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Enapotamab Vedotin (HuMax-AXL-ADC) Safety Study in Patients With Solid Tumors

Primary Purpose

Ovarian Cancer, Cervical Cancer, Endometrial Cancer

Status
Completed
Phase
Phase 1
Locations
International
Study Type
Interventional
Intervention
Enapotamab vedotin (HuMax-AXL-ADC)
Sponsored by
Genmab
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Ovarian Cancer

Eligibility Criteria

18 Years - undefined (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  1. For the dose escalation part: Patients with selected, relapsed solid tumors who have failed available standard therapy or who are not candidates for standard therapy.
  2. For the expansion part: Patients with relapsed, advanced and/or metastatic solid tumors who are not candidates for standard therapy
  3. Patients must have measurable disease according to Response Evaluation Criteria In Solid Tumors (RECIST).
  4. For the expansion patients must provide a fresh tumor biopsy at enrolment
  5. Age ≥ 18 years.
  6. Acceptable renal function
  7. Acceptable liver function
  8. Acceptable hematological status
  9. Have an Eastern Cooperative Oncology Group (ECOG) performance status of 0 or 1.
  10. Life expectancy of at least three months.
  11. Patients, both females and males, of childbearing/reproductive potential must agree to use adequate contraception while included in the trial and for six months after the last infusion of HuMax-AXL-ADC
  12. Patients must provide a signed informed consent form before any trial relates activities are carried out.

Exclusion Criteria:

  1. Acute deep vein thrombosis or clinically relevant pulmonary embolism, not stable for at least 4 weeks prior to first IMP administration.
  2. Have clinically significant cardiac disease
  3. Known congestive heart failure and/ or a known decreased cardiac ejection fraction of < 45%. A baseline QT interval as corrected by Fridericia's formula (QTcF) > 480 msec, a complete left bundle branch block (defined as a QRS interval ≥ 120 msec in left bundle branch block form) or an incomplete left bundle branch block.
  4. Uncontrolled hypertension
  5. Have received granulocyte colony stimulating factor (G-CSF) or granulocyte/macrophage colony stimulating factor support 3 weeks prior to first IMP administration.
  6. Have received a cumulative dose of corticosteroid ≥ 150 mg prednisone (or equivalent doses of corticosteroids) within two weeks before the first Investigational Medicinal Product (IMP) administration.
  7. History of ≥ grade 3 allergic reactions to monoclonal antibody therapy as well as known or suspected allergy or intolerance to any agent given in the course of this trial.
  8. Major surgery within four weeks before first IMP administration.
  9. Any history of intracerebral arteriovenous malformation, cerebral aneurysm, brain metastases or stroke.
  10. Any anticancer therapy including; small molecules, immunotherapy, chemotherapy monoclonal antibodies or any other experimental drug within five half-lives but maximum four weeks before first infusion. Accepted exceptions are bisphosphonates, denosumab and gonadotropin-releasing hormone agonist or antagonist.
  11. Prior therapy with a conjugated or unconjugated auristatin derivative/vinca-binding site targeting payload.
  12. Radiotherapy within 14 days prior to first IMP administration.
  13. Known past or current malignancy other than inclusion diagnosis, except for:

    • Cervical carcinoma of Stage 1B or less.
    • Non-invasive basal cell or squamous cell skin carcinoma.
    • Non-invasive, superficial bladder cancer.
    • Prostate cancer with a current PSA level < 0.1 ng/mL.
    • Breast cancer in BRCA1 or BRCA2 positive ovarian cancer patients.
    • Any curable cancer with a complete response (CR) of > 2 years duration.
  14. Melanoma patients with an LDH ≥ 3 x ULN.
  15. Ongoing significant, uncontrolled medical condition including:

    o Serious, non-healing wound, skin ulcer (of any grade), or bone fracture.

  16. Grade 2 or higher peripheral neuropathy.
  17. Clinically significant active viral, bacterial or fungal infection
  18. Known human immunodeficiency virus seropositivity.
  19. Known positive serology for hepatitis B (unless due to vaccination or passive immunization due to immunoglobulin therapy)
  20. Known positive serology for hepatitis C (unless due to immunoglobulin therapy)
  21. Substance abuse, medical, psychological or social conditions that may interfere with the patient's participation in the trial or evaluation of the trial result
  22. History of organ allograft (except for corneal transplant) or autologous or allogeneic bone marrow transplant, or stem cell rescue within 3 months prior to the first dose of IMP
  23. Body weight < 40 kg
  24. Women who are pregnant or breast feeding.
  25. Pulmonary hemorrhage or hemoptysis > 2.5 ml blood within 6 weeks unless cause has been addressed and is medically resolved.
  26. History of acute pneumonitis.

