Study Of PF-06817024 In Healthy Subjects, In Patients With Chronic Rhinosinusitis With Nasal Polyps And in Patients With Atopic Dermatitis

February 28, 2022 updated by: Pfizer

A PHASE 1, RANDOMIZED, DOUBLE-BLIND, THIRD-PARTY OPEN, PLACEBO-CONTROLLED, DOSE ESCALATING STUDY TO EVALUATE THE SAFETY, TOLERABILITY, PHARMACOKINETICS AND PHARMACODYNAMICS OF SINGLE AND/OR MULTIPLE INTRAVENOUS AND/OR SUBCUTANEOUS DOSES OF PF-06817024 IN HEALTHY SUBJECTS WHO MAY BE MILDLY ATOPIC, SUBJECTS WITH CHRONIC RHINOSINUSITIS WITH NASAL POLYPS, AND SUBJECTS WITH MODERATE-SEVERE ATOPIC DERMATITIS

The purpose of this study is to evaluate safety, tolerability, pharmacokinetics, and pharmacodynamics of PF-06817024 in healthy volunteers, in participants with chronic rhinosinusitis, with nasal polyps and in participants with moderate-to-severe Atopic Dermatitis

Study Overview

Status

Completed

Conditions

Intervention / Treatment

Detailed Description

The purpose of the study for Part 1 is to evaluate the safety and tolerability of PF-06817024 in healthy subjects.

The purpose of the study for Part 2 is to evaluate the safety and tolerability of PF-06817024 in patients with chronic rhinosinusitis with nasal polyps.

The purpose of the study for Part 3 is to evaluate the safety and tolerability of PF-06817024 in patients with moderate-to-severe Atopic Dermatitis

Study Type

Interventional

Enrollment (Actual)

Phase

Phase 1

Contacts and Locations

This section provides the contact details for those conducting the study, and information on where this study is being conducted.

Study Locations

United States
- California
  - Sacramento, California, United States, 95816
    - UC Davis Dermatology
  - Sacramento, California, United States, 95817
    - UC Davis CTSC Clinical Research Center
  - Sacramento, California, United States, 95817
    - UC Davis Health
- Connecticut
  - New Haven, Connecticut, United States, 06511
    - New Haven Clinical Research Unit
  - Shelton, Connecticut, United States, 06484
    - Dermatology Physicians of Connecticut
- Florida
  - Tampa, Florida, United States, 33613
    - Forcare Clinical Research
- Indiana
  - Indianapolis, Indiana, United States, 46256
    - Dawes Fretzin Clinical Research Group, LLC
  - Indianapolis, Indiana, United States, 46256
    - Dawes Fretzin Dermatology Group, LLC
  - Plainfield, Indiana, United States, 46168
    - The Indiana Clinical Trials Center
- Minnesota
  - Edina, Minnesota, United States, 55435
    - Academic Dermatology
  - Minneapolis, Minnesota, United States, 55402
    - Clinical Research Institute, Inc.
  - Minneapolis, Minnesota, United States, 55404
    - Ear, Nose & Throat Specialty Care of Minnesota, P.A.
  - Saint Paul, Minnesota, United States, 55114
    - Prism research, LLC
- New Jersey
  - Berlin, New Jersey, United States, 08009
    - Hassman Research Institute
- North Carolina
  - Raleigh, North Carolina, United States, 27612
    - Carolina Phase 1 Research, LLC
- Oklahoma
  - Tulsa, Oklahoma, United States, 74136
    - Vital Prospects Clinical Research Institute, PC
- South Dakota
  - Rapid City, South Dakota, United States, 57702
    - Health Concepts
- Texas
  - San Antonio, Texas, United States, 78213
    - Lee Medical Associates, PA
  - San Antonio, Texas, United States, 78213
    - Progressive Clinical Research, PA
- Virginia
  - Norfolk, Virginia, United States, 23502
    - Virginia Clinical Research, Inc.

Participation Criteria

Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.

