Inflammation and Regeneration (Feb 2023)

A lesion-selective albumin-CTLA4Ig as a safe and effective treatment for collagen-induced arthritis

  • Fu-Yao Jiang,
  • Yan-Zhu Zhang,
  • Yuan-Hong Tai,
  • Chien-Yu Chou,
  • Yu-Ching Hsieh,
  • Ya-Chi Chang,
  • Hsiao-Chen Huang,
  • Zhi-Qin Li,
  • Yuan-Chin Hsieh,
  • I-Ju Chen,
  • Bo-Cheng Huang,
  • Yu-Cheng Su,
  • Wen-Wei Lin,
  • Hsin-Chieh Lin,
  • Jui-I Chao,
  • Shyng-Shiou F. Yuan,
  • Yun-Ming Wang,
  • Tian-Lu Cheng,
  • Shey-Cherng Tzou

DOI
https://doi.org/10.1186/s41232-023-00264-8
Journal volume & issue
Vol. 43, no. 1
pp. 1 – 16

Abstract

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Abstract Background CTLA4Ig is a dimeric fusion protein of the extracellular domain of cytotoxic T-lymphocyte protein 4 (CTLA4) and an Fc (Ig) fragment of human IgG1 that is approved for treating rheumatoid arthritis. However, CTLA4Ig may induce adverse effects. Developing a lesion-selective variant of CTLA4Ig may improve safety while maintaining the efficacy of the treatment. Methods We linked albumin to the N-terminus of CTLA4Ig (termed Alb-CTLA4Ig) via a substrate sequence of matrix metalloproteinase (MMP). The binding activities and the biological activities of Alb-CTLA4Ig before and after MMP digestion were analyzed by a cell-based ELISA and an in vitro Jurkat T cell activation assay. The efficacy and safety of Alb-CTLA4Ig in treating joint inflammation were tested in mouse collagen-induced arthritis. Results Alb-CTLA4Ig is stable and inactive under physiological conditions but can be fully activated by MMPs. The binding activity of nondigested Alb-CTLA4Ig was at least 10,000-fold weaker than that of MMP-digested Alb-CTLA4Ig. Nondigested Alb-CTLA4Ig was unable to inhibit Jurkat T cell activation, whereas MMP-digested Alb-CTLA4Ig was as potent as conventional CTLA4Ig in inhibiting the T cells. Alb-CTLA4Ig was converted to CTLA4Ig in the inflamed joints to treat mouse collagen-induced arthritis, showing similar efficacy to that of conventional CTLA4Ig. In contrast to conventional CTLA4Ig, Alb-CTLA4Ig did not inhibit the antimicrobial responses in the spleens of the treated mice. Conclusions Our study indicates that Alb-CTLA4Ig can be activated by MMPs to suppress tissue inflammation in situ. Thus, Alb-CTLA4Ig is a safe and effective treatment for collagen-induced arthritis in mice.

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