AET 2024: Leveraging cutting-edge DNA Technologies to build precision libraries for Antibody Engineering

Presented by

Radha Parmar

Twist

Covered in this Webinar

How structure-based machine-learning was used to design predicted antibody binders against the GPCR target C5aR1

Twist’s oligo-synthesis platform and its use to create a highly diverse CDR-shuffle library and construct a de-novo phage-display

The identification of several high-affinity leads that functionally blocked C5aR1 signaling in cellular assays

Structure-based machine learning was leveraged to design predicted antibody binders against the GPCR target C5aR1. The CDR sequences of these predicted binders were then used to construct a de-novo phage-display library. Twist’s oligo-synthesis platform enabled fabrication of a highly diverse CDR-shuffle library with excellent variant representation and with no unwanted bias or motifs. Following panning, several high-affinity leads were identified that functionally blocked C5aR1 signaling in cellular assays.

This symposium was part of the event Antibody Engineering & Therapeutics Europe 2024.

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Genes

Oligo Pools

NGS Target Enrichment Solutions

Variant Libraries

Synthetic Controls

Antibody Discovery

AET 2024: Leveraging cutting-edge DNA Technologies to build precision libraries for Antibody Engineering

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