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Spatial distribution of biopsy cores and the detection of intra-lesion pathologic heterogeneity

机译:活检核的空间分布及病变病理异质性的检测

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Objectives: The objective of this study was to determine if spatial distribution of multiparametric magnetic resonance imaging–transrectal ultrasound (mpMRI-TRUS) fusion biopsy cores to the index lesion reveals trends in the detection of intra-lesion Gleason heterogeneity and a more optimal prostate biopsy strategy. Methods: Index lesion was the lesion with longest diameter on T2-weighted (T2W)-MRI. In cohort 1, fusion biopsy cores biopsies were taken in areas in the center of the target as well as 1 cm laterally on each side. For cohort 2, targeted biopsies were taken from the center of the lesion only. Heterogeneity was defined as difference in maximum Gleason score obtained from fusion cores in the center of the index lesion versus cores obtained from the periphery (cohort 1), or any difference in maximum Gleason score obtained from fusion cores targeted to the index lesion (cohort 2) compared with systematic 12 cores TRUS biopsy. Results: Ninety-nine consecutive patients (35 and 64 in cohorts 1 and 2, respectively) with median age (SD) and prostate-specific antigen (PSA) of 66.9 (±5.9) and 9.7 (±8.2) respectively, were included. Age, PSA, Prostate Imaging Reporting and Data System (PI-RADS) score, and preoperative MRI lesion size were not significantly different between cohorts. Gleason heterogeneity was observed at a significantly higher rate in cohort 1 versus cohort 2 (58% versus 24%; p = 0.041). In cohort 1, cores obtained from the center of the lesion had higher Gleason score than cores obtained from the periphery of the targeted lesion in 57% of cases. Conclusions: We demonstrate that there is observable tumor heterogeneity in biopsy specimens, and that increased number of cores, as well as cores focused on the center and periphery of the largest lesion in the prostate, provide more comprehensive diagnostic information about the patient’s clinical risk category than taking nonspecific cores targeted within the tumor.
机译:目的:本研究的目的是确定多射磁共振成像 - 转基因超声(MPMRI-TRUS)融合活检核心对指数病变的空间分布揭示了病变内部肠道异质性的趋势和更良好的前列腺活组织检查战略。方法:指数损伤是T2加权(T2W)-MRI最长直径的病变。在群组1中,融合活检芯活组织检查在目标中心的区域中,每侧横向1厘米。对于群组2,仅从病变中心取出目标活组织检查。异质性被定义为从融合芯中从偏差核,与从周边(群组1)获得的核心,或者从归属于指数病变的融合核(COHORT 2的融合核心的最大肠道评分的任何差异(COHORT 2 )与系统的12个核心复活相比。结果:分别包括99例连续患者(分别为25和64例,分别为25和24例)中位年龄(SD)和前列腺特异性抗原(PSA)分别为66.9(±5.9)和9.7(±8.2)。年龄,PSA,前列腺成像报告和数据系统(PI-RADS)得分,并且术前MRI病变尺寸在群组之间没有显着差异。在群组1与队列2中以显着较高的速率观察到玻璃六件异质性(58%对24%; P = 0.041)。在队列1中,从病变中心获得的核心较高的Gleason得分,而不是在57%的病例中从靶位病变的周边获得的核心。结论:我们证明活组织检查标本中有可观察到的肿瘤异质性,并且核心增加的核心以及集中在前列腺中最大病变的中心和周边,为患者的临床风险类别提供了更全面的诊断信息而不是服用靶向靶向的非特异性核心。

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