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SPECT/CT 联合 PSMA 配体 99mTc-MIP-1404 对前列腺癌患者进行全身初步分期。

SPECT/CT With the PSMA Ligand 99mTc-MIP-1404 for Whole-Body Primary Staging of Patients With Prostate Cancer.

出版信息

Clin Nucl Med. 2018 Apr;43(4):225-231. doi: 10.1097/RLU.0000000000001991.

Abstract

BACKGROUND

Tc-MIP-1404 (Progenics Pharmaceuticals, Inc, New York, NY) is a novel ligand binding to prostate-specific membrane antigen suitable for SPECT. There are, as yet, no data concerning its use in whole-body primary staging and its interobserver variability in patients with prostate cancer (PC) prior to therapy.

METHODS

A search of our clinical database from April 2013 to May 2017 yielded 93 patients with histologically confirmed cancer in whom Tc-MIP-1404 SPECT/CT had been performed for primary whole-body staging before therapy. Whole-body planar and SPECT/CT images of the lower abdomen and thorax had been obtained 3 to 4 hours postinjection of 706 ± 72 MBq Tc-MIP-1404. Images were visually analyzed for extent and location of abnormal uptake by 2 experienced nuclear physicians. Interobserver agreement for detection of primary tumor and metastatic lesions was assessed. In addition, SUVs of prostate-specific membrane antigen-positive regions of the prostate were determined in all patients, and from these, a variable reflecting total tumor load in the prostate gland was calculated (TUprostate). Follow-up reports of subsequent therapeutic interventions were available in 52 (56%) of all patients with a median follow-up of 18 months.

RESULTS

In 90 (97%) of 93 patients, prostate uptake above background was detected as correlate of the histologically diagnosed PC. Forty-eight lymph node and 29 bone metastases were detected in 16 and 9 patients, respectively. In addition, 3 patients had disseminated bone metastases. No distant organ metastases were found. Interobserver agreement was high for the overall scan result (97%), as well as for the detection of the primary tumor (97%), of lymph node metastases (97%), and of bone metastases (99%). Recurrence of PC occurred in 5 patients in whom follow-up was available (10%). TUprostate was significantly higher in patients with Gleason scores of 8 or greater compared with patients with Gleason scores of 7 or less and at prostate-specific antigen (PSA) serum levels of 10 ng/mL or greater compared with PSA serum levels of 10 ng/mL or less. TUprostate of greater than 26 in the primary tumor predicted the occurrence of lymph node or bone metastases with a sensitivity of 82% and specificity of 76%.

CONCLUSIONS

MIP-1404 SPECT/CT has a high accuracy and low interobserver variability in the diagnosis of PC and allows detection of lymph node and bone metastases in a significant proportion of as yet untreated PC patients. TUprostate is correlated with Gleason score and PSA serum concentration and allows prediction of the occurrence of lymph node and bone metastases with moderate accuracy at primary staging.

摘要

背景

Tc-MIP-1404(Progenics Pharmaceuticals,Inc.,纽约州,纽约)是一种新型配体,可与前列腺特异性膜抗原结合,适用于 SPECT。目前尚无关于其在治疗前前列腺癌(PC)患者全身初步分期中的应用以及其在观察者之间的变异性的数据。

方法

对 2013 年 4 月至 2017 年 5 月期间的临床数据库进行检索,发现 93 例经组织学证实患有癌症的患者,这些患者在治疗前均进行了 Tc-MIP-1404 SPECT/CT 全身初步分期。在注射 706±72MBq Tc-MIP-1404 后 3 至 4 小时,获得下腹部和胸部的全身平面和 SPECT/CT 图像。两位有经验的核医学医师对异常摄取的范围和位置进行了视觉分析。评估了检测原发性肿瘤和转移性病变的观察者间一致性。此外,对所有患者的前列腺特异性膜抗原阳性区域的 SUV 进行了测定,并由此计算了反映前列腺内总肿瘤负荷的变量(TUprostate)。在所有 93 例患者中,有 52 例(56%)患者可获得后续治疗干预的随访报告,中位随访时间为 18 个月。

结果

在 93 例患者中,90 例(97%)患者的前列腺摄取率高于背景,这与组织学诊断的 PC 相关。16 例和 9 例患者分别检测到 48 个淋巴结转移和 29 个骨转移。此外,3 例患者有骨转移。未发现远处器官转移。总体扫描结果(97%)、原发性肿瘤(97%)、淋巴结转移(97%)和骨转移(99%)的观察者间一致性均较高。在可获得随访的 5 例患者中,PC 复发(10%)。与前列腺特异性抗原(PSA)血清水平为 10ng/mL 或更低的患者相比,Gleason 评分≥8 的患者的 TUprostate 显著更高,与 PSA 血清水平为 10ng/mL 或更低的患者相比,PSA 血清水平为 10ng/mL 或更低的患者的 TUprostate 显著更高。原发性肿瘤的 TUprostate 大于 26 预测淋巴结或骨转移的发生,其敏感性为 82%,特异性为 76%。

结论

MIP-1404 SPECT/CT 在诊断 PC 方面具有较高的准确性和较低的观察者间变异性,并且可以在相当一部分未经治疗的 PC 患者中检测到淋巴结和骨转移。TUprostate 与 Gleason 评分和 PSA 血清浓度相关,可在初步分期时以中等准确性预测淋巴结和骨转移的发生。

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