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CD8+ T Cells Impact Rising PSA in Biochemically Relapsed Cancer Patients Using Immunotherapy Targeting Tumor-Associated Antigens
Journal article   Open access

CD8+ T Cells Impact Rising PSA in Biochemically Relapsed Cancer Patients Using Immunotherapy Targeting Tumor-Associated Antigens

N. D. Shore, M. P. Morrow, T. McMullan, K. A. Kraynyak, A. Sylvester, K. Bhatt, J. Cheung, J. D. Boyer, L. Liu, B. Sacchetta, …
Molecular Therapy, Vol.28(5)
2020

Abstract

CD8 cytotoxic lymphocyte DNA immune response immunotherapy prostate cancer ADP ribosyl cyclase/cyclic ADP ribose hydrolase 1 antineoplastic agent ino 5150 ino 9012 interleukin 12 perforin prostate specific antigen prostate specific membrane antigen syncon tumor antigen unclassified drug FOLH1 protein, human glutamate carboxypeptidase II membrane antigen adult Article biochemical recurrence body weight loss brachytherapy cancer combination chemotherapy cancer immunotherapy cancer patient cancer radiotherapy cancer surgery CD8+ T lymphocyte cohort analysis controlled study drug efficacy drug potentiation drug safety drug targeting drug tolerability electroporation external beam radiotherapy fatigue hematuria human human cell hyperglycemia hypertension injection site contusion injection site erythema injection site pain injection site swelling major clinical study male multicenter study phase 1 clinical trial phase 2 clinical trial postoperative period progression free survival prostatectomy side effect tumor doubling time tumor immunogenicity aged blood clinical trial cytotoxic T lymphocyte drug therapy follow up gene therapy genetics immunity immunology middle aged pathology plasmid procedures prostate tumor tumor recurrence very elderly Aged, 80 and over Antigens, Surface Follow-Up Studies Genetic Therapy Humans Interleukin-12 Neoplasm Recurrence, Local Plasmids Progression-Free Survival Prostate-Specific Antigen Prostatic Neoplasms T-Lymphocytes, Cytotoxic
url
https://doi.org/10.1016/j.ymthe.2020.02.018View
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