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1. Corrigendum to 'Edoxaban for treatment of venous thromboembolism in patient groups with different types of cancer: Results from the Hokusai VTE Cancer study' [Thromb. Res. vol. 185, January 2020, pages 13-19]

Author

George Zhang, Frits I. Mulder, Annelise Segers, Peter Verhamme, M. Di Nisio, Manila Gaddh, Noémie Kraaijpoel, Marc Carrier, Ajay K. Kakkar, David A. Garcia, N. van Es, Michael A. Grosso, Gordon Royle, Saskia Middeldorp, Michele Mercuri, H. R. Büller, J. I. Weitz, Tzu-Fei Wang, Gary E. Raskob, Sudeep Shivakumar, and Anil Duggal

Subjects
Oncology, medicine.medical_specialty, business.industry, MEDLINE, Cancer, Regret, Hematology, 030204 cardiovascular system & hematology, medicine.disease, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Primary outcome, chemistry, Edoxaban, 030220 oncology & carcinogenesis, Internal medicine, medicine, Cumulative incidence, In patient, business, Venous thromboembolism
Abstract

The authors regret that panel E of Fig. 1 was missing, showing the cumulative incidence of the primary outcome in hematologic cancer. The authors would like to apologise for any inconvenience caused.

Published
2020

2. Addressing the burden of hospital‐related venous thromboembolism: the role of extended anticoagulant prophylaxis

Author

Peter L. Gross, Noel C. Chan, and J. I. Weitz

Subjects
0301 basic medicine, medicine.medical_specialty, 030204 cardiovascular system & hematology, Fibrin Fibrinogen Degradation Products, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, Anticoagulant prophylaxis, medicine, Humans, Postoperative Period, Intensive care medicine, business.industry, Anticoagulants, Thrombosis, Venous Thromboembolism, Hematology, Heparin, Low-Molecular-Weight, United States, Hospitalization, 030104 developmental biology, Research Design, Patient Safety, Pulmonary Embolism, business, Venous thromboembolism
Published
2018

3. Once versus twice daily aspirin after coronary bypass surgery: a randomized trial

Author

Jack Hirsh, J. I. Weitz, Richard P. Whitlock, Guillaume Paré, Jeffrey S. Ginsberg, Jeremy S. Paikin, Noel C. Chan, and John W. Eikelboom

Subjects
Blood Platelets, Male, medicine.medical_specialty, Time Factors, Platelet Aggregation, Platelet Function Tests, 030204 cardiovascular system & hematology, Drug Administration Schedule, law.invention, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Randomized controlled trial, law, medicine, Humans, Pooled data, 030212 general & internal medicine, Myocardial infarction, Dosing, Coronary Artery Bypass, Aged, Ontario, Aspirin, business.industry, Hematology, Middle Aged, medicine.disease, Surgery, Thromboxane B2, Treatment Outcome, surgical procedures, operative, medicine.anatomical_structure, chemistry, Bypass surgery, Anesthesia, Female, business, Biomarkers, Platelet Aggregation Inhibitors, Artery, medicine.drug
Abstract

Essentials Coronary artery bypass graft (CABG) failure is associated with myocardial infarction and death. We tested whether more frequent dosing improves aspirin (ASA) response following CABG surgery. Twice-daily compared with once-daily dosing reduces ASA hyporesponsiveness after CABG surgery. The efficacy of twice-daily ASA needs to be tested in a trial powered for clinical outcomes. SummaryBackground Acetyl-salicylic acid (ASA) hyporesponsiveness occurs transiently after coronary artery bypass graft (CABG) surgery and may compromise the effectiveness of ASA in reducing thrombotic graft failure. A reduced response to ASA 81 mg once-daily after CABG surgery is overcome by four times daily ASA dosing. Objectives To determine whether ASA 325 mg once-daily or 162 mg twice-daily overcomes a reduced response to ASA 81 mg once-daily after CABG surgery. Methods Adults undergoing CABG surgery were randomized to ASA 81 mg once-daily, 325 mg once-daily or 162 mg twice-daily. The primary outcome was median serum thromboxane B2 (TXB2) level on postoperative day 4. We pooled the results with those of our earlier study to obtain better estimates of the effect of ASA 325 mg once-daily or in divided doses over 24 h. Results We randomized 68 patients undergoing CABG surgery. On postoperative day 4, patients randomized to receive ASA 81 mg once-daily had a median day 4 TXB2 level of 4.2 ng mL−1 (Q1, Q3: 1.5, 7.5 ng mL−1), which was higher than in those randomized to ASA 162 mg twice-daily (1.1 ng mL−1; Q1, Q3: 0.7, 2.7 ng mL−1) and similar to those randomized to ASA 325 mg once-daily (1.9 ng mL−1; Q1, Q3: 0.9, 4.7 ng mL−1). Pooled data showed that the median TXB2 level on day 4 in groups receiving ASA 162 mg twice-daily or 81 mg four times daily was 1.1 ng mL−1 compared with 2.2 ng mL−1 in those receiving ASA 325 mg once-daily. Conclusions Multiple daily dosing of ASA is more effective than ASA 81 mg once-daily or 325 mg once-daily at suppressing serum TXB2 formation after CABG surgery. A twice-daily treatment regimen needs to be tested in a clinical outcome study.

Published
2017

4. When and how to use antidotes for the reversal of direct oral anticoagulants: guidance from the SSC of the ISTH

Author

Mark Crowther, J. I. Weitz, Jerrold H. Levy, Walter Ageno, Noel C. Chan, and Peter Verhamme

Subjects
medicine.medical_specialty, Antidotes, MEDLINE, Administration, Oral, Hemorrhage, 030204 cardiovascular system & hematology, Pharmacology, Antibodies, Monoclonal, Humanized, Arginine, Piperazines, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, Internal medicine, Humans, Medicine, 030212 general & internal medicine, Blood Coagulation, Hematology, biology, Coagulants, business.industry, Anticoagulants, Recombinant Proteins, Factor Xa, Monoclonal, biology.protein, Recombinant DNA, Antibody, business
Published
2016

5. Rapid quantitative D‐dimer to exclude pulmonary embolism: a prospective cohort management study

Author

S. Takach Lapner, Shannon M. Bates, Jim A. Julian, Peter L. Gross, Lori-Ann Linkins, J. I. Weitz, Frederick A. Spencer, Sam Schulman, James D. Douketis, Agnes Y.Y. Lee, Sameer Parpia, Clive Kearon, Mark Crowther, J. Ginsberg, and Wendy Lim

Subjects
Adult, Male, Canada, medicine.medical_specialty, Time Factors, 030204 cardiovascular system & hematology, Drug Administration Schedule, Fibrin Fibrinogen Degradation Products, Tertiary Care Centers, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Risk Factors, Internal medicine, D-dimer, medicine, Humans, In patient, Prospective Studies, 030212 general & internal medicine, Prospective cohort study, Aged, business.industry, Anticoagulants, Reproducibility of Results, Venous Thromboembolism, Hematology, Middle Aged, Prognosis, medicine.disease, Confidence interval, Surgery, Latex fixation test, Pulmonary embolism, Anticoagulant therapy, Female, Pulmonary Embolism, business, Venous thromboembolism, Biomarkers, Latex Fixation Tests
Abstract

ESSENTIALS: It is not known if D-dimer testing alone can safely exclude pulmonary embolism (PE). We studied the safety of using a quantitative latex agglutination D-dimer to exclude PE in 808 patients. 52% of patients with suspected PE had a negative D-dimer test and were followed for 3 months. The negative predictive value of D-dimer testing alone was 99.8%, suggesting it may safely exclude PE. Background Strategies are needed to exclude pulmonary embolism (PE) efficiently without the need for imaging tests. Although validated rules for clinical probability assessment can be combined with D-dimer testing to safely exclude PE, the rules can be complicated or partially subjective, which limits their use. Objectives To determine if PE can be safely excluded in patients with a negative D-dimer without incorporating clinical probability assessment. Patients/methods We enrolled consecutive outpatients and inpatients with suspected PE from four tertiary care hospitals. All patients underwent D-dimer testing using the MDA D-dimer test, a quantitative latex agglutination assay. PE was excluded in patients with a D-dimer less than 750 μg FEU L(-1) without further testing. Patients with D-dimer levels of 750 μg FEU L(-1) or higher underwent standardized imaging tests for PE. All patients in whom PE was excluded had anticoagulant therapy withheld and were followed for 3 months for venous thromboembolism (VTE). Suspected events during follow-up were adjudicated centrally. Results Eight hundred and eight patients were enrolled, of whom 99 (12%) were diagnosed with VTE at presentation. Four hundred and twenty (52%) patients had a negative D-dimer level at presentation and were not treated with anticoagulants; of these, one had VTE during follow-up. The negative predictive value of D-dimer testing for PE was 99.8% (95% confidence interval, 98.7-99.9%). Conclusions A negative latex agglutination D-dimer assay is seen in about one-half of patients with suspected PE and reliably excludes PE as a stand-alone test.

