用5-氟尿嘧啶、奥沙利铂、伊立替康和西妥昔单抗处理的结直肠肿瘤细胞表现出与己糖激酶活性和葡萄糖转运相对应的18F-氟代脱氧葡萄糖摄取变化。

Colorectal tumor cells treated with 5-FU, oxaliplatin, irinotecan, and cetuximab exhibit changes in 18F-FDG incorporation corresponding to hexokinase activity and glucose transport.

作者信息

Sharma Rituka I, Smith Tim A D

机构信息

School of Medical Sciences (Biomedical Physics), University of Aberdeen, Foresterhill, Aberdeen, United Kingdom.

出版信息

J Nucl Med. 2008 Aug;49(8):1386-94. doi: 10.2967/jnumed.107.047886. Epub 2008 Jul 16.

DOI:10.2967/jnumed.107.047886

PMID:18632807

Abstract

UNLABELLED

The purpose of this study was to determine therapy-induced changes in 18F-FDG incorporation at the colorectal tumor cell level in response to conventional and novel chemotherapy agents and examine how these changes relate to factors involved in 18F-FDG incorporation.

METHODS

SW620 cells were treated with inhibitory concentration of 50% (IC50) doses (determined by MTT) of 5-fluorouracil (5-FU), oxaliplatin, and irinotecan; HCT-8 cells were treated with IC50 doses of irinotecan, cetuximab, and irinotecan plus cetuximab. 18F-FDG incorporation, glucose transport, hexokinase (HK) activity, adenosine triphosphate (ATP) content, annexin V binding, and cell cycle distribution were determined after 24-, 48-, and 72-h treatments. Eight-hour treatments with and without subsequent incubation in drug-free medium were also examined. A clonogenic assay was used to determine the tumor-forming ability of treated cells.

RESULTS

Apoptosis was evident in SW620 cells, especially after treatment with irinotecan and 5-FU. 18F-FDG incorporation was increased in SW620 cells after 24- or 48-h treatments with some agents and in HCT-8 cells after irinotecan treatment but was decreased in all 72-h treatments or cell-line combinations including cetuximab. Treatment of SW620 cells for 8 h followed by 64 h in drug-free medium also resulted in decreased 18F-FDG incorporation. Decreased 18F-FDG incorporation broadly corresponded to glucose transport in HCT-8 cells and to HK activity in SW620 cells. Inhibition of glucose transport decreased 18F-FDG incorporation into HCT-8 but not into SW620 cells. ATP levels were decreased by oxaliplatin treatment and increased at 48 or 72 h after irinotecan treatment.

CONCLUSION

18F-FDG incorporation is modulated by therapy-induced changes in both glucose transport and HK activity depending on the tumor cell. Colorectal cells treated with IC50 doses of cetuximab also exhibit decreased 18F-FDG.

摘要

未标记

本研究的目的是确定在接受传统和新型化疗药物治疗后，结直肠肿瘤细胞水平上18F-FDG摄取的治疗诱导变化，并研究这些变化与参与18F-FDG摄取的因素之间的关系。

方法

用5-氟尿嘧啶（5-FU）、奥沙利铂和伊立替康的50%抑制浓度（IC50）剂量（通过MTT测定）处理SW620细胞；用伊立替康、西妥昔单抗以及伊立替康加西妥昔单抗的IC50剂量处理HCT-8细胞。在处理24、48和72小时后，测定18F-FDG摄取、葡萄糖转运、己糖激酶（HK）活性、三磷酸腺苷（ATP）含量、膜联蛋白V结合以及细胞周期分布。还检测了有无后续在无药物培养基中孵育的8小时处理情况。采用克隆形成试验来确定处理后细胞的肿瘤形成能力。

结果

SW620细胞中凋亡明显，尤其是在用伊立替康和5-FU处理后。在用某些药物处理24或48小时后，SW620细胞中的18F-FDG摄取增加，在伊立替康处理后HCT-8细胞中的18F-FDG摄取增加，但在所有72小时处理或包括西妥昔单抗的细胞系组合中18F-FDG摄取减少。对SW620细胞处理8小时后再在无药物培养基中培养64小时，也导致18F-FDG摄取减少。18F-FDG摄取减少大致与HCT-8细胞中的葡萄糖转运以及SW620细胞中的HK活性相对应。葡萄糖转运的抑制降低了18F-FDG在HCT-8细胞中的摄取，但未降低在SW620细胞中的摄取。奥沙利铂处理使ATP水平降低，伊立替康处理后48或72小时ATP水平升高。