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Engineered Human Antibody with Improved Endothelin Receptor Type A Binding Affinity, Developability, and Serum Persistence Exhibits Excellent Antitumor Potency. | LitMetric

AI Article Synopsis

  • - Endothelin receptor A (ET) is linked to cancer progression and metastasis, making it a potential target for cancer treatment, but current therapies are limited to small-molecule drugs.
  • - Researchers developed an antibody called AG8 that specifically binds to ET and shows anticancer effects, but improvements in its performance were necessary.
  • - The study engineered a new antibody, MJF1-PFc29, which has better stability and binding to ET, achieving improved tumor growth inhibition in colorectal cancer models, indicating its strong potential as a cancer therapy.

Article Abstract

Endothelin receptor A (ET), a class A G protein-coupled receptor (GPCR), is a promising tumor-associated antigen due to its close association with the progression and metastasis of many types of cancer, such as colorectal, breast, lung, ovarian, and prostate cancer. However, only small-molecule drugs have been developed as ET antagonists with anticancer effects. In a previous study, we identified an antibody (AG8) with highly selective binding to human ET through screening of a human naïve immune antibody library. Although both in vitro and in vivo experiments indicated that the identified AG8 had anticancer effects, there is a need for improvement in biochemical and physicochemical properties such as the ET binding affinity, thermostability, and productivity. In this study, we engineered the framework regions of AG8 and isolated an anti-ET antibody (MJF1) exhibiting significantly improved thermostability and ET binding affinity. Subsequently, our previously isolated PFc29, an Fc variant with an enhanced pH-dependent human FcRn binding profile, was introduced to MJF1, and the resulting Fc-engineered anti-ET antibody (MJF1-PFc29) inhibited the proliferation of tumor cells comparably to MJF1 and showed a 4.2-fold increased serum half-life in human FcRn transgenic mice. Moreover, MJF1-PFc29 elicited higher tumor growth inhibition in colorectal cancer xenograft mice compared to MJF1. Our results demonstrate that the engineered human anti-ET antibody MJF1-PFc29 has great therapeutic potential and high antitumor potency against various types of cancers including colorectal cancer.

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Source
http://dx.doi.org/10.1021/acs.molpharmaceut.2c00923DOI Listing

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