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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01225822
Other study ID # 1160.19
Secondary ID
Status Completed
Phase Phase 2
First received October 20, 2010
Last updated May 8, 2014
Start date November 2002

Study information

Verified date February 2014
Source Boehringer Ingelheim
Contact n/a
Is FDA regulated No
Health authority Austria:Belgium:Czech Republic:Denmark:Finland:France:Hungary:Italy: Ethics CommitteeNetherlands:Norway:South Africa:Sweden:
Study type Interventional

Clinical Trial Summary

The primary objective of this study is to establish the dose-response relationship with regard to efficacy and safety of BIBR 1048 (50 mg bis in die(b.i.d), 150 mg b.i.d, 225 mg b.i.d. and 300 mg quaque die(q.d) ) in preventing venous thromboembolism(VTE) in patients undergoing primary elective total hip and knee replacement.


Recruitment information / eligibility

Status Completed
Enrollment 1973
Est. completion date
Est. primary completion date August 2003
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion criteria

1. Patients scheduled to undergo a primary elective total hip or knee replacement.

2. Male of female being 18 years or older.

3. Patients weighing at least 40 kg.

4. Written informed consent for study participation.

Exclusion criteria

1. Bleeding diathesis, constitutional or acquired coagulation disorders.

2. Major surgery or trauma(e.g., hip fracture) within the last 3 months.

3. Cardiovascular disease

4. Any history of haemorrhagic stroke, intracranial or intraocular bleeding or cerebral ischaemic attacks lasting more than 24 hours and / or with cardiovascular pathological findings.

5. Deep vein thrombosis(DVT), gastrointestinal or pulmonary bleeding, gastric or duodenal ulcer within the last year.

6. History of or acute intracranial disease

7. Liver disease

8. Renal disease

9. Use of long-term anticoagulants or antiplatelet drugs within 7 days prior to hip/knee replacement operation.

10. Pre-menopausal women who are not surgically steriles, are nursing and are of child-bearing potential and are not practising acceptable methods of birth control

11. Known allergy to contrast media

12. Thrombocytopenia

13. Allergy against heparin.

14. Active malignant disease or current cytostatic treatment.

15. Treatment with an investigational drug in the past month.

16. Leg amputee

17. Known alcohol or drug abuse

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Prevention


Related Conditions & MeSH terms


Intervention

Drug:
Enoxaparin
Enoxaparin 40 mg s.c once a day for 5-10 days of treatment period
BIBR 1048
50 mg b.i.d BIBR 1048 capsule twice a day for 5-10 days of treatment period
BIBR 1048
150 mg b.i.d BIBR 1048 capsule twice a day for 5-10 treatment period
BIBR 1048
225 mg b.i.d BIBR 1048 capsule twice a day for 5-10 treatment period
BIBR 1048
300 mg q.d BIBR 1048 capsule for 5-10 treatment period