Published
2016

6. Medical device‐induced thrombosis: what causes it and how can we prevent it?

Author

Iqbal H. Jaffer, James C. Fredenburgh, Jack Hirsh, and J. I. Weitz

Subjects
Catheter Obstruction, medicine.medical_specialty, Medical device, Prosthesis Design, Coated Materials, Biocompatible, Fibrinolytic Agents, Blood vessel prosthesis, Internal medicine, medicine, Animals, Humans, Thrombus, Heart-Assist Devices, Intensive care medicine, Blood Coagulation, business.industry, Graft Occlusion, Vascular, Anticoagulants, Thrombosis, Prostheses and Implants, Hematology, medicine.disease, Biocompatible material, Blood Vessel Prosthesis, Prosthesis Failure, Heart Valve Prosthesis, Cardiology, Stents, business, Vascular Access Devices, Fibrinolytic agent
Abstract

Blood-contacting medical devices, such as vascular grafts, stents, heart valves, and catheters, are often used to treat cardiovascular diseases. Thrombus formation is a common cause of failure of these devices. This study (i) examines the interface between devices and blood, (ii) reviews the pathogenesis of clotting on blood-contacting medical devices, (iii) describes contemporary methods to prevent thrombosis on blood-contacting medical devices, (iv) explains why some anticoagulants are better than others for prevention of thrombosis on medical devices, and (v) identifies future directions in biomaterial research for prevention of thrombosis on blood-contacting medical devices.

Published
2015

7. Multiple daily doses of acetyl‐salicylic acid (ASA) overcome reduced platelet response to once‐daily ASA after coronary artery bypass graft surgery: a pilot randomized controlled trial

Author

Jeremy S. Paikin, Noel C. Chan, Guillaume Paré, John W. Eikelboom, Jeffrey S. Ginsberg, J. I. Weitz, Jack Hirsh, M. Johnston, and Richard P. Whitlock

Subjects
Blood Platelets, Male, medicine.medical_specialty, Time Factors, Platelet Aggregation, Platelet Function Tests, Drug Resistance, Pilot Projects, Drug Administration Schedule, law.invention, chemistry.chemical_compound, Randomized controlled trial, law, medicine, Humans, Platelet, Coronary Artery Bypass, Aged, Ontario, Aspirin, Platelet Count, business.industry, Hematology, Perioperative, Middle Aged, Surgery, Thromboxane B2, Treatment Outcome, surgical procedures, operative, medicine.anatomical_structure, Quartile, chemistry, Anesthesia, Platelet aggregation inhibitor, Female, business, Biomarkers, Platelet Aggregation Inhibitors, Artery, medicine.drug
Abstract

Summary Background The efficacy of ASA for prevention of graft failure following CABG surgery may be limited by incomplete platelet inhibition due to increased post-operative platelet turnover. Objectives To determine whether acetyl-salicylic acid (ASA) 325 mg once-daily or 81 mg four-times daily overcomes the impaired response to ASA 81 mg once-daily in post-operative coronary artery bypass graft (CABG) patients. Methods We randomized 110 patients undergoing CABG surgery to either ASA 81 mg once-daily, 81 mg four times daily or 325 mg once-daily and compared their effects on serum thromboxane B2 (TXB2) suppression and arachidonate-induced platelet aggregation. Results One hundred patients were included in the final analysis. Platelet counts fell after surgery, reached a nadir on day 2, and then gradually increased. Although there was near complete suppression of TXB2 on the second or third post-operative day, TXB2 levels increased in parallel with the rise in platelet count on subsequent days. This increase was most marked in patients receiving ASA 81 mg once-daily and less evident in those receiving ASA four times daily. On post-operative day 4, (i) median TXB2 levels were lower with four times daily ASA than with either ASA 81 mg once-daily (1.1 ng/mL; Quartile(Q) Q1,Q3: 0.5, 2.4 and 13.3 ng/mL; Q1,Q3: 7.8, 30.8 ng/mL, respectively; P

Published
2015

8. Rivaroxaban reversal with prothrombin complex concentrate or tranexamic acid in healthy volunteers

Author

J. I. Weitz, Matthew D. Neal, J. Ariyawansa, Kenneth Todd Moore, Jerrold H. Levy, David J. Schneider, and V. S. Marcsisin

Subjects
Adult, Male, Adolescent, medicine.medical_treatment, Antidotes, Hemorrhage, Pilot Projects, 030204 cardiovascular system & hematology, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Double-Blind Method, Rivaroxaban, Healthy volunteers, Biopsy, medicine, Humans, 030212 general & internal medicine, Adverse effect, Saline, Blood Coagulation, Prothrombin time, medicine.diagnostic_test, business.industry, Hematology, Kansas, Middle Aged, Prothrombin complex concentrate, Antifibrinolytic Agents, Blood Coagulation Factors, Healthy Volunteers, Tranexamic Acid, Anesthesia, Prothrombin Time, Female, business, Tranexamic acid, medicine.drug, Factor Xa Inhibitors
Abstract

Essentials Specific reversal agents for managing severe factor Xa inhibitor-associated bleeding are lacking. We assessed 4-factor-prothrombin complex concentrate (4F-PCC) and tranexamic acid (TXA). 4F-PCC, but not TXA, reduced the prothrombin time and increased endogenous thrombin potential. These agents may be viable options for reversal of therapeutic doses of rivaroxaban. SummaryBackground Oral activated factor X inhibitors such as rivaroxaban are widely used, but specific reversal agents are lacking. Although four-factor prothrombin complex concentrate (4F-PCC) and tranexamic acid (TXA) are sometimes used to manage serious bleeding, their efficacy is unknown. Prior studies in healthy subjects taking rivaroxaban revealed that 4F-PCC partially reverses the prolonged prothrombin time (PT), and fully restores the endogenous thrombin potential (ETP). The effect of TXA has not been evaluated. Methods In this double-blind, parallel-group study, 147 healthy volunteers given rivaroxaban 20 mg twice daily for 3 days were randomized after their morning dose on day 4 to receive intravenous 4F-PCC (50 IU kg−1), TXA (1.0 g), or saline. Standardized punch biopsies were performed at baseline and after 4F-PCC, TXA or saline administration. Reversal was assessed by measuring bleeding duration and bleeding volume at biopsy sites, and by determining the PT and ETP. Results As compared with saline, 4F-PCC partially reversed the PT and completely reversed the ETP, whereas TXA had no effect. Neither 4F-PCC nor TXA reduced bleeding duration or volume. All treatments were well tolerated, with no recorded adverse events. Conclusions Although 4F-PCC reduced the PT and increased the ETP in volunteers given supratherapeutic doses of rivaroxaban, neither 4F-PCC nor TXA influenced punch biopsy bleeding.

Published
2017

9. Antithrombin-heparin covalent complex reduces microemboli during cardiopulmonary bypass in a pig model

Author

Anthony K.C. Chan, Petr Klement, Lesley J. Smith, Henry Wood, Jack Hirsh, Paul Tressel, Nethnapha Paredes, Leslie R. Berry, Nihal Haque, Peng Liao, and J. I. Weitz

Subjects
medicine.medical_specialty, Protamine sulfate, Ultrasonography, Doppler, Transcranial, medicine.drug_class, Sus scrofa, Immunology, Biochemistry, Antithrombins, law.invention, law, Internal medicine, Cardiopulmonary bypass, Animals, Embolism, Air, Medicine, Thrombus, Blood Coagulation, Cardiopulmonary Bypass, Hematology, Heparin, business.industry, Antithrombin, Anticoagulant, Anticoagulants, Brain, Cell Biology, medicine.disease, Embolism, Anesthesia, Female, business, circulatory and respiratory physiology, medicine.drug
Abstract

Transcranial Doppler-detected high-intensity transient signals (HITS) during cardiopulmonary bypass (CPB) surgery have been associated with postoperative neurocognitive dysfunction, suggesting microemboli in the brain could be a contributing factor. HITS occur despite administration of unfractionated heparin (UFH). This study was done to determine whether antithrombin-heparin covalent complex (ATH), a more potent anticoagulant than heparin, can reduce HITS during CPB. In a pig CPB model, ATH, UFH, or UFH + antithrombin (AT) was intravenously administered to female Yorkshire pigs after sternotomy. Twenty minutes later, hypothermic CPB was initiated and continued for 1.25 hours, then normothermia was re-established for 45 minutes. Protamine sulfate was given to neutralize the anticoagulants, and pigs were allowed to recover. HITS were monitored using an arterial flow probe placed over the carotid artery. Compared with UFH (300 or 1000 U/kg), ATH reduced the number of HITS during CPB in a dose-dependent manner. AT (3 mg/kg) + UFH (300 U/kg) resulted in an intermediate HITS rate between UFH and ATH (2 mg/kg in terms of AT). Examination of brain sections for emboli formation confirmed that, similar to HITS, number of thrombi decreased in direct proportion to ATH dosage. These results support the hypotheses that the majority of HITS represent thromboemboli and that ATH reduces emboli formation during CPB.

