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A novel fluorescence in situ hybridization assay for synovial sarcoma

机译:滑膜肉瘤的荧光原位杂交新方法

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Synovial sarcoma, which is difficult to diagnose precisely, is one of the most common childhood nonrhabdomyosarcoma soft-tissue sarcomas. The purpose of this study is to develop new molecular cytogenetic assay. We used two sets of two-color break-apart FISH probes, flanking either the SSX1/. SSX4 or SSX2 locus. Each set of probes is composed of differentially labeled DNA fragments complementary to sequences proximal or distal to the break point within the SSX1/. SSX4 or SSX2 locus, which are applied separately to histopathological sections. Interphase nuclei containing a translocation that disrupts either SSX1, SSX2, or SSX4 locus will display two single-color signals that have "broken apart" from each other. We applied it to two synovial sarcoma cell lines and clinical samples. This assay can detect translocation at either SSX1/. SSX4, or SSX2 locus on interphase spread prepared from synovial sarcoma cell line and histopathological sections, which is sufficient to diagnose as synovial sarcoma. Our new FISH assay has several advantages, including its applicability to paraffin-embedded samples, discrimination of the SS18- SSX1 and SS18- SSX2 translocations particularly in cases with aneuploidy, and potentially detecting translocations in all cases of synovial sarcoma, even with variant translocations. Our strategy will improve the accuracy of diagnoses, thereby facilitating appropriate treatment planning.
机译:滑膜肉瘤很难准确诊断,是儿童期最常见的非横纹肌肉瘤软组织肉瘤之一。这项研究的目的是开发新的分子细胞遗传学检测方法。我们使用了两组两色分开的FISH探针,两侧是SSX1 /。 SSX4或SSX2基因座。每组探针由与SSX1 /内断裂点近端或远端序列互补的差异标记的DNA片段组成。 SSX4或SSX2基因座,分别应用于组织病理学切片。包含破坏SSX1,SSX2或SSX4基因座的易位的相间核将显示两个彼此“分离”的单色信号。我们将其应用于两种滑膜肉瘤细胞系和临床样品。该测定法可以检测到SSX1 /处的易位。由滑膜肉瘤细胞系和组织病理学切片制备的SSX4或SSX2位点间扩散,足以诊断为滑膜肉瘤。我们的新FISH检测方法具有多个优势,包括其适用于石蜡包埋的样品,对SS18-SSX1和SS18-SSX2易位的辨别力(尤其是在非整倍性情况下),并有可能在所有滑膜肉瘤病例中检测到易位,即使变异易位。我们的策略将提高诊断的准确性,从而促进适当的治疗计划。

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