Generation and characterization of induced pluripotent stem cells of small apes.

IF 4.6 2区生物学 Q2 CELL BIOLOGY

Frontiers in Cell and Developmental Biology Pub Date : 2025-03-19 eCollection Date: 2025-01-01 DOI:10.3389/fcell.2025.1536947

Yusuke Hamazaki, Hiroto Akuta, Hikaru Suzuki, Hideyuki Tanabe, Kenji Ichiyanagi, Takuya Imamura, Masanori Imamura

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引用次数: 0

Abstract

Small apes (family Hylobatidae), encompassing gibbons and siamangs, occupy a pivotal evolutionary position within the hominoid lineage, bridging the gap between great apes and catarrhine monkeys. Although they possess distinctive genomic and phenotypic features-such as rapid chromosomal rearrangements and adaptations for brachiation-functional genomic studies on small apes have been hindered by the limited availability of biological samples and developmental models. Here, we address this gap by successfully reprogramming primary skin fibroblasts from three small ape species: lar gibbons (Hylobates lar), Abbott's gray gibbons (Hylobates abbotti), and siamangs (Symphalangus syndactylus). Using Sendai virus-based stealth RNA vectors, we generated 31 reprogrammed cell lines, five of which were developed into transgene-free induced pluripotent stem cells. These iPSCs displayed canonical features of primed pluripotency, both morphologically and molecularly, consistent with other primate iPSCs. Directed differentiation experiments confirmed the capacity of the small ape iPSCs to generate cells representing all three germ layers. In particular, their successful differentiation into limb bud mesoderm cells underscores their utility in investigating the molecular and developmental mechanisms unique to small ape forelimb evolution. Transcriptomic profiling of small ape iPSCs revealed significant upregulation of pluripotency-associated genes, alongside elevated expression of transposable elements. Remarkably, LAVA retrotransposons-a class of elements specific to small apes-exhibited particularly high expression levels in these cells. Comparative transcriptomic analyses with iPSCs from humans, great apes, and macaques identified evolutionary trends and clade-specific gene expression signatures. These signatures highlighted processes linked to genomic stability and cell death, providing insights into small ape-specific adaptations. This study positions small ape iPSCs as a transformative tool for advancing functional genomics and evolutionary developmental biology. By facilitating detailed investigations into hominoid genome evolution and phenotypic diversification, this system bridges critical gaps in comparative research, enabling deeper exploration of the genetic and cellular underpinnings of small ape-specific traits.

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小类人猿诱导多能干细胞的生成与鉴定。

包括长臂猿和长臂猿在内的小型类人猿在类人猿谱系中占据着关键的进化地位，弥合了类人猿和卡河猴之间的差距。尽管它们具有独特的基因组和表型特征，如快速的染色体重排和对臂部的适应，但由于生物样本和发育模型的有限可用性，对小型类人猿的功能基因组研究一直受到阻碍。在这里，我们通过成功地重新编程三种小型类人猿物种的原代皮肤成纤维细胞来解决这一差距：大长臂猿（hyloates lar），雅培灰色长臂猿（hyloates abbotti）和暹罗猴（Symphalangus syndactylus）。利用基于仙台病毒的隐形RNA载体，我们获得了31个重编程细胞系，其中5个培养成无转基因诱导多能干细胞。这些iPSCs在形态和分子上都表现出与其他灵长类iPSCs一致的引物多能性的典型特征。定向分化实验证实了小类人猿iPSCs产生代表所有三种胚层的细胞的能力。特别是，它们成功分化为肢芽中胚层细胞，强调了它们在研究小猿前肢进化的分子和发育机制方面的作用。小猿猴iPSCs的转录组学分析显示，多能性相关基因显著上调，同时转座因子表达升高。值得注意的是，LAVA反转录转座子——一类小猿特有的元件——在这些细胞中表现出特别高的表达水平。利用来自人类、类人猿和猕猴的iPSCs进行转录组学比较分析，确定了进化趋势和分支特异性基因表达特征。这些特征突出了与基因组稳定性和细胞死亡相关的过程，为小型猿类的特异性适应提供了见解。这项研究将小猿类iPSCs定位为推进功能基因组学和进化发育生物学的变革工具。通过促进对类人猿基因组进化和表型多样化的详细研究，该系统弥补了比较研究中的关键空白，使人们能够更深入地探索小型类人猿特异性性状的遗传和细胞基础。

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

Frontiers in Cell and Developmental Biology Biochemistry, Genetics and Molecular Biology-Cell Biology

CiteScore

9.70

自引率

3.60%

发文量

2531

审稿时长

12 weeks

期刊介绍： Frontiers in Cell and Developmental Biology is a broad-scope, interdisciplinary open-access journal, focusing on the fundamental processes of life, led by Prof Amanda Fisher and supported by a geographically diverse, high-quality editorial board. The journal welcomes submissions on a wide spectrum of cell and developmental biology, covering intracellular and extracellular dynamics, with sections focusing on signaling, adhesion, migration, cell death and survival and membrane trafficking. Additionally, the journal offers sections dedicated to the cutting edge of fundamental and translational research in molecular medicine and stem cell biology. With a collaborative, rigorous and transparent peer-review, the journal produces the highest scientific quality in both fundamental and applied research, and advanced article level metrics measure the real-time impact and influence of each publication.