^(131)I的甲状腺击晕效应

阐述了甲状腺击晕效应的概念、判定标准及诊断性131I的剂量、完成诊断性显像到服用去除剂量131I之间的时间间隔等因素对其产生的影响。这对于临床上制定最佳的显像及治疗方案有着重要的指导意义。

甲状腺全切术结合^(131)Ⅰ清甲治疗甲状腺嗜酸细胞肿瘤的临床效果观察

目的观察和探讨甲状腺全切术结合131Ⅰ清甲治疗甲状腺嗜酸细胞肿瘤(HCT)的临床疗效及安全性。方法将2003年1月至2013年1月期间收治的25例HCT患者作为研究对象。患者行甲状腺癌全切术和131Ⅰ清甲治疗,观察治疗后并发症及甲状旁腺功能减退发生情况,并根据131Ⅰ显像及Tg含量检测结果进行疗效评定,随访1年,观察肿瘤复发情况。结果所有患者术后无声嘶、感染等并发症,1例术后出现手足麻木。治疗总有效率为88.00%。随访1年期间复查颈部B超,未见甲状腺床及颈部淋巴结异常肿大,也未见甲状旁腺功能持续性减退。结论甲状腺全切术结合131Ⅰ清甲治疗HCT,疗效满意,安全性高,中远期疗效仍有待进一步观察。

TgAb水平预测TgAb阳性分化型甲状腺癌患者^(131)I治疗后病灶转移的价值分析

目的观察抗甲状腺球蛋白抗体(TgAb)阳性分化型甲状腺癌(DTC)患者^(131)I治疗后血清TgAb水平的变化趋势,探讨TgAb水平变化对转移灶的预测价值。方法回顾性分析158例^(131)I治疗前TgAb阳性的DTC患者的临床资料,根据^(131)I治疗后随访1年时TgAb水平,分为TgAb转阴组和未转阴组,比较两组患者的病灶转移率,观察确诊转移与未转移患者的血清TgAb水平变化趋势。结果TgAb未转阴组的转移率明显高于TgAb转阴组,差异有统计学意义(P=0.002)。TgAb水平升高组与稳定组的转移发生率大致相仿,且高于TgAb水平下降组,但三组间差异无统计学意义(P=0.600)。进一步研究发现,19例确诊转移与139例未转移患者^(131)I治疗后血清TgAb水平变化趋势比较,差异有统计学意义(P=0.002)。结论当血清甲状腺球蛋白(Tg)阴性时,TgAb水平可作为TgAh阳性DTC患者^(131)I治疗后预测转移的监测指标。

甲状腺乳头状癌患者首次131I治疗前刺激性Tg与TSH比值与最佳治疗反应的关系

目的:探讨甲状腺乳头状癌(papillary thyroid carcinoma,PTC)患者首次131I治疗前刺激性Tg与TSH比值对最佳治疗反应的预测价值。方法:回顾性收集2015年1月至2016年6月于我院核医学科首次行131I治疗的PTC患者80例,中位随访时间为50.7个月。监测患者术后首次131I治疗前24 h内刺激性甲状腺球蛋白(preablation stimulated thyroglobulin,psTg)和促甲状腺激素(thyroid stimulating hormone,TSH)水平。根据治疗反应评估体系将其治疗效果分为最佳治疗反应(excellent response,ER)组和非最佳反应(non-excellent response,NER)组。用独立样本t检验、χ2检验和Mann-Whitney U秩和检验或Fisher检验观察比较两组临床病理特征有无统计学差异;对影响ER的因素进行Logistic回归分析;用ROC(receiver operating characteristic)曲线及最佳诊断界值点(diagnostic critical point,DCP)评估psTg、psTg/TSH、肿瘤大小三个指标对ER的预测价值;用Kaplan-meier曲线评估psTg/TSH及肿瘤大小发生非ER的累积风险。结果:两组间psTg(P=0.000)、psTg/TSH(P=0.000)、肿瘤大小(P=0.027)指标差异均有统计学意义(P均<0.05),且psTg、psTg/TSH、肿瘤大小三者的最佳诊断界值点分别为8.26μg/L、0.089、1.1 cm,当psTg/TSH以0.089为界值点时对应的灵敏性和特异性较高,分别为77.59%、95.66%。在原发灶直径小于6 cm时,随着肿瘤的增长,psTg/TSH>0.089组患者的非ER风险明显高于psTg/TSH≤0.089。结论:psTg/TSH与PTC最佳治疗反应有一定关系,低水平psTg/TSH提示治疗效果较好;其与原发灶大小的结合可以更全面的预测初始治疗后的治疗疗效。

A comparative study of influential factors correlating with early and late hypothyroidism after ^131I therapy for Graves＇ disease

