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DCE-MRI Radiomics Analysis in Differentiating Luminal A and Luminal B Breast Cancer Molecular Subtypes

机译:DCE-MRI 影像组学分析鉴别 Luminal A 和 Luminal B 乳腺癌分子亚型

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Rationale and Objectives: The aim of the present study was to investigate the association between Luminal A and Luminal B molecular subtypes and radiomic features of dynamic contrast-enhanced magnetic resonance imaging in patients with invasive breast cancer.Materials and Methods: Seventy-three patients with histopathologically proven invasive ductal cancer (IDC) were selected. Tumors were classified into molecular subtypes: Luminal A (estrogen receptor (ER)-positive and/or progesterone receptor (PR)-positive, human epider-mal growth factor receptor type 2 (HER2)-negative, proliferation marker Ki-6720). A total of 81 tumoral lesions were evaluated on T1-weighted fat-suppressed sagittal post-contrast late-phase MRI images after the required "pre-process" steps and 3D segmentations were made. Forty-three radiomic fea-tures including: 1 conventional, 4 shape, 6 histogram, 7 Grey-Level Co-occurrence Matrix (GLCM), 11 Grey-Level Run-Length Matrix (GLRLM), 3 Neighborhood Grey-Level Difference Matrix (NGLDM), 11 Grey-Level Zone-Length Matrix (GLZLM) were extracted by using the software LIFEX.Results: A statistically significant difference was found in radiomic features including; a) Histogram: "skewness", b) Shape: "volume-ml, volume-voxel," c) GLCM: "entropy.log10, entropy.log2, energy", d) GLRLM: "GLNU, RLNU, HGRE," e) NGLDM: "busyness," f) GLZLM: "GLNU, HGZE, ZLNU, SZE" between two different molecular subtypes. The model combining Shape-volume (ml) and GLZLM-HGZE yielded 0.746 area under the curve (AUC), 0.744 sensitivity, 0.643 specificity and 0.694 accuracy.Conclusion: Radiomic properties that may distinguish Luminal A and Luminal B molecular subtypes of IDC were identified. The radiomic features were thought to reflect the intratumoral heterogeneity in molecular subtypes. This study demonstrated that the characterization of Luminal A and Luminal B tumors could be made non-invasively by radiomics analysis.
机译:基本原理和目的:本研究的目的是探讨浸润性乳腺癌患者 Luminal A 和 Luminal B 分子亚型与动态对比增强磁共振成像的影像组学特征之间的关联。材料和方法: 选取 73 例经组织病理学证实的浸润性导管癌 (IDC) 患者。肿瘤分为分子亚型:管腔 A(雌激素受体 (ER) 阳性和/或孕激素受体 (PR) 阳性、人表皮生长因子受体 2 型 (HER2) 阴性、增殖标志物 Ki-6720)。在进行所需的“预处理”步骤和 3D 分割后,在 T1 加权脂肪抑制矢状面造影剂后期 MRI 图像上评估了总共 81 个肿瘤病灶。利用LIFEX软件提取了43个辐射组学特征,包括1个常规矩阵、4个形状矩阵、6个直方图、7个灰度共生矩阵(GLCM)、11个灰度游程矩阵(GLRLM)、3个邻域灰度差分矩阵(NGLDM)、11个灰度区域长度矩阵(GLZLM)。结果:在影像组学特征方面发现统计学上的显着差异,包括:a) 直方图:“偏度”,b) 形状:“体积-ml,体积-体素”,c) GLCM:“entropy.log10,熵。log2,能量“,d)GLLRLM:”GLNU,RLNU,HGRE“,e)NGLDM:”忙碌“,f)GLZLM:”GLNU,HGZE,ZLNU,SZE“在两种不同的分子亚型之间。结合形状-体积 (ml) 和 GLZLM-HGZE 的模型产生了 0.746 的曲线下面积 (AUC)、0.744 的灵敏度、0.643 的特异性和 0.694 的准确度。结论:鉴定了可区分IDC的Luminal A和Luminal B分子亚型的影像组学特性。影像组学特征被认为反映了分子亚型的瘤内异质性。本研究表明,通过影像组学分析可以无创地表征 Luminal A 和 Luminal B 肿瘤。

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