The Cause and Clinical Significance of Central Tumor Photopenia on Thallium Scintigraphy of Pediatric Osteosarcoma of the Extremity

doi:10.2214/AJR.06.0292

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Original Research

The Cause and Clinical Significance of Central Tumor Photopenia on Thallium Scintigraphy of Pediatric Osteosarcoma of the Extremity

M. Beth McCarville¹, Ellen H. Barton¹^,2, Jason R. Cameron¹^,3, Xiaoping Xiong⁴, Najat C. Daw⁵, Sue C. Kaste¹, Shenjie Wu⁴, John O. Glass¹ and Wilburn E. Reddick¹

¹ Department of Radiological Sciences, Division of Diagnostic Imaging, St. Jude Children's Research Hospital, 332 N Lauderdale St., Memphis, TN 38105-2974.
² Present address: Methodist University Hospital, Memphis, TN.
³ Present address: Abercrombie Radiological Consultants, Knoxville, TN.
⁴ Department of Biostatistics, St. Jude Children's Research Hospital, Memphis, TN.
⁵ Department of Oncology, St. Jude Children's Research Hospital, Memphis, TN

OBJECTIVE. The objectives of our study were to determine whether centraltumor photopenia on thallium-201 (²⁰¹Tl) scintigraphy of primaryosteosarcoma results from central tumor necrosis or dense central tumorossification and to determine the relation of this finding totumor response to chemotherapy and to patient survival.

MATERIALS AND METHODS. After the institutional review boardapproved our study and waived the need for patient or parentalconsent, two radiologists independently reviewed ²⁰¹Tl scans,conventional radiographs, and MR images of 57 patients obtainedat diagnosis of extremity primary nonmetastatic osteosarcomato detect the presence of central tumor photopenia on ²⁰¹Tlscintigraphy and estimate outer tumor ossification versus innertumor ossification and enhancement. The dynamic enhanced MRIparameters dynamic vector magnitude (DVM) and k_ep (measure ofthe exchange rate between plasma and extracellular fluid space) werecompared for outer tumor versus inner tumor, and the relationamong ²⁰¹Tl scintigraphy, conventional radiography, MRI, andthe dynamic enhanced MRI parameters was analyzed. We examinedwhether central tumor photopenia on ²⁰¹Tl imaging was relatedto histologic response or to patient survival.

RESULTS. Thirty-three patients (58%) had central tumor photopeniaon ²⁰¹Tl imaging that was not associated with central tumor ossification(p = 0.8) or with the difference between outer tumor and innertumor contrast enhancement (p = 0.4). Central tumor photopenia on²⁰¹Tl scintigraphy was significantly associated with an increasingdifference between outer tumor DVM and inner tumor DVM (i.e.,outer tumor DVM minus inner tumor DVM) (p = 0.05), an increasingdifference between outer tumor k_ep and inner tumor k_ep (i.e.,outer k_ep minus inner k_ep) (p = 0.01), and an increasing outerk_ep-inner k_ep ratio (p = 0.02). We found no relation betweencentral tumor photopenia and histologic response (p $≥$ 0.2). Olderpatients (age, $≥$ 13 years) with central tumor photopenia wereleast likely to survive, whereas younger patients (age, <13 years) without central tumor photopenia were most likelyto survive (p = 0.07).

CONCLUSION. Central tumor photopenia on ²⁰¹Tl scintigraphy ofprimary osteosarcoma is unlikely to reflect central ossificationbut may be due to central necrosis reflected by higher outer tumorDVM and k_ep than inner tumor DVM and k_ep and may be negativelyassociated with survival in older patients. Prospective studies areneeded to determine the value of this information in planning treatment.

Keywords: dynamic enhanced MRI • musculoskeletal system • oncologic imaging • osteosarcoma • pediatric imaging • scintigraphy • thallium scintigraphy

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