A Combination Clinical Study of PLX3397 and Pembrolizumab... | NCT02452424 | Trialant
NCT02452424
Sponsor
Daiichi Sankyo
Status
Terminated
Last Update Posted
Mar 5, 2020Actual
Enrollment
78Actual
Phase
Phase 1Phase 2
Conditions
Melanoma
Non-small Cell Lung Cancer
Squamous Cell Carcinoma of the Head and Neck
Gastrointestinal Stromal Tumor (GIST)
Ovarian Cancer
Interventions
PLX3397
Pembrolizumab
Countries
United States
Protocol Section
Identification Module
NCT ID
NCT02452424
Obsolete or Duplicate NCT IDs
Not provided
Organization Study
PLX108-14
Secondary IDs
ID
Type
Description
Link
KEYNOTE-103
Other Identifier
Merck Sharp & Dohme Corp.
Brief Title
A Combination Clinical Study of PLX3397 and Pembrolizumab To Treat Advanced Melanoma and Other Solid Tumors
Official Title
Phase 1/2a Study of Double-Immune Suppression Blockade By Combining a CSF1R Inhibitor (PLX3397) With An Anti-PD-1 Antibody (Pembrolizumab) To Treat Advanced Melanoma And Other Solid Tumors
Acronym
Not provided
Organization
Daiichi SankyoINDUSTRY
Status Module
Record Verification Date
Feb 2020
Overall Recruitment Status or Expanded Access Status
Terminated
Last Known Status
Not provided
Delayed Posting
Not provided
Why Stopped
Terminated early for insufficient evidence of clinical efficacy
Expanded Access Info
No
Start Date
Jul 2, 2015Actual
Primary Completion Date
Aug 17, 2018Actual
Completion Date
Oct 12, 2018Actual
First Submitted Date
May 20, 2015
First Submission Date that Met QC Criteria
May 20, 2015
First Posted Date
May 22, 2015Estimated
Results Waived
Not provided
Results First Submitted Date
Aug 22, 2019
Results First Submitted that Met QC Criteria
Sep 18, 2019
Results First Posted Date
Oct 9, 2019Actual
Certification/Extension (aka Delayed Results) First Submitted Date
Not provided
Certification/Extension First Submitted that Passed QC Review
Not provided
Certification/Extension First Posted Date
Not provided
Last Update Submitted Date
Feb 18, 2020
Last Update Posted Date
Mar 5, 2020Actual
Sponsor/Collaborators Module
Responsible Party, by Official Title
Sponsor
Lead Sponsor
Daiichi SankyoINDUSTRY
Collaborators
Name
Class
Plexxikon
INDUSTRY
Merck Sharp & Dohme LLC
INDUSTRY
Oversight Module
Has Data Monitoring Committee (DMC)
No
Is FDA Regulated Drug
Yes
Is FDA Regulated Device
No
Is Unapproved Device
Not provided
Pediatric Postmarket Surveillance of a Device Product
Not provided
Product Exported from US
Not provided
FDAAA801 Violation
Not provided
Description Module
Brief Summary
The goal of this clinical research study is to learn how PLX3397 and pembrolizumab work together to affect cancer cells.
PLX3397 is designed to target the receptor for CSF1 (CSF1R). Pembrolizumab is designed to block the interaction between the receptor PD-1 and molecules that bind PD-1. In this study, PLX3397 and pembrolizumab are being given together in order to study their combined effects on patients' immune responses to their tumors. Tumor-specific immune responses have been shown to kill cancer cells and/or to stop tumors from growing.
Part 1 of the study (dose-escalation phase) will establish the safest dose of PLX3397 to be given in combination with pembrolizumab. Part 2 of the study (expansion phase) will include an evaluation of efficacy of this combination in the following tumor types:
Advanced melanoma: prior anti-PD-1/PD-L1 therapy but never responded
Advanced melanoma: prior anti-PD-1/PD-L1 therapy and responded but later progressed as defined by irRECIST while on therapy
Non-small cell lung cancer
Ovarian cancer
Gastrointestinal Stromal Tumor (GIST)
Squamous cell cancer of the head and neck
Detailed Description
Not provided
Conditions Module
Conditions
Melanoma
Non-small Cell Lung Cancer
Squamous Cell Carcinoma of the Head and Neck
Gastrointestinal Stromal Tumor (GIST)
Ovarian Cancer
Keywords
Not provided
Design Module
Study Type
Interventional
Number of References to an Expanded Access Study
Not provided
Expanded Access Types
Not provided
Patient Registry
Not provided
Target Follow-Up Duration
Not provided
Phases
Phase 1Phase 2
Interventional Study Design
Allocation
Biospecimen
No data available
No data is available for this block.
