Prasad V, Baum R P
Department of Nuclear Medicine/Center for PET, Zentralklinik Bad Berka, Bad Berka, Germany.
Q J Nucl Med Mol Imaging. 2010 Feb;54(1):61-7.
The aim of the study was 1) to determine the normal biodistribution of radiolabeled somatostatin analogue (68)Ga DOTA-NOC; 2) to establish the range of its uptake in liver, bone and lymph node metastases in patients with NET, 3) to establish the cut-off value for differentiating between physiological uptake and tumor related sstr expression in the processus uncinatus of pancreas.
Maximum standardized uptake values (SUV(max)) of (68)Ga DOTA-NOC were determined in normal organs of 89 NET patients undergoing receptor PET/CT. In addition, SUV(max) of primary pancreatic neuroendocrine tumors (pNET), liver, bone and lymph node metastases were evaluated.
SUV(max) (mean + or - standard deviation) were determined in: pituitary gland 2.6 + or - 1.3, thyroid: 3.4 + or - 1.4, lung: 0.9 + or - 0.8, normal liver: 6.9 + or - 2 , spleen: 22.0 + or - 10.0, adrenal 6.0 + or - 2.5, kidney: 12.9 + or - 3.8, gastrointestinal tract 2.3 + or - 1.0, gluteal muscle:1.0 + or - 0.3, femur 0.8 + or - 0.3, blood pool 2.6 + or - 1.2 and processus uncinatus of pancreas 5.8 + or - 2.0. SUV(max) of (68)Ga DOTA-NOC was 19.6 + or - 13.4 (N.=200) in liver metastases, 12.5 + or - 10 (N.=67) in lymph nodes metastasis, 9.5 + or - 6.0 (N.=78) in bone lesions, and 20.8 + or - 10.8 (N.=26) in pancreatic neuroendocrine primary tumors. Target to non target (T/NT) ratios were 3.4 + or - 2.3 for liver metastases (with normal
There is a broad range of sstr expression in metastastic lesions and in pNET. The splenic uptake of (68)Ga DOTA-NOC is highly variable. (68)Ga DOTA-NOC is an excellent tracer for imaging somatostatin receptor positive tumors, which, due to the high target to non-target ratios, allows the detection of very small lesions, especially of lymph node and bone metastases.
本研究的目的是:1)确定放射性标记的生长抑素类似物(68)Ga DOTA-NOC的正常生物分布;2)确定其在神经内分泌肿瘤(NET)患者肝脏、骨骼和淋巴结转移灶中的摄取范围;3)确定区分胰腺钩突部生理性摄取和肿瘤相关生长抑素受体(sstr)表达的临界值。
在89例接受受体PET/CT检查的NET患者的正常器官中测定(68)Ga DOTA-NOC的最大标准化摄取值(SUV(max))。此外,还评估了原发性胰腺神经内分泌肿瘤(pNET)、肝脏、骨骼和淋巴结转移灶的SUV(max)。
各部位的SUV(max)(平均值±标准差)分别为:垂体2.6±1.3,甲状腺:3.4±1.4,肺:0.9±0.8,正常肝脏:6.9±2,脾脏:22.0±10.0,肾上腺6.0±2.5,肾脏:12.9±3.8,胃肠道2.3±1.0,臀大肌:1.0±0.3,股骨0.8±0.3,血池2.6±1.2,胰腺钩突部5.8±2.0。(68)Ga DOTA-NOC在肝转移灶中的SUV(max)为19.6±13.4(n=200),在淋巴结转移灶中为12.5±10(n=67),在骨病变中为9.5±6.0(n=78),在胰腺神经内分泌原发性肿瘤中为20.8±10.8(n=26)。肝转移灶的靶非靶(T/NT)比值为3.4±2.3(正常……)
转移灶和pNET中存在广泛的sstr表达。(68)Ga DOTA-NOC在脾脏中的摄取差异很大。(68)Ga DOTA-NOC是一种用于成像生长抑素受体阳性肿瘤的优秀示踪剂,由于其高靶非靶比值,能够检测到非常小的病变,尤其是淋巴结和骨转移灶。