Eligibility Criteria

Ages Eligible for Study

18 years to 75 years (Adult, Older Adult)

Accepts Healthy Volunteers

Genders Eligible for Study

All

Description

Inclusion Criteria

Healthy male subjects, healthy female subjects of non-childbearing potential, 18-55 years of age (Part 1)
Male subjects, female subjects of non-childbearing potential, female subjects of childbearing potential with documented bilateral tubal ligation (tubes tied) or bilateral salpingectomy (tubes removed), 18-65 years of age, and 2 of the following symptoms: nasal congestion/obstruction, nasal discharge, face pain/pressure,or reduction/loss of smell (Part 2)
Male or female subjects between the ages of 18 and 75 years, inclusive with moderate-to-severe Atopic Dermatitis, agree to avoid prolonged exposure to the sun and not to use tanning booths, sun lamps, or other ultraviolet light sources during the study (Part 3)

Exclusion Criteria:

Clinically significant diseases (cardiac, psychiatric, autoimmune, renal, etc.), positive urine drug test, fever within 7 days of dosing, active infections within 28 days of dosing (Part 1 and 2 and 3)
History of allergic reaction to topical lidocaine, nasal surgery within 6 months (Part 2)
Exposure to live or attenuated vaccines, have skin conditions other than Atopic Dermatitis, use of JAK inhibitors and biologics (Part 3)

Study Plan

This section provides details of the study plan, including how the study is designed and what the study is measuring.

How is the study designed?

Design Details

Primary Purpose: Treatment
Allocation: Randomized
Interventional Model: Sequential Assignment
Masking: Quadruple

Number of Arms

Arms and Interventions

Participant Group / Arm	Intervention / Treatment
Experimental: Cohort 1 10 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 2 30 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 3 100 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 4 300 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 5 1000 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 6 2000 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 7 30 mg subcutaneous dose of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 8 300 mg of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 9 IV dose to be determined of PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 10 PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 11 PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 12 PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously
Experimental: Cohort 13 PF-06817024 or placebo	Biological: PF-06817024 Subjects will be given one dose of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 intravenously Biological: PF-06817024 Subjects will be given one dose of PF-06817024 subcutaneously Other: Placebo for PF-06817024 Subjects will be given one dose of placebo for PF-06817024 subcutaneously Biological: PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given two doses of PF-06817024 intravenously Biological: PF-06817024 Subjects will be given 2 doses intravenously Other: Placebo for PF-06817024 Subjects will be given 2 doses intravenously Biological: PF-06817024 Subjects will be given doses of PF-06817024 intravenously Other: Placebo for PF-06817024 Subjects will be given doses of Placebo intravenously

What is the study measuring?

Primary Outcome Measures

Secondary Outcome Measures

Collaborators and Investigators

This is where you will find people and organizations involved with this study.

Sponsor

Pfizer

Publications and helpful links

The person responsible for entering information about the study voluntarily provides these publications. These may be about anything related to the study.

Helpful Links

To obtain contact information for a study center near you, click here.

Study record dates

These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.

Study Major Dates

Study Start (Actual)

April 27, 2016

Primary Completion (Actual)

March 9, 2021

Study Completion (Actual)

March 9, 2021

Study Registration Dates

First Submitted

April 15, 2016

First Submitted That Met QC Criteria

April 15, 2016

First Posted (Estimate)

April 19, 2016

Study Record Updates

Last Update Posted (Actual)

May 19, 2022

Last Update Submitted That Met QC Criteria

February 28, 2022

Last Verified

February 1, 2022

More Information

Terms related to this study

Keywords

FIH, Pharmacokinetics, Pharmacodynamics, Safety, Tolerability, Atopic Dermatitis, Chronic Rhinosinusitis, Nasal Polyps

Additional Relevant MeSH Terms

Other Study ID Numbers

C0341001

Plan for Individual participant data (IPD)

Plan to Share Individual Participant Data (IPD)?

IPD Plan Description

Pfizer will provide access to individual de-identified participant data and related study documents (e.g. protocol, Statistical Analysis Plan (SAP), Clinical Study Report (CSR)) upon request from qualified researchers, and subject to certain criteria, conditions, and exceptions. Further details on Pfizer's data sharing criteria and process for requesting access can be found at: https://www.pfizer.com/science/clinical_trials/trial_data_and_results/data_requests.

