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MTOR 通路突变与肾低级别嗜酸细胞瘤(LOT)诊断的一致性。

Concordance of MTOR Pathway Mutations and the Diagnosis of Renal Low-Grade Oncocytic Tumor (LOT).

机构信息

Department of Pathology, Brigham and Women's Hospital and Harvard Medical School, Boston, MA, USA.

Department of Pathology, Indiana University School of Medicine, Indianapolis, IN, USA.

出版信息

Int J Surg Pathol. 2024 Apr;32(2):316-330. doi: 10.1177/10668969231178032. Epub 2023 Jun 26.

DOI:10.1177/10668969231178032
Abstract

The differential diagnosis for oncocytic renal tumors spans the spectrum from benign entities to more aggressive renal cell carcinomas (RCC). Recent work has characterized a provisional renal oncocytic neoplasm, namely the low-grade oncocytic tumor (LOT), which demonstrates overlapping morphologic features with oncocytoma and chromophobe RCC, but also has a unique immunoprofile (ie, diffusely positive for KRT7, negative for KIT) and a high rate (80% to 100%) of mTOR pathway gene alterations. Given the diagnostic overlap among oncocytic tumors, we looked for concordance between mTOR pathway mutations and LOT. Thirty low-grade renal oncocytic neoplasms underwent histologic review and immunohistochemistry for KRT7 and KIT. Tumors were classified as "determinate" (eg, LOT) for tumors with solid, nested or vaguely tubular growth and diffuse KRT7 staining and negative KIT, or "indeterminate" if the morphology and/or immunostains did not fully support a definitive LOT diagnosis. Next-generation sequencing was performed without any knowledge of the diagnoses, and identified mTOR pathway mutations in 80% (12/15) of the determinate tumors, compared with 7% (1/15) in the indeterminate group. One determinate tumor was reclassified as papillary RCC ( mutation negative) and 6 indeterminate tumors were confirmed to be oncocytoma (N = 4), clear cell RCC or papillary RCC with reverse polarity, respectively. Overall, integration of morphology, immunohistochemistry, and molecular data enabled a final definitive diagnosis for 70% of tumors (21 of the total 30), with a high concordance (93%) for LOT specifically in the determinate group; the remaining 9 tumors (30%) were classified as renal oncocytic neoplasm, not otherwise specified.

摘要

肾嗜酸细胞瘤的鉴别诊断范围从良性肿瘤到更具侵袭性的肾细胞癌(RCC)。最近的研究已经确定了一种暂定的肾嗜酸细胞瘤,即低级别嗜酸细胞瘤(LOT),它与嗜酸细胞瘤和嫌色细胞 RCC 具有重叠的形态特征,但也具有独特的免疫表型(即,广泛表达 KRT7,不表达 KIT)和高比例(80%至 100%)的 mTOR 通路基因改变。鉴于嗜酸细胞瘤之间存在诊断重叠,我们研究了 mTOR 通路突变与 LOT 之间的一致性。30 例低级别肾嗜酸细胞瘤进行了组织学检查和 KRT7 和 KIT 的免疫组织化学检查。如果肿瘤具有实性、巢状或模糊管状生长以及弥漫性 KRT7 染色和阴性 KIT,则将其分类为“确定的”(例如 LOT);如果形态和/或免疫组化不能完全支持明确的 LOT 诊断,则将其分类为“不确定的”。进行了下一代测序,并且在 80%(12/15)的确定肿瘤中鉴定出了 mTOR 通路突变,而在不确定组中则为 7%(1/15)。1 例确定的肿瘤被重新分类为乳头状 RCC(突变阴性),6 例不确定的肿瘤分别被确认为嗜酸细胞瘤(N=4)、透明细胞 RCC 或具有反转极性的乳头状 RCC。总体而言,形态学、免疫组织化学和分子数据的综合分析使 70%的肿瘤(总共 30 个中的 21 个)获得了最终的明确诊断,特别是在确定组中 LOT 的一致性很高(93%);其余 9 个肿瘤(30%)被归类为未特指的肾嗜酸细胞瘤。

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