Prognostic Significance of Histologic Features, DNA Content, Expression of Proliferating Cell Nuclear Antigen (PCNA), c-fos Protein and Transforming Growth Factor (TGF)-alpha and -beta in Giant Cell Tumor of Bone.
- Author:
Hee Kyung CHANG
;
Sung Hun YOON
;
Jae Do KIM
;
Man Ha HUH
- Publication Type:Original Article
- Keywords:
Bone;
Giant cell tumor;
PCNA;
TGF-alpha & beta;
Ploidy pattern
- MeSH:
Aneuploidy;
Carcinogenesis;
Diploidy;
DNA*;
Giant Cell Tumor of Bone*;
Giant Cell Tumors*;
Giant Cells*;
Hemorrhage;
Lung;
Necrosis;
Negative Staining;
Neoplasm Metastasis;
Oncogenes;
Ploidies;
Prevalence;
Prognosis;
Proliferating Cell Nuclear Antigen*;
Recurrence;
Stromal Cells;
Transforming Growth Factor alpha;
Transforming Growth Factor beta;
Transforming Growth Factors*
- From:Journal of the Korean Cancer Association
1997;29(2):266-279
- CountryRepublic of Korea
- Language:Korean
-
Abstract:
PURPOSE: This study was attempted to investigate the prevalence of the expression of c-fos protein, TGF-alpha and -beta, PCNA , DNA ploidy pattern and histopathological parameters of giant cell tumor (GCT) of bone and to correlate with prognosis and to extend our understanding on tumorigenesis of GCT. MATERIALS AND METHODS: Twenty eight cases of paraffin-embedded tissue were studied, classified as recurrent (5 cases) and non-recurrent group (12cases) within the limits of the cases which afforded surgical material on first operation. RESULTS: No significant difference was observed in cellularity of stromal cells, atypia of stromal and giant cells, presence of hemorrhage and necrosis between recurrent and non-recurrent group. However, presence of more than 10 mitotic figures in 10 high power fields in recurrent group was significantly higher than non-recurrent group (p<0.05). The immunoreactivity for PCNA was seen only in nuclei of stromal cells, whereas nuclei of giant cells showed negative staining. The positivity of PCNA revealed no significant difference between non-recurrent (mean; 40.9%) and recurrent group (34.4%). The expression of c-fos oncogene was seen in 5 cases (100%) in recurrent group, and 8 cases (66.7%) in non-recurrent group, and no significant difference was seen. No significant difference of expression of TGF-alpha was seen in 5 cases (100%) in recurrent group and in 11 cases (91.7%) in non-recurrent group. The expression of TGF-beta in stromal cells was significantly higher in non-recurrent group (80%) compared to recurrent group (100%) (p<0.05). In DNA analysis out of 18 cases, 4 cases (22.2%) were aneuploidy and 14 cases (77.8%) were diploidy. Among 4 aneuploidy cases, 3 cases (75%) had no recurrence, and 1 case (25%) had metastasis to lung and expired. No significant difference of DNA ploidy pattern was seen between the recurrent and non-recurrent group. CONCLUSION: Presence of more than 10 mitotic figures in 10 high power fields and less expression of TGF-beta are related to higher possibility of recurrence and it is suggested that the number of mitotic figure (more than 10/10HPF) and expression of TGF-beta could be helpful parameters in predicting recurrence of GCT.