组蛋白甲基转移酶 DOT1B 对于墨西哥利什曼原虫的阶段分化和巨噬细胞感染是不可或缺的

Nicole Eisenhuth, Elisa Theres Rauh, Melina Mitnacht, Andrea Debus, Falk Butter, Ulrike Schleicher, Katerina Pruzinova, Petr Volf, Christian J Janzen
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摘要

保守的 DOT1 家族组蛋白甲基转移酶参与了锥虫的复制调控、细胞周期进展、阶段分化和基因调控。然而,这些酶的具体功能取决于寄生虫的宿主逃避策略。在这项研究中,我们研究了 DOT1B 在墨西哥利什曼原虫中的作用,重点是生命周期的进展和传染性。在布氏锥虫中,DOT1B 是哺乳动物感染性血流型向昆虫原环型分化的关键,与此不同的是,墨西哥利什曼原虫 DOT1B(LmxDOT1B)在体外并不是原核向母核分化的关键。此外,缺失 LmxDOT1B 的菌株与对照菌株在巨噬细胞或沙蝇载体中的感染或分化能力也没有明显差异。这些发现凸显了 DOT1B 在这些相关寄生虫中的功能差异,表明组蛋白修饰在生命周期进展和宿主适应过程中的使用具有种属特异性。
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The histone methyltransferase DOT1B is dispensable for stage differentiation and macrophage infection in Leishmania mexicana
Conserved histone methyltransferases of the DOT1 family are involved in replication regulation, cell cycle progression, stage differentiation and gene regulation in trypanosomatids. However, the specific functions of these enzymes depend on the host evasion strategies of the parasites. In his study, we investigated the role of DOT1B in Leishmania mexicana, focusing on life cycle progression and infectivity. In contrast to Trypanosoma brucei, in which DOT1B is essential for the differentiation of mammal-infective bloodstream forms to insect procyclic forms, L. mexicana DOT1B (LmxDOT1B) is not critical for the differentiation of promastigotes to amastigotes in vitro. Additionally, there are no significant differences in the ability to infect or differentiate in macrophages or sand fly vectors between the LmxDOT1B-depleted and control strains. These findings highlight the divergency of the function of DOT1B in these related parasites, suggesting genus-specific adaptations in the use of histone modifications for life cycle progression and host adaptation processes.
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