MGD019 DART® Protein in Unresectable/Metastatic Cancer

• ClinicalTrials.gov Identifier: NCT03761017
• Recruitment Status: Active, not recruiting
• First Posted: December 3, 2018
• Last Update Posted: February 14, 2024
• Sponsor: MacroGenics
• Information provided by (Responsible Party): MacroGenics

Study Description

Brief Summary:

The purpose of this study is to evaluate the safety and tolerability, pharmacokinetics (PK) pharmacodynamics and preliminary antitumor activity of lorigerlimab.

This Phase 1, open-label study will characterize safety, dose-limiting toxicities (DLTs), and maximum tolerated/administered dose (MTD/MAD) of MGD019. Dose escalation will occur in a 3+3+3 design in patients with advanced solid tumors of any histology. Once the MTD/MAD is determined, a Cohort Expansion Phase will be enrolled to further characterize safety and initial anti-tumor activity in patients with specific tumor types anticipated to be sensitive to dual checkpoint blockade.

Condition or disease	Intervention/treatment	Phase
Squamous Cell Non Small Cell Lung Cancer; Prostate Cancer Metastatic; Cutaneous Melanoma; Colorectal Cancer; Advanced Cancer; Solid Tumor, Adult	Biological: Lorigerlimab	Phase 1

Study Design

• Study Type: Interventional (Clinical Trial)
• Actual Enrollment: 162 participants
• Allocation: Non-Randomized
• Intervention Model: Sequential Assignment
• Masking: None (Open Label)
• Primary Purpose: Treatment
• Official Title: A Phase 1, First-in-Human, Open-Label, Dose Escalation and Cohort Expansion Study of MGD019, a Bispecific DART® Protein Binding PD-1 and CTLA-4 in Patients With Unresectable or Metastatic Neoplasms
• Actual Study Start Date: December 12, 2018
• Estimated Primary Completion Date: July 2024
• Estimated Study Completion Date: December 2024

Arms and Interventions

Arm	Intervention/treatment
Experimental: Cohort 1; 0.03 mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019
Experimental: Cohort 2; 0.1 mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019
Experimental: Cohort 3; 0.3 mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019
Experimental: Cohort 4; 1.0 mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019
Experimental: Cohort 5; 30. mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019
Experimental: Cohort 6; 6.0 mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019
Experimental: Cohort 7; 10.0 mg/kg administered IV every 3 weeks.	Biological: Lorigerlimab; Bispecific DART protein binding PD-1 and CTLA-4; Other Name: MGD019

Outcome Measures

Primary Outcome Measures :

1. Incidence of treatment-emergent adverse events [ Time Frame: 30 days after last dose ]
   Safety is based on evaluation of adverse events (AEs) and serious adverse events (SAEs) from the time of study drug administration through the End of Study visit.

Secondary Outcome Measures :

1. Cmax [ Time Frame: up to 108 weeks ]
   Maximum Plasma Concentration of lorigerlimab
2. Tmax [ Time Frame: up to 108 weeks ]
   Time to reach maximum (peak) plasma concentration of lorigerlimab
3. AUC [ Time Frame: up to 108 weeks ]
   Area Under the Plasma Concentration versus Time Curve of lorigerlimab
4. Ctrough [ Time Frame: up to 108 weeks ]
   Trough plasma concentration of lorigerlimab
5. CL [ Time Frame: up to 108 weeks ]
   Total body clearance of the drug from plasma of lorigerlimab
6. Vss [ Time Frame: up to 108 weeks ]
   Apparent volume of distribution at steady state of lorigerlimab
7. t1/2 [ Time Frame: up to 108 weeks ]
   Terminal half life of lorigerlimab
8. Percent of patients with anti-drug antibodies against lorigerlimab [ Time Frame: up to 108 weeks ]
   Immunogenicity
9. Objective response rate (ORR) [ Time Frame: Every 12 weeks, up to 4 years ]
   The number of participants who have a complete response (CR) or partial response (PR) to treatment. Efficacy assessed using conventional Response Evaluation Criteria in Solid Tumors version 1.1 (RECIST v1.1)
10. Duration of Response (DoR) [ Time Frame: Every 12 weeks until withdrawal of consent, lost to follow up, death, or end of the study, up to 4 years ]
    DoR is defined as the time from the date of initial response (CR or PR) to the date of first documented PD or death from any cause, whichever occurs first
11. Progression free survival (PFS) [ Time Frame: Tumor status assessed every 12 weeks. Survival status is assessed approximately every 12 weeks after the last dose of study treatment until withdrawal of consent, lost to follow up, death, or end of the study, up to 4 years ]
    PFS is defined as the time from the first dose date to the date of first documented PD or death from any cause, whichever occurs first.
12. Overall survival (OS) [ Time Frame: OS status is assessed approximately every 12 weeks after the last dose of study treatment until withdrawal of consent, lost to follow up, death, or end of the study, up to 4 years ]
    OS is defined as the time from the first dose date to the date of death from any cause.
13. Prostate specific antigen (PSA) response rate in mCRPC [ Time Frame: Every 3 weeks on treatment, then every 3 months up to 2 years post last treatment ]
    Percent of patients with 50% or more decline in PSA and confirmed 3 weeks later
14. Best PSA percent change in mCRPC [ Time Frame: Every 3 weeks on treatment, then every 3 months up to 2 years post last treatment ]
    Best percent change in PSA from baseline
15. Duration of PSA response [ Time Frame: Every 3 weeks on treatment, then every 3 months up to 2 years post last treatment ]
    Time from PSA response to time of PSA progression
16. Radiographic progression-free survival (PFS) in metastatic castration-resistant prostate cancer (mCRPC) [ Time Frame: up to 2 years post last treatment ]
    Time from first dose to first occurrence of radiographic progression, or death
17. Time to PSA progression in mCRPC [ Time Frame: PSA is assessed every 3 weeks while on treatment, every 3 months for up to 2 years post-treatment ]
    The time from the first dose of MGD019 to the first documented PSA progression. PSA progression is defined as an increase that is ≥ 25% and ≥ 2 ng/mL the baseline or lowest value observed, and which confirmed by a second value at least 3 weeks later

Eligibility Criteria

• Ages Eligible for Study: 18 Years and older (Adult, Older Adult)
• Sexes Eligible for Study: All
• Accepts Healthy Volunteers: No

Criteria

Inclusion Criteria:

• Dose escalation: Patients with histologically proven, unresectable, locally advanced or metastatic solid tumors for whom no approved therapy with demonstrated clinical benefit is available or patients who are intolerant to standard therapy.
• Cohort Expansion Phase:

• Checkpoint inhibitor-naïve squamous cell NSCLC, including:

  1. Patients that have progressed during or following treatment with platinum-based chemotherapy for advanced disease. Patients harboring an activating epidermal growth factor receptor (EGFR) mutation or anaplastic lymphoma kinase (ALK) rearrangement must have progressed following at least one available EGFR or ALK targeted therapy. ROS1 rearrangement or BRAF mutation must have progressed following at least 1 available EGFR (including osimertinib for EGFR T790M-mutated NSCLC), ALK, ROS1 or BRAF targeted therapy, respectively
  2. Patients that have progressed during or following treatment with platinum-based chemotherapy for advanced disease and patients with previously untreated squamous cell NSCLC without activating mutations for whom checkpoint inhibitor therapy is not approved or available.
• Advanced non-microsatellite instability-high colorectal cancer (CRC) with recurrence, progression, or intolerance to standard therapy consisting of at least 2 prior standard regimens. CRC harboring an activating EGFR mutation must have progressed during or following at least one available EGFR targeted therapy. Patients who are inappropriate candidates for or have refused treatment with these regimens are also eligible. Patients should have received no more than 4 prior lines of systemic therapy.
• Checkpoint inhibitor-naïve mCRPC that has progressed during or following no more than 2 prior lines of an androgen receptor antagonist or androgen synthesis inhibitor (e.g., enzalutamide or abiraterone, respectively), if approved and available, with a PSA value of at least 2 ng/mL and meeting at least one of the following:
• Progression in measurable disease (RECIST v1.1).
• Appearance of 2 or more new bone lesions according to Prostate Cancer Working Group 2 (PCWG-2).
• Rising PSA defined as at least two sequential rises in PSA.
• Eligible patients may have received prior chemotherapy (i.e. docetaxel), and patients with known homologous recombination (HRR) pathway gene alterations must have received the applicable approved therapy (e.g. olaparib).
• Cutaneous melanoma that has progressed during or following systemic treatment for unresectable, locally advanced, or metastatic disease. Patients will have received PD-(L)1 and/or CTLA-4 pathway inhibitors where available and indicated.
• Eastern Cooperative Oncology Group (ECOG) performance status of 0-1
• Life expectancy ≥ 12 weeks.
• Measurable disease as per RECIST 1.1 for the purpose of response assessment must either (a) not reside in a field that has been subjected to prior radiotherapy or (b) have demonstrated clear evidence of radiographic progression since the completion of prior radiotherapy and prior to study enrollment.
• All patients must have an identified formalin-fixed, paraffin embedded (FFPE) tumor specimen (up to 20 slides or a block) for immunohistochemical evaluation of pharmacodynamic markers of interest. Patients may undergo a fresh tumor biopsy during the screening period if a tumor sample is not available. Patients in the mCRPC expansion cohort with bone only disease not amenable to fresh biopsy may be eligible in consultation with the Sponsor.
• Acceptable laboratory parameters and adequate organ reserve.

Exclusion Criteria:

• In patients who have previously received an immune checkpoint inhibitor (e.g., anti-PD-L1, anti-PD-1, anti-CTLA-4), toxicities related to the checkpoint inhibitor must have resolved to ≤ Grade 1 or baseline. Patients with well controlled immune endocrinopathies secondary to prior checkpoint therapy are eligible.
• Patients with symptomatic CNS metastases. Patients with history of prior CNS metastasis must have been treated, must be asymptomatic, and must not have concurrent treatment for the CNS disease, progression of CNS metastases on magnetic resonance imaging (MRI) or computed tomography (CT) for at least 14 days after last day of prior therapy for the CNS metastases, or concurrent leptomeningeal disease or cord compression.
• Patients who sustained the following Grade 3 immune checkpoint inhibitor related AEs are ineligible: Ocular AE, changes in liver function tests that met the criteria for Hy's law (> 3 × ULN of either ALT or AST with concurrent > 2 × ULN of total bilirubin and without alternate etiology), neurologic toxicity, colitis, renal toxicity, pneumonitis.
• Patients who have received prior therapy with a combination of monoclonal antibodies against PD-1/PD-L1 and CTLA-4 will be excluded in the Cohort Expansion (this does not apply to the melanoma expansion cohort).
• Patients with any history of known or suspected autoimmune disease with certain exceptions
• History of prior allogeneic bone marrow, stem-cell, or solid organ transplantation.
• History of trauma or major surgical procedure within 4 weeks prior to initiation of study drug administration.
• Systemic antineoplastic therapy, or investigational therapy (for all tumor types) or androgen receptor antagonist/androgen synthesis inhibitor for mCRPC (e.g., enzalutamide or abiraterone, respectively) within the 4 weeks prior to initiation of study drug administration.
• Treatment with radiation therapy within 2 weeks prior to initiation of study drug administration.
• Radioligand (e.g., radium-223) within 6 months prior to initiation of study drug administration for mCRPC in the Cohort Expansion Phase.
• Serum testosterone > 50 ng/dl or > 1.7 nmol/L for mCRPC in the Cohort Expansion Phase.
• Confirmed or presumed COVID-19/SARS-CoV-2 infection. While SARS-CoV-2 testing is not mandatory for study entry, testing should follow local clinical practice guidelines/standards. Patients with a positive test result for SARS-CoV-2 infection, known asymptomatic infection, or presumed infection are excluded. Patients may be considered eligible after a resolved SARS-CoV-2 infection once he or she remains afebrile for at least 72 hours and after other SARS-CoV-2-related symptoms have fully recovered to baseline for a minimum of 72 hours

Contacts and Locations

Locations

United States, Illinois

University of Chicago Medical Center

Chicago, Illinois, United States, 60637

United States, Massachusetts

Beth Israel Deaconess Medical Center

Boston, Massachusetts, United States, 02215

Dana Farber Cancer Institute

Boston, Massachusetts, United States, 02215

Massachusetts General Hospital

Boston, Massachusetts, United States, 02215

United States, Michigan

START Midwest

Grand Rapids, Michigan, United States, 49546

United States, Nebraska

Oncology Hematology West p.c. dba Nebraska Cancer Specialists

Grand Island, Nebraska, United States, 68803

Nebraska Cancer Specialists

Omaha, Nebraska, United States, 68130

United States, Oregon

Providence Portland Medical Center

Portland, Oregon, United States, 97213

United States, Pennsylvania

UPMC Hillman Cancer Center

Camp Hill, Pennsylvania, United States, 17011

UPMC Hillman Cancer Center

Carlisle, Pennsylvania, United States, 17015

UPMC Hillman Cancer Center

Erie, Pennsylvania, United States, 16505

UPMC Pinnacle Harrisburg

Harrisburg, Pennsylvania, United States, 17101

UPMC Pinnacle - Community Osteopathic Medical Sciences Pavilion (MSP)

Harrisburg, Pennsylvania, United States, 17109

UPMC Pinnacle - Ortenzio Cancer Center (OCC)

Mechanicsburg, Pennsylvania, United States, 17050

UPMC Hillman Cancer Center

Pittsburgh, Pennsylvania, United States, 20850

UPMC Hillman Cancer Center at UPMC Memorial

York, Pennsylvania, United States, 17408

United States, Tennessee

The Sarah Cannon Research Institute / Tennessee Oncology

Nashville, Tennessee, United States, 37203

Bulgaria

Complex Oncology Center - Burgas" EOOD, Department of Medical Oncology

Burgas, Bulgaria, 8000

Multiprofile Hospital for Active Treatment-Uni Hospital

Panagyurishte, Bulgaria

Multiprofile Hospital for Active Treatment "Heart and Brain"" EAD, Clinic of Medical Oncology

Pleven, Bulgaria

Complex Oncology Center - Ruse EOOD

Ruse, Bulgaria, 7002

Poland

University Clinical Centre, Early Clinical Trials Unit

Gdańsk, Poland, 80-214

Pratia MCM Krakow

Kraków, Poland

Europejskie Centrum Zdrowia Otwock

Otwock, Poland, 05-400

Med-Polonia Sp. z.o.o.

Poznań, Poland, 60-693

LUX MED Onkologia Sp. z.o.o.

Warszawa, Poland, 01-748

Narodowy Instytut Onkologii im

Warszawa, Poland, 02-781

Mazovian Onkological Hospital

Wieliszew, Poland

Spain

ICO Badalona / Hospital Universitari Germans Trias i Pujol

Badalona, Barcelona, Spain, 08916

Hospital Ruber Internacional

Madrid, Spain, 20834

Hospital Universitario La Princesa

Madrid, Spain, 28006

Ukraine

Communal Non-profit Enterprise "City Clinical Hospital #4" of Dnipro

Dnipro, Ukraine

Communal Non-Profit Enterprise "Regional Center of Oncology", Oncosurgical Department of Head and Neck

Kharkiv, Ukraine

Communal Nonprofit Enterprise "Regional Clinical Oncology Center of Kirovohrad Regional Council"

Kirovohrad, Ukraine

Kyiv City Clinical Oncological Centre

Kyiv, Ukraine

National Cancer Institute of Ukraine

Kyiv, Ukraine

Sumy Clinical Oncological Hospital

Sumy, Ukraine

Communal Nonprofit Enterprise "Podilsky Regional Center of Oncology"

Vinnytsia, Ukraine

Sponsors and Collaborators

MacroGenics

Investigators

• Study Director: Denise Casey, MD; MacroGenics

More Information

Additional Information:

Link to published 2020 manuscript 

Publications:

Berezhnoy A, Sumrow BJ, Stahl K, Shah K, Liu D, Li J, Hao SS, De Costa A, Kaul S, Bendell J, Cote GM, Luke JJ, Sanborn RE, Sharma MR, Chen F, Li H, Diedrich G, Bonvini E, Moore PA. Development and Preliminary Clinical Activity of PD-1-Guided CTLA-4 Blocking Bispecific DART Molecule. Cell Rep Med. 2020 Dec 22;1(9):100163. doi: 10.1016/j.xcrm.2020.100163. eCollection 2020 Dec 22.

• Responsible Party: MacroGenics
• ClinicalTrials.gov Identifier: NCT03761017
• Other Study ID Numbers: CP-MGD019-01
• First Posted: December 3, 2018
• Last Update Posted: February 14, 2024
• Last Verified: February 2024

Individual Participant Data (IPD) Sharing Statement:

• Plan to Share IPD: No

• Studies a U.S. FDA-regulated Drug Product: Yes
• Studies a U.S. FDA-regulated Device Product: No

Additional relevant MeSH terms:

Melanoma; Melanoma, Cutaneous Malignant; Neoplasms by Site; Neoplasms; Neuroendocrine Tumors; Neuroectodermal Tumors; Neoplasms, Germ Cell and Embryonal; Neoplasms by Histologic Type; Neoplasms, Nerve Tissue; Nevi and Melanomas; Skin Neoplasms; Skin Diseases