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| Name | Class |
|---|---|
| Regeneron Pharmaceuticals | INDUSTRY |
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This is a Phase 2 study designed to determine the preliminary anti-tumor activity and confirm the safety of VV1 in combination with cemiplimab. The study will enroll patients with three distinct separate tumor cohorts. The cancers types are colorectal, head and neck carcinoma, and melanoma that are progressing on CPI treatment. (CRC and melenoma cohorts are now closed to new patients)
Patients enrolled into three parallel doublet cohorts with an optimal Simon's two stage design. Patients will receive Voyager V1 as a direct to tumor injection (IT) in all 3 cancer groups and cemiplimab via IV infusion. Patients will return for treatment every 3 weeks until lack of clinical benefit or limiting toxicity. Efficacy evaluations will be conducted every 6 weeks.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Melanoma intratumoral | Experimental | (CLOSED): Melanoma, IT VV1 + IV cemiplimab Patients will receive both treatments on Day 1 and every 3 weeks thereafter until lack of clinical benefit or limiting toxicity. VV1 or cemiplimab can continue after the first dose in combination or as a single agent treatment in subsequent doses. |
|
| Head and Neck SCC intratumoral | Experimental | HNSCC, IT VV1 + IV cemiplimab, Patients will receive both treatments on Day 1 and every 3 weeks thereafter until lack of clinical benefit or limiting toxicity. VV1 or cemiplimab can continue after the first dose in combination or as a single agent treatment in subsequent doses. |
|
| Colo-rectal Carcinoma intratumoral (Arm closed) | Experimental | (CLOSED) IT VV1 + IV cemiplimab, Patients will receive both treatments on Day 1 and every 3 weeks thereafter until lack of clinical benefit or limiting toxicity. VV1 or cemiplimab can continue after the first dose in combination or as a single agent treatment in subsequent doses. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| VV1 | Biological | VV1 is to be administered on Day 1 and every 3 weeks as long as there is clinical benefit |
|
| Measure | Description | Time Frame |
|---|---|---|
| Objective response rate (ORR) per imaging assessment | Percentage of participants with objective response is assessed every six weeks from Cycle 1 Day 1 through disease progression, by investigator review based on RECIST version 1.1 | within 24 months |
| Measure | Description | Time Frame |
|---|---|---|
| Incidence of Treatment-Emergent Adverse Events assessed by CTCAE v5.0 | Safety and tolerability | within 24 months |
| Serum concentration time | Serum concentration time data using RT-PCR of VSV-IFNβ-NIS and systemic cemiplimab levels |
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Inclusion:
Age ≥18 years on day of signing informed consent.
Specific by tumor cohorts:
a. For the HSNCC cohort, histologically confirmed diagnosis of advanced and/or metastatic HSNCC suitable for first line immunotherapy.
i. HPV+ and HPV- patients are allowed.
ii. Primary tumor locations of oropharynx, oral cavity, hypopharynx, or larynx. Participants may not have a primary tumor site of nasopharynx (any histology) or salivary gland tumors.
iii. PD-L1 status ≥ 1% per local CPS score. Samples should be provided to central lab for post-hoc centralized testing.
iv. At least 12 months between last dose of prior adjuvant therapy and date of relapse diagnosis (if given). For the purposes of this protocol, "prior adjuvant therapy" only applies to full dose systemic chemotherapy (such as pre-operative systemic induction chemotherapy), but does not include radiation + surgery, or radiation + low or partial dose platinum radiosensitization. There is no time limit (washout) between the end of any prior radiation/ chemoradiation and the start of study drug v. No prior anti-PD-(L)1 treatment for HNSCC.
b. For the melanoma cohorts, histologically confirmed diagnosis of advanced and/or metastatic cutaneous melanoma for which no existing options are considered to provide clinical benefit.
i. Best response of uPR, SD or PD to an anti-PD-(L)1-containing regimen.
ii. Prior anti-PD-(L)1 therapy must have lasted ≥ 12 weeks.
iii. Radiological progression was demonstrated during or after therapy with a PD-(L)1 immune CPI (only one prior line of PD-(L)1 therapy is permitted.
iv. If patient received anti-PD-1 as prior adjuvant therapy, patient should have relapsed during therapy or within the subsequent 6 months after last dose. Note: Progression on ipilimumab is not required.
v. Patients with BRAF V600-positive tumor(s) should have received prior treatment with a BRAF inhibitor (alone or in combination with a MEK inhibitor) in addition to treatment with an anti-PD-1 or to have declined targeted therapy. Note: Patients with BRAF V600-positive tumors with no clinically significant tumor-related symptoms nor evidence of rapidly progressive disease are not required to be treated with a BRAF inhibitor (alone or in combination with a MEK inhibitor) based on investigator's decision
c. For the CRC cohort, a histologically confirmed diagnosis of advanced and/or metastatic CRC.
i. Received or are not eligible for standard of care fluoropyrimidine(s), oxaliplatin, irinotecan, anti-VEGF and EGFR-targeted therapies.
ii. Non-microsatellite instability high (non-MSI high).
iii. Progression on previous systemic therapy.
At least one tumor lesion amenable to IT injection and biopsy that has not been previously irradiated.
Measurable disease based on RECIST 1.1., including ≥ 1 measurable lesion(s) to be injected
Performance status of 0 or 1 on the ECOG Performance Scale
Life expectancy of >3 months.
Willingness to provide biological samples required for the duration of the study, including a fresh tumor biopsy sample whilst on study.
