Novel anti-malarial hydroxynaphthoquinones with potent broad spectrum anti-protozoal activity

Hudson, A. T.; Randall, A. W.; Fry, Mitchell; Ginger, Colin D.; Hill, B. D.; Latter, Victoria S.; McHardy, N.; Williams, R. B.

doi:10.1017/s0031182000049003

Cited by 176 publications

(85 citation statements)

References 23 publications

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“…The B-cell characteristics of this line grown in our laboratory have been confirmed recently (Moreau et al, 1999), and its cultivation has been described previously (Chaussepied et al, 1998). To eliminate the parasite, the hydroxynaphthoquinone derivative BW720 (Hudson et al, 1985) was added at 30 ng ml 21 . BW720c treatment was performed for 48±72 h, and cell viability was routinely tested by trypan blue exclusion (BW720c-treated cells are also referred to in this text as cured').…”

Section: Cells and Cell Culturementioning

confidence: 82%

“…The macroschizont induces its host leucocyte to proliferate, and the transformation process both propagates the parasite and clonally expands the host cell population, with often fatal consequences for the infected animal (reviewed by Chaussepied and Langsley, 1996). Unusually for a transformed cell, the phenotype can be reversed as, upon drug-induced parasite death, the leucocyte either returns to a quiescent state, or dies (Hudson et al, 1985). Theileria-transformed leucocytes can be grown continuously in vitro without the addition of any exogenous growth factors, and form metastatic tumours when injected into scid mice (Fell et al, 1990).…”

Section: Introductionmentioning

confidence: 99%

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Constitutive PI3-K activity is essential for proliferation, but not survival, of Theileria parva-transformed B cells

et al. 2000

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SummaryTheileria is an intracellular parasite that causes lymphoproliferative disorders in cattle, and infection of leucocytes induces a transformed phenotype similar to tumour cells, but the mechanisms by which the parasite induces this phenotype are not understood. Here, we show that infected B lymphocytes display constitutive phosphoinositide 3-kinase (PI3-K) activity, which appears to be necessary for proliferation, but not survival. Importantly, we demonstrate that one mechanism by which PI3-K mediates the proliferation of infected B lymphocytes is through the induction of a granulocyte±monocyte colony-stimulating factor (GM-CSF)-dependent autocrine loop. PI3-K induction of GM-CSF appears to be at the transcriptional level and, consistently, we demonstrate that PI3-K is also involved in the constitutive induction of AP-1 and NF-kB, which characterizes Theileria-infected leucocytes. Taken together, our results highlight a novel strategy exploited by the intracellular parasite Theileria to induce continued proliferation of its host leucocyte.

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Section: Cells and Cell Culturementioning

confidence: 82%

Section: Introductionmentioning

confidence: 99%

Constitutive PI3-K activity is essential for proliferation, but not survival, of Theileria parva-transformed B cells

et al. 2000

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“…It is difficult to explain the mechanism of this synergism (arteether and buparvaquone) in the present study. Buparvaquone acts selectively against the parasite's electron transport system at ubiquinone-cytochrome c reductase of the respiratory chain [14,11] while artemisinin-type compounds are found to block heme polymerization, causing a buildup of monomeric free heme toxic to the parasite [23]. Hence the combination might have worked well to suppress the increasing parasitaemia.…”

Section: Discussionmentioning

confidence: 99%

<i>In-vivo</i> Therapeutic Efficacy Trial with Artemisinin Derivative, Buparvaquone and Imidocarb Dipropionate against <i>Babesia equi</i> Infection in Donkeys

Kumar

Gupta

Pal

et al. 2003

The Journal of Veterinary Medical Science

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ABSTRACT. The therapeutic efficacy of imidocarb, artesunate, arteether, buparvaquone and arteether+buparvaquone combination was evaluated against Babesia equi of Indian origin in splenectomised donkeys with experimentally induced acute infection. Efficacies of these drugs were tested by administering each drug or drug combination to groups of donkeys (having three donkeys each group). One gr oup of donkey was kept as untreated control for comparing the results. Parasitaemia, haematology (WBC, RBC, PCV, granulocytes and h aemoglobin), biochemical parameters (SAST, SALT, alkaline phosphatase, albumin/globulin ratio) were monitored at regular intervals. Individually, arteether and buparvaquone were found to have no parasite clearing efficacy and the treated animals died within 5-6 days after showing high parasitaemia and clinical symptoms of the disease. However, artesunate treated animals were able to restrict the parasite multiplication but only during the treatment period. Animals treated with imidocarb and arteether+buparvaquone combination were able to clear the parasite from the blood circulation after 2-5 days post-treatment (PT). After 55-58 days PT, recrudescence of B. equi parasite was observed in both these groups and a mean survival period of 66 days and 69 days, respectively, was recorded in these groups. Results of haemato-biochemical parameters had shown that imidocarb had deleterious effect on the liver function while on the other hand arteether+buparvaquone combination was found to be safe. This limited study indicates that arteether+buparvaquone combination c ould be a better choice than imidocarb for treating B. equi infection, but further trials are required in detail. KEY WORDS: artemisinin derivative, Babesia equi, buparvaquone, imidocarb dipropionate, treatment.

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“…These transformed cells, primarily T cells, disseminate to lymphoid and nonlymphoid tissues, including the lung, kidney, and, intestine, where they mimic the behavior of lymphoid tumors (10,11). Remarkably unlike true lymphomas, T. parva-induced transformation can be reversed by killing the parasite (9,(10)(11)(12). This drug-induced reversal to normal lymphocyte regulation indicates that T. parva alone is sufficient and responsible for transformation.…”

Section: Introductionmentioning

confidence: 99%

“…This autocrine growth is, at least partially, attributable to parasite-induced expression of both interleukin 2 (IL-2) and the ␣-chain of the IL-2 receptor (IL-2R␣) (9,(13)(14)(15)(16). Treatment with the theilericidal drug BW720c (a protozoal-specific hydronaphthoquinone) results in down-regulation of IL-2 and IL-2R␣ expression and restoration of growth factor dependence (9,12). Both IL-2 and IL-2R␣ are transcriptionally regulated by cis-acting B enhancer elements that are, in turn, controlled by dimeric complexes of the NFB family of transcription factors (17,18).…”

Section: Introductionmentioning

confidence: 99%

Parasite-mediated nuclear factor κB regulation in lymphoproliferation caused byTheileria parva infection

Palmer

Machado²,

Fernández³

et al. 1997

Proc. Natl. Acad. Sci. U.S.A.

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one of the authors regrets that she inadvertently omitted references to the computer program and protein potential function that the authors used for their simulations of barnase cited above. The following sentence should have been the first sentence of the Methods section: Molecular dynamics simulations were performed with the program ENCAD (44) and the potential energy function of Levitt et al. (45).

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Novel anti-malarial hydroxynaphthoquinones with potent broad spectrum anti-protozoal activity

Abstract: Novel hydroxynaphthoquinones are reported with outstanding efficacy against Plasmodium, Eimeria and Theileria species. Biochemical evidence is presented for the selective toxicity of these compounds being due to inhibition of parasite respiratory systems.

Cited by 176 publications

References 23 publications

Constitutive PI3-K activity is essential for proliferation, but not survival, of Theileria parva-transformed B cells

Constitutive PI3-K activity is essential for proliferation, but not survival, of Theileria parva-transformed B cells

<i>In-vivo</i> Therapeutic Efficacy Trial with Artemisinin Derivative, Buparvaquone and Imidocarb Dipropionate against <i>Babesia equi</i> Infection in Donkeys

Parasite-mediated nuclear factor κB regulation in lymphoproliferation caused byTheileria parva infection

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