If The E.ncapsulator is to be adopted as a drug delivery platform, it must be able to synthesise any polypeptide. To this end, we have designed a 'universal adaptor' such that peptides which do not begin with the amino acid methionine can be synthesised. In addition, we have 'codon optimised' all non native E.coli genes to maximise gene expression efficiency.

In The E.ncapsulator, polypeptide synthesis (Module 1) and encapsulation of the cells(Module 2) occur in the same place. This duel production and delivery platform means that there is no need for expensive downstream purification processes.

As The E.ncapsulator is designed to be safe to consume, purification of the drug is not necessary. This means that our solution represents a cost-effective alternative to current production methods.

Storage has been considered in two ways. Firstly trehalose facilitates freeze drying and secondly we have been experimenting with a number if secondary encapsulation technologies including: xantham gum, milk protein and gelatin.


Trehalose is a naturally occuring sugar which is known to be important in resistance to dessication and temperature shock by many bacterial species. We have included several genes coding for the enzymes responsible for the conversion of glucose to trehalose. Secondary encapsulation is further processing that can be performed to allow for pill manufacture.

The encapsulation of the cell with the colanic acid coat facilitates transport of The E.ncapsulator through the stomach, and protecting the contents against acid breakdown. Furthermore, we have experimented with different secondary capsules that are edible and cheap to produce. This post-processing means transport and dose control of the product is much easier.