Sites / Locations

  • Mayo Clinic - Phoenix
  • University of Colorado Hospital
  • Yale University, Smilow Cancer Center at Yale New Haven Hospital
  • Mayo Clinic Jacksonville
  • Moffitt Cancer Center
  • Emory University School of Medicine, Winship Cancer Institute
  • University of Iowa
  • Dana-Farber Cancer Institute
  • University of Michigan Comprehensive Cancer Center
  • Mayo Clinic Rochester
  • Washington University
  • Roswell Park Comprehensive Cancer Center
  • Laura and Isaac Perlmutter Cancer Center at NYU Langone
  • Herbert Irving Comprehensive Cancer Center
  • Duke Cancer Institute
  • Fox Chase Cancer Center
  • Mary Crowley Cancer Research Center
  • University of Texas MD Anderson Cancer Center
  • University of Utah Huntsman Cancer Institute
  • University of Wisconsin Carbone Cancer Center
  • Universitair Ziekenhuizen Leuven
  • Institut Roi Albert II - Cliniques Universitaires Saint Luc
  • Universitair Ziekenhuis Brussel - Oncologisch Centrum
  • Medische oncologie, Oncologisch Centrum - AZ Groeninge
  • U.Z. Leuven Gasthuisberg, Department of General Medical Oncology
  • CHU de Liège, Medical Oncology et. Domaine Universitaire du Sart Tilman
  • Rigshospitalet, Copenhagen University Hospital
  • The Netherlands Cancer Institute - Antoni van Leeuwenhoek Hospital
  • Leiden University Medical Centre
  • Erasmus MC, Medical Oncology
  • UMC Utrecht Cancer Center
  • Hospital Unversitario Vall D'hebron
  • Oncologia Mèdica/ Medical Oncology Department Institut Catalá d'Oncologia (ICO)
  • University Hospital of Girona
  • Hospital Universitario 12 Octubre Servicio de Oncologia Medica
  • Hospital Virgen de la Victoria
  • University Hospital Lozano Blesa, Aragón Health Research Institute (IIS Aragón)
  • University College London Hospitals
  • The Christie NHS Foundation Trust Clinical Trials Unit
  • Sir Bobby Robson Clinical Trials Unit at the Northern Centre for Cancer Care, Freeman Hospital
  • The Royal Marsden Hospital

Arms of the Study

Arm 1

Arm Type

Experimental

Arm Label

Enapotamab vedotin (HuMax-AXL-ADC)

Arm Description

Participants in all cohorts of the trial (both in escalation and expansion phase) will be administered enapotamab vedotin (HuMax-AXL-ADC) intravenously (IV).

Outcomes

Primary Outcome Measures

Number of Participants With Dose-limiting Toxicities (DLTs) for Dose-escalation Part
The DLTs were defined as Grade (G) 4 neutropenia or G4 thrombocytopenia for a minimal duration of 7 days, G3 and G4 febrile neutropenia, >=G3 hemorrhage associated with >=G3 thrombocytopenia, G4 anemia; Stevens Johnson syndrome, toxic epidermal necrolysis, >=G3 cutaneous vasculitis; G3 neuropathy (not improved to G1 within 3 weeks following pausing of dosing) and G4 neuropathy; G3 infusion-related reactions (IRR) that did not resolve to G1 or baseline within 24 hours; G4 IRR or G4 anaphylaxis events; >= G3 diarrhoea and/or vomiting persisting >48 hours or G3 nausea lasting 7 days (both despite optimal medical management); or any >=G3 related non-hematological AEs, which occurred during the Cycle 1 and regarded as medically important as assessed by the Data Monitoring Committee (excluding Grade 3 fatigue or non-hematological laboratory abnormalities as specified in protocol).
Number of Participants With Treatment-emergent Adverse Events (TEAEs) and Treatment-emergent Serious Adverse Events (TESAEs)
An adverse event (AE) is any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. An SAE is defined as an AE that meets one of the following criteria: requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant incapacity or substantial disruption of the ability to conduct normal life functions, is a congenital anomaly/birth defect, is medically important, results in death, or is life-threatening. In this trial, a TEAE was defined as an AE occurring or worsening between the first dose of enapotamab vedotin and 30 days after the last dose received.
Number of Participants With Treatment-emergent Infusion-related AEs and TEAEs Related to Enapotamab Vedotin
Number of participants with treatment-emergent infusion-related AEs and TEAEs related to enapotamab vedotin is reported.
Number of Participants With >= Grade 3 TEAEs as Assessed by National Cancer Institute - Common Terminology Criteria for Adverse Events (NCI-CTCAE) Version 4.03
Number of participants with TEAEs of >= Grade 3 as assessed by NCI-CTCAE v4.03 is reported. The NCI-CTCAE is a descriptive terminology is used for AE reporting. The NCI-CTCAE v4.03 displays Grades 1 through 5 with unique clinical descriptions of severity for each AE, based on this general guideline: Grade 1 as mild AE, Grade 2 as moderate AE, Grade 3 as severe AE, Grade 4 as life-threatening or disabling AE, and Grade 5 as death. If a participant reported multiple severity grades for an AE, only the maximum grade was used.
Number of Participants With Grade 3 or 4 Laboratory Results
Number of participants with laboratory measurements graded as Grade 3 or 4 by NCI-CTCAE v 4.03 is reported.

