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Accuracy of tumor segmentation from multi-parametric prostate MRI and 18F-choline PET/CT for focal prostate cancer therapy applications

机译:多参数前列腺MRI和 18 F-胆碱PET / CT进行肿瘤分割在局灶性前列腺癌治疗中的准确性

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Background The study aims to assess the accuracy of multi-parametric prostate MRI (mpMRI) and~(18)F-choline PET/CT in tumor segmentation for clinically significant prostate cancer.~(18)F-choline PET/CT and 3?T mpMRI were performed in 10 prospective subjects prior to prostatectomy. All subjects had a single biopsy-confirmed focus of Gleason ≥?3+4 cancer. Two radiologists (readers 1 and 2) determined tumor boundaries based on in vivo mpMRI sequences, with clinical and pathologic data available.~(18)F-choline PET data were co-registered to T2-weighted 3D sequences and a semi-automatic segmentation routine was used to define tumor volumes. Registration of whole-mount surgical pathology to in vivo imaging was conducted utilizing two ex vivo prostate specimen MRIs, followed by gross sectioning of the specimens within a custom-made 3D-printed plastic mold. Overlap and similarity coefficients of manual segmentations (seg1, seg2) and~(18)F-choline-based segmented lesions (seg3) were compared to the pathologic reference standard. Results All segmentation methods greatly underestimated the true tumor volumes. Human readers (seg1, seg2) and the PET-based segmentation (seg3) underestimated an average of 79, 80, and 58% of the tumor volumes, respectively. Combining segmentation volumes (union of seg1, seg2, seg3?=?seg4) decreased the mean underestimated tumor volume to 42% of the true tumor volume. When using the combined segmentation with 5?mm contour expansion, the mean underestimated tumor volume was significantly reduced to 0.03?±?0.05?mL (2.04?±?2.84%). Substantial safety margins up to 11–15?mm were needed to include all tumors when the initial segmentation boundaries were drawn by human readers or the semi-automated~(18)F-choline segmentation tool. Combining MR-based human segmentations with the metabolic information based on~(18)F-choline PET reduced the necessary safety margin to a maximum of 9?mm to cover all tumors entirely. Conclusions To improve the outcome of focal therapies for significant prostate cancer, it is imperative to recognize the full extent of the underestimation of tumor volumes by mpMRI. Combining metabolic information from~(18)F-choline with MRI-based segmentation can improve tumor coverage. However, this approach requires confirmation in further clinical studies.
机译:背景技术本研究旨在评估多参数前列腺MRI(mpMRI)和〜(18)F-胆碱PET / CT在具有临床意义的前列腺癌的肿瘤分割中的准确性。〜(18)F-胆碱PET / CT和3?在前列腺切除术之前,对10位预期受试者进行了T mpMRI检查。所有受试者均经活检确认为格里森≥?3 + 4癌症。两名放射科医生(阅读器1和2)根据体内mpMRI序列确定了肿瘤边界,并获得了临床和病理数据。〜(18)F-胆碱PET数据与T2加权3D序列共配准,并进行了半自动分割常规用于定义肿瘤体积。使用两次离体前列腺标本MRI将整个手术病理与体内成像进行配准,然后在定制的3D打印塑料模具中对标本进行大体切片。将手动分割(seg1,seg2)和基于(18)F-胆碱的分割病变(seg3)的重叠和相似系数与病理参考标准进行比较。结果所有分割方法都大大低估了真实的肿瘤体积。人类读者(seg1,seg2)和基于PET的分割(seg3)分别低估了平均79%,80%和58%的肿瘤体积。组合分割体积(seg1,seg2,seg3?=?seg4的联合)可将平均被低估的肿瘤体积降低至真实肿瘤体积的42%。当使用轮廓扩展为5?mm的组合分割时,平均低估的肿瘤体积显着降低至0.03?±?0.05?mL(2.04?±?2.84%)。当人类阅读器或半自动〜(18)F-胆碱分割工具绘制初始分割边界时,包括所有肿瘤都需要达到11–15?mm的大量安全裕度。将基于MR的人体分割与基于〜(18)F-胆碱PET的代谢信息相结合,将必要的安全裕度降低到最大9?mm,以完全覆盖所有肿瘤。结论为改善重大前列腺癌的局灶性治疗结果,必须通过mpMRI充分认识肿瘤体积的低估。将〜(18)F-胆碱的代谢信息与基于MRI的分割相结合可以改善肿瘤的覆盖率。但是,这种方法需要进一步的临床研究证实。

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