Primaquine–quinoxaline 1,4-di-N-oxide hybrids with action on the exo-erythrocytic forms of Plasmodium induce their effect by the production of reactive oxygen species

Bonilla-Ramirez, Leonardo; Galiano, Silvia; Quiliano, Miguel; Aldana, Ignacio; Pabón, Adriana

doi:10.1186/s12936-019-2825-8

Cited by 13 publications

(6 citation statements)

References 42 publications

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“…Since many studies on QdNO derivatives are focused on their evolution as anti-tumor agents, one further prominent area of research is focused on anthelmintic compounds, notably those used to treat disorders namely malaria and trypanosomiasis, popularly known to be Chagas disease (Bonilla-Ramírez et al, 2019;Marin et al, 2008;Zarranz et al, 2006Zarranz et al, , 2011. Nifurtimox and benznidazole are the best-known medication for trypanosomiasis; these drugs act potent and effective in the initial phase of the disease, but in the chronic phase, their activity was found to be less active than initial phase.…”

Section: Anthelmintic Activitymentioning

confidence: 99%

An appraisal on synthetic and pharmaceutical perspectives of quinoxaline 1,4‐di‐N‐oxide scaffold

Agrawal

Bhardwaj

2022

Chem Biol Drug Des

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Quinoxaline 1,4‐di‐N‐oxides (QdNOs) exhibit multifaceted biological properties, wherein antimicrobial, anticancer, antitrypanosomal, and anti‐inflammatory properties are included. Because of their various activities in clinical practice and research, they have a wide spectrum of uses and possibilities. QdNOs have received a significant amount of attention, and research into their medicinal chemistry is still a part of experimental investigation and analytical studies. In this review, QdNOs are classified depending on their actions, which include antibacterial and anti‐mycobacterial, anticancer or antitumor, antimalarial, antifungal, and other activities. In a conclusion, it's important to base the development of novel synthetic techniques and the design of new QdNO derivatives on the most up‐to‐date knowledge gleaned from recent research. With the summarised structure–activity relationship of fascinating QdNOs, this review aims to provide insights into the developments in the chemistry and biological activity of QdNO derivatives.

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Section: Anthelmintic Activitymentioning

confidence: 99%

An appraisal on synthetic and pharmaceutical perspectives of quinoxaline 1,4‐di‐N‐oxide scaffold

Agrawal

Bhardwaj

2022

Chem Biol Drug Des

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“…However, several PQ‐QdNO hybrids inhibited the developmental process of P. yoelii within HepG2‐CD81 cells by promoting ROS formation in the parasite and did not produce any mitochondrial depolarization, suggesting a mechanism of damage independent of mitochondrial signaling. The increase in ROS production was also associated with an increase in total glutathione levels (tGSH) in the infected cells and the alteration of the expression of some molecules related to oxidative stress, such as glutathione peroxidase 1 (GPX1) and DJ‐1 protein (Bonilla‐Ramírez et al., 2019).…”

Section: Quinoxaline and Qdnos Derivatives Main Targetsmentioning

confidence: 99%

Current status of quinoxaline and quinoxaline 1,4‐di‐N‐oxides derivatives as potential antiparasitic agents

Soto‐Sanchez

Ospina-Villa

2021

Chem Biol Drug Des

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Parasitic diseases are a public health problem, especially in developing countries where millions of people are affected every year. Current treatments have several drawbacks: emerging resistance to the existing drugs, lack of efficacy, and toxic side effects. Therefore, new antiparasitic drugs are urgently needed to treat and control diseases that affect human health, such as malaria, Chagas disease, leishmaniasis, amebiasis, giardiasis schistosomiasis, and filariasis, among others. Quinoxaline is a compound containing a benzene ring and a pyrazine ring. The oxidation of both pyrazine ring nitrogens allows the obtention of quinoxaline 1,4-di-N-oxides (QdNOs) derivatives. By modifying the chemical structure of these compounds, it is possible to obtain a wide variety of biological properties. This review investigated the activity of quinoxaline derivatives and QdNOs against different protozoan parasites and helminths. We also cover the structure-activity relationship (SAR) and summarize the main findings related to their mechanisms of action from published works in recent years. However, further studies are needed to determine specific molecular targets. This review aims to highlight the new development of antiparasitic drugs with better pharmacological profiles than current treatments.

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“…Failure to convert heme to its biocrystallization or biomineralization form will oxidize the parasite food vacuole membranes destroying it in the process. Chloroquine and other 4-aminoquinolines use this principle to dislocate parasite proliferation by inhibiting heme biocrystallization in pRBC's and increasing OS [85][86][87][88][89].…”

Section: Malarial Oxidative Stress-driven Inflammatory Responsementioning

confidence: 99%

Malarial Inflammation-Driven Pathophysiology and Its Attenuation by Triterpene Phytotherapeutics

Mavondo¹,

Mkhwanazi²,

Mzingwane³

et al. 2020

Parasitology and Microbiology Research

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Malaria driven pathophysiology inimically conjoined to systemic inflammation response cascade in a vicious feed-forward cycle destined to a terrible debilitation or demise of the host. The Plasmodium parasite initiates physiological changes when it is transmitted into the human host by intermediate host and vector. Sporozoites injection elicits immunological and inflammatory response suppression facilitating movement into the blood stream undetected, destined to hepatocyte. Subsequently, hepatocyte invasion culminates in intracellular growth and conversion of the parasites rapturing hepatocytes releasing merozoites into the extrahepatic circulation. Inflammatory and immunological response initiation results in overt malarial disease symptoms. Initially, inflammatory response alleviates and curtails infection. Activation of leukocytes, lymphocytes, monocytes, and phagocytes secretes inflammatory mediators, chemokines, cytokines cytoadhering molecules which accelerate infection patency. Hormonal processes influence disease tolerance without necessarily interfering with parasitemia. Current treatment is anti-parasitic. Phytotherapeutic intervention in malaria is anti-parasitic and anti-disease effects that terminate the vicious cycle and alleviating disease. The phytochemicals, in malarial experimental and clinical work, include asiatic acid, maslinic acid, oleanolic acid, and inflammatory and immunological aberrations evolving in malaria and the effects of phytochemical therapeutics in the alleviation of the disease to enable leverage of future treatment regimens through harnessing existing plants materials is explored.

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Primaquine–quinoxaline 1,4-di-N-oxide hybrids with action on the exo-erythrocytic forms of Plasmodium induce their effect by the production of reactive oxygen species

Cited by 13 publications

References 42 publications

An appraisal on synthetic and pharmaceutical perspectives of quinoxaline 1,4‐di‐N‐oxide scaffold

An appraisal on synthetic and pharmaceutical perspectives of quinoxaline 1,4‐di‐N‐oxide scaffold

Current status of quinoxaline and quinoxaline 1,4‐di‐N‐oxides derivatives as potential antiparasitic agents

Malarial Inflammation-Driven Pathophysiology and Its Attenuation by Triterpene Phytotherapeutics

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