High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas

Barry M. Kacinski; Darryl Carter; Khushbakhat Mittal; Ernest I. Kohorn; R. Shaeffer Bloodgood; John Donahue; Lisa Donofrio; Rob Edwards; Peter E. Schwartz; Joseph T. Chambers; Setsuko K. Chambers

doi:10.1016/0360-3016(88)90113-7

High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas

Barry M. Kacinski, Darryl Carter, Khushbakhat Mittal, Ernest I. Kohorn, R. Shaeffer Bloodgood, John Donahue, Lisa Donofrio, Rob Edwards, Peter E. Schwartz, Joseph T. Chambers, Setsuko K. Chambers

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Abstract

Six micron paraffin sections of paraformaldehyde-fixed endometrial currettings of 21 benign and neoplastic endometrial specimens were assayed for tumor cell-specific oncogene expression by in situ hybridization with probes for six oncogenes, beta-actin, and the E. coli plasmid pBR322. In the benign hyperplasias and invasive adenocarcinomas, multiple oncogenes, including erbB, fms, c-myc, and Ki-ras were expressed at significant levels. For the adenocarcinomas, statistical analysis demonstrated that high levels of expression of fms-complementary mRNA correlated strongly with clinicopathologic features (high FIGO histologic grade, high FIGO clinical stage, deep myometrial penetration) predictive of aggressive clinical behavior and poor outcome. The authors discuss the role which M-CSF receptor (the fms gene product) and locally-produced M-CSF may play in the development of the observed aggressively-malignant phenotypes. They also propose that pre-hysterectomy assay of fms gene expression in endometrial currettings in FIGO Stage I patients might be clinically useful to help identify preoperatively those patients with deep myometrial penetration or other locoregional spread.

Original language	English (US)
Pages (from-to)	823-829
Number of pages	7
Journal	International Journal of Radiation Oncology, Biology, Physics
Volume	15
Issue number	4
DOIs	https://doi.org/10.1016/0360-3016(88)90113-7
State	Published - 1988
Externally published	Yes

Keywords

CSF-1 receptor
Endometrial carcinoma
FMS oncogene
Growth factor receptors
In situ hybridization
Tumor/stromal interactions

ASJC Scopus subject areas

Oncology
Radiology Nuclear Medicine and imaging
Radiation

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10.1016/0360-3016(88)90113-7

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Kacinski, B. M., Carter, D., Mittal, K., Kohorn, E. I., Bloodgood, R. S., Donahue, J., Donofrio, L., Edwards, R., Schwartz, P. E., Chambers, J. T., & Chambers, S. K. (1988). High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas. International Journal of Radiation Oncology, Biology, Physics, 15(4), 823-829. https://doi.org/10.1016/0360-3016(88)90113-7

Kacinski, BM, Carter, D, Mittal, K, Kohorn, EI, Bloodgood, RS, Donahue, J, Donofrio, L, Edwards, R, Schwartz, PE, Chambers, JT & Chambers, SK 1988, 'High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas', International Journal of Radiation Oncology, Biology, Physics, vol. 15, no. 4, pp. 823-829. https://doi.org/10.1016/0360-3016(88)90113-7

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title = "High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas",

abstract = "Six micron paraffin sections of paraformaldehyde-fixed endometrial currettings of 21 benign and neoplastic endometrial specimens were assayed for tumor cell-specific oncogene expression by in situ hybridization with probes for six oncogenes, beta-actin, and the E. coli plasmid pBR322. In the benign hyperplasias and invasive adenocarcinomas, multiple oncogenes, including erbB, fms, c-myc, and Ki-ras were expressed at significant levels. For the adenocarcinomas, statistical analysis demonstrated that high levels of expression of fms-complementary mRNA correlated strongly with clinicopathologic features (high FIGO histologic grade, high FIGO clinical stage, deep myometrial penetration) predictive of aggressive clinical behavior and poor outcome. The authors discuss the role which M-CSF receptor (the fms gene product) and locally-produced M-CSF may play in the development of the observed aggressively-malignant phenotypes. They also propose that pre-hysterectomy assay of fms gene expression in endometrial currettings in FIGO Stage I patients might be clinically useful to help identify preoperatively those patients with deep myometrial penetration or other locoregional spread.",

