Safety, feasibility and functionality of activated autologous dendritic cells for intratumoral injection in solid tumors: a Phase I clinical trial

BackgroundDendritic cells (DC) are proficient in initiating adaptive immune responses, through the uptake and subsequent presentation to the immune system of antigenic compounds. In preclinical studies, activated DC (aDC; DCVax®-Direct) were shown to be superior to immature DC in clearing tumors fro...

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Published in:Journal for immunotherapy of cancer 2015-11, Vol.3 (Suppl 2), p.P199-P199
Main Authors: Subbiah, Vivek, Murthy, Ravi, Hong, David, Prins, Robert, Hosing, Chitra, Brown, Robert, Mary, McGuire, Naing, Aung, Fu, Siquing, Conley, Anthony, Kaur, Indreshpaul, Hendricks, Kyle, Kolli, Deepthi, Noffsinger, Lori, Bosch, Marnix
Format: Article
Language:English
Subjects:
Biopsy
Cancer
Care and treatment
Dendritic cells
Health aspects
Immunotherapy
Methods
Patient outcomes
Poster Presentation
Tumors
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Summary:BackgroundDendritic cells (DC) are proficient in initiating adaptive immune responses, through the uptake and subsequent presentation to the immune system of antigenic compounds. In preclinical studies, activated DC (aDC; DCVax®-Direct) were shown to be superior to immature DC in clearing tumors from mice, upon intratumoral injection.MethodsForty patients were enrolled in a Phase I dose escalation trial to test the safety and feasibility of intratumoral injection of aDC in solid tumors. aDC were administered intratumorally under image guidance, at a dose of 2 million, 6 million, or 15 million live, activated, autologous DC per injection. At each injection visit (days 0, 7, 14, then weeks 8, 16 and 32), a single lesion was injected. Biopsies were assessed for tumor necrosis and for infiltrating lymphocytes. Tumor size was monitored through standard imaging procedures, and blood was collected for immune monitoring. The aDC were assessed for expression of co-stimulatory molecules and for the production of cytokines.ResultsIntratumoral injection under image guidance was generally well tolerated and feasible. In total, 149 i.t. injections were performed, in 17 patients at the 2 million, 20 at the 6 million, and 3 at the 15 million dose level, with mild to moderate fevers as the most frequently observed adverse events. Biopsies of the injected tumors showed appearance of tumor necrosis in 62%, and T cell infiltrates in 54%. Stabilization of disease was found to correlate with survival, and with a specific cytokine profile of the aDC which is consistent with induction of Th-1 type immune responses.ConclusionsIntratumoral injection of autologous, activated DC is feasible without significant toxicity in multiple solid tumors, and can elicit local and systemic immune responses. Specific characteristics of the injected dendritic cells may predict tumor response and survival.Trial registrationClinicalTrials.gov identifier NCT01882946.
ISSN:2051-1426
2051-1426
DOI:10.1186/2051-1426-3-S2-P199