Evaluate The Pharmacokinetics and Safety Of Oxycodone Oral Solution In Pediatric and Adolescent Subjects
Status: | Recruiting |
---|---|
Conditions: | Chronic Pain |
Therapuetic Areas: | Musculoskeletal |
Healthy: | No |
Age Range: | Any - 17 |
Updated: | 11/30/2018 |
Start Date: | October 2013 |
End Date: | January 2020 |
Contact: | Thomas Hochadel, Pharm.D |
Email: | thochadel@cogres.com |
Phone: | 727-897-9000 |
A Phase IV Study to Evaluate the Pharmacokinetics and Safety of Oxycodone Oral Solution in Pediatric and Adolescent Subjects
The objective of this study is to characterize the pharmacokinetics and to evaluate the
safety of single and multiple doses of Oxycodone Oral Solution in pediatric and adolescent
subjects for postoperative pain.
safety of single and multiple doses of Oxycodone Oral Solution in pediatric and adolescent
subjects for postoperative pain.
This is a Phase IV study to characterize the pharmacokinetics and to evaluate the safety of
Oxycodone Oral Solution administered to pediatric and adolescent subjects for postoperative
pain. It is an open label, multicenter study conducted at up to 10 sites. Subjects will be
enrolled preoperatively up to 14 days before surgery with the expectation that they will
require intravenous (IV) access after the surgery for at least 24 hours and postoperative
analgesia with an opiate level medication. After dosing with Oxycodone Oral Solution (0.1
mg/kg for children ages 2 to 6, 0.08 mg/kg for ages 7 to 12, 0.07 mg/kg for ages 13 to 17,
and a dose to be determined based on pharmacokinetic (PK) modeling from the interim analyses
for subjects under age 2), subjects will be carefully monitored for safety. A total of 110
pediatric and adolescent male or female subjects will be enrolled, including a minimum of 20
subjects under age 2 (5 subjects ages 0 to <2 months, 5 subjects ages 2 to <6 months, and 10
subjects ages 6 months to <2 years), 30 ages 2 to 6 years, 30 ages 7 to 12 years and 30 ages
13 to <17 years. Subjects within each age group will be evenly distributed by age and gender.
An interim analysis will be run after 10 subjects ages 2 to 6 years, 10 ages 7 to 12 years
and 10 ages 13 to <17 years have completed the study. The interim analysis will include PK,
pulse oximetry readings, vital sign measurements, adverse events (AEs) and concomitant
medications. The dose of Oxycodone Oral Solution that the subjects ages 6 months to <2 years
will receive will be based on PK modeling from the interim analysis.
An additional interim analysis will be run after at least half of the subjects aged 6 months
to <2 years have completed the study. The interim analysis will include PK, pulse oximetry
readings, vital sign measurements, AEs and concomitant medications. The dose of Oxycodone
Oral Solution that the subjects ages 0 to <2 months and 2 months to <6 months will receive
will be based on PK modeling from the interim analysis.
The study will consist of a Screening period within 14 days of surgery; a predose check-in
(Day −1); a treatment period after surgery (Day 1, Time Zero); and an End of Study
assessment. The total duration of the study, excluding Screening, will be approximately 1
full day.
Eligible subjects who provide assent (7 to <17 years old) and whose parent(s) or legal
guardian(s) provide consent as required will have study assessments performed at Screening.
Following surgery, subjects will receive standard care, including parenteral analgesia with a
nonoxycodone, nonoxymorphone medication that will not interfere with the measurement or
metabolism of oxycodone. At this time (during Day −1), they will have a predose check-in to
have eligibility confirmed.
After subjects ages 2 to <17 have been postoperatively cleared to transition to oral pain
medication, Oxycodone Oral Solution will be administered at Time Zero of Day 1 in place of
the standard analgesic medication. The first 10 subjects in each of the 2 to 6, 7 to 12 and
13 to <17 age groups, who will be included in the first interim analysis, will only receive 1
dose of Oxycodone Oral Solution. Subjects in these age groups enrolled in the study after the
interim analysis is completed may receive additional doses every 4-6 hours as needed. If pain
control is inadequate with Oxycodone Oral Solution, the investigator may administer an IV
dose of ketorolac (0.5 mg/kg) every 6 hours or an IV dose of Morphine Sulfate (0.1 mg/kg)
every 4 hours as rescue medication for breakthrough pain after dosing. Use of other rescue
pain medication is permissible in accordance with hospital pain management guidelines or
facilities standard of care. Any rescue medications used will be provided by the study site
pharmacy.