Enrollment
78Actual
Arms/Interventions Module
Arm Groups
Label
Type
Description
Intervention Names
PLX3397 and Pembrolizumab (Part 1)
Experimental
Open-label, sequential PLX3397 dose escalation with a fixed dose of pembrolizumab in approximately 24 patients with advanced solid tumors.
(Enrollment complete- 33 enrolled)
Drug: PLX3397
Biological: Pembrolizumab
PLX3397 and Pembrolizumab (Part 2)
Experimental
Extension cohort at the RP2D of PLX3397 in combination with pembrolizumab in approximately 376 patients with advanced solid tumors
(Enrollment Complete- 45 enrolled)
Drug: PLX3397
Biological: Pembrolizumab
Interventions
Name
Type
Description
Arm Group Labels
Other Names
PLX3397
Drug
PLX3397 capsules, 200 mg
PLX3397 and Pembrolizumab (Part 1)
PLX3397 and Pembrolizumab (Part 2)
Outcomes Module
Primary Outcomes
Measure
Description
Time Frame
Treatment-emergent Adverse Events (TEAEs) in Participants Regardless of Causality While Taking PLX3397 in Combination With Pembrolizumab
Treatment-emergent Adverse Events (TEAEs) in participants regardless of causality while taking PLX3397 in combination with pembrolizumab are reported
1 year (Dose Escalation); 2 years (Dose Expansion)
Secondary Outcomes
Measure
Description
Time Frame
Summary of the Percentage of Participants With Objective Response Rate Assessed by RECIST v1.1 During Pembrolizumab and PLX3397
Objective response rate was defined as the proportion of subjects who achieved a best disease response of either Complete or Partial (CR or PR) based on the Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.1) for target lesions and assessed generally by MRI, CT, or PET-CT and are summarized as: Complete Response (CR), Disappearance of all target lesions; Partial Response (PR), >=30% decrease in the sum of the longest diameter of target lesions. Participants who discontinued study therapy due to clinical progression, radiographic progression, or death without the required tumor assessments were considered to be non-responders in the Objective Response Rate (ORR) calculation. The efficacy analysis included all subjects with baseline tumor measurements who received at least 1 dose of study drug.
Other Outcomes
Not provided
Eligibility Module
Eligibility Criteria
Inclusion Criteria:
A subject must satisfy all of the following criteria to be considered for inclusion in the study:
Subjects with histologically or cytologically-confirmed diagnosis of cancer that is recurrent, metastatic, or persistent, who have relapsed from or are refractory to treatment and who also meet the following corresponding requirements for the cohort or phase of the study into which they will enroll:
Dose-escalation Phase: Subjects with advanced solid tumors (any tumor type) considered to have no standard-of care treatment for their malignancy with a curative intent, either as initial therapy or after progressing to prior therapies; subjects who have been treated previously with a CSF1R inhibitor or an anti PD1/PDL1 inhibitor may enroll.
Expansion Phase: Subjects with 1 of the tumor types who have relapsed from or are refractory to standard treatment. Subjects with non-small-cell lung cancer (non-squamous; EGFR, ALK wild type), advanced melanoma, ovarian cancer, unresectable RCC with component of clear-cell histology and/or component of sarcomatoid histology, glioblastoma or gliosarcoma, gastrointestinal stromal tumor.
Subjects with melanoma must have a histologically confirmed diagnosis of stage III disease not amenable to local therapy. Melanoma subjects may have received any number of prior lines of therapy for metastatic disease and must have measurable disease per RECISTv1.1. Subjects with melanoma who have received prior treatment with a BRAF/MEK inhibitor are acceptable candidates.
Expansion cohorts: Subjects must have relapsed or been refractory to standard treatment. NSCLC, SCCHN, and Melanoma must show primary progression with antiPD1/anti-PDL1 therapy. They must have tumor accessible for sequential biopsy (core needle biopsy or excision required) and be willing to provide on study tumor tissue biopsy. Subjects for whom newly obtained samples cannot be obtained (e.g. inaccessible or patient safety concern) may submit an archived specimen onlyupon agreement from the Sponsor.
ECOG performance status 0 or 1.
Women of childbearing potential must have a negative serum pregnancy test within 72 hours prior to initiation of dosing.
Women of childbearing potential should be willing to use 2 methods of birth control or be surgically sterile or abstain from heterosexual activity for the course of the study through 120 days after the last dose of study medication. Women of non-child bearing potential may be included if they are either surgically sterile or have been postmenopausal for ≥1 year.
Fertile men must agree to use an effective method of birth control starting with the first dose of study treatment through 120 days after the last dose of study treatment.
