Clinical Trial Details
— Status: Recruiting
Administrative data
| NCT number |
NCT05370820 |
| Other study ID # |
041737 |
| Secondary ID |
|
| Status |
Recruiting |
| Phase |
Phase 2
|
| First received |
|
| Last updated |
|
| Start date |
December 28, 2022 |
| Est. completion date |
June 2024 |
Study information
| Verified date |
April 2024 |
| Source |
George Washington University |
| Contact |
Jaclyn Phillips, MD |
| Phone |
2027412500 |
| Email |
japhillips[@]mfa.gwu.edu |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
In part 1 of the study, the investigators conducted a prospective, open-label, dose finding
pharmacokinetic (PK) study in 43 pregnant 3rd trimester women scheduled for non-emergent
cesarean section.
The investigators administered three doses of the drug (5 mg/kg, 10 mg/kg and 15 mg/kg) in an
escalating fashion by cohort with the lowest dose first. The drug was administered
intravenously at the time of umbilical cord clamping for a non-emergent cesarean section. A
maximum of 1 gram was administered. TXA serum levels at several time points after delivery
were assayed to see if they reach the target plasma concentration of 10 microg/mL. A PK model
was constructed for determining the optimal TXA dose administered at parturition.
In part 2 of the study, the investigators aim to compare PKPD endpoints using prophylactic
TXA via IV and IM routes administered pre-cord clamp. The investigators will administer 1000
mg TXA within 10 minutes of skin incision via intravenous infusion (up to n=15), intravenous
bolus < 2 minutes (up to n=15) and intramuscular injection (up to n=15). The investigators
will target women undergoing scheduled cesarean delivery greater than 34 weeks gestation,
women undergoing vaginal delivery > 34 weeks of gestation and morbidly obese women (BMI>50)
undergoing either a vaginal or cesarean delivery. The investigators will use advanced
modeling techniques to determine time to achieve PKPD targets and duration remaining at those
targets. The goal will be to determine how the optimal dose may vary if route of
administration is modified. The investigators plan to enroll 45 patients in addition to the
43 that were enrolled during part 1. Our goal is to 30 participants, but the investigators
will enroll 45 to account for lost to follow-up. The investigatorsalso aim to enroll 30
patients undergoing vaginal delivery and 30 morbidly obese women (BMI > 50) undergoing either
a vaginal or cesarean delivery but the investigators will enroll 45 patients for each of
these groups to account for loss to follow up. In addition, the investigators will enroll 30
pregnant patients receiving no medication acting as the control group, but the investigators
will enroll 45 to account for loss to follow up.
Description:
The study will enroll 45 additional third trimester pregnant women scheduled for nonemergent
cesarean sections who are at high risk for hemorrhage. The investigators plan to enroll 30,
but to account for lost to follow-up, the investigators will enroll 45. The investigatorswill
also enroll 30 pregnant patients > 34 weeks of gestation undergoing vaginal delivery, and 30
morbidly obese (BMI > 50) pregnant patients undergoing either vaginal or cesarean delivery.
However, the investigators will enroll 45 patients in each of these two groups to account for
loss to follow up. The investigators will also enroll 45 patients as a control group that
will not receive TXA. The total number of enrolled patients will thus be 223.
A total of 1 gram of TXA will be administered to patients prior to fetal delivery via three
different routes of administration: IV infusion, IV push, and IM injection. The subjects in
each group will be divided into three subgroups:
Group 1: Up to 15 subjects, TXA dose: 1 gram, Route: IV infusion over 10 minutes Group 2: Up
to 15 subjects, TXA dose: 1 gram, Route: IV Push for <2 minutes Group 3: Up to 15 subjects,
TXA dose: 1 gram, Route: IM Injection
Plasma sampling: Timing of samples will be relative to the end of drug administration (t = 0)
and include: Pre-drug administration, 5-10 minutes, 30-60 minutes, 60-90 minutes, 1.5-3
hours, 3-4 hours, 4-5 hours, 7-8 hours, and 10-18 hours. Each volume of blood draw will be
approximately 7-9 mL. Actual times of plasma sampling will be documented. A second IV will be
required for participating in the study. Citrated plasma samples will be centrifuged and
supernatant will be stored at -70 degree Celsius. Breast milk sampling of no more than 2 mL
per time point will occur at time points coinciding with maternal feedings.
Procedure:
1. Subject recruitment will take place in the GW MFA routine prenatal clinic among other
prenatal patients. In addition, inpatient charting will utilize a screening tool
developed for research projects at GW called 'Power Trials' to help screen eligibIe
subjects admitted to L&D. Interested subjects will be consented by either a physican
investigator or research coordinator as described below. The subjects serum creatinine
levels will be obtained if indicated at the time of delivery.
2. TXA administration will be given in cohort fashion as outlined in the chart above with
up to15 subjects enrolled being placed in Group 1 (1g TXA via IV infusion over 10 mins),
up to 15 subjects enrolled will be placed in Group 2 (1g TXA via IV push for < 2 mins),
and up to 15 subjects enrolled will be placed in Group 3 (1g TXA via IM injection). Each
patient will be assigned to either one of three cohorts. The participants are not
randomly assigned to each cohort since the focus of this study is not efficacy, and
randomization in pharmacodynamic-pharmacokinetic (PKPD) studies such as this one is not
typically done.
