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The frequency of p53, k‐ ras mutations, and microsatellite instability differs in uterine endometrioid and serous carcinoma
Author(s) -
Lax Sigurd F.,
Kendall Brian,
Tashiro Hironori,
Slebos Robbert J. C.,
Ellenson Lora Hedrick
Publication year - 2000
Publication title -
cancer
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.052
H-Index - 304
eISSN - 1097-0142
pISSN - 0008-543X
DOI - 10.1002/(sici)1097-0142(20000215)88:4<814::aid-cncr12>3.0.co;2-u
Subject(s) - microsatellite instability , serous fluid , exon , mutation , carcinoma , polymerase chain reaction , cancer research , gene , biology , medicine , microsatellite , microbiology and biotechnology , pathology , genetics , allele
BACKGROUND The two most common types of uterine endometrial carcinoma, endometrioid (UEC) and serous (USC), differ in their histopathologic appearance and biologic behavior. Recent studies suggest that these differences may be associated with distinct molecular genetic alterations. METHODS In the current study, the authors compared the frequencies of K‐ ras and p53 mutations and microsatellite instability (MI) between UEC and USC by analyzing all 3 molecular genetic changes in one set of tumors. Furthermore, the distribution of these molecular genetic alterations was determined among UECs of different histopathologic grade. The authors analyzed 58 UECs with known MI status for K‐ ras and p53 mutations. The K‐ ras and p53 genes were analyzed in 45 and 6 cases of USC, respectively. These results were combined with previous data on p53 mutations (21 cases) and MI (34 cases) in USC. RESULTS MI was present in 16 of 57 UECs (28%) but in none of 34 USCs. p53 mutations were found in 7 of 42 UECs (17%) and 25 of 27 USCs (93%) by direct sequencing of exons 5–8. UECs and USCs with p53 mutations showed strong immunoreactivity for p53 in about 85% of the cases, whereas about 15% of the cases were immunonegative. K‐ ras mutations at codon 12 were found in 15 of 58 UECs (26%) and in only 1 of 45 USC (2%) by dot blot oligohybridization after polymerase chain reaction amplification of exon 1. Notably, the frequency of both K‐ ras and p53 mutations and MI was significantly different between UEC and USC ( P < 0.001). In UECs, MI and K‐ ras mutations occurred in low grade as well as in high grade tumors, whereas p53 mutations were present almost exclusively in high grade tumors. CONCLUSIONS The results of this study suggest that different molecular genetic pathways are involved in the pathogenesis of UEC and USC and that low grade UEC may progress to high grade UEC. These findings support the hypothesis that UEC and USC are separate entities and suggest that different molecular genetic alterations may be responsible for their distinct morphology and biologic behavior. Cancer 2000;88:814–24. © 2000 American Cancer Society.