Long-Term Survival and Immune Response Dynamics in Melanoma Patients Undergoing TAPCells-Based Vaccination Therapy

Author:

Tittarelli Andrés1ORCID,Pereda Cristian2ORCID,Gleisner María A.23ORCID,López Mercedes N.2,Flores Iván2,Tempio Fabián2,Lladser Alvaro45ORCID,Achour Adnane67ORCID,González Fermín E.8ORCID,Durán-Aniotz Claudia9ORCID,Miranda Juan P.10,Larrondo Milton11,Salazar-Onfray Flavio2367ORCID

Affiliation:

1. Programa Institucional de Fomento a la Investigación, Desarrollo e Innovación, Universidad Tecnológica Metropolitana, Santiago 8940577, Chile

2. Disciplinary Program of Immunology, Institute of Biomedical Sciences, Faculty of Medicine, Universidad de Chile, Santiago 8380453, Chile

3. Millennium Institute on Immunology and Immunotherapy, Faculty of Medicine, Universidad de Chile, Santiago 8380453, Chile

4. Centro Científico y Tecnológico de Excelencia Ciencia & Vida, Fundación Ciencia & Vida, Santiago 8580702, Chile

5. Facultad de Medicina y Ciencia, Universidad San Sebastián, Santiago 8580702, Chile

6. Science for Life Laboratory, Department of Medicine Solna, Karolinska Institute, 17176 Stockholm, Sweden

7. Division of Infectious Diseases, Karolinska University Hospital, 17176 Stockholm, Sweden

8. Laboratory of Experimental Immunology & Cancer, Faculty of Dentistry, Universidad de Chile, Santiago 8380000, Chile

9. Latin American Brain Health Institute (BrainLat), Center for Social and Cognitive Neuroscience (CSCN), School of Psychology, Universidad Adolfo Ibañez, Santiago 7941169, Chile

10. Instituto Nacional del Cáncer, Santiago 8380000, Chile

11. Banco de Sangre, Hospital Clínico de la Universidad de Chile, Santiago 8380453, Chile

Abstract

Cancer vaccines present a promising avenue for treating immune checkpoint blockers (ICBs)-refractory patients, fostering immune responses to modulate the tumor microenvironment. We revisit a phase I/II trial using Tumor Antigen-Presenting Cells (TAPCells) (NCT06152367), an autologous antigen-presenting cell vaccine loaded with heat-shocked allogeneic melanoma cell lysates. Initial findings showcased TAPCells inducing lysate-specific delayed-type hypersensitivity (DTH) reactions, correlating with prolonged survival. Here, we extend our analysis over 15 years, categorizing patients into short-term (<36 months) and long-term (≥36 months) survivors, exploring novel associations between clinical outcomes and demographic, genetic, and immunologic parameters. Notably, DTHpos patients exhibit a 53.1% three-year survival compared to 16.1% in DTHneg patients. Extended remissions are observed in long-term survivors, particularly DTHpos/M1cneg patients. Younger age, stage III disease, and moderate immune events also benefit short-term survivors. Immunomarkers like increased C-type lectin domain family 2 member D on CD4+ T cells and elevated interleukin-17A were detected in long-term survivors. In contrast, toll-like receptor-4 D229G polymorphism and reduced CD32 on B cells are associated with reduced survival. TAPCells achieved stable long remissions in 35.2% of patients, especially M1cneg/DTHpos cases. Conclusions: Our study underscores the potential of vaccine-induced immune responses in melanoma, emphasizing the identification of emerging biological markers and clinical parameters for predicting long-term remission.

Funder

National Fund for Scientific and Technological Development

Fund for the Promotion of Scientific and Technological Development

Millennium Science Initiative, National Agency for Research and Development

Basal Funding for Centers of Scientific and Technological Excellence, National Agency for Research and Development

First Call for the Promotion of Scientific and Technological-based Business Creation

Universidad Tecnológica Metropolitana

Publisher

MDPI AG

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