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A Clinical Study to Evaluate Z7200 (Budesonide/Formoterol) Pharmacokinetics Profile in Healthy Volunteers

NCT ID: NCT02237508

Last Updated: 2022-02-23

Study Results

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Basic Information

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Recruitment Status

COMPLETED

Clinical Phase

PHASE1

Total Enrollment

90 participants

Study Classification

INTERVENTIONAL

Study Start Date

2014-09-30

Study Completion Date

2015-02-28

Brief Summary

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The primary objective was:

\- to assess the bioequivalence of a single dose (two inhalations) of the test product compared to the reference product, with and without charcoal blockade.

The secondary objectives were:

* to assess the pharmacokinetic profile of budesonide and formoterol in plasma after a single dose (two inhalations) of the test product and the reference product, with and without charcoal blockade.
* to assess the safety and tolerability of the test product and the reference product, with and without charcoal blockade.

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Detailed Description

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This was a single center, open label, randomized, five-period crossover, single-dose study in healthy volunteers aged 18 to 45 years. A total of 90 volunteers were enrolled, with 9 subjects in each of the 10 treatment sequences.

The study consisted of 5 treatment periods, each lasting approximately 48h, separated by a washout period of a minimum of 5 days. RS01 and/or Symbicort Turbohaler device use training was provided on Day -1 and Day 1 of each treatment period. Subjects were screened for eligibility to participate in the study -28 to -2 days prior to the first treatment period, and were randomized to one of 10 treatment sequencies containing the following 5 treatment arms on Day 1 of the first treatment period:

Treatment A: Z7200 without oral activated charcoal\* Treatment B1: Symbicort 1 without oral activated charcoal\* Treatment B2: Symbicort 2 without oral activated charcoal\* Treatment C: Z7200 with oral activated charcoal\*\* Treatment D: Symbicort with oral activated charcoal\*\*

Subjects were admitted to the clinical unit at 8.00 on the morning of Day -1, and were dosed on the morning of Day 1 following an overnight fast (minimum of 8h). On Day 2, following collection of the 24-h PK blood sample, subjects were discharged.

\* Subjects who received treatments A, B1 and B2 rinsed their mouth vigorously with 50 mL water for 3 to 5 sec immediately after the second inhalation.

\*\* A charcoal blockade was used to prevent absorption from oropharyngeal and GI tract, in order to assess the pulmonary deposition of budesonide and formoterol, with periods performed without a charcoal blockade allowing the assessment of the total systemic exposure to the drug.

Conditions

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Asthma

Study Design

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Allocation Method

RANDOMIZED

Intervention Model

CROSSOVER

Primary Study Purpose

TREATMENT

Blinding Strategy

NONE

Study Groups

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A-B1-B2-C-D

Subjects were dosed on Day 1 of each treatment period with one of the following 5 treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 days followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

B1-C-A-D-B2

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

C-D-B1-B2-A

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

D-B2-C-A-B1

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

B2-A-D-B1-C

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

D-C-B2-B1-A

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

B2-D-A-C-B1

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

A-B2-B1-D-C

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

B1-A-C-B2-D

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

C-B1-D-A-B2

Subjects were dosed on Day 1 of each treatment period with one of the following five treatments according to the randomization schedule using a Williams Latin Square design:

1. Treatment A: Z7200 without oral activated charcoal
2. Treatment B1: Symbicort 1 without oral activated charcoal
3. Treatment B2: Symbicort 2 without oral activated charcoal
4. Treatment C: Z7200 with oral activated charcoal
5. Treatment D: Symbicort with oral activated charcoal

A washout period of a minimum of 5 day followed treatment periods 1 to 4.

Treatment B1 and B2 denote Symbicort without oral activated charcoal administered in two different period, designated as Symbicort 1 and Symbicort 2.

Group Type EXPERIMENTAL

Z7200 without oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Symbicort Turbohaler without oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Z7200 with oral activated charcoal

Intervention Type DRUG

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Symbicort Turbohaler with oral activated charcoal

Intervention Type DRUG

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

Interventions

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Z7200 without oral activated charcoal

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler (Treatment A).

Intervention Type DRUG

Symbicort Turbohaler without oral activated charcoal

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation (Treatments B1 and B2).