After subjects under age 2 have been postoperatively cleared to transition to oral pain
medication, they will receive a single dose of Oxycodone Oral Solution at Time Zero of Day 1
in place of the standard analgesic medication. The dose will be determined based on PK
modeling from the interim analyses. If pain control is inadequate with Oxycodone Oral
Solution, as indicated by a score of moderate to severe (4-10) on the FLACC, the subject will
be given Fentanyl via Nurse-Controlled Analgesia (NCA). The Fentanyl will be provided by the
study site pharmacy.
Subjects will undergo an End-of-Study assessment at least 24 hours after receiving the first
dose of Oxycodone Oral Solution. At that time, if the study staff determines that it is safe
to do so, subjects will be discharged from the study.
Safety will be assessed by monitoring AEs, clinical laboratory test results, vital sign
measurements, temperature, pulse oximetry, and physical examination findings.
The Faces, Legs, Activity, Crying, Consolability Scale (FLACC) will be used to measure pain
prior to and 20, 40, 60, 90, 120, 180, and 240 minutes after the dose of Oxycodone Oral
Solution in subjects under age 2. The FLACC will also be administered prior to the subject
receiving each dose of Fentanyl.
Serial blood samples for PK analysis will be collected for the determination of plasma
concentrations of oxycodone and its metabolites (noroxycodone, oxymorphone and
noroxymorphone) prior to the first dose (within 15 minutes of dosing); 5, 15, 30, and 60
minutes after dosing; and 2, 4, 6, 8, 12, and 24 hours after dosing. For subjects under age
2, serial blood samples for PK analysis will be collected prior to the first dose (within 15
minutes of dosing); 15, 30, and 60 minutes after dosing; and 2, 6, 12, and 24 hours after
dosing.
Oxycodone Oral Solution administered to pediatric and adolescent subjects for postoperative
pain. It is an open label, multicenter study conducted at up to 10 sites. Subjects will be
enrolled preoperatively up to 14 days before surgery with the expectation that they will
require intravenous (IV) access after the surgery for at least 24 hours and postoperative
analgesia with an opiate level medication. After dosing with Oxycodone Oral Solution (0.1
mg/kg for children ages 2 to 6, 0.08 mg/kg for ages 7 to 12, 0.07 mg/kg for ages 13 to 17,
and a dose to be determined based on pharmacokinetic (PK) modeling from the interim analyses
for subjects under age 2), subjects will be carefully monitored for safety. A total of 110
pediatric and adolescent male or female subjects will be enrolled, including a minimum of 20
subjects under age 2 (5 subjects ages 0 to <2 months, 5 subjects ages 2 to <6 months, and 10
subjects ages 6 months to <2 years), 30 ages 2 to 6 years, 30 ages 7 to 12 years and 30 ages
13 to <17 years. Subjects within each age group will be evenly distributed by age and gender.
An interim analysis will be run after 10 subjects ages 2 to 6 years, 10 ages 7 to 12 years
and 10 ages 13 to <17 years have completed the study. The interim analysis will include PK,
pulse oximetry readings, vital sign measurements, adverse events (AEs) and concomitant
medications. The dose of Oxycodone Oral Solution that the subjects ages 6 months to <2 years
will receive will be based on PK modeling from the interim analysis.
An additional interim analysis will be run after at least half of the subjects aged 6 months
to <2 years have completed the study. The interim analysis will include PK, pulse oximetry
readings, vital sign measurements, AEs and concomitant medications. The dose of Oxycodone
Oral Solution that the subjects ages 0 to <2 months and 2 months to <6 months will receive
will be based on PK modeling from the interim analysis.
The study will consist of a Screening period within 14 days of surgery; a predose check-in
(Day −1); a treatment period after surgery (Day 1, Time Zero); and an End of Study
assessment. The total duration of the study, excluding Screening, will be approximately 1
full day.
Eligible subjects who provide assent (7 to <17 years old) and whose parent(s) or legal
guardian(s) provide consent as required will have study assessments performed at Screening.