Background 131Ⅰ therapy is recognized as the simplest, safest, least expensive, and most effective treatment, and accepted by more and more patients. However its curative effect is influenced by many factors, therefore there are some difficulties for doctors to establish individual treatment strategy. The aims of this study were to determine the incidence of early and late hypothyroidism after 131Ⅰ treatment for Graves＇ disease （GD） and to compare their correlation, to observe and analyze the influential factors and to understand the predictabilities of them.Methods Five hundred GD patients （144 males, 356 females; age （41.2±12.3） years） received 131Ⅰ treatment for the first time. The therapeutic procedure was carried out as the following： undergoing 131Ⅰ uptake test to obtain maximum of thyroid uptake value and effective half-life （EHL） time; estimating the thyroid＇s weight by ultrasonography; determination of thyroid hormones and correlative antibodies; pre-therapy physical examination; thyroid imaging; calculating 131Ⅰtherapeutic dosage; per os uptake of the determined 131Ⅰ dosage; follow-up appraisal of curative effect. The observing parameters included age, gender, thyroid weight, GD duration, condition of onset, state of disease, course of treatment, EHL time, maximum of thyroid uptake value, 131Ⅰ dosage and titer of correlative antibodies. We sorted out the data and used both univariate and multivariate analysis to evaluate them statistically.Results The incidence rates of early and late hypothyroidism were 33.2% and 6.6% respectively after 131Ⅰ treatment and approximately 22.2% cases of late hypothyroidism developed from early hypothyroidism. The influential factors of early hypothyroidism included course of GD, the highest thyroid uptake ratio of 131Ⅰ, EHL time and thyroid microsome antibody （TMAb）, etc. A multivariate analysis on late hypothyroidism showed that female patients, with recurrence after anti-thyroid drug treatment and higher thyroid weight, had lower possibility of late hypothyroidism after 131Ⅰ therapy.Conclusions The incidence of early hypothyroidism is higher than that of late hypothyroidism. The highest thyroid uptake ratio of 131Ⅰ, EHL and TMAb will increase the possibility of early hypothyroidism, while GD course is the protective factor. Higher 131Ⅰ dosage, longer EHL and higher TMAb titer will also increase the possibility of late hypothyroidism. The multi-perspective and multi-factor analysis has the benefit to establish individualized treatment strategy.

治疗前血清Tg、TgAb、VEGF、MIP-1α对分化型甲状腺癌术后患者首次131碘清甲治疗效果的影响

目的:探讨治疗前血清甲状腺球蛋白(Tg)、甲状腺球蛋白抗体(Tg Ab)、血管内皮生长因子(VEGF)、巨噬细胞炎性蛋白-1α(MIP-1α)对分化型甲状腺癌术后患者首次131碘清甲治疗效果的影响。方法:选择2019年10月至2021年10月在我院接受诊治的分化型甲状腺癌患者120例作为甲状腺癌组,另选取同期在我院体检的健康体检者70例作为健康对照组,比较两组研究对象血清Tg、Tg Ab、VEGF、MIP-1α水平。甲状腺癌组患者术后实施首次131碘清甲治疗,根据治疗效果将患者分为清甲治疗成功组(n=75)、清甲治疗失败组(n=45),比较两组患者血清Tg、Tg Ab、VEGF、MIP-1α水平。采用单因素和多因素Logistic回归分析影响分化型甲状腺癌患者术后首次131碘清甲治疗成功率的危险因素。结果:甲状腺癌组血清Tg、Tg Ab、VEGF、MIP-1α水平均明显高于健康对照组(P<0.05)。清甲治疗成功组治疗前血清Tg、Tg Ab、VEGF、MIP-1α水平均明显低于清甲治疗失败组(P<0.05)。单因素分析结果显示,清甲治疗成功组与清甲治疗失败组性别、年龄、病理类型比较差异无统计学意义(P>0.05);两组131碘首次治疗前促甲状腺激素(TSH)水平、原发病灶直径、淋巴结远处转移、手术方式存在统计学差异(P<0.05)。多因素Logistic回归分析结果显示,131碘首次治疗前低TSH水平、原发病灶直径较大、存在淋巴结远处转移、甲状腺腺叶切除手术方式、治疗前高血清Tg水平、高血清Tg Ab水平、高血清VEGF水平、高血清MIP-1α水平是影响分化型甲状腺癌患者术后首次131碘清甲治疗成功率的独立危险因素(P<0.05)。结论:分化型甲状腺癌患者血清Tg、Tg Ab、VEGF、MIP-1α水平明显高于健康人群;低131碘首次治疗前TSH水平、原发病灶直径较大、出现淋巴结远处转移、甲状腺次全切手术方式、治疗前高血清Tg水平、高血清Tg Ab水平、高血清VEGF水平、高血清MIP-1α水平是影响分化型甲状腺癌患者术后首次131碘清甲治疗成功率的独立危险因素。

Cotransfecting norepinephrine transporter and vesicular monoamine transporter 2 genes for increased retention of metaiodobenzylguanidine labeled with iodine 131 in malignant hepatocarcinoma cells

Norepinephrine transporter （NET） transfection leads to significant uptake of iodine-131-labeled metaiodobenzylguanidine （^131I-MIBG） in non-neuroendocrine tumors. However, the use of ^131I-MIBG is limited by its short retention time in target cells. To prolong the retention of ^131I-MIBG in target cells, we infected hepatocarcinoma （HepG2） cells with Lentivirus-encoding human NET and vesicular monoamine transporter 2 （VMAT2） genes to obtain NET-expressing, NET-VMAT2-coexpressing, and negative-control cell lines. We evaluated the uptake and efflux of 131I-MIBG both in vitro and in vivo in mice bearing transfected tumors. NET- expressing and NET-VMAT2-coexpressing cells respectively showed 2.24 and 2.22 times higher ^131I-MIBG uptake than controls. Two hours after removal of ^131I-MIBG-containing medium, 25.4% efflux was observed in NET- VMAT2-coexpressing cells and 38.6% in NET-expressing cells. In vivo experiments were performed in nude mice bearing transfected tumors; results revealed that NET-VMAT2-coexpressing tumors had longer ^131I-MIBG retention time than NET-expressing tumors. Meanwhile, NET-VMAT2-coexpressing and NET-expressing tumors displayed 0.54% and 0.19%, respectively, of the injected dose per gram of tissue 24 h after ^131I-MIBG administration. Cotransfection of HepG2 cells with NET and VMAT2 resulted in increased ^131I-MIBG uptake and retention. However, the degree of increase was insufficient to be therapeutically effective in target cells.