123I-mIBG scintigraphy in neuroblastoma : development of a SIOPEN semi-quantitative reporting method by an international panel

A robust method is required to standardise objective reporting of diagnostic I-123-mIBG images in neuroblastoma. Prerequisites for an appropriate system are low inter- and intra-observer error and reproducibility across a broad disease spectrum. We present a new reporting method, developed and teste...

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Hauptverfasser: Lewington, V, Lambert, Bieke, Poetschger, U, Sever, Z Bar, Giammarile, F, McEwan, AJB, Castellani, Rita, Lynch, T, Shulkin, B, Drobics, M, Staudenherz, A, Ladenstein, R
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Sprache:eng
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Zusammenfassung:A robust method is required to standardise objective reporting of diagnostic I-123-mIBG images in neuroblastoma. Prerequisites for an appropriate system are low inter- and intra-observer error and reproducibility across a broad disease spectrum. We present a new reporting method, developed and tested for SIOPEN by an international expert panel. Patterns of abnormal skeletal I-123-mIBG uptake were defined and assigned numerical scores [0-6] based on disease extent within 12 body segments. Uptake intensity was excluded from the analysis. Data sets from 82 patients were scored independently by six experienced specialists as unblinded pairs (pre- and post-induction chemotherapy) and in random order as a blinded study. Response was defined as ae50 % reduction in post induction score compared with baseline. In total, 1968 image sets were reviewed individually. Response rates of 88 % and 82 % were recorded for patients with baseline skeletal scores ae23 and 24-48 respectively, compared with 44 % response in patients with skeletal scores > 48 (p = 0.02). Reducing the number of segments or extension scale had a small but statistically negative impact upon the number of responses detected. Intraclass correlation coefficients [ICCs] calculated for the unblinded and blinded study were 0.95 at diagnosis and 0.98 and 0.99 post-induction chemotherapy, respectively. The SIOPEN mIBG score method is reproducible across the full spectrum of disease in high risk neuroblastoma. Numerical assessment of skeletal disease extent avoids subjective evaluation of uptake intensity. This robust approach provides a reliable means with which to examine the role of 123I mIBG scintigraphy as a prognostic indicator in neuroblastoma.
ISSN:1619-7070
1619-7089