Secondary Outcome Measures

Area Under the Plasma Concentration-time Curve From Time 0 to Infinity (AUC0-inf) of Conjugated Enapotamab Vedotin for 1Q3W Dose-escalation Part
The AUC0-inf of conjugated enapotamab vedotin for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Area Under the Plasma Concentration-time Curve From Time 0 to Last Measurable Concentration (AUC0-last) of Conjugated Enapotamab Vedotin for 1Q3W Dose-escalation Part
The AUC0-last of conjugated enapotamab vedotin for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Maximum Observed Plasma Concentration (Cmax) of Conjugated Enapotamab Vedotin for Dose-escalation Part
The Cmax of conjugated enapotamab vedotin for dose-escalation part is reported.
Total Clearance (CL) of Conjugated Enapotamab Vedotin in Dose-escalation Part
The total CL of conjugated enapotamab vedotin in dose-escalation part is reported.
Time of Maximum Plasma Concentration (Tmax) of Conjugated Enapotamab Vedotin for Dose-escalation Part
The Tmax of conjugated enapotamab vedotin for dose-escalation part is reported.
Half-life Lambda-z (t1/2) of Conjugated Enapotamab Vedotin for Dose-escalation Part
The t1/2 of conjugated enapotamab vedotin for dose-escalation part is reported.
Volume of Distribution at Steady State (Vss) of Conjugated Enapotamab Vedotin for Dose-escalation Part
The Vss of conjugated enapotamab vedotin for dose-escalation part is reported.
AUC0-inf of Free Toxin Monomethyl Auristatin E (MMAE) for 1Q3W Dose-escalation Part
The AUC0-inf of MMAE for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
AUC0-last of MMAE for 1Q3W Dose-escalation Part
The AUC0-last of MMAE for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Cmax of MMAE for Dose-escalation Part
The Cmax of MMAE for dose-escalation part is reported.
Total CL of MMAE in Dose-escalation Part
The total CL of MMAE in dose-escalation part is reported.
Tmax of MMAE for Dose-escalation Part
The Tmax of MMAE for dose-escalation part is reported.
t1/2 of MMAE for Dose-escalation Part
The t1/2 of MMAE for dose-escalation part is reported.
Number of Participants With Antidrug Antibodies (ADAs) Confirmed Positive to Enapotamab Vedotin
The ADA assessment was performed according to a tiered approach. First samples were screened for an ADA response; positively screened samples were analyzed in a confirmation method. Subsequently confirmed positive samples were analyzed for titre and the presence of neutralizing antibodies. Number of participants with ADA confirmed positive to enapotamab vedotin is reported.
Number of Participants With Objective Response (OR) Based on Response Evaluation Criteria in Solid Tumors Version 1.1 (RECIST v1.1) As Assessed by Investigator
Radiological evaluation based on RECIST v1.1 was performed by the investigator using computed tomography (CT) scans/ magnetic resonance imaging (MRI) scans/ positron emission tomography (PET) scans. The OR was defined as confirmed CR or confirmed PR per RECIST v1.1. The changes in tumor measurements that were confirmed by repeat assessments performed no less than 4 weeks after initial response are called confirmed responses. The CR was defined as disappearance of all target and non-target lesions and all pathological lymph nodes must have decreased to < 10 mm in short axis. The PR was defined as at least a 30% decrease in the sum of the longest diameters (LD) of target lesions taking as reference the baseline sum of LD.
Number of Participants With Best Cancer Antigen 125 (CA-125) Response
The best CA-125 response was evaluated in participants with ovarian cancer. A CA-125 partial response was defined as at least a 50% reduction in CA-125 levels in blood from a pretreatment sample. Participants who had a CA-125 partial response and had CA-125 level falls to within the reference range (0-35 units/mL) were classified as CA-125 complete responders. The response was confirmed and maintained for at least 28 days. The best overall response (CA-125 partial response and CA-125 complete response) is reported.
Duration of Response (DoR) Based on RECIST v1.1 as Assessed by Investigator for Expansion Part
The DoR was defined as the number of months from the first documentation of objective tumor response (CR or PR) to the date of first progressive disease (PD) or death. The OR was defined as confirmed CR or confirmed PR per RECIST v1.1. The changes in tumor measurements that were confirmed by repeat assessments performed no less than 4 weeks after initial response are called confirmed responses. The CR was defined as disappearance of all target and non-target lesions and all pathological lymph nodes must have decreased to < 10 mm in short axis. The PR was defined as at least a 30% decrease in the sum of the longest diameters (LD) of target lesions taking as reference the baseline sum of LD. The PD was defined as at least 20% increase in the sum of LD of target lesions taking as reference the smallest sum of the LD recorded since the treatment started or the appearance of one or more new target and non-target lesions and/or unequivocal progression of existing non-target lesions.
Progression Free Survival (PFS) as Assessed by Investigator
The PFS was defined as the number of months from the date of first study drug administration to first PD or death. The PD was defined as at least 20% increase in the sum of longest diameters of target lesions taking as reference the smallest sum of the longest diameters recorded since the treatment started or the appearance of one or more new lesions. The PFS was estimated using Kaplan-Meier method.
Overall Survival (OS)
Overall survival was defined as the number of months from date of first study drug administration to death. The OS was estimated using Kaplan-Meier method.
Change in AXL Expression (Total Tumor H-score) From Baseline to EOT Visit for Expansion Part
Change in AXL expression (total humor H-score in membrane or cytoplasm) from Baseline to EOT visit for the expansion part is reported. The H-score captures both the intensity and proportion of AXL positive tumor cells and was defined by the formula: H-score = (1 × % 1+ tumor cells) + (2 × % 2+ tumor cells) + (3 × % 3+ tumor cells); where '1+' indicates weak staining intensity, '2+' indicates medium staining intensity, and '3+' indicates strong staining intensity. The H-score values ranges from 0 to 300. Lower H-scores represent lower AXL expression in the tumor sample, while higher scores represent stronger AXL expression in the tumor samples.

