In vitro and in vivo anti-malarial activity of novel harmine-analog heat shock protein 90 inhibitors: a possible partner for artemisinin

Bayih, Abebe Genetu; Folefoc, Asongna; Mohon, Abu Naser; Eagon, Scott; Anderson, Marc O.; Pillai, Dylan R.

doi:10.1186/s12936-016-1625-7

Cited by 37 publications

(14 citation statements)

References 41 publications

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“…A 72 h in vitro growth inhibition assay [40,41] was used to test the antimalarial activity of LZ1. P. falciparum line 3D7 was cultured in complete RPMI-1640 medium with 2% hematocrit and incubated in a humidified atmosphere with 5% O 2 , 5% CO 2 , and 90% N 2 at 37 °C.…”

Section: Methodsmentioning

confidence: 99%

In Vitro and In Vivo Antimalarial Activity of LZ1, a Peptide Derived from Snake Cathelicidin

Fang

Zhang

et al. 2019

Toxins

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Antimalarial drug resistance is an enormous global threat. Recently, antimicrobial peptides (AMPs) are emerging as a new source of antimalarials. In this study, an AMP LZ1 derived from snake cathelicidin was identified with antimalarial activity. In the in vitro antiplasmodial assay, LZ1 showed strong suppression of blood stage Plasmodium falciparum (P. falciparum) with an IC50 value of 3.045 μM. In the in vivo antiplasmodial assay, LZ1 exerted a significant antimalarial activity against Plasmodium berghei (P. berghei) in a dose- and a time- dependent manner. In addition, LZ1 exhibited anti-inflammatory effects and attenuated liver-function impairment during P. berghei infection. Furthermore, by employing inhibitors against glycolysis and oxidative phosphorylation in erythrocytes, LZ1 specifically inhibited adenosine triphosphate (ATP) production in parasite-infected erythrocyte by selectively inhibiting the pyruvate kinase activity. In conclusion, the present study demonstrates that LZ1 is a potential candidate for novel antimalarials development.

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Section: Methodsmentioning

confidence: 99%

In Vitro and In Vivo Antimalarial Activity of LZ1, a Peptide Derived from Snake Cathelicidin

Fang

Zhang

et al. 2019

Toxins

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“…Similarly, 17A and 21A, two harmine derivatives acting as anti-malarial agents. These were found more active as compared to chloroquine and artemisinin due to the substitution of halogens (Bayih et al, 2016).…”

Section: Structure Activity Relationshipmentioning

confidence: 99%

“…Primitive studies have declared that harmine is an auspicious anti-malarial agent selectively targeting P. falciparum PfHsp90. The unique and non-toxic harmine analogues 17A and 21A have the affinity to bind with heat shock protein-90, inhibits P. falciparum at concentration of 4.2 ± 1.3 µM and 5.7 ± 1.7 µM during in vitro investigation, decreases parasitaemia and extends survival of P. berghei-affected BALB/c mice (100 mg/kg) in vivo (Bayih et al, 2016).…”

Section: Other Biological Activities Of Harminementioning

confidence: 99%

Harmine and its derivatives: Biological activities and therapeutic potential in human diseases

Javeed

Rasul

Hussain

et al. 2018

Bangladesh J Pharmacol

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<p>This review article aims to provide an update on the sources, pharmaco-logical and biological profile of a β-carboline alkaloid, harmine which is a major bioactive component of various plants mainly Peganum harmala. Harmine’s wide range of pharmacological properties has been well-documented as anti-cancer, anti-inflammatory, anti-oxidant, neuroprotective, anti-depressant, and antimicrobial. Although reported data suggests a multifunctional pharmacological role of harmine but farther experimentation on its molecular mechanism of action, synthetic chemistry approaches, and preclinical studies are yet obligatory to fully uncover its pharmacological efficacy.</p>

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“…Targeting of Hsp90 in combination therapy has been shown to be effective in reversing resistance to chloroquine by P. falciparum [60]. In addition, two harmine-based inhibitors of PfHsp90 (harmine 17A and harmine 21A) were reportedly effective at reversing both chloroquine and artemisinin resistance based on a mouse malaria model (Figure 2) [60,64,75]. This further highlights the prospects of targeting heat shock proteins in combination therapies against parasites to recover the efficacy of traditional drugs to which parasites are currently resistant.…”

Section: Hsp90 Familymentioning

confidence: 99%

Small Molecule Inhibitors Targeting the Heat Shock Protein System of Human Obligate Protozoan Parasites

Zininga

Shonhai

2019

IJMS

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Obligate protozoan parasites of the kinetoplastids and apicomplexa infect human cells to complete their life cycles. Some of the members of these groups of parasites develop in at least two systems, the human host and the insect vector. Survival under the varied physiological conditions associated with the human host and in the arthropod vectors requires the parasites to modulate their metabolic complement in order to meet the prevailing conditions. One of the key features of these parasites essential for their survival and host infectivity is timely expression of various proteins. Even more importantly is the need to keep their proteome functional by maintaining its functional capabilities in the wake of physiological changes and host immune responses. For this reason, molecular chaperones (also called heat shock proteins)—whose role is to facilitate proteostasis—play an important role in the survival of these parasites. Heat shock protein 90 (Hsp90) and Hsp70 are prominent molecular chaperones that are generally induced in response to physiological stress. Both Hsp90 and Hsp70 members are functionally regulated by nucleotides. In addition, Hsp70 and Hsp90 cooperate to facilitate folding of some key proteins implicated in cellular development. In addition, Hsp90 and Hsp70 individually interact with other accessory proteins (co-chaperones) that regulate their functions. The dependency of these proteins on nucleotide for their chaperone function presents an Achille’s heel, as inhibitors that mimic ATP are amongst potential therapeutic agents targeting their function in obligate intracellular human parasites. Most of the promising small molecule inhibitors of parasitic heat shock proteins are either antibiotics or anticancer agents, whose repurposing against parasitic infections holds prospects. Both cancer cells and obligate human parasites depend upon a robust protein quality control system to ensure their survival, and hence, both employ a competent heat shock machinery to this end. Furthermore, some inhibitors that target chaperone and co-chaperone networks also offer promising prospects as antiparasitic agents. The current review highlights the progress made so far in design and application of small molecule inhibitors against obligate intracellular human parasites of the kinetoplastida and apicomplexan kingdoms.

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In vitro and in vivo anti-malarial activity of novel harmine-analog heat shock protein 90 inhibitors: a possible partner for artemisinin

Cited by 37 publications

References 41 publications

In Vitro and In Vivo Antimalarial Activity of LZ1, a Peptide Derived from Snake Cathelicidin

In Vitro and In Vivo Antimalarial Activity of LZ1, a Peptide Derived from Snake Cathelicidin

Harmine and its derivatives: Biological activities and therapeutic potential in human diseases

Small Molecule Inhibitors Targeting the Heat Shock Protein System of Human Obligate Protozoan Parasites

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