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首页> 外文期刊>American Journal of Surgical Pathology >PAX2 distinguishes benign mesonephric and mullerian glandular lesions of the cervix from endocervical adenocarcinoma, including minimal deviation adenocarcinoma.
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PAX2 distinguishes benign mesonephric and mullerian glandular lesions of the cervix from endocervical adenocarcinoma, including minimal deviation adenocarcinoma.

机译:PAX2可以将子宫颈的良性中肾和苗勒氏腺病变与宫颈内膜腺癌(包括最小偏差腺癌)区分开。

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摘要

Mesonephric remnants of the cervix are vestiges of the embryonic mesonephric system which typically regresses during female development. Uncommonly, hyperplasia of the mesonephric remnants may occur. The differential diagnosis of exuberant mesonephric hyperplasia includes minimal deviation adenocarcinoma of the cervix, a tumor with deceptively bland morphology for which no reliable diagnostic biomarkers currently exist. PAX2 encodes a transcription factor necessary in the development of the Wolffian duct system, and the protein is expressed in several tumors of mesonephric origin, including renal cell carcinoma, Wilm tumor, and nephrogenic adenoma. We hypothesized that PAX2 may also be expressed in mesonephric lesions of the cervix and may distinguish mesonephric hyperplasia from minimal deviation adenocarcinoma of the cervix. We demonstrated that PAX2 was strongly and diffusely expressed in mesonephric remnants (6 of 6) and in mesonephric hyperplasia (18 of 18); however, no expression was noted in mesonephric adenocarcinoma (0 of 1). PAX2 was expressed in normal endocervical glands (including tunnel clusters and Nabothian cysts) (86 of 86), lobular endocervical glandular hyperplasia (5 of 5), tubal/tuboendometrioid metaplasia (8 of 8), and cervical endometriosis (13 of 14). In contrast, only 2 cases of endocervical adenocarcinoma were positive for PAX2 [invasive adenocarcinoma of the minimal deviation type (0 of 5), usual type (1 of 22), and endometrioid type (1 of 1)]. Adjacent adenocarcinoma in situ, as well as cases of pure adenocarcinoma in situ (0 of 6), were also PAX2 negative. PAX2 expression in the 2 positive endocervical adenocarcinomas was patchy and weak. Most (11 of 15) stage II endometrial endometrioid adenocarcinomas lacked PAX2 expression but 1 of 10 grade 1 tumors and 3 of 5 grade 2 tumors did express PAX2. These results suggest that PAX2 immunoreactivity may be useful to (1) distinguish mesonephric hyperplasia from minimal deviation adenocarcinoma, (2) to distinguish lobular endocervical glandular hyperplasia from minimal deviation adenocarcinoma, and (3) to distinguish endocervical tubal metaplasia or cervical endometriosis from endocervical adenocarcinoma in situ. Overall, a strong, diffuse nuclear PAX2 expression pattern in a cervical glandular proliferation predicts a benign diagnosis (positive predictive value 90%, negative predictive value 98%; P<0.001); however, PAX2 should not be interpreted in isolation from the architectural and cytologic features of the lesion as it may be expressed in some stage II endometrial adenocarcinomas involving the cervix.
机译:子宫颈的中肾残余是胚胎中肾系统的痕迹,通常在女性发育过程中退化。罕见地,可能会发生中肾残余的增生。旺盛的中肾增生的鉴别诊断包括子宫颈的最小偏差腺癌,这是一种具有欺骗性温和形态的肿瘤,目前尚无可靠的诊断生物标志物。 PAX2编码在Wolffian管道系统发育中必需的转录因子,并且该蛋白在中肾起源的几种肿瘤中表达,包括肾细胞癌,Wilm肿瘤和肾原性腺瘤。我们假设PAX2也可能在子宫颈的中肾病变中表达,并且可能将子宫颈增生与子宫颈最小偏差腺癌区分开。我们证明PAX2在中肾残片(6中的6)和中肾增生(18中的18)中强烈而弥漫地表达。然而,在中肾腺癌中未发现任何表达(1中的0)。 PAX2在正常宫颈管腺体(包括隧道簇和纳博斯囊肿)中表达(86个中有86个),小叶宫颈内膜增生(5个中的5个),输卵管/肾小管内膜异位化生(8个中的8个)和宫颈内异症(14个中的13个)表达。相比之下,只有2例宫颈内膜腺癌PAX2阳性(最小偏差型(5分之0),普通型(22分之1)和子宫内膜样类型(1分之1)的浸润性腺癌]。相邻的原位腺癌以及纯原位腺癌(6个中的0个)病例也均为PAX2阴性。 2例阳性宫颈内腺癌中PAX2的表达不规则且微弱。大多数(15个中的11个)II期子宫内膜子宫内膜样腺癌缺乏PAX2表达,但是10个1级肿瘤中的1个和5个2级肿瘤中的3个确实表达了PAX2。这些结果表明,PAX2免疫反应性可能对(1)将中肾增生与最小偏差腺癌区分开来;(2)将小叶宫颈内膜增生与最小偏差腺癌区分开来;以及(3)从宫颈内膜腺癌中区分宫颈管内化生或宫颈内异症原地。总体而言,子宫颈腺增生中强烈的弥漫性核PAX2表达模式可预示良性诊断(阳性预测值90%,阴性预测值98%; P <0.001)。但是,PAX2不应与病变的结构和细胞学特征分开解释,因为它可能在某些涉及子宫颈的II期子宫内膜腺癌中表达。

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