Drug and device information, study documents

Studies a U.S. FDA-regulated drug product

Yes

Studies a U.S. FDA-regulated device product

product manufactured in and exported from the U.S.

This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.

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Outcome Measure	Measure Description	Time Frame
Number of Participants With All-causality Treatment Emergent Adverse Events (TEAEs) and Serious Adverse Events (SAEs) in Part 1 Time Frame: From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).	An adverse event (AE) was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. An SAE was any untoward medical occurrence at any dose that: results in death, is life threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, or results in congenital anomaly/birth defect.	From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).
Number of Participants With Treatment-Related TEAEs and SAEs in Part 1 Time Frame: From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. An SAE was any untoward medical occurrence at any dose that: results in death, is life threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, or results in congenital anomaly/birth defect. The causality of TEAEs and SAEs was determined by the investigator.	From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).
Number of All-Causality TEAEs According to Severity in Part 1 Time Frame: From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).	An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. TEAE was assessed by the investigator according to severity; Mild: did not interfere with participant's usual function; moderate: interfered to some extent with participant's usual function; severe: interfered significantly with participant's usual function.	From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).
Number of Participants With Permanent Discontinuation Due to TEAEs in Part 1 Time Frame: From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state.	From Study Day 1 (baseline) up to Day 421 (Cohort 1 and 2), Day 601 (Cohort 3), Day 691 (Cohort 4), Day 781 (Cohort 5), and Day 511 (Cohort 7).
Number of Participants With All-Causality TEAEs and SAEs in Part 2 Time Frame: From Study Day 1 (baseline) up to Day 691.	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. An SAE was any untoward medical occurrence at any dose that: results in death, is life threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, or results in congenital anomaly/birth defect.	From Study Day 1 (baseline) up to Day 691.
Number of Participants With Treatment-Related TEAEs and SAEs in Part 2 Time Frame: From Study Day 1 (baseline) up to Day 691.	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. An SAE was any untoward medical occurrence at any dose that: results in death, is life threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, or results in congenital anomaly/birth defect. The causality of TEAEs and SAEs was determined by the investigator.	From Study Day 1 (baseline) up to Day 691.
Number of All-Causality TEAEs According to Severity in Part 2 Time Frame: From Study Day 1 (baseline) up to Day 691.	An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. TEAE was assessed by the investigator according to severity; Mild: did not interfere with participant's usual function; moderate: interfered to some extent with participant's usual function; severe: interfered significantly with participant's usual function.	From Study Day 1 (baseline) up to Day 691.
Number of Participants With Permanent Discontinuation Due to TEAEs in Part 2 Time Frame: From Study Day 1 (baseline) up to Day 691.	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state.	From Study Day 1 (baseline) up to Day 691.
Number of Participants With All-Causality TEAEs and SAEs in Part 3 Time Frame: From Study Day 1 (baseline) up to Day 1105.	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. An SAE was any untoward medical occurrence at any dose that: results in death, is life threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, or results in congenital anomaly/birth defect.	From Study Day 1 (baseline) up to Day 1105.
Number of Participants With Treatment-Related TEAEs and SAEs in Part 3 Time Frame: From Study Day 1 (baseline) up to Day 1105.	An AE was any untoward medical occurrence in a clinical investigation where participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. An SAE was any untoward medical occurrence at any dose that: results in death, is life threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, or results in congenital anomaly/birth defect. The causality of TEAEs and SAEs was determined by the investigator.	From Study Day 1 (baseline) up to Day 1105.
