TY - JOUR
T1 - Increased levels of phorbin, c‐myc, and ornithine decarboxylase RNAs in human colon cancer
AU - Guillem, Jose G.
AU - Levy, Miriam F.
AU - Hsieh, Ling Ling
AU - Johnson, Mark D.
AU - Logerfo, Paul
AU - Forde, Kenneth A.
AU - Weinstein, I. Bernard
PY - 1990
Y1 - 1990
N2 - Our previous work on protein kinase C (PKC) and colon cancer has shown altered levels of PKC activity in human colon tumors, as well as activation of PKC by colon tumor promoters such as bile acids. To understand further the role of PKC in colon carcinogenesis, we analyzed the expression of phorbin, a gene induced by PKC activation, in a series of different stages of human colon tumors. As shown by northern blot analyses of poly (A)+ RNA, higher levels of phorbin RNA were seen in 26 colon tumor samples than in their adjacent normal colonic mucosa. There also appeared to be a correlation between the abundance of phorbin RNA in the tumors and the extent of invasion (tumor‐to‐normal tissue phorbin RNA ratio = 4.2, 8.0, and 11.9 for Dukes' A, B, and C, respectively). Phorbin RNA was also abundant in a human colon cancer line (HT29). We also examined the expression of other mitogen‐responsive genes (c‐myc, ODC, and β‐actin) in a set of 19 colon tumor samples. All tumors displayed significant (mean 3.8‐fold) increases in the level of c‐myc RNA compared with their adjacent normal colonic mucosa. About 47% and 16% of these tumor samples also showed increased levels of ODC (mean 3.1‐fold) and β‐actin (mean 1.6‐fold) RNA, respectively. The increased levels of c‐myc, ODC, and β‐actin RNA did not correlate with the extent of tumor invasion. Taken together, these results demonstrate that human colon tumors usually display increased levels of both phorbin and c‐myc RNAs. The marked increases in phorbin RNA suggest that this could serve as a useful biomarker in studies on human colon cancer.
AB - Our previous work on protein kinase C (PKC) and colon cancer has shown altered levels of PKC activity in human colon tumors, as well as activation of PKC by colon tumor promoters such as bile acids. To understand further the role of PKC in colon carcinogenesis, we analyzed the expression of phorbin, a gene induced by PKC activation, in a series of different stages of human colon tumors. As shown by northern blot analyses of poly (A)+ RNA, higher levels of phorbin RNA were seen in 26 colon tumor samples than in their adjacent normal colonic mucosa. There also appeared to be a correlation between the abundance of phorbin RNA in the tumors and the extent of invasion (tumor‐to‐normal tissue phorbin RNA ratio = 4.2, 8.0, and 11.9 for Dukes' A, B, and C, respectively). Phorbin RNA was also abundant in a human colon cancer line (HT29). We also examined the expression of other mitogen‐responsive genes (c‐myc, ODC, and β‐actin) in a set of 19 colon tumor samples. All tumors displayed significant (mean 3.8‐fold) increases in the level of c‐myc RNA compared with their adjacent normal colonic mucosa. About 47% and 16% of these tumor samples also showed increased levels of ODC (mean 3.1‐fold) and β‐actin (mean 1.6‐fold) RNA, respectively. The increased levels of c‐myc, ODC, and β‐actin RNA did not correlate with the extent of tumor invasion. Taken together, these results demonstrate that human colon tumors usually display increased levels of both phorbin and c‐myc RNAs. The marked increases in phorbin RNA suggest that this could serve as a useful biomarker in studies on human colon cancer.
KW - Key words
KW - Protein kinase C
KW - colon neoplasm
KW - myc, orthinine decarboxylase
KW - phorbin
UR - http://www.scopus.com/inward/record.url?scp=0025345014&partnerID=8YFLogxK
U2 - 10.1002/mc.2940030204
DO - 10.1002/mc.2940030204
M3 - 文章
C2 - 1693276
AN - SCOPUS:0025345014
SN - 0899-1987
VL - 3
SP - 68
EP - 74
JO - Molecular Carcinogenesis
JF - Molecular Carcinogenesis
IS - 2
ER -