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首页> 外文期刊>International journal of molecular medicine >A comprehensive analysis of RHOA mutation positive and negative angioimmunoblastic T-cell?lymphomas by targeted deep sequencing, expression profiling and single cell digital image analysis
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A comprehensive analysis of RHOA mutation positive and negative angioimmunoblastic T-cell?lymphomas by targeted deep sequencing, expression profiling and single cell digital image analysis

机译:综合分析RhoA突变阳性和负血管免疫瘤细胞β淋巴瘤通过靶向深序,表达分析和单细胞数字图像分析

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Angioimmunoblastic T?cell lymphoma (AITL) is a uniquely aggressive mature T?cell neoplasm. In recent years, recurrent genetic mutations in ras homolog family member A (RHOA), tet methylcytosine dioxygenase 2 (TET2), DNA methyltransferase 3 alpha (DNMT3A) and isocitrate dehydrogenase [NADP(+)] 2 (IDH2) have been identified as associated with AITL. However, a deep molecular study assessing both DNA mutations and RNA expression profile combined with digital image analysis is lacking. The present study aimed to evaluate the significance of molecular and morphologic features by high resolution digital image analysis in several cases of AITL. To do so, a total of 18 separate tissues from 10?patients with AITL were collected and analyzed. The results identified recurrent mutations in RHOA, TET2, DNMT3A, and IDH2, and demonstrated increased DNA mutations in coding, promoter and CCCTC binding factor (CTCF) binding sites in RHOA mutated AITLs vs. RHOA non?mutated cases, as well as increased overall survival in RHOA mutated patients. In addition, single cell computational digital image analysis morphologically characterized RHOA mutated AITL cells as distinct from cells from RHOA mutation negative patients. Computational analysis of single cell morphological parameters revealed that RHOA mutated cells have decreased eccentricity (more circular) compared with RHOA non?mutated AITL cells. In conclusion, the results from the present study expand our understanding of AITL and demonstrate that there are specific cell biological and morphological manifestations of RHOA mutations in cases of AITL.
机译:血管免疫汞细胞T?细胞淋巴瘤(AIT1)是一种唯一侵略性的成熟T 2细胞肿瘤。近年来,RAS同源物家庭成员A(RHOA),TET甲基胞嘧啶二氧化酶2(TET2),DNA甲基转移酶3α(DNMT3A)和异柠檬酸脱氢酶[NADP(+)] 2(IDH2)中的复发遗传突变已被确定为相关联与aitl。然而,缺乏评估DNA突变和RNA表达谱的深度分子研究与数字图像分析结合。本研究旨在评估通过高分辨率数字图像分析的分子和形态特征在几种Ait1例中进行重要性。为此,总共18个单独的组织来自10个?患有Ait1的患者被收集并分析。结果确定了RhOA,TET2,DNMT3A和IDH2中的复发突变,并证明了RHOA突变的AITLS中的编码,启动子和CCCTC结合因子(CTCF)结合位点的增加的DNA突变与RHOA非α突变的病例,以及总体增加RhoA突变患者的存活。此外,单细胞计算数字图像分析形态学地表征了RHOA突变的AIT1细胞,与来自rhOA突变阴性患者的细胞不同。单细胞形态学参数的计算分析表明,与RhOA非致抗Ait1细胞相比,RHOA突变细胞具有降低的偏心率(更圆形)。总之,本研究的结果扩大了我们对AIT1的理解,并证明了在AIT1的情况下有rhOA突变的细胞生物学和形态学表现。

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