Abstract
Bcl-2 is known to inhibit apoptosis and is thought to play a role in colorectal tumour development. Studies of the promoter region of bcl-2 have indicated the presence of a p53 responsive element which downregulates bcl-2 expression. Since p53 is commonly mutated in colorectal cancers, but rarely in those tumours showing microsatellite instability (MSI), the aim of this study was to examine the relationship of bcl-2 protein expression to MSI, as well as to other clinicopathological and molecular variables, in colorectal adenocarcinomas. Expression of bcl-2 was analysed by immunohistochemistry in 71 colorectal cancers which had been previously assigned to three classes depending upon their levels of MSI. MSI-high tumours demonstrated instability in three or more of six microsatellite markers tested, MSI-low tumours in one or two of six, and MSI-null in none of six. Bcl-2 expression in tumours was quantified independently by two pathologists and assigned to one of five categories, with respect to the number of cells which showed positive staining: 0, up to 5%; 1, 6 – 25%; 2, 26 – 50%; 3, 51 – 75%; and 4, ⩾76%. Bcl-2 negative tumours were defined as those with a score of 0. Bcl-2 protein expression was tested for association with clinicopathological stage, differentiation level, tumour site, age, sex, survival, evidence of p53 inactivation and MSI level. A significant association was found between bcl-2 expression and patient survival (P=0.012, Gehan Wilcoxon test). Further, a significant reciprocal relationship was found between bcl-2 expression and the presence of MSI (P=0.012, Wilcoxon rank sum test). We conclude that bcl-2 expressing colorectal cancers are more likely to be MSI-null, and to be associated with improved patient survival.
This is a preview of subscription content, access via your institution
Access options
Subscribe to this journal
Receive 50 print issues and online access
$259.00 per year
only $5.18 per issue
Buy this article
- Purchase on Springer Link
- Instant access to full article PDF
Prices may be subject to local taxes which are calculated during checkout
Similar content being viewed by others
References
Bedi A, Pasricha PJ, Akhtar AJ, Barber JP, Bedi GC, Giardiello FM, Zehnbauer BA, Hamilton SR and Jones RJ. . 1995 Cancer Res. 55: 1811–1816.
Bjerkeset T, Morild I, Mork S and Soreide O. . 1987 Dis. Colon. Rectum 30: 934–938.
Bronner MP, Culin C, Reed JC and Furth EE. . 1995 Am. J. Pathol. 146: 20–26.
Cottu PH, Muzeau F, Estreicher A, Flejou JF, Iggo R, Thomas G and Hamelin R. . 1996 Oncogene 13: 2727–2730.
Frampton J, Ramqvist T and Graf T. . 1996 Genes Dev. 10: 2720–2731.
Hague A, Moorghen M, Hicks D, Chapman M and Paraskeva C. . 1994 Oncogene 9: 3367–3370.
Henriksen R, Wilander E and Oberg K. . 1995 Br. J. Cancer 72: 1324–1329.
Hockenberry D, Nunez G, Millman C, Schreiber RD and Korsmeyer SJ. . 1990 Nature 348: 334–336.
Jass JR, Do K-A, Simms LA, Iino H, Wynter C, Pillay SP, Searle J, Radford-Smith G, Young J and Leggett B. . 1998 Gut 42: 673–679.
Jones MH and Nakamura Y. . 1992 Genes Chromosomes Cancer 5: 89–90.
Kaklamanis L, Savage A, Mortensen N, Tsiotos P, Doussis-Anagnostopoulou I, Biddolph S, Whitehouse R, Harris A and Gatter K. . 1996 J. Path. 179: 10–14.
Kastan MB, Onyinye O, Sidransky D, Vogelstein B and Craig R. . 1991 Cancer Res. 51: 6304–6311.
Konishi M, Kikuchi-Yanoshita R, Tanaka K, Muraoka M, Onda A, Okumura Y, Kishi N, Iwama T, Mori T, Koike M, Ushio K, Chiba M, Nomizu S, Konishi F, Utsunomiya J and Miyaki M. . 1996 Gastroenterology 111: 307–317.
Kuerbitz SJ, Plunkett BS, Walsh WV and Kastan MB. . 1992 Proc. Natl. Acad. Sci. USA 89: 7491–7495.
Lukish JR, Muro K, DeNobile J, Katz R, Williams J, Cruess DF, Drucker W, Kirsch I and Hamilton SR. . 1998 Ann. Surg. 227: 51–56.
