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TRIM63 is a sensitive and specific biomarker for MiT family aberration-associated renal cell carcinoma

机译:Trim63是一种敏感的和特异性生物标志物,用于MIT家族畸变相关的肾细胞癌

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Microphthalmia-associated transcription factor (MiT) family aberration-associated renal cell carcinoma (MiTF-RCC) is a subtype of renal cell carcinoma harboring recurrent chromosomal rearrangements involving TFE3 or TFEB genes. MiTF-RCC is morphologically diverse, can histologically resemble common RCC subtypes like clear cell RCC and papillary RCC, and often poses a diagnostic challenge in genitourinary clinical and pathology practice. To characterize the MiTF-RCC at the molecular level and identify biomarker signatures associated with MiTF-RCC, we analyzed RNAseq data from MiTF-RCC, other RCC subtypes and benign kidney. Upon identifying TRIM63 as a cancer-specific biomarker in MiTF-RCC, we evaluated its expression independently by RNA in situ hybridization (RNA-ISH) in whole tissue sections from 177 RCC cases. We specifically included 31 cytogenetically confirmed MiTF-RCC cases and 70 RCC cases suspicious for MiTF-RCC in terms of clinical and morphological features, to evaluate and compare TRIM63 RNA-ISH results with theresults from TFE3/TFEB fluorescence in situ hybridization (FISH), which is the current clinical standard. We confirmed that TRIM63 mRNA was highly expressed in all classes of MiTF-RCC compared to other renal tumor categories, where it was mostly absent to low. While the TRIM63 RNA-ISH and TFE3/TFEB FISH results were largely concordant, importantly, TRIM63 RNA-ISH was strongly positive in TFE3 FISH false-negative cases with RBM10-TFE3 inversion. In conclusion, TRIM63 can serve as a diagnostic marker to distinguish MiTF-RCC from other renal tumor subtypes with overlapping morphology. We suggest a combination of TFE3/TFEB FISH and TRIM63 RNA-ISH assays to improve the accuracy and efficiency of MiTF-RCC diagnosis. Accurate diagnosis of MiTF-RCC and other RCC subtypes would enable effective targeted therapy and avoid poor therapeutic response due to tumor misclassification.
机译:微蛋白相关的转录因子(MIT)家族像差相关的肾细胞癌(MITF-RCC)是肾细胞癌的亚型,涉及涉及TFE3或TFEB基因的复发性染色体重排。 MITF-RCC是形态样的,可以组织学类似地类似于透明细胞RCC和乳头状RCC等常见的RCC亚型,并且经常在泌尿族临床和病理学实践中造成诊断攻击。为了在分子水平下表征MITF-RCC并鉴定与MITF-RCC相关的生物标志物签名,我们分析了来自MITF-RCC,其他RCC亚型和良性肾脏的RNASEQ数据。在MITF-RCC中鉴定TRIM63作为癌症特异性生物标志物时,我们通过177 rCC案例的整个组织切片中的RNA在原位杂交(RNA-ISH)中独立评估其表达。我们特异性包括31种细胞遗传学证实的MITF-RCC病例和70例RCC病例在临床和形态学特征方面对MITF-RCC可疑,评价和比较TRE63 RNA-ISH结果,从TFE3 / TFEB荧光原位杂交(鱼),这是目前的临床标准。我们证实,与其他肾肿瘤类别相比,在所有类别的MITF-RCC中,TREM63 mRNA高度表达,其中它主要缺乏低点。虽然Trim63 RNA-ISH和TFE3 / TFEB鱼类结果很大,重要的是,Trim63 RNA ISH在TFE3鱼错误阴性病例中强烈阳性,RBM10-TFE3反转。总之,TRIM63可以用作诊断标志物,以区分MITF-RCC与具有重叠形态的肾肿瘤亚型的MITF-RCC。我们建议TFE3 / TFEB鱼和TRIM63 RNA-ISH测定的组合,提高MITF-RCC诊断的准确性和效率。准确诊断MITF-RCC和其他RCC亚型将使有效的靶向治疗能够避免由于肿瘤错误分类而导致的治疗反应差。

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