Full Information

First Posted
December 1, 2016
Last Updated
July 31, 2023
Sponsor
Genmab
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1. Study Identification

Unique Protocol Identification Number
NCT02988817
Brief Title
Enapotamab Vedotin (HuMax-AXL-ADC) Safety Study in Patients With Solid Tumors
Official Title
First-in-human, Open-label, Dose-escalation Trial With Expansion Cohorts to Evaluate Safety of Axl-specific Antibody-drug Conjugate (Enapotamab Vedotin, HuMax®-AXL-ADC) in Patients With Solid Tumors
Study Type
Interventional

2. Study Status

Record Verification Date
July 2023
Overall Recruitment Status
Completed
Study Start Date
November 23, 2016 (Actual)
Primary Completion Date
November 12, 2021 (Actual)
Study Completion Date
November 12, 2021 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Genmab

4. Oversight

Studies a U.S. FDA-regulated Drug Product
Yes
Data Monitoring Committee
Yes

5. Study Description

Brief Summary
The purpose of the trial is to determine the maximum tolerated dose and to establish the safety profile of HuMax-AXL-ADC in a mixed population of patients with specified solid tumors
Detailed Description
The trial consists of two parts; a dose escalation part (phase I, first in-human (FIH)) and an expansion part (phase IIa). The dose escalation part has 2 dosing schedules: 1 dose every 3 weeks (1Q3W) dose regimen, and 3 doses every 4 weeks (3Q4W) dosing regimen. The Expansion part of the trial will further explore the recommended phase 2 dose and dosing regimens of HuMax-AXL-ADC as determined in dose escalation part.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Ovarian Cancer, Cervical Cancer, Endometrial Cancer, Non Small Cell Lung Cancer (NSCLC), Thyroid Cancer, Melanoma, Sarcoma, Solid Tumors

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 1, Phase 2
Interventional Study Model
Sequential Assignment
Masking
None (Open Label)
Allocation
N/A
Enrollment
306 (Actual)

