Scientific Reports (Dec 2023)

Heavy-chain antibody targeting of CD38 NAD+ hydrolase ectoenzyme to prevent fibrosis in multiple organs

  • Bo Shi,
  • Asif Amin,
  • Pranjali Dalvi,
  • Wenxia Wang,
  • Nicholas Lukacs,
  • Li Kai,
  • Paul Cheresh,
  • Thais R. Peclat,
  • Claudia C. Chini,
  • Eduardo N. Chini,
  • Wim van Schooten,
  • John Varga

DOI
https://doi.org/10.1038/s41598-023-49450-1
Journal volume & issue
Vol. 13, no. 1
pp. 1 – 10

Abstract

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Abstract The functionally pleiotropic ectoenzyme CD38 is a glycohydrolase widely expressed on immune and non-hematopoietic cells. By converting NAD+ to ADP-ribose and nicotinamide, CD38 governs organismal NAD+ homeostasis and the activity of NAD+-dependent cellular enzymes. CD38 has emerged as a major driver of age-related NAD+ decline underlying adverse metabolic states, frailty and reduced health span. CD38 is upregulated in systemic sclerosis (SSc), a chronic disease characterized by fibrosis in multiple organs. We sought to test the hypothesis that inhibition of the CD38 ecto-enzymatic activity using a heavy-chain monoclonal antibody Ab68 will, via augmenting organismal NAD+, prevent fibrosis in a mouse model of SSc characterized by NAD+ depletion. Here we show that treatment of mice with a non-cytotoxic heavy-chain antibody that selectively inhibits CD38 ectoenzyme resulted in NAD+ boosting that was associated with significant protection from fibrosis in multiple organs. These findings suggest that targeted inhibition of CD38 ecto-enzymatic activity could be a potential pharmacological approach for SSc fibrosis treatment.