Literature DB >> 7645476

Osteosarcoma and Ewing's sarcoma after neoadjuvant chemotherapy: value of dynamic MR imaging in detecting viable tumor before surgery.

H J van der Woude1, J L Bloem, K L Verstraete, A H Taminiau, M A Nooy, P C Hogendoorn.   

Abstract

OBJECTIVE: This study analyzed the value of dynamic contrast-enhanced and subtraction MR images in detecting residual viable tumor before surgery, with emphasis on timing of enhancement, in patients with high-grade osteosarcoma and Ewing's sarcoma after neoadjuvant chemotherapy. SUBJECTS AND METHODS: Twenty-one patients with proved osteosarcoma or Ewing's sarcoma were treated with neoadjuvant chemotherapy followed by surgery. After IV administration of gadopentetate dimeglumine, dynamic enhancement patterns on preoperative MR images were compared with corresponding areas on histologic sections of the resected specimens. On dynamic subtraction images obtained with high temporal resolution (1.5-3 sec), the interval between arrival of the bolus of contrast agent in an artery and start of tumoral enhancement was used to distinguish residual viable tumor. Early enhancing foci (interval artery-tumor < 6 sec) and late or nonenhancing areas seen on MR images were correlated with the histopathologic findings in these areas of the resected specimens.
RESULTS: Early and progressively enhancing structures seen on MR images corresponded to feeding arteries, physeal vessels, or residual viable tumor at specific preferential sites on corresponding histologic sections of the resected specimens. Tumor foci as small as 3-5 mm2 could be detected on dynamic MR images. Remnant viable tumor was often located subperiosteally and at the margins of the tumor. Occasionally, active periosteal reaction without presence of viable tumor contributed to early enhancement. Late and gradually enhancing or nonenhancing areas corresponded histopathologically to regions of chemotherapy-induced necrosis, mucomyxoid degeneration, or fibrosis. Alternatively, late or nonenhancing areas were associated with reactive changes such as edema, hemorrhage, or osteomyelitis or with tumor-related extracellular matrices such as abundant osteoid or chondroid. Viable tumor areas with scarce formation of matrix on microscopy, such as small cell osteosarcoma areas or Ewing's sarcoma, showed early enhancement with rapid washout of contrast agent on the dynamic MR images.
CONCLUSION: Fast dynamic contrast-enhanced sequences are essential for identifying residual tumor before surgery. A short time interval of less than 6 sec between arterial enhancement and tumoral enhancement strongly correlates with presence of viable tumor. Both therapy-related alterations of tissue and tumor-related matrices must be considered when late or lack of enhancement is noted on dynamic MR images.

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Year:  1995        PMID: 7645476     DOI: 10.2214/ajr.165.3.7645476

Source DB:  PubMed          Journal:  AJR Am J Roentgenol        ISSN: 0361-803X            Impact factor:   3.959


  29 in total

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Authors:  C Baunin; G Schmidt; K Baumstarck; C Bouvier; J C Gentet; A Aschero; A Ruocco; B Bourlière; G Gorincour; C Desvignes; N Colavolpe; G Bollini; P Auqier; P Petit
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Review 2.  Imaging tumour angiogenesis.

Authors:  Tony Jeswani; Anwar R Padhani
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3.  Gray-scale and color Doppler ultrasonographic evaluation of reactivated post-traumatic/postoperative chronic osteomyelitis.

Authors:  A P Balanika; O Papakonstantinou; C J Kontopoulou; C S Baltas; S Athanassia; K Kanelakopoulou; E Brountzos; A Gouliamos; N L Kelekis
Journal:  Skeletal Radiol       Date:  2008-12-10       Impact factor: 2.199

Review 4.  Percent slope analysis of dynamic magnetic resonance imaging for assessment of chemotherapy response of osteosarcoma or Ewing sarcoma: systematic review and meta-analysis.

Authors:  Tadahiko Kubo; Taisuke Furuta; Muhammad P Johan; Nobuo Adachi; Mitsuo Ochi
Journal:  Skeletal Radiol       Date:  2016-05-26       Impact factor: 2.199

5.  Triple-phase contrast-enhanced MRI for the prediction of preoperative chemotherapeutic effect in patients with osteosarcoma: comparison with (99m)Tc-MIBI scintigraphy.

Authors:  Hiroshi Wakabayashi; Junko Saito; Junichi Taki; Nanako Hashimoto; Hiroyuki Tsuchiya; Toshifumi Gabata; Seigo Kinuya
Journal:  Skeletal Radiol       Date:  2015-09-18       Impact factor: 2.199

Review 6.  Musculoskeletal tumors: how to use anatomic, functional, and metabolic MR techniques.

Authors:  Laura M Fayad; Michael A Jacobs; Xin Wang; John A Carrino; David A Bluemke
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Review 7.  Imaging of malignant tumours of the long bones in children: monitoring response to neoadjuvant chemotherapy and preoperative assessment.

Authors:  Hervé Brisse; Liliane Ollivier; Véronique Edeline; Hélène Pacquement; Jean Michon; Christophe Glorion; Sylvia Neuenschwander
Journal:  Pediatr Radiol       Date:  2004-04-22

8.  Evaluation of tumor blood flow in musculoskeletal lesions: dynamic contrast-enhanced MR imaging and its possibility when monitoring the response to preoperative chemotherapy-work in progress.

Authors:  Makoto Kajihara; Yoshifumi Sugawara; Kenshi Sakayama; Keiichi Kikuchi; Teruhito Mochizuki; Kenya Murase
Journal:  Radiat Med       Date:  2007-04-27

9.  Imaging spectrum in soft tissue sarcomas.

Authors:  Pallavi Aga; Ragini Singh; Anit Parihar; Umesh Parashari
Journal:  Indian J Surg Oncol       Date:  2011-12-10

Review 10.  Musculoskeletal primary tumours: treatment evaluation and detection of recurrences.

Authors:  Daniel Vanel
Journal:  Cancer Imaging       Date:  2007-10-01       Impact factor: 3.909

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