Published
2010

10. Real-world variability in dabigatran levels in patients with atrial fibrillation

Author

John W. Eikelboom, Sam Schulman, J. I. Weitz, James D. Douketis, Noel C. Chan, Michiel Coppens, Thomas Vanassche, Jeffrey S. Ginsberg, Jack Hirsh, ACS - Amsterdam Cardiovascular Sciences, and Vascular Medicine

Subjects
Male, medicine.medical_specialty, Time Factors, Renal function, Hemorrhage, Antithrombins, Dabigatran, Predictive Value of Tests, Risk Factors, Internal medicine, Atrial Fibrillation, medicine, Humans, Drug Dosage Calculations, Prospective Studies, Prospective cohort study, Blood Coagulation, Stroke, Aged, Blood coagulation test, Aged, 80 and over, business.industry, Reproducibility of Results, Atrial fibrillation, Hematology, Middle Aged, medicine.disease, Treatment Outcome, Quartile, Predictive value of tests, Female, Blood Coagulation Tests, Drug Monitoring, business, medicine.drug
Abstract

BACKGROUND In clinical practice, physicians are given the choice of selecting one of two dabigatran doses based on patient characteristics, with the lower dose typically used in patients at a higher risk of bleeding. OBJECTIVES The objectives of the study were to (i) estimate the inter- and intra-patient variability in dabigatran levels with 110 mg (DE110) and 150 mg (DE150) doses, (ii) examine the effect of physicians' dose selection on levels in DE110 and DE150 subgroups, and (iii) explore whether a single trough measurement identifies patients with extreme levels on subsequent visits. METHODS In this prospective observational study of 100 patients with atrial fibrillation (AF), peak and trough levels of dabigatran were measured with the Hemoclot(®) assay at baseline and every 2 months thereafter (maximum four visits). RESULTS Inter-patient variability in dabigatran levels (geometric coefficient of variation [gCV], 51-64%) was greater than intra-patient variability (gCV, 32-40%). Similar medians and distributions of levels were observed in DE110 and DE150 subgroups. Patients receiving DE110 were older, had lower renal function and weighed less than those receiving DE150. Up to 40% of patients whose trough levels were in the upper extremes, and up to 80% of patients whose trough levels were in the lower extremes at baseline, showed subsequent levels that fell in the middle quartiles. CONCLUSIONS Our data support the practice of selecting the dabigatran dose based upon clinical characteristics because it results in similar levels of drug exposure in patients given DE110 or DE150. They do not support the concept that a single Hemoclot(®) measurement reliably identifies patients with consistently high or low values.

Published
2015

11. New anticoagulants

Author

J I, Weitz and S M, Bates

Subjects
Venous Thrombosis, Benzylamines, Pyridines, Thrombin, Anticoagulants, Hematology, Models, Biological, Blood Coagulation Factors, Dabigatran, Factor IX, Fibrinolytic Agents, Thromboembolism, Animals, Azetidines, Humans, Benzimidazoles, Blood Coagulation, Protein C
Abstract

The limitations of heparin and warfarin have prompted the development of new anticoagulant drugs for prevention and treatment of venous and arterial thromboembolism. Novel parenteral agents include synthetic analogs of the pentasaccharide sequence of heparin that mediates its interaction with antithrombin. Fondaparinux, the first synthetic pentasaccharide, is licensed for prevention of venous thromboembolism (VTE) after major orthopedic surgery and for initial treatment of patients with VTE. Idraparinux, a long-acting pentasaccharide that is administered subcutaneously once-weekly, is being compared with warfarin for treatment of VTE and for prevention of cardioembolic events in patients with atrial fibrillation. New oral anticoagulants include direct inhibitors of thrombin, factor Xa and factor IXa. Designed to provide more streamlined anticoagulation than warfarin, these agents can be given without routine coagulation monitoring. Ximelagatran, the first oral direct thrombin inhibitor, is as effective and safe as warfarin for prevention of cardioembolic events in patients with atrial fibrillation. However, ximelagatran produces a three-fold elevation in alanine transaminase levels in 7.9% of patients treated for more than a month, the long-term significance of which is uncertain. Whether other direct thrombin inhibitors or inhibitors of factors Xa or IXa also have this problem is under investigation. After a brief review of coagulation pathways, this paper focuses on new anticoagulants in advanced stages of clinical testing.

Published
2005

12. Comparison of 1 month with 3 months of anticoagulation for a first episode of venous thromboembolism associated with a transient risk factor

Author

Louis Desjardins, Alexander G.G. Turpie, James D. Douketis, Michael Gent, Clive Kearon, J. I. Weitz, Phil Wells, Michael J. Kovacs, Marilyn Johnston, Susan R. Kahn, Susan Solymoss, Jeannine Kassis, Jim A. Julian, Catherine Demers, P. Van Nguyen, David Anderson, David Green, Jack Hirsh, William Geerts, Jeffrey S. Ginsberg, and Betsy MacKinnon

Subjects
Adult, Male, Time Factors, Hemorrhage, Receptors, Cell Surface, Placebo, Drug Administration Schedule, Double-Blind Method, Risk Factors, Thromboembolism, Secondary Prevention, medicine, Humans, Point Mutation, Risk factor, Aged, Venous Thrombosis, First episode, business.industry, Warfarin, Absolute risk reduction, Anticoagulants, Hematology, Middle Aged, medicine.disease, Confidence interval, Discontinuation, Venous thrombosis, Anesthesia, Antibodies, Antiphospholipid, Female, Prothrombin, business, medicine.drug
Abstract

Summary. Background: The risk of recurrence is lower after treatment of an episode of venous thromboembolism associated with a transient risk factor, such as recent surgery, than after an episode associated with a permanent, or no, risk factor. Retrospective analyses suggest that 1 month of anticoagulation is adequate for patients whose venous thromboembolic event was provoked by a transient risk factor. Methods: In this double-blind study, patients who had completed 1 month of anticoagulant therapy for a first episode of venous thromboembolism provoked by a transient risk factor were randomly assigned to continue warfarin or to placebo for an additional 2 months. Our goal was to determine if the duration of treatment could be reduced without increasing the rate of recurrent venous thromboembolism during 11 months of follow-up. Results: Of 84 patients assigned to placebo, five (6.0%) had recurrent venous thromboembolism, compared with three of 81 (3.7%) assigned to warfarin, resulting in an absolute risk difference of 2.3%[95% confidence interval (CI) − 5.2, 10.0]. The incidence of recurrent venous thromboembolism after discontinuation of warfarin was 6.8% per patient-year in those who received warfarin for 1 month and 3.2% per patient-year in those who received warfarin for 3 months (rate difference of 3.6% per patient-year; 95% CI − 3.8, 11.0). There were no major bleeds in either group. Conclusion: Duration of anticoagulant therapy for venous thromboembolism provoked by a transient risk factor should not be reduced from 3 months to 1 month as this is likely to increase recurrent venous thromboembolism without achieving a clinically important decrease in bleeding.

Published
2004

13. A Protease TAMER: a nucleic acid‐based anticoagulant

Author

James C. Fredenburgh, Colin A. Kretz, and J. I. Weitz

Subjects
Protease, Chemistry, medicine.drug_class, medicine.medical_treatment, Aptamer, Antidotes, Anticoagulant, Thrombin, Anticoagulants, RNA, Hematology, Aptamers, Nucleotide, Thrombin generation, Molecular biology, Article, Biochemistry, Thrombin activity, medicine, Nucleic acid, Animals, Humans, Prothrombin, Blood Coagulation, circulatory and respiratory physiology
Abstract

See also Bompiani KM, Monroe DM, Church FC, Sullenger BA. A high affinity, antidote-controllable prothrombin and thrombin-binding RNA aptamer inhibits thrombin generation and thrombin activity. This issue, pp 870–80.

Published
2012

14. Active metabolite concentration of clopidogrel in patients taking different doses of aspirin: results of the interaction trial

Author

John W. Eikelboom, Jack Hirsh, Yan Liang, J. I. Weitz, Guillaume Paré, P. Gao, D. Sloane, and Jun Zhu

Subjects
Male, medicine.medical_specialty, Ticlopidine, Genotype, medicine.drug_class, Proton-pump inhibitor, Renal function, CYP2C19, Pharmacology, Gastroenterology, Loading dose, Drug Administration Schedule, Activation, Metabolic, Pharmacokinetics, Risk Factors, Internal medicine, Medicine, Humans, Drug Interactions, Active metabolite, Aged, Aspirin, business.industry, Hematology, Middle Aged, Clopidogrel, Cytochrome P-450 CYP2C19, Phenotype, Drug Therapy, Combination, Female, Drug Monitoring, business, Platelet Aggregation Inhibitors, medicine.drug
Abstract

Background The CURRENT-OASIS-7 and PLATO trials suggest that the benefit of clopidogrel is influenced by the dose of aspirin. Objective To explore a potential pharmacokinetic interaction between aspirin and clopidogrel, and determinants of clopidogrel active metabolite (AM) levels. Methods In part 1, using a 2 × 2 factorial design, we randomized patients to clopidogrel 600 mg loading dose (LD) followed by 150 mg day(-1) for 6 days and 75 mg day(-1) thereafter, or clopidogrel 300 mg LD followed by 75 mg day(-1) thereafter, and compared aspirin at 325 mg or 81 mg day(-1) . In part 2, patients were given a 600-mg clopidogrel LD, and were randomly allocated to aspirin 325 mg or 81 mg day(-1) . We combine the data from the two parts. Blood samples were collected 1 h after administration of the study drug. Results We randomized 302 patients (mean age 60.4 ± 9.9 years). Clopidogrel AM levels were similar in patients randomized to aspirin 325 or 81 mg (geometric mean, 12.70 ng mL(-1) ; 95% CI, 10.96-14.72 ng mL(-1) ; and geometric mean, 12.55 ng mL(-1) ; 95% CI, 10.80-14.58 ng mL(-1) ; P = 0.91). Blood levels of clopidogrel were lower in CYP2C19*2 loss-of-function (LOF) carriers compared with non-carriers (10.72 ng mL(-1) ; 95% CI, 8.83-13.01 ng mL(-1) ; and 15.21 ng mL(-1) ; 95% CI, 13.30-17.40 ng mL(-1) , respectively; P = 0.003) whereas levels in gain of function carriers and non-carriers were similar (13.31 ng mL(-1) ; 95% CI, 11.53-15.35 ng mL(-1) ; and 14.07 ng mL(-1) ; 95% CI, 11.74-16.87 ng mL(-1) , respectively; P = 0.4). Independent baseline predictors of clopidogrel AM levels were LOF genotype, body mass index, diabetes, proton pump inhibitor use and creatinine clearance, but accounted for only 20% of the variability in levels. Conclusion Aspirin dose does not predict clopidogrel AM levels 1 h post-LD. Most of the variability in clopidogrel AM levels is not explained by patient characteristics or CYP2C19 metabolizer status.

