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NCT04015700 Clinical Trial

Neoantigen-based Personalized DNA Vaccine in Patients With Newly Diagnosed, Unmethylated Glioblastoma

Glioblastoma Clinical Trial

Official title:
A Pilot Study to Assess the Safety, Feasibility, and Immunogenicity of a Neoantigen-based Personalized in Patients With Newly Diagnosed, Unmethylated Glioblastoma

Clinical Trial Details — Status: Active, not recruiting

Administrative data
NCT number NCT04015700
Other study ID # 202003072
Secondary ID
Status Active, not recruiting
Phase Phase 1
First received
Last updated
Start date July 14, 2020
Est. completion date December 31, 2024

Study information
Verified date March 2024
Source Washington University School of Medicine
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a single institution, open-label, single arm, study assessing the safety, feasibility, and immunogenicity of a personalized neoantigen-based vaccine in subjects with newly diagnosed, unmethylated glioblastoma.

Recruitment information / eligibility
Status Active, not recruiting
Enrollment 9
Est. completion date December 31, 2024
Est. primary completion date May 13, 2022
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Newly diagnosed histologically confirmed MGMT unmethylated glioblastoma multiforme (WHO grade IV). Patients with secondary glioblastoma, in particular those who are IDH1 or IDH2 mutant, will not be excluded. High grade gliomas with molecular features of glioblastoma will be included. MGMT methylation status must be confirmed by standard a PCR-based assay. - Patients who had prior craniotomy with biopsy, subtotal resection, total gross resection, or re-resection will be permitted. - Consent to genome sequencing and dbGaP-based data sharing and has provided or will provide germline (PBMC) and tumor DNA/RNA samples of adequate quality for sequencing. (Acquisition of specimens for sequencing and the sequencing itself may be done as part of routine care or another research project.) - At least 18 years of age. - Karnofsky performance status = 60% - Normal bone marrow and organ function as defined below: - Absolute neutrophil count = 1,500/mcL - Platelets = 100,000/mcL - Total bilirubin = 1.5 x IULN - AST(SGOT)/ALT(SGPT) = 3.0 x IULN - Creatinine = IULN OR creatinine clearance = 60 mL/min/1.73 m2 for patients with creatinine levels above institutional normal - Systemic corticosteroid therapy is permitted provided dosing is no greater than 4 mg per day (dexamethasone or equivalent) on the day of vaccine administration. - Bevacizumab will be allowed if given for symptomatic control of vasogenic edema and to avoid high dose of corticosteroids. - Women of childbearing potential and men must agree to use adequate contraception (hormonal or barrier method of birth control, abstinence) prior to study entry and for the duration of study participation, including at least 5 months (for women of childbearing potential) and at least 7 months (for men) after last dose of study drug. Should a woman become pregnant or suspect she is pregnant while participating in this study, she must inform her treating physician immediately. - Ability to understand and willingness to sign an IRB approved written informed consent document (or that of legally authorized representative, if applicable). Exclusion Criteria: - As this study aims to assess the immunogenicity of personalized neoantigen DNA vaccine plus plasmid encoded IL-12 as an adjuvant, no prior immunotherapy will be permitted. - Inadequate tissue acquisition to allow for neoantigen screening. - No candidate neoantigen identified during screening. - A history of other malignancy = 3 years previous with the exception of non-melanoma skin cancer, any in situ cancer that has been successfully resected and cured, treated superficial bladder cancer, or any early-stage solid tumor that was successfully resected without need for adjuvant radiation or chemotherapy. - Receiving any other investigational agents within 4 weeks of beginning study treatment. - Known allergy, or history of serious adverse reaction to, vaccines such as anaphylaxis, hives, or respiratory difficulty. - A history of allergic reactions attributed to compounds of similar chemical or biologic composition to any agents used in the study. - Uncontrolled intercurrent illness including, but not limited to, ongoing or active infection, symptomatic congestive heart failure, unstable angina pectoris, cardiac arrhythmia, or psychiatric illness/social situations that would limit compliance with study requirements. - History of immunodeficiency disorder or autoimmune condition requiring active immunosuppressive therapy. This includes inflammatory bowel disease, ulcerative colitis, Crohn's disease, systemic vasculitis, scleroderma, psoriasis, multiple sclerosis, hemolytic anemia, immune-mediated thrombocytopenia, rheumatoid arthritis, systemic lupus erythematosus, Sjögren's syndrome, sarcoidosis, or other rheumatologic disease or any other medical condition or use of medication which might make it difficult for the patient to complete the full course of treatments or to generate an immune response to vaccines. - Presence of clinically significant increased intracranial pressure (e.g. impending herniation) or hemorrhage, uncontrolled seizures, or requirement for immediate palliative treatment. - Pregnant and/or breastfeeding. Women of childbearing potential must have a negative pregnancy test within 7 days of first dose of vaccine. - Presence of acute or chronic bleeding or clotting disorder that would contraindicate IM injections - Fewer than 2 acceptable sites available for IM injection and CELLECTRA® 2000 EP considering the deltoid and anterolateral quadriceps muscles: - Tattoos, keloids, or hypertrophic scars located within 2 cm of intended administration site - Implantable-cardioverter-defibrillator (ICD) or pacemaker (to prevent a life-threatening arrhythmia) that is located ipsilateral to the deltoid injection site (unless deemed acceptable by a cardiologist) - Any metal implants or implantable medical device within the intended treatment site (i.e. electroporation area).

