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The significance of allelic deletions and aneuploidy in colorectal carcinoma : Results of a 5-year follow-up study

✍ Scribed by Kenneth H. Cohn; Deborah L. Ornstein; Fusheng Wang; Fidelina DeSoto LaPaix; Kathy Phipps; Cheryl Edelsberg; Rosemary Zuna; Leila A. Mott; John L. Dunn


Publisher
John Wiley and Sons
Year
1997
Tongue
English
Weight
159 KB
Volume
79
Category
Article
ISSN
0008-543X

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✦ Synopsis


Background:

A prospective study was initiated to analyze the prognostic value of both the deletion of candidate tumor suppressor genes and the dna content in colorectal carcinoma specimens.

Methods:

A prospective study was initiated in 1988, into which 104 patients from the brooklyn va medical center were accrued through march 1992. dna restriction endonuclease digests, obtained by the southern blot technique, were examined for allelic deletions by cdna probes pnm23-h1 (17q21) ynz 22.1 (17p13), and p15-65 (18q21). dna content was measured by image analysis cytometry of feulgen-stained tumor imprints. median follow-up was 5.5 years (range, 4-8.5 years).

Results:

Patients with nm23-h1 allelic deletions were 3 times as likely to develop distant metastases as patients without nm23-h1 deletions (relative risk [rr], 3.89; 95% confidence interval [ci], 1.39, 10.89). this connection was even stronger after adjustment for tnm stage and site of primary tumor (rr, 5.27; 95% ci, 1.67, 16.68). no significant association of 17p or 18q deletions or ploidy with either distant metastases or overall survival was noted. in multivariate analysis, clinicopathologic variables associated with decreased survival included intracellular mucin production, nuclear grade, tnm stage, and nerve invasion.

Conclusions:

A combination of clinicopathologic and molecular biologic variables may identify patients at high risk for death from disseminated colorectal carcinoma.


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