Published
2014

15. Guidance, guidelines, and communications

Author

J. I. Weitz and James D. Douketis

Subjects
World Wide Web, Text mining, business.industry, Neoplasms, Cardiology, Medicine, Humans, Hematology, Venous Thromboembolism, business
Published
2014

16. Comparison of the effects of apixaban and rivaroxaban on prothrombin and activated partial thromboplastin times using various reagents

Author

Jack Hirsh, Brian Dale, John W. Eikelboom, J. I. Weitz, Jeffrey S. Ginsberg, Marilyn Johnston, Dale, BJ, Ginsberg, JS, Johnston, M, Hirsh, J, Weitz, JI, and Eikelboom, JW

Subjects
anticoagulants, Pyridones, Morpholines, apixaban, Thiophenes, Rivaroxaban, Predictive Value of Tests, activated partial thromboplastin time, medicine, Coagulation testing, Thromboplastin, Humans, rivaroxaban, Blood Coagulation, Prothrombin time, Chromatography, medicine.diagnostic_test, Dose-Response Relationship, Drug, Chemistry, Reproducibility of Results, Hematology, Plasma levels, prothrombin time, Anesthesia, Reagent, Prothrombin Time, Pyrazoles, Apixaban, Partial Thromboplastin Time, medicine.drug, Partial thromboplastin time, Factor Xa Inhibitors
Abstract

Background: Clinical situations occur where expedient assessment of the anticoagulant activity of the direct factor Xa (FXa) inhibitors is required. Although quantitative anti-FXa (FXa) assays can be used to measure plasma levels of apixaban or rivaroxaban, turnaround is often slow and many laboratories do not perform these assays. Objective: We compared the in vitro effects of apixaban and rivaroxaban on two readily available laboratory tests, the prothrombin time (PT) and activated partial thromboplastin time (APTT), performed with different reagents. We aimed to identify the most sensitive reagents. Methods: Rivaroxaban or apixaban was added to human plasma at a range of concentrations covering expected peak and trough levels, and concentrations were confirmed using calibrated anti-FXa assays. Samples were assayed with six PT and seven APTT reagents using different coagulometers. Results and Conclusions: TriniCLOT PT Excel S was the only reagent to demonstrate sensitivity to apixaban. All of the PT reagents were sensitive to rivaroxaban with TriniCLOT PT Excel S and HemosIL HS PLUS being the most sensitive. Sensitivity to rivaroxaban varied among APTT reagents; four reagents exhibited the greatest responsiveness, and of these, Actin FSL was the most responsive. Commonly used coagulation tests may be useful for assessing the anticoagulant effect of rivaroxaban but not of apixaban. The reason for the different effects of apixaban and rivaroxaban on the PT and APTT is unknown. Refereed/Peer-reviewed

Published
2014

17. Comparison of three-factor and four-factor prothrombin complex concentrates regarding reversal of the anticoagulant effects of rivaroxaban in healthy volunteers

Author

J. I. Weitz, Marcel Levi, M. Raghoebar, Samuel Z. Goldhaber, C. F. Castillejos, Kenneth Todd Moore, Jerrold H. Levy, Scott D. Berkowitz, Dagmar Kubitza, Manesh R. Patel, and Vascular Medicine

Subjects
Adult, Male, Time Factors, Adolescent, medicine.drug_class, medicine.medical_treatment, Morpholines, Hemorrhage, Thiophenes, Pharmacology, Drug Administration Schedule, Body Mass Index, Factor IX, Young Adult, Rivaroxaban, Healthy volunteers, medicine, Humans, Saline, Prothrombin time, medicine.diagnostic_test, business.industry, Anticoagulant, Thrombin, Anticoagulants, Hematology, Factor VII, Middle Aged, Blood Coagulation Factors, Healthy Volunteers, Drug Combinations, Treatment Outcome, Pharmacodynamics, Area Under Curve, Factor X, Prothrombin Time, Female, Partial Thromboplastin Time, Prothrombin, business, PROTHROMBIN COMPLEX, Andexanet alfa, medicine.drug
Abstract

Summary Background Four-factor prothrombin complex concentrates (PCCs), which contain factor II, FVII, FIX, and FX, have shown the potential to reverse the anticoagulant effect of rivaroxaban in healthy volunteers. The purpose of this study was to determine whether a three-factor PCC, which contains little FVII, has a similar effect. Methods and results We performed an open-label, single-center, parallel-group study comparing the effect of a three-factor PCC (Profilnine SD) with that of a four-factor PCC (Beriplex P/N) on the pharmacodynamics of rivaroxaban in 35 healthy volunteers. After receiving 4 days of rivaroxaban 20 mg twice daily to obtain supratherapeutic steady-state concentrations, volunteers were randomized to receive a single 50 IU kg−1 bolus dose of four-factor PCC, three-factor PCC or saline 4 h after the morning dose of rivaroxaban on day 5, and the effects of these interventions on prothrombin time and thrombin generation were determined. Within 30 min, four-factor PCC reduced mean prothrombin time by 2.5–3.5 s, whereas three-factor PCC produced only a 0.6–1.0-s reduction. In contrast, three-factor PCC reversed rivaroxaban-induced changes in thrombin generation more than four-factor PCC. Conclusions This study demonstrates the potential of both three-factor and four-factor PCCs to at least partially reverse the anticoagulant effects of rivaroxaban in healthy adults. The discrepant effects of the PCC preparations may reflect differences in the procoagulant components present in each.

Published
2013

18. Homocysteine-Induced Endoplasmic Reticulum Stress and Growth Arrest Leads to Specific Changes in Gene Expression in Human Vascular Endothelial Cells

Author

J. I. Weitz, Jun Li, Sudesh K. Sood, S. I. Pfeifer, Thomas J. Podor, P. A. Outinen, Sushmita Pamidi, and Richard C. Austin

Subjects
Regulation of gene expression, medicine.medical_specialty, Clusterin, biology, Homocysteine, Gadd45, Endoplasmic reticulum, Immunology, Cell Biology, Hematology, Biochemistry, Cell biology, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Gene expression, medicine, Unfolded protein response, biology.protein, Northern blot
Abstract

Alterations in the cellular redox potential by homocysteine promote endothelial cell (EC) dysfunction, an early event in the progression of atherothrombotic disease. In this study, we demonstrate that homocysteine causes endoplasmic reticulum (ER) stress and growth arrest in human umbilical vein endothelial cells (HUVEC). To determine if these effects reflect specific changes in gene expression, cDNA microarrays were screened using radiolabeled cDNA probes generated from mRNA derived from HUVEC, cultured in the absence or presence of homocysteine. Good correlation was observed between expression profiles determined by this method and by Northern blotting. Consistent with its adverse effects on the ER, homocysteine alters the expression of genes sensitive to ER stress (ie, GADD45, GADD153, ATF-4, YY1). Several other genes observed to be differentially expressed by homocysteine are known to mediate cell growth and differentiation (ie, GADD45, GADD153, Id-1, cyclin D1, FRA-2), a finding that supports the observation that homocysteine causes a dose-dependent decrease in DNA synthesis in HUVEC. Additional gene profiles also show that homocysteine decreases cellular antioxidant potential (glutathione peroxidase, NKEF-B PAG, superoxide dismutase, clusterin), which could potentially enhance the cytotoxic effects of agents or conditions known to cause oxidative damage. These results successfully demonstrate the use of cDNA microarrays in identifying homocysteine-respondent genes and indicate that homocysteine-induced ER stress and growth arrest reflect specific changes in gene expression in human vascular EC.