Adequate organ function as demonstrated by laboratory values.
Exclusion Criteria:
A subject who meets any of the following criteria will be disqualified from entering the study:
Disease that is suitable for local therapy administered with curative intent.
Diagnosis of immunodeficiency or is receiving systemic steroid therapy or any other form of immunosuppressive therapy within 7 days prior to the first dose of study treatment.
Is currently participating and receiving study therapy or has participated in a study of an investigational agent and received study therapy or used an investigational device within 28 days prior to the first dose of study treatment.
Has had monoclonal antibody within 28 days of first dose of study treatment or has not recovered from AEs due to agents administered more than 28 days earlier.
Has had chemotherapy, targeted small molecule therapy, or radiation therapy within 14 days prior to first dose of study treatment or who has not recovered from AEs due to a previously administered agent.
Note: Subjects with ≤ Grade 2 neuropathy or ≤ Grade 2 alopecia are an exception to this criterion and may qualify for the study.
Note: If a subject received major surgery, he or she must have recovered adequately from the toxicity and/or complications from the intervention prior to starting study treatment.
Has received transfusion of blood products (including platelets or red blood cells [RBC]) or administration of colony stimulating factors (including granulocyte colony-stimulating factor, granulocyte macrophage colony-stimulating factor, or recombinant erythropoietin) within 28 days prior to Day 1.
Evidence of interstitial lung disease or active, noninfectious pneumonitis.
Has a known additional malignancy that is progressing or requires active treatment. Exceptions include basal cell carcinoma of the skin, squamous cell carcinoma of the skin that has undergone potentially curative therapy, in situ cervical cancer and isolated elevation of prostate-specific antigen. Subjects with a completely treated prior malignancy with no evidence of disease for ≥ 2 years are eligible.
For Dose escalation cohort: patients with liver metastases, inclusion of patients with liver metastases in subsequent cohorts will be based upon clinical data.
For Expansion cohort subjects who have previously received an anti-PD-1, anti-PD-L1, or anti#PD-L2 agent or has previously participated in pembrolizumab clinical trials are excluded, except the following tumor types Melanoma, NSCLC and SCCHN (who must show primary progression to anti-PD1/anti-PDL1 therapy).
Radiation therapy within 14 days of first dose of study treatment.- remove since it's repetitive
Has active autoimmune disease that has required systemic treatment in past 2 years (i.e., with use of disease modifying agents, corticosteroids, or immunosuppressive drugs). Replacement therapy is not considered a form of systemic treatment.
Has an active infection requiring systemic therapy.
Has known central nervous system metastases and/or carcinomatous meningitis.
o Note: Subjects with previously treated brain metastases may participate if they meet the following criteria: 1) are stable for at least 28 days prior to the first dose of study treatment and if all neurologic symptoms returned to baseline); 2) have no evidence of new or enlarging brain metastases; and 3) have not been using steroids for at least 7 days prior to first dose of study treatment. This exception does not include carcinomatous meningitis, which is excluded regardless of clinical stability.
Uncontrolled intercurrent illness.
Refractory nausea and vomiting, malabsorption, external biliary shunt, or significant small bowel resection that would preclude adequate absorption.
QT interval corrected using Fridericia's formula (QTc) ≥ 450 msec (males) or ≥ 470 msec (females) at Screening.
Congenital long QT syndrome or patients taking concomitant medications known to prolong the QT interval.
Major surgery within 28 days prior to first dose of study treatment.
Has received a live vaccine administered within 30 days prior to first dose of study treatment.
Has a history or current evidence of any condition, therapy, or laboratory abnormality that might confound the results of the trial, interfere with the subject's participation for the full duration of the trial, or is not in the best interest of the subject to participate, in the opinion of the treating investigator.
Active and clinically significant bacterial, fungal or viral infection, including hepatitis B virus (HBV), hepatitis C virus (HCV), known human immunodeficiency virus (HIV) or acquired immunodeficiency syndrome related illness (HIV testing is not required), including subjects who have an active infection requiring systemic therapy.
Any of the following within 48 weeks (~1 year) prior to first dose of study treatment: myocardial infarction, uncontrolled angina, coronary/peripheral artery bypass graft, symptomatic congestive heart failure, cerebrovascular accident or transient ischemic attack.
Is pregnant or breastfeeding, or expecting to conceive or father children within the projected duration of the trial, starting with the screening visit through 120 days after the last dose of study treatment.
Has known psychiatric or substance abuse disorders that would interfere with cooperation with the requirements of the trial.
Has had prior exposure to PLX3397.
Has had hypersensitivity (≥Grade 3) reaction to pembrolizumab and/or any of its excipients.
