A New Strategy for the In Vitro Selection of Stapled Peptide Inhibitors by mRNA Display

Authors

Emil S. Iqbal, Virginia Commonwealth University
Stacie L. Richardson, Virginia Commonwealth University
Nicolas A. Abrigo, Virginia Commonwealth University
Kara K. Dods, Virginia Commonwealth University
H. Estheban Osorio Franco, Virginia Commonwealth University
Heather S. Gerrish, Virginia Commonwealth University
Hari Kiran Kotapati, University of Southern MississippiFollow
Iain M. Morgan, Virginia Commonwealth University
Douglas S. Masterson, University of Southern MississippiFollow
Matthew C.T. Hartman, Virginia Commonwealth University

Document Type

Article

Publication Date

7-10-2019

Department

Chemistry and Biochemistry

School

Mathematics and Natural Sciences

Abstract

Hydrocarbon stapled peptides are promising therapeutics for inhibition of intracellular protein–protein interactions. Here we develop a new high-throughput strategy for hydrocarbon stapled peptide discovery based on mRNA display of peptides containing α-methyl cysteine and cyclized with m-dibromoxylene. We focus on development of a peptide binder to the HPV16 E2 protein.

Publication Title

Chemical Communications

Volume

55

First Page

8959

Last Page

8962

Recommended Citation

Iqbal, E. S., Richardson, S. L., Abrigo, N. A., Dods, K. K., Franco, H. O., Gerrish, H. S., Kotapati, H. K., Morgan, I. M., Masterson, D. S., Hartman, M. C. (2019). A New Strategy for the In Vitro Selection of Stapled Peptide Inhibitors by mRNA Display. Chemical Communications, 55, 8959-8962.
Available at: https://aquila.usm.edu/fac_pubs/16481