Published
1999

19. A simple clinical model for the diagnosis of deep-vein thrombosis combined with impedance plethysmography: potential for an improvement in the diagnostic process

Author

Alberto Cogo, Jeffrey S. Ginsberg, Clive Kearon, J. I. Weitz, P. S. Wells, D. R. Anderson, Paolo Prandoni, A. W. A. Lensing, Jack Hirsh, Gary Foster, Robert D'Ovidio, and Antonio Girolami

Subjects
Score test, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Deep vein, Venography, Surgery, Pre- and post-test probability, medicine.anatomical_structure, Internal Medicine, Medicine, Plethysmograph, Radiology, Medical diagnosis, business, Prospective cohort study, Lower limbs venous ultrasonography
Abstract

Wells PS, Hirsh J, Anderson DR, Lensing AWA, Foster G, Kearon C, Weitz J, D'Ovidio R, Cogo A, Prandoni P, Girolami A, Ginsberg JS (Ottawa Civic Hospital, Ottawa, Hamilton Civic Hospitals Research Centre, Henderson General Hospital, and McMaster University, Hamilton, Ontario, and Victoria General Hospital, Nova Scotia, Canada; Instituto di Semeioti Medica, Padua, Italy; and Academic Medical Centre, Amsterdam, the Netherlands). A simple clinical model for the diagnosis of deep-vein thrombosis combined with impedance plethysmography: potential for an improvement in the diagnostic process. J Intern Med 1998; 243: 15–23. Objectives We recently demonstrated the utility of a clinical model combined with ultrasonography to assist the diagnostic approach in patients with suspected deep-vein thrombosis (DVT). In this study we also sought to demonstrate that the model is useful with impedance plethysmography, a less accurate and less utilized diagnostic test. The original clinical model is slightly cumbersome to use; thus at the completion of the study we attempted to develop a simpler scoring system with a goal of maintaining accuracy. Design An open, nonrandomized, multicentre trial. Setting Three centres, two in Canada, and one in Italy. Subjects Ambulatory patients with suspected deep-vein thrombosis. Interventions All patients were assessed clinically to determine the probability for deep-vein thrombosis prior to performing impedance plethysmography and venography. We compared the accuracy of impedance plethysmography between the three pretest probability categories of high, moderate and low. All of the above were performed and interpreted by independent observers. When the study was completed, we revised the clinical model by first performing a simple regression analysis then a multiple logistic regression analysis; a scoring system was devised using the latter. Results Impedance plethysmography is significantly more sensitive and less specific for all DVT in patients with high pretest probability for deep-vein thrombosis (P= 0.001). The post- test probability (positive predictive value) for deep-vein thrombosis with an abnormal impedance plethysmography result was significantly different (P= 0.0001) between the three pretest probability categories. Multiple regression analysis has provided a new model with only nine variables and a simple scoring system. The retrospective application of the revised clinical model, which is simpler to use, suggests it will provide similar results as the original clinical model when combined with impedance plethysmography. The combination of impedance plethysmography and the clinical model suggests patients are likely to have false positive results if they have a low or moderate pretest probability for deep-vein thrombosis and false negative results if the pretest probability is high. The combination of a low pretest probability and a normal impedance plethysmography result may exclude the need for serial testing, and represented more than 50% of our patient population. Conclusions The use of the clinical model in conjunction with impedance plethysmography would decrease the number of false positive and negative diagnoses and could markedly decrease the need for serial impedance plethysmography. Combining the clinical model with impedance plethysmography could overcome the fact that impedance plethysmography is clearly less accurate than venous ultrasound imaging. The use of the revised clinical model may increase acceptability and utility, but prospective testing is required before widespread use.

Published
1998

20. Low-molecular-weight heparin in the treatment of patients with venous thromboembolism

Author

CA Hoefnagel, B StJacques, Jareer Kassis, Krystyna Kinnon, Terri Finch, M Berger, E Ascari, F. Turkstra, J Stanford, M Escribano, Mmw Koopman, Judy Kovacs, D ElKouri, Agg Turpie, J vanderMeer, Antonio Girolami, Eki Code, PM Manucci, Beverly Morrow, Paolo Bucciarelli, A vanBarneveld, Susan Haley, Sergio Siragusa, Paul Ockelford, Manuel Monreal, G Garrido, P Nguyen, Marco Moia, D Cohlan, S Bornais, D. P. M. Brandjes, M Barone, B Girolami, Dianne Donovan, Sabina Villalta, S Roy, E Lafoz, Ejr vanBeek, S Serafini, Judith Johnson, L Biagioni, B Petiteau, Patrick Brill-Edwards, L Rossi, Beng H. Chong, L Wilkinson, MA Pistorius, Jeffrey S. Ginsberg, B Planchon, P Bagatella, M vonLewinski, J Jagot, Sylvia Haas, Moira Cruickshank, YP Graafsma, R. Baildon, Michael Gent, Awa Lensing, J. I. Weitz, Christine Demers, JN Fiesinger, Richard M. Jay, Alexander Gallus, William Geerts, Gth Que, S Finkenbine, Clive Kearon, C N Chesterman, Eleanor Boyle, L Couture, L LIberale, Anderson, LT Eimers, C Rich, G Simonneau, F Parent, WM Smid, Pmm Kuijer, B Palmer, R Faivre, J CoteDesjardins, KS Robinson, F Lossner, WM Brien, K Redekop, [No Value] Cusson, M deRijk, Paolo Prandoni, T Bynon, James D. Douketis, D Goudie, Janis Bormanis, [No Value] Leclerc, Louis Desjardins, C Beltrametti, JW tenCate, H Jagt, Martin H. Prins, Michael J. Kovacs, FA Spengel, S Whittaker, M Ruel, H. R. Büller, P. S. Wells, Franco Piovella, Jack Hirsh, John Cade, Barbara A. Hutten, J Poulin, JC Sahuquillo, J Villenueve, Jgp Tijssen, Rohan J. K. Hettiarachchi, S Pritchard, Other departments, and Faculteit Medische Wetenschappen/UMCG

Subjects
Male, medicine.medical_specialty, medicine.drug_class, Venography, INTRAVENOUS UNFRACTIONATED HEPARIN, Low molecular weight heparin, Hemorrhage, Death, Sudden, SUSPECTED PULMONARY-EMBOLISM, Recurrence, STANDARD HEPARIN, medicine, MANAGEMENT, Humans, DEEP-VEIN THROMBOSIS, HOME, METAANALYSIS, medicine.diagnostic_test, Heparin, business.industry, Mortality rate, Anticoagulants, General Medicine, Heparin, Low-Molecular-Weight, Middle Aged, Thrombophlebitis, Reviparin sodium, medicine.disease, Thrombosis, Surgery, Pulmonary embolism, VENOGRAPHY, Treatment Outcome, INITIAL TREATMENT, Female, Pulmonary Embolism, business, Venous thromboembolism, medicine.drug
Abstract

Background Low-molecular-weight heparin is known to be safe and effective for the initial Treatment of patients with proximal deep-vein thrombosis. However, its application to patients with pulmonary embolism or previous episodes of thromboembolism has not been studied.Methods We randomly assigned 1021 patients with symptomatic venous thromboembolism to fixed-dose, subcutaneous low-molecular-weight heparin (reviparin sodium) or adjusted-dose, intravenous unfractionated heparin. Oral anticoagulant therapy with a coumarin derivative was started concomitantly and continued for 12 weeks, Approximately one third of the patients had associated pulmonary embolism, The outcome events studied over the 12 weeks were symptomatic recurrent venous thromboembolism, major bleeding, and death. We sought to determine whether low-molecular-weight heparin is at least equivalent to unfractionated heparin in patients with venous thromboembolism.Results Twenty-seven of the 510 patients assigned to low-molecular-weight heparin (5.3 percent) had recurrent thromboembolic events, as compared with 25 of the 511 patients assigned to unfractionated heparin (4.9 percent). The difference of 0.4 percentage point indicates that the two therapies have equivalent value according to our predetermined definition of equivalence. Sixteen patients assigned to low-molecular-weight heparin (3.1 percent) and 12 patients assigned to unfractionated heparin (2.3 percent) had episodes of major bleeding (P=0.63), and the mortality rates in the two groups were 7.1 percent and 7.6 percent, respectively (P=0.89).Conclusions Fixed-dose, subcutaneous low-molecular-weight heparin is as effective and safe as adjusted-dose, intravenous unfractionated heparin for the initial management of venous thromboembolism, regardless of whether the patient has pulmonary embolism or a history of venous thromboembolism. (C) 1997, Massachusetts Medical Society.