Accepts Healthy Volunteers
No
Sex
All
Sex/Gender Based
Not provided
Sex/Gender Description
Not provided
Minimum Age
18 Years
Maximum Age
Not provided
Standard Ages
AdultOlder Adult
Study Population
Not provided
Sampling Method
Not provided
Contacts/Locations Module
Central Contacts
Not provided
Overall Officials
Not provided
Locations
Facility
Status
City
State
ZIP
Country
Contacts
HonorHealth Research Institute
Scottsdale
Arizona
85258
United States
Marin Cancer Care
References Module
No data available
No data is available for this block.
IPD Sharing Statement Module
Plan to Share IPD
Yes
Description
De-identified individual participant data (IPD) and applicable supporting clinical trial documents may be available upon request at https://vivli.org/. In cases where clinical trial data and supporting documents are provided pursuant to our company policies and procedures, Daiichi Sankyo will continue to protect the privacy of our clinical trial participants. Details on data sharing criteria and the procedure for requesting access can be found at this web address: https:// vivli.org/ourmember/daiichi-sankyo/
Types
Study Protocol
Statistical Analysis Plan (SAP)
Clinical Study Report (CSR)
Time Frame
Studies for which the medicine and indication have received European Union (EU) and United States (US), and/or Japan (JP) marketing approval on or after 01 January 2014 or by the US or EU or JP Health Authorities when regulatory submissions in all regions are not planned and after the primary study results have been accepted for publication.
Access Criteria
Formal request from qualified scientific and medical researchers on IPD and clinical study documents from clinical trials supporting products submitted and licensed in the United States, the European Union and/or Japan from 01 January 2014 and beyond for the purpose of conducting legitimate research. This must be consistent with the principle of safeguarding study participants' privacy and consistent with provision of informed consent.
Dose Escalation: Up to 42 participants with advanced solid tumors (any type) were to be enrolled sequentially in up to 7 cohorts (3+3 design).
Dose Expansion: Up to 483 participants were planned with the sample size for each tumor type based on a truncated sequential probability ratio test (max sample size 28 to 48 participants per tumor type).
Recruitment Details
Dose Escalation: 33 participants who met the inclusion and none of the exclusion criteria were enrolled and received study drug.
Dose Expansion: 45 participants with melanoma, non-small cell lung cancer (NSCLC), ovarian cancer, squamous cell carcinoma of the head and neck (SCCHN), and gastrointestinal stromal tumor (GIST) were enrolled.
Type of Units Analyzed
Not provided
Arm/Group Information
ID
Title
Description
FG000
Dose Escalation: 400 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 400 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 200 mg in the evening).
FG001
Dose Escalation: 600 mg/Day
Periods
Title
Milestones
Reasons Not Completed
Overall Study
Type
Comment
Milestone Data
STARTED
Baseline Characteristics Module
Baseline Analysis Population Description
Not provided
Outcome Measures Module
Outcome Measures
Adverse Events Module
Frequency Threshold
5
More Info Module
Limitations and Caveats
Annotation Section
No data available
No data is available for this block.
Document Section
Large Document Module
Document Has No Statistical Analysis Plan (SAP)
Not provided
Uploaded Document Information
Type
Includes Protocol
Includes SAP
Includes ICF
Document Label
Document Date
Document Uploaded Date
Document File Name
Prot_SAP
Yes
Yes
No
Study Protocol and Statistical Analysis Plan
Dec 14, 2017
Derived Section
Miscellaneous Info Module
Version Holder
Jul 10, 2026
Removed Countries
Not provided
Submission Tracking
No data available
No data is available for this block.
