Total Synthesis and Antimalarial Activity of 2-(p-Hydroxybenzyl)-prodigiosins, Isoheptylprodigiosin, and Geometric Isomers of Tambjamine MYP1 Isolated from Marine Bacteria

  • J Med Chem. 2021 Jun 24;64(12):8739-8754. doi: 10.1021/acs.jmedchem.1c00748.
Papireddy Kancharla  1 Yuexin Li  2 Monish Yeluguri  1 Rozalia A Dodean  2 Kevin A Reynolds  1 Jane X Kelly  1  2
Affiliations
  • 1. Department of Chemistry, Portland State University, Portland, Oregon 97201, United States.
  • 2. Department of Veterans Affairs Medical Center, Portland, Oregon 97239, United States.
Abstract

Highly efficient and straightforward synthetic routes toward the first total synthesis of 2-(p-hydroxybenzyl)-prodigiosins (2-5), isoheptylprodigiosin (6), and geometric isomers of tambjamine MYP1 ((E/Z)-7) have been developed. The crucial steps involved in these synthetic routes are the construction of methoxy-bipyrrole-carboxaldehydes (MBCs) and a 20-membered macrocyclic core and a regioselective demethylation of MBC analogues. These new synthetic routes enabled us to generate several natural prodiginines 24-27 in larger quantity. All of the synthesized natural products exhibited potent asexual blood-stage antiplasmodial activity at low nanomolar concentrations against a panel of Plasmodium falciparum parasites, with a great therapeutic index. Notably, prodiginines 6 and 24-27 provided curative in vivo efficacy against erythrocytic Plasmodium yoelii at 25 mg/kg × 4 days via oral route in a murine model. No overt clinical toxicity or behavioral change was observed in any mice treated with prodiginines and tambjamines.