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宫颈上皮内瘤变:活检与免疫组织化学

Cervical Pre-cancers: Biopsy and Immunohistochemistry.

作者信息

Kamal Meherbano

机构信息

Department of Pathology, Government Medical College, Nagpur, Maharashtra, India.

出版信息

Cytojournal. 2022 Jun 14;19:38. doi: 10.25259/CMAS_03_13_2021. eCollection 2022.

Abstract

The existence of precursor lesions for invasive cervical cancer has been recognized for more than 50 years. Our understanding of the pathobiology and behavior of cervical cancer precursors has evolved considerably over the past five decades. Furthermore, the terminology used to classify pre-invasive lesions of the cervix has frequently changed. The realization that human papillomavirus (HPV) infections constitute a morphologic continuum has prompted efforts to include them within a single classification system, specifically the squamous intraepithelial lesions (SILs) which have now been embraced by the surgical pathologists. The reduced number of specific pathological categories has made clinical decision-making more straightforward. The generic criteria for SIL have two important histological parameters: Alterations in the density of superficial epithelial cells and superficial squamous atypia. The flat condyloma or cervical intraepithelial neoplasia (CIN) I is generally associated with intermediate and high-risk HPV types as against the low-risk viruses that cause exophytic/papillary growth patterns of condylomas. The diagnosis of low-grade SIL (LSIL) (flat and exophytic condylomas) requires first excluding benign mimics of LSIL and second to confirm the characteristic cytologic atypia. For high-grade SILs (HSILs), the extent and degree of atypia generally exceed the limits of that described in flat or exophytic condylomas (LSILs). Less maturation, abnormal cell differentiation, loss of cell polarity, and increased mitotic index with abnormal mitotic figures occupying increasing thickness of the epithelium define a lesion as CIN II or CIN III. Atypical immature metaplasia associated with inflammation and atrophy is a challenge in cervical biopsy interpretation. Careful attention to the growth pattern of the epithelium, the distribution of the atypia, nuclear spacing, and the degree of anisokaryosis and the presence of enlarged hyperchromatic nuclei help in differentiating a non-neoplastic from a neoplastic process. This chapter describes in depth the diagnostic difficulties in the interpretation of cervical biopsies. It also provides useful criteria in distinguishing benign mimics from true precancerous lesions and the role of biomarkers such as the p16ink4 and Ki-67 in the differential diagnosis of precursor lesions and the reactive and metaplastic epithelium.

摘要

浸润性宫颈癌前体病变的存在已被认识超过50年。在过去的五十年里,我们对宫颈癌前体病变的病理生物学和行为的理解有了很大的发展。此外,用于对宫颈浸润前病变进行分类的术语也经常变化。认识到人类乳头瘤病毒(HPV)感染构成一种形态学连续体,促使人们努力将其纳入单一分类系统,特别是外科病理学家现在所采用的鳞状上皮内病变(SILs)。特定病理类别的减少使临床决策更加直接。SIL的通用标准有两个重要的组织学参数:表层上皮细胞密度的改变和表层鳞状细胞异型性。扁平湿疣或宫颈上皮内瘤变(CIN)I通常与中、高危HPV类型相关,而导致湿疣外生性/乳头状生长模式的是低危病毒。低级别SIL(LSIL)(扁平湿疣和外生性湿疣)的诊断首先需要排除LSIL的良性模仿病变,其次要确认特征性的细胞学异型性。对于高级别SIL(HSIL),异型性的范围和程度通常超过扁平或外生性湿疣(LSIL)中所描述的限度。成熟度降低、细胞分化异常、细胞极性丧失以及有丝分裂指数增加且异常有丝分裂象占据上皮层厚度增加,将病变定义为CIN II或CIN III。与炎症和萎缩相关的非典型未成熟化生是宫颈活检解读中的一个挑战。仔细关注上皮的生长模式、异型性的分布、核间距、核大小不均程度以及是否存在增大的深染核,有助于区分非肿瘤性过程和肿瘤性过程。本章深入描述了宫颈活检解读中的诊断困难。它还提供了区分良性模仿病变与真正癌前病变的有用标准,以及生物标志物如p16ink4和Ki-67在鉴别前体病变与反应性和化生上皮中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c03b/9345137/d2a6f1a34385/Cytojournal-19-38-g001.jpg

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