Number of All-Causality TEAEs According to Severity in Part 3 Time Frame: From Study Day 1 (baseline) up to Day 1105.	An AE was any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state. TEAE was assessed by the investigator according to severity; Mild: did not interfere with participant's usual function; moderate: interfered to some extent with participant's usual function; severe: interfered significantly with participant's usual function.	From Study Day 1 (baseline) up to Day 1105.
Number of Participants With Permanent Discontinuation Due to TEAEs in Part 3 Time Frame: From Study Day 1 (baseline) up to Day 1105.	An AE was any untoward medical occurrence in a clinical investigation participants administered a product or medical device; the event needed not necessarily have a causal relationship with the treatment or usage. TEAEs were events between first dose of study drug and up to discharge from study that were absent before treatment or that worsened relative to pretreatment state.	From Study Day 1 (baseline) up to Day 1105.
Number of Participants With Clinically Significant Laboratory Abnormalities in Hematology, Chemistry, and Urinalysis in Part 1 Time Frame: Part 1 single-dose cohorts: from Study Day 1 (baseline) up to Day 211. Part 1 multiple-dose cohorts: from Study Day 1 (baseline) up to Day 241.	Hematology parameters included hemoglobin, hematocrit, red blood cell, mean corpuscular volume, mean corpuscular hemoglobin, mean corpuscular hemoglobin concentration, platelet and white blood cell count, total neutrophils, eosinophils, monocytes, basophils and lymphocytes. Chemistry parameters included blood urea nitrogen, glucose (fasting), calcium, sodium, potassium, chloride, bicarbonate, aspartate aminotransferase, alanine aminotransferase, total bilirubin, alkaline phosphatase, uric acid, albumin, total protein. Urine parameters included pH, glucose, protein, blood, ketones, nitrites, leukocyte esterase, urobilinogen, urine bilirubin, microscopy. Clinical significance was judged by the investigator and those met the criteria of AE are listed here. Clinically significant laboratory abnormalities reported for at least 1 participant in the whole study are presented here.	Part 1 single-dose cohorts: from Study Day 1 (baseline) up to Day 211. Part 1 multiple-dose cohorts: from Study Day 1 (baseline) up to Day 241.
Number of Participants With Clinically Significant Laboratory Abnormalities in Hematology, Chemistry, and Urinalysis in Part 2 Time Frame: Part 2: from Study Day 1 (baseline) up to Day 211.	Hematology parameters included hemoglobin, hematocrit, red blood cell, mean corpuscular volume, mean corpuscular hemoglobin, mean corpuscular hemoglobin concentration, platelet and white blood cell count, total neutrophils, eosinophils, monocytes, basophils and lymphocytes. Chemistry parameters included blood urea nitrogen, glucose (fasting), calcium, sodium, potassium, chloride, bicarbonate, aspartate aminotransferase, alanine aminotransferase, total bilirubin, alkaline phosphatase, uric acid, albumin, total protein. Urine parameters included pH, glucose, protein, blood, ketones, nitrites, leukocyte esterase, urobilinogen, urine bilirubin, microscopy. Clinical significance was judged by the investigator and those met the criteria of AE are listed here. Clinically significant laboratory abnormalities reported for at least 1 participant in the whole study are presented here.	Part 2: from Study Day 1 (baseline) up to Day 211.
Number of Participants With Clinically Significant Laboratory Abnormalities in Hematology, Chemistry, and Urinalysis in Part 3 Time Frame: Part 3: from Study Day 1 (baseline) up to Day 966.	Hematology parameters included hemoglobin, hematocrit, red blood cell, mean corpuscular volume, mean corpuscular hemoglobin, mean corpuscular hemoglobin concentration, platelet and white blood cell count, total neutrophils, eosinophils, monocytes, basophils and lymphocytes. Chemistry parameters included blood urea nitrogen, glucose (fasting), calcium, sodium, potassium, chloride, bicarbonate, aspartate aminotransferase, alanine aminotransferase, total bilirubin, alkaline phosphatase, uric acid, albumin, total protein. Urine parameters included pH, glucose, protein, blood, ketones, nitrites, leukocyte esterase, urobilinogen, urine bilirubin, microscopy. Clinical significance was judged by the investigator and those met the criteria of AE are listed here. Clinically significant laboratory abnormalities reported for at least 1 participant in the whole study are presented here.	Part 3: from Study Day 1 (baseline) up to Day 966.
