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Value of fine needle aspiration biopsy in childhood rhabdomyosarcoma: Twenty-six years of experience in Slovenia

โœ Scribed by Pohar-Marin?ek, ?iva ;An?i?, Jo?ica ;Jereb, Berta


Publisher
John Wiley and Sons
Year
2002
Tongue
English
Weight
172 KB
Volume
38
Category
Article
ISSN
0098-1532

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โœฆ Synopsis


Abstract

Background

Chemotherapy (Cht) for rhabdomyosarcoma (RMS) given before local treatment can prevent mutilating surgery and highโ€dose irradiation (RT). Fine needle aspiration biopsy (FNAB) can confirm the diagnosis and neoadjuvant treatment can start without delay. The purpose of our study was to assess the role of FNAB in the management of childhood RMS in Slovenia.

Procedure

A total of 78 children and young adults were included. FNAB provided the preโ€treatment diagnosis in 37 and surgical biopsy in 41 patients. In 61 cases recurrent/metastatic disease was aspirated. Cytological diagnoses were compared to the original histological diagnoses. All case histories, cytological and histological material were reviewed and immunocytochemical staining performed when necessary.

Results

FNAB provided a correct diagnosis of malignancy in all 37 primary tumours, a specific diagnosis of RMS was given in 29 (78%). With the use of immunocytochemistry during the last 15 years, the accuracy has risen to 87%. FNAB provided the diagnosis of recurrence/metastasis in 57/61 cases. No complications of FNAB were noted. Review of histology reclassified five original diagnoses of RMS into one malignant rhabdoid tumour and four sarcomas NOS. In review of cytology we were able to sub classify 80% of RMS.

Conclusions

FNAB is a safe method, which enables us to establish the preโ€treatment diagnosis of RMS, and to some extent even its type, without delay. In our study, FNAB successfully replaced surgical biopsy in 87% of RMS patients during the last 15 years. Neoadjuvant Cht was started immediately, surgery was delayed and more conservative. Consequently, the risk for treatment sequelae was considerably reduced. Med Pediatr Oncol 2002;38:416โ€“420. ยฉ 2002 Wileyโ€Liss, Inc.


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