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18F-多巴PET和增强CT成像在先天性高胰岛素血症中的应用:从技术人员角度看英国的初步经验

18F-DOPA PET and enhanced CT imaging for congenital hyperinsulinism: initial UK experience from a technologist's perspective.

作者信息

Meintjes Marguerite, Endozo Raymond, Dickson John, Erlandsson Kjel, Hussain Khalid, Townsend Caroline, Menezes Leon, Bomanji Jamshed

机构信息

Institute of Nuclear Medicine, University College London Hospital NHS Trust, London, UK.

出版信息

Nucl Med Commun. 2013 Jun;34(6):601-8. doi: 10.1097/MNM.0b013e32836069d0.

Abstract

INTRODUCTION

Congenital hyperinsulinism (CHI) is the most common cause of persistent hypoglycaemia in infants and children. Histologically, there are two subgroups, diffuse and focal. The aim of this study was to evaluate the accuracy of (18)F-fluoro-L-dihydroxyphenylalanine ((18)F-DOPA) PET/computed tomography (CT) and contrast-enhanced CT in distinguishing between focal and diffuse lesions in infants with CHI who are unresponsive to medical therapy. In addition, this paper describes the detailed protocol used for imaging and analysis of (18)F-DOPA PET/CT images in our clinical practice.

MATERIALS AND METHODS

Twenty-two (18)F-DOPA PET/CT and contrast-enhanced CT imaging studies were carried out on 18 consecutive patients (nine boys and nine girls) with CHI (median age, 2 years and 1 month; range, 1-84 months) who had positive dominant ABCC8 mutation genetic results or negative ABCC8/t results but did not respond to first-line medical therapy with high-dose diazoxide. (18)F-DOPA was produced by the cyclotron unit of Woolfson Molecular Imaging Centre, Manchester, and transported to our centre in central London after synthesis and implementation of quality control measures. (18)F-DOPA was administered intravenously at a dose of 4 MBq/kg, and iodine contrast medium was injected intravenously at a dose of 1.5 ml/kg. Single bed position PET/CT images of the pancreas were acquired under light sedation with oral chloral hydrate. Four PET dynamic data acquisition scans were taken 20, 40, 50 and 60 min after injection for a duration of 10 min each. The results were assessed by visual interpretation and quantitative measurements of standardized uptake values (SUVs) in the head, body, and tail of the pancreas.

RESULTS

Of the 18 patients, 13 showed diffuse and five showed focal (18)F-DOPA PET pancreatic uptake. Three regions of interest were drawn over the head, body and tail of the pancreas to calculate the SUV(max). Using the formula - highest SUV(max)/next highest SUV(max) - a ratio was calculated. Five patients had an accumulation of F-DOPA in the pancreas and an SUV ratio greater than 1.5, indicating focal disease with an SUV(max) more than 50% higher than that of the unaffected areas of the pancreas. The remaining 13 patients had diffuse accumulation of (18)F-DOPA in the pancreas (SUV ratio<1.3). Using this ratio, a focal lesion can be distinguished from diffuse uptake and normal pancreatic uptake. The sizes of these regions of interest varied according to the age of the child. All patients diagnosed with focal lesions underwent surgery and were cured eventually. Lesions were accurately localized by PET/CT and confirmed by histological results after surgery. Three of these patients had to undergo second (18)F-DOPA scans and second surgeries after unsuccessful excision during their first surgery. Three patients with diffuse disease underwent a partial pancreatectomy, and histological results confirmed diffuse disease. One patient was cured and two remain on high-dose diazoxide therapy because of persistent hypoglycaemia.

CONCLUSION

(18)F-DOPA PET/CT offers excellent differentiation of focal from diffuse CHI, and the contrast-enhanced CT technique permits precise preoperative localization of the lesion and anatomical landmarks.

摘要

引言

先天性高胰岛素血症(CHI)是婴幼儿持续性低血糖最常见的病因。组织学上,可分为两个亚组,即弥漫性和局灶性。本研究旨在评估18F-氟-L-二羟基苯丙氨酸(18F-DOPA)PET/计算机断层扫描(CT)及增强CT在鉴别对药物治疗无反应的CHI婴儿局灶性和弥漫性病变中的准确性。此外,本文还描述了我们临床实践中用于18F-DOPA PET/CT图像成像及分析的详细方案。

材料与方法

对18例连续的CHI患者(9例男孩和9例女孩,中位年龄2岁1个月,范围1 - 84个月)进行了22次18F-DOPA PET/CT及增强CT成像研究,这些患者ABCC8突变基因检测结果为阳性或ABCC8/t结果为阴性,但对高剂量二氮嗪一线药物治疗无反应。18F-DOPA由曼彻斯特伍尔夫森分子影像中心的回旋加速器生产,经合成及质量控制措施后转运至位于伦敦市中心的我们的中心。18F-DOPA以4 MBq/kg的剂量静脉注射,碘造影剂以1.5 ml/kg的剂量静脉注射。在口服水合氯醛轻度镇静下采集胰腺的单床位PET/CT图像。注射后20、40、50和60分钟进行4次PET动态数据采集扫描,每次持续10分钟。通过视觉解读及对胰腺头部、体部和尾部标准化摄取值(SUV)的定量测量来评估结果。

结果

18例患者中,13例显示弥漫性18F-DOPA PET胰腺摄取,5例显示局灶性摄取。在胰腺的头部、体部和尾部绘制三个感兴趣区以计算SUV(最大值)。使用公式 - 最高SUV(最大值)/次高SUV(最大值) - 计算比值。5例患者胰腺中F-DOPA积聚且SUV比值大于1.5,表明为局灶性病变,其SUV(最大值)比胰腺未受影响区域高50%以上。其余13例患者胰腺中18F-DOPA呈弥漫性积聚(SUV比值<1.3)。利用该比值可区分局灶性病变与弥漫性摄取及正常胰腺摄取。这些感兴趣区的大小因患儿年龄而异。所有诊断为局灶性病变的患者均接受了手术并最终治愈。病变通过PET/CT准确定位,并在术后经组织学结果证实。其中3例患者在首次手术切除失败后不得不接受第二次18F-DOPA扫描及第二次手术。3例弥漫性疾病患者接受了部分胰腺切除术,组织学结果证实为弥漫性疾病。1例患者治愈,2例因持续性低血糖仍接受高剂量二氮嗪治疗。

结论

18F-DOPA PET/CT能出色地区分局灶性与弥漫性CHI,增强CT技术可实现病变的精确术前定位及解剖标志显示。

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