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Cancer Chemotherapy and Pharmacology
Published in: Cancer Chemotherapy and Pharmacology 2/2011

01-08-2011 | Original Article

Is there any impact of plasma M30 and M65 levels on progression-free survival of patients with advanced gastric cancer?

Authors: Ahmet Bilici, Bala Basak Oven Ustaalioglu, Serif Ercan, Asuman Orcun, Mesut Seker, Taflan Salepci, Mahmut Gumus

Published in: Cancer Chemotherapy and Pharmacology | Issue 2/2011

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Abstract

Purpose

M30 and M65 are different circulating fragments of cytokeratin 18. They release during apoptotic cell death, so it is believed that they reflect cell death of epithelial tumors. The aim of this study was to determine the prognostic value of plasma M30 and M65 levels in predicting of survival for patients with advanced gastric cancer compare with healthy controls.

Methods

Thirty-four patients with advanced gastric cancer and thirty-two healthy controls were included. Plasma M30 and M65 values were measured by quantitative ELISA method.

Results

The median age of patients and control groups was 60 and 56 years, respectively. No difference was detected between patient and control groups with respect to plasma median M30 values (390.4 vs. 270.7 U/l, respectively, P = 0.10). The median plasma M65 values of patients were significantly higher than those of control group (1232.1 vs. 580.1 U/l, P < 0.001). The best cut-off values for plasma M30 and M65 for predicting progression-free survival (PFS) were 277.7 and 1434.9 U/l in ROC analysis. The patients whose plasma M30 values were higher than 277.7 U/l had worse PFS than patients with plasma M30 value <277.7 U/l (8.9 vs. 11.2, respectively, P = 0.01). The median PFS of patients whose M65 levels lower than or equal to 1434.9 U/l was better than that of patients whose M65 levels were >1434.9 U/l (12.4 vs. 10.4, respectively, P = 0.04). But plasma M30 and M65 level in patient group were not found to be an important prognostic factor for PFS in the multivariate analysis.

Conclusions

These results showed that plasma M65 values were significantly elevated in patients with advanced gastric cancer compared to healthy people. Moreover, both increased plasma M30 and M65 levels can predict PFS in patients with gastric cancer.
Literature
1.
Caulín C, Salvesen GS, Oshima RG (1997) Caspase cleavage of keratin 18, reorganization of intermediate filaments during epithelial cell apoptosis. J Cell Biol 138:1379–1394PubMedCrossRef
2.
Ku NO, Liao J, Omary MB (1997) Apoptosis generates stable fragments of human type I keratins. J Biol Chem 272:33197–33203PubMedCrossRef
3.
Bivén K, Erdal H, Hägg M et al (2003) A novel assay for discovery, characterization of pro-apoptotic drugs, for monitoring apoptosis in patient sera. Apoptosis 8:263–268PubMedCrossRef
4.
Kramer G, Erdal H, Mertens HJ et al (2004) Differentiation between cell death modes using measurements of different soluble forms of extracellular cytokeratin 18. Cancer Res 64:1751–1756PubMedCrossRef
5.
Ueno T, Toi M, Linder S (2005) Detection of epithelial cell death in the body by cytokeratin 18 measurement. Biomed Pharmacother 59:S359–S362PubMedCrossRef
6.
Leers MP, Kölgen W, Björklund V et al (1999) Immunocytochemical detection, mapping of a cytokeratin 18 neo-epitope exposed during early apoptosis. J Pathol 187:567–572PubMedCrossRef
7.
Galluzzi L, Maiuri MC, Vitale I, Zischka H, Castedo M, Zitvogel L, Kroemer G (2007) Cell death modalities: classification, pathophysiological implications. Cell Death Differ 14:1237–1243PubMedCrossRef
8.
Yaman E, Coskun U, Sancak B, Buyukberber S, Ozturk B, Benekli M (2010) Serum M30 levels are associated with survival in advanced gastric carcinoma patients. Int Immunopharmacol 10:719–722
9.
Demiray M, Ulukaya EE, Arslan M et al (2006) Response to neoadjuvant chemotherapy