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[6,6'-H]果糖作为肝癌的氘代谢成像探针。

[6,6'- H ] fructose as a deuterium metabolic imaging probe in liver cancer.

机构信息

Department of Radiology, Memorial Sloan Kettering Cancer Center, New York, New York, USA.

Molecular Pharmacology Program, Memorial Sloan Kettering Cancer Center, New York, New York, USA.

出版信息

NMR Biomed. 2023 Oct;36(10):e4989. doi: 10.1002/nbm.4989. Epub 2023 Jun 19.

Abstract

Hepatocellular carcinoma (HCC) is one of the leading causes of cancer-related deaths. Imaging plays a crucial role in the early detection of HCC, although current methods are limited in their ability to characterize liver lesions. Most recently, deuterium metabolic imaging (DMI) has been demonstrated as a powerful technique for the imaging of metabolism in vivo. Here, we assess the metabolic flux of [6,6'- H ] fructose in cell cultures and in subcutaneous mouse models at 9.4 T. We compare these rates with the most widely used DMI probe, [6,6'- H ] glucose, exploring the possibility of developing H fructose to overcome the limitations of glucose as a novel DMI probe for detecting liver tumors. Comparison of the in vitro metabolic rates implies their similar glycolytic metabolism in the TCA cycle due to comparable production rates of H glutamate/glutamine (glx) for the two precursors, but overall higher glycolytic metabolism from H glucose because of a higher production rate of H lactate. In vivo kinetic studies suggest that HDO can serve as a robust reporter for the consumption of the precursors in liver tumors. As fructose is predominantly metabolized in the liver, deuterated water (HDO) produced from H fructose is probably less contaminated from whole-body metabolism in comparison with glucose. Moreover, in studies of the normal liver, H fructose is readily converted to H glx, enabling the characterization of H fructose kinetics. This overcomes a major limitation of previous H glucose studies in the liver, which were unable to confidently discern metabolic flux due to overlapped signals of H glucose and its metabolic product, H glycogen. This suggests a unique role for H fructose metabolism in HCC and the normal liver, making it a useful approach for assessing liver-related diseases and the progression to oncogenesis.

摘要

肝细胞癌 (HCC) 是癌症相关死亡的主要原因之一。影像学在 HCC 的早期检测中起着至关重要的作用,尽管目前的方法在描述肝脏病变方面能力有限。最近,氘代谢成像 (DMI) 已被证明是一种强大的活体代谢成像技术。在这里,我们在 9.4T 下评估 [6,6'- H] 果糖在细胞培养物和皮下小鼠模型中的代谢通量。我们将这些速率与最广泛使用的 DMI 探针 [6,6'- H] 葡萄糖进行比较,探索开发 H 果糖以克服葡萄糖作为检测肝癌新型 DMI 探针的局限性的可能性。体外代谢率的比较表明,由于两种前体产生的 H 谷氨酸/谷氨酰胺 (glx) 速率相当,它们在 TCA 循环中的糖酵解代谢相似,但由于 H 乳酸的产生速率较高,整体糖酵解代谢更高。体内动力学研究表明 HDO 可以作为肝肿瘤中前体消耗的有力示踪剂。由于果糖主要在肝脏中代谢,与葡萄糖相比,来自 H 果糖的氘化水 (HDO) 可能较少受到全身代谢的污染。此外,在正常肝脏的研究中,H 果糖很容易转化为 H glx,从而能够对 H 果糖动力学进行特征描述。这克服了以前在肝脏中进行的 H 葡萄糖研究的一个主要限制,由于 H 葡萄糖及其代谢产物 H 糖原的信号重叠,这些研究无法自信地辨别代谢通量。这表明 H 果糖代谢在 HCC 和正常肝脏中具有独特的作用,使其成为评估肝脏相关疾病和向癌变进展的有用方法。

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