[SMARCB1(INI1)-deficient renal cell carcinoma: medullary and beyond : Evolving concepts].

4区 医学 Q3 Medicine Pathologe Pub Date : 2021-11-01 Epub Date: 2021-10-05 DOI:10.1007/s00292-021-00985-y
Abbas Agaimy, Arndt Hartmann
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引用次数: 1

Abstract

During the last decades, the SWI/SNF chromatin-remodeling complex has received enormous recognition as a major player in the molecular pathogenesis of diverse neoplasms. Accordingly, SWI/SNF defects affecting different subunits of the complex became defining genetic features in the nosology of different neoplastic entities. In the kidney, loss of SMARCB1(INI1) as a major component of the SWI/SNF complex has emerged as the defining genetic marker for renal medullary carcinoma and pediatric malignant rhabdoid tumor. Diagnosis of these two rare entities is based on a set of defined demographic, clinicopathological, immunophenotypic, and genetic (SMARCB1 loss) criteria. Moreover, the sickle cell trait is considered a prerequisite for renal medullary carcinoma. Current knowledge illustrates that SMARCB1 loss is encountered in three major tumor categories in the kidney: (1) histologically defined neoplasms that are primarily driven by de novo SMARCB1 loss (renal medullary carcinoma and malignant rhabdoid tumor); (2) SMRACB1-deficient renal cell carcinoma (RCC) with variable non-specific histology ranging from collecting duct-like, papillary high-grade (papillary type 2), or medullary-like (lacking sickle cell trait), to fully undifferentiated; and (3) biphasic (dedifferentiated) RCC showing a variable SMARCB1-deficient undifferentiated component. The latter variant most frequently originates from pre-existing clear cell RCC but may rarely superimpose on papillary or chromophobe RCC. This review summarizes the major defining features of the emerging SMARCB1-deficient renal neoplasms. All SMARCB1-deficient carcinomas have a poor prognosis in common. Therefore, exact diagnosis of these tumors is a prerequisite for studies investigating new therapies.

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[SMARCB1(INI1)缺陷肾细胞癌:髓质及其他:不断发展的概念]。
在过去的几十年里,SWI/SNF染色质重塑复合体在多种肿瘤的分子发病机制中扮演着重要的角色,这一点已经得到了广泛的认可。因此,影响该复合体不同亚基的SWI/SNF缺陷在不同肿瘤实体的分类学中成为决定性的遗传特征。在肾脏中,SMARCB1(INI1)作为SWI/SNF复合物的主要组成部分的缺失已经成为肾髓样癌和儿童恶性横纹肌样肿瘤的决定性遗传标记。这两种罕见的实体的诊断是基于一套定义的人口统计学,临床病理,免疫表型和遗传(SMARCB1丢失)标准。此外,镰状细胞特征被认为是肾髓质癌的先决条件。目前的知识表明,SMARCB1的丢失主要发生在三种主要的肾脏肿瘤中:(1)组织学上确定的主要由新生SMARCB1丢失驱动的肿瘤(肾髓样癌和恶性横纹肌样瘤);(2) smracb1缺陷型肾细胞癌(RCC)具有可变的非特异性组织学,从收集管状,乳头状高级别(乳头状2型)或髓样(缺乏镰状细胞特征)到完全未分化;(3)双相(去分化)RCC显示可变的缺乏smarcb1的未分化成分。后一种变异最常起源于已有的透明细胞RCC,但可能很少叠加在乳头状或憎色细胞RCC上。本文综述了新出现的smarcb1缺陷肾肿瘤的主要特征。所有smarcb1缺陷癌都有一个共同的不良预后。因此,准确诊断这些肿瘤是研究新疗法的先决条件。
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来源期刊
Pathologe
Pathologe 医学-病理学
CiteScore
1.50
自引率
0.00%
发文量
40
审稿时长
4-8 weeks
期刊介绍: Der Pathologe is an internationally recognized journal and combines practical relevance with scientific competence. The journal informs all pathologists working on departments and institutes as well as morphologically interested scientists about developments in the field of pathology. The journal serves both the scientific exchange and the continuing education of pathologists. Comprehensive reviews on a specific topical issue focus on providing evidenced based information under consideration of practical experience. Freely submitted original papers allow the presentation of important clinical studies and serve the scientific exchange.
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