Phage-displayed peptides as biosensor reagents

## Abstract A phage display library with disulfide‐cyclized peptides was screened for peptides binding to chitinases from __Serratia marcescens__. One of those peptides was found to efficiently inhibit chitinase A and two others were inhibitors of chitinase B. Complete substitutional analysis of al

Major histocompatibility complex class I (MHC-I) molecules sample peptides from the intracellular environment and present them to cytotoxic T cells (CTL). To establish a selection system, and, thereby, enable a library approach to identify the specificities involved (that of the MHC-I for peptides a

## Abstract Peptides possess appropriate pharmacokinetic properties to serve as cancer imaging or therapeutic targeting agents. Currently, only a small number of rationally‐derived, labeled peptide analogues that target only a limited subset of antigens are available. Thus, finding new cancer targe