Positron emission tomography imaging of drug-induced tumor apoptosis with a caspase-3/7 specific [~(18)F]-labeled isatin sulfonamide

Quang-De Nguyen; Graham Smith; Matthias Glaser; Meg Perumal; Erik Arstad; Eric O. Aboagye

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Positron emission tomography imaging of drug-induced tumor apoptosis with a caspase-3/7 specific [~(18)F]-labeled isatin sulfonamide

机译：用caspase-3 / 7特异性[〜（18）F]标记的靛红磺酰胺对药物诱导的肿瘤凋亡进行正电子发射断层成像

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Of the molecular biochemical alterations that occur during apoptosis, activation of caspases, notably caspase-3, is probably the most attractive for developing specific in vivo molecular imaging probes. We recently designed a library of isatin-5 sulfonamides and selected [~(18)F]ICMT-11 for further evaluation on the basis of sub-nanomolar affinity for activated capsase-3, high metabolic stability, and facile radiolabeling. In this present study, we have demonstrated that [~(18)F]ICMT-11 binds to a range of drug-induced apoptotic cancer cells in vitro and to 38C13 murine lymphoma xenografts in vivo by up to 2-fold at 24 h posttreatment compared to vehicle treatment. We further demonstrated that the increased signal intensity in tumors after drug treatment, detected by whole body in vivo microPET imaging, was associated with increased apoptosis. In summary, we have characterized [~(18)F]ICMT-11 as a caspase-3/7 specific PET imaging radiotracer for the assessment of tumor apoptosis that could find utility in anticancer drug development and the monitoring of early responses to therapy.

机译：在凋亡过程中发生的分子生物化学变化中，胱天冬酶特别是caspase-3的激活可能是开发特定的体内分子成像探针最有吸引力的。我们最近设计了一个isatin-5磺酰胺文库，并基于亚纳莫拉对活化Capsase-3的亲和力，高代谢稳定性和简便的放射性标记，选择了[〜（18）F] ICMT-11进行进一步评估。在本研究中，我们证明了[〜（18）F] ICMT-11在体外与一系列药物诱导的凋亡癌细胞结合，在体内与38C13鼠淋巴瘤异种移植物在治疗后24小时最多结合2倍。相比车辆治疗。我们进一步证明了通过体内microPET全身成像检测到的药物治疗后肿瘤中信号强度的增加与凋亡的增加有关。总之，我们已将[〜（18）F] ICMT-11表征为caspase-3 / 7特异性PET成像放射性示踪剂，用于评估肿瘤细胞凋亡，可以发现其在抗癌药物开发中的用途以及对治疗的早期反应的监测。

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《Proceedings of the National Academy of Sciences of the United States of America》 |2009年第38期|16375-16380|共6页
作者
Quang-De Nguyen; Graham Smith; Matthias Glaser; Meg Perumal; Erik Arstad; Eric O. Aboagye;
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作者单位

Comprehensive Cancer Imaging Center, Department of Oncology, Imperial College London Faculty of Medicine, Hammersmith Hospital, Du Cane Road, London W12 0NN, United Kingdom;

Comprehensive Cancer Imaging Center, Department of Oncology, Imperial College London Faculty of Medicine, Hammersmith Hospital, Du Cane Road, London W12 0NN, United Kingdom;

MDx Discovery (part of GE Healthcare) at Hammersmith Imanet Ltd., Hammersmith Hospital, Du Cane Road, London W12 0NN, United Kingdom;

Comprehensive Cancer Imaging Center, Department of Oncology, Imperial College London Faculty of Medicine, Hammersmith Hospital, Du Cane Road, London W12 0NN, United Kingdom;

MDx Discovery (part of GE Healthcare) at Hammersmith Imanet Ltd., Hammersmith Hospital, Du Cane Road, London W12 0NN, United Kingdom;

Comprehensive Cancer Imaging Center, Department of Oncology, Imperial College London Faculty of Medicine, Hammersmith Hospital, Du Cane Road, London W12 0NN, United Kingdom;

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收录信息美国《科学引文索引》(SCI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
中图分类
关键词
cell death; response to treatment; small animal imaging;

机译：细胞死亡;对治疗的反应;小动物成像;

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1. Al 18 18 F labeled sulfonamide‐conjugated positron emission tomography tracer in vivo tumor‐targeted imaging [J] . Liu Fan, Zhao Biao, Xia Xiao‐Tian, Journal of cellular biochemistry. . 2019,第10期

机译：Al 18 18 18 F标记磺胺酰胺共轭正电子发射断层摄影跟踪器，体内肿瘤靶向成像
2. Imaging apoptosis with positron emission tomography: 'Bench to bedside' development of the caspase-3/7 specific radiotracer [ 18F]ICMT-11 [J] . NguyenQ.-D., ChallapalliA., SmithG., European journal of cancer: official journal for European Organization for Research and Treatment of Cancer (EORTC) [and] European Association for Cancer Research (EACR) . 2012,第4期

机译：用正电子发射断层成像术对细胞凋亡进行成像：caspase-3 / 7特异性放射性示踪剂的“从台到床”发展[18F] ICMT-11
3. The nonpeptidyl caspase binding radioligand (S)-1-(4-(2-[~(18)F]Fluoroethoxy)-benzyl)-5-[1-(2-methoxymethylpyrrolidinyl)sulfonyl]isatin ([~(18)F]CbR) as potential positron emission tomography-compatible apoptosis imaging agent [J] . A. FAUST, S. WAGNER, M. P. LAW, The quarterly journal of nuclear medicine and molecular imaging . 2007,第1期

机译：与非肽基胱天蛋白酶结合的放射性配体（S）-1-（4-（2- [〜（18）F]氟乙氧基）-苄基）-5- [1-（2-甲氧基甲基吡咯烷基）磺酰基] isatin（[〜（18）F ] CbR）作为潜在的正电子发射断层扫描兼容的凋亡显像剂
4. Synthesis of ¹⁸F-labeled probes on EWOD platform for Positron Emission Tomography (PET) preclinical imaging [C] . Chen S., Keng P.Y., van Dam R.M., 2011 IEEE 24th International Conference on Micro Electro Mechanical Systems . 2011

机译：在EWOD平台上合成^{18 F标记的探针，用于正电子发射断层扫描（PET）临床前成像}
5. Development of positron emission tomography (PET) labeled polypeptide nanoparticles for tumor imaging and targeting. [D] . Mohd Janib, Siti Najila. 2013

机译：用于肿瘤成像和靶向的正电子发射断层扫描（PET）标记的多肽纳米颗粒的开发。
6. Positron emission tomography imaging of drug-induced tumor apoptosis with a caspase-3/7 specific 18F-labeled isatin sulfonamide [O] . Quang-Dé Nguyen, Graham Smith, Matthias Glaser, 2009

机译：用caspase-3 / 7特异性18F标记的靛红磺酰胺对药物诱导的肿瘤凋亡进行正电子发射断层成像
7. Positron emission tomography imaging of drug-induced tumor apoptosis with a caspase-3/7 specific [18F]-labeled isatin sulfonamide [O] . Nguyen, Quang-Dé, Smith, Graham, Glaser, Matthias, 2009

机译：用caspase-3 / 7特异性[18F]标记的靛红磺酰胺对药物诱导的肿瘤凋亡进行正电子发射断层成像

Positron emission tomography imaging of drug-induced tumor apoptosis with a caspase-3/7 specific [~(18)F]-labeled isatin sulfonamide

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