A compact and simple method of achieving differential transgene expression by exploiting translational readthrough

Author:

Sillibourne James E1ORCID,Agliardi Giulia12,Righi Matteo1ORCID,Smetanova Katerina1,Rowley Grant13,Speller Simon1,Dolor Abigail1,Lamb Katarina1,Allen Christopher1,Karattil Rajeev1,Parekh Farhaan1ORCID,Vargas Frederick Arce1,Thomas Simon1,Cordoba Shaun1,Pule Martin12ORCID

Affiliation:

1. Autolus Therapeutics plc, Mediaworks, 191 Wood Lane, London, W12 7FP, UK

2. Department of Haematology, University College London Cancer Institute, Paul O’Gorman Building, London, WC1E 6DD, UK

3. Department of Biochemistry, Imperial College London, South Kensington Campus, London, SW7 2AZ, UK

Abstract

The development of multicistronic vectors enabling differential transgene expression is a goal of gene therapy and poses a significant engineering challenge. Current approaches rely on the insertion of long regulatory sequences that occupy valuable space in vectors, which have a finite and limited packaging capacity. Here we describe a simple method of achieving differential transgene expression by inserting stop codons and translational readthrough motifs (TRMs) to suppress stop codon termination. TRMs reduced downstream transgene expression ∼sixfold to ∼140-fold, depending on the combination of stop codon and TRM used. We show that a TRM can facilitate the controlled secretion of the highly potent cytokine IL-12 at therapeutically beneficial levels in an aggressive immunocompetent mouse melanoma model to prevent tumor growth. Given their compact size (6 bp) and ease of introduction, we envisage that TRMs will be widely adopted in recombinant DNA engineering to facilitate differential transgene expression.

Publisher

Future Science Ltd

Subject

General Biochemistry, Genetics and Molecular Biology,Biotechnology

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