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采用功能质谱成像技术研究小鼠乳腺肿瘤中甘氨酸摄取及其代谢转化为谷胱甘肽的过程。

Mapping glycine uptake and its metabolic conversion to glutathione in mouse mammary tumors using functional mass spectrometry imaging.

机构信息

FTMS Laboratory for Human Health Research, Department of Chemistry, NC State University, 2700 Stinson Dr., Raleigh, NC, 27607, USA.

UNC/NCSU Joint Department of Biomedical Engineering, 1840 Entrepreneur Drive, Raleigh, NC, 27695, USA.

出版信息

Free Radic Biol Med. 2022 Nov 20;193(Pt 2):677-684. doi: 10.1016/j.freeradbiomed.2022.11.010. Epub 2022 Nov 17.

Abstract

Although glutathione plays a key role in cancer cell viability and therapy response there is no clear trend in relating the level of this antioxidant to clinical stage, histological grade, or therapy response in patient tumors. The likely reason is that static levels of glutathione are not a good indicator of how a tissue deals with oxidative stress. A better indicator is the functional capacity of the tissue to maintain glutathione levels in response to this stress. However, there are few methods to assess glutathione metabolic function in tissue. We have developed a novel functional mass spectrometry imaging (fMSI) method that can map the variations in the conversion of glycine to glutathione metabolic activity across tumor tissue sections by tracking the fate of three glycine isotopologues administered in a timed sequence to tumor-bearing anesthetized mice. This fMSI method generates multiple time point kinetic data for substrate uptake and glutathione production from each spatial location in the tissue. As expected, the fMSI data shows glutathione metabolic activity varies across the murine 4T1 mammary tumor. Although glutathione levels are highest at the tumor periphery there are regions of high content but low metabolic activity. The timed infusion method also detects variations in delivery of the glycine isotopologues thereby providing a measure of tissue perfusion, including evidence of intermittent perfusion, that contributes to the observed differences in metabolic activity. We believe this new approach will be an asset to linking molecular content to tissue function.

摘要

虽然谷胱甘肽在癌细胞活力和治疗反应中起着关键作用,但将这种抗氧化剂的水平与患者肿瘤的临床分期、组织学分级或治疗反应联系起来并没有明显的趋势。可能的原因是,谷胱甘肽的静态水平并不是组织如何应对氧化应激的良好指标。一个更好的指标是组织维持谷胱甘肽水平以应对这种应激的功能能力。然而,评估组织中谷胱甘肽代谢功能的方法很少。我们开发了一种新的功能质谱成像 (fMSI) 方法,该方法可以通过跟踪在定时序列中给予荷瘤麻醉小鼠的三种甘氨酸同位素类似物的命运,来绘制肿瘤组织切片中甘氨酸向谷胱甘肽代谢活性转化的变化。这种 fMSI 方法从组织中的每个空间位置生成用于底物摄取和谷胱甘肽产生的多个时间点动力学数据。正如预期的那样,fMSI 数据显示谷胱甘肽代谢活性在小鼠 4T1 乳腺肿瘤中发生变化。尽管谷胱甘肽水平在肿瘤边缘最高,但存在高含量但低代谢活性的区域。定时输注方法还检测甘氨酸同位素类似物的输送变化,从而提供组织灌注的衡量标准,包括间歇性灌注的证据,这有助于解释代谢活性的差异。我们相信这种新方法将有助于将分子含量与组织功能联系起来。

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