A CD6-targeted antibody-drug conjugate as a potential therapy for T cell–mediated disorders
Lingjun Zhang, Liping Luo, Jin Y. Chen, Rupesh Singh, William M. Baldwin III, David A. Fox, Daniel J. Lindner, Daniel F. Martin, Rachel R. Caspi, Feng Lin
Lingjun Zhang, Liping Luo, Jin Y. Chen, Rupesh Singh, William M. Baldwin III, David A. Fox, Daniel J. Lindner, Daniel F. Martin, Rachel R. Caspi, Feng Lin
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Research Article

A CD6-targeted antibody-drug conjugate as a potential therapy for T cell–mediated disorders

Abstract

The selective targeting of pathogenic T cells is a holy grail in the development of new therapeutics for T cell–mediated disorders, including many autoimmune diseases and graft versus host disease. We describe the development of a CD6-targeted antibody-drug conjugate (CD6-ADC) by conjugating an inactive form of monomethyl auristatin E (MMAE), a potent mitotic toxin, onto a mAb against CD6, an established T cell surface marker. Even though CD6 is present on all T cells, only the activated (pathogenic) T cells vigorously divide and thus are susceptible to the antimitotic MMAE-mediated killing via the CD6-ADC. We found CD6-ADC selectively killed activated proliferating human T cells and antigen-specific mouse T cells in vitro. Furthermore, in vivo, whereas the CD6-ADC had no significant detrimental effect on normal T cells in naive CD6-humanized mice, the same dose of CD6-ADC, but not the controls, efficiently treated 2 preclinical models of autoimmune uveitis and a model of graft versus host disease. These results provide evidence suggesting that CD6-ADC could be further developed as a potential therapeutic agent for the selective elimination of pathogenic T cells and treatment of many T cell–mediated disorders.

Authors

Lingjun Zhang, Liping Luo, Jin Y. Chen, Rupesh Singh, William M. Baldwin III, David A. Fox, Daniel J. Lindner, Daniel F. Martin, Rachel R. Caspi, Feng Lin

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Figure 2

CD6-ADC kills activated antigen-specific T cells.

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CD6-ADC kills activated antigen-specific T cells. Splenocytes from immun...
Splenocytes from immunized mice were restimulated with 20 μg/mL of the same IRBP peptide in the presence of different concentrations (0.5, 2, 4 nM) of CD6-ADC or anti-CD6 IgG or mIgG for 3 days. BrdU was added 16 hours before the analyses. Proliferating CD4+ T cells after IRBP restimulation were identified as CD4+BrdU+ cells by flow cytometry. (A) Representative results of the CD4+BrdU+ T cells in different groups. (B) Summary results of the CD4+BrdU+ T cell quantification in different groups. Data represent mean ± SEM. **P < 0.01. Two-way ANOVA and Bonferroni’s multiple-comparison test.