Following surgery, subjects will receive standard care, including parenteral analgesia with a
nonoxycodone, nonoxymorphone medication that will not interfere with the measurement or
metabolism of oxycodone. At this time (during Day −1), they will have a predose check-in to
have eligibility confirmed.
After subjects ages 2 to <17 have been postoperatively cleared to transition to oral pain
medication, Oxycodone Oral Solution will be administered at Time Zero of Day 1 in place of
the standard analgesic medication. The first 10 subjects in each of the 2 to 6, 7 to 12 and
13 to <17 age groups, who will be included in the first interim analysis, will only receive 1
dose of Oxycodone Oral Solution. Subjects in these age groups enrolled in the study after the
interim analysis is completed may receive additional doses every 4-6 hours as needed. If pain
control is inadequate with Oxycodone Oral Solution, the investigator may administer an IV
dose of ketorolac (0.5 mg/kg) every 6 hours or an IV dose of Morphine Sulfate (0.1 mg/kg)
every 4 hours as rescue medication for breakthrough pain after dosing. Use of other rescue
pain medication is permissible in accordance with hospital pain management guidelines or
facilities standard of care. Any rescue medications used will be provided by the study site
pharmacy.
After subjects under age 2 have been postoperatively cleared to transition to oral pain
medication, they will receive a single dose of Oxycodone Oral Solution at Time Zero of Day 1
in place of the standard analgesic medication. The dose will be determined based on PK
modeling from the interim analyses. If pain control is inadequate with Oxycodone Oral
Solution, as indicated by a score of moderate to severe (4-10) on the FLACC, the subject will
be given Fentanyl via Nurse-Controlled Analgesia (NCA). The Fentanyl will be provided by the
study site pharmacy.
Subjects will undergo an End-of-Study assessment at least 24 hours after receiving the first
dose of Oxycodone Oral Solution. At that time, if the study staff determines that it is safe
to do so, subjects will be discharged from the study.
Safety will be assessed by monitoring AEs, clinical laboratory test results, vital sign
measurements, temperature, pulse oximetry, and physical examination findings.
The Faces, Legs, Activity, Crying, Consolability Scale (FLACC) will be used to measure pain
prior to and 20, 40, 60, 90, 120, 180, and 240 minutes after the dose of Oxycodone Oral
Solution in subjects under age 2. The FLACC will also be administered prior to the subject
receiving each dose of Fentanyl.
Serial blood samples for PK analysis will be collected for the determination of plasma
concentrations of oxycodone and its metabolites (noroxycodone, oxymorphone and
noroxymorphone) prior to the first dose (within 15 minutes of dosing); 5, 15, 30, and 60
minutes after dosing; and 2, 4, 6, 8, 12, and 24 hours after dosing. For subjects under age
2, serial blood samples for PK analysis will be collected prior to the first dose (within 15
minutes of dosing); 15, 30, and 60 minutes after dosing; and 2, 6, 12, and 24 hours after
dosing.
Inclusion Criteria:
1. Is male or female <17 years of age at the time of dosing.
2. Subject 2 to <17 years of age, be in at least the 25% for weight according to the
Center for Disease Control pediatric growth charts and weighs at least 28 lb at the
time of dosing with study drug.
3. Is generally healthy as documented by medical history (except for the condition for
which the procedure is being performed); physical examination (including, but not
limited to, the cardiovascular, gastrointestinal, respiratory, and central nervous
systems); vital sign assessments; 12-lead electrocardiograms; clinical laboratory
assessments; and general observations. Has a negative serum pregnancy test at
Screening and predose check in for females of childbearing potential.
4. Is an outpatient for a surgical procedure and is expected to remain hospitalized for
at least 24 hours after dosing with study drug.
5. Is anticipated to have postsurgical pain requiring a parenteral analgesic regimen
using a short-acting opioid analgesic and is anticipated to be switched to an oral
opioid for at least 1 dose (according to institution standard of care).
6. Has an indwelling access catheter for blood sampling.
7. Agrees to comply with all protocol requirements. If not old enough, the legally
responsible parent(s) or legal guardian(s) must agree to comply with all protocol
requirements.
8. Has been informed of the nature of the study and informed consent and assent (as
appropriate) have been obtained from the legally responsible parent(s) or legal
guardian(s) and the subject, respectively, in accordance with institutional review
board requirements.
