Effect of BIA 6-512 at Steady-state on the Levodopa Pharmacokinetics

Sponsor

Bial - Portela C S.A. (Industry)

Overall Status

Completed

CT.gov ID

NCT03094156

Collaborator

(none)

Enrollment

Location

Arms

2.5

Actual Duration (Months)

15.6

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

The purpose of the study was to To investigate whether the administration of BIA 6-512 (25 mg, 50 mg, 75 mg and 100 mg) at steady-state affects the pharmacokinetics of levodopa when administered in combination with a single-dose of immediate release levodopa/benserazide 200/50 mg or with a single-dose of immediate release levodopa/benserazide 200/50 mg plus a single-dose of entacapone 200 mg.

Condition or Disease	Intervention/Treatment	Phase
Parkinson Disease	Drug: Placebo Drug: BIA 6-512 Drug: Madopar® 250 Drug: Comtan®	Phase 1

Detailed Description

Single centre, double-blind, randomised, placebo-controlled, rising multiple-dose study in four sequential groups of healthy male and female subjects. Eligible subjects were admitted to the Human Pharmacology Unit (UFHBIAL - Portela & Cª, SA) on the day prior to receiving the first study medication. Starting in the morning of Day 1 (first dose), subjects received BIA 6-512/Placebo thrice-daily until the morning of Day 5 (last dose). Concomitantly with the morning dose of BIA 6-512/Placebo, on Day 4 a levodopa/benserazide 200/50 mg (Madopar® 250) single-dose was administered. On Day 5, a Madopar® 250 single-dose and a entacapone 200 mg (Comtan®) single-dose were administered concomitantly with the morning dose of BIA 6-512/Placebo. In the morning of Day 4 and Day 5, products were administered in fasting of at least 8 hours and subjects remained fasted until 2 h post-dose. Subjects were resident in the UFH from admission (Day 0) until at least 24 h post last dose (Day 6); then, they were discharged and returned for the follow-up visit.

Study Design

Study Type:

Interventional

Actual Enrollment :

39 participants

Allocation:

Randomized

Intervention Model:

Sequential Assignment

Masking:

Double (Participant, Investigator)

Primary Purpose:

Treatment

Official Title:

A Double-blind, Randomised, Placebo-controlled, Rising Multiple Dose Study in Healthy Volunteers to Investigate the Effect of BIA 6-512 at Steady-state on the Levodopa Pharmacokinetics When Administered in Combination With a Single-dose of Levodopa/Benserazide 200/50 mg or With a Single-dose of Levodopa/Benserazide 200/50 mg Plus a Single-dose of Entacapone 200 mg

Actual Study Start Date :

Apr 26, 2006

Actual Primary Completion Date :

Jul 11, 2006

Actual Study Completion Date :