Published
1997

21. Diannexin, an annexin A5 homodimer, binds phosphatidylserine with high affinity and is a potent inhibitor of platelet-mediated events during thrombus formation

Author

Margaret L. Rand, Alan R. Stafford, Fred G. Pluthero, H. Wang, Nima Vaezzadeh, A. C. Allison, Peter L. Gross, J. I. Weitz, Ran Ni, and Walter H. A. Kahr

Subjects
Blood Platelets, Male, Time Factors, Lipid Bilayers, Phosphatidylserines, Flow cytometry, chemistry.chemical_compound, Mice, Fibrinolytic Agents, medicine, Animals, Humans, Platelet, Platelet activation, Thrombus, Annexin A5, Blood Coagulation, Hemostasis, Microscopy, Video, medicine.diagnostic_test, Dose-Response Relationship, Drug, Chemistry, Thrombin, Thrombosis, Hematology, Phosphatidylserine, Surface Plasmon Resonance, medicine.disease, Flow Cytometry, Platelet Activation, Molecular biology, In vitro, Thrombelastography, Mice, Inbred C57BL, Disease Models, Animal, Dimerization, Platelet Aggregation Inhibitors
Abstract

Summary. Background: Shielding of procoagulant phosphatidylserine (PS) with annexin A5 attenuates thrombosis, but annexin A5 (35.7 kDa) is rapidly cleared from the circulation. In contrast, Diannexin, a 73.1 kDa homodimer of annexin A5, has an extended half-life. Objectives: To quantify the affinity of Diannexin for PS, examine its interaction with activated platelets and determine its effects on platelet-mediated events during thrombus formation. Methods: The affinities of Diannexin and annexin A5 for PS-containing lipid bilayers were compared using surface plasmon resonance, and binding to activated platelets was assessed by flow cytometry. Calibrated automated thrombography and thromboelastography were employed to study the effects of Diannexin on thrombin generation and platelet-fibrin clot formation, respectively, whereas intravital videomicroscopy was used to examine its effect on platelet accumulation and activation after laserinduced injury to murine cremaster arterioles, and a tail tip bleeding model was used to explore its effects on hemostasis. Results: Diannexin and annexin A5 bind PS with KD values of 0.6 and 5 nM, respectively, and both bind to the same subpopulation of PS-exposing platelets. Diannexin inhibited thrombin generation and platelet-fibrin clot formation in vitro at 10 nM (P < 0.05–0.001 compared with control), and reduced platelet accumulation at 1 l gg )1 (P < 0.05) and activation at 0.25 l gg )1 (P < 0.001) in experimentally induced arterial thrombi in mice while increasing blood loss at 1 l gg )1 (P

Published
2012

22. Elevated tissue factor procoagulant activity in CD133-positive cancer cells

Author

Janusz Rak, G. M. Anderson, Chloe Milsom, and J. I. Weitz

Subjects
business.industry, Hematology, Thromboplastin, Tissue factor, Text mining, Antigens, CD, Cell Line, Tumor, Cancer cell, Cancer research, Carcinoma, Squamous Cell, Neoplastic Stem Cells, Medicine, Humans, Tissue Factor Procoagulant, AC133 Antigen, Caco-2 Cells, business, Peptides, Glycoproteins
Published
2007

27. The mechanism of action of thrombin inhibitors

Author

S M, Bates and J I, Weitz

Subjects
Fibrin, Coronary Thrombosis, Humans, Receptors, Thrombin, Thrombolytic Therapy, Angioplasty, Balloon, Coronary, Platelet Activation, Platelet Factor 4, Blood Coagulation, Antithrombins
Abstract

Although heparin is widely used to treat arterial thrombosis, it has limitations in this setting. These limitations reflect heparin's inability to inactivate fibrin-bound thrombin, a major stimulus for thrombus growth, and the fact that heparin is neutralized by platelet factor 4, large quantities of which are released from platelets at the site of plaque rupture. Heparin also has a propensity to bind non-specifically to other plasma proteins. Because plasma levels of these heparin-binding proteins vary from patient to patient, the anticoagulant response to heparin is unpredictable and careful laboratory monitoring is necessary to ensure that an adequate anticoagulant effect is achieved. Direct thrombin inhibitors, such as bivalirudin and hirudin, overcome many of the limitations of heparin. These agents inhibit fibrin-bound thrombin, as well as fluid-phase thrombin. Direct thrombin inhibitors also produce a more predictable anticoagulant response than heparin because they do not bind to plasma proteins and are not neutralized by platelet factor 4. Bivalirudin appears to have a wider therapeutic window than hirudin. Because this may permit administration of higher doses of bivalirudin, this agent may also have an efficacy advantage over hirudin. Differences observed between hirudin and bivalirudin demonstrate that not all direct thrombin inhibitors have the same risk-benefit profile.

Published
2001

28. Thrombin-activable fibrinolysis inhibitor attenuates (DD)E-mediated stimulation of plasminogen activation by reducing the affinity of (DD)E for tissue plasminogen activator. A potential mechanism for enhancing the fibrin specificity of tissue plasminogen activator

Author

R J, Stewart, J C, Fredenburgh, J A, Rischke, L, Bajzar, and J I, Weitz

Subjects
Carboxypeptidase B2, Fibrin, Lysine, Carboxypeptidases, Arginine, Carboxypeptidase B, Amino Acid Chloromethyl Ketones, Enzyme Activation, Fibrin Fibrinogen Degradation Products, Kinetics, Models, Chemical, Tissue Plasminogen Activator, Humans, Electrophoresis, Polyacrylamide Gel, Fibrinolysin
Abstract

A complex of d-dimer noncovalently associated with fragment E ((DD)E), a degradation product of cross-linked fibrin that binds tissue plasminogen activator (t-PA) and plasminogen (Pg) with affinities similar to those of fibrin, compromises the fibrin specificity of t-PA by stimulating systemic Pg activation. In this study, we examined the effect of thrombin-activable fibrinolysis inhibitor (TAFI), a latent carboxypeptidase B (CPB)-like enzyme, on the stimulatory activity of (DD)E. Incubation of (DD)E with activated TAFI (TAFIa) or CPB (a) produces a 96% reduction in the capacity of (DD)E to stimulate t-PA-mediated activation of Glu- or Lys-Pg by reducing k(cat) and increasing K(m) for the reaction; (b) induces the release of 8 mol of lysine/mol of (DD)E, although most of the stimulatory activity is lost after release of only 4 mol of lysine/mol (DD)E; and (c) reduces the affinity of (DD)E for Glu-Pg, Lys-Pg, and t-PA by 2-, 4-, and 160-fold, respectively. Because TAFIa- or CPB-exposed (DD)E produces little stimulation of Glu-Pg activation by t-PA, (DD)E is not degraded into fragment E and d-dimer, the latter of which has been reported to impair fibrin polymerization. These data suggest a novel role for TAFIa. By attenuating systemic Pg activation by (DD)E, TAFIa renders t-PA more fibrin-specific.

Published
2000

29. Reactivation of coagulation after stopping infusions of recombinant hirudin and unfractionated heparin in unstable angina and myocardial infarction without ST elevation: results of a randomized trial. OASIS Pilot Study Investigators. Organization to Assess Strategies for Ischemic++ Syndromes

Author

M D, Flather, J I, Weitz, S, Yusuf, J, Pogue, B, Sussex, J, Campeau, J, Gill, R, Schuld, C D, Joyner, A L, Morris, C, Lai, P, Théroux, J F, Marquis, Y K, Chan, G, Venkatesh, and A, Jessel

Subjects
Male, Canada, Heparin, Antithrombin III, Myocardial Infarction, Anticoagulants, Hirudins, Middle Aged, Antithrombins, Drug Administration Schedule, Peptide Fragments, Recombinant Proteins, Electrocardiography, Fibrinolytic Agents, Humans, Female, Partial Thromboplastin Time, Prothrombin, Angina, Unstable, Infusions, Intravenous, Blood Coagulation, Biomarkers
Abstract

To compare effects of heparin and hirudin on biochemical markers of coagulation.Patients (n=395) with unstable angina or myocardial infarction without ST elevation were randomized to a 72-h infusion of one of three regimens: unfractionated heparin (bolus of 5000 IU followed by an infusion of 1200 IU. h(-1)), low-dose hirudin (HBW 023; 0.2 mg. kg(-1)bolus followed by 0.10 mg. kg(-1). h(-1)) or medium-dose hirudin (0.4 mg. kg(-1)bolus followed by 0.15 mg. kg(-1). h(-1)). Infusions were adjusted to maintain an activated partial thromboplastin time of between 60-100 s. Activated partial thromboplastin time, prothrombin fragment 1.2 (F1.2), thrombin antithrombin III complex and D-dimer were measured before, during and after the infusion. Median activated partial thromboplastin time was similar in the two groups early on, but was significantly lower in the heparin group than in the combined hirudin group 48 h after starting the infusion (53 s and 75 s, respectively;P0.001), and 6 h after stopping (31 s and 46 s, respectively;P0.001). Median F1.2 levels were not significantly different between the groups during the infusion. Median thrombin antithrombin III levels in the heparin and hirudin groups were 2.8 microg. l(-1)and 2.3 microg. l(-1), respectively, at 6 h (P0.001), and 3.0 microg. l(-1)and 2.3 microg. l(-1), respectively, at 48 h (P0.001). Median D-dimer levels were 320 ng. ml(-1)and 260 ng. ml(-1)48 h after starting the infusion in the heparin and hirudin groups, respectively (P0.001), and 415 ng. ml(-1)and 280 ng. ml(-1), respectively (P0.001) 6 h after stopping. D-dimer levels were significantly elevated above baseline values in both groups 24-48 h after stopping the infusions.The greater reduction of thrombin antithrombin III and D-dimer during the hirudin infusion supports the hypothesis that hirudin is a more potent antithrombin agent than heparin. Increased D-dimer levels after stopping heparin or hirudin suggest that there is an ongoing pro-coagulant state. These results point to the greater efficacy of hirudin in preventing early clinical events (death, myocardial infarction and refractory ischaemia) compared with heparin that have been observed in large randomized trials. Persistent activation of coagulation afterstopping infusions in our study suggests that a longer course of antithrombotic treatment may be needed to pacify the thrombus.