Meltzer SJ, Yin J, Huang Y, McDaniel TK, Newkirk C, Iseri O, Vogelstein B and Resau JH. . 1991 Proc. Natl. Acad. Sci. USA 88: 4976–4980.
Miller SA, Dykes DD and Polesky HF. . 1988 Nucl. Acids Res. 16: 1215.
Miyashita T, Harigai M, Hanada M and Reed JC. . 1994 Cancer Res. 54: 3131–3135.
Ofner D, Riehemann K, Maier H, Riedmann B, Nehoda H, Totsch M, Bocker W, Jasani B and Schmid KW. . 1995 Br. J. Cancer. 72: 981–985.
Olschwang S, Laurent-Puig P, Vassal A, Salmon RJ and Thomas G. . 1991 Hum. Genet. 86: 369–370.
Pietenpol J, Papadopoulous N, Markowitz S, Willson J, Kinzler K and Vogelstein B. . 1994 Cancer Res. 54: 3714–3717.
Reed JC. . 1994 J. Cell Biol. 124: 1–6.
Salomoni P, Perrotti D, Martinez R, Franceschi C and Calabretta B. . 1997 Proc. Natl. Acad. Sci. USA 94: 3296–3301.
Simms LA, Zou TT, Young J, Shi YQ, Lei J, Appel R, Rhyu MG, Sugimura H, Chenevix-Trench G, Souza RF, Meltzer SJ and Leggett BA. . 1997 Oncogene 14: 2613–2618.
Simms LA, Radford-Smith G, Biden KG, Buttenshaw R, Cummings M, Jass JR, Young J, Meltzer SJ and Leggett BA. . 1998 Oncogene 17: 2003–2005.
Sinicrope FA, Ruan SB, Cleary KR, Stephens LC, Lee JJ and Levin B. . 1995 Cancer Res. 55: 237–241.
Sun XF, Carstensen JM, Stal O, Zhang H, Boeryd B and Nordenskjold B. . 1996 APMIS 104: 35–38.
Taylor D, Badiani P and Weston K. . 1996 Genes Dev. 10: 2732–2744.
Thibodeau SN, Bren G and Schaid D. . 1993 Science 260: 816–819.
Thompson MA, Flegg R, Westin EH and Ramsay RG. . 1997 Oncogene 14: 1715–1723.
Tsujimoto Y, Cossman J, Jaffe E and Croce C. . 1985 Science 228: 1440–1443.
Vairo G, Innes KM and Adams JM. . 1996 Oncogene 13: 1511–1519.
Vaux D, Cory S and Adams J. . 1988 Nature 335: 440–442.
Watson AJ, Merritt AJ, Jones LS, Askew JN, Anderson E, Becciolini A, Balzi M, Potten CS and Hickman JA. . 1996 Br. J. Cancer. 73: 889–895.
Young R and Korsmeyer SJ. . 1993 Mol. Cell. Biol. 13: 3686–3697.
Acknowledgements
This work was supported by a grant from the Queensland Cancer Fund. During this study, JY and RB were supported by the Royal Brisbane Hospital, and SM by grants CA67497, DK47717, CA77057, CA78843, and the Office of Medical Research, Veterans Affairs.
Author information
Authors and Affiliations
Rights and permissions
About this article
Cite this article
Biden, K., Simms, L., Cummings, M. et al. Expression of Bcl-2 protein is decreased in colorectal adenocarcinomas with microsatellite instability. Oncogene 18, 1245–1249 (1999). https://doi.org/10.1038/sj.onc.1202413
Received:
Revised:
Accepted:
Published:
Issue Date:
DOI: https://doi.org/10.1038/sj.onc.1202413
Keywords
This article is cited by
-
Evaluation of chemopreventive potential of Strobilanthes crispus against colon cancer formation in vitro and in vivo
BMC Complementary and Alternative Medicine (2015)
-
DNA hypermethylation and decreased mRNA expression of MAL, PRIMA1, PTGDR and SFRP1 in colorectal adenoma and cancer
BMC Cancer (2015)
-
Sporadic colorectal carcinomas with low-level microsatellite instability: a distinct subgroup with specific clinicopathological and molecular features
International Journal of Colorectal Disease (2011)
-
Clinical Relevance of Apoptotic Regulatory Proteins in Colorectal Cancers
Current Colorectal Cancer Reports (2010)
-
The immunogenicity of colorectal cancers with high-degree microsatellite instability
World Journal of Surgical Oncology (2005)