keywords = "CSF-1 receptor, Endometrial carcinoma, FMS oncogene, Growth factor receptors, In situ hybridization, Tumor/stromal interactions",

author = "Kacinski, {Barry M.} and Darryl Carter and Khushbakhat Mittal and Kohorn, {Ernest I.} and Bloodgood, {R. Shaeffer} and John Donahue and Lisa Donofrio and Rob Edwards and Schwartz, {Peter E.} and Chambers, {Joseph T.} and Chambers, {Setsuko K.}",

year = "1988",

doi = "10.1016/0360-3016(88)90113-7",

language = "English (US)",

volume = "15",

pages = "823--829",

journal = "International Journal of Radiation Oncology, Biology, Physics",

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T1 - High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas

AU - Kacinski, Barry M.

AU - Carter, Darryl

AU - Mittal, Khushbakhat

AU - Kohorn, Ernest I.

AU - Bloodgood, R. Shaeffer

AU - Donahue, John

AU - Donofrio, Lisa

AU - Edwards, Rob

AU - Schwartz, Peter E.

AU - Chambers, Joseph T.

AU - Chambers, Setsuko K.

PY - 1988

Y1 - 1988

N2 - Six micron paraffin sections of paraformaldehyde-fixed endometrial currettings of 21 benign and neoplastic endometrial specimens were assayed for tumor cell-specific oncogene expression by in situ hybridization with probes for six oncogenes, beta-actin, and the E. coli plasmid pBR322. In the benign hyperplasias and invasive adenocarcinomas, multiple oncogenes, including erbB, fms, c-myc, and Ki-ras were expressed at significant levels. For the adenocarcinomas, statistical analysis demonstrated that high levels of expression of fms-complementary mRNA correlated strongly with clinicopathologic features (high FIGO histologic grade, high FIGO clinical stage, deep myometrial penetration) predictive of aggressive clinical behavior and poor outcome. The authors discuss the role which M-CSF receptor (the fms gene product) and locally-produced M-CSF may play in the development of the observed aggressively-malignant phenotypes. They also propose that pre-hysterectomy assay of fms gene expression in endometrial currettings in FIGO Stage I patients might be clinically useful to help identify preoperatively those patients with deep myometrial penetration or other locoregional spread.

AB - Six micron paraffin sections of paraformaldehyde-fixed endometrial currettings of 21 benign and neoplastic endometrial specimens were assayed for tumor cell-specific oncogene expression by in situ hybridization with probes for six oncogenes, beta-actin, and the E. coli plasmid pBR322. In the benign hyperplasias and invasive adenocarcinomas, multiple oncogenes, including erbB, fms, c-myc, and Ki-ras were expressed at significant levels. For the adenocarcinomas, statistical analysis demonstrated that high levels of expression of fms-complementary mRNA correlated strongly with clinicopathologic features (high FIGO histologic grade, high FIGO clinical stage, deep myometrial penetration) predictive of aggressive clinical behavior and poor outcome. The authors discuss the role which M-CSF receptor (the fms gene product) and locally-produced M-CSF may play in the development of the observed aggressively-malignant phenotypes. They also propose that pre-hysterectomy assay of fms gene expression in endometrial currettings in FIGO Stage I patients might be clinically useful to help identify preoperatively those patients with deep myometrial penetration or other locoregional spread.

KW - CSF-1 receptor

KW - Endometrial carcinoma

KW - FMS oncogene

KW - Growth factor receptors

KW - In situ hybridization

KW - Tumor/stromal interactions

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High level expression of fms proto-oncogene mRNA is observed in clinically aggressive human endometrial adenocarcinomas

Abstract

Keywords

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