<i>In Vitro</i>
            Antimalarial Activity of Novel Semisynthetic Nocathiacin I Antibiotics

Sharma, Indu; Sullivan, Margery; McCutchan, Thomas F.

doi:10.1128/aac.04294-14

Cited by 18 publications

(14 citation statements)

References 26 publications

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“…498 Thus, unlike other eukaryotes, P. falciparum is sensitive to many thiopeptides such as thiostrepton, micrococcin, and GE2270, and nocathiacin. 499–508 Other protein synthesis inhibitors also have demonstrated a similar anti-malarial activity. 509–511 However, it should be noted that protease inhibitors are additionally known to be active against the Plasmodium parasite, as the proteasome is crucial for development.…”

Section: Thiopeptidesmentioning

confidence: 99%

YcaO-Dependent Posttranslational Amide Activation: Biosynthesis, Structure, and Function

et al. 2017

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With advances in sequencing technology, uncharacterized proteins and domains of unknown function (DUFs) are rapidly accumulating in sequence databases and offer an opportunity to discover new protein chemistry and reaction mechanisms. The focus of this review, the formerly enigmatic YcaO superfamily (DUF181), has been found to catalyze a unique phosphorylation of a ribosomal peptide backbone amide upon attack by different nucleophiles. Established nucleophiles are the side chains of Cys, Ser, and Thr which gives rise to azoline/azole biosynthesis in ribosomally synthesized and posttranslationally modified peptide (RiPP) natural products. However, much remains unknown about the potential for YcaO proteins to collaborate with other nucleophiles. Recent work suggests potential in forming thioamides, macroamidines, and possibly additional post-translational modifications. This review covers all knowledge through mid-2016 regarding the biosynthetic gene clusters (BGCs), natural products, functions, mechanisms, and applications of YcaO proteins and outlines likely future research directions for this protein superfamily.

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Section: Thiopeptidesmentioning

confidence: 99%

YcaO-Dependent Posttranslational Amide Activation: Biosynthesis, Structure, and Function

et al. 2017

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“…Their mechanisms of action on Plasmodium have not been as well described, although a number of studies have addressed this issue. There are three categories of ribosomes in Plasmodium : mitochondrial, plastid and nuclear [ 28 ]. As suggested by three studies [ 29 – 31 ], tetracycline may directly inhibit mitochondrial protein synthesis and also decrease the activity of a mitochondrial enzyme (i.e., dihydroorotate dehydrogenase) involved in de novo pyrimidine synthesis [ 32 ].…”

Section: Mechanism Of Actionmentioning

confidence: 99%

“…Doxycycline at a dose of 100 mg/day starting at the day of arrival in endemic areas and continuing for up to 4 weeks after returning, still remains highly effective as P. falciparum prophylaxis. Concerning the treatment of malaria, studies conducted in the 1950s [ 28 , 39 ] and in 1970 [ 40 , 41 , 66 , 67 ] have shown the effectiveness of cycline monotherapy in treating simple access to P. falciparum . Later, the need for a minimum 7-day treatment was demonstrated; the disappearance of parasites was effective only after 5 days at a dose of 200 mg daily [ 68 ].…”

Section: Clinical Effectivenessmentioning

confidence: 99%

Tetracyclines in malaria

Gaillard

Madamet

Pradines

2015

Malar J

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Malaria, a parasite vector-borne disease, is one of the greatest health threats in tropical regions, despite the availability of malaria chemoprophylaxis. The emergence and rapid extension of Plasmodium falciparum resistance to various anti-malarial drugs has gradually limited the number of potential malaria therapeutics available to clinicians. In this context, doxycycline, a synthetically derived tetracycline, constitutes an interesting alternative for malaria treatment and prophylaxis. Doxycycline is a slow-acting blood schizontocidal agent that is highly effective at preventing malaria. In areas with chloroquine and multidrug-resistant P. falciparum parasites, doxycycline has already been successfully used in combination with quinine to treat malaria, and it has been proven to be effective and well-tolerated. Although not recommended for pregnant women and children younger than 8 years of age, severe adverse effects are rarely reported. In addition, resistance to doxycycline is rarely described. Prophylactic and clinical failures of doxycycline have been associated with both inadequate doses and poor patient compliance. The effects of tetracyclines on parasites are not completely understood. A better comprehension of the mechanisms underlying drug resistance would facilitate the identification of molecular markers of resistance to predict and survey the emergence of resistance.

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“…A water-soluble derivative of nocathiacin exerted an irreversible growth inhibition within the first growth cycle at a nanomolar range against chloroquine-susceptible and resistant P. falciparum strains and was immediately effective [120]. Further investigations need to be done on this drug and its derivatives to understand its mode of action P. falciparum .…”

Section: Thiopeptides: Thiostrepton and Nocathiacinmentioning

confidence: 99%

Antibiotics in malaria therapy: which antibiotics except tetracyclines and macrolides may be used against malaria?

Gaillard

Madamet

Tsombeng

et al. 2016

Malar J

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Malaria, a parasite vector-borne disease, is one of the most significant health threats in tropical regions, despite the availability of individual chemoprophylaxis. Malaria chemoprophylaxis and chemotherapy remain a major area of research, and new drug molecules are constantly being developed before drug-resistant parasites strains emerge. The use of anti-malarial drugs is challenged by contra-indications, the level of resistance of Plasmodium falciparum in endemic areas, clinical tolerance and financial cost. New therapeutic approaches are currently needed to fight against this disease. Some antibiotics that have shown potential effects on malaria parasite have been recently studied in vitro or in vivo intensively. Two families, tetracyclines and macrolides and their derivatives have been particularly studied in recent years. However, other less well-known have been tested or are being used for malaria treatment. Some of these belong to older families, such as quinolones, co-trimoxazole or fusidic acid, while others are new drug molecules such as tigecycline. These emerging antibiotics could be used to prevent malaria in the future. In this review, the authors overview the use of antibiotics for malaria treatment.

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In Vitro Antimalarial Activity of Novel Semisynthetic Nocathiacin I Antibiotics

Cited by 18 publications

References 26 publications

YcaO-Dependent Posttranslational Amide Activation: Biosynthesis, Structure, and Function

YcaO-Dependent Posttranslational Amide Activation: Biosynthesis, Structure, and Function

Tetracyclines in malaria

Antibiotics in malaria therapy: which antibiotics except tetracyclines and macrolides may be used against malaria?

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