Semi-Synthetic Analogues of Cryptolepine as a Potential Source of Sustainable Drugs for the Treatment of Malaria, Human African Trypanosomiasis, and Cancer

Yabalu Z Abacha; Arnold Donkor Forkuo; Stephen Y Gbedema; Nimisha Mittal; Sabine Ottilie; Frances Rocamora; Elizabeth A Winzeler; Donelly A van Schalkwyk; John M Kelly; Martin C Taylor; Janette Reader; Lyn-Marie Birkholtz; David R Lisgarten; Jeremy K Cockcroft; John N Lisgarten; Rex A Palmer; Rosemary C Talbert; Steven D Shnyder; Colin W Wright

doi:10.3389/fphar.2022.875647

Semi-Synthetic Analogues of Cryptolepine as a Potential Source of Sustainable Drugs for the Treatment of Malaria, Human African Trypanosomiasis, and Cancer

Front Pharmacol. 2022 Apr 26:13:875647. doi: 10.3389/fphar.2022.875647. eCollection 2022.

Authors

Yabalu Z Abacha^{1

2}, Arnold Donkor Forkuo³, Stephen Y Gbedema⁴, Nimisha Mittal⁵, Sabine Ottilie⁵, Frances Rocamora⁵, Elizabeth A Winzeler⁵, Donelly A van Schalkwyk⁶, John M Kelly⁶, Martin C Taylor⁶, Janette Reader⁷, Lyn-Marie Birkholtz⁷, David R Lisgarten⁸, Jeremy K Cockcroft⁹, John N Lisgarten¹⁰, Rex A Palmer¹¹, Rosemary C Talbert⁸, Steven D Shnyder¹², Colin W Wright¹

Affiliations

¹ School of Pharmacy and Medical Sciences, University of Bradford, Bradford, United Kingdom.
² Department of Pharmacognosy, Faculty of Pharmacy, University of Maiduguri, Maiduguri, Nigeria.
³ Department of Pharmacology, Faculty of Pharmacy and Pharmaceutical Sciences, College of Health Sciences, Kwame Nkrumah University of Science and Technology (KNUST), Kumasi, Ghana.
⁴ Department of Pharmaceutics, Faculty of Pharmacy and Pharmaceutical Sciences, College of Health Sciences, KNUST, Kumasi, Ghana.
⁵ Malaria Drug Accelerator (MalDA) Consortium, School of Medicine, University of California, San Diego, La Jolla, CA, United States.
⁶ Department of Infection Biology, Faculty of Infectious and Tropical Diseases, London School of Hygiene and Tropical Medicine, London, United Kingdom.
⁷ Department of Biochemistry, Genetics and Microbiology, Faculty of Natural and Agricultural Sciences, Institute for Sustainable Malaria Control, University of Pretoria, Hatfield, South Africa.
⁸ Biomolecular Research Group, School of Psychology and Life Sciences, Canterbury Christ Church University, Canterbury, United Kingdom.
⁹ Department of Chemistry, Christopher Ingold Laboratories, University College London, London, United Kingdom.
¹⁰ School of Science, University of Greenwich, Chatham, United Kingdom.
¹¹ Department of Crystallography, Biochemical Sciences, Birkbeck College, University of London, London, United Kingdom.
¹² School of Pharmacy and Medical Sciences, Institute of Cancer Therapeutics, University of Bradford, Bradford, United Kingdom.

Abstract

The prospect of eradicating malaria continues to be challenging in the face of increasing parasite resistance to antimalarial drugs so that novel antimalarials active against asexual, sexual, and liver-stage malaria parasites are urgently needed. In addition, new antimalarials need to be affordable and available to those most in need and, bearing in mind climate change, should ideally be sustainable. The West African climbing shrub Cryptolepis sanguinolenta is used traditionally for the treatment of malaria; its principal alkaloid, cryptolepine (1), has been shown to have antimalarial properties, and the synthetic analogue 2,7-dibromocryptolepine (2) is of interest as a lead toward new antimalarial agents. Cryptolepine (1) was isolated using a two-step Soxhlet extraction of C. sanguinolenta roots, followed by crystallization (yield 0.8% calculated as a base with respect to the dried roots). Semi-synthetic 7-bromo- (3), 7, 9-dibromo- (4), 7-iodo- (5), and 7, 9-dibromocryptolepine (6) were obtained in excellent yields by reaction of 1 with N-bromo- or N-iodosuccinimide in trifluoroacetic acid as a solvent. All compounds were active against Plasmodia in vitro, but 6 showed the most selective profile with respect to Hep G2 cells: P. falciparum (chloroquine-resistant strain K1), IC₅₀ = 0.25 µM, SI = 113; late stage, gametocytes, IC₅₀ = 2.2 µM, SI = 13; liver stage, P. berghei sporozoites IC₅₀ = 6.13 µM, SI = 4.6. Compounds 3-6 were also active against the emerging zoonotic species P. knowlesi with 5 being the most potent (IC₅₀ = 0.11 µM). In addition, 3-6 potently inhibited T. brucei in vitro at nM concentrations and good selectivity with 6 again being the most selective (IC₅₀ = 59 nM, SI = 478). These compounds were also cytotoxic to wild-type ovarian cancer cells as well as adriamycin-resistant and, except for 5, cisplatin-resistant ovarian cancer cells. In an acute oral toxicity test in mice, 3-6 did not exhibit toxic effects at doses of up to 100 mg/kg/dose × 3 consecutive days. This study demonstrates that C. sanguinolenta may be utilized as a sustainable source of novel compounds that may lead to the development of novel agents for the treatment of malaria, African trypanosomiasis, and cancer.

Keywords: Plasmodium falciparum; Plasmodium knowlesi; Trypanosoma brucei; halogenation of cryptolepine; ovarian cancer; sustainable pharmaceuticals.

Grants and funding

MR/T015969/1/MRC_/Medical Research Council/United Kingdom