Jul 11, 2006

Arms and Interventions

Arm	Intervention/Treatment
Experimental: Placebo Subjects were administered with those investigational products at approximately 8-h intervals, starting in the morning (approximately at 8h00) of Day 1 and finishing in the morning of Day 5 (last dose). On Day 4, concomitantly with the Placebo morning dose, one tablet of Madopar® 250 was administered. On Day 5, concomitantly with the Placebo morning dose, one tablet of Madopar® 250 and one tablet of Comtan® were administered.	Drug: Placebo 1 capsule of placebo [to be taken orally, with 240 mL of potable water] Drug: Madopar® 250 Levodopa/benserazide immediate release tablets 200mg/50mg [to be taken orally, with 240 mL of potable water] Drug: Comtan® Entacapone 200 mg tablets [to be taken orally, with 240 mL of potable water]
Experimental: BIA 6-512 25 mg Subjects were administered with those investigational products at approximately 8-h intervals, starting in the morning (approximately at 8h00) of Day 1 and finishing in the morning of Day 5 (last dose). On Day 4, concomitantly with the BIA 6-512 25 mg morning dose, one tablet of Madopar® 250 was administered. On Day 5, concomitantly with the BIA 6-512 25 mg morning dose, one tablet of Madopar® 250 and one tablet of Comtan® were administered.	Drug: BIA 6-512 1 capsule of BIA 6-512 25mg or 1 capsule of BIA 6-512 50 mg or 1 capsule of BIA 6-512 75 mg or 1 capsule of BIA 6-512 100 mg [to be taken orally, with 240 mL of potable water] Other Names: Trans-resveratrol Drug: Madopar® 250 Levodopa/benserazide immediate release tablets 200mg/50mg [to be taken orally, with 240 mL of potable water] Drug: Comtan® Entacapone 200 mg tablets [to be taken orally, with 240 mL of potable water]
Experimental: BIA 6-512 50 mg Subjects were administered with those investigational products at approximately 8-h intervals, starting in the morning (approximately at 8h00) of Day 1 and finishing in the morning of Day 5 (last dose). On Day 4, concomitantly with the BIA 6-512 50 mg morning dose, one tablet of Madopar® 250 was administered. On Day 5, concomitantly with the BIA 6-512 50 mg morning dose, one tablet of Madopar® 250 and one tablet of Comtan® were administered.	Drug: BIA 6-512 1 capsule of BIA 6-512 25mg or 1 capsule of BIA 6-512 50 mg or 1 capsule of BIA 6-512 75 mg or 1 capsule of BIA 6-512 100 mg [to be taken orally, with 240 mL of potable water] Other Names: Trans-resveratrol Drug: Madopar® 250 Levodopa/benserazide immediate release tablets 200mg/50mg [to be taken orally, with 240 mL of potable water] Drug: Comtan® Entacapone 200 mg tablets [to be taken orally, with 240 mL of potable water]
Experimental: BIA 6-512 75 mg Subjects were administered with those investigational products at approximately 8-h intervals, starting in the morning (approximately at 8h00) of Day 1 and finishing in the morning of Day 5 (last dose). On Day 4, concomitantly with the BIA 6-512 75 mg morning dose, one tablet of Madopar® 250 was administered. On Day 5, concomitantly with the BIA 6-512 75 mg morning dose, one tablet of Madopar® 250 and one tablet of Comtan® were administered.	Drug: BIA 6-512 1 capsule of BIA 6-512 25mg or 1 capsule of BIA 6-512 50 mg or 1 capsule of BIA 6-512 75 mg or 1 capsule of BIA 6-512 100 mg [to be taken orally, with 240 mL of potable water] Other Names: Trans-resveratrol Drug: Madopar® 250 Levodopa/benserazide immediate release tablets 200mg/50mg [to be taken orally, with 240 mL of potable water] Drug: Comtan® Entacapone 200 mg tablets [to be taken orally, with 240 mL of potable water]
Experimental: BIA 6-512 100 mg Subjects were administered with those investigational products at approximately 8-h intervals, starting in the morning (approximately at 8h00) of Day 1 and finishing in the morning of Day 5 (last dose). On Day 4, concomitantly with the BIA 6-512 100 mg morning dose, one tablet of Madopar® 250 was administered. On Day 5, concomitantly with the BIA 6-512 100 mg morning dose, one tablet of Madopar® 250 and one tablet of Comtan® were administered.	Drug: BIA 6-512 1 capsule of BIA 6-512 25mg or 1 capsule of BIA 6-512 50 mg or 1 capsule of BIA 6-512 75 mg or 1 capsule of BIA 6-512 100 mg [to be taken orally, with 240 mL of potable water] Other Names: Trans-resveratrol Drug: Madopar® 250 Levodopa/benserazide immediate release tablets 200mg/50mg [to be taken orally, with 240 mL of potable water] Drug: Comtan® Entacapone 200 mg tablets [to be taken orally, with 240 mL of potable water]

Outcome Measures

Primary Outcome Measures

Day 4 - Maximum observed plasma drug concentration (Cmax) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8 and 16 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 4
Day 4 - Time of occurrence of Cmax (tmax) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8 and 16 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 4
Day 4 - Area under the plasma concentration-time curve (AUC) from time zero to the last sampling time at which concentrations were at or above the limit of quantification (AUC0-t) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8 and 16 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 4
Day 4 - AUC from time zero to 8 h post-dose (AUC0-τ) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8 and 16 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 4
Day 4 - Apparent terminal elimination half-life, calculated from ln 2/λz (t1/2) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8 and 16 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 4
Day 4 - Area under the plasma concentration versus time curve from time zero to infinity (AUC0-∞) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8 and 16 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 4
Day 5 - Maximum observed plasma drug concentration (Cmax) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8, 16 and 24 hours post-dose]
Day 5 - Time of occurrence of Cmax (tmax) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8, 16 and 24 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 5
Day 5 - Area under the plasma concentration-time curve (AUC) from time zero to the last sampling time at which concentrations were at or above the limit of quantification (AUC0-t) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8, 16 and 24 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 5
Day 5 - AUC from time zero to 8 h post-dose (AUC0-τ) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8, 16 and 24 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 5
Day 5 - Apparent terminal elimination half-life, calculated from ln 2/λz (t1/2) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8, 16 and 24 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 5
Day 5 - Area under the plasma concentration versus time curve from time zero to infinity (AUC0-∞) [pre-dose, ¼, ½, ¾, 1, 1½, 2, 3, 4, 6, 8, 16 and 24 hours post-dose]
BIA 6-512, levodopa, 3-OMD and entacapone pharmacokinetic parameters on day 5

