Oral field cancerization: Current evidence and future perspectives

被引:77
作者
Punnya V. Angadi
J. K. Savitha
Sanjay S. Rao
Y. Sivaranjini
机构
[1] KLE VK Institute of Dental Sciences and Hospital
[2] Raja Rajeshwari Dental College, Bangalore, Karnataka
[3] Mamata Dental College, Khammam, Andhra Pradesh
来源
Oral and Maxillofacial Surgery | 2012年 / 16卷 / 2期
关键词
Field cancerization; Oral cancer; Premalignant lesions; Tobacco;
D O I
10.1007/s10006-012-0317-x
中图分类号
学科分类号
摘要
Introduction: Oral field cancerization implies that oral cancer does not arise as an isolated cellular phenomenon but rather as an anaplastic tendency involving many cells at once and results in the multifocal development of cancer at various rates within the entire field in response to a carcinogen especially tobacco. This concept has been frequently used to explain the occurrence of multiple primary cancers and recurrences following complete excision of oral cancer. Discussion: This review deals in detail with the origin, principle, various theories used to explain this effect and molecular, genetic, as well as cytogenetic findings related to oral field cancerization. Further, the clinical implications and future research directives are also discussed. © 2012 Springer-Verlag.
引用
收藏
页码:171 / 180
页数:9
相关论文
共 81 条
[11]  
Partridge M., Emilion G., Pateromichelakis S., Philips E., Langdon, Field cancerization of oral cavity: comparison of the spectrum of molecular alterations in cases presenting with both dysplastic and malignant lesions, Oral Oncol, 33, pp. 332-337, (1997)
[12]  
Day G., Blot W.J., Shore R.E., McLaughlin J.K., Austin D.F., Greenberg R.S., Second cancers following oral and pharyngeal cancers: role of tobacco and alcohol, J Natl Cancer Inst, 86, pp. 131-137, (1994)
[13]  
Cianfriglia F., Di Gregorio D.A., Manieri A., Multiple primary tumors in patients with oral squamous cell carcinoma, Oral Oncol, 35, pp. 157-163, (1999)
[14]  
Prevo L.J., Sanchez C.A., Galipeau P.C., Reid B.J., p53-mutant clones and field effects in Barrett's esophagus, Cancer Res, 59, pp. 4784-4787, (1999)
[15]  
Jang S.J., Chiba I., Hirai A., Hong W.K., Mao L., Multiple oral squamous epithelial lesions: are they genetically related?, Oncogene, 20, pp. 2235-2242, (2001)
[16]  
Tabor M.P., Brakenhoff R.H., Rujiter-Schippers H.J., van der Wal J.E., Snow G.B., Leemans C.R., Braakhuis B.J., Multiple head and neck tumors frequently originate from a single preneoplastic lesion, Am J Pathol, 161, pp. 1051-1060, (2002)
[17]  
Simon R., Eltze E., Schafer K.L., Burger H., Semjonow A., Hertle L., Dockhorn-Dworniczak B., Terpe H.J., Bocker W., Cytogenetic analysis of multifocal bladder cancer supports a monoclonal origin and intraepithelial spread of tumor cells, Cancer Res, 61, pp. 355-362, (2001)
[18]  
Braakhuis B.J., Tabor M.P., Leemans C.R., Second primary tumors and field cancerization in oral and or pharyngeal cancer: molecular techniques provide new insights and definitions, Head Neck, 24, pp. 198-206, (2002)
[19]  
Boudewijin J.M., Braakhuis B.J., Leemans C.R., Brakenhoff R.H., A genetic progression model of oral cancer: current evidence and clinical implications, J Oral Pathol Med, 33, pp. 317-322, (2004)
[20]  
Wright A., Shear M., Epithelial dysplasia immediately adjacent to oral squamous cell carcinomas, J Oral Pathol, 14, pp. 559-564, (1985)
123456789