R. Sitko, Philippe G. Nantermet, Bobby J. Lucas, Jacquelyn J. Cook, Carl F. Homnick, Elizabeth A. Lyle, and Christina L. Newton

Subjects

Male, Models, Molecular, Proline, Stereochemistry, Administration, Oral, Biological Availability, In Vitro Techniques, Crystallography, X-Ray, Chemical synthesis, Rats, Sprague-Dawley, Structure-Activity Relationship, Thrombin, Dogs, Pharmacokinetics, Oral administration, In vivo, Drug Discovery, medicine, Potency, Animals, Humans, Fluorenes, biology, Chemistry, Stereoisomerism, Blood Proteins, Macaca mulatta, Rats, Enzyme inhibitor, biology.protein, Microsomes, Liver, Molecular Medicine, medicine.drug, Discovery and development of direct thrombin inhibitors, Half-Life, Protein Binding

Abstract

Optimization of a previously reported thrombin inhibitor, 9-hydroxy-9-fluorenylcarbonyl-l-prolyl-trans-4-aminocyclohexylmethylamide (1), by replacing the aminocyclohexyl P1 group provided a new lead structure, 9-hydroxy-9-fluorenylcarbonyl-l-prolyl-2-aminomethyl-5-chlorobenzylamide (2), with improved potency (K(i) = 0.49 nM for human thrombin, 2x APTT = 0.37 microM in human plasma) and pharmacokinetic properties (F = 39%, iv T(1/2) = 13 h in dogs). An effective strategy for reducing plasma protein binding of 2 and improving efficacy in an in vivo thrombosis model in rats was to replace the lipophilic fluorenyl group in P3 with an azafluorenyl group. Systematic investigation of all possible azafluorenyl P3 isomers and azafluorenyl-N-oxide analogues of 2 led to the identification of an optimal compound, 3-aza-9-hydroxyfluoren-9(R)-ylcarbonyl-l-prolyl-2-aminomethyl-5-chlorobenzylamide (19b), with high potency (K(i) = 0.40 nM, 2x APTT = 0.18 microM), excellent pharmacokinetic properties (F = 55%, T(1/2) = 14 h in dogs), and complete efficacy in the in vivo thrombosis model in rats (inhibition of FeCl(3)-induced vessel occlusions in six of six rats receiving an intravenous infusion of 10 microg/kg/min of 19b). The stereochemistry of the azafluorenyl group in 19b was determined by X-ray crystallographic analysis of its N-oxide derivative (23b) bound in the active site of human thrombin.

Published

2005

12. An antibody against the exosite of the cloned thrombin receptor inhibits experimental arterial thrombosis in the African green monkey

Author

Bohumil Bednar, Ruth F. Nutt, Dong-Mei Feng, Jacquelynn J. Cook, Jules A. Shafer, Thomas M. Connolly, G. R. Sitko, M J Mellott, Robert J. Gould, and Cindra L. Condra

Subjects

Platelet Aggregation, Pharmacology, Fibrin, Antibodies, Thrombin, In vivo, Physiology (medical), Thrombin receptor, Chlorocebus aethiops, medicine, Animals, Platelet, Platelet activation, Receptor, biology, business.industry, Thrombosis, Recombinant Proteins, Immunology, Antibody Formation, biology.protein, Receptors, Thrombin, Cardiology and Cardiovascular Medicine, business, circulatory and respiratory physiology, Discovery and development of direct thrombin inhibitors, medicine.drug