Condition Browse Module
MeSH Terms
Intervention Browse Module
MeSH Terms
Non-Randomized
Intervention Model
Single Group Assignment
Intervention Model Description
Not provided
Primary Purpose
Treatment
Observational Model
Not provided
Time Perspective
Not provided
Masking Info
Masking
None (Open Label)
Masking Description
Not provided
Who Masked
Not provided
Pexidartinib
Pembrolizumab
Biological
Pembrolizumab, 200 mg, IV
PLX3397 and Pembrolizumab (Part 1)
PLX3397 and Pembrolizumab (Part 2)
Keytruda, MK-3475, SCH 900475
1 year (Dose Escalation); 2 years (Dose Expansion)
Greenbrae
California
94904
United States
Ronald Reagan UCLA Medical Center
Los Angeles
California
90095
United States
Massachusetts General Hospital
Boston
Massachusetts
02114
United States
Beth Israel Deaconess Medical Center
Boston
Massachusetts
02115
United States
Dana-Farber Cancer Institute
Boston
Massachusetts
02215
United States
Karmanos Cancer Institute
Detroit
Michigan
48201
United States
Washington University St. Louis Siteman Cancer Center
St Louis
Missouri
63130
United States
Memorial Sloan Kettering Cancer Center
New York
New York
10065
United States
Medical University Health Hollings Cancer Center
Charleston
South Carolina
29425
United States
Vanderbilt Ingram Cancer Center
Nashville
Tennessee
37212
United States
South Texas Accelerated Research Therapeutics
San Antonio
Texas
78229
United States
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG002
Dose Escalation: 600 mg/Day (Liver Metastases
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG003
Dose Escalation: 600 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG004
Dose Escalation: 800 mg/Day (Liver Metastases)
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
FG005
Dose Escalation: 800 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
FG006
Dose Expansion: Melanoma
Participants with melanoma received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG007
Dose Expansion: NSCLC
Participants with NSCLC received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG008
Dose Expansion: Ovarian Cancer
Participants with ovarian cancer received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG009
Dose Expansion: SCCHN
Participants with SCCHN received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG010
Dose Expansion: GIST
Participants with GIST received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
FG0004 subjects
FG0013 subjects
FG0027 subjects
FG0039 subjects
FG0044 subjects
FG0056 subjects
FG00613 subjects
FG0078 subjects
FG00815 subjects
FG0093 subjects
FG0106 subjects
COMPLETED
FG0002 subjects
FG0010 subjects
FG0020 subjects
FG0031 subjects
FG0042 subjects
FG0055 subjects
FG0063 subjects
FG0074 subjects
FG0089 subjects
FG0091 subjects
FG0104 subjects
NOT COMPLETED
FG0002 subjects
FG0013 subjects
FG0027 subjects
FG0038 subjects
FG0042 subjects
FG0051 subjects
FG00610 subjects
FG0074 subjects
FG0086 subjects
FG0092 subjects
FG0102 subjects
Type
Comment
Reasons
Death
FG0002 subjects
FG0012 subjects
FG0022 subjects
FG0036 subjects
FG0042 subjects
FG0050 subjects
FG0065 subjects
FG0071 subjects
FG0083 subjects
FG0091 subjects
FG0100 subjects
Lost to Follow-up
FG0000 subjects
FG0011 subjects
FG0021 subjects
FG0030 subjects
FG004
Withdrawal by Subject
FG0000 subjects
FG0010 subjects
FG0023 subjects
FG0032 subjects
FG004
Other
FG0000 subjects
FG0010 subjects
FG0021 subjects
FG0030 subjects
FG004
Progressive disease (per RECIST)
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG004
Adverse Event
FG0000 subjects
FG0010 subjects
FG0020 subjects
FG0030 subjects
FG004
Type of Units Analyzed
Not provided
Arm/Group Information
ID
Title
Description
BG000
Dose Escalation: 400 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 400 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 200 mg in the evening)..
BG001
Dose Escalation: 600 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG002
Dose Escalation: 600 mg/Day (Liver Metastases
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG003
Dose Escalation: 600 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG004
Dose Escalation: 800 mg/Day (Liver Metastases)
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
BG005
Dose Escalation: 800 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening)..
BG006
Dose Expansion: Melanoma
Participants with melanoma received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG007
Dose Expansion: NSCLC
Participants with NSCLC received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG008
Dose Expansion: Ovarian Cancer
Participants with ovarian cancer received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG009
Dose Expansion: SCCHN
Participants with SCCHN received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG010
Dose Expansion: GIST
Participants with GIST received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
BG011
Total
Total of all reporting groups
Denominators
Units
Counts
Participants
BG0004
BG0013
BG0027
BG0039
BG0044
BG0056
BG00613
BG0078
BG00815
BG0093
BG0106
BG01178
Baseline Measures
Title
Description
Population Description
Parameter Type
Dispersion Type
Unit of Measure
Calculate Percentage
Denominator Units Selected
Denominators
Classes
Age, Categorical
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
<=18 years
BG0000
BG0010
BG0020
BG003
Age, Continuous
Mean
Standard Deviation
years
Title
Denominators
Categories
Title
Measurements
BG00064.5± 8.6
BG00154.7± 10.2
BG002
Sex: Female, Male
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
Female
BG0002
BG0011
BG002
Race (NIH/OMB)
Count of Participants
Participants
Title
Denominators
Categories
Title
Measurements
American Indian or Alaska Native
BG0000
BG0010
BG002
Region of Enrollment
Number
participants
Title
Denominators
Categories
United States
Title
Measurements
BG0004
BG0013
BG002
Type
Title
Description
Population Description
Reporting Status
Anticipated Posting Date
Parameter Type
Dispersion Type
Unit of Measure
Calculate Percentage
Time Frame
Units Analyzed
Denominator Units Selected
Arm/Group Information
Denominators
Classes
Analyses
Primary
Treatment-emergent Adverse Events (TEAEs) in Participants Regardless of Causality While Taking PLX3397 in Combination With Pembrolizumab
Treatment-emergent Adverse Events (TEAEs) in participants regardless of causality while taking PLX3397 in combination with pembrolizumab are reported
Safety events were assessed in the Safety Population.