Number of Participants With Vital Sign Abnormalities in Part 1 Time Frame: Study Day 1 (baseline) up to end of study (Study Day 211 for Part 1 SD cohorts, and Study Day 241 for Part 1 MD cohorts).	Criteria for abnormality in vital signs: supine pulse rate <40 beats per minute (bpm) or >120 bpm; supine diastolic blood pressure (DBP) <50 mmHg, maximum increase or decrease from baseline of >=20 mmHg; supine systolic blood pressure (SBP) <90 mmHg, maximum increase or decrease from baseline of >=30 mmHg. Baseline was defined as the last measurement prior to the first dosing. Vital sign abnormalities reported for at least 1 participant are presented here.	Study Day 1 (baseline) up to end of study (Study Day 211 for Part 1 SD cohorts, and Study Day 241 for Part 1 MD cohorts).
Number of Participants With Vital Sign Abnormalities in Part 2 Time Frame: Study Day 1 (baseline) up to end of study (Study Day 211).	Criteria for abnormality in vital signs: supine pulse rate <40 bpm or >120 bpm; supine DBP <50 mmHg, maximum increase or decrease from baseline of >=20 mmHg; supine SBP <90 mmHg, maximum increase or decrease from baseline of >=30 mmHg. Baseline was defined as the last measurement prior to the first dosing. Vital sign abnormalities reported for at least 1 participant are presented here.	Study Day 1 (baseline) up to end of study (Study Day 211).
Number of Participants With Vital Sign Abnormalities in Part 3 Time Frame: Study Day 1 (baseline) up to end of study (Study Day 337).	Criteria for abnormality in vital signs: supine pulse rate <40 bpm or >120 bpm; supine DBP <50 mmHg, maximum increase or decrease from baseline of >=20 mmHg; supine SBP <90 mmHg, maximum increase or decrease from baseline of >=30 mmHg. Baseline was defined as the last measurement prior to the first dosing. Vital sign abnormalities reported for at least 1 participant are presented here.	Study Day 1 (baseline) up to end of study (Study Day 337).
Number of Participants With Electrocardiogram (ECG) Abnormalities in Part 1 Time Frame: Study Day 1 (baseline) up to end of study (Study Day 211 for Part 1 SD cohorts, and Study Day 241 for Part 1 MD cohorts).	ECG abnormalities criteria included: 1) maximum QTc interval adjusted according Fridericia formula (QTcF) (msec): 450<= QTcF <480, 480<= QTcF <500, and QTcF >=500; QTcF maximum increase from baseline(msec): 30<= change <60, and change >=60; 2) maximum PR interval (msec): >=300; PR increase from baseline (msec): baseline >200 with 25% increase at maximum, baseline <=200 with 50% increase at maximum; 3) maximum QRS (msec): >=140; QRS increase from baseline (msec) >=50%. Baseline was defined as the average of the last triplicate measurement prior to the first dosing. ECG abnormalities reported for at least 1 participant are presented here.	Study Day 1 (baseline) up to end of study (Study Day 211 for Part 1 SD cohorts, and Study Day 241 for Part 1 MD cohorts).
Number of Participants With ECG Abnormalities in Part 2 Time Frame: Study Day 1 (baseline) up to end of study (Study Day 211).	ECG abnormalities criteria included: 1) maximum QTc interval adjusted according Fridericia formula (QTcF) (msec): 450<= QTcF <480, 480<= QTcF <500, and QTcF >=500; QTcF maximum increase from baseline(msec): 30<= change <60, and change >=60; 2) maximum PR interval (msec): >=300; PR increase from baseline (msec): baseline >200 with 25% increase at maximum, baseline <=200 with 50% increase at maximum; 3) maximum QRS (msec): >=140; QRS increase from baseline (msec) >=50%. Baseline was defined as the average of the last triplicate measurement prior to the first dosing. ECG abnormalities reported for at least 1 participant are presented here.	Study Day 1 (baseline) up to end of study (Study Day 211).
Number of Participants With ECG Abnormalities in Part 3 Time Frame: Study Day 1 (baseline) up to end of study (Study Day 337).	ECG abnormalities criteria included: 1) maximum QTc interval adjusted according Fridericia formula (QTcF) (msec): 450<= QTcF <480, 480<= QTcF <500, and QTcF >=500; QTcF maximum increase from baseline(msec): 30<= change <60, and change >=60; 2) maximum PR interval (msec): >=300; PR increase from baseline (msec): baseline >200 with 25% increase at maximum, baseline <=200 with 50% increase at maximum; 3) maximum QRS (msec): >=140; QRS increase from baseline (msec) >=50%. Baseline was defined as the average of the last triplicate measurement prior to the first dosing. ECG abnormalities reported for at least 1 participant are presented here.	Study Day 1 (baseline) up to end of study (Study Day 337).

