Subscribe to RSS
Download PDF
DOI: 10.1055/s-0032-1312860
Lung, Liver and Lymph Node Metastases in Follow-Up MSCT: Comprehensive Volumetric Assessment of Lesion Size Changes
Lungen-, Leber- und Lymphknotenmetastasen in der MSCT Verlaufskontrolle: umfassende volumetrische Analyse von LäsionsgrößenänderungenPublication History
26 September 2011
20 April 2012
Publication Date:
07 August 2012 (online)
Abstract
Purpose: To investigate measurement accuracy in terms of precision and inter-rater variability in the simultaneous volumetric assessment of lung, liver and lymph node metastasis size change over time in comparison to RECIST 1.1.
Materials and Methods: Three independent readers evaluated multislice CT data from clinical follow-up studies (chest/abdomen) in 50 patients with metastases. A total of 117 lung, 77 liver and 97 lymph node metastases were assessed manually (RECIST 1.1) and by volumetry with semi-automated software. The quality of segmentation and need for manual adjustments were recorded. Volumes were converted to effective diameters to allow comparison to RECIST. For statistical assessment of precision and interobserver agreement, the Wilcoxon-signed rank test and Bland-Altman plots were utilized.
Results: The quality of segmentation after manual correction was acceptable to excellent in 95 % of lesions and manual corrections were applied in 21 – 36 % of all lesions, most predominantly in lymph nodes. Mean precision was 2.6 – 6.3 % (manual) with 0.2 – 1.5 % (effective) relative measurement deviation (p <.001). Inter-reader median variation coefficients ranged from 9.4 – 12.8 % (manual) and 2.9 – 8.2 % (volumetric) for different lesion types (p < .001). The limits of agreement were ± 9.8 to ± 11.2 % for volumetric assessment.
Conclusion: Superior precision and inter-rater variability of volumetric over manual measurement of lesion change over time was demonstrated in a whole body setting.
Zusammenfassung
Ziel: Erforschung von Messgenauigkeit im Hinblick auf Präzision und Inter-Observer-Variabilität der gleichzeitigen volumetrischen Untersuchung der Größenänderung im Follow-up von Lungen-, Leber- und Lymphknotenmetastasen im Vergleich zu RECIST 1.1.
Material und Methoden: 3 unabhängige Radiologen untersuchten Multislice-CT-Daten von 50 Patienten mit Metastasen aus klinischen Verlaufsuntersuchungen (Thorax/Abdomen). Insgesamt wurden 117 Lungen-, 77 Lebermetastasen und 97 Lymphknoten manuell (RECIST 1.1) und volumetrisch mit einer halbautomatischen Software vermessen. Die Qualität der Segmentation und der Einsatz manueller Nachverarbeitung wurden erfasst. Volumina wurden in Effektivdurchmesser umgewandelt, um sie direkt mit RECIST vergleichen zu können. Zur statistischen Analyse von Präzision und Inter-Observer-Variabilität wurden Wilcoxon-Vorzeichen-Rangtest und Bland-Altman Diagramme verwendet.
Ergebnisse: Die Qualität der Segmentation nach manueller Korrektur wurde als akzeptabel bis hervorragend in 95 % bewertet, manuelle Korrekturen in 21 – 36 % aller Läsionen vorgenommen, am häufigsten an Lymphknoten. Mittlere Präzision war 2,3 – 6,3 % (manuell) und 0,2 – 1,5 % (Effektivdurchmesser) relative Messwert-Abweichung (p < 0,001). Mediane Inter-Observer-Variabilität lag im Bereich von 9,4 – 12,8 % (manuell) und 2,9 – 8,2 % (volumetrisch) in verschiedenen Läsionskategorien (p < 0,001). Limits of Agreement waren ± 9,8 bis ± 11,2 % in der volumetrischen Analyse.
Schlussfolgerung: Volumetrische Messung der Größenänderungen im Follow-up zeigte eine signifikante Verbesserung von Präzision und Inter-Observer-Variabilität gegenüber manueller Messung im untersuchten Ganzkörperparadigma.
