使用正电子发射断层扫描对乳腺癌化学激素疗法进行代谢监测：初步评估

Metabolic monitoring of breast cancer chemohormonotherapy using positron emission tomography: initial evaluation.

作者信息

Wahl R L, Zasadny K, Helvie M, Hutchins G D, Weber B, Cody R

机构信息

Department of Internal Medicine, University of Michigan Medical Center, Ann Arbor 48109-0028.

出版信息

J Clin Oncol. 1993 Nov;11(11):2101-11. doi: 10.1200/JCO.1993.11.11.2101.

DOI:10.1200/JCO.1993.11.11.2101

PMID:8229124

Abstract

PURPOSE

We assessed the feasibility of noninvasive metabolic monitoring of cancer chemohormonotherapy using sequential quantitative positron emission tomographic (PET) scans of tumor glucose metabolism with the glucose analog 2-[18F]-fluoro-2-deoxy-D-glucose (FDG).

PATIENTS AND METHODS

Eleven women with newly diagnosed primary breast cancers larger than 3 cm in diameter beginning a chemohormonotherapy program underwent a baseline and four follow-up quantitative PET scans during the first three cycles of treatment (days 0 to 63). Tumor response was sequentially determined clinically, radiographically, and then pathologically after nine treatment cycles.

RESULTS

Eight patients had partial or complete pathologic responses. Their maximal tumor uptake of FDG assessed by PET decreased promptly with treatment to the following: day 8, 78 +/- 9.2% (P < .03); day 21, 68.1 +/- 7.5% (P < .025); day 42, 60 +/- 5.1% (P < .001); day 63, 52.4 +/- 4.4% (P < .0001) of the basal values. Tumor diameter did not decrease significantly during this period through 63 days. Prompt decreases in the FDG influx rate (K) from basal levels (from .019 to .014 mL/cm3/min) after 8 days of treatment (P < .02) and in the estimated rate of FDG phosphorylation to FDG-6-phosphate (k3) from .055 to .038 min-1 after 8 days of treatment (P < .02) to .029 +/- .004 min-1 at 21 days) (P < .02) were observed. Three nonresponding patients had no significant decrease in tumor uptake of FDG (81 +/- 18% of basal value), influx rate (.015 to .012 mL/cm3/min), or tumor size (81 +/- 12% of basal diameter) comparing basal versus 63-day posttreatment values.

CONCLUSION

Quantitative FDG PET scans of primary breast cancers showed a rapid and significant decrease in tumor glucose metabolism after effective treatment was initiated, with the reduction in metabolism antedating any decrement in tumor size. No significant decrease in FDG uptake (SUV) after three cycles of treatment was observed in the nonresponding patients. FDG PET scanning has substantial promise as an early noninvasive metabolic marker of the efficacy of cancer treatment.

摘要

目的

我们使用葡萄糖类似物2-[18F]-氟-2-脱氧-D-葡萄糖（FDG）对肿瘤葡萄糖代谢进行序贯定量正电子发射断层扫描（PET），评估癌症化学激素疗法无创代谢监测的可行性。

患者与方法

11名新诊断的直径大于3 cm的原发性乳腺癌女性患者开始化学激素治疗方案，在治疗的前三个周期（第0至63天）接受了一次基线和四次随访定量PET扫描。在九个治疗周期后，依次通过临床、影像学，然后病理确定肿瘤反应。

结果

8名患者有部分或完全病理反应。通过PET评估，她们肿瘤对FDG的最大摄取量随治疗迅速下降至以下水平：第8天，为基线值的78±9.2%（P<.03）；第21天，为68.1±7.5%（P<.025）；第42天，为60±5.1%（P<.001）；第63天，为52.4±4.4%（P<.0001）。在此期间直至63天，肿瘤直径未显著减小。治疗8天后，FDG流入率（K）从基线水平（从.019降至.014 mL/cm³/min）迅速下降（P<.02），治疗8天后，FDG磷酸化生成6-磷酸-FDG的估计速率（k3）从.055降至.038 min⁻¹（P<.02），至21天时降至.029±.004 min⁻¹（P<.02）。3名无反应患者肿瘤对FDG的摄取量（为基线值的81±18%）、流入率（从.015降至.012 mL/cm³/min）或肿瘤大小（为基线直径的81±12%），与基线值和治疗后63天的值相比均无显著下降。