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犬胚胎衍生干细胞向幼稚样多能性转变过程中的代谢可塑性。

Metabolic plasticity during transition to naïve-like pluripotency in canine embryo-derived stem cells.

作者信息

Tobias I C, Isaac R R, Dierolf J G, Khazaee R, Cumming R C, Betts D H

机构信息

Department of Physiology and Pharmacology, Schulich School of Medicine & Dentistry, Western University, London, Ontario, Canada.

Department of Biology, Faculty of Science, Western University, London, Ontario, Canada.

出版信息

Stem Cell Res. 2018 Jul;30:22-33. doi: 10.1016/j.scr.2018.05.005. Epub 2018 May 17.

Abstract

Pluripotent stem cells (PSCs) have been described in naïve or primed pluripotent states. Domestic dogs are useful translational models in regenerative medicine, but their embryonic stem cells (cESCs) remain narrowly investigated. Primed-like cESCs expanded in the presence of leukemia inhibitory factor and fibroblast growth factor 2 (LIF-FGF2) acquire features of naïve pluripotency when exposed to chemical inhibitors and LIF (2iL). However, proliferation of cESCs is influenced by the pluripotent state and is comparatively slower than human or mouse PSCs. We propose that different metabolic pathway activities support ATP generation and biomass accumulation necessary for LIF-FGF2 and 2iL cESC proliferation. We found that 2iL cESCs have greater respiratory capacity, altered mitochondrial chain complex stoichiometry and elevated mitochondrial polarization state. Yet, 2iL-enriched cESCs exhibited immature ultrastructure, including previously unrecognized changes to cristae organization. Enhanced ATP level in 2iL cESCs is associated with altered retrograde signalling, whereas LIF-FGF2 cESCs exhibit a lipogenic phenotype. Inhibition of oxidative phosphorylation impaired proliferation and ATP production in 2iL cESCs but not LIF-FGF2 cESCs, which remained sensitive to glycolysis inhibition. Our study reveals distinct bioenergetic mechanisms contributing to steady-state expansion of distinct canine pluripotent states that can be exploited to improve derivation and culture of canine PSCs.

摘要

多能干细胞(PSC)已被描述为处于原始或预处理多能状态。家犬是再生医学中有用的转化模型,但其胚胎干细胞(cESC)仍未得到充分研究。在白血病抑制因子和成纤维细胞生长因子2(LIF-FGF2)存在下扩增的类预处理cESC,在暴露于化学抑制剂和LIF(2iL)时会获得原始多能性特征。然而,cESC的增殖受多能状态影响,且比人类或小鼠PSC相对较慢。我们提出,不同的代谢途径活动支持LIF-FGF2和2iL cESC增殖所需的ATP生成和生物量积累。我们发现,2iL cESC具有更强的呼吸能力、改变的线粒体链复合物化学计量和升高的线粒体极化状态。然而,富含2iL的cESC表现出不成熟的超微结构,包括以前未识别的嵴组织变化。2iL cESC中ATP水平的升高与逆行信号的改变有关,而LIF-FGF2 cESC表现出脂肪生成表型。抑制氧化磷酸化会损害2iL cESC的增殖和ATP产生,但不会损害LIF-FGF2 cESC,后者对糖酵解抑制仍敏感。我们的研究揭示了不同的生物能量机制,这些机制有助于不同犬多能状态的稳态扩增,可用于改善犬PSC的衍生和培养。

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