首页> 外文会议>IEEE International Symposium on Biomedical Imaging >IMPROVED AUTOMATED LOCALIZATION AND QUANTIFICATION OF PROTEIN MULTIPLEXES VIA MULTISPECTRAL FLUORESCENCE IMAGING IN HETEROGENOUS BIOPSY SAMPLES
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IMPROVED AUTOMATED LOCALIZATION AND QUANTIFICATION OF PROTEIN MULTIPLEXES VIA MULTISPECTRAL FLUORESCENCE IMAGING IN HETEROGENOUS BIOPSY SAMPLES

机译:通过多光谱荧光成像在异质活组织检查样品中改善自动定位和蛋白质多路复用的定量

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We present a novel improvement of our previously published image analysis system for the automated localization and quantification of protein biomarker expression in immunofluorescence (IF) microscopic images. The improvement has been developed primarily for biopsy based images which are by nature of variable quality and heterogeneous. The innovative method is employed for discriminating the biomarker signal from background, where signal may be the expression of multiple biomarkers or counterstains used in IF. The method is dynamic and it derives a threshold for a true biomarker signal based on the relationship between disease and non-disease tissue components. In addition, a new dynamic range feature construction is presented that is less affected by processing and other variations in tissue. The utility of the approach is demonstrated in predicting, based on the diagnostic biopsy tissue, prostate cancer disease progression within eight years after a radical prostatectomy. For this purpose, androgen receptor (AR) and Ki67 biomarker expression in prostate biopsy samples was quantified and features from the proposed approach were shown to be associated with disease progression in a univariate analysis and manifested improved performance over prior systems. Furthermore, AR and Ki67 features were selected in a multivariate model integrating clinical, histological, and biomarker features, proving their independent prognostic value.
机译:我们提出了我们先前发表的图像分析系统的新颖改进,用于免疫荧光(IF)显微图像中蛋白质生物标志物表达的自动定位和定量。改进主要是用于基于活检的图像的开发,这是可变质量和异质的性质。创新方法用于区分从背景中的生物标志物信号,其中信号可能是在IF中使用的多种生物标志物或备受宿主的表达。该方法是动态的,并且它基于疾病和非疾病组织成分之间的关​​系来衍生真正的生物标志物信号的阈值。此外,提出了一种新的动态范围特征结构,其受到组织的处理和其他变化的影响较小。该方法的效用在基于诊断活检组织,在激进前列腺切除术后八年内的前列腺癌疾病进展预测。为此目的,量化前列腺活检样品中的雄激素受体(Ar)和Ki67生物标志物表达被定量,并且从拟议方法中的特征显示出与单变量分析中的疾病进展相关,并表现出对先前系统的改进性能。此外,在多变量模型中选择Ar和Ki67特征,其集成临床,组织学和生物标志物特征,证明其独立的预后价值。

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