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Treatment of acute hypernatremia in severely burned patients using continuous veno-venous hemofiltration with gradient sodium replacement fluid: A report of nine cases

机译:梯度钠替代液持续静脉静脉血液滤过治疗重度烧伤患者急性高钠血症9例报告

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Purpose: The objective of the study was to validate an adaptive, contrast-oriented thresholding algorithm (COA) for tumour delineation in 18F-fluorodeoxyglucose (FDG) positron emission tomography (PET) for non-small cell lung cancer (NSCLC) in comparison with pathological findings. The impact of tumour localization, tumour size and uptake heterogeneity on PET delineation results was also investigated. Methods: PET tumour delineation by COA was compared with both CT delineation and pathological findings in 15 patients to investigate its validity. Correlations between anatomical volume, metabolic volume and the pathology reference as well as between the corresponding maximal diameters were determined. Differences between PET delineations and pathological results were investigated with respect to tumour localization and uptake heterogeneity. Results: The delineated volumes and maximal diameters measured on PET and CT images significantly correlated with the pathology reference (both r 0.95, p 0.0001). Both PET and CT contours resulted in overestimation of the pathological volume (PET 32.5 ± 26.5 %, CT 46.6 ± 27.4 %). CT volumes were larger than those delineated on PET images (CT 60.6 ± 86.3 ml, PET 48.3 ± 61.7 ml). Maximal tumour diameters were similar for PET and CT (51.4 ± 19.8 mm for CT versus 53.4 ± 19.1 mm for PET), slightly overestimating the pathological reference (mean difference CT 4.3 ± 3.2 mm, PET 6.2 ± 5.1 mm). PET volumes of lung tumours located in the lower lobe were significantly different from those determined from pathology (p = 0.037), whereas no significant differences were observed for tumours located in the upper lobe (p = 0.066). Only minor correlation was found between pathological tumour size and PET heterogeneity (r = -0.24). Conclusion: PET tumour delineation by COA showed a good correlation with pathological findings. Tumour localization had an influence on PET delineation results. The impact of tracer uptake heterogeneity on PET delineation should be considered carefully and individually in each patient. Altogether, PET tumour delineation by COA for NSCLC patients is feasible and reliable with the potential for routine clinical application.
机译:目的:本研究的目的是与非小细胞肺癌(NSCLC)相比,验证一种适用于18F-氟脱氧葡萄糖(FDG)正电子发射断层扫描(PET)中肿瘤定位的自适应,对比导向的阈值算法(COA)病理结果。还研究了肿瘤定位,肿瘤大小和摄取异质性对PET勾画结果的影响。方法:比较15例患者的COA PET轮廓线与CT轮廓线和病理结果,以探讨其有效性。确定了解剖体积,代谢体积和病理参考之间的相关性,以及相应的最大直径之间的相关性。在肿瘤定位和摄取异质性方面,研究了PET轮廓与病理结果之间的差异。结果:在PET和CT图像上测得的轮廓体积和最大直径与病理参考显着相关(r> 0.95,p <0.0001)。 PET和CT等高线均导致高估了病理体积(PET 32.5±26.5%,CT 46.6±27.4%)。 CT体积大于PET图像上描绘的体积(CT 60.6±86.3 ml,PET 48.3±61.7 ml)。 PET和CT的最大肿瘤直径相似(CT为51.4±19.8 mm,PET为53.4±19.1 mm),略高估了病理参考值(平均差CT为4.3±3.2 mm,PET为6.2±5.1 mm)。位于下叶的肺部肿瘤的PET体积与根据病理学确定的PET体积显着不同(p = 0.037),而位于上叶的肺部肿瘤的PET体积无明显差异(p = 0.066)。在病理性肿瘤大小和PET异质性之间仅发现很小的相关性(r = -0.24)。结论:COA对PET肿瘤的描绘与病理结果具有良好的相关性。肿瘤定位对PET描绘结果有影响。示踪剂摄取异质性对PET轮廓的影响应在每位患者中仔细考虑和单独考虑。总之,COA对NSCLC患者的PET肿瘤勾画是可行和可靠的,具有常规临床应用的潜力。

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