Literature DB >> 34371731

mRNA-Based Anti-TCR CDR3 Tumour Vaccine for T-Cell Lymphoma.

Marina Tusup1,2, Severin Läuchli1,2, Natalia Teresa Jarzebska1,3, Lars E French4,5, Yun-Tsan Chang6, Maya Vonow-Eisenring7, Andreas Su8, Thomas M Kündig1,2, Emmanuella Guenova1,2,6, Steve Pascolo1,2.   

Abstract

Efficient vaccination can be achieved by injections of in vitro transcribed mRNA (ivt mRNA) coding for antigens. This vaccine format is particularly versatile and allows the production of individualised vaccines conferring, T-cell immunity against specific cancer mutations. The CDR3 hypervariable regions of immune receptors (T-cell receptor, TCR or B-cell receptor, BCR) in the context of T- or B-cell leukaemia or lymphoma are targetable and specific sequences, similar to cancer mutations. We evaluated the functionality of an mRNA-based vaccine designed to trigger immunity against TCR CDR3 regions in an EL4 T-lymphoma cell line-derived murine in vivo model. Vaccination against the hypervariable TCR regions proved to be a feasible approach and allowed for protection against T-lymphoma, even though immune escape in terms of TCR downregulation paralleled the therapeutic effect. However, analysis of human cutaneous T-cell lymphoma samples indicated that, as is the case in B-lymphomas, the clonotypic receptor may be a driver mutation and is not downregulated upon treatment. Thus, vaccination against TCR CDR3 regions using customised ivt mRNA is a promising immunotherapy method to be explored for the treatment of patients with T-cell lymphomas.

Entities:  

Keywords:  CDR3; CTCL; T-cell lymphoma; TCR; in vitro transcribed mRNA; ivt mRNA; vaccine

Year:  2021        PMID: 34371731     DOI: 10.3390/pharmaceutics13071040

Source DB:  PubMed          Journal:  Pharmaceutics        ISSN: 1999-4923            Impact factor:   6.321


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  2 in total

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