An atlas of spider development at single-cell resolution provides new insights into arthropod embryogenesis.

IF 4.1 2区生物学 Q1 DEVELOPMENTAL BIOLOGY

Evodevo Pub Date : 2024-05-10 DOI:10.1186/s13227-024-00224-4

Daniel J Leite, Anna Schönauer, Grace Blakeley, Amber Harper, Helena Garcia-Castro, Luis Baudouin-Gonzalez, Ruixun Wang, Naïra Sarkis, Alexander Günther Nikola, Venkata Sai Poojitha Koka, Nathan J Kenny, Natascha Turetzek, Matthias Pechmann, Jordi Solana, Alistair P McGregor

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引用次数: 0

Abstract

Spiders are a diverse order of chelicerates that diverged from other arthropods over 500 million years ago. Research on spider embryogenesis, particularly studies using the common house spider Parasteatoda tepidariorum, has made important contributions to understanding the evolution of animal development, including axis formation, segmentation, and patterning. However, we lack knowledge about the cells that build spider embryos, their gene expression profiles and fate. Single-cell transcriptomic analyses have been revolutionary in describing these complex landscapes of cellular genetics in a range of animals. Therefore, we carried out single-cell RNA sequencing of P. tepidariorum embryos at stages 7, 8 and 9, which encompass the establishment and patterning of the body plan, and initial differentiation of many tissues and organs. We identified 20 cell clusters, from 18.5 k cells, which were marked by many developmental toolkit genes, as well as a plethora of genes not previously investigated. We found differences in the cell cycle transcriptional signatures, suggestive of different proliferation dynamics, which related to distinctions between endodermal and some mesodermal clusters, compared with ectodermal clusters. We identified many Hox genes as markers of cell clusters, and Hox gene ohnologs were often present in different clusters. This provided additional evidence of sub- and/or neo-functionalisation of these important developmental genes after the whole genome duplication in an arachnopulmonate ancestor (spiders, scorpions, and related orders). We also examined the spatial expression of marker genes for each cluster to generate a comprehensive cell atlas of these embryonic stages. This revealed new insights into the cellular basis and genetic regulation of head patterning, hematopoiesis, limb development, gut development, and posterior segmentation. This atlas will serve as a platform for future analysis of spider cell specification and fate, and studying the evolution of these processes among animals at cellular resolution.

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单细胞分辨率的蜘蛛发育图谱为节肢动物胚胎发育提供了新的视角。

蜘蛛是一种多样化的螯足纲动物，5 亿多年前从其他节肢动物中分化出来。对蜘蛛胚胎发生的研究，特别是利用普通家蛛 Parasteatoda tepidariorum 进行的研究，为了解动物发育的进化做出了重要贡献，包括轴的形成、分节和模式化。然而，我们对构建蜘蛛胚胎的细胞、它们的基因表达谱和命运还缺乏了解。单细胞转录组分析在描述一系列动物复杂的细胞遗传学景观方面具有革命性意义。因此，我们对P. tepidariorum胚胎的第7、8和9阶段进行了单细胞RNA测序，这些阶段包括体表结构的建立和模式化，以及许多组织和器官的初步分化。我们从 18.5 千个细胞中发现了 20 个细胞群，这些细胞群中有许多发育工具基因，以及大量以前未研究过的基因。我们发现细胞周期转录特征存在差异，这表明增殖动态不同，与外胚层细胞集群相比，内胚层细胞集群和一些中胚层细胞集群存在差异。我们发现许多 Hox 基因是细胞集群的标记，而 Hox 基因的同源物往往存在于不同的集群中。这为这些重要的发育基因在蛛形纲祖先（蜘蛛、蝎子及相关类）的全基因组复制后的次功能化和/或新功能化提供了更多证据。我们还研究了每个群的标记基因的空间表达，以生成这些胚胎阶段的综合细胞图谱。这揭示了头部模式化、造血、四肢发育、肠道发育和后节发育的细胞基础和遗传调控的新见解。该图谱将作为未来分析蜘蛛细胞规格和命运的平台，并以细胞分辨率研究这些过程在动物间的进化。

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

Evodevo EVOLUTIONARY BIOLOGY-DEVELOPMENTAL BIOLOGY

CiteScore

7.50

自引率

0.00%

发文量

审稿时长

>12 weeks

期刊介绍： EvoDevo publishes articles on a broad range of topics associated with the translation of genotype to phenotype in a phylogenetic context. Understanding the history of life, the evolution of novelty and the generation of form, whether through embryogenesis, budding, or regeneration are amongst the greatest challenges in biology. We support the understanding of these processes through the many complementary approaches that characterize the field of evo-devo. The focus of the journal is on research that promotes understanding of the pattern and process of morphological evolution. All articles that fulfill this aim will be welcome, in particular: evolution of pattern; formation comparative gene function/expression; life history evolution; homology and character evolution; comparative genomics; phylogenetics and palaeontology

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