CHEMICAL AND BIOSYNTHETIC APPROACHES TO THE PRODUCTION OF NOVEL POLYPEPTIDE MATERIALS

Three approaches to the synthesis of the repetitive copolypeptide [‐(GlyAla)3‐ GlyProGlu‐]n (1) are described. Direct chemical synthesis of 1 via classical solution methods required 18 steps and afforded a polydisperse product with an average molecular weight of less than 10 000. Two alternative genetic strategies were also explored. In the first, chemically synthesized DNA oligomers were self‐ligated to produce a population of multimers, which were fitted with translational start and stop signals and inserted into an expression plasmid containing the λ PL promoter and a synthetic ribosome binding site. Transformation of E. coli led to the isolation of a stable recombinant plasmid carrying an insert encoding 12 repeats of sequence 1. Attempts to identify polypeptide 1 after induction of transformed cultures were unsuccessful. A second strategy, generating a tripartite derivative of sequence 1 carrying short N‐and C‐terminal extensions, afforded excellent yields of product. The relative merits of chemical and genetic approaches to repetitive polypeptide materials are discussed. Copyright © 1990 American Institute of Chemical Engineers (AIChE)