Abstract

Background Thrombin inhibitors have been shown to be efficacious in animal models of thrombosis and in initial human clinical trials. It is unknown if their efficacy is due to their prevention of thrombin-mediated fibrin formation or to an inhibitory effect on thrombin-stimulated platelet activation. Appropriate tools to address this question have not been available. Therefore, to evaluate the role of the platelet thrombin receptor in intravascular thrombus formation, a polyclonal antibody was raised against a peptide derived from the thrombin-binding exosite region of the cloned human thrombin receptor. This antibody serves as a selective inhibitor of the thrombin receptor for in vivo evaluation. Methods and Results The immune IgG (IgG 9600) inhibited thrombin-stimulated aggregation and secretion of human platelets. In contrast, it had no effect on platelet activation induced by other agonists including ADP, collagen, or the thrombin receptor–derived peptide SFLLR-NH 2 . IgG 9600 also inhibited thrombin-induced aggregation of African Green monkey (AGM) platelets. By Western blot analysis, the IgG identified a protein of ≈64 kD in homogenates of both human and AGM platelets. The effect of thrombin receptor blockade by this antibody on arterial thrombosis was evaluated in an in vivo model of platelet-dependent cyclic flow reductions (CFRs) in the carotid artery of the AGM. The intravenous administration of IgG 9600 (10 mg/kg) abolished CFRs in three monkeys and reduced CFR frequency by 50% in a fourth monkey. Ex vivo platelet aggregation in response to up to 100 nmol/L thrombin was completely inhibited during the 120-minute postbolus observation period in all four animals. There was a twofold increase in bleeding time, which was not statistically different from baseline, and ex vivo clotting time (APTT) was not changed. The glycoprotein IIb/IIIa receptor antagonist MK-0852 and the thrombin inhibitor recombinant hirudin also demonstrated inhibitory effects on CFRs at doses that did not significantly prolong template bleeding time. Control IgG had no effect on CFRs, ex vivo platelet aggregation, bleeding time, or APTT. Conclusions These results demonstrate that blockade of the platelet thrombin receptor can prevent arterial thrombosis in this animal model without significantly altering hemostatic parameters and suggest that the thrombin receptor is an attractive antithrombotic target.

Published

1995

13. Conjunctive enhancement of enzymatic thrombolysis and prevention of thrombotic reocclusion with the selective factor Xa inhibitor, tick anticoagulant peptide. Comparison to hirudin and heparin in a canine model of acute coronary artery thrombosis

Author

I I Stabilito, George P. Vlasuk, G R Sitko, Denise Ramjit, Joseph J. Lynch, and D Lehman

Subjects

Male, medicine.drug_class, medicine.medical_treatment, Hirudin, Coronary Disease, Myocardial Reperfusion, Arthropod Proteins, Bolus (medicine), Dogs, Recurrence, Physiology (medical), Coronary Circulation, Antithrombotic, medicine, Animals, Thrombus, Hemostasis, business.industry, Heparin, Anticoagulant, Hemodynamics, Drug Synergism, Thrombolysis, Hirudins, medicine.disease, Recombinant Proteins, Anesthesia, Tissue Plasminogen Activator, Coronary vessel, Intercellular Signaling Peptides and Proteins, Female, Cardiology and Cardiovascular Medicine, business, Peptides, medicine.drug, Factor Xa Inhibitors

Abstract

BACKGROUND Effective thrombolytic recanalization of an occluded coronary vessel is often limited by acute thrombotic reocclusion, which has galvanized the search for effective adjunctive or conjunctive antithrombotic agents. METHODS AND RESULTS Recombinant versions of tick anticoagulant peptide (rTAP) and hirudin (rHIR) are highly selective and potent polypeptide inhibitors of factor Xa and thrombin, respectively. The comparative antithrombotic efficacies of rTAP, rHIR, and heparin, administered conjunctively with recombinant tissue-type plasminogen activator (rt-PA), on thrombolytic reperfusion and reocclusion, were determined in a canine model of occlusive coronary artery thrombosis with a superimposed critical stenosis. In this model, a platelet-rich occlusive thrombus was formed after damage to the intimal surface of the left circumflex coronary artery induced by electrolytic injury. Fifteen minutes after occlusion, the dogs received a systemic intravenous administration of either saline (control), heparin (200 units/kg bolus + 2 units/kg/min, heparin (HEP) 200 or 100 units/kg bolus + 1 unit/kg/min, HEP 100), rHIR (50 or 100 micrograms/kg/min, rHIR 50 or 100, respectively), or rTAP (100 micrograms/kg/min, rTAP 100) followed 15 minutes later by rt-PA (100 micrograms/kg bolus + 10 micrograms/kg/min over 90 minutes). Infusions of the conjunctive agents were discontinued 60 minutes after termination of rt-PA. The incidence and time (mean +/- SEM) to thrombolytic reperfusion were determined for control (five of 12; 68.0 +/- 7.8 minutes), HEP 100 (six of eight; 40.1 +/- 8.3 minutes), HEP 200 (six of eight; 39.8 +/- 9.5 minutes), rHIR 50 (six of eight; 51.7 +/- 14.6 minutes), rHIR 100 (eight of eight; 19.5 +/- 4.2 minutes), and rTAP 100 (eight of eight; 22.8 +/- 10.0 minutes). The incidence and time to reocclusion after rt-PA were determined for control (four of five; 45.7 +/- 12.5 minutes), HEP 100 (four of six; 18.2 +/- 10.7 minutes), HEP 200 (five of six; 26.2 +/- 20.7 minutes), rHIR 50 (four of six; 47.3 +/- 21.6 minutes), rHIR 100 (six of eight; 89.8 +/- 5.9 minutes), and rTAP 100 (three of eight; 54.0 +/- 16.3 minutes). All of the dogs that reoccluded in the rHIR 100 group did so after termination of the inhibitor infusion, whereas two of the three dogs in the rTAP 100 group that reoccluded did so during the inhibitor infusion. Coronary artery blood flow was characterized by intermittent periods of reocclusion and recanalization in all groups except rTAP 100. CONCLUSIONS The potent antithrombotic effects of rTAP in this model directly implicate de novo thrombin formation as a major source of thrombin activity within the highly thrombogenic residual thrombus. These findings suggest that direct inhibition of prothrombinase activity may be an effective strategy in the development of a new class of conjunctive agents.

