Expression of the Reverse Transcriptase Domain of Telomerase Reverse Transcriptase Induces Lytic Cellular Response in DNA-Immunized Mice and Limits Tumorigenic and Metastatic Potential of Murine Adenocarcinoma 4T1 Cells

Juris Jansons; Ekaterina Bayurova; Dace Skrastina; Alisa Kurlanda; Ilze Fridrihsone; Dmitry Kostyushev; Anastasia Kostyusheva; Alexander Artyuhov; Erdem Dashinimaev; Darya Avdoshina; Alla Kondrashova; Vladimir Valuev-Elliston; Oleg Latyshev; Olesja Eliseeva; Stefan Petkov; Maxim Abakumov; Laura Hippe; Irina Kholodnyuk; Elizaveta Starodubova; Tatiana Gorodnicheva; Alexander Ivanov; Ilya Gordeychuk; Maria Isaguliants

doi:10.3390/vaccines8020318

Expression of the Reverse Transcriptase Domain of Telomerase Reverse Transcriptase Induces Lytic Cellular Response in DNA-Immunized Mice and Limits Tumorigenic and Metastatic Potential of Murine Adenocarcinoma 4T1 Cells

Vaccines (Basel). 2020 Jun 18;8(2):318. doi: 10.3390/vaccines8020318.

Authors

Juris Jansons^{1

2}, Ekaterina Bayurova^{3

4}, Dace Skrastina², Alisa Kurlanda¹, Ilze Fridrihsone¹, Dmitry Kostyushev⁵, Anastasia Kostyusheva⁵, Alexander Artyuhov⁶, Erdem Dashinimaev^{6

7}, Darya Avdoshina⁴, Alla Kondrashova⁴, Vladimir Valuev-Elliston⁸, Oleg Latyshev³, Olesja Eliseeva³, Stefan Petkov⁹, Maxim Abakumov^{3

10

11}, Laura Hippe¹, Irina Kholodnyuk¹, Elizaveta Starodubova⁸, Tatiana Gorodnicheva¹², Alexander Ivanov^{3

8}, Ilya Gordeychuk^{3

4

13}, Maria Isaguliants^{1

3

4

9}

Affiliations

¹ Department of Research, and Department of Pathology, Pathology, Rīga Stradiņš University, LV-1007 Riga, Latvia.
² Latvian Biomedical Research and Study Centre, LV-1067 Riga, Latvia.
³ N.F. Gamaleya National Research Center for Epidemiology and Microbiology, Moscow 127994, Russia.
⁴ Chumakov Federal Scientific Center for Research and Development of Immune-and-Biological Products of Russian Academy of Sciences, Moscow 127994, Russia.
⁵ National Medical Research Center of Tuberculosis and Infectious Diseases, Ministry of Health, Moscow 127994, Russia.
⁶ Center for Precision Genome Editing and Genetic Technologies, Pirogov Russian National Research Medical University, Moscow 127994, Russia.
⁷ Koltzov Institute of Developmental Biology of Russian Academy of Sciences, Moscow 127994, Russia.
⁸ Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, Moscow 127994, Russia.
⁹ Department of Microbiology, Tumor and Cell Biology, Karolinska Institutet, 17177 Stockholm, Sweden.
¹⁰ Laboratory of Biomedical Nanomaterials, National University of Science and Technology MISIS, Moscow 127994, Russia.
¹¹ Department of Medical Nanobiotechnologies, Pirogov Russian National Research Medical University, Moscow 127994, Russia.
¹² Evrogen, Moscow 127994, Russia.
¹³ Institute for Translational Medicine and Biotechnology, Sechenov First Moscow State Medical University, Moscow 127994, Russia.

Abstract

Telomerase reverse transcriptase (TERT) is a classic tumor-associated antigen overexpressed in majority of tumors. Several TERT-based cancer vaccines are currently in clinical trials, but immune correlates of their antitumor activity remain largely unknown. Here, we characterized fine specificity and lytic potential of immune response against rat TERT in mice. BALB/c mice were primed with plasmids encoding expression-optimized hemagglutinin-tagged or nontagged TERT or empty vector and boosted with same DNA mixed with plasmid encoding firefly luciferase (Luc DNA). Injections were followed by electroporation. Photon emission from booster sites was assessed by in vivo bioluminescent imaging. Two weeks post boost, mice were sacrificed and assessed for IFN-γ, interleukin-2 (IL-2), and tumor necrosis factor alpha (TNF-α) production by T-cells upon their stimulation with TERT peptides and for anti-TERT antibodies. All TERT DNA-immunized mice developed cellular and antibody response against epitopes at the N-terminus and reverse transcriptase domain (rtTERT) of TERT. Photon emission from mice boosted with TERT/TERT-HA+Luc DNA was 100 times lower than from vector+Luc DNA-boosted controls. Bioluminescence loss correlated with percent of IFN-γ/IL-2/TNF-α producing CD8+ and CD4+ T-cells specific to rtTERT, indicating immune clearance of TERT/Luc-coexpressing cells. We made murine adenocarcinoma 4T1luc2 cells to express rtTERT by lentiviral transduction. Expression of rtTERT significantly reduced the capacity of 4T1luc2 to form tumors and metastasize in mice, while not affecting in vitro growth. Mice which rejected the tumors developed T-cell response against rtTERT and low/no response to the autoepitope of TERT. This advances rtTERT as key component of TERT-based therapeutic vaccines against cancer.

Keywords: CD4+ and CD8+ lytic T cell response; antibodies; electroporation; epitopes; intradermal DNA immunization; lentiviral transduction; metastasis; murine adenocarcinoma cells; rejection; reverse transcriptase domain; suppression; telomerase reverse transcriptase (TERT); therapeutic cancer vaccines; tumor growth.

Abstract

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