Locations

Country Name City State
Austria 1160.19.43004 Krankenhaus der Barmherzigen Schwestern Linz Linz
Austria 1160.19.43002 Orthopädisches Spital Speising Wien
Austria 1160.19.43001 A.ö. Krankenhaus d. Statutarstadt Wiener Neustadt Wr. Neustadt
Belgium 1160.19.32002 V.U.B. Jette Brussel
Belgium 1160.19.32004 UZ Gent Gent
Belgium 1160.19.32005 Virga Jesseziekenhuis Gent
Belgium 1160.19.32006 Boehringer Ingelheim Investigational Site Huy
Belgium 1160.19.32007 C.H.U. de Tivoli La Louvière
Czech Republic 1160.19.42004 University Hospital Brno Brno-Bohunice
Czech Republic 1160.19.42001 Hospital Kladno Kladno
Czech Republic 1160.19.42006 Hospital Mlada Boleslav Mlada Boleslav
Czech Republic 1160.19.42003 University Hospital Ostrava Ostrava
Czech Republic 1160.19.42005 University Hospital Plzen Plzen
Czech Republic 1160.19.42009 University Hospital Na Bulovce Prague 8
Denmark 1160.19.45042 Orthopedic Surgical Clinic Frederiksberg
Denmark 1160.19.45045 Gentofte Hospital Hellerup
Denmark 1160.19.45043 Herlev Hospital Herlev
Denmark 1160.19.45041 Hørsholm Sygehus Hørsholm
Denmark 1160.19.45044 Orthopedic Surgical Dept. Silkeborg
Finland 1160.19.35802 Keski-Suomen keskussairaala Jyväskylä
Finland 1160.19.35801 Oulun yliopistollinen sairaala, Leikkaus- ja tehohoidon yks. Oulu
France 1160.19.33004 Div Illkirch cedex
France 1160.19.33007 Clinique du Mail La Rochelle
France 1160.19.33009 Hôpital Edouard Herriot Lyon cedex 03
France 1160.19.33006 Clinique Mutualiste Saint-Etienne cedex 2
France 1160.19.33008 Clinique de l'Atlantique St Herblain cedex
Hungary 1160.19.36003 Sándor Péterfy Hospital Budapest
Hungary 1160.19.36001 Kálmán Pándy County Hospital Gyula
Hungary 1160.19.36004 Bács-Kiskun County Hospital Kecskemét
Hungary 1160.19.36002 Albert Szent-Györgyi Medical and Pharmacological Center Szeged
Hungary 1160.19.36005 Szent György Hospital Székesfehérvár
Italy 1160.19.39003 U. O. Ortopedia e Traumatologia Bergamo
Italy 1160.19.39005 Modulo Coordinazione Dipartimentale di Ricerca e Anestesia Bologna
Italy 1160.19.39002 Fondazione Centro S. Raffaele Milano
Italy 1160.19.39001 IRCCS Policlinico San Matteo Pavia
Italy 1160.19.39004 Ospedale di Circolo di Varese Varese
Netherlands 1160.19.31001 Boehringer Ingelheim Investigational Site Amsterdam
Netherlands 1160.19.31003 Boehringer Ingelheim Investigational Site Hilversum
Netherlands 1160.19.31005 Hengstdal 3 Nijmegen
Netherlands 1160.19.31006 Boehringer Ingelheim Investigational Site Sittard
Netherlands 1160.19.31004 Boehringer Ingelheim Investigational Site Zwolle
Norway 1160.19.47003 Helse Sunnmøre HF, Ålesund sykehus Ålesund
Norway 1160.19.47004 Martina Hansens Hospital Bærum Postterminal
Norway 1160.19.47008 Martina Hansens Hospital Bærum Postterminal
Norway 1160.19.47001 Nordlandssykehuset HF, Bodø Bodø
Norway 1160.19.47007 Sykehuset Innlandet HF, Avd. Elverum Elverum
Norway 1160.19.47005 Haugesund sjukehus HF Haugesund
Norway 1160.19.47002 Sykehuset Telemark HF, Avd. Skien Skien
South Africa 1160.19.27001 Dept. of Haematology Johannesburg
South Africa 1160.19.27002 Suite 203 Johannesburg
Sweden 1160.19.46002 Kirurgavdelningen Falköping
Sweden 1160.19.46001 Göteborg
Sweden 1160.19.46004 Ortopediska kliniken, Länssjukhuset, Halmstad Halmstad
Sweden 1160.19.46003 Ortopediska kliniken, Länssjukhuset i Kalmar Kalmar
Sweden 1160.19.46007 Kungälvs sjukhus Kungälvs
Sweden 1160.19.46005 Kirurg Ortopediska kliniken, Sjukhuset i Lidköping Lidköping
Sweden 1160.19.46008 Ortopediska Institutionen Linköping
Sweden 1160.19.46009 Sahlgrenska Universitetssjukhuset, Mölndal Mölndal
Sweden 1160.19.46006 Boehringer Ingelheim Investigational Site Varberg

Sponsors (1)

