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首页> 外文期刊>Thyroid: official journal of the American Thyroid Association >Clinical Applicability of Low Levels of Thyroglobulin Autoantibodies as Cutoff Point for Thyroglobulin Autoantibody Positivity
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Clinical Applicability of Low Levels of Thyroglobulin Autoantibodies as Cutoff Point for Thyroglobulin Autoantibody Positivity

机译:低水平甲状腺素自身抗体作为甲状腺素自身抗体阳性截止点的临床适用性

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摘要

Background: Thyroglobulin (Tg) is an established tumor marker in differentiated thyroid carcinoma (DTC). However, Tg assays can be subject to interference by autoantibodies against Tg (TgAbs). No clinical consensus exists on the cutoff value of TgAb positivity and its relationship to Tg assay interference. The aims of this study were to investigate the most applicable cutoff value for TgAb positivity in clinical practice and to evaluate whether tumor characteristics differ between TgAb+ and TgAb? patients during ablation therapy using the manufacturer's cutoff (MCO) and institutional cutoff (ICO). Methods: This single-center cohort study included 230 DTC patients diagnosed between January 2006 and December 2014. Serum Tg and TgAbs were measured with the Tg-IRMA (Thermo Fisher Scientific) and ARCHITECT Anti-Tg (Abbott Laboratories) assays. Patients were divided into TgAb? and TgAb+ based on the limit of detection (LoD; ≥0.07 IU/mL), functional sensitivity (FS; ≥0.31 IU/mL), MCO (≥4.11 IU/mL), and ICO (≥10 IU/mL). Results: All patients were TgAb+ based on the LoD; one patient was negative on FS. Fifty-five (23.9%) and 34 (14.8%) patients had TgAbs above the MCO and ICO, respectively. Histology, presence of multifocality, tumor-node-metastasis, and American Thyroid Assocation risk stratification did not differ between TgAb? and TgAb+ patients using MCO and ICO during ablation. Conclusions: This study supports the use of a higher cutoff value than that of the FS for TgAb positivity in clinical settings. The LoD and FS are too sensitive to discriminate TgAb positivity and negativity in DTC patients during ablation therapy. The presence of TgAbs during ablation is not related to tumor characteristics and risk profile. This implies that TgAb positivity should not be considered a separate risk factor.
机译:背景:甲状腺球蛋白(Tg)是分化的甲状腺癌(DTC)中的已建立的肿瘤标志物。然而,TG测定可以受到针对TG(TGAB)的自身抗体的干扰。在TGAB阳性的截止值及其与TG测定干扰的关系中不存在临床共识。本研究的目的是研究临床实践中TGAB积极性最适用的截止值,并评估肿瘤特性是否在TGAB +和TGAB之间存在差异?使用制造商的截止(MCO)和机构截止(ICO)的消融治疗患者。方法:该单中心队列研究包括230名诊断为2006年1月至2014年12月的DTC患者。用TG-IRMA(Thermo Fisher Scientific)和建筑师反TG(Abbott Laboratories)测定来测量血清TG和TGAB。患者分为TGAB?和TGAB +基于检测限(LOD;≥0.07IU / mL),功能敏感性(FS;≥0.31IU/ mL),MCO(≥4.11IU / mL)和ICO(≥10IU / mL)。结果:所有患者均为基于LOD的TGAB +;一个患者对FS负阴性。五十五(23.9%)和34名(14.8%)患者分别在MCO和ICO上方有TGAB。组织学,多焦点,肿瘤节点转移和美国甲状腺缔合风险分层的存在在TGAB之间没有区别?和TGAB +患者在消融期间使用MCO和ICO。结论:本研究支持使用临床环境中TGAB积极性的FS的截止值更高的截止值。 LOD和FS对消融治疗期间DTC患者中的TGAB阳性和消极性太敏感。消融期间TGAB的存在与肿瘤特征和风险概况无关。这意味着TGAB阳性不应被认为是单独的危险因素。

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