Affiliation:
1. Division of Pharmacology and Pharmaceutical Sciences School of Pharmacy University of Missouri‐Kansas City 2464 Charlotte Street Kansas City MO 64108 USA
Abstract
AbstractCancer immunotherapy targeting adaptive immune cells has been attracting considerable interest due to its great success in treating multiple cancers. Recently, there is also increasing interest in agents that can stimulate innate immune cell activities. Immune checkpoint inhibitors targeting innate immune cells can block inhibitory interactions (“don't eat me” signals) between tumor cells and phagocytes. CD47 is a transmembrane protein overexpressed in various cancers and acts as a potent “do not eat me” signal that contributes to the immune evasion of cancer cells. Anti‐CD47 peptides that can bind to CD47 and block its interaction with signal regulatory protein alpha (SIRPα) are discovered using a novel phage display biopanning strategy. Anti‐CD47 peptides enhance the macrophage‐mediated phagocytosis of NCI‐H82 tumor cells in vitro. Unlike anti‐CD47 antibodies, these peptides do not induce the agglutination of red blood cells. Moreover, anti‐CD47 peptides exhibit high specificity for MC‐38 cancer cells expressing CD47. CMP‐22 peptide show the ability to increase the antitumor activity of doxorubicin and extends the survival of CT26 tumor‐bearing mice. The discovered anti‐CD47 peptides can be considered potential candidates for cancer immunotherapy by blocking the CD47/SIRPα interaction, especially in combination with chemotherapy, to elicit synergistic effects.
Funder
National Institutes of Health
Subject
Pharmacology (medical),Biochemistry (medical),Genetics (clinical),Pharmaceutical Science,Pharmacology,Medicine (miscellaneous)