Phase 2
N=364
A Study Of PF-06463922 An ALK/ROS1 Inhibitor In Patients With Advanced Non Small Cell Lung Cancer With Specific Molecular Alterations
ALK-positive Non Small Cell Lung Cancer (NSCLC) and ROS1-positive NSCLC
Bottom Line
View on ClinicalTrials.gov: NCT01970865 ↗Enrolled (actual)
364
Serious AEs
50.0%
Results posted
May 2018
Primary outcome: Primary: Number of Participants With Cycle 1 Dose-Limiting Toxicities (DLTs) in Phase 1 — 0; 0; 0; 0 Participants
Study Design & Population
- Study type
- Interventional
- Phase
- Phase 2
- Interventions
- PF-06463922 (Drug); Crizotinib (Drug)
- Age
- Adult, Older Adult · 18+ yrs
- Sex
- All
- Sponsor
- Pfizer
- Primary completion
- Mar 2017
Outcome Measures
| Outcome | Result | p-value |
|---|---|---|
| PRIMARY Number of Participants With Cycle 1 Dose-Limiting Toxicities (DLTs) in Phase 1 |
0; 0; 0; 0; 0; 0 | — |
| PRIMARY Percentage of Participants With Overall and Intracranial Objective Response (Phase 2) |
90.0; 74.1; 50.8; 41.5; 34.8; 36.2 | — |
| SECONDARY Percentage of Participants With Overall and Intracranial Objective Response (Phase 1) |
39.0; 50.0; 41.2; 50.0 | — |
| SECONDARY Time to Tumor Response (TTR) and Intracranial TTR (Phase 1) |
1.4; 1.4; 1.4; 1.4 | — |
| SECONDARY Number of Participants With Duration of Response (DOR) and Intracranial DOR (Phase 1) |
1; 0; 6; 0; 0; 1 | — |
| SECONDARY Percentage of Participants Achieving Disease Control and Intracranial Disease Control at 12 and 24 Weeks (Phase 1) |
53.7; 58.3; 39.0; 50.0; 50.0; 37.5 | — |
| SECONDARY Probability of First Event Being a Central Nervous System (CNS) Progression, Non CNS Progression, or Death (Phase 1) |
0.260; 0.352; 0.060 | — |
| SECONDARY Progression-Free Survival (PFS) (Phase 1) |
5.4; 10.1 | — |
| SECONDARY Overall Survival (OS) (Phase 1) |
22.3; NA | — |
| SECONDARY Maximum Observed Plasma Concentration (Cmax) of PF-06463922 Following Single Oral Doses (Phase 1) |
50.80; 149.2; NA; 489.1; 595.5; 760.0 | — |
| SECONDARY Maximum Observed Plasma Concentration (Cmax) of PF-06463922 Following Multiple Oral Doses (Phase 1) |
67.29; 138.1; 359.7; 429.6; 550.2; 541.0 | — |
| SECONDARY Time for Cmax (Tmax) of PF-06463922 Following Single Oral Doses (Phase 1) |
1.98; 2.00; 1.25; 1.09; 1.96; 1.05 | — |
| SECONDARY Time for Cmax (Tmax) of PF-06463922 Following Multiple Oral Doses (Phase 1) |
1.00; 1.00; 2.00; 1.03; 1.13; 1.30 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero to Time Tau (AUCtau) of PF-06463922 Following Single Oral Doses (Phase 1) |
488.2; 1387; NA; 3990; 5110; 7474 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero to Time Tau (AUCtau) of PF-06463922 Following Multiple Oral Doses (Phase 1) |
752.1; 1701; 3367; 4107; 5121; 6157 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero Extrapolated to Infinite Time (AUCinf) of PF-06463922 Following Single Oral Doses (Phase 1) |
NA; NA; 7663; 8236; 18340; NA | — |
| SECONDARY Apparent Oral Clearance (CL/F) of PF-06463922 Following Single Oral Doses (Phase 1) |
NA; NA; 9.788; 12.14; 10.90; NA | — |
| SECONDARY Apparent Oral Clearance (CL/F) of PF-06463922 Following Multiple Oral Doses (Phase 1) |
13.27; 14.72; 14.84; 17.66; 19.52; 24.37 | — |
| SECONDARY Apparent Volume of Distribution (Vz/F) of PF-06463922 Following Single Oral Doses (Phase 1) |
NA; NA; 367.9; 356.3; 307.8; NA | — |
| SECONDARY Observed Accumulation Ratio (Rac) of PF-06463922 Following Multiple Oral Doses (Phase 1) |
1.543; 1.237; 1.105; 1.121; 1.071; 1.000 | — |
