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[Cancer Research 60, 3348-3353, July 1, 2000]
© 2000 American Association for Cancer Research


Advances in Brief

High Resolution Allelotype of Microdissected Primary Nasopharyngeal Carcinoma1

Kwok-Wai Lo2, Peter M. L. Teo, Angela Bik-Yu Hui, Ka-Fai To, Yuen-Shan Tsang, Sylvia Yat-Yee Chan, Ko-Fung Mak, Joseph C. K. Lee and Dolly P. Huang

Departments of Anatomical and Cellular Pathology [K-W. L., A. B-Y. H., K-F. T., Y-S. T., S. Y-Y. C., K-F. M., J. C. K. L., D. P. H.], and Clinical Oncology [P. M. L. T.], Prince of Wales Hospital, The Chinese University of Hong Kong, Hong Kong SAR, China

Nasopharyngeal carcinoma (NPC) is a common cancer in South China but is rare in other parts of the world. To better understand the molecular basis of this cancer, we performed high-resolution allelotyping on 27 microdissected primary tumors using 382 microsatellite markers. We have detected high frequencies of allelic imbalance on 3p (96.3%), 9p (85.2%), 9q (88.9%), 11q (74.1%), 12q (70.4%), 13q (55.6%), 14q (85.2%), and 16q (55.6%). Nonrandom allelic changes of 12q and 16q were revealed for the first time. In addition, loss of heterozygosity on chromosomal arms 1p (37.0%), 5q (44.4%), and 12p (44.4%) were also common in NPC. Multiple minimally deleted regions, 7–40 cM, were identified at 3p14–24.2, 11q21–23, 13q12–14, 13q31–32, 14q24–32, and 16q22–23. Frequent deletions of these minimally deleted regions implied the presence of tumor suppressor genes that may be involved in the development of NPC. Consistent loss of heterozygosity on 3p, 9p, and 14q in almost all tumors suggested that such changes are critical events in NPC tumorigenesis.




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