Outcome Measure	Measure Description	Time Frame
Maximum Observed Serum Concentration (Cmax) of PF-06817024 Following Single Dose in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).	Maximum observed serum concentration (Cmax) of PF-06817024 following single dose in Part 1; Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).
Cmax of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
Cmax of PF-06817024 in Part 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).	Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).
Cmax of PF-06817024 in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	Cmax was defined as the maximum observed serum concentration.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Dose Normalized Maximum Observed Serum Concentration (Cmax[dn]) of PF-06817024 Following Single Dose in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).	Cmax(dn) was defined as the dose normalized maximum observed serum concentration, and calculated by Cmax/Dose. Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).
Cmax(dn) of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Cmax(dn) was defined as dose normalized maximum observed serum concentration, and calculated by Cmax/Dose. Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
Cmax(dn) of PF-06817024 in Part 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).	Cmax(dn) was defined as the dose normalized maximum observed serum concentration, and calculated by Cmax/Dose. Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).
Cmax(dn) of PF-06817024 in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	Cmax(dn) was defined as the dose normalized maximum observed serum concentration, and calculated by Cmax/Dose. Cmax was defined as the maximum observed serum concentration.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Time to Reach Maximum Observed Serum Concentration (Tmax) of PF-06817024 Following Single Dose in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).	Time to reach maximum observed serum concentration (Tmax) of PF-06817024 in Part 1; Tmax was defined as time to reach maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).
Tmax of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Tmax was defined as time to reach maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
Tmax of PF-06817024 in Part 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).	Tmax was defined as time to reach maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).
Tmax of PF-06817024 in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	Tmax was defined as time to reach maximum observed serum concentration.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Area Under the Curve From Time Zero to Infinity Concentration (AUCinf) of PF-06817024 Following Single Dose in Part 1 and 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to 780 days for Part 1 and 690 days for Part 2). For Part 1 only: at post-dose 48 and 72 hour, Days 46 and 151.	Area under the curve from time zero to infinity concentration (AUCinf) of PF-06817024 following single dose in Part 1 and 2; AUCinf was defined as area under the curve from time zero to infinity concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to 780 days for Part 1 and 690 days for Part 2). For Part 1 only: at post-dose 48 and 72 hour, Days 46 and 151.
Area Under the Curve From Time Zero to Last Quantifiable Concentration (AUClast) of PF-06817024 Following Single Dose in Part 1 and 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to 780 days for Part 1 and 690 days for Part 2). For Part 1 only: at post-dose 48 and 72 hour, Days 46 and 151.	Area under the curve from time zero to last quantifiable concentration (AUClast) of PF-06817024 following single dose in Part 1 and 2; AUClast was defined as area under the curve from time zero to last quantifiable concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to 780 days for Part 1 and 690 days for Part 2). For Part 1 only: at post-dose 48 and 72 hour, Days 46 and 151.
Area Under the Curve Within Dosing Interval (AUCtau) of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Area under the curve within dosing interval (AUCtau) of PF-06817024 following multiple doses in Part 1; AUCtau was defined as area under the curve within dosing interval. The dosing interval was 720 hours.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
