Our Platform

The Orbit Peptide Discovery Platform

The Orbit Discovery Affinity Screening services offers the opportunity to interrogate populations of binding peptides using FACS. This capability offers a significant throughput benefit beyond more traditional screening techniques, such as phage display or ribosomal display. As well as screening against soluble targets, the platform can be combined with other internal capabilities to offer a unique ability to address cell surface targets in a primary peptide screen, a particularly useful benefit for identifying targeting peptides.

The bead-based technology enables the construction of massive libraries with peptides displayed on their surface. Each bead carries a unique DNA sequence, which is translated into peptide using in vitro transcription translation(IVTT) performed in an emulsion (emIVTT).  Each droplet of the emulsion acts as a micro-compartment which allows translation of the DNA on each individual bead to occur separately. The result is a library of unique beads each displaying thousands of copies of peptide, providing massive chemical diversity and the ability to perform rapid screens for high affinity binders against soluble or more complex target proteins, such as GPCRs and ion channels.

The platform is flexible, allows for different library structures (linear, cyclic, helical), peptide lengths, diversity, and chemistries. Effectively, we are agnostic to starting point, if the peptide can be encoded in DNA, we can create libraries reflecting desired populations. To date we have stockpiled random linear and cyclic libraries which are available for immediate use. Furthermore, we have also used client scaffolds (where only certain regions need to randomised) and outputs from AI/ML to create bespoke peptide libraries which were subsequently screened for binders.  The high diversity that can be covered produces an abundance of hits that can be further optimised as therapeutic candidates. Binders are analysed for conserved motifs and structures, these can be synthesised, and binding confirmed (peptide microarray, internalisation assays, thermal shift, SPR or cell assays can be performed) prior to taking into further medicinal chemistry. Alternatively, binders can be used to design smaller more refined libraries that can be taken into cell based functional screening.
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