Epidermal Growth Factor Receptor (EGFR) Inhibitors Screened from Autodisplayed Fv-Antibody Library
- Authors
- Sung, Jeong Soo; Jung, Jaeyong; Kim, Tae-Hun; Kwon, Soonil; Bae, Hyung Eun; Kang, Min-Jung; Jose, Joachim; Lee, Misu; Pyun, Jae-Chul
- Issue Date
- 2024-09
- Publisher
- American Chemical Society
- Citation
- Bioconjugate Chemistry, v.35, no.9, pp.1324 - 1334
- Abstract
- Inhibitors of the epithermal growth factor receptor (EGFR) were screened from an autodisplayed Fv-antibody library using an anti-EGF antibody. The Fv-antibody library was expressed on the outer membrane of Escherichia coli, which corresponds to the heavy chain V-H region of immunoglobulin G. The library was constructed by randomizing the CDR3 region of expressed V-H regions (11 amino acid residues) by site-directed mutagenesis. Using an anti-EGF antibody as a screening probe, amino acid sequences (CDR3 region) with antibody binding affinity were screened from the Fv-antibody library. These amino acid sequences were considered to have similar chemical properties to EGF, which can bind to EGFR. Two autodisplayed clones with Fv-antibodies against EGFR were screened from the Fv-antibody library, and the screened Fv-antibodies were expressed as soluble proteins. The binding affinity (K-D) was estimated using an SPR biosensor, and the inhibitory activity of expressed Fv-antibodies was observed for PANC-1 pancreatic tumor cells and T98G glioblastoma cells using Western blot analysis of proteins in the EGFR-mediated signaling pathway. The viability of PANC-1 and T98G cells was observed to decrease via the inhibitory activity of expressed Fv-antibodies. Finally, interactions between Fv-antibodies and EGFR were analyzed by using molecular docking simulations.
- Keywords
- CELL LUNG-CANCER; MONOCLONAL-ANTIBODY; PANCREATIC-CANCER; COMBINATION; EXPRESSION; THERAPY; RESISTANCE; DIVERSITY; DOCKING; CASCADE
- ISSN
- 1043-1802
- URI
- https://pubs.kist.re.kr/handle/201004/150592
- DOI
- 10.1021/acs.bioconjchem.4c00256
- Appears in Collections:
- KIST Article > 2024
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