Literature DB >> 10333319

Bisquinoline antimalarials: their role in malaria chemotherapy.

K Raynes1.   

Abstract

Quinoline compounds, such as chloroquine, are used widely to treat malaria; however, the malarial parasite is rapidly becoming resistant to the drugs currently available. Presently, rational drug design is hindered considerably due to the mode of action of chloroquine being poorly understood. We rely on serendipity, rather than solid structural evidence, to generate new antimalarials. Hence any insight into the possible modes of action of quinoline antimalarials, including the bisquinolines, would greatly aid rational drug design. The quinoline antimalarial drugs, chloroquine, quinine and mefloquine, are thought to act by interfering with the digestion of haemoglobin in the blood stages of the malaria life-cycle. These quinoline antimalarials traverse down the pH gradient to accumulate to millimolar concentrations in the acidic vacuole of the parasite. It has been suggested that this high intravacuolar concentration prevents haem sequestration, causing a build up of the toxic haem moiety and the death of the parasite by its own toxic waste. The actual mechanism by which the parasite sequesters haem and the drug target(s) during this process, however, still remains elusive. As a consequence, haem polymerisation and the efficiency of quinoline antimalarials, including the bisquinolines, as inhibitors of this process has been investigated. In this paper, the potential role of the bisquinolines in the fight against chloroquine-resistant malaria is addressed.

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Year:  1999        PMID: 10333319     DOI: 10.1016/s0020-7519(98)00217-3

Source DB:  PubMed          Journal:  Int J Parasitol        ISSN: 0020-7519            Impact factor:   3.981


  16 in total

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Authors:  Warren A Andayi; Timothy J Egan; Jiri Gut; Philip J Rosenthal; Kelly Chibale
Journal:  ACS Med Chem Lett       Date:  2013-05-20       Impact factor: 4.345

5.  Piperaquine and Lumefantrine resistance in Plasmodium berghei ANKA associated with increased expression of Ca2+/H+ antiporter and glutathione associated enzymes.

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6.  Outer-Sphere Control for Divergent Multicatalysis with Common Catalytic Moieties.

Authors:  Christopher R Shugrue; Bianca R Sculimbrene; Elizabeth R Jarvo; Brandon Q Mercado; Scott J Miller
Journal:  J Org Chem       Date:  2019-01-16       Impact factor: 4.354

7.  In vitro sensitivities of Plasmodium falciparum isolates from the China-Myanmar border to piperaquine and association with polymorphisms in candidate genes.

Authors:  Mingming Hao; Dandan Jia; Qing Li; Yongshu He; Lili Yuan; Shuhui Xu; Kexuan Chen; Jia Wu; Lijuan Shen; Lin Sun; Hongbin Zhao; Zhaoqing Yang; Liwang Cui
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8.  Potent Antimalarial Activity of Two Arenes Linked with Triamine Designed To Have Multiple Interactions with Heme.

Authors:  Yosuke Sakata; Kosuke Yabunaka; Yuko Kobayashi; Hirohisa Omiya; Naoki Umezawa; Hye-Sook Kim; Yusuke Wataya; Yoshimi Tomita; Yosuke Hisamatsu; Nobuki Kato; Hirokazu Yagi; Tadashi Satoh; Koichi Kato; Haruto Ishikawa; Tsunehiko Higuchi
Journal:  ACS Med Chem Lett       Date:  2018-09-24       Impact factor: 4.345

9.  Dihydroartemisinin-piperaquine and artemether-lumefantrine for treating uncomplicated malaria in African children: a randomised, non-inferiority trial.

Authors:  Quique Bassat; Modest Mulenga; Halidou Tinto; Patrice Piola; Steffen Borrmann; Clara Menéndez; Michael Nambozi; Innocent Valéa; Carolyn Nabasumba; Philip Sasi; Antonella Bacchieri; Marco Corsi; David Ubben; Ambrose Talisuna; Umberto D'Alessandro
Journal:  PLoS One       Date:  2009-11-17       Impact factor: 3.240

10.  Plasmodium berghei ANKA: selection of resistance to piperaquine and lumefantrine in a mouse model.

Authors:  D M Kiboi; B N Irungu; B Langat; S Wittlin; R Brun; J Chollet; O Abiodun; J K Nganga; V C S Nyambati; G M Rukunga; A Bell; A Nzila
Journal:  Exp Parasitol       Date:  2009-03-24       Impact factor: 2.011

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