Acellular scaffold-based approach for in situ genetic engineering of host T-cells in solid tumor immunotherapy

Hiren Y Dandia; Mamatha M Pillai; Deepak Sharma; Meghna Suvarna; Neha Dalal; Ayush Madhok; Arvind Ingle; Shubhada V Chiplunkar; Sanjeev Galande; Prakriti Tayalia

doi:10.1186/s40779-023-00503-6

Acellular scaffold-based approach for in situ genetic engineering of host T-cells in solid tumor immunotherapy

Mil Med Res. 2024 Jan 4;11(1):3. doi: 10.1186/s40779-023-00503-6.

Authors

Affiliations

¹ Department of Biosciences and Bioengineering, Indian Institute of Technology Bombay, Powai, Mumbai, 400076, India.
² Radiation Biology and Health Sciences Division, Bhabha Atomic Research Centre, Mumbai, 400085, India.
³ Centre of Excellence in Epigenetics, Department of Biology, Indian Institute of Science Education and Research, Pune, 411008, India.
⁴ Advanced Centre for Treatment, Research and Education in Cancer (ACTREC), Tata Memorial Centre, Kharghar, Mumbai, 410210, India.
⁵ Department of Biosciences and Bioengineering, Indian Institute of Technology Bombay, Powai, Mumbai, 400076, India. prakriti@iitb.ac.in.

Abstract

Background: Targeted T-cell therapy has emerged as a promising strategy for the treatment of hematological malignancies. However, its application to solid tumors presents significant challenges due to the limited accessibility and heterogeneity. Localized delivery of tumor-specific T-cells using biomaterials has shown promise, however, procedures required for genetic modification and generation of a sufficient number of tumor-specific T-cells ex vivo remain major obstacles due to cost and time constraints.

Methods: Polyethylene glycol (PEG)-based three-dimensional (3D) scaffolds were developed and conjugated with positively charged poly-L-lysine (PLL) using carbamide chemistry for efficient loading of lentiviruses (LVs) carrying tumor antigen-specific T-cell receptors (TCRs). The physical and biological properties of the scaffold were extensively characterized. Further, the scaffold loaded with OVA-TCR LVs was implanted in B16F10 cells expressing ovalbumin (B16-OVA) tumor model to evaluate the anti-tumor response and the presence of transduced T-cells.

Results: Our findings demonstrate that the scaffolds do not induce any systemic inflammation upon subcutaneous implantation and effectively recruit T-cells to the site. In B16-OVA melanoma tumor-bearing mice, the scaffolds efficiently transduce host T-cells with OVA-specific TCRs. These genetically modified T-cells exhibit homing capability towards the tumor and secondary lymphoid organs, resulting in a significant reduction of tumor size and systemic increase in anti-tumor cytokines. Immune cell profiling revealed a significantly high percentage of transduced T-cells and a notable reduction in suppressor immune cells within the tumors of mice implanted with these scaffolds.

Conclusion: Our scaffold-based T-cell therapy presents an innovative in situ localized approach for programming T-cells to target solid tumors. This approach offers a viable alternative to in vitro manipulation of T-cells, circumventing the need for large-scale in vitro generation and culture of tumor-specific T-cells. It offers an off-the-shelf alternative that facilitates the use of host cells instead of allogeneic cells, thereby, overcoming a major hurdle.

Keywords: B16F10-OVA melanoma; Lentiviruses; Poly-L-lysine; Polyethylene glycol diacrylate; T-cell therapy.

MeSH terms

Animals
Cell Line, Tumor
Genetic Engineering
Immunotherapy
Melanoma, Experimental* / pathology
Melanoma, Experimental* / therapy
Mice
Receptors, Antigen, T-Cell / genetics
T-Lymphocytes* / pathology

Substances

Receptors, Antigen, T-Cell

Abstract

MeSH terms

Substances

Grants and funding