International Journal of Molecular Sciences (Jan 2024)

Re-Engineering Therapeutic Anti-Aβ Monoclonal Antibody to Target Amyloid Light Chain

  • Jingyi Bai,
  • Xi Li,
  • Jun Zhao,
  • Huifang Zong,
  • Yuan Yuan,
  • Lei Wang,
  • Xiaoshuai Zhang,
  • Yong Ke,
  • Lei Han,
  • Jianrong Xu,
  • Buyong Ma,
  • Baohong Zhang,
  • Jianwei Zhu

DOI
https://doi.org/10.3390/ijms25031593
Journal volume & issue
Vol. 25, no. 3
p. 1593

Abstract

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Amyloidosis involves the deposition of misfolded proteins. Even though it is caused by different pathogenic mechanisms, in aggregate, it shares similar features. Here, we tested and confirmed a hypothesis that an amyloid antibody can be engineered by a few mutations to target a different species. Amyloid light chain (AL) and β-amyloid peptide (Aβ) are two therapeutic targets that are implicated in amyloid light chain amyloidosis and Alzheimer’s disease, respectively. Though crenezumab, an anti-Aβ antibody, is currently unsuccessful, we chose it as a model to computationally design and prepare crenezumab variants, aiming to discover a novel antibody with high affinity to AL fibrils and to establish a technology platform for repurposing amyloid monoclonal antibodies. We successfully re-engineered crenezumab to bind both Aβ42 oligomers and AL fibrils with high binding affinities. It is capable of reversing Aβ42-oligomers-induced cytotoxicity, decreasing the formation of AL fibrils, and alleviating AL-fibrils-induced cytotoxicity in vitro. Our research demonstrated that an amyloid antibody could be engineered by a few mutations to bind new amyloid sequences, providing an efficient way to reposition a therapeutic antibody to target different amyloid diseases.

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