TY - JOUR
T1 - Loss of heterozygosity and microsatellite instability in De novo versus Ex-adenoma carcinomas of the colorectum
AU - Mueller, James D.
AU - Haegle, Nina
AU - Keller, Gisela
AU - Mueller, Elke
AU - Saretzky, Gabriele
AU - Bethke, Birgit
AU - Stolte, Manfred
AU - Höfler, Heinz
N1 - Funding Information:
The curators of the following herbaria are acknowledged for willingly providing information, specimens, or photocopies of their appropriate holdings: A, B, BA, BAF, Fig. 2 Neotype of Prumnopitys elegans Phil. (Photo: Fl 3955, courtesy Herbarium Universitatis Florentinae) BM, BR, C, CHR, CORD, F, Fl, G, GOET, H, HAL, HBG, JE, K, KIEL, L, LAU, LE, LZ, M, MA, MO, NY, OXF, P, PC, PRC, SGO, SI, US, W, and WRSL. We are especially grateful to Patricia Geissler at G, and Riccardo Baldini at Fl for supplying photographs of type material; Philip Short, Robert Makinson, and Don Foreman, successive Australian Botanical Liaison Officers at Kew, for arranging copies of early taxonomic literature; the staff at CHR Lincoln for assistance with loan material; and Uwe Fritz and Fritz Obst, Tierkunde Museum, Dresden, for verification of Poeppig's handwriting. Funds for the senior author were provided by the Foundation for Research, Science and Technology under Contract C09618.
PY - 1998/12
Y1 - 1998/12
N2 - Small adenocarcinomas of the colorectum showing no evidence of origin from an adenoma have been called de novo carcinomas, a name that implies an origin via a different molecular genetic mechanism than the usual colorectal carcinoma which develops from an adenoma. Using microsatellite analysis, 35 early (pT1) de novo and 36 pT1 ex-adenoma carcinomas were compared using 8 microsatellite loci at 6 different chromosomal loci (1p, 2p, 8p, 5q, 17p, and 18q) known or hypothesized to be important for colorectal carcinogenesis. The rate of loss of heterozygosity (LOH) at the 17p locus (near the p53 gene) was significantly higher in the de novo than in the exadenoma group (73 vs. 37%, P = 0.004). The rates of LOH at the other loci (including the APC and DCC genes) and the rate of MSI were not significantly different in the two groups. These results indicate that de novo carcinomas of the colorectum develop via a similar carcinogenetic pathway as conventional exadenoma carcinomas; however, their higher rate of LOH at 17p is evidence for a biologically more advanced lesion with more frequent p53 mutations, consistent with clinicopathological data indicating that de novo carcinomas are more aggressive than ex-adenoma carcinomas.
AB - Small adenocarcinomas of the colorectum showing no evidence of origin from an adenoma have been called de novo carcinomas, a name that implies an origin via a different molecular genetic mechanism than the usual colorectal carcinoma which develops from an adenoma. Using microsatellite analysis, 35 early (pT1) de novo and 36 pT1 ex-adenoma carcinomas were compared using 8 microsatellite loci at 6 different chromosomal loci (1p, 2p, 8p, 5q, 17p, and 18q) known or hypothesized to be important for colorectal carcinogenesis. The rate of loss of heterozygosity (LOH) at the 17p locus (near the p53 gene) was significantly higher in the de novo than in the exadenoma group (73 vs. 37%, P = 0.004). The rates of LOH at the other loci (including the APC and DCC genes) and the rate of MSI were not significantly different in the two groups. These results indicate that de novo carcinomas of the colorectum develop via a similar carcinogenetic pathway as conventional exadenoma carcinomas; however, their higher rate of LOH at 17p is evidence for a biologically more advanced lesion with more frequent p53 mutations, consistent with clinicopathological data indicating that de novo carcinomas are more aggressive than ex-adenoma carcinomas.
UR - http://www.scopus.com/inward/record.url?scp=0031740545&partnerID=8YFLogxK
U2 - 10.1016/S0002-9440(10)65711-2
DO - 10.1016/S0002-9440(10)65711-2
M3 - Article
C2 - 9846987
AN - SCOPUS:0031740545
SN - 0002-9440
VL - 153
SP - 1977
EP - 1984
JO - American Journal of Pathology
JF - American Journal of Pathology
IS - 6
ER -