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Imaging mass spectrometry demonstrates age-related decline in human adipose plasticity

机译:成像质谱表明与年龄有关的人类脂肪可塑性下降

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摘要

Quantification of stable isotope tracers has revealed the dynamic state of living tissues. A new form of imaging mass spectrometry quantifies isotope ratios in domains much smaller than a cubic micron, enabling measurement of cell turnover and metabolism with stable isotope tracers at the single-cell level with a methodology we refer to as multi-isotope imaging mass spectrometry. In a first-in-human study, we utilize stable isotope tracers of DNA synthesis and de novo lipogenesis to prospectively measure cell birth and adipocyte lipid turnover. In a study of healthy adults, we elucidate an age-dependent decline in new adipocyte generation and adipocyte lipid turnover. A linear regression model suggests that the aging effect could be mediated by a decline in insulin-like growth factor-1 (IGF-1). This study therefore establishes a method for measurement of cell turnover and metabolism in humans with subcellular resolution while implicating the growth hormone/IGF-1 axis in adipose tissue aging.
机译:稳定同位素示踪剂的定量显示了活组织的动态状态。一种新型的质谱成像方法可以量化远小于立方微米的区域中的同位素比率,从而可以使用我们称为多同位素成像质谱法的方法在单细胞水平上用稳定的同位素示踪剂测量细胞更新和代谢。在一项首次人类研究中,我们利用DNA合成的稳定同位素示踪剂和从头开始的脂肪生成来前瞻性地测量细胞的出生和脂肪细胞脂质的更新。在对健康成年人的研究中,我们阐明了新的脂肪细胞生成和脂肪细胞脂质更新的年龄依赖性下降。线性回归模型表明,衰老作用可能由胰岛素样生长因子-1(IGF-1)的下降介导。因此,这项研究建立了一种以亚细胞分辨率测量人体细胞更新和代谢的方法,同时将生长激素/ IGF-1轴牵连到脂肪组织的衰老中。

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