Published
2000

30. Homocysteine-induced endoplasmic reticulum stress and growth arrest leads to specific changes in gene expression in human vascular endothelial cells

Author

P A, Outinen, S K, Sood, S I, Pfeifer, S, Pamidi, T J, Podor, J, Li, J I, Weitz, and R C, Austin

Subjects
Intracellular Signaling Peptides and Proteins, Proteins, Endoplasmic Reticulum, Activating Transcription Factor 4, DNA-Binding Proteins, Gene Expression Regulation, CCAAT-Enhancer-Binding Proteins, Erythroid-Specific DNA-Binding Factors, Humans, Endothelium, Vascular, Homocysteine, Cell Division, Cells, Cultured, Transcription Factor CHOP, YY1 Transcription Factor, Transcription Factors
Abstract

Alterations in the cellular redox potential by homocysteine promote endothelial cell (EC) dysfunction, an early event in the progression of atherothrombotic disease. In this study, we demonstrate that homocysteine causes endoplasmic reticulum (ER) stress and growth arrest in human umbilical vein endothelial cells (HUVEC). To determine if these effects reflect specific changes in gene expression, cDNA microarrays were screened using radiolabeled cDNA probes generated from mRNA derived from HUVEC, cultured in the absence or presence of homocysteine. Good correlation was observed between expression profiles determined by this method and by Northern blotting. Consistent with its adverse effects on the ER, homocysteine alters the expression of genes sensitive to ER stress (ie, GADD45, GADD153, ATF-4, YY1). Several other genes observed to be differentially expressed by homocysteine are known to mediate cell growth and differentiation (ie, GADD45, GADD153, Id-1, cyclin D1, FRA-2), a finding that supports the observation that homocysteine causes a dose-dependent decrease in DNA synthesis in HUVEC. Additional gene profiles also show that homocysteine decreases cellular antioxidant potential (glutathione peroxidase, NKEF-B PAG, superoxide dismutase, clusterin), which could potentially enhance the cytotoxic effects of agents or conditions known to cause oxidative damage. These results successfully demonstrate the use of cDNA microarrays in identifying homocysteine-respondent genes and indicate that homocysteine-induced ER stress and growth arrest reflect specific changes in gene expression in human vascular EC.

Published
1999

31. A histomorphometric evaluation of heparin-induced bone loss after discontinuation of heparin treatment in rats

Author

S G, Shaughnessy, J, Hirsh, M, Bhandari, J M, Muir, E, Young, and J I, Weitz

Subjects
Rats, Sprague-Dawley, Osteoblasts, Fibrinolytic Agents, Heparin, Injections, Subcutaneous, Animals, Osteoclasts, Osteoporosis, Female, Femur, Rats
Abstract

Although it is well established that long-term heparin therapy causes osteoporosis, it is unknown whether heparin-induced bone loss is reversible when heparin treatment is stopped. To address this question, we randomized rats to once daily subcutaneous injections of either unfractionated heparin (1.0 U/g or 0.5 U/g) or saline for 28 days and then followed the rats for an additional 28 days off treatment. Based on histomorphometric analysis of the distal third of the right femur proximal to the epiphyseal growth plate, 1.0 U/g heparin caused a 30% loss in cancellous bone volume over the first 28 days. This was accompanied by a 137% increase in osteoclast surface and a 60% decrease in both osteoblast and osteoid surface. One month after cessation of heparin treatment, no recovery in these parameters was observed. Similarly, serum levels of alkaline phosphatase, a biochemical marker of bone formation, which continued to decrease over the course of heparin treatment, showed no signs of recovery in the subsequent 28 days off treatment. To explore the mechanism responsible for the prolonged effect of heparin on bone, we repeated the experiment giving 125I-labeled heparin in place of unlabeled heparin. 125I-labeled heparin was found to accumulate in bone during the course of its administration, and be retained in bone for at least 56 days after stopping heparin treatment. These findings suggest that heparin-induced osteoporosis is not rapidly reversible because heparin is sequestered in bone for an extended period.

Published
1999

32. Homocysteine-dependent alterations in mitochondrial gene expression, function and structure. Homocysteine and H2O2 act synergistically to enhance mitochondrial damage

Author

R C, Austin, S K, Sood, A M, Dorward, G, Singh, S G, Shaughnessy, S, Pamidi, P A, Outinen, and J I, Weitz

Subjects
Free Radicals, Cell Survival, Gene Expression, Drug Synergism, Chaperonin 60, Hydrogen Peroxide, Blotting, Northern, DNA, Mitochondrial, Cell Line, Mitochondria, Rats, Structure-Activity Relationship, Oxygen Consumption, Animals, Humans, RNA, Messenger, Homocysteine, Copper
Abstract

Mitochondrial abnormalities have been identified in hepatocytes of patients with hyperhomocysteinemia and in endothelial cells from the aortas of rats with diet-induced hyperhomocysteinemia. However, the mechanism by which homocysteine affects mitochondria is unknown. In this report, homocysteine-induced expression of the mitochondrial electron transport chain gene, cytochrome c oxidase III/ATPase 6,8 (CO3/ATPase 6,8), was identified in a human megakaryocytic cell line DAMI using mRNA differential display. Steady-state mRNA levels of CO3/ATPase 6,8, as well as other mitochondrial transcripts, were increased in DAMI cells by homocysteine in a concentration- and time-dependent manner. Despite an increase in mitochondrial RNA levels and changes in mitochondrial ultrastructure, no effect on either cell growth or mitochondrial respiration rates was observed in DAMI cells exposed to homocysteine at concentrations up to 1 mM. In contrast, 1 mM homocysteine in the presence of Cu2+, which is known to generate H2O2, significantly decreased mitochondrial RNA levels, caused gross morphological changes in mitochondrial ultrastructure, and inhibited both cell growth and mitochondrial respiration rates. However, precursors of cellular glutathione and preexposure to heat shock blocked the decrease in mitochondrial RNA levels caused by homocysteine and Cu2+. The observations that (i) homocysteine and H2O2, but not H2O2 alone, caused a decrease in mitochondrial RNA levels, (ii) intracellular levels of H2O2 were significantly increased in the presence of homocysteine and Cu2+, and (iii) catalase, but not free radical scavengers, prevented a decrease in mitochondrial RNA levels, provide evidence that homocysteine and H2O2 act synergistically to cause mitochondrial damage. Furthermore, our findings suggest that intracellular glutathione and heat shock proteins play a role in protecting mitochondria against the adverse effects elicited by homocysteine and H2O2.

Published
1998

33. Characterization of the stress-inducing effects of homocysteine

Author

Richard C. Austin, Thomas J. Podor, Nobuyo Maeda, J. I. Weitz, Patricia C. Liaw, Jack Hirsh, Kevin D. Sarge, P. A. Outinen, José C.O Ribau, and Sudesh K. Sood

Subjects
medicine.medical_specialty, Homocysteine, Cystathionine beta-Synthase, Biology, medicine.disease_cause, Biochemistry, Mice, chemistry.chemical_compound, Stress, Physiological, Internal medicine, Heat shock protein, Gene expression, medicine, Animals, Humans, HSP70 Heat-Shock Proteins, RNA, Messenger, Endoplasmic Reticulum Chaperone BiP, Molecular Biology, Cells, Cultured, Heat-Shock Proteins, chemistry.chemical_classification, Glutathione peroxidase, Muscle, Smooth, Hydrogen Peroxide, Cell Biology, Immunohistochemistry, Molecular biology, Cystathionine beta synthase, Hsp70, DNA-Binding Proteins, Heat shock factor, Disease Models, Animal, Endocrinology, Gene Expression Regulation, chemistry, CCAAT-Enhancer-Binding Proteins, biology.protein, Endothelium, Vascular, Carrier Proteins, Transcription Factor CHOP, Oxidative stress, Research Article, Molecular Chaperones, Transcription Factors
Abstract

The mechanism by which homocysteine causes endothelial cell (EC) injury and/or dysfunction is not fully understood. To examine the stress-inducing effects of homocysteine on ECs, mRNA differential display and cDNA microarrays were used to evaluate changes in gene expression in cultured human umbilical-vein endothelial cells (HUVEC) exposed to homocysteine. Here we show that homocysteine increases the expression of GRP78 and GADD153, stress-response genes induced by agents or conditions that adversely affect the function of the endoplasmic reticulum (ER). Induction of GRP78 was specific for homocysteine because other thiol-containing amino acids, heat shock or H2O2 did not appreciably increase GRP78 mRNA levels. Homocysteine failed to elicit an oxidative stress response in HUVEC because it had no effect on the expression of heat shock proteins (HSPs) including HSP70, nor did it activate heat shock transcription factor 1. Furthermore homocysteine blocked the H2O2-induced expression of HSP70. In support of our findings in vitro, steady-state mRNA levels of GRP78, but not HSP70, were elevated in the livers of cystathionine β-synthase-deficient mice with hyperhomocysteinaemia. These studies indicate that the activation of stress response genes by homocysteine involves reductive stress leading to altered ER function and is in contrast with that of most other EC perturbants. The observation that homocysteine also decreases the expression of the antioxidant enzymes glutathione peroxidase and natural killer-enhancing factor B suggests that homocysteine could potentially enhance the cytotoxic effect of agents or conditions known to cause oxidative stress.