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years to 45 Years

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Yes

Inclusion Criteria:

Male or female subjects aged between 18 and 45 years, inclusive.
Subjects of body mass index (BMI) between 19 and 30 kg/m2, inclusive.
Subjects who were healthy as determined by pre-study medical history, physical examination, vital signs, complete neurological examination and 12-lead ECG.
Subjects who had negative tests for HBsAg, anti-HCVAb and HIV-1 and HIV-2 Ab at screening
Subjects who had clinical laboratory test results clinically acceptable at screening and admission.
Subjects who had a negative screen for alcohol and drugs of abuse at screening and admission.
Subjects who were non-smokers or who smoked ≤ 10 cigarettes or equivalent per day.
Subjects who were able and willing to gave written informed consent.
(If female) She was not of childbearing potential by reason of surgery or, if of childbearing potential, she used one of the following methods of contraception: double barrier, intrauterine device or abstinence.
(If female) She had a negative urine pregnancy test at screening and admission.

Exclusion Criteria:

Subjects who had a clinically relevant history or presence of respiratory, gastrointestinal, renal, hepatic, haematological, lymphatic, neurological, cardiovascular, psychiatric, musculoskeletal, genitourinary, immunological, dermatological, endocrine, connective tissue diseases or disorders.
Subjects who had a clinically relevant surgical history.
Subjects who had a clinically relevant family history.
Subjects who had a history of relevant atopy.
Subjects who had a history of relevant drug hypersensitivity.
Subjects who had a history of alcoholism or drug abuse.
Subjects who consumed more than 14 units of alcohol a week.
Subjects who had a significant infection or known inflammatory process on screening or admission.
Subjects who had acute gastrointestinal symptoms (e.g., nausea, vomiting, diarrhoea, heartburn) at the time of screening or admission.
Subjects who had used medicines within 2 weeks of admission that may affect the safety or other study assessments, in the investigator's opinion.
Subjects who had previously participated in a clinical trial with BIA 6-512.
Subjects who had used any investigational drug or participated in any clinical trial within 6 months prior to screening.
Subjects who had participated in more than 2 clinical trials within the 12 months prior to screening.
Subjects who had donated or received any blood or blood products within the 3 months prior to screening.
Subjects who were vegetarians, vegans or have medical dietary restrictions.
Subjects who cannot communicate reliably with the investigator.
Subjects who were unlikely to co-operate with the requirements of the study.
Subjects who were unwilling or unable to give written informed consent.
(If female) She was pregnant or breast-feeding.
(If female) She was of childbearing potential and she did not use an effective contraceptive method (double-barrier, intra-uterine device or abstinence) or she used oral contraceptives.

Contacts and Locations

Locations

	Site	City	State	Country	Postal Code
1	Human Pharmacology Unit (UFH) - BIAL - Portela & Cª, SA	S. Mamede do Coronado		Portugal	4745-457

Sponsors and Collaborators

Bial - Portela C S.A.

Investigators

None specified.

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

Bial - Portela C S.A.

ClinicalTrials.gov Identifier:

NCT03094156

Other Study ID Numbers:

BIA-6512-106

First Posted:

Mar 29, 2017

Last Update Posted:

Mar 30, 2017

Last Verified:

Mar 1, 2017

Individual Participant Data (IPD) Sharing Statement:

Undecided

Plan to Share IPD:

Undecided

Studies a U.S. FDA-regulated Drug Product:

Studies a U.S. FDA-regulated Device Product:

Additional relevant MeSH terms:

Parkinson Disease

Resveratrol

Benserazide, levodopa drug combination

Study Results

No Results Posted as of Mar 30, 2017