| SECONDARY Terminal Half-Life of PF-06463922 Following Single Oral Doses (Phase 1) |
NA; 23.70; 27.22; 20.89; 19.80; 25.55 | — |
| SECONDARY Steady State Accumulation Ratio (Rss) of PF-06463922 Following Multiple Oral Doses (Phase 1) |
NA; 0.5600; 0.6131; 0.6603; 0.3935; NA | — |
| SECONDARY Renal Clearance (CLr) of PF-06463922 (Phase 1) |
61.31 | — |
| SECONDARY Percent of PF-06463922 Recovered Unchanged in Urine up to Dosing Interval (AEtau%) (Phase 1) |
0.4017 | — |
| SECONDARY Maximum Observed Plasma Concentration (Cmax) of Midazolam (Phase 1) |
16.06; 11.56; 9.697; 5.734 | — |
| SECONDARY Time for Cmax (Tmax) of Midazolam (Phase 1) |
0.50; 0.50; 0.50; 0.50 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero to the Time of the Last Quantifiable Concentration (AUClast) of Midazolam (Phase 1) |
51.30; 36.49; 20.43; 14.44 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero Extrapolated to Infinite Time (AUCinf) of Midazolam (Phase 1) |
54.53; NA; 21.32; 16.09 | — |
| SECONDARY Apparent Oral Clearance (CL/F) of Midazolam (Phase 1) |
36.68; NA; 93.86; 124.2 | — |
| SECONDARY Apparent Volume of Distribution (Vz/F) of Midazolam (Phase 1) |
229.0; NA; 404.4; 702.2 | — |
| SECONDARY Terminal Half-Life of Midazolam (Phase 1) |
4.620; 5.120; 3.343; 5.257 | — |
| SECONDARY Number of Participants With ALK Mutation Based on Plasma CNA Analysis (Phase 1) |
14 | — |
| SECONDARY Number of Participants With ALK Mutation Based on Tumor Tissue Analysis (Phase 1) |
7 | — |
| SECONDARY Number of Participants Who Improved, Worsened or Remained Stable in EORTC QLQ-C30 (Phase 1) |
19; 13; 11; 5; 29; 9 | — |
| SECONDARY Number of Participants Who Improved, Worsened or Remained Stable in EORTC QLQ-LC13 (Phase 1) |
9; 23; 11; 23; 12; 8 | — |
| SECONDARY Change From Baseline in Mini Mental State Examination (MMSE) Score (Phase 1) |
1.0; -0.5; -0.9; 0.8; 0.0; 0.0 | — |
| SECONDARY Time to Tumor Response (TTR) and Intracranial TTR (Phase 2 and DDI Sub-study) |
1.4; 1.4; 1.4; 2.6; 1.4; 1.4 | — |
| SECONDARY Duration of Response (DOR) and Intracranial DOR (Phase 2 and DDI Substudy) |
17.16; 16.56; 11.10; 15.08; 7.03; 19.61 | — |
| SECONDARY Percentage of Participants Achieving Disease Control and Intracranial Disease Control at Week 12 and 24 (Phase 2 and DDI Substudy) |
93.3; 85.2; 68.3; 64.6; 50.0; 66.0 | — |
| SECONDARY Time to Progression on the Last Prior Therapy (Phase 2) |
11.5; 12.8; 10.2; 3.7; 11.5; 13.8 | — |
| SECONDARY Time to Tumor Progression (TTP) and Intracranial TTP (Phase 2 and DDI Substudy) |
17.7; 20.6; 8.2; 8.4; 5.6; 12.5 | — |
| SECONDARY Probability of First Event Being a Central Nervous System (CNS) Progression, Non CNS Progression, or Death (Phase 2) |
0.179; 0.325; 0.055 | — |
| SECONDARY Progression-Free Survival (PFS) (Phase 2 and DDI Substudy) |
16.6; 20.6; 6.9; 7.3; 5.5; 9.9 | — |
| SECONDARY Overall Survival (Phase 2 and DDI Substudy) |
NA; 52.5; NA; 18.7; 20.4; 49.7 | — |
| SECONDARY Maximum Observed Plasma Concentration (Cmax) of PF-06463922 (Phase 2) |
695.2; 576.5 | — |
| SECONDARY Time for Cmax (Tmax) of PF-06463922 (Phase 2) |
1.15; 1.96 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero Extrapolated to Infinite Time (AUCinf) of PF-06463922 (Phase 2) |
9088 | — |
| SECONDARY Area Under the Plasma Concentration-Time Profile From Time Zero to Time Tau (AUCtau) of PF-06463922 (Phase 2) |
5308; 5650 | — |
| SECONDARY Apparent Oral Clearance (CL/F) of PF-06463922 (Phase 2) |
11.01; 17.70 | — |
| SECONDARY Apparent Volume of Distribution (Vz/F) of PF-06463922 (Phase 2) |