8. Arms, Groups, and Interventions

Arm Title
Enapotamab vedotin (HuMax-AXL-ADC)
Arm Type
Experimental
Arm Description
Participants in all cohorts of the trial (both in escalation and expansion phase) will be administered enapotamab vedotin (HuMax-AXL-ADC) intravenously (IV).
Intervention Type
Biological
Intervention Name(s)
Enapotamab vedotin (HuMax-AXL-ADC)
Intervention Description
Enapotamab vedotin (HuMax-AXL-ADC) will be administered intravenously.
Primary Outcome Measure Information:
Title
Number of Participants With Dose-limiting Toxicities (DLTs) for Dose-escalation Part
Description
The DLTs were defined as Grade (G) 4 neutropenia or G4 thrombocytopenia for a minimal duration of 7 days, G3 and G4 febrile neutropenia, >=G3 hemorrhage associated with >=G3 thrombocytopenia, G4 anemia; Stevens Johnson syndrome, toxic epidermal necrolysis, >=G3 cutaneous vasculitis; G3 neuropathy (not improved to G1 within 3 weeks following pausing of dosing) and G4 neuropathy; G3 infusion-related reactions (IRR) that did not resolve to G1 or baseline within 24 hours; G4 IRR or G4 anaphylaxis events; >= G3 diarrhoea and/or vomiting persisting >48 hours or G3 nausea lasting 7 days (both despite optimal medical management); or any >=G3 related non-hematological AEs, which occurred during the Cycle 1 and regarded as medically important as assessed by the Data Monitoring Committee (excluding Grade 3 fatigue or non-hematological laboratory abnormalities as specified in protocol).
Time Frame
From Day 1 to Day 21 of first cycle for 1Q3W dosing regimen and from Day 1 to Day 28 of first cycle for 3Q4W dosing regimen
Title
Number of Participants With Treatment-emergent Adverse Events (TEAEs) and Treatment-emergent Serious Adverse Events (TESAEs)
Description
An adverse event (AE) is any untoward medical occurrence in a participant who received study drug without regard to possibility of causal relationship. An SAE is defined as an AE that meets one of the following criteria: requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant incapacity or substantial disruption of the ability to conduct normal life functions, is a congenital anomaly/birth defect, is medically important, results in death, or is life-threatening. In this trial, a TEAE was defined as an AE occurring or worsening between the first dose of enapotamab vedotin and 30 days after the last dose received.
Time Frame
Day 1 through Day 1130 (maximum observed duration)
Title
Number of Participants With Treatment-emergent Infusion-related AEs and TEAEs Related to Enapotamab Vedotin
Description
Number of participants with treatment-emergent infusion-related AEs and TEAEs related to enapotamab vedotin is reported.
Time Frame
Day 1 through Day 1130 (maximum observed duration)
Title
Number of Participants With >= Grade 3 TEAEs as Assessed by National Cancer Institute - Common Terminology Criteria for Adverse Events (NCI-CTCAE) Version 4.03
Description
Number of participants with TEAEs of >= Grade 3 as assessed by NCI-CTCAE v4.03 is reported. The NCI-CTCAE is a descriptive terminology is used for AE reporting. The NCI-CTCAE v4.03 displays Grades 1 through 5 with unique clinical descriptions of severity for each AE, based on this general guideline: Grade 1 as mild AE, Grade 2 as moderate AE, Grade 3 as severe AE, Grade 4 as life-threatening or disabling AE, and Grade 5 as death. If a participant reported multiple severity grades for an AE, only the maximum grade was used.
Time Frame
Day 1 through Day 1130 (maximum observed duration)
Title
Number of Participants With Grade 3 or 4 Laboratory Results
Description
Number of participants with laboratory measurements graded as Grade 3 or 4 by NCI-CTCAE v 4.03 is reported.
Time Frame
Day 1 through Day 1130 (maximum observed duration)
Secondary Outcome Measure Information:
Title
Area Under the Plasma Concentration-time Curve From Time 0 to Infinity (AUC0-inf) of Conjugated Enapotamab Vedotin for 1Q3W Dose-escalation Part
Description
The AUC0-inf of conjugated enapotamab vedotin for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Time Frame
Predose, end of infusion (EOI), and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3
Title
Area Under the Plasma Concentration-time Curve From Time 0 to Last Measurable Concentration (AUC0-last) of Conjugated Enapotamab Vedotin for 1Q3W Dose-escalation Part
Description
The AUC0-last of conjugated enapotamab vedotin for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Time Frame
Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3
Title
Maximum Observed Plasma Concentration (Cmax) of Conjugated Enapotamab Vedotin for Dose-escalation Part
Description
The Cmax of conjugated enapotamab vedotin for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose and EOI on Days 1 and 8 of Cycles 1 and 3; and predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Total Clearance (CL) of Conjugated Enapotamab Vedotin in Dose-escalation Part
Description
The total CL of conjugated enapotamab vedotin in dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Time of Maximum Plasma Concentration (Tmax) of Conjugated Enapotamab Vedotin for Dose-escalation Part
Description
The Tmax of conjugated enapotamab vedotin for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Half-life Lambda-z (t1/2) of Conjugated Enapotamab Vedotin for Dose-escalation Part
Description
The t1/2 of conjugated enapotamab vedotin for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Volume of Distribution at Steady State (Vss) of Conjugated Enapotamab Vedotin for Dose-escalation Part
Description
The Vss of conjugated enapotamab vedotin for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
AUC0-inf of Free Toxin Monomethyl Auristatin E (MMAE) for 1Q3W Dose-escalation Part
Description
The AUC0-inf of MMAE for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Time Frame
Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3
Title
AUC0-last of MMAE for 1Q3W Dose-escalation Part
Description
The AUC0-last of MMAE for 1Q3W dose-escalation part is reported. Sample scheduling of the 3Q4W dosing regimen did not allow calculation of the specific outcome measure.
