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牛乳铁蛋白通过与血红素结合来抑制疟原虫生长。

Bovine lactoferrin inhibits Plasmodium berghei growth by binding to heme.

机构信息

Division of Molecular Functions of Food, Department of Biochemistry and Biotechnology, Kagoshima University, 1-21-24 Korimoto, Kagoshima, 890-0065, Japan.

Laboratory of Veterinary Parasitology, School of Veterinary Medicine, Kitasato University, 23-35-1 Higashi, Towada, Aomori, 034-8628, Japan.

出版信息

Sci Rep. 2024 Sep 2;14(1):20344. doi: 10.1038/s41598-024-70840-6.

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.

摘要

牛乳铁蛋白(bLF)是一种 77 kDa 的糖蛋白,在牛乳中含量丰富,具有多种生物活性功能,包括抗菌和抗病毒功能。很少有研究探讨 bLF 对寄生虫的活性。我们发现 bLF 通过与血红素结合来影响疟原虫血红素的合成,抑制疟原虫血红素铁聚合,从而抑制疟原虫在感染的红细胞中的生存,同时 bLF 也与疟原虫血红素结合,导致其解聚。在一项挑战试验中,与未处理组相比,bLF 给药抑制了鼠疟原虫的生长。为了确定 bLF 中的铁含量是否影响疟原虫生长的抑制,我们测试了含有不同铁含量的 bLF(apo-bLF、native-bLF 和 holo-bLF),但发现它们的作用没有显著差异。这表明活性位点位于 bLF 本身内部。进一步的研究表明,bLF 的 C 结构域可以抑制疟原虫血红素的形成和生长。对 C 结构域胃蛋白酶降解产物的评估确定了一个 47 个氨基酸的 C-1 片段,作为可以抑制疟原虫血红素形成的最小有效区域。本研究强调了 bLF 作为一种新型抗疟疾治疗药物的潜力,突出了其非铁依赖性生物活性位点在抑制寄生虫生长方面的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f5d/11369202/5c08cf5b46ff/41598_2024_70840_Fig1_HTML.jpg

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