Venous Thrombosis Clinical Trial
Official title:
The Effects of Oral Contraceptive Pills vs Hormonal Patch on Coagulation Parameters
This study was a randomized, investigator-blinded, cross-over, clinic trial using twenty-four healthy women aged 18-35. All women received two months of the birth control patch or birth control pill, two months without any drug, then two months of the alternative drug. The birth control patch contained 0.75 milligrams ethinyl estradiol and 6 milligrams norelgestromin. The birth control pill contained 35 micrograms ethinyl estradiol and 250 micrograms norgestimate. Blood samples were taken before and after each treatment and were analyzed for the following lab values: D-dimer, von Willebrand factor, factor VIII, total and free protein S, antithrombin, fibrinogen, C-reactive protein and normalized activated protein C sensitivity ratio (nAPCsr). Two thrombin generation-based assays were used: the α2macroglobulin-thrombin endpoint method (α2M-IIa) and calibrated automated thrombinography (CAT).
Twenty-four non-pregnant women 18-35 years of age, who had not been on hormonal
contraception for at least 2 months prior to the study or who were least 3 months postpartum
and non-lactating, were enrolled in this study between October 2003 and February 2005. The
study protocol was approved by the University of Vermont Institutional Review Board, and all
participants gave written informed consent. Exclusion criteria for participation were
personal or family history of venous thromboembolism or coagulation disorders, pregnancy,
uncontrolled hypertension, cardiovascular disease, complicated migraine headaches, breast
cancer, diabetes, abnormal uterine bleeding, liver disease, or desire for pregnancy in less
than 6 months.
This study was a randomized investigator-blind, cross-over clinical trial. The daily oral
contraceptive contained 35 micrograms ethinyl estradiol and 250 micrograms norgestimate
(Ortho Cylen®). The weekly transdermal hormonal contraceptive contained 0.75 milligrams
ethinyl estradiol and 6.0 milligrams norelgestromin (Ortho Evra®). Norelgestromin is the
active progestin metabolite of orally administered norgestimate. For the oral form the
average steady state plasma concentration (Css) of ethinyl estradiol was 49.3
picograms/milliliter and of norelgestromin 0.73 nanograms/milliliter and for the transdermal
form these concentrations were 80.0 picograms/milliliter and 0.888 nanograms/milliliter,
respectively at the end of the second month of use.17 The average weekly exposure,
calculated as area under the curve (AUC0-168pg.h/mL) for ethinyl estradiol was 55% higher
with transdermal than with the oral contraceptive. The maximum ethinyl estradiol and
norelgestromin levels (Cmax) were 133 pg/ml and 2.16 ng/ml for the oral form and 97.4 pg/ml
and 1.12 ng/ml for the transdermal form.17 The application location of the patch does not
alter the Css or Cmax.18 Medications were supplied to the patients by a research nurse and
the completed packets were returned to document compliance. The contraceptives and the
funding for the study were supplied by research grants from the University of Vermont
Department of Obstetrics and Gynecology.
Prior to enrollment, participants underwent a physical examination including gynecologic
examination. Women on hormonal contraceptives at recruitment were given barrier
contraceptives for two months prior to starting the study. Participants were assigned a
random identification number which indicated the sequence in which transdermal or oral
contraceptives would be given. The daily oral contraceptive or weekly transdermal
contraceptive was given with the typical dosing of three weeks active treatment followed by
one week without hormone use. Following the first two months of hormonal contraceptive, each
participated returned to barrier contraceptive for a two month washout period, then received
two months of the alternative hormonal contraceptive. The investigators were blind to the
order of contraceptive assigned for each participant.
There were four phlebotomies performed for each subject. Blood was drawn on menstrual cycle
day 18 to 21 prior to the study, within 4 days of either the last pill or removal of the
last patch, and on cycle day 18 to 21 in the second month of the washout period. Blood was
collected using standardized methods with minimal stasis into vacutainer tubes, immediately
placed on ice and centrifuged at 4oC. Plasma and serum was stored at -70oC until completion
of the study.
Laboratory assays were performed in batch with each participant's serial samples analyzed in
the same run. D-dimer, von Willebrand factor and antithrombin were measured using
immuno-turbidometric assays on the STA-R analyzer (Liatest D-Di, Liatest vWF, Liatest ATIII,
Diagnostica Stago, Parsippany, NJ) with coefficients of variation (CVs) of 3.0%, 3.85%, and
4.0-8.0% respectively. Factor VIII was determined by measuring the clotting time of the
sample in factor VIII deficient plasma (STA-Deficient VIII; Diagnostica Stago, Parsippany,
NJ) with a CV of 3.5%. Free and total protein S were measured by immunoassay (Asserachrom
Free and Total Protein S, Diagnostica Stago, Parsippany, NJ) with CVs of 14.0% and 4.0%
respectively. Fibrinogen and C-reactive protein were measured by immunonephelometry using
the BNII instrument (N Antiserum to Human Fibrinogen, N High Sensitivity CRP, Dade-Behring,
Deerfield, IL) with CVs of 2.3-4% and 2.6% respectively.
The normalized activated protein C sensitivity ratio (nAPCsr) was measured using two
thrombin generation assays. In the first assay, coagulation was triggered in defibrinated
plasma with tissue factor in the presence and absence of activated protein C and the amount
of thrombin captured in complex with a2-macroglobulin over 30 minutes was taken as a measure
for thrombin generation and used to calculate the nAPCsr (nAPCsr α2M-IIa).14 In the second
assay, the nAPCsr (nAPCsr CAT) was determined by measuring thrombin generation in the
presence and absence of activated protein C in full plasma in real-time with a fluorogenic
thrombin substrate using calibrated automated thrombinography (CAT).19 The CV's of the
nAPCsr α2M-IIa and nAPCsr CAT were 3.5% and 7%, respectively.
Repeated measures analyses of variance corresponding to a cross-over design incorporating
both baseline and washout periods were used to determine the significance associated with
differences between the hormonal contraceptive treatments for each of the biomarkers tested.
Pre-planned contrasts were used to test for differences between the pre-treatment periods
corresponding to oral and transdermal active treatments. Contrasts were also used to test
for changes from pre-treatment to active treatment within each treatment and to determine
whether these changes were parallel across the two active treatments. Biomarkers that had
non-normal distributions based on residual plots were log transformed prior to analysis.
Based on the analyses of variance results, there was no evidence of any significant order
effects for any of the biomarkers. Analyses were performed using SAS Version 8.2 (SAS
Institute, Cary, NC). Statistical significance was determined based on a=.05
;
Allocation: Randomized, Intervention Model: Crossover Assignment, Masking: Single Blind (Investigator), Primary Purpose: Treatment
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