AUCtau of PF-06817024 in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	AUCtau was defined as area under the curve within dosing interval. The dosing interval was 672 hours.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Dose Normalized Area Under the Curve Within Dosing Interval (AUCtau[dn]) of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Dose normalized area under the curve within dosing interval (AUCtau[dn]) of PF-06817024 following multiple doses in Part 1; AUCtau(dn) was defined as dose normalized area under the curve within dosing interval. The dosing interval was 720 hours.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
AUCtau(dn) of PF-06817024 Following Multiple Doses in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	AUCtau(dn) was defined as dose normalized area under the curve within dosing interval. The dosing interval was 672 hours.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Average Concentration Over Dosing Interval (Cav) of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Average concentration over dosing interval (Cav) of PF-06817024 following multiple doses in Part 1; Cav was defined as average concentration over dosing interval. The dosing interval was 720 hours.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
Cav of PF-06817024 Following Multiple Doses in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	Cav was defined as average concentration over dosing interval. The dosing interval was 672 hours.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Terminal Elimination Half Life (t1/2) of PF-06817024 Following Single Dose in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).	t1/2 was defined as terminal elimination half life, and was calculated by Loge(2)/kel, where kel was the terminal elimination phase rate constant calculated by a linear regression of the log-linear concentration-time curve.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).
t1/2 of PF-06817024 Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	T1/2 of PF-06817024 following multiple doses in Part 1; t1/2 was defined as terminal elimination half life.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
t1/2 of PF-06817024 in Part 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).	t1/2 was defined as terminal elimination half life, and was calculated by Loge(2)/kel, where kel was the terminal elimination phase rate constant calculated by a linear regression of the log-linear concentration-time curve.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to a maximum of 690 days/16560 hours post dose).
t1/2 of PF-06817024 in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	t1/2 was defined as terminal elimination half life, and was calculated by Loge(2)/kel, where kel was the terminal elimination phase rate constant calculated by a linear regression of the log-linear concentration-time curve. For Part 3 Cohort 13: PF-06817024 600 mg + 300 mg IV AD, t1/2 of the last dose on Day 85 was reported in the table.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Apparent Volume of Distribution (Vz/F) of PF-06817024 for the Subcutaneous Cohort in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).	Apparent volume of distribution (Vz/F) of PF-06817024 for the subcutaneous cohort in Part 1; Vz/F was defined as apparent volume of distribution.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).
Apparent Clearance (CL/F) of PF-06817024 for the Subcutaneous Cohort in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).	Apparent clearance (CL/F) of PF-06817024 for the subcutaneous cohort in Part 1; CL/F was defined as apparent clearance.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, 96 hours post dose on Day 1, and on Follow-up Days 8, 15, 32, 46, 61, 91, 121, 151, 181, 211, and at Extended Follow-Up visits (up to a maximum of 780 days/18720 hours post dose).
Volume of Distribution at Steady State (Vss) of PF-06817024 Following Single Intravenous Dose in Part 1 and Part 2 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to 780 days for Part 1 and 690 days for Part 2). For Part 1 only: at post-dose 48 and 72 hour, Days 46 and 151.	Volume of distribution at steady state (Vss) of PF-06817024 following a single dose in Part 1 and Part 2; Vss was defined as volume of distribution at steady state.	Pre-dose, 1, 2, 4, 8, 12, 24, and 96 hour post dose on Day 1, and Days 8, 15, 32, 61, 91, 121, 181, 211, and at Extended Follow-Up visits (up to 780 days for Part 1 and 690 days for Part 2). For Part 1 only: at post-dose 48 and 72 hour, Days 46 and 151.