Lead Sponsor Collaborator
Boehringer Ingelheim

Countries where clinical trial is conducted

Austria,  Belgium,  Czech Republic,  Denmark,  Finland,  France,  Hungary,  Italy,  Netherlands,  Norway,  South Africa,  Sweden, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants With Venous Thromboembolic (VTE) Events Deep vein thrombosis (DVT) (proximal and distal) as detected by routine bilateral venography on day 8 +/- 2, plus symptomatic DVT confirmed by venography during the treatment period or PE confirmed by objective testing Treatment period (up to day 8+/-2 days visit) No
Primary Number of Participants With Major Bleeding Events (MBE) From approximately 14 days prior to surgery to 4-6 weeks post surgery Yes
Secondary Number of Participants With VTE Events and All Cause Mortality Deep venous thrombosis (DVT) (proximal and distal) as detected by routine bilateral venography on day 8 +/- 2, plus symptomatic DVT confirmed by venography during the treatment period or Pulmonary Embolism (PE) confirmed by objective testing and all deaths. Treatment period (up to day 8+/-2 days visit) No
Secondary Number of Participants With Proximal DVT, PE (Pulmonary Embolism) and VTE Related Mortality Deep venous thrombosis (DVT) (proximal) as detected by routine bilateral venography on day 8 +/- 2, plus symptomatic proximal DVT confirmed by venography during the treatment period or PE confirmed by objective testing plus VTE related mortality Treatment period (up to day 10) No
Secondary Number of Participants With Proximal DVT Deep venous thrombosis (DVT) (proximal) as detected by routine bilateral venography on day 8 +/- 2, plus symptomatic proximal DVT confirmed by venography during the treatment period Treatment period (up to day 8+/-2 days visit) No
Secondary Volume of Blood Loss Volume of blood loss was to be analysed using an analysis of variance (ANOVA), which included treatment and centre. Day 1 (Day of surgery) No
Secondary Rate of Transfusions Due to Bleedings Percentage of patients requiring transfusions due to bleeding .Rate of need of transfusion were to be analysed using a logistic regression with treatment and centre. Day 1 (Day of surgery) No
Secondary Number of Participants With Clinically Significant, Minor or Any Bleeding Events Number of participants with Clinically Significant, minor or any bleeding events. Clinically significant bleeding events are defined as
Spontaneous skin haematoma larger than >25 cm²
Wound haematoma >100 cm²
Spontaneous nose bleed >5 minutes
Macroscopic haematurea, either spontaneous or lasting more than 24 hours if associated with an intervention
Spontaneous rectal bleeding (more than spot on toilet paper)
Gingival bleeding >5 minutes
Any other bleeding event considered as clinically significant by the investigator All other bleeding events that did not fulfil the criteria of MBE or clinically significant bleeding event were classified as minor bleeding events.
Treatment period (up to day 8+/-2 days visit) No
Secondary Laboratory Analyses Number of patients with possible clinically significant abnormalities, i.e. with values out of normal range.
Normal ranges are defined as:
Haematocrit [%]: (0.35-0.45) for women and (0.39-0.51) for men Haemoglobin [g/dL]: (11.6-15.4) for women and (13.2-17.3) for men White Blood Cell count [10^9/L]: (4-10.3) for women and (3.9-10.3) for men Platelets [10^9/L]: (145-420) for women and men Sodium [mmol/L]: (135-146) for women and men Potassium [mmol/L]: (3.5-5) for women and men Aspartate aminotransferase (AST) [U/L]: (11-37) for women and (11-39) for men Alanine aminotransferase (ALT) [U/L]: (8-43) for women and (8-45) for men Alkaline Phosphatase [U/L]: (36-118) for women and (35-123) for men Creatinine [mg/dL]: (0.57-1.06)for women and (0.72-1.3) for men Bilirubin, total [mg/dL]: (0.22-1.28) for women and men Uric acid [mg/dL]: (2.4-6.47) for women and men
Screening to end of treatment No
Secondary Plasma Concentration (Cmax) of Dabigatran Maximum plasma concentration of Dabigatran (at steady-state) and Pre-dose plasma concentrations at steady state.
Cmax represents the maximum concentration of Dabigatran in plasma. Cmax,ss represents the maximum concentration of Dabigatran in plasma at steady state.
Cpre,ss represents pre-dose concentration of Dabigatran in plasma at steady state
Day 1 to end of treatment No
Secondary Area Under the Plasma Concentration-time Curve During a Dosing Interval Area under the plasma concentration-time curve during a dosing interval (at steady-state). The AUC0-12h (for b.i.d. treatment regimens) and AUC0-24h (300 mg q.d.) after the first dose on day of surgery calculated by extrapolation using the elimination rate constant, reported only if the extrapolated fraction of AUC was less than 30 % of the total AUC. up to day 8+/-2 days visit No
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