Biomedicines (Oct 2018)

Azasulfurylpeptide Modulation of CD36-Mediated Inflammation Without Effect on Neovascularization

  • Stéphane Turcotte,
  • Katia Mellal,
  • Ramesh Chingle,
  • Mukandila Mulumba,
  • Samy Omri,
  • Lylia Dif-Yaiche,
  • Sylvain Chemtob,
  • Huy Ong,
  • William D. Lubell

DOI
https://doi.org/10.3390/biomedicines6040098
Journal volume & issue
Vol. 6, no. 4
p. 98

Abstract

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Modulation of the cluster of differentiation-36 receptor (CD36) has proven promising for dampening pro-inflammatory macrophage signaling. For example, azapeptides (e.g., 1 and 2) bind CD36 selectively with high affinity, mitigate Toll-like receptor (TLR) agonist-induced overproduction of nitric oxide (NO), and reduce pro-inflammatory cytokine and chemokine production in macrophages. Moreover, semicarbazides 1 and 2 inhibit microvascular sprouting mediated through CD36 in the choroid explant. Seeking a selective CD36 modulator that mediated inflammation without influencing neovascularization, a set of azasulfurylpeptides (e.g., 3a–e) were synthesized in which the semicarbazide was replaced by an N-aminosulfamide residue using a novel solid-phase approach. Notably, azasulfurylpeptide 3c diminished selectively CD36-mediated TLR-2-triggered inflammatory response without affecting neovascularization. Subtle chemical modification at the peptide backbone from a carbonyl to a sulfuryl residue has had a selective effect on biological activity providing a valuable probe for studying CD36 chemical biology.

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