同位素示踪揭示了多种组织学儿童肿瘤的糖酵解和氧化代谢。

Med (New York, N.y.) Pub Date : 2021-04-09 Epub Date: 2021-02-23 DOI:10.1016/j.medj.2021.01.002
Kendra Johnston, Panayotis Pachnis, Alpaslan Tasdogan, Brandon Faubert, Lauren G Zacharias, Hieu Sy Vu, Laurie Rodgers-Augustyniak, Allison Johnson, Fang Huang, Sean Ricciardo, Zhiyu Zhao, Thomas P Mathews, Tanya Watt, Patrick Leavey, Ralph J DeBerardinis
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引用次数: 22

摘要

背景:儿童高危实体瘤患者的生存率仍然很低。重编程代谢促进肿瘤生长,并可能包含治疗缺陷。使用术中13c -葡萄糖输注评估成人肿瘤代谢。儿童肿瘤与成人癌症的不同之处在于其低突变负担和来自胚胎组织。在这里,我们使用13C输注来检测儿童的肿瘤代谢,比较肿瘤类型之间以及儿童和成人癌症之间的表型。方法:纳入研究NCT03686566的患者在肿瘤切除术期间接受术中输注[U-13C]葡萄糖,以评估肿瘤中的中心碳途径,同时使用代谢组学提供代谢的广泛概述。采用多重比较试验和混合效应分析确定差异特征。结果:我们研究了22例患者的23个肿瘤。用[U-13C]葡萄糖分析的所有肿瘤都含有糖酵解和三羧酸(TCA)循环中间体的标记。在TCA循环中标记丙酮酸脱氢酶(PDH)和丙酮酸羧化酶(PC)的活性,以PDH为主。与其他儿童癌症和肺癌相比,神经母细胞瘤具有较高的乳酸标记,并以与儿茶酚胺合成一致的丰富酪氨酸分解代谢物来区分。结论:术中[U13C]葡萄糖输注治疗小儿肿瘤是安全且有益的。不同组织学的肿瘤使用糖酵解和氧化代谢,在这个小队列中有明显的亚型选择差异。扩大这一队列可能会发现肿瘤代谢的预测性生物标志物和治疗靶点。资助:国家科学基金资助P.L. (R21CA220090-01A1)和R.J.D. (R35CA22044901);H.H.M.I.资助R.J.D.;儿童临床研究咨询委员会资助K.J.
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Isotope tracing reveals glycolysis and oxidative metabolism in childhood tumors of multiple histologies.

Background: Survival among children with high-risk solid tumors remains poor. Reprogrammed metabolism promotes tumor growth and may contain therapeutic liabilities. Tumor metabolism has been assessed in adults using intra-operative 13C-glucose infusions. Pediatric tumors differ from adult cancers in their low mutational burden and derivation from embryonic tissues. Here we used 13C infusions to examine tumor metabolism in children, comparing phenotypes among tumor types and between childhood and adult cancers.

Methods: Patients recruited to study NCT03686566 received an intra-operative infusion of [U-13C]glucose during tumor resection to evaluate central carbon pathways in the tumor, with concurrent metabolomics to provide a broad overview of metabolism. Differential characteristics were determined using multiple comparison tests and mixed effect analyses.

Findings: We studied 23 tumors from 22 patients. All tumors analyzed by [U-13C]glucose contained labeling in glycolytic and tricarboxylic acid (TCA) cycle intermediates. Labeling in the TCA cycle indicated activity of pyruvate dehydrogenase (PDH) and pyruvate carboxylase (PC), with PDH predominating. Neuroblastomas had high lactate labeling relative to other childhood cancers and lung cancer, and were distinguished by abundant tyrosine catabolites consistent with catecholamine synthesis.

Conclusions: Intra-operative [U13C]glucose infusions are safe and informative in pediatric cancer. Tumors of various histologies use glycolysis and oxidative metabolism, with subtype-selective differences evident from this small cohort. Expanding this cohort may uncover predictive biomarkers and therapeutic targets from tumor metabolism.

Funding: N.C.I grants to P.L. (R21CA220090-01A1) and R.J.D. (R35CA22044901); H.H.M.I. funding to R.J.D.; Children's Clinical Research Advisory Committee funding to K.J.

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