Scientific Reports (Jul 2024)

Biparatopic anti-PCSK9 antibody enhances the LDL-uptake in HepG2 cells

  • Xinyang Li,
  • Wei Zhang,
  • Yu Shu,
  • Rui Huo,
  • Chengyang Zheng,
  • Qi Qi,
  • Pengfei Fu,
  • Jie Sun,
  • Yuhuan Wang,
  • Yan Wang,
  • Juxu Lu,
  • Xiangjie Zhao,
  • Guoyou Yin,
  • Qingqing Wang,
  • Jun Hong

DOI
https://doi.org/10.1038/s41598-024-66290-9
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 11

Abstract

Read online

Abstract Proprotein convertase subtilisin/kexin type 9 (PCSK9) has emerged as a promising therapeutic target to reduce lipids. In 2020, we reported a chimeric camelid-human heavy chain antibody VHH-B11-Fc targeting PCSK9. Recently, it was verified that VHH-B11 binds one linear epitope in the PCSK9 hinge region. To enhance its druggability, we have developed a novel biparatopic B11-H2-Fc Ab herein. Thereinto, surface plasmon resonance (SPR) confirmed the epitope differences in binding-PCSK9 among VHH-B11, VHH-H2 and the approved Repatha. Additionally, SPR revealed the B11-H2-Fc exhibits an avidity of approximately 0.036 nM for PCSK9, representing a considerable increase compared to VHH-B11-Fc (~ 0.69 nM). Moreover, we found the Repatha and B11-H2-Fc exhibited > 95% PCSK9 inhibition efficiency compared to approximately 48% for the VHH-Fc at 7.4 nM (P 0.05). These findings provide the first evidence of the efficacy of a novel Ab targeting PCSK9 in the field of lipid-lowering drugs.

Keywords