Heme Detoxification Protein (PfHDP) is essential for the hemoglobin uptake and metabolism in Plasmodium falciparum

IF 2.5 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY FASEB bioAdvances Pub Date : 2022-06-24 DOI:10.1096/fba.2022-00021
Priya Gupta, Rajan Pandey, Vandana Thakur, Sadaf Parveen, Inderjeet Kaur, Ashutosh Panda, Rashmita Bishi, Sonali Mehrotra, Asif Akhtar, Dinesh Gupta, Asif Mohmmed, Pawan Malhotra
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引用次数: 5

Abstract

Hemoglobin degradation is crucial for the growth and survival of Plasmodium falciparum in human erythrocytes. Although the process of Hb degradation has been studied in detail, the mechanisms of Hb uptake remain ambiguous to date. Here, we characterized Heme Detoxification Protein (PfHDP); a protein localized in the parasitophorus vacuole, parasite food vacuole, and infected erythrocyte cytosol for its role in Hb uptake. Immunoprecipitation of PfHDP-GFP fusion protein from a transgenic line using GFP trap beads showed the association of PfHDP with Hb as well as with the members of PTEX translocon complex. Association of PfHDP with Hb or Pfexp-2, a component of translocon complex was confirmed by protein–protein interaction and immunolocalization tools. Based on these associations, we studied the role of PfHDP in Hb uptake using the PfHDP-HA-GlmS transgenic parasites line. PfHDP knockdown significantly reduced the Hb uptake in these transgenic parasites in comparison to the wild-type parasites. Morphological analysis of PfHDP-HA-GlmS transgenic parasites in the presence of GlcN showed food vacuole abnormalities and parasite stress, thereby causing a growth defect in the development of these parasites. Transient knockdown of a member of translocon complex, PfHSP101 in HSP101-DDDHA parasites also showed a decreased uptake of Hb inside the parasite. Together, these results advocate an interaction between PfHDP and the translocon complex at the parasitophorus vacuole membrane and also suggest a role for PfHDP in the uptake of Hb and parasite development. The study thus reveals new insights into the function of PfHDP, making it an extremely important target for developing new antimalarials.

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血红素解毒蛋白(PfHDP)对恶性疟原虫的血红蛋白摄取和代谢至关重要
血红蛋白降解对恶性疟原虫在人红细胞中的生长和存活至关重要。虽然Hb降解的过程已被详细研究,但摄取Hb的机制至今仍不清楚。在这里,我们对血红素解毒蛋白(PfHDP)进行了表征;一种定位于寄生物液泡、寄生物食物液泡和被感染红细胞胞浆中的蛋白质,在Hb摄取中起作用。使用GFP诱捕珠免疫沉淀转基因细胞系的PfHDP-GFP融合蛋白显示PfHDP与Hb以及PTEX易位复合物成员的关联。通过蛋白-蛋白相互作用和免疫定位工具证实了PfHDP与Hb或Pfexp-2(易位复合物的一个组成部分)的关联。基于这些关联,我们利用PfHDP- ha - glms转基因寄生虫系研究了PfHDP在Hb摄取中的作用。与野生型寄生虫相比,PfHDP敲除显著降低了这些转基因寄生虫对Hb的摄取。对转基因PfHDP-HA-GlmS寄生虫在GlcN存在下的形态分析显示食物液泡异常和寄生虫应激,从而导致这些寄生虫发育出现生长缺陷。在HSP101-DDDHA寄生虫中,瞬时敲低易位复合体成员PfHSP101也显示寄生虫内Hb摄取减少。总之,这些结果表明PfHDP与寄生物液泡膜上的转位复合体之间存在相互作用,并且PfHDP在Hb的摄取和寄生虫发育中也发挥了作用。因此,该研究揭示了PfHDP功能的新见解,使其成为开发新的抗疟药物的极其重要的靶点。
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来源期刊
FASEB bioAdvances
FASEB bioAdvances Multiple-
CiteScore
5.40
自引率
3.70%
发文量
56
审稿时长
10 weeks
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