PLoS Biology (Jun 2019)

Specific activation of pro-Infliximab enhances selectivity and safety of rheumatoid arthritis therapy.

  • Yun-Chi Lu,
  • Chih-Hung Chuang,
  • Kuo-Hsiang Chuang,
  • I-Ju Chen,
  • Bo-Cheng Huang,
  • Wen-Han Lee,
  • Hsin-Ell Wang,
  • Jia-Je Li,
  • Yi-An Cheng,
  • Kai-Wen Cheng,
  • Jaw-Yuan Wang,
  • Yuan-Chin Hsieh,
  • Wen-Wei Lin,
  • Tian-Lu Cheng

DOI
https://doi.org/10.1371/journal.pbio.3000286
Journal volume & issue
Vol. 17, no. 6
p. e3000286

Abstract

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During rheumatoid arthritis (RA) treatment, long-term injection of antitumor necrosis factor α antibodies (anti-TNFα Abs) may induce on-target toxicities, including severe infections (tuberculosis [TB] or septic arthritis) and malignancy. Here, we used an immunoglobulin G1 (IgG1) hinge as an Ab lock to cover the TNFα-binding site of Infliximab by linking it with matrix metalloproteinase (MMP) -2/9 substrate to generate pro-Infliximab that can be specifically activated in the RA region to enhance the selectivity and safety of treatment. The Ab lock significantly inhibits the TNFα binding and reduces the anti-idiotypic (anti-Id) Ab binding to pro-Infliximab by 395-fold, 108-fold compared with Infliximab, respectively, and MMP-2/9 can completely restore the TNFα neutralizing ability of pro-Infliximab to block TNFα downstream signaling. Pro-Infliximab was only selectively activated in the disease site (mouse paws) and presented similar pharmacokinetics (PKs) and bio-distribution to Infliximab. Furthermore, pro-Infliximab not only provided equivalent therapeutic efficacy to Infliximab but also maintained mouse immunity against Listeria infection in the RA mouse model, leading to a significantly higher survival rate (71%) than that of the Infliximab treatment group (0%). The high-selectivity pro-Infliximab maintains host immunity and keeps the original therapeutic efficiency, providing a novel strategy for RA therapy.