SUN-domain proteins of the malaria parasite Plasmodium falciparum are essential for proper nuclear division and DNA repair.

IF 5.1 1区生物学 Q1 MICROBIOLOGY

mBio Pub Date : 2025-04-09 Epub Date: 2025-03-05 DOI:10.1128/mbio.00216-25

Sofiya Kandelis-Shalev, Manish Goyal, Tal Elam, Shany Assaraf, Noa Dahan, Omer Farchi, Eduard Berenshtein, Ron Dzikowski

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引用次数: 0

Abstract

The protozoan parasite Plasmodium falciparum, which is responsible for the deadliest form of human malaria, accounts for over half a million deaths a year. These parasites proliferate in human red blood cells by consecutive rounds of closed mitoses called schizogony. Their virulence is attributed to their ability to modify the infected red cells to adhere to the vascular endothelium and to evade immunity through antigenic switches. Spatial dynamics at the nuclear periphery were associated with the regulation of processes that enable the parasites to establish long-term infection. However, our knowledge of components of the nuclear envelope (NE) in Plasmodium remains limited. One of the major protein complexes at the NE is the linker of nucleoskeleton and cytoskeleton (LINC) complex that forms a connecting bridge between the cytoplasm and the nucleus through the interaction of SUN and KASH domain proteins. Here, we have identified two SUN-domain proteins as possible components of the LINC complex of P. falciparum and show that their proper expression is essential for the parasite's proliferation in human red blood cells, and their depletion leads to the formation of membranous whorls and morphological changes of the NE. In addition, their differential expression highlights different functions at the nuclear periphery as PfSUN2 is specifically associated with heterochromatin, while PfSUN1 expression is essential for activation of the DNA damage response. Our data provide indications for the involvement of the LINC complex in crucial biological processes in the intraerythrocytic development cycle of malaria parasites.

Importance: Plasmodium falciparum, the parasite causing the deadliest form of malaria, is able to thrive in its human host by tight regulation of cellular processes, orchestrating nuclear dynamics with cytoplasmic machineries that are separated by the nuclear envelope. One of the major protein complexes that connect nuclear and cytoplasmic processes in eukaryotes is the linker of nucleoskeleton and cytoskeleton (LINC) complex. However, while the nuclear periphery of P. falciparum was implicated in several important functions, the role of the LINC complex in Plasmodium biology is unknown. Here, we identify two components of P. falciparum LINC complex and demonstrate that they are essential for the parasites' proliferation in human blood, and their depletion leads to the formation of morphological changes in the cell. In addition, the two components have different functions in activating the DNA damage response and in their association with heterochromatin. Our data provide evidence for their essential roles in the parasites' cell cycle.

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恶性疟原虫的太阳结构域蛋白对正常的核分裂和DNA修复至关重要。

原生动物寄生虫恶性疟原虫（Plasmodium falciparum）是最致命的人类疟疾，每年造成50多万人死亡。这些寄生虫通过被称为分裂体的连续几轮闭合的有丝分裂在人类红细胞中增殖。它们的毒性是由于它们能够修饰被感染的红细胞，使其粘附在血管内皮上，并通过抗原开关逃避免疫。核外围的空间动力学与使寄生虫建立长期感染的过程的调节有关。然而，我们对疟原虫核膜（NE）成分的了解仍然有限。NE上的主要蛋白复合物之一是核骨架和细胞骨架（LINC）复合物，它通过SUN和KASH结构域蛋白的相互作用形成细胞质和细胞核之间的连接桥梁。在这里，我们已经确定了两个太阳结构域蛋白作为恶性疟原虫LINC复合体的可能组成部分，并表明它们的适当表达对于疟原虫在人红细胞中的增殖至关重要，它们的消耗导致膜状螺旋的形成和NE的形态变化。此外，它们的差异表达突出了在核外周的不同功能，因为PfSUN2特异性地与异染色质相关，而PfSUN1的表达对于DNA损伤反应的激活至关重要。我们的数据为LINC复合物参与疟疾寄生虫红细胞内发育周期的关键生物学过程提供了指示。重要性：恶性疟原虫是导致最致命形式疟疾的寄生虫，它能够在人类宿主体内茁壮成长，是通过对细胞过程的严格调控，与被核膜隔开的细胞质机制协调核动力学。核骨架和细胞骨架（LINC）复合物是真核生物中连接细胞核和细胞质过程的主要蛋白质复合物之一。然而，尽管恶性疟原虫的核外周与几种重要功能有关，但LINC复合物在疟原虫生物学中的作用尚不清楚。在这里，我们鉴定了恶性疟原虫LINC复合物的两个组成部分，并证明它们是寄生虫在人血液中增殖所必需的，它们的消耗导致细胞形态变化的形成。此外，这两种成分在激活DNA损伤反应和与异染色质的关联方面具有不同的功能。我们的数据为它们在寄生虫细胞周期中的重要作用提供了证据。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

mBio MICROBIOLOGY-

CiteScore

10.50

自引率

3.10%

发文量

762

审稿时长

1 months

期刊介绍： mBio® is ASM''s first broad-scope, online-only, open access journal. mBio offers streamlined review and publication of the best research in microbiology and allied fields.