Journal
RSC MEDICINAL CHEMISTRY
Volume 12, Issue 3, Pages 406-409Publisher
ROYAL SOC CHEMISTRY
DOI: 10.1039/d0md00337a
Keywords
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Funding
- Japanese Society for the Promotion of Sciences (JSPS) KAKENHI [18K19148, 19H03356]
- Research Fellowship for Young Scientists (JSPS) [17J05032]
- Advanced Graduate Course on Molecular Systems for Devices (Kyushu University)
- Grants-in-Aid for Scientific Research [19H03356, 18K19148, 17J05032] Funding Source: KAKEN
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A novel Fc-binding antibody-recruiting molecule (Fc-ARM) was synthesized using the monocyclic peptide 15-Lys8Leu, which binds strongly to the Fc region to target FR-positive cancer cells. This peptide, easily synthesized, is suitable for various applications including the development of Fc-ARMs.
Antibody-recruiting molecules (ARMs) are bispecific molecules composed of an antibody-binding motif and a target-binding motif that redirect endogenous antibodies to target cells to elicit immune responses. To enhance the translational potential of ARMs, it is crucial to design antibody/target-binding motifs that have strong affinity and are easy to synthesize. Here, we synthesized a novel Fc-binding ARM (Fc-ARM) that targets folate receptor (FR)-positive cancer cells, Reo-3, using a recently developed monocyclic peptide 15-Lys8Leu, which binds strongly to the Fc region of an antibody. Reo-3 bound to the Fc region of the antibody with a K-d of 5.8 nM, and recruited a clinically used antibody mixture to attack FR-positive IGROV-1 cells as efficiently as Fc-ARM2, in which a bicyclic Fc-binding peptide was used. These results indicate that 15-Lys8Leu, which can be synthesized readily, is suitable for various applications including the development of Fc-ARMs.
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