Neutralization of Toxic Heme by Plasmodium Falciparum Histidine-Rich Protein 2

doi:10.1093/jb/mvg089

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J. Biochem, 2003, Vol. 133, No. 5 693-698
© 2003 Japanese Biochemical Society

BIOCHEMISTRY

Neutralization of Toxic Heme by Plasmodium Falciparum Histidine-Rich Protein 2

Nguyen Tien Huy, Satoshi Serada, Dai Thi Xuan Trang, Ryo Takano, Yoshiro Kondo, Kenji Kanaori, Kunihiko Tajima, Saburo Hara and Kaeko Kamei⁺

Department of Applied Biology, Kyoto Institute of Technology, Matsugasaki, Sakyo-ku, Kyoto 606-8585

Plasmodium falciparum histidine-rich protein 2 (PfHRP2) hasbeen suggested to be an initiator of the polymerization of heme,which is produced as by-product on the digestion of hemoglobin,and a promoter of the H₂O₂-induced degradation of heme in foodvacuoles of the malarial parasite. In this work, we have designedPfHRP2 model peptides, R18 and R27 (18 and 27 residues, respectively),and used them for optical and electron spin resonance spectroscopicmeasurements to confirm that the axial ligands of the heme-PfHRP2complex are the nitrogenous donors derived from the imidazolemoieties of histidine residues of PfHRP2. In addition, we revealedthat the affinities of R18 and R27 for heme (K_d = 2.21 x 10^–6M and 0.71 x 10^–6 M, respectively) might be as high asthat of PfHRP2 (K_d = 0.94 x 10^–6 M). The R27 peptide canremove heme from membrane-intercalated heme and inhibit heme-inducedhemolysis. Therefore, we suggest another function of PfHRP2:it may play an important role in the neutralization of toxicheme in the parasite cytoplasm and infected erythrocytes byremoving heme from heme-bound membranes or reducing heme-inducedhemolysis.

⁺ To whom correspondence should be addressed. Tel: +81-75-724-7553,Fax: +81-75-724-7532, E-mail: kame{at}ipc.kit.ac.jp

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Journal of Biochemistry

BIOCHEMISTRY

Neutralization of Toxic Heme by Plasmodium Falciparum Histidine-Rich Protein 2