Time Frame
Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3
Title
Cmax of MMAE for Dose-escalation Part
Description
The Cmax of MMAE for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose and EOI on Days 1 and 8 of Cycles 1 and 3; and predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Total CL of MMAE in Dose-escalation Part
Description
The total CL of MMAE in dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Tmax of MMAE for Dose-escalation Part
Description
The Tmax of MMAE for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
t1/2 of MMAE for Dose-escalation Part
Description
The t1/2 of MMAE for dose-escalation part is reported.
Time Frame
For 1Q3W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 1 of Cycles 1 and 3; For 3Q4W dosing regimen: Predose, EOI, and 2 and 5 hours after EOI on Day 15 of Cycles 1 and 3
Title
Number of Participants With Antidrug Antibodies (ADAs) Confirmed Positive to Enapotamab Vedotin
Description
The ADA assessment was performed according to a tiered approach. First samples were screened for an ADA response; positively screened samples were analyzed in a confirmation method. Subsequently confirmed positive samples were analyzed for titre and the presence of neutralizing antibodies. Number of participants with ADA confirmed positive to enapotamab vedotin is reported.
Time Frame
Day 1 through Day 1130 (Dose-escalation part: Predose of Day 1 of Cycles 1 to 12, end of treatment [EOT], and 30 days after last study drug; Expansion part: Predose on Day 1 of Cycles 1 to 5, then every fourth cycle until PD)
Title
Number of Participants With Objective Response (OR) Based on Response Evaluation Criteria in Solid Tumors Version 1.1 (RECIST v1.1) As Assessed by Investigator
Description
Radiological evaluation based on RECIST v1.1 was performed by the investigator using computed tomography (CT) scans/ magnetic resonance imaging (MRI) scans/ positron emission tomography (PET) scans. The OR was defined as confirmed CR or confirmed PR per RECIST v1.1. The changes in tumor measurements that were confirmed by repeat assessments performed no less than 4 weeks after initial response are called confirmed responses. The CR was defined as disappearance of all target and non-target lesions and all pathological lymph nodes must have decreased to < 10 mm in short axis. The PR was defined as at least a 30% decrease in the sum of the longest diameters (LD) of target lesions taking as reference the baseline sum of LD.
Time Frame
Day 1 through 44.5 months (maximum observed duration)
Title
Number of Participants With Best Cancer Antigen 125 (CA-125) Response
Description
The best CA-125 response was evaluated in participants with ovarian cancer. A CA-125 partial response was defined as at least a 50% reduction in CA-125 levels in blood from a pretreatment sample. Participants who had a CA-125 partial response and had CA-125 level falls to within the reference range (0-35 units/mL) were classified as CA-125 complete responders. The response was confirmed and maintained for at least 28 days. The best overall response (CA-125 partial response and CA-125 complete response) is reported.
Time Frame
From Screening (within 2 weeks before starting of the study treatment) through Day 1130 (maximum observed duration)
Title
Duration of Response (DoR) Based on RECIST v1.1 as Assessed by Investigator for Expansion Part
Description
The DoR was defined as the number of months from the first documentation of objective tumor response (CR or PR) to the date of first progressive disease (PD) or death. The OR was defined as confirmed CR or confirmed PR per RECIST v1.1. The changes in tumor measurements that were confirmed by repeat assessments performed no less than 4 weeks after initial response are called confirmed responses. The CR was defined as disappearance of all target and non-target lesions and all pathological lymph nodes must have decreased to < 10 mm in short axis. The PR was defined as at least a 30% decrease in the sum of the longest diameters (LD) of target lesions taking as reference the baseline sum of LD. The PD was defined as at least 20% increase in the sum of LD of target lesions taking as reference the smallest sum of the LD recorded since the treatment started or the appearance of one or more new target and non-target lesions and/or unequivocal progression of existing non-target lesions.
Time Frame
Day 1 through 44.5 months (maximum observed duration)
Title
Progression Free Survival (PFS) as Assessed by Investigator
Description
The PFS was defined as the number of months from the date of first study drug administration to first PD or death. The PD was defined as at least 20% increase in the sum of longest diameters of target lesions taking as reference the smallest sum of the longest diameters recorded since the treatment started or the appearance of one or more new lesions. The PFS was estimated using Kaplan-Meier method.
Time Frame
Day 1 through 44.5 months (maximum observed duration)
Title
Overall Survival (OS)
Description
Overall survival was defined as the number of months from date of first study drug administration to death. The OS was estimated using Kaplan-Meier method.
Time Frame
Day 1 through 44.5 months (maximum observed duration)
Title
Change in AXL Expression (Total Tumor H-score) From Baseline to EOT Visit for Expansion Part
Description
Change in AXL expression (total humor H-score in membrane or cytoplasm) from Baseline to EOT visit for the expansion part is reported. The H-score captures both the intensity and proportion of AXL positive tumor cells and was defined by the formula: H-score = (1 × % 1+ tumor cells) + (2 × % 2+ tumor cells) + (3 × % 3+ tumor cells); where '1+' indicates weak staining intensity, '2+' indicates medium staining intensity, and '3+' indicates strong staining intensity. The H-score values ranges from 0 to 300. Lower H-scores represent lower AXL expression in the tumor sample, while higher scores represent stronger AXL expression in the tumor samples.
Time Frame
Baseline (Study Days -21 to 1) and EOT visit (Day 1100)

