Maren Meysing scite author profile

The enrichment of open reading frames (ORFs) from large gene libraries and the presentation of the corresponding polypeptides on filamentous phage M13 (phage display) is frequently used to identify binding partners of unknown ORFs. In particular phage display is a valuable tool for the identification of pathogen-related antigens and a first step for the development of new diagnostics and therapeutics. Here, we introduce a significant improvement of phage-based ORF enrichment by using Hyperphage, a helperphage with a truncated gIII. The methods allow both the enrichment of ORFs from cDNA libraries and the display of the corresponding polypeptides on phage, thus combining ORF enrichment with a screening for binding in one step without any further subcloning steps. We demonstrated the benefits of the method by isolating the sequences encoding two predicted immunogenic epitopes of the outer membrane protein D encoding gene (ompD) of Salmonella typhimurium. Here, we showed that when using a mixture of three constructs with only one containing an ORF solely this correct construct could be reisolated in phage particles. Further; both epitopes were detected by enzyme-linked immunosorbent assay (ELISA), demonstrating correct translation of fusion proteins. Furthermore, the enrichment system was evaluated by the enrichment of ORFs from total cDNA of lymphocytes. Here, we could show that 60% of the phage contained ORFs, which is an increase of an order of magnitude compared with conventional phage expression system. Together these data show that the Hyperphage-based enrichment system significantly improves the enrichment of ORFs and directly allows the display of the corresponding polypeptide on bacteriophage M13.

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Novel Ubiquitin-derived High Affinity Binding Proteins with Tumor Targeting Properties

Lorey¹,

Fiedler²,

Kunert³

et al. 2014

Journal of Biological Chemistry

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Background: Targeting molecules to tumor cells is a promising mode of action for cancer therapy.Results: Ubiquitin-based high affinity, specific, and stable binding molecules for extradomain B are accumulated in the tumor.Conclusion: Ubiquitin may be engineered for high affinity target binding and modified with half-life extension technologies.Significance: Ubiquitin qualifies as a well suited scaffold protein adaptable to specific tasks.

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Limiting factors of the translation machinery

Freischmidt

Meysing²,

Liss³

et al. 2010

Journal of Biotechnology

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Entwicklung eines Verfahrens zur kontinuierlichen, gerichteten Evolution hochaffiner Protein-Liganden in vitro

Meysing¹

2010

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Maren Meysing

Enrichment of Open Reading Frames Presented on Bacteriophage M13 Using Hyperphage

Novel Ubiquitin-derived High Affinity Binding Proteins with Tumor Targeting Properties

Limiting factors of the translation machinery

Entwicklung eines Verfahrens zur kontinuierlichen, gerichteten Evolution hochaffiner Protein-Liganden in vitro

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