厄洛替尼治疗对表皮生长因子受体（EGFR）突变的晚期非小细胞肺癌（NSCLC）中[¹¹C]厄洛替尼摄取的影响

Effects of erlotinib therapy on [(11)C]erlotinib uptake in EGFR mutated, advanced NSCLC.

作者信息

Bahce Idris, Yaqub Maqsood, Errami Hanane, Schuit Robert C, Schober Patrick, Thunnissen Erik, Windhorst Albert D, Lammertsma Adriaan A, Smit Egbert F, Hendrikse N Harry

机构信息

Department of Pulmonary Diseases, VU University Medical Center, PO Box 7057, 1007MB, Amsterdam, The Netherlands.

Department of Radiology & Nuclear Medicine, VU University Medical Center, Amsterdam, The Netherlands.

出版信息

EJNMMI Res. 2016 Dec;6(1):10. doi: 10.1186/s13550-016-0169-8. Epub 2016 Feb 9.

DOI:10.1186/s13550-016-0169-8

PMID:26857779

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4746207/

Abstract

BACKGROUND

In non-small cell lung cancer (NSCLC) patients off erlotinib therapy, positron emission tomography (PET) using [(11)C]erlotinib distinguished epidermal growth factor receptor (EGFR) mutations from wild-type EGFR. However, tumor uptake of [(11)C]erlotinib during erlotinib therapy is unknown. Therefore, the aims of this study were to evaluate tumor [(11)C]erlotinib uptake in NSCLC patients both on and off erlotinib therapy, to evaluate the effect of erlotinib therapy on tumor perfusion and its correlation to tumor [(11)C]erlotinib uptake, and also, to investigate simplified uptake parameters using arterial and venous blood samples.

METHODS

Ten patients were to be scanned twice with a 1-2-week interval, i.e., on (E+) and off (E-) erlotinib therapy. Each procedure consisted of a low-dose CT scan, a 10-min dynamic [(15)O]H2O PET scan, and a 60-min dynamic [(11)C]erlotinib PET scan with arterial and venous sampling at six time points. In patients(E+), the optimal compartment model was analyzed using Akaike information criterion. In patients(E-), the uptake parameter was the volume of distribution (V T), estimated by using metabolite-corrected plasma input curves based on image-derived input functions and discrete arterial and venous blood samples. Tumor blood flow (TBF) was determined by rate constant of influx (K1) of [(15)O]H2O using the 1T2k model and correlated with V T and K1 values of [(11)C]erlotinib. The investigated simplified parameters were standardized uptake value (SUV) and tumor-to-blood ratio (TBR) at 40-60 min pi interval.

RESULTS

Of the 13 patients included, ten were scanned twice. In patients(E+), [(11)C]erlotinib best fitted the 2T4k model with V T. In all patients, tumor V T(E+) was lower than V T(E-) (median V T(E-) = 1.61, range 0.77-3.01; median V T(E+) = 1.17, range 0.53-1.74; P = 0.004). Using [(15)O]H2O, five patients were scanned twice. TBF did not change with erlotinib therapy, TBF showed a positive trend towards correlation with [(11)C]erlotinib K1, but not with V T. TBR40-50 and TBR50-60, using both arterial and venous sampling, correlated with V T(E-) (all r s >0.9, P < 0.001), while SUV did not. In patients off and on therapy, venous TBR underestimated arterial TBR by 26 ± 12 and 9 ± 9 %, respectively.

CONCLUSIONS

In patients on erlotinib in therapeutic dose, tumor V T decreases with high variability, independent of tumor perfusion. For simplification of [(11)C]erlotinib PET scanning protocols, both arterial and venous TBR 40-60 min post injection can be used; however, arterial and venous TBR values should not be interchanged as venous values underestimate arterial values.

TRIAL REGISTRATION

Registered at the Netherlands Trial Registry: NTR3670 .

摘要

背景

在非小细胞肺癌（NSCLC）患者中，使用[（11）C]厄洛替尼的正电子发射断层扫描（PET）可区分表皮生长因子受体（EGFR）突变与野生型EGFR。然而，厄洛替尼治疗期间肿瘤对[（11）C]厄洛替尼的摄取情况尚不清楚。因此，本研究的目的是评估接受和未接受厄洛替尼治疗的NSCLC患者肿瘤对[（11）C]厄洛替尼的摄取情况，评估厄洛替尼治疗对肿瘤灌注的影响及其与肿瘤[（11）C]厄洛替尼摄取的相关性，并研究使用动脉血和静脉血样本的简化摄取参数。

方法

10例患者将在1 - 2周的间隔内进行两次扫描，即接受（E +）和未接受（E -）厄洛替尼治疗时。每次检查包括一次低剂量CT扫描、一次10分钟的动态[（15）O]H2O PET扫描以及一次60分钟的动态[（11）C]厄洛替尼PET扫描，并在六个时间点采集动脉血和静脉血样本。在（E +）组患者中，使用赤池信息准则分析最佳房室模型。在（E -）组患者中，摄取参数为分布容积（VT），通过基于图像衍生输入函数和离散动脉血与静脉血样本的代谢物校正血浆输入曲线进行估计。使用1T2k模型通过[（15）O]H2O的流入速率常数（K1）确定肿瘤血流量（TBF），并将其与[（11）C]厄洛替尼的VT和K1值相关联。研究的简化参数为注射后40 - 60分钟期间的标准化摄取值（SUV）和肿瘤与血液比值（TBR）。

结果

纳入的13例患者中，10例进行了两次扫描。在（E +）组患者中，[（11）C]厄洛替尼最符合具有VT的2T4k模型。在所有患者中，肿瘤VT（E +）低于VT（E -）（VT（E -）中位数 = 1.61，范围0.77 - 3.01；VT（E +）中位数 = 1.17，范围0.53 - 1.74；P = 0.004）。使用[（15）O]H2O对5例患者进行了两次扫描。TBF在厄洛替尼治疗后未发生变化，TBF与[（11）C]厄洛替尼K1呈正相关趋势，但与VT无相关性。使用动脉血和静脉血样本的TBR40 - 50和TBR50 - 60与VT（E -）相关（所有rs>0.9，P<0.001），而SUV则不然。在接受治疗和未接受治疗的患者中，静脉TBR分别比动脉TBR低26±12%和9±9%。

结论

在接受治疗剂量厄洛替尼的患者中，肿瘤VT降低且变异性高，与肿瘤灌注无关。为简化[（11）C]厄洛替尼PET扫描方案，可使用注射后40 - 60分钟的动脉血和静脉血TBR；然而，动脉血和静脉血TBR值不应互换，因为静脉血值低于动脉血值。

试验注册

在荷兰试验注册中心注册：NTR3670 。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ebf3/4746207/45102afa7dc7/13550_2016_169_Fig1_HTML.jpg

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厄洛替尼治疗对表皮生长因子受体（EGFR）突变的晚期非小细胞肺癌（NSCLC）中[¹¹C]厄洛替尼摄取的影响

Effects of erlotinib therapy on [(11)C]erlotinib uptake in EGFR mutated, advanced NSCLC.

作者信息

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