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: For the dose escalation part: Patients with selected, relapsed or refractory solid tumors who have failed available standard therapy or who are not candidates for standard therapy. For the expansion part: Patients with advanced and/or metastatic solid tumors who are not candidates for standard therapy Patients must have measurable disease according to Response Evaluation Criteria In Solid Tumors (RECIST). For the expansion patients must provide a tumor tissue sample from archival tissue or fresh biopsy at enrolment Age ≥ 18 years. Acceptable renal function Acceptable liver function Acceptable hematological status Have an Eastern Cooperative Oncology Group (ECOG) performance status of 0 or 1. Life expectancy of at least three months. Patients, both females and males, of childbearing/reproductive potential must agree to use adequate contraception while included in the trial and for six months after the last infusion of HuMax-AXL-ADC Patients must provide a signed informed consent form before any trial relates activities are carried out. Exclusion Criteria: Acute deep vein thrombosis or clinically relevant pulmonary embolism, not stable for at least 4 weeks prior to first IMP administration. Have clinically significant cardiac disease Known congestive heart failure and/ or a known decreased cardiac ejection fraction of < 45%. A baseline QT interval as corrected by Fridericia's formula (QTcF) > 480 msec, a complete left bundle branch block (defined as a QRS interval ≥ 120 msec in left bundle branch block form) or an incomplete left bundle branch block. Uncontrolled hypertension Have received granulocyte colony stimulating factor (G-CSF) or granulocyte/macrophage colony stimulating factor support 3 weeks prior to first IMP administration. Have received a cumulative dose of corticosteroid > 150 mg prednisone (or equivalent doses of corticosteroids) within two weeks before the first Investigational Medicinal Product (IMP) administration. History of ≥ grade 3 allergic reactions to monoclonal antibody therapy as well as known or suspected allergy or intolerance to any agent given in the course of this trial. Major surgery within four weeks before first IMP administration. Any history of intracerebral arteriovenous malformation, cerebral aneurysm, brain metastases or stroke. Any anticancer therapy including; small molecules, immunotherapy, chemotherapy monoclonal antibodies or any other experimental drug within five half-lives but maximum four weeks before first infusion. Accepted exceptions are bisphosphonates, denosumab and gonadotropin-releasing hormone agonist or antagonist. Prior therapy with a conjugated or unconjugated auristatin derivative/vinca-binding site targeting payload. Radiotherapy within 14 days prior to first IMP administration. Known past or current malignancy other than inclusion diagnosis, except for: Cervical carcinoma of Stage 1B or less. Non-invasive basal cell or squamous cell skin carcinoma. Non-invasive, superficial bladder cancer. Prostate cancer with a current prostate specific antigen (PSA) level < 0.1 ng/mL. Breast cancer in BRCA1 or BRCA2 positive ovarian cancer patients. Any curable cancer with a complete response (CR) of > 2 years duration. Melanoma patients with an lactate dehydrogenase (LDH) ≥ 3 x upper limit normal (ULN). Ongoing significant, uncontrolled medical condition including: o Serious, non-healing wound, skin ulcer (of any grade), or bone fracture. Grade 2 or higher peripheral neuropathy. Clinically significant active viral, bacterial or fungal infection Known human immunodeficiency virus seropositivity. Known positive serology for hepatitis B (unless due to vaccination or passive immunization due to immunoglobulin therapy) Known positive serology for hepatitis C (unless due to immunoglobulin therapy) Substance abuse, medical, psychological or social conditions that may interfere with the patient's participation in the trial or evaluation of the trial result History of organ allograft (except for corneal transplant) or autologous or allogeneic bone marrow transplant, or stem cell rescue within 3 months prior to the first dose of IMP Body weight < 40 kg Women who are pregnant or breast feeding. Pulmonary hemorrhage or hemoptysis > 2.5 ml blood within 6 weeks unless cause has been addressed and is medically resolved. History of acute pneumonitis.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Ignace Vergote, Professor
Organizational Affiliation
Universitair Ziekenhuizen Leuven
Official's Role
Principal Investigator
Facility Information:
Facility Name
Mayo Clinic - Phoenix
City
Phoenix
State/Province
Arizona
ZIP/Postal Code
85054
Country
United States
Facility Name
University of Colorado Hospital
City
Aurora
State/Province
Colorado
ZIP/Postal Code
80045
Country
United States
Facility Name
Yale University, Smilow Cancer Center at Yale New Haven Hospital
City
New Haven
State/Province
Connecticut
ZIP/Postal Code
06520
Country
United States
Facility Name
Mayo Clinic Jacksonville
City
Jacksonville
State/Province
Florida
ZIP/Postal Code
32224
Country
United States
Facility Name
Moffitt Cancer Center
City
Tampa
State/Province
Florida
ZIP/Postal Code
33612
Country
United States
Facility Name
Emory University School of Medicine, Winship Cancer Institute
City
Atlanta
State/Province
Georgia
ZIP/Postal Code
30322
Country
United States
Facility Name
University of Iowa
City
Iowa City
State/Province
Iowa
ZIP/Postal Code
52242
Country
United States
Facility Name
Dana-Farber Cancer Institute
City
Boston
State/Province
Massachusetts
ZIP/Postal Code
02115
Country
United States
Facility Name
University of Michigan Comprehensive Cancer Center
City
Ann Arbor
State/Province
Michigan
ZIP/Postal Code
48109
Country
United States
Facility Name
Mayo Clinic Rochester
City
Rochester
State/Province
Minnesota
ZIP/Postal Code
55905
Country
United States
Facility Name
Washington University
City
Saint Louis
State/Province
Missouri
ZIP/Postal Code
63110
Country
United States
Facility Name
Roswell Park Comprehensive Cancer Center
City
Buffalo
State/Province
New York
ZIP/Postal Code
14263
Country
United States
Facility Name
Laura and Isaac Perlmutter Cancer Center at NYU Langone
City
New York
State/Province
New York
ZIP/Postal Code
10016
Country
United States
Facility Name
Herbert Irving Comprehensive Cancer Center
City
New York
State/Province
New York
ZIP/Postal Code
10034
Country
United States
Facility Name
Duke Cancer Institute
City
Durham
State/Province
North Carolina
ZIP/Postal Code
27710
Country
United States
Facility Name
Fox Chase Cancer Center
City
Philadelphia
State/Province
Pennsylvania
ZIP/Postal Code
19111
Country
United States
Facility Name
Mary Crowley Cancer Research Center
City
Dallas
State/Province
Texas
ZIP/Postal Code
75230
Country
United States
Facility Name
University of Texas MD Anderson Cancer Center
City
Houston
State/Province
Texas
ZIP/Postal Code
77030
Country
United States
Facility Name
University of Utah Huntsman Cancer Institute
City
Salt Lake City
State/Province
Utah
ZIP/Postal Code
84112
Country
United States
Facility Name
University of Wisconsin Carbone Cancer Center
City
Madison
State/Province
Wisconsin
ZIP/Postal Code
53792
Country
United States
Facility Name
Universitair Ziekenhuizen Leuven
City
Leuven
State/Province
Flemish Brabant
ZIP/Postal Code
3000
Country
Belgium
Facility Name
Institut Roi Albert II - Cliniques Universitaires Saint Luc
City
Bruxelles
ZIP/Postal Code
1200
Country
Belgium
Facility Name
Universitair Ziekenhuis Brussel - Oncologisch Centrum
City
Jette
ZIP/Postal Code
1090
Country
Belgium
Facility Name
Medische oncologie, Oncologisch Centrum - AZ Groeninge
City
Kortrijk
ZIP/Postal Code
8500
Country
Belgium
Facility Name
U.Z. Leuven Gasthuisberg, Department of General Medical Oncology
City
Leuven
ZIP/Postal Code
3000
Country
Belgium
Facility Name
CHU de Liège, Medical Oncology et. Domaine Universitaire du Sart Tilman
City
Liege
ZIP/Postal Code
4000
Country
Belgium
Facility Name
Rigshospitalet, Copenhagen University Hospital
City
Copenhagen
ZIP/Postal Code
DK-2100
Country
Denmark
Facility Name
The Netherlands Cancer Institute - Antoni van Leeuwenhoek Hospital
City
Amsterdam
ZIP/Postal Code
1066
Country
Netherlands
Facility Name
Leiden University Medical Centre
City
Leiden
ZIP/Postal Code
2333
Country
Netherlands
Facility Name
Erasmus MC, Medical Oncology
City
Rotterdam
ZIP/Postal Code
3015
Country
Netherlands
Facility Name
UMC Utrecht Cancer Center
City
Utrecht
ZIP/Postal Code
3584
Country
Netherlands
Facility Name
Hospital Unversitario Vall D'hebron
City
Barcelona
ZIP/Postal Code
08035
Country
Spain
Facility Name
Oncologia Mèdica/ Medical Oncology Department Institut Catalá d'Oncologia (ICO)
City
Barcelona
ZIP/Postal Code
08909
Country
Spain
Facility Name
University Hospital of Girona
City
Girona
ZIP/Postal Code
17007
Country
Spain
Facility Name
Hospital Universitario 12 Octubre Servicio de Oncologia Medica
City
Madrid
ZIP/Postal Code
28041
Country
Spain
Facility Name
Hospital Virgen de la Victoria
City
Málaga
ZIP/Postal Code
29016
Country
Spain
Facility Name
University Hospital Lozano Blesa, Aragón Health Research Institute (IIS Aragón)
City
Zaragoza
ZIP/Postal Code
50009
Country
Spain
Facility Name
University College London Hospitals
City
London
ZIP/Postal Code
NW1 2PG
Country
United Kingdom
Facility Name
The Christie NHS Foundation Trust Clinical Trials Unit
City
Manchester
ZIP/Postal Code
M20 4BX
Country
United Kingdom
Facility Name
Sir Bobby Robson Clinical Trials Unit at the Northern Centre for Cancer Care, Freeman Hospital
City
Newcastle
ZIP/Postal Code
NE7 7DN
Country
United Kingdom
Facility Name
The Royal Marsden Hospital
City
Sutton
ZIP/Postal Code
SM2 5PT
Country
United Kingdom

12. IPD Sharing Statement

Learn more about this trial

Enapotamab Vedotin (HuMax-AXL-ADC) Safety Study in Patients With Solid Tumors

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