Positron emission tomography imaging of the sodium iodide symporter senses real-time energy stress in vivo.

IF 6 3区 医学 Q1 CELL BIOLOGY
Piotr Dzien, Agata Mackintosh, Gaurav Malviya, Emma Johnson, Dmitry Soloviev, Gavin Brown, Alejandro Huerta Uribe, Colin Nixon, Scott K Lyons, Oliver Maddocks, Karen Blyth, David Y Lewis
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引用次数: 1

Abstract

Background: Tissue environment is critical in determining tumour metabolic vulnerability. However, in vivo drug testing is slow and waiting for tumour growth delay may not be the most appropriate endpoint for metabolic treatments. An in vivo method for measuring energy stress would rapidly determine tumour targeting in a physiologically relevant environment. The sodium-iodide symporter (NIS) is an imaging reporter gene whose protein product co-transports sodium and iodide, and positron emission tomography (PET) radiolabelled anions into the cell. Here, we show that PET imaging of NIS-mediated radiotracer uptake can rapidly visualise tumour energy stress within minutes following in vivo treatment.

Methods: We modified HEK293T human embryonic kidney cells, and A549 and H358 lung cancer cells to express transgenic NIS. Next, we subjected these cells and implanted tumours to drugs known to induce metabolic stress to observe the impact on NIS activity and energy charge. We used [18F]tetrafluoroborate positron emission tomography (PET) imaging to non-invasively image NIS activity in vivo.

Results: NIS activity was ablated by treating HEK293T cells in vitro, with the Na+/K+ ATPase inhibitor digoxin, confirming that radiotracer uptake was dependent on the sodium-potassium concentration gradient. NIS-mediated radiotracer uptake was significantly reduced (- 58.2%) following disruptions to ATP re-synthesis by combined glycolysis and oxidative phosphorylation inhibition in HEK293T cells and by oxidative phosphorylation inhibition (- 16.6%) in A549 cells in vitro. PET signal was significantly decreased (- 56.5%) within 90 min from the onset of treatment with IACS-010759, an oxidative phosphorylation inhibitor, in subcutaneous transgenic A549 tumours in vivo, showing that NIS could rapidly and sensitively detect energy stress non-invasively, before more widespread changes to phosphorylated AMP-activated protein kinase, phosphorylated pyruvate dehydrogenase, and GLUT1 were detectable.

Conclusions: NIS acts as a rapid metabolic sensor for drugs that lead to ATP depletion. PET imaging of NIS could facilitate in vivo testing of treatments targeting energetic pathways, determine drug potency, and expedite metabolic drug development.

Abstract Image

Abstract Image

Abstract Image

碘化钠同向体的正电子发射断层成像可以实时感知体内的能量压力。
背景:组织环境是决定肿瘤代谢易感性的关键因素。然而,体内药物测试是缓慢的,等待肿瘤生长延迟可能不是代谢治疗最合适的终点。一种体内测量能量压力的方法将在生理相关环境中快速确定肿瘤靶向。碘化钠同向转运体(NIS)是一种成像报告基因,其蛋白产物将钠和碘化物以及正电子发射断层扫描(PET)放射性标记的阴离子共同转运到细胞中。在这里,我们展示了nis介导的放射性示踪剂摄取的PET成像可以在体内治疗后几分钟内快速显示肿瘤能量应激。方法:对HEK293T人胚胎肾细胞、A549和H358肺癌细胞进行修饰,表达转基因NIS。接下来,我们将这些细胞和植入的肿瘤置于已知可诱导代谢应激的药物中,观察对NIS活性和能量电荷的影响。我们使用[18F]四氟硼酸盐正电子发射断层扫描(PET)成像对体内NIS活性进行无创成像。结果:在体外用Na+/K+ atp酶抑制剂地高辛处理HEK293T细胞后,NIS活性减弱,证实放射性示踪剂的摄取依赖于钠钾浓度梯度。通过糖酵解和氧化磷酸化联合抑制HEK293T细胞和体外氧化磷酸化抑制A549细胞破坏ATP再合成后,nis介导的放射性示踪剂摄取显著降低(- 58.2%)。在体内皮下转基因A549肿瘤中,使用氧化磷酸化抑制剂IACS-010759治疗后90分钟内,PET信号显著降低(- 56.5%),表明NIS可以快速、灵敏地无创检测能量应激,然后才能检测到更广泛的磷酸化amp活化蛋白激酶、磷酸化丙酮酸脱氢酶和GLUT1的变化。结论:NIS可作为导致ATP耗竭的药物的快速代谢传感器。NIS的PET成像可以促进针对能量途径的治疗方法的体内测试,确定药物效力,并加快代谢药物的开发。
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来源期刊
自引率
1.70%
发文量
17
审稿时长
14 weeks
期刊介绍: Cancer & Metabolism welcomes studies on all aspects of the relationship between cancer and metabolism, including: -Molecular biology and genetics of cancer metabolism -Whole-body metabolism, including diabetes and obesity, in relation to cancer -Metabolomics in relation to cancer; -Metabolism-based imaging -Preclinical and clinical studies of metabolism-related cancer therapies.
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