-
References
- 1 Eisenhauer EA, Therasse P, Bogaerts J et al. New response evaluation criteria in solid tumours: revised RECIST guideline (version 1.1). Eur J Cancer 2009; 45: 228-247
- 2 Gebauer B, Bohnsack O, Riess H. Radiologische Evaluation des Tumoransprechens in onkologischen Therapiestudien (Tumor Response Evaluation). Fortschr Röntgenstr 2011; 183: 695-703
- 3 Schwartz LH, Mazumdar M, Brown W et al. Variability in response assessment in solid tumors: effect of number of lesions chosen for measurement. Clin Cancer Res 2003; 9: 4318-4323
- 4 Erasmus JJ, Gladish GW, Broemeling L et al. Interobserver and intraobserver variability in measurement of non-small-cell carcinoma lung lesions: implications for assessment of tumor response. J Clin Oncol 2003; 21: 2574-2582
- 5 Wormanns D, Kohl G, Klotz E et al. Volumetric measurements of pulmonary nodules at multi-row detector CT: in vivo reproducibility. Eur Radiol 2004; 14: 86-92
- 6 Hein PA, Romano VC, Rogalla P et al. Linear and volume measurements of pulmonary nodules at different CT dose levels – intrascan and interscan analysis. Fortschr Röntgenstr 2009; 181: 24-31
- 7 Vogel MN, Vonthein R, Schmücker S et al. Lungenrundherdvolumetrie mit optimiertem Segmentierungsalgorithmus. Genauigkeit bei verschiedenen Schichtdicken verglichen mit ein- und zweidimensionalen Messungen. Fortschr Röntgenstr 2008; 180: 791-797
- 8 Keil S, Behrendt FF, Stanzel S et al. Semi-automated measurement of hyperdense, hypodense and heterogeneous hepatic metastasis on standard MDCT slices. Comparison of semi-automated and manual measurement of RECIST and WHO criteria. Eur Radiol 2008; 18: 2456-2465
- 9 Puesken M, Buerke B, Fortkamp R et al. Liver Lesion Segmentation in MSCT: Effect of Slice Thickness on Segmentation Quality, Measurement Precision and Interobserver Variability. Fortschr Röntgenstr 2011; 183: 372-380
- 10 Rothe JH, Steffen IG, Lehmkuhl L et al. Volume measurement of liver metastases using multidetector computed tomography: comparison of lesion diameter and volume segmentation – a phantom study. Fortschr Röntgenstr 2010; 182: 1082-1090
- 11 Keil S, Behrendt FF, Stanzel S et al. RECIST and WHO criteria evaluation of cervical, thoracic and abdominal lymph nodes in patients with malignant lymphoma: manual versus semi-automated measurement on standard MDCT slices. Fortschr Röntgenstr 2009; 181: 888-895
- 12 Fabel M, von Tengg-Kobligk H, Giesel FL et al. Semi-automated volumetric analysis of lymph node metastases in patients with malignant melanoma stage III/IV – a feasibility study. Eur Radiol 2008; 18: 1114-1122
- 13 Fabel M, Bolte H, von Tengg-Kobligk H et al. Semi-automated volumetric analysis of lymph node metastases during follow-up-initial results. Eur Radiol 2011; 21: 683-692
- 14 Bauknecht H, Romano VC, Rogalla P et al. Intra- and interobserver variability of linear and volumetric measurements of brain metastases using contrast-enhanced magnetic resonance imaging. Invest Radiol 2010; 45: 49-56
- 15 Kostis WJ, Yankelevitz DF, Reeves AP et al. Small pulmonary nodules: reproducibility of three-dimensional volumetric measurement and estimation of time to follow-up CT. Radiology 2004; 231: 446-452
- 16 Heussel CP, Meier S, Wittelsberger S et al. Quantitative CT-Verlaufskontrolle von Lebermalignomen nach RECIST und WHO im Vergleich zur Volumetrie. Fortschr Röntgenstr 2007; 179: 958-964
- 17 Kalkmann J, Ladd S, de Greiff A et al. Suitability of Semi-Automated Tumor Response Assessment of Liver Metastases using a Dedicated Software Package. Fortschr Röntgenstr 2010; 182: 581-588
- 18 Moltz JH, Bornemann L, Kuhnigk J et al. Advanced Segmentation Techniques for Lung Nodules, Liver Metastases, and Enlarged Lymph Nodes in CT Scans. IEEE J Sel Top Signal Process 2009; 3: 122-134
- 19 Bland JM, Altman DG. Statistical methods for assessing agreement between two methods of clinical measurement. Lancet 1986; 1: 307-310
- 20 Buerke B, Puesken M, Beyer F et al. Semiautomatic lymph node segmentation in multislice computed tomography: impact of slice thickness on segmentation quality, measurement precision, and interobserver variability. Invest Radiol 2010; 45: 82-88
- 21 Bolte H, Riedel C, Müller-Hülsbeck S et al. Precision of computer-aided volumetry of artificial small solid pulmonary nodules in ex vivo porcine lungs. Br J Radiol 2007; 80: 414-421
- 22 de Hoop B, Gietema H, van Ginneken B et al. A comparison of six software packages for evaluation of solid lung nodules using semi-automated volumetry: what is the minimum increase in size to detect growth in repeated CT examinations. Eur Radiol 2009; 19: 800-808
- 23 Hahn S, Heusner T, Zhou X et al. Computer-aided detection (CAD) and assessment of malignant lesions in the liver and lung using a novel PET/CT software tool: initial results. Fortschr Röntgenstr 2010; 182: 243-247
- 24 Ashraf H, de Hoop B, Shaker SB et al. Lung nodule volumetry: segmentation algorithms within the same software package cannot be used interchangeably. Eur Radiol 2010; 20: 1878-1885
- 25 Bolte H, Jahnke T, Schäfer FKW et al. Interobserver-variability of lung nodule volumetry considering different segmentation algorithms and observer training levels. Eur J Radiol 2007; 64: 285-295
- 26 Bolte H, Riedel C, Jahnke T et al. Reproducibility of computer-aided volumetry of artificial small pulmonary nodules in ex vivo porcine lungs. Invest Radiol 2006; 41: 28-35
- 27 Keil S, Plumhans C, Behrendt FF et al. Semi-automated quantification of hepatic lesions in a phantom. Invest Radiol 2009; 44: 82-88
- 28 Keil S, Plumhans C, Nagy IA et al. Dose reduction for semi-automated volumetry of hepatic metastasis in MDCT studies. Invest Radiol 2010; 45: 77-81
- 29 Ray S, Hagge R, Gillen M et al. Comparison of two-dimensional and three-dimensional iterative watershed segmentation methods in hepatic tumor volumetrics. Med Phys 2008; 35: 5869-5881
- 30 Puesken M, Buerke B, Gerss J et al. Prediction of lymph node manifestations in malignant lymphoma: significant role of volumetric compared with established metric lymph node analysis in multislice computed tomography. J Comput Assist Tomogr 2010; 34: 564-569