Intervention Type DRUG

Z7200 with oral activated charcoal

160 ug budesonide and 4.5 ug formoterol fumarate dihydrate, administered as two inhalations (2 x Z7200 capsules) of budesonide 80 ug/inhalation and formoterol 2.25 ug/inhalation, using an RS01 inhaler with a charcoal blockade (Treatment C).

Intervention Type DRUG

Symbicort Turbohaler with oral activated charcoal

320 ug budesonide and 9 ug formoterol fumarate dihydrate, administered as two inhalations of budesonide 160 ug/inhalation and formoterol 4.5 ug/inhalation from a Symbicort Turbohaler, with charcoal blockade (Treatment D).

Intervention Type DRUG

Other Intervention Names

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budesonide/formoterol budesonide/formoterol budesonide/formoterol with coadministration of charcoal budesonide/formoterol with coadministration of charcoal

Eligibility Criteria

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Inclusion Criteria

* Male or female 18 to 45 years of age.
* If female, is currently not pregnant/breast feeding/ or attempting to become pregnant has a negative serum pregnancy test, or is of non-childbearing potential or is of child-bearing potential, willing to commit to using a consistent and acceptable method of birth control or is of child-bearing potential and not sexually active
* Body mass index (BMI) of 18.5 to 29.9 kg/m² inclusive and a body weight ≥50 kg.

Exclusion Criteria

* FEV1 value less than 80% of the predicted value and FEV1/FVC ratio \<0.7.
* History or current evidence of a clinically significant disease or disorder capable of altering the absorption, metabolism, distribution or elimination of drugs.
* History or current evidence of a clinically significant disease including, but not limited to: cardiovascular, hepatic, renal, haematological, neuropsychological, endocrine, gastrointestinal or pulmonary.
* Presence of glaucoma, cataracts, ocular herpes simplex, malignancy, regardless of the clinical significance or current stability of the disease.
* History or presence of silent infections, including positive tests for HIV1, HIV2, Hepatitis B and Hepatitis C.
* Bacterial or viral infection of the upper respiratory tract (including the common cold and flu), sinus, or middle ear within 2 weeks of dosing.
* Lower respiratory tract infection/pneumonia within the past 3 months.
* Presence of any disease or condition or regular concomitant treatment (including vitamins and herbal products) known to interfere with the absorption, distribution, metabolism or excretion of drugs.
* Screening haemoglobin value of less than 1g/dL above the ULN (or 10g/L)
* History of recurrent vasovagal collapses.
* History of anaphylactic/anaphylactoid reactions.
* History of seizures including febrile seizures excluding childhood febrile convulsions.
* Unable to demonstrate proper inhalation techniques involved in using the delivery devices at screening.
* Exposure to any investigational drug within 90 days of the Screening Visit.
* Known or suspected hypersensitivity or idiosyncratic reaction to any steroid, any β2 agonist,or to lactose monohydrate, leucine or Tween 80.
* History of allergy to milk protein.
* Use of an inhaled corticosteroid within 30 days or systemic corticosteroid within 60 days of the Screening Visit.
* Use of medications or herbal medicines that are strong cytochrome P450 3A4 (CYP3A4) inhibitors or inducers within 30 days prior to Screening Visit
* Any clinically significant abnormal laboratory value or physical finding that may interfere with the interpretation of test results or cause a health risk for the subject if he/she participates in the study.
* Use of caffeine containing beverages more than 600 mg of caffeine/day.
* Current smokers or ex-smokers who have stopped smoking for less than 10 years.
* Recent or current (suspected) drug abuse or positive result in the drugs abuse test.
* Recent or current alcohol abuse (regular drinking more than 21 units per week for males and more than 14 units per week for females \[1 unit = 4 cl spirits or equivalent\]).
* Predictable poor compliance, intolerance to charcoal solution, or inability to communicate well with the study centre personnel or inability to participate in all treatment periods.
* The subject is not able to understand and comply with protocol requirements, instructions and protocol-stated restrictions, has participated in a clinical research study within the previous three months or has previously been enrolled in this study.
Minimum Eligible Age