Adequate organ function assessed by laboratory values obtained ≤14 days prior to enrollment
Exclusion:
Patients meeting any of the following exclusion criteria at screening/Day -1 of first dosing will not be enrolled in the study:
Availability of and patient acceptance of an alternative curative therapeutic option.
Patients with tumor lesion(s) > 5cm in diameter.
Recent or ongoing serious infection, including any active Grade 3 or higher per the NCI CTCAE, v5.0 viral, bacterial, or fungal infection within 2 weeks of registration.
Patients who have a diagnosis of ocular, mucosal or acral melanoma.
Known seropositivity for and with active infection with HIV.
Seropositive for and with evidence of active viral infection with HBV.
Seropositive for and with active viral infection with HCV.
Known history of active or latent TB.
Any concomitant serious health condition, which, in the opinion of the investigator, would place the patient at undue risk from the study, including uncontrolled hypertension and/or diabetes, clinically significant pulmonary disease (e.g., chronic obstructive pulmonary disease requiring hospitalization within 3 months) or neurological disorder (e.g., seizure disorder active within 3 months).
Prior therapy within the following timeframe before the planned start of study treatment as follows:
NYHA classification III or IV, known symptomatic coronary artery disease, or symptoms of coronary artery disease on systems review, or known cardiac arrhythmias (atrial fibrillation or SVT).
Any known or suspected active organ-threatening autoimmune disease, such as inflammatory bowel disease, autoimmune hepatitis, lupus, or pneumonitis, with the exception of hypothyroidism and type 1 diabetes that are controlled with treatment
Immunodeficiency or immunosuppression, including systemic corticosteroids at >10 mg/day prednisone or equivalent within 1 week prior to planned start of study treatment.
History of Grade 3 or 4 immune-mediated adverse reaction to immune CPIs.
Toxicities from previous therapies that have not resolved to a Grade 1 or less.
History of non-infectious pneumonitis that required steroids, or current pneumonitis.
High volume disease, as assessed clinically by the medical monitor via parameters such as radiologic impression and tumor markers or lactate dehydrogenase (LDH).
Portal vein thrombosis involving more than intrahepatic portal vein branches: thrombosis of the right or left portal vein branch or the bifurcation, partial or complete obstruction of the portal vein trunk.
18.19. Known concurrent malignancy.
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| Name | Affiliation | Role |
|---|---|---|
| Alice Bexon, MD | CMO | Study Chair |
| Stephen J Russell, MD, Ph.D. | Clinical Lead | Study Director |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Saint John's Health Center - John Wayne Cancer Institute (JWCI) | Santa Monica | California | 90404 | United States | ||
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| Cemiplimab | Biological | Cemiplimab should be given on Day 8 of Cycle 1 (28 days) and then Day 1 of each subsequent 21-day cycle. |
|
|
| within 24 months |
| To investigate the pharmacodynamics (PD) of VV1 by measuring serum IFNβ | To investigate the pharmacodynamics (PD) of VV1 by measuring serum IFNβ expression | within 24 months |
| Yale University |
| New Haven |
| Connecticut |
| 06520-8032 |
| United States |
| University of Miami | Miami | Florida | 33136 | United States |
| Ochsner Clinic Foundation | New Orleans | Louisiana | 70121 | United States |
| Mayo Clinic | Rochester | Minnesota | 55905 | United States |
| Billings Clinic Montana Cancer Consortium | Billings | Montana | 59101 | United States |
| Icahn School of Medicine at Mount Sinai | New York | New York | 10029 | United States |
| University of Cincinnati Medical Center | Cincinnati | Ohio | 45219 | United States |
| Sanford Cancer Center | Sioux Falls | South Dakota | 57104 | United States |
| Hospital Sao Rafael | Salvador | BR | 41253-190 | Brazil |
| INCA | Rio de Janeiro | Rio de Janeiro | 20231-050 | Brazil |
| Hospital Moinhos de Vento | Porto Alegre | Rio Grande do Sul | 90035-000 | Brazil |
| Hospital de Amor de Barretos | Barretos | São Paulo | 14.784-400 | Brazil |
| ID | Term |
|---|---|
| D008545 | Melanoma |
| D000077195 | Squamous Cell Carcinoma of Head and Neck |
| D003110 | Colonic Neoplasms |
| ID | Term |
|---|---|
| D018358 | Neuroendocrine Tumors |
| D017599 | Neuroectodermal Tumors |
| D009373 | Neoplasms, Germ Cell and Embryonal |
| D009370 | Neoplasms by Histologic Type |
| D009369 | Neoplasms |
| D009380 | Neoplasms, Nerve Tissue |
| D018326 | Nevi and Melanomas |
| D012878 | Skin Neoplasms |
| D009371 | Neoplasms by Site |
| D012871 | Skin Diseases |
| D017437 | Skin and Connective Tissue Diseases |
| D002294 | Carcinoma, Squamous Cell |
| D002277 | Carcinoma |
| D009375 | Neoplasms, Glandular and Epithelial |
| D006258 | Head and Neck Neoplasms |
| D015179 | Colorectal Neoplasms |
| D007414 | Intestinal Neoplasms |
| D005770 | Gastrointestinal Neoplasms |
| D004067 | Digestive System Neoplasms |
| D004066 | Digestive System Diseases |
| D005767 | Gastrointestinal Diseases |
| D003108 | Colonic Diseases |
| D007410 | Intestinal Diseases |
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| ID | Term |
|---|---|
| C000627974 | cemiplimab |
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