A protein chimera strategy supports production of a model "difficult-to-express" recombinant target.

Hirra Hussain,Alan J Dickson,David I Fisher,Robert G Roth,Manuel Alejandro Carballo‐Amador,Jim Warwicker,W Mark Abbott

doi:10.1002/1873-3468.13170

Abstract

Due in part to the needs of the biopharmaceutical industry, there has been an increased drive to generate high quality recombinant proteins in large amounts. However, achieving high yields can be a challenge as the novelty and increased complexity of new targets often makes them ‘difficult‐to‐express’. This study aimed to define the molecular features that restrict the production of a model ‘difficult‐to‐express’ recombinant protein, Tissue Inhibitor Metalloproteinase‐3 (TIMP‐3). Building from experimental data, computational approaches were used to rationalize the redesign of this recombinant target to generate a chimera with enhanced secretion. The results highlight the importance of early identification of unfavourable sequence attributes, enabling the generation of engineered protein forms that bypass ‘secretory’ bottlenecks and result in efficient recombinant protein production.

Highlights

Over recent years the use of mammalian expression systems has increased for the production of approved biotherapeutics [1,2]
We have shown that Tissue inhibitors of metalloproteinases (TIMPs)-2 and Tissue Inhibitor Metalloproteinase-3 (TIMP-3) were secreted to significantly different extents in a transient Chinese Hamster Ovary (CHO) expression system [26]
Amino acid sequences and secondary structures of specific proteins contain features associated with limitations in recombinant protein production in CHO cells [30,31,32]

Summary

Introduction

Over recent years the use of mammalian expression systems has increased for the production of approved biotherapeutics [1,2]. Efficient recombinant protein production of secreted targets in mammalian cells requires the balance between different steps/processes as proteins process through the complex secretory pathway [3,4,5]. Little is known regarding the mechanisms underpinning poor recombinant protein production, between proteins of high sequence similarity. Reports surrounding production of monoclonal antibodies (mAbs) suggest that unique sequence features influence the effectiveness of recombinant protein production [30,31,32].

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Results

Conclusion