An inner membrane complex protein IMC1g in Plasmodium berghei is involved in asexual stage schizogony and parasite transmission.

IF 5.1 1区 生物学 Q1 MICROBIOLOGY
mBio Pub Date : 2024-11-22 DOI:10.1128/mbio.02652-24
Yinjie Liu, Shitong Cheng, Gang He, Dawei He, Duo Wang, Sicong Wang, Lumeng Chen, Liying Zhu, Yonghui Feng, Liwang Cui, Yaming Cao, Xiaotong Zhu
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Abstract

The inner membrane complex (IMC), a double-membrane organelle underneath the plasma membrane in apicomplexan parasites, plays a significant role in motility and invasion and confers shape to the cell. We characterized the function of PbIMC1g, a component of the IMC1 family member in Plasmodium berghei. PbIMC1g is recruited to the IMC in late schizonts, activated gametocytes, and ookinetes. Pairwise yeast two-hybrid assays demonstrate that PbIMC1g interacts with IMC1c, a component of the PHIL1 complex, and the core sub-repeat motif "EKI(V)V(I)EVP" in PbIMC1g is essential for this interaction. Localization of PbIMC1g to the IMC was dependent on its IMCp domain, while its C-terminus and palmitoylation sites were required for the full efficiency of proper IMC targeting. PbIMC1g is required for asexual stage development, and its conditional knockdown resulted in a defect in schizogony. Additionally, PbIMC1g was also important for male gametogenesis and ookinete development. As an IMC component that assists in anchoring the glideosome to the subpellicular network, PbIMC1g was also involved in ookinete motility and mosquito midgut invasion. IMC1g from the human parasite Plasmodium vivax could functionally replace PbIMC1g in P. berghei, confirming the evolutionary conservation of IMC1g proteins in Plasmodium spp. Together, this work reveals an essential role of IMC1g in the parasite life cycle and suggests that IMC1 family members likely contribute to parasite gliding and invasion.

Importance: The malaria parasite's inner membrane complex is critical to maintain its structural integrity and motility. Here, we identified the function of the IMC1g protein, a member of the IMC1 family, in invasive and proliferative stages of P. berghei. We found that the IMCp domain of PbIMC1g is critical for proper IMC targeting, and PbIMC1g interacts with PbIMC1c. Conditional knockdown of PbIMC1g expression affects schizogony, gametogenesis, and ookinete conversion. PbIMC1g interacts with IMC1c to firmly anchor the glideosome to the subpellicular network. Additionally, we confirmed that IMC1g is functionally conserved in Plasmodium spp. These data reveal the function of IMC1g protein in anchoring the glideosome, providing further insight into the mechanism of the glideosome function.

疟原虫内膜复合蛋白 IMC1g 参与了无性阶段的分裂和寄生虫传播。
内膜复合体(IMC)是一种位于类鼻疽寄生虫质膜下的双膜细胞器,在运动和侵袭中发挥着重要作用,并赋予细胞形状。我们研究了疟原虫中 IMC1 家族成员 PbIMC1g 的功能。PbIMC1g 在晚期裂殖体、活化配子细胞和卵细胞中被招募到 IMC 中。配对酵母双杂交试验证明,PbIMC1g 与 PHIL1 复合物的一个成分 IMC1c 相互作用,PbIMC1g 中的核心亚重复基序 "EKI(V)V(I)EVP "对这种相互作用至关重要。PbIMC1g 在 IMC 上的定位依赖于其 IMCp 结构域,而其 C 端和棕榈酰化位点则是适当 IMC 定位充分有效的必要条件。无性阶段的发育需要 PbIMC1g,条件性敲除 PbIMC1g 会导致裂殖缺陷。此外,PbIMC1g 对雄性配子发生和卵子发育也很重要。PbIMC1g 作为 IMC 的一个组成部分,协助将视频体固定在小球下网络上,它还参与了卵子的运动和蚊子中肠的入侵。这项工作揭示了 IMC1g 在寄生虫生命周期中的重要作用,并表明 IMC1 家族成员可能有助于寄生虫的滑行和入侵:疟原虫的内膜复合体对维持其结构完整性和运动性至关重要。在这里,我们确定了 IMC1 家族成员 IMC1g 蛋白在伯格氏疟原虫入侵和增殖阶段的功能。我们发现 PbIMC1g 的 IMCp 结构域对于 IMC 的正确定位至关重要,而且 PbIMC1g 与 PbIMC1c 相互作用。条件性敲除 PbIMC1g 的表达会影响分裂、配子发生和卵子转化。PbIMC1g与IMC1c相互作用,将视频体牢固地固定在小球下网络上。这些数据揭示了 IMC1g 蛋白在锚定视频体方面的功能,为我们进一步了解视频体的功能机制提供了依据。
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
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.
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