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甲状腺细胞病理学中意义不明确的非典型病变相关的恶性风险及可重复性。

Malignancy risk and reproducibility associated with atypia of undetermined significance on thyroid cytology.

作者信息

Mathur Aarti, Najafian Alireza, Schneider Eric B, Zeiger Martha A, Olson Matthew T

机构信息

Department of Surgery, Johns Hopkins University School of Medicine, Baltimore, MD.

Department of Pathology, Johns Hopkins University School of Medicine, Baltimore, MD.

出版信息

Surgery. 2014 Dec;156(6):1471-6; discussion1476. doi: 10.1016/j.surg.2014.08.026. Epub 2014 Sep 11.

Abstract

BACKGROUND

The Bethesda System for Reporting Thyroid Cytopathology (TBSRTC) describes several subcategories within atypia of undetermined significance (AUS), including (1) presence of focal nuclear atypia (AUS-N), (2) focal microfollicular proliferation (AUS-F), (3) focal Hürthle cell proliferation (AUS-HC), and (4) other (AUS-O). Several publications suggest that 5-15% is an underestimate of the malignancy risk for AUS, and that the underestimation is owing to the similarity between AUS-N and suspicious for malignancy (SFM). Thus, we investigated the AUS subcategories during morphologic re-review at a tertiary care center and their associated malignancy risk.

METHODS

Of 4,827 fine-needle aspiration specimens were sent between January 2009 and August 2013 for morphologic re-review, 806 were categorized as AUS. Comparison of AUS subcategory diagnoses were made between outside and re-review results. The malignancy risk was also determined for 255 nodules with available surgical pathology.

RESULT

The outside diagnoses of the 806 cases read as AUS on second review were as follows: 5 insufficient (0.1%), 149 benign (19%), 463 AUS (57%), 124 SFN or suspicious for follicular or Hürthle cell neoplasm (15%), 56 SFM (7%), and 9 malignant (1%). Of the 463 cases in which both the outside and re-review diagnosis was AUS, the distribution of the subcategories in order of increasing frequency was 53 AUS-HC (11%), 74 AUS-O (16%), 79 AUS-F (17%), and 257 AUS-N (56%). Of the 255 resected nodules, 99 (39%) were malignant. Subcategory malignancy rates were: AUS-HC, 19% (9/47); AUS-O, 26% (14/54); AUS-F, 39% (19/49); and AUS-N, 54% (57/105). Cases in which both the referring institution and re-review agreed about the AUS-N subcategory had an even greater risk of malignancy (68%; 17/25).

CONCLUSION

Disagreement about the diagnosis of AUS between institutions is frequent. The malignancy risk for AUS is higher than originally proposed by TBSRTC and attributable to the high risk of AUS-N. Furthermore, agreement on AUS-N after re-review portends a malignancy risk that borders on that of SFM. This suggests that AUS-N may have discrete features that can provide specific morphologic predictors and enable the consolidation of AUS-N into SFM.

摘要

背景

甲状腺细胞病理学报告的贝塞斯达系统(TBSRTC)描述了意义不明确的非典型病变(AUS)中的几个亚类,包括(1)局灶性核非典型性(AUS-N),(2)局灶性微滤泡增生(AUS-F),(3)局灶性许特耳细胞增生(AUS-HC),以及(4)其他(AUS-O)。一些出版物表明,5%-15%低估了AUS的恶性风险,并且这种低估是由于AUS-N与恶性可疑(SFM)之间的相似性。因此,我们在一家三级医疗中心对AUS亚类进行了形态学复查,并研究了其相关的恶性风险。

方法

在2009年1月至2013年8月期间送去进行形态学复查的4827份细针穿刺标本中,806份被归类为AUS。比较了外部诊断与复查结果之间AUS亚类的诊断情况。还确定了255个有可用手术病理结果的结节的恶性风险。

结果

806例在二次复查时被诊断为AUS的病例,其外部诊断结果如下:5例不足(0.1%),149例良性(19%),463例AUS(57%),124例滤泡性或许特耳细胞瘤可疑或可疑滤泡性或许特耳细胞瘤(15%),56例SFM(7%),以及9例恶性(1%)。在外部诊断和复查诊断均为AUS的463例病例中,亚类分布按频率增加顺序为:53例AUS-HC(11%),74例AUS-O(16%),79例AUS-F(17%),以及257例AUS-N(56%)。在255个切除的结节中,99个(39%)为恶性。亚类恶性率分别为:AUS-HC,19%(9/47);AUS-O,26%(14/54);AUS-F,39%(19/49);以及AUS-N,54%(57/105)。转诊机构和复查机构对AUS-N亚类诊断一致的病例具有更高的恶性风险(68%;17/25)。

结论

机构之间对AUS诊断的分歧很常见。AUS的恶性风险高于TBSRTC最初提出的风险,并且归因于AUS-N的高风险。此外,复查后对AUS-N的一致诊断预示着接近SFM的恶性风险。这表明AUS-N可能具有离散特征,可提供特定的形态学预测指标,并使AUS-N能够合并到SFM中。

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