Posted
Count of Participants
Participants
1 year (Dose Escalation); 2 years (Dose Expansion)
ID
Title
Description
OG000
Dose Escalation: 400 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 400 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 200 mg in the evening).
OG001
Dose Escalation: 600 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG002
Dose Escalation: 600 mg/Day (Liver Metastases
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG003
Dose Escalation: 600 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG004
Dose Escalation: 800 mg/Day (Liver Metastases)
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
OG005
Dose Escalation: 800 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
OG006
Dose Expansion: Melanoma
Participants with melanoma received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG007
Dose Expansion: NSCLC
Participants with NSCLC received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG008
Dose Expansion: Ovarian Cancer
Participants with ovarian cancer received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG009
Dose Expansion: SCCHN
Participants with SCCHN received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG010
Dose Expansion: GIST
Participants with GIST received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
Units
Counts
Participants
OG0004
OG0013
OG0027
OG003
Title
Denominators
Categories
Title
Measurements
OG0004
OG0013
OG0027
OG003
Secondary
Summary of the Percentage of Participants With Objective Response Rate Assessed by RECIST v1.1 During Pembrolizumab and PLX3397
Objective response rate was defined as the proportion of subjects who achieved a best disease response of either Complete or Partial (CR or PR) based on the Response Evaluation Criteria In Solid Tumors Criteria (RECIST v1.1) for target lesions and assessed generally by MRI, CT, or PET-CT and are summarized as: Complete Response (CR), Disappearance of all target lesions; Partial Response (PR), >=30% decrease in the sum of the longest diameter of target lesions. Participants who discontinued study therapy due to clinical progression, radiographic progression, or death without the required tumor assessments were considered to be non-responders in the Objective Response Rate (ORR) calculation. The efficacy analysis included all subjects with baseline tumor measurements who received at least 1 dose of study drug.
Overall best response was assessed in the Efficacy Analysis Set.
Posted
Count of Participants
Participants
1 year (Dose Escalation); 2 years (Dose Expansion)
ID
Title
Description
OG000
Dose Escalation: 400 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 400 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 200 mg in the evening).
OG001
Dose Escalation: 600 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
Time Frame
Adverse event data were collected for each subject from after the first dose was administered to 30 days after the last dose, through study completion at Cycle 16 (up to approximately 100 weeks)
Description
Adverse events that emerge (or worsen) after the first dose of study drug and within 30 days after the last dose.
All-Cause Mortality Comment
Not provided
Arm/Groups
ID
Title
Description
Deaths (Affected)
Deaths (At Risk)
Serious Events (Affected)
Serious Events (At Risk)
Other Events (Affected)
Other Events (At Risk)
EG000
Dose Escalation: 400 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 400 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 200 mg in the evening).
2
4
2
4
4
4
EG001
Dose Escalation: 600 mg/Day
Participants received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
2
3
1
3
3
3
EG002
Dose Escalation: 600 mg/Day (Liver Metastases
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
2
7
3
7
7
7
EG003
Dose Escalation: 600 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
6
9
3
9
9
9
EG004
Dose Escalation: 800 mg/Day (Liver Metastases)
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
2
4
2
4
4
4
EG005
Dose Escalation: 800 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
0
6
3
6
6
6
EG006
Dose Expansion: Melanoma
Participants with melanoma received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
5
13
3
13
12
13
EG007
Dose Expansion: NSCLC
Participants with NSCLC received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
1
8
3
8
8
8
EG008
Dose Expansion: Ovarian Cancer
Participants with ovarian cancer received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
3
15
5
15
15
15
EG009
Dose Expansion: SCCHN
Participants with SCCHN received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
1
3
1
3
3
3
EG010
Dose Expansion: GIST
Participants with GIST received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
0
6
0
6
6
6
Serious Adverse Events
Term
Organ System
Source Vocabulary
Assessment Type
Notes
Statistical Information
Febrile neutropenia
Blood and lymphatic system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG0030 affected9 at risk
EG004
Splenic infarction
Blood and lymphatic system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pericardial effusion
Cardiac disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Abdominal pain lower
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Diarrhoea
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Faecaloma
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Gastrointestinal haemorrhage
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Lower gastrointestinal haemorrhage
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Obstruction gastric
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rectal haemorrhage
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Small intestinal obstruction
Gastrointestinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Generalised oedema
General disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pyrexia
General disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Drug-induced liver injury
Hepatobiliary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected3 at risk
EG0020 affected7 at risk
EG003
Drug hypersensitivity
Immune system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Parotitis
Infections and infestations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Urinary tract infection
Infections and infestations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Urosepsis
Infections and infestations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Radiation oesophagitis
Injury, poisoning and procedural complications
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Alanine aminotransferase increased
Investigations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Aspartate aminotransferase increased
Investigations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hepatic enzyme increased
Investigations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Liver function test abnormal
Investigations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Transaminases increased
Investigations
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Dehydration
Metabolism and nutrition disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0022 affected7 at risk
EG003
Cancer pain
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Tumour pain
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Tumour pain (All grades)
Neoplasms benign, malignant and unspecified (incl cysts and polyps)
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Cerebral infarction (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Cognitive disorder (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Dizziness (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0022 affected7 at risk
EG003