Published
1998
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34. A histomorphometric comparison of the effects of heparin and low-molecular-weight heparin on cancellous bone in rats

Author

J M, Muir, J, Hirsh, J I, Weitz, M, Andrew, E, Young, and S G, Shaughnessy

Subjects
Bone Development, Heparin, Heparin, Low-Molecular-Weight, Alkaline Phosphatase, Bone and Bones, Rats, Rats, Sprague-Dawley, Bone Diseases, Metabolic, Tinzaparin, Fibrinolytic Agents, Animals, Female, Collagen, Amino Acids, Bone Resorption, Biomarkers
Abstract

Long-term heparin treatment causes osteoporosis through, an as yet, undefined mechanism. To investigate this phenomenon and to determine the relative benefits of low-molecular-weight heparin (LMWH) use, we treated rats with once daily subcutaneous injections of either unfractionated heparin (1.0 U/g or 0.5 U/g), the LMWH, Tinzaparin (1.0 U/g or 0.5 U/g), or placebo (saline) for a period of 32 days. The effects on bone were then compared both histomorphometrically and biochemically by measuring urinary type I collagen cross-linked pyridinoline (PYD) and serum alkaline phosphatase, markers of bone resorption and formation, respectively. Histomorphometric analysis of the distal third of the right femur, in the region proximal to the epiphyseal growth plate, demonstrated that both heparin and LMWH decrease cancellous bone volume in a dose-dependent fashion, but that heparin causes significantly more cancellous bone loss than does LMWH. Although both heparin and LMWH decrease osteoblast and osteoid surface to a similar extent, only heparin increases osteoclast surface. In support of these histomorphometric findings, biochemical markers of bone turnover demonstrated that both heparin and LMWH treatment produce a dose-dependent decrease in serum alkaline phosphatase, consistent with reduced bone formation, whereas only heparin causes a transient increase in urinary PYD, consistent with an increase in bone resorption. Based on these observations, we conclude that heparin decreases cancellous bone volume both by decreasing the rate of bone formation and increasing the rate of bone resorption. In contrast, LMWH, causes less osteopenia than heparin because it only decreases the rate of bone formation.

Published
1997

35. Randomized trial to examine the effect of ASA dose or ASA dosing frequency on ASA resistance after coronary artery bypass graft surgery

Author

Guillaume Paré, J. I. Weitz, Jeremy S. Paikin, John W. Eikelboom, Richard P. Whitlock, Jack Hirsh, and Jeffrey S. Ginsberg

Subjects
medicine.medical_specialty, medicine.anatomical_structure, Randomized controlled trial, business.industry, law, Anesthesia, Medicine, Cardiology and Cardiovascular Medicine, business, Dosing Frequency, law.invention, Surgery, Artery
Published
2013

36. Histomorphometric analysis of the effects of standard heparin on trabecular bone in vivo

Author

J M, Muir, M, Andrew, J, Hirsh, J I, Weitz, E, Young, P, Deschamps, and S G, Shaughnessy

Subjects
Osteoblasts, Heparin, Osteoclasts, Tetracycline, Alkaline Phosphatase, Bone and Bones, Rats, Rats, Sprague-Dawley, Animals, Osteoporosis, Female, Collagen, Amino Acids, Bone Resorption, Epiphyses
Abstract

Long-term heparin treatment causes osteoporosis through an as yet undefined mechanism. To investigate this phenomenon, we treated rats with once daily subcutaneous injections of heparin (in doses ranging from 0.25 to 1.0 U/g) or saline for 8 to 32 days and monitored the effects on bone both histomorphometrically and by serial measurements of urinary type 1 collagen cross linked-pyridinoline (PYD) and serum alkaline phosphatase, markers of bone resorption and formation, respectively. Histomorphometric analysis of the distal third of the right femur in the region proximal to the epiphyseal growth plate showed that heparin induces both a time- and dose-dependent decreased in trabecular bone volume, with the majority of trabecular bone loss occurring within the first 8 days of treatment. Thus, heparin doses of 1.0 U/g/d resulted in a 32% loss of trabecular bone. Heparin-treated rats also showed a 37% decrease in osteoblast surface as well as a 75% decrease in osteoid surface. In contrast, heparin treatment had the opposite effect on osteoclast surface, which was 43% higher in heparin-treated rats, as compared with that in control rats. Biochemical markers of bone turnover showed that heparin treatment produced a dose-dependent decrease in serum alkaline phosphatase and a transient increase in urinary PYD, thus confirming the histomorphometric data. Based on these observations, we conclude that heparin decreases trabecular bone volume both by decreasing the rate of bone formation and increasing the rate of bone resorption.

Published
1996

37. Alpha 2-antiplasmin supplementation inhibits tissue plasminogen activator-induced fibrinogenolysis and bleeding with little effect on thrombolysis

Author

Jack Hirsh, Petr Klement, J. I. Weitz, and Beverly A. Leslie

Subjects
medicine.medical_specialty, Plasmin, medicine.medical_treatment, Alpha (ethology), Hemorrhage, Tissue plasminogen activator, Fibrinogenolysis, Aprotinin, Alpha 2-antiplasmin, Internal medicine, Fibrinolysis, medicine, Animals, Humans, alpha-2-Antiplasmin, business.industry, Fibrinogen, Drug Synergism, General Medicine, Thrombolysis, medicine.disease, Endocrinology, Tissue Plasminogen Activator, Immunology, Rabbits, business, medicine.drug, Research Article
Abstract

Tissue plasminogen activator (t-PA) causes fibrinogen proteolysis when alpha 2-antiplasmin levels fall, and this may contribute to t-PA-induced hemorrhage. Because clot-bound plasmin is protected from alpha 2-antiplasmin inhibition, we tested the possibility that alpha 2-antiplasmin supplementation would block t-PA-induced fibrinogenolysis and bleeding without affecting thrombolysis. When added to human or rabbit plasma, alpha 2-antiplasmin inhibits t-PA-induced fibrinogenolysis, but hat little effect on the lysis of 125I-fibrin clots. To examine its effect in vivo, rabbits with preformed 125I-labeled-jugular vein thrombi were randomized to receive t-PA, t-PA and alpha 2-antiplasmin, or saline. alpha 2-Antiplasmin infusion produced a modest decrease in t-PA-induced thrombolysis (from 40.2% to 30.1%, P = 0.12), but reduced fibrinogen consumption from 87% to 27% (P = 0.0001), and decreased blood loss from standardized ear incisions from 5,594 to 656 microliter (P < 0.0001). We hypothesize that alpha 2-antiplasmin limits t-PA-induced hemorrhage by inhibiting fibrinogenolysis and subsequent fragment X formation because (a) SDS-PAGE and immunoblot analysis indicate less fragment X formation in alpha 2-antiplasmin treated animals, and (b) when added to a solution of fibrinogen and plasminogen clotted with thrombin in the presence of t-PA, fragment X shortens the lysis time in a concentration-dependent fashion. These findings suggest that fragment X incorporation into hemostatic plugs contributes to t-PA-induced bleeding. By blocking t-PA-mediated fibrinogenolysis, alpha 2-antiplasmin supplementation may improve the safety of fibrin-specific plasminogen activators.

Published
1993

38. Urokinase has direct catalytic activity against fibrinogen and renders it less clottable by thrombin

Author

B Leslie and J. I. Weitz

Subjects
medicine.medical_treatment, Hirudin, In Vitro Techniques, Fibrinogen, Fibrinogenolysis, Substrate Specificity, Plasma, Thrombin, Fibrinolysis, medicine, Humans, Aprotinin, Blood Coagulation, Chromatography, High Pressure Liquid, Fibrinopeptide B, Urokinase, Enzyme Precursors, Chemistry, General Medicine, medicine.disease, Molecular biology, Urokinase-Type Plasminogen Activator, Molecular Weight, Kinetics, Plasminogen activator, medicine.drug, Research Article
Abstract

Recently, we demonstrated that tissue plasminogen activator directly releases fibrinopeptides A and B (FPA and FPB) from fibrinogen. The purpose of this study was to determine whether urokinase has similar activity. Incubation of urokinase with fibrinogen or heparinized plasma results in concentration-dependent FPB release unaccompanied by FPA cleavage. For equivalent amidolytic activity, high molecular weight urokinase releases twofold more FPB than the low molecular weight species. In contrast, prourokinase does not release FPB until activated to urokinase. Contaminating thrombin or plasma is not responsible for urokinase-mediated FPB release because this activity is unaccompanied by FPA or B beta 1-42 cleavage, and is unaffected by heparin, hirudin, a monospecific antibody against thrombin, aprotinin, or alpha 2-antiplasmin. FPB release reflects a direct action of urokinase on fibrinogen because release is completely inhibited by a monospecific antibody against the enzyme. Further, urokinase releases FPB from the FPB-containing substrate B beta 1-42, thus confirming its specificity for the B beta 14 (Arg)-B beta 15 (Gly) bond. In addition to FPB release, SDS-PAGE analysis of the time course of urokinase-mediated fibrinogenolysis indicates progressive proteolysis of both the A alpha- and B beta-chains of fibrinogen that occurs after FPB release is completed. As a consequence of urokinase-mediated fibrinogenolysis, there is progressive prolongation of the thrombin clotting time. These studies indicate that urokinase has direct catalytic activity against fibrinogen. By releasing FPB, a potent chemoattractant, and by rendering fibrinogen less clottable by thrombin, urokinase may participate in processes extending beyond fibrinolysis.

Published
1990

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