Clearance (CL) of PF-06817024 Following Single Intravenous Dose in Part 1 and Part 2 Time Frame: On Day 1 at pre-dose, post-dose 1, 2, 4, 8, 12, 24, 96 hour, Day 8, 15, 32, 61, 91, 121,181, 211, 241, 331, and 421. For Part 1 only: at post-dose 48 and 72 hour, Day 46 and 151. For Part 2 only: on Day 511, 601, and 691.	CL was defined as Clearance, calculated by Dose/AUCinf. AUCinf was defined as area under the curve from time zero to infinity concentration.	On Day 1 at pre-dose, post-dose 1, 2, 4, 8, 12, 24, 96 hour, Day 8, 15, 32, 61, 91, 121,181, 211, 241, 331, and 421. For Part 1 only: at post-dose 48 and 72 hour, Day 46 and 151. For Part 2 only: on Day 511, 601, and 691.
Trough Serum Concentration (Cmin) of PF-06817024 Post Second Dose Following Multiple Doses in Part 1 Time Frame: At pre-dose on Day 31 or Day 46.	Trough serum concentration (Cmin) of PF-06817024 post second dose following multiple doses in Part 1; Cmin was defined as the trough serum concentration.	At pre-dose on Day 31 or Day 46.
Cmin of PF-06817024 Post Last Dose Following Multiple Doses in Part 3 Time Frame: At pre dose (0 hour) on Day 85.	Cmin of PF-06817024 post last dose following multiple doses in Part 3; Cmin was defined as the trough serum concentration.	At pre dose (0 hour) on Day 85.
Accumulation Ratio for Cmax (Rac, Cmax) of PF-06817024 Post Second Dose Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Rac, Cmax was defined as accumulation ratio for Cmax, and was calculated by (Cmax on Day 31 or Day 46) / Cmax on Day 1. Cmax was defined as the maximum observed serum concentration.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
Rac, Cmax of PF-06817024 Post Last Dose Following Multiple Doses in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	Rac, Cmax was defined as accumulation ratio for Cmax, and was calculated by (Cmax on Day 85) / (Cmax on Day 1). Cmax was defined as the maximum observed serum concentration.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Accumulation Ratio for AUCtau (Rac) of PF-06817024 Post Second Dose Following Multiple Doses in Part 1 Time Frame: Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).	Rac was defined as accumulation ratio for AUCtau. AUCtau was defined as area under the curve within dosing interval. The dosing interval was 720 hours.	Pre-dose, 1, 2, 4, 8, 12, 24, 48, 72, and 96 hr post dose on Day 1, Days 8 and 15, Day 31/46 (at pre-dose, 1, 2, 4, 8, 12, 24, 48 hr), Days 61, 91, 121, 151, 181, 211, 241, at Extended Follow-Up visits (up to a maximum of 645 days/15480 hr post dose).
Rac of PF-06817024 Post Last Dose Following Multiple Doses in Part 3 Time Frame: On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).	Rac was defined as accumulation ratio for AUCtau. AUCtau was defined as area under the curve within dosing interval. The dosing interval was 672 hours.	On Day 1 (at pre-dose, 1.5, 4, and 168 hours post dose), and Days 29, 57, and 85 (at pre-dose, 1.5 and 4 hours post dose), and on Days 113, 253, 337, and Extended Follow-Up visits (up to a maximum of 882 days/21168 hours post dose on Day 85).
Number of Participants With Treatment-Induced Anti-Drug Antibody (ADA) Against PF-06817024 in Part 1, 2, and 3 Time Frame: Part 1 SD cohorts: baseline up to Day 780; Part 1 MD cohort: baseline up to Day 693; Part 2: baseline up to Day 692, Part 3: baseline up to Day 964.	ADA was an immunogenicity endpoint. A participant had treatment-induced ADA when baseline titer was missing or negative and the participant had >=1 post-treatment positive titer.	Part 1 SD cohorts: baseline up to Day 780; Part 1 MD cohort: baseline up to Day 693; Part 2: baseline up to Day 692, Part 3: baseline up to Day 964.
Number of Participants With Treatment-Induced Neutralizing Antibodies (NAbs) Against PF-06817024 in Part 1, 2, and 3 Time Frame: Part 1 SD cohorts: baseline up to Day 780; Part 1 MD cohort: baseline up to Day 693; Part 2: baseline up to Day 692, Part 3: baseline up to Day 964.	NAb was an immunogenicity endpoint. A participant had treatment-induced NAb when baseline titer was missing or negative and the participant had >=1 post-treatment positive titer.	Part 1 SD cohorts: baseline up to Day 780; Part 1 MD cohort: baseline up to Day 693; Part 2: baseline up to Day 692, Part 3: baseline up to Day 964.

Study Of PF-06817024 In Healthy Subjects, In Patients With Chronic Rhinosinusitis With Nasal Polyps And in Patients With Atopic Dermatitis

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