351.5 | — |
| SECONDARY Terminal Half-Life of PF-06463922 (Phase 2) |
23.58 | — |
| SECONDARY Observed Accumulation Ratio (Rac) of PF-06463922 Following Multiple Oral Doses (Phase 2) |
1.082 | — |
| SECONDARY Steady State Accumulation Ratio (Rss) of PF-06463922 Following Multiple Oral Doses (Phase 2) |
0.6577 | — |
| SECONDARY Number of Participants With ALK Mutation Based on Plasma CNA Analysis (Phase 2) |
0; 6; 8; 17; 14 | — |
| SECONDARY Number of Participants With ALK Mutation Based on Tumor Tissue Analysis (Phase 2) |
0; 7; 8; 12; 13 | — |
| SECONDARY Number of Participants Who Improved, Worsened or Remained Stable in EORTC QLQ-C30 (Phase 2 and DDI Sub-study) |
17; 11; 18; 25; 17; 19 | — |
| SECONDARY Number of Participants Who Improved, Worsened or Remained Stable in EORTC QLQ-LC13 (Phase 2 and DDI Sub-study) |
11; 5; 9; 21; 12; 12 | — |
| SECONDARY Number of Participants With Treatment-Emergent Adverse Events (Phase 1, Phase 2 and DDI Sub-study) |
3; 3; 3; 12; 17; 3 | — |
| SECONDARY Number of Participants With Laboratory Abnormalities (Phase 1, Phase 2 and DDI Sub-study) - Hematology |
3; 3; 3; 10; 16; 3 | — |
| SECONDARY Number of Participants With Laboratory Abnormalities (Phase 1, Phase 2 and DDI Sub-study) - Chemistry |
2; 1; 1; 6; 9; 2 | — |
| SECONDARY Number of Participants With Laboratory Abnormalities (Phase 1, Phase 2 and DDI Sub-study) - Coagulation, Lipids and Urinalysis |
1; 0; 1; 3; 2; 0 | — |
| SECONDARY Number of Participants With Vital Signs Data Meeting Pre-defined Criteria (Phase 1, Phase 2 and DDI Sub-study) |
0; 0; 0; 0; 3; 2 | — |
| SECONDARY Number of Participants With Maximum Decrease From Baseline Greater Than or Equal to 20 Percent in Left Ventricular Ejection Fraction (LVEF) (Phase 1, Phase 2 and DDI Sub-study) |
1; 0; 1; 3; 5; 2 | — |
| SECONDARY Number of Participants With Absolute Values and Change From Baseline in QTcF Meeting Pre-defined Criteria (Phase 1, Phase 2 and DDI Sub-study) |
1; 0; 0; 2; 1; 1 | — |
| SECONDARY Number of Participants With Suicidal Ideation and Suicidal Behavior (Phase 2) |
1; 0; 2; 1; 1; 2 | — |
| SECONDARY Change From Baseline in Total Scores for Beck Depression Inventory (BDI)-II (Mood Assessment) (Phase 2) |
-2.59; -3.27; -2.26; -2.17; -1.52; -2.43 | — |
| SECONDARY Change From Baseline in Total Scores for Detection Test (Cognitive Function Assessment) (Phase 2) |
0.01; 0.04; -0.01; 0.02; -0.02; 0.01 | — |
| SECONDARY Change From Baseline in Total Scores for Identification Test (Cognitive Function Assessment) (Phase 2) |
-0.02; -0.02; -0.01; -0.01; -0.02; -0.01 | — |
| SECONDARY Change From Baseline in Total Scores for One Back Test (Cognitive Function Assessment) (Phase 2) |
0.01; 0.02; 0.02; 0.01; 0.02; 0.01 | — |
| SECONDARY Change From Baseline in Total Scores for International Shopping List Test (Cognitive Function Assessment) (Phase 2) |
-0.02; -1.13; 0.25; -0.45; 0.96; 0.16 | — |
| SECONDARY Change From Baseline in Total Scores for International Shopping List Test-Delayed Recall (Cognitive Function Assessment) (Phase 2) |
0.10; -0.84; -0.12; -0.59; -0.22; -0.25 | — |
| SECONDARY Number of Participants With Absolute Values and Change From Baseline in PR Interval Meeting Pre-defined Criteria (Phase 2 and DDI Substudy) |
4; 3; 8; 9; 6; 10 | — |
Summary
Phase 1 and 2 trial to study the safety, pharmacokinetics, pharmacodynamics, patient reported outcomes and efficacy of PF-06463922 in ALK + advanced non-small cell lung cancer patients and ROS1+ advanced non small cell lung cancer patients .
