Bovine lactoferrin inhibits Plasmodium berghei growth by binding to heme

Author:

Obayashi Momoka1,Kimura Momoko1,Haraguchi Asako2,Gotanda Mari1,Kitagawa Taiki1,Matsuno Misato1,Sakao Kozue1,Hamanaka Daisuke1,Kusakisako Kodai2,Ibrahim Hisham1,Miyata Takeshi1,Ikadai Hiromi2

Affiliation:

1. Kagoshima University

2. Kitasato University

Abstract

Abstract

Bovine lactoferrin (bLF) is a 77 kDa glycoprotein that is abundant in bovine breast milk and exerts various bioactive functions, including antibacterial and antiviral functions. Few studies have explored bLF activity against parasites. We found that bLF affects hemozoin synthesis by binding to heme, inhibiting heme iron polymerization necessary for Plasmodium berghei ANKA survival in infected erythrocytes, and also binds to hemozoin, causing it to disassemble. In a challenge test, bLF administration inhibited the growth of murine malaria parasites compared to untreated group growth. To determine whether the iron content of bLF affects the inhibition of malaria growth, we tested bLFs containing different amounts of iron (apo-bLF, native-bLF, and holo-bLF), but found no significant difference in their effects. This indicated that the active sites were located within the bLFs themselves. Further studies showed that the C-lobe domain of bLF can inhibit hemozoin formation and the growth of P. berghei ANKA. Evaluation of pepsin degradation products of the C-lobe identified a 47-amino-acid section, C-1, as the smallest effective region that could inhibit hemozoin formation. This study highlights bLF’s potential as a novel therapeutic agent against malaria, underscoring the importance of its non-iron-dependent bioactive sites in combating parasite growth.

Publisher

Springer Science and Business Media LLC

Reference47 articles.

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