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对 幼虫和生殖细胞培养物的全基因组转录组分析揭示了参与寄生虫干细胞功能的基因。

Genome-wide transcriptome analysis of larvae and germinative cell cultures reveals genes involved in parasite stem cell function.

机构信息

Consultant Laboratory for Echinococcosis, Institute of Hygiene and Microbiology, University of Würzburg, Würzburg, Germany.

Parasite Genomics, Wellcome Sanger Institute, Cambridge, United Kingdom.

出版信息

Front Cell Infect Microbiol. 2024 Jan 25;14:1335946. doi: 10.3389/fcimb.2024.1335946. eCollection 2024.

Abstract

The lethal zoonosis alveolar echinococcosis is caused by tumour-like growth of the metacestode stage of the tapeworm within host organs. We previously demonstrated that metacestode proliferation is exclusively driven by somatic stem cells (germinative cells), which are the only mitotically active parasite cells that give rise to all differentiated cell types. The gene repertoire required for germinative cell maintenance and differentiation has not been characterised so far. We herein carried out Illumina sequencing on cDNA from metacestode vesicles, from metacestode tissue depleted of germinative cells, and from primary cell cultures. We identified a set of ~1,180 genes associated with germinative cells, which contained numerous known stem cell markers alongside genes involved in replication, cell cycle regulation, mitosis, meiosis, epigenetic modification, and nucleotide metabolism. Interestingly, we also identified 44 stem cell associated transcription factors that are likely involved in regulating germinative cell differentiation and/or pluripotency. By hybridization and pulse-chase experiments, we also found a new general stem cell marker, , and we provide evidence implying the presence of a slow cycling stem cell sub-population expressing the extracellular matrix factor . RNA-Seq analyses on primary cell cultures revealed that metacestode-derived stem cells display an expanded differentiation capability and do not only form differentiated cell types of the metacestode, but also cells expressing genes specific for protoscoleces, adult worms, and oncospheres, including an ortholog of the schistosome praziquantel target, EmTRPM. Finally, we show that primary cell cultures contain a cell population expressing an ortholog of the tumour necrosis factor α receptor family and that mammalian TNFα accelerates the development of metacestode vesicles from germinative cells. Taken together, our analyses provide a robust and comprehensive characterization of the germinative cell transcriptome, demonstrate expanded differentiation capability of metacestode derived stem cells, and underscore the potential of primary germinative cell cultures to investigate developmental processes of the parasite. These data are relevant for studies into the role of stem cells in parasite development and will facilitate the design of anti-parasitic drugs that specifically act on the parasite germinative cell compartment.

摘要

致死性人畜共患泡球蚴病是由绦虫的中绦期幼虫在宿主器官内呈肿瘤样生长引起的。我们之前的研究表明,中绦期幼虫的增殖完全由体干细胞(生殖细胞)驱动,生殖细胞是唯一具有有丝分裂活性的寄生虫细胞,可产生所有分化细胞类型。迄今为止,尚未对维持和分化生殖细胞所需的基因库进行描述。在此,我们对来自中绦期囊泡、去除生殖细胞的中绦期组织和原代细胞培养物的 cDNA 进行了 Illumina 测序。我们鉴定了一组与生殖细胞相关的约 1180 个基因,其中包含许多已知的干细胞标记物以及参与复制、细胞周期调控、有丝分裂、减数分裂、表观遗传修饰和核苷酸代谢的基因。有趣的是,我们还鉴定了 44 个可能参与调节生殖细胞分化和/或多能性的与干细胞相关的转录因子。通过杂交和脉冲追踪实验,我们还发现了一个新的通用的 干细胞标记物 ,并提供了证据表明存在表达细胞外基质因子 的缓慢循环干细胞亚群。对原代细胞培养物的 RNA-Seq 分析表明,中绦期衍生的 干细胞具有扩展的分化能力,不仅形成中绦期的分化细胞类型,还形成表达原头节、成虫和六钩蚴特异性基因的细胞,包括血吸虫吡喹酮靶标 EmTRPM 的同源物。最后,我们表明原代细胞培养物中存在表达肿瘤坏死因子 α 受体家族同源物的细胞群,哺乳动物 TNFα 可加速生殖细胞向中绦期囊泡的发育。总之,我们的分析为 生殖细胞转录组提供了一个强大而全面的描述,证明了中绦期衍生干细胞的扩展分化能力,并强调了原代生殖细胞培养物在研究寄生虫发育过程中的潜力。这些数据与研究寄生虫发育过程中 干细胞的作用有关,并将有助于设计专门针对寄生虫生殖细胞区室的抗寄生虫药物。

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