Exclusion Criteria:
1. Has the presence or history of a clinically significant disorder involving the
cardiovascular, respiratory, renal, gastrointestinal, immunologic, hematologic,
endocrine, or neurologic system(s) or psychiatric disease (except for the condition
for which the procedure is being performed) as determined by the clinical
investigator.
2. Has any clinical laboratory test result outside the normal range.
3. Has a positive test result for hepatitis B surface antigen, hepatitis C antibody, or
human immunodeficiency virus antibody.
4. Had a clinically significant illness, except for the condition for which the procedure
is being performed, in the 28 days before dosing with study drug as determined by the
clinical investigator.
5. Is a lactating or breastfeeding female.
6. Uses any medication known to be an inhibitor or inducer of CYP3A4 within 14 days (for
inhibitors such as the azole-antifungal agents voriconazole and ketoconazole,
macrolide antibiotics such as erythromycin, and protease inhibitors such as ritonavir)
or 28 days (for inducers such as rifampin, carbamazepine, and phenytoin) of dosing
with study drug. Use of all other prescription medications, except required pre-op
medications and birth control, is prohibited within 3 days of dosing with study drug.
Use of any over-the-counter medications (including herbal or dietary supplements and
therapeutic doses of vitamins), except for required pre-op medications, is prohibited
within 24 hours of dosing with study drug, with the exception of topical spermicide.
Use of St. John's wort is prohibited from 28 days before dosing until 14 days after
dosing. Standard daily dose multivitamins (nontherapeutic doses) may be taken until
enrollment into the study but will be restricted during the study.
7. Consumes alcohol-, caffeine-, or xanthine-containing products within 48 hours before
dosing and during periods when blood samples are collected.
8. Consumes grapefruit, grapefruit products, Seville oranges, or pomelo-containing
products within 14 days of dosing. Fruit juices, with the exception of apple and
grape, will be prohibited during the study.
9. Is a smoker or has used nicotine or nicotine-containing products within 30 days of
dosing.
10. Has a history of alcohol or drug addiction or abuse within the last year.
11. Subject 2 to <17 years of age, has a positive urine test result for drugs of abuse
(amphetamines, barbiturates, cannabinoids, cocaine metabolites, opiates,
phencyclidine, and benzodiazepines) or alcohol at Screening (not required for subjects
less than 2 years of age).
12. Donated blood within 28 days or plasma within 14 days of dosing or plans to donate
them within 4 weeks after completing the study.
13. Has a history of relevant drug allergies, food allergies, or both (i.e., allergy to
oxycodone, allergy to related drugs, or any significant food allergy that could
interfere with the study).
14. Is intolerant to direct venipuncture.
15. Received an investigational drug within 28 days of dosing.
16. Has taken oxycodone or oxymorphone within the 48 hours before anticipated dosing with
study drug.
17. Is not suitable for entry into the study in the opinion of the investigator.
We found this trial at
9
sites
Nashville, Tennessee 37232
Principal Investigator: Andrew Franklin, MD
Phone: 615-343-6223
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1200 Moursund Street
Houston, Texas 77030
Houston, Texas 77030
(713) 798-4951
Principal Investigator: Chris Glover, MD
Phone: 832-824-3388
Baylor College of Medicine Baylor College of Medicine in Houston, the only private medical school...
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3100 SW 62nd Ave
Miami, Florida 33155
Miami, Florida 33155
(305) 666-6511
Principal Investigator: Cathy Burnweit, MD
Phone: 786-624-2853
Miami Children's Hospital Welcome to Miami Children
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1 Tampa General Cir
Tampa, Florida 33606
Tampa, Florida 33606
(813) 844-7000
Principal Investigator: Charles Paidas, MD
Phone: 813-417-9950
Tampa General Hospital In a diverse city known for its rich culture and beautiful beaches,...
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CHapel Hill, North Carolina 27599
Principal Investigator: Robert Valley, MD
Phone: 919-966-5136
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Cincinnati, Ohio 45229
Principal Investigator: Senthil Sadhasivam, MD
Phone: 513-803-4552
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1935 Medical District Dr
Dallas, Texas 75235
Dallas, Texas 75235
(214) 456-7000
Principal Investigator: Peter Szmuk, MD
Children's Medical Center of Dallas Children's Medical Center is private, not-for-profit, and is the fifth-largest...
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Orange, California 92868
Principal Investigator: Jeffrey Sarmiento, MD
Phone: 714-509-8735
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