Eligibility Criteria
Inclusion Criteria
- Evidence of histologically or cytologically confirmed diagnosis of metastatic NSCLC (Stage IV, AJCC v7.0) that carries an ALK rearrangement, as determined by the Food and Drug Administration (FDA) approved FISH assay (Abbott Molecular Inc) or by Immunohistochemistry (IHC) (Ventana Inc), or a ROS1 rearrangement as determined by FISH or RT PCR or Next Generation Sequencing (NGS) via a local diagnostic test (LDT). All patients (ALK positive and ROS1 positive) must have archival tissue sample available and collected prior to enrollment.
- Disease Status Requirements:
Phase 1: ALK-positive NSCLC and ROS1-positive patients must either be treatment naïve in the advanced setting or have had disease progression after at least 1 previous ALK/ROS1 inhibitor therapy(ies).
Phase 2:
ALK-positive NSCLC patients must either be or have had:
- Treatment naïve (ie, no prior chemotherapy in the metastatic disease setting and no prior ALK inhibitor therapy allowed).
- Disease progression after crizotinib only. No prior chemotherapy is allowed in the metastatic disease setting.
- Disease progression after crizotinib and 1 or 2 prior regimens of chemotherapy in the metastatic disease setting.
- Disease progression after 1 prior ALK inhibitor therapy other than crizotinib. Patients may have had any number of prior chemotherapy regimens in any disease setting.
- Disease progression after 2 prior ALK inhibitor therapies. Patients may have had any number of prior chemotherapy regimens in any disease setting.
- Disease progression after 3 prior ALK inhibitor therapies. Patients may have had any number of prior chemotherapy regimens in any disease setting.
ROS1-positive NSCLC patients may be:
- Treatment naïve (ie, no prior chemotherapy in the metastatic disease setting and no prior ROS inhibitor therapy).
- Any number of prior therapies (ie, chemotherapy and/or ROS inhibitor therapies).
- Tumor Requirements:
All Patients must have at least one measurable target extracranial lesion according to RECIST v1.1. In addition patients with asymptomatic CNS metastases (including patients asymptomatic by means of stable or decreasing doses of steroids within the last 2 weeks prior to study entry) will be eligible. Patients who have leptomeningeal disease (LM) or carcinomatous meningitis (CM) are eligible.
- Adequate Bone Marrow, Pancreatic Function, Renal Function and Liver Function.
- Negative Serum pregnancy test for females of childbearing potential Exclusion Criteria
- Radiation therapy (except palliative to relieve bone pain) within 2 weeks of study entry. Whole brain radiation must have completed at least 4 weeks prior to study entry.
- Systemic anti cancer therapy completed within a minimum of 5 half lives of study entry.
- Prior therapy with an antibody or drug specifically targeting T-cell co-stimulation or immune checkpoint pathways, including, but not limited to, anti-PD-1, anti-PD-L1, anti-PD-L2, anti-CD137, or anti-cytotoxic T lymphocyte associated antigen 4 (anti-CTLA-4) antibody.
- Active and clinically significant bacterial, fungal, or viral infection including hepatitis B (HBV), hepatitis C (HCV), known human immunodeficiency virus (HIV), or acquired immunodeficiency syndrome (AIDS) related illness.
- Clinically significant cardiovascular disease (that is, active or 220 msec. Ongoing cardiac dysrhythmias of NCI CTCAE Grade ≥2, uncontrolled atrial fibrillation of any grade, bradycardia defined as 470 msec, or congenital long QT syndrome.
- History of extensive, disseminated, bilateral or presence of Grade 3 or 4 interstitial fibrosis or interstitial lung disease including a history of pneumonitis, hypersensitivity pneumonitis, interstitial pneumonia, interstitial lung disease, obliterative bronchiolitis and pulmonary fibrosis.
- Current use or anticipated need for food or drugs that are known strong or moderate CYP3A4 inhibitors, inducers and substrates; drugs that are CYP2C9 substrates; drugs that are sensitive CYP2B
Data sourced from ClinicalTrials.gov (NCT01970865). Outcome figures and adverse-event rates are extracted automatically from the registry's posted results and are provided for clinician reference, not as a substitute for the primary publication.