Dysarthria (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Dysgeusia (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Encephalopathy (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Haemorrhage intracranial (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Headache (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hydrocephalus (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hypoaesthesia (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Migraine with aura (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Neuralgia
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Neuropathy peripheral
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Paraesthesia (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Peripheral sensory neuropathy
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Presyncope (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Syncope (All grades)
Nervous system disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Anxiety (All grades)
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Completed suicide
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Confusional state (All grades)
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Hallucination (All grades)
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Insomnia (All grades)
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Mental status changes (All grades)
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Restlessness
Psychiatric disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Acute kidney injury
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Chromaturia
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Dysuria
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Haematuria (All grades)
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pollakiuria
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Proteinuria (All grades)
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Urinary retention
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Urinary tract pain
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Urine abnormality
Renal and urinary disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Benign prostatic hyperplasia
Reproductive system and breast disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Menstruation irregular
Reproductive system and breast disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Penile discharge (All grades)
Reproductive system and breast disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Perineal pain (All grades)
Reproductive system and breast disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Alveolar lung disease
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Aspiration
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Atelectasis
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Cough (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Dysphonia (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Dyspnoea (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected3 at risk
EG0021 affected7 at risk
EG003
Dyspnoea at rest
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Dyspnoea exertional (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Epistaxis (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Haemoptysis (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Hypoxia (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Lung disorder
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Nasal congestion
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Nasal discharge discolouration
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Oropharyngeal pain (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Paranasal sinus hypersecretion
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pharyngeal erythema (All grade)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Pleural effusion (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pleuritic pain (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Pneumonia aspiration
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pneumonitis
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pneumothorax
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Productive cough
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pulmonary embolism (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rales
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Respiratory tract congestion
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rhinorrhea (All grades)
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Sinus congestion
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Sneezing
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Tachypnoea
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Throat irritation
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Upper respiratory tract congestion
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Upper-airway cough syndrome
Respiratory, thoracic and mediastinal disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Acne
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Alopecia
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Blister
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Cold sweat (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Dry skin
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Erythema (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hair colour changes (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Hyperhidrosis (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Ingrowing nail
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Night sweats (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Palmar-plantar erythrodysaesthesia syndrome
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Photosensitivity reaction
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Pruritus (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0023 affected7 at risk
EG003
Pruritus generalised
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rash (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rash erythematous (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rash generalized (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Rash macular
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Rash maculo-papular (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0011 affected3 at risk
EG0020 affected7 at risk
EG003
Rash pruritic
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Skin discolouration (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Skin exfoliation
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Skin hyperpigmentation (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Skin hypopigmentation (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0021 affected7 at risk
EG003
Skin lesion (All grades)
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Swelling face
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Vitiligo
Skin and subcutaneous tissue disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Flushing
Vascular disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Haematoma
Vascular disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hot flush
Vascular disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hyperaemia
Vascular disorders
MedDRA (18.0)
Systematic Assessment
EG0000 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hypertension (All grades)
Vascular disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Hypotension (All grades)
Vascular disorders
MedDRA (18.0)
Systematic Assessment
EG0001 affected4 at risk
EG0010 affected3 at risk
EG0020 affected7 at risk
EG003
Enrollment for this study was terminated early for insufficient evidence of clinical efficacy. Some of the planned statistical analyses described in the protocol and Statistical Analysis Plan (SAP) were not performed.
Female Urogenital Diseases and Pregnancy Complications
D000091642
Urogenital Diseases
D005833
Genital Neoplasms, Female
D014565
Urogenital Neoplasms
D000091662
Genital Diseases
D004700
Endocrine System Diseases
D006058
Gonadal Disorders
Browse Leaves
Not provided
Browse Branches
Not provided
ID
Term
C000600259
pexidartinib
C582435
pembrolizumab
Ancestor Terms
Not provided
Browse Leaves
Not provided
Browse Branches
Not provided
0 subjects
FG0050 subjects
FG0060 subjects
FG0070 subjects
FG0080 subjects
FG0090 subjects
FG0100 subjects
0 subjects
FG0050 subjects
FG0061 subjects
FG0070 subjects
FG0081 subjects
FG0091 subjects
FG0100 subjects
0 subjects
FG0051 subjects
FG0064 subjects
FG0073 subjects
FG0080 subjects
FG0090 subjects
FG0101 subjects
0 subjects
FG0050 subjects
FG0060 subjects
FG0070 subjects
FG0082 subjects
FG0090 subjects
FG0100 subjects
0 subjects
FG0050 subjects
FG0060 subjects
FG0070 subjects
FG0080 subjects
FG0090 subjects
FG0101 subjects
0
BG0040
BG0050
BG0060
BG0070
BG0080
BG0090
BG0100
BG0110
Between 18 and 65 years
BG0001
BG0012
BG0026
BG0037
BG0040
BG0053
BG0069
BG0076
BG00810
BG0092
BG0104
BG01150
>=65 years
BG0003
BG0011
BG0021
BG0032
BG0044
BG0053
BG0064
BG0072
BG0085
BG0091
BG0102
BG01128
51.1
± 17.0
BG00355.9± 10.9
BG00472.0± 5.3
BG00561.7± 8.7
BG00661.8± 8.3
BG00757.0± 11.3
BG00860.4± 12.5
BG00952.7± 16.3
BG01059.7± 8.8
BG01159.3± 11.5
3
BG0033
BG0042
BG0054
BG0064
BG0075
BG00815
BG0090
BG0102
BG01141
Male
BG0002
BG0012
BG0024
BG0036
BG0042
BG0052
BG0069
BG0073
BG0080
BG0093
BG0104
BG01137
0
BG0030
BG0040
BG0050
BG0060
BG0070
BG0080
BG0090
BG0100
BG0110
Asian
BG0000
BG0010
BG0020
BG0030
BG0040
BG0050
BG0060
BG0071
BG0081
BG0090
BG0100
BG0112
Native Hawaiian or Other Pacific Islander
BG0000
BG0010
BG0020
BG0030
BG0040
BG0050
BG0060
BG0070
BG0080
BG0090
BG0100
BG0110
Black or African American
BG0001
BG0010
BG0020
BG0031
BG0040
BG0051
BG0060
BG0071
BG0080
BG0090
BG0101
BG0115
White
BG0003
BG0013
BG0026
BG0038
BG0043
BG0055
BG00612
BG0076
BG00814
BG0093
BG0105
BG01168
More than one race
BG0000
BG0010
BG0020
BG0030
BG0040
BG0050
BG0060
BG0070
BG0080
BG0090
BG0100
BG0110
Unknown or Not Reported
BG0000
BG0010
BG0021
BG0030
BG0041
BG0050
BG0061
BG0070
BG0080
BG0090
BG0100
BG0113
7
BG0039
BG0044
BG0056
BG00613
BG0078
BG00815
BG0093
BG0106
BG01178
9
OG0044
OG0056
OG00613
OG0078
OG00815
OG0093
OG0106
9
OG0044
OG0056
OG00612
OG0078
OG00815
OG0093
OG0106
OG002
Dose Escalation: 600 mg/Day (Liver Metastases
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG003
Dose Escalation: 600 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG004
Dose Escalation: 800 mg/Day (Liver Metastases)
Participants with liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
OG005
Dose Escalation: 800 mg/Day (no Liver Metastases)
Participants with no liver metastases received pembrolizumab 200 mg IV every 3 weeks in combination with of PLX3397 at 800 mg/day (administered twice daily [BID] as a split dose of 400 mg in the morning and 400 mg in the evening).
OG006
Dose Expansion: Melanoma
Participants with melanoma received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG007
Dose Expansion: NSCLC
Participants with NSCLC received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG008
Dose Expansion: Ovarian Cancer
Participants with ovarian cancer received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG009
Dose Expansion: SCCHN
Participants with SCCHN received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).
OG010
Dose Expansion: GIST
Participants with GIST received pembrolizumab 200 mg IV every 3 weeks in combination with PLX3397 at 600 mg/day (administered twice daily [BID] as a split dose of 200 mg in the morning and 400 mg in the evening).