Published

1992

14. Non-Peptide GPIIb/IIIa Inhibitors. 20. Centrally Constrained Thienothiophene α-Sulfonamides Are Potent, Long Acting in Vivo Inhibitors of Platelet Aggregation

Author

Carl F. Homnick, G. R. Sitko, Robert J. Gould, George D. Hartman, Bohumil Bednar, R. J. Lynch, L.M. Vassallo, Melissa S. Egbertson, Laura A. Libby, Marie A. Holahan, Stanley L. Gaul, Maria T. Stranieri, John D. Prugh, Jacquelynn J. Cook, Rodney A. Bednar, and Joseph J. Lynch

Subjects

Blood Platelets, Male, Bleeding Time, Fibrinogen receptor, Drug Evaluation, Preclinical, Administration, Oral, Platelet Glycoprotein GPIIb-IIIa Complex, Thiophenes, Pharmacology, In Vitro Techniques, Binding, Competitive, Radioligand Assay, Structure-Activity Relationship, Dogs, Bleeding time, In vivo, Drug Discovery, medicine, Animals, Humans, Platelet, IC50, Sulfonamides, medicine.diagnostic_test, Chemistry, Biochemistry, Injections, Intravenous, Platelet aggregation inhibitor, Molecular Medicine, Female, Ex vivo, Platelet Aggregation Inhibitors

Abstract

The synthesis and pharmacology of 4, a potent thienothiophene non-peptide fibrinogen receptor antagonist, are reported. Compound 4 inhibited the aggregation of human gel-filtered platelets with an IC50 of 8 nM and demonstrated an 8-fold improvement in affinity for isolated GPIIb/IIIa receptors over analogues possessing an isoindolinone backbone. Flow cytometry studies revealed that the binding of 4 to resting platelets is a diffusion-controlled process (kon = 3.3 x 10(6) M-1 s-1) and that 4 binds to dog and human platelets with comparable affinity (Kd = 0.04 and 0.07 nM, respectively). Ex vivo platelet aggregation in dogs was completely inhibited by an iv dose of 5 microg/kg [corrected], and an oral dose of 50-90 microg/kg [corrected] followed by low daily doses of 10 microg/kg [corrected] was sufficient to maintain approximately 80% inhibition of ex vivo platelet aggregation over several days. Inhibition of ADP-induced platelet aggregation in anesthetized dogs at 77 +/- 7% resulted in a moderate 2.5-fold increase in bleeding time, while complete inhibition (100%) resulted in an approximately 10-min bleeding time. Additional doses were required to increase the bleeding time to the maximum time allowed in the protocol (15 min), thus indicating a potentially useful and safe separation of efficacy and bleeding time.

Published

1999