18 Years

Maximum Eligible Age

45 Years

Eligible Sex

ALL

Accepts Healthy Volunteers

Yes

Sponsors

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Zambon SpA

INDUSTRY

Sponsor Role lead

Responsible Party

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Responsibility Role SPONSOR

Principal Investigators

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Phil Evans, MBChB

Role: PRINCIPAL_INVESTIGATOR

Quotient Clinical Limited

Locations

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Quotient Clinical Ltd

Ruddington, , United Kingdom

Site Status

Countries

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United Kingdom

Other Identifiers

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2014-002081-69

Identifier Type: EUDRACT_NUMBER

Identifier Source: secondary_id

Z7200J02

Identifier Type: -

Identifier Source: org_study_id

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NCT02850484 COMPLETED PHASE1
A Comparison of Symbicort® pMDI 2 x 160/4.5 μg Bid and 2 x 80/4.5 μg Bid With Formoterol Turbuhaler® 2 x 4.5 μg Bid and Placebo in Patients With COPD
NCT00206167 COMPLETED PHASE3
Comparing the Efficacy of Symbicort® pMDI and Formoterol Turbuhaler in Reducing Exacerbations in Patients With Cronic Obstructive Pulmonary Disease
NCT02157935 COMPLETED PHASE3
Clinical Pharmacology Study to Evaluate the Total Systemic Exposure and Lung Bioavailability of CHF 5993 pMDI Combination in Healthy Volunteers
NCT02359292 COMPLETED PHASE1
Assess Particle Deposition and Acute Effects of Symbicort® Forte Turbohaler®) in COPD Patients.
NCT01329276 COMPLETED PHASE4
A Comparison of SYMBICORT® pMDI With Formoterol Turbuhaler® in Subjects With COPD
NCT00419744 COMPLETED PHASE3
Pharmacokinetic Pilot Study on Budesonide/Formoterol Device-metered Dry Powder Inhalers
NCT01181063 COMPLETED PHASE1
Comparison of Salmeterol and Fluticasone Propionate Absorption From Salmeterol/Fluticasone Easyhaler With Seretide Diskus
NCT01856621 COMPLETED PHASE1
Active Controlled Trial of CHF5993 Pressurized Metered-dose Inhaler ( pMDI) vs Symbicort®Turbuhaler® in Patients With Chronic Obstructive Pulmonary Disease ( COPD)
NCT03197818 COMPLETED PHASE3
Foster® pMDI (CHF 1535) Versus Symbicort® Turbohaler in COPD Patient
NCT03888131 COMPLETED PHASE3
Bioequivalence Study to Assess Systemic Exposure of FP and SAL FDC From Different DPIs
NCT02215122 COMPLETED PHASE1
A Study to Investigate the Differential Effects of Inhaled Symbicort and Advair on Lung Microbiota
NCT02833480 UNKNOWN PHASE2
Studying Genes in Blood and Lung Fluid Samples From Patients With Chronic Obstructive Pulmonary Disease With or Without a Previous Diagnosis of Lung Cancer or With Asthma Treated With Budesonide and Formoterol
NCT00569712 COMPLETED PHASE1
Pharmacokinetic Pilot Study on Budesonide/Formoterol
NCT01457716 COMPLETED NA
Efficacy and Safety of Twice Daily 60mg AZD9668 in COPD for 12 Weeks in Patients on Background Budesonide/Formoterol
NCT01023516 COMPLETED PHASE2
Multi-centre Study to Assess the Efficacy and Safety of AZD5423 in COPD Patients on a Background Therapy of Formoterol
NCT01555099 COMPLETED PHASE2
A Comparison of Symbicort® pMDI 2 x 160/4.5 μg Bid and Symbicort® pMDI 2 x 80/4.5 μg Bid With Formoterol Turbuhaler®, Budesonide pMDI, the Combination of Formoterol Turbuhaler® and Budesonide pMDI, and Placebo in COPD Patients
NCT00206154 COMPLETED PHASE3
Comparison Between Symbicort® and Prednisolone in COPD
NCT00259779 COMPLETED PHASE3
Single-dose Crossover Study to Compare the Safety and Efficacy of FlutiForm With Fluticasone and Formoterol Concurrently or Alone in Asthma Patients
NCT00830102 COMPLETED PHASE2
Comparison of Salmeterol and Fluticasone Propionate Absorption From Salmeterol/Fluticasone Easyhaler and Seretide Diskus
NCT01766843 COMPLETED PHASE1