Study Design

Related Conditions & MeSH terms

Intervention

Biological:
Personalized neoantigen DNA vaccine supplied by Geneos Therapeutics
-The neoantigen DNA vaccines are also known as DNA plasmid vector expressing tumor-specific antigens.
Device:
CELLECTRA®2000 EP Device supplied by Geneos Therapeutics
CELLECTRA® 2000 Device is a system indicated for use to enhance the uptake and expression of plasmid-based biologics in order to enhance vaccine efficacy.
Drug:
Plasmid encoded IL-12
The INO-9012 vials will be supplied by Geneos Therapeutics

Locations
Country Name City State
United States Washington University School of Medicine Saint Louis Missouri

Sponsors (3)
Lead Sponsor Collaborator
Washington University School of Medicine Geneos Therapeutics, The Foundation for Barnes-Jewish Hospital

Country where clinical trial is conducted

United States, 

Outcome
Type Measure Description Time frame Safety issue
Primary Safety and tolerability of a personalized neoantigen DNA vaccine as measured by dose-limiting toxicities (DLTs) A DLT will be defined as any grade 3 toxicity or greater according to CTCAE v5 considered at least possibly related to study treatment. The DLT observation period begins with Cycle 1 Day 1 (date of first vaccine administration) and continues for 30 days Up to 30 days
Primary Feasibility of generating a personalized neoantigen DNA vaccine for patients with newly diagnosed, unmethylated GBM as measured by the ability to identify candidate tumor-specific neoantigens 4 weeks post-completion of radiotherapy (day 1 of treatment regimen)
Primary Feasibility of generating a personalized neoantigen DNA vaccine for patients with newly diagnosed, unmethylated GBM as measured by the ability to manufacture a neoantigen-based DNA vaccine 4 weeks post-completion of radiotherapy (day 1 of treatment regimen)
Primary Feasibility of generating a personalized neoantigen DNA vaccine for patients with newly diagnosed, unmethylated GBM as measured by the ability to administer the vaccine to a patient 4 weeks post-completion of radiotherapy (day 1 of treatment regimen)
Secondary Immunogenicity of a personalized neoantigen DNA vaccine as measured by the ability to generate a measurable neoantigen-specific CD8 T cell response in vaccinated patients Week 10 post-vaccination
Secondary Immunogenicity of a personalized neoantigen DNA vaccine as measured by the number of individual neoantigens per number of neoantigens vaccinated against, with which a measurable CD8 T cell-specific response is identified Week 10 post-vaccination
Secondary Number of high quality candidates neoantigens present in patients with newly diagnosed GBM -High quality neoantigens will be defined as those that meet criteria for inclusion in a vaccine Week 24 post-vaccination
Secondary Progression-free survival (PFS) rate PFS=duration of time from start of treatment to time of progression or death, whichever occurs first.
Progression: any of the following
= 25% increase in sum products of perpendicular diameters of enhancing lesions compared with the smallest tumor measurement obtained either at baseline or best response, on stable or increasing doses of corticosteroids*. The absolute increase in any dimension must be at least 5mm when calculating the products.
Significant increase in T2/FLAIR nonenhancing lesion on stable/increasing doses of corticosteroids compared with baseline scan or best response after initiation of therapy* not caused by comorbid events
New measureable lesion.
Clear clinical deterioration not attributable to other causes apart from the tumor (e.g. seizures, medication adverse effects, complications of therapy, cerebrovascular events, infection, and so on) or changes in corticosteroid dose.		 6 months
Secondary Overall survival rate 12 months
Secondary Immunogenicity of a personalized neoantigen DNA vaccine as measured by T-cell phenotype, myeloid derived suppressor cell frequency by flow cytometry Week 24 post-vaccination
Secondary Immunogenicity of a personalized neoantigen DNA vaccine as measured by diversity of clonality from T cell receptor sequencing Week 24 post-vaccination
Secondary Immunogenicity of a personalized neoantigen DNA vaccine as measured by putative antigen specificity from T cell receptor sequencing Week 24 post-vaccination
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