Antiplasmodial Activity of [(Aryl)arylsulfanylmethyl]Pyridine

doi:10.1128/AAC.00898-07

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Antimicrobial Agents and Chemotherapy, February 2008, p. 705-715, Vol. 52, No. 2
0066-4804/08/$08.00+0 doi:10.1128/AAC.00898-07
Copyright © 2008, American Society for Microbiology. All Rights Reserved.

Antiplasmodial Activity of [(Aryl)arylsulfanylmethyl]Pyridine ^,^,

Sanjay Kumar,¹ Sajal Kumar Das,² Sumanta Dey,³ Pallab Maity,³ Mithu Guha,³ Vinay Choubey,¹ Gautam Panda,²^* and Uday Bandyopadhyay³^*

Drug Target Discovery and Development Division,¹ Medicinal and Process Chemistry Division, Central Drug Research Institute, Lucknow-226001, UP, India,² Division of Infectious Diseases and Immunology, Indian Institute of Chemical Biology, 4, Raja S. C. Mullick Road, Jadavpur, Kolkata 700032, West Bengal, India³

Received 10 July 2007/ Returned for modification 6 August 2007/ Accepted 29 October 2007

A series of [(aryl)arylsufanylmethyl]pyridines (AASMP) havebeen synthesized. These compounds inhibited hemozoin formation,formed complexes (K_D = 12 to 20 µM) with free heme (ferriprotoporphyrinIX) at a pH close to the pH of the parasite food vacuole, andexhibited antimalarial activity in vitro. The inhibition ofhemozoin formation may develop oxidative stress in Plasmodiumfalciparum due to the accumulation of free heme. Interestingly,AASMP developed oxidative stress in the parasite, as evidentfrom the decreased level of glutathione and increased formationof lipid peroxide, H₂O₂, and hydroxyl radical (·OH) inP. falciparum. AASMP also caused mitochondrial dysfunction bydecreasing mitochondrial potential ( ${Delta}$ ${Psi}$ m) in malaria parasite,as measured by both flow cytometry and fluorescence microscopy.Furthermore, the generation of ·OH may be mainly responsiblefor the antimalarial effect of AASMP since ·OH scavengerssuch as mannitol, as well as spin trap ${alpha}$ -phenyl-n-tertbutylnitrone,significantly protected P. falciparum from AASMP-mediated growthinhibition. Cytotoxicity testing of the active compounds showedselective activity against malaria parasite with selectivityindices greater than 100. AASMP also exhibited profound antimalarialactivity in vivo against chloroquine resistant P. yoelii. Thus,AASMP represents a novel class of antimalarial.

* Corresponding authors. Mailing address for U. Bandyopadhyay: Division of Infectious Diseases and Immunology, Indian Institute of Chemical Biology, 4, Raja S. C. Mullick Road, Jadavpur, Kolkata 700032, West Bengal, India. Phone: 91-33-247330491. Fax: 91-33-24735197. E-mail: ubandyo_1964{at}yahoo.com. Mailing address for G. Panda: Medicinal and Process Chemistry Division, Central Drug Research Institute, Lucknow-226001, UP, India. Fax: 91-522-2612411. Phone: 91-522-2623405. E-mail: gautam.panda{at}gmail.com

Published ahead of print on 19 November 2007.

Supplemental material for this article may be found at http://aac.asm.org/.

Central Drug Research Institute communication 7191.

Antimicrobial Agents and Chemotherapy, February 2008, p. 705-715, Vol. 52, No. 2
0066-4804/08/$08.00+0 doi:10.1128/AAC.00898-07
Copyright © 2008, American Society for Microbiology. All Rights Reserved.

Antiplasmodial Activity of [(Aryl)arylsulfanylmethyl]Pyridine ,,

Antiplasmodial Activity of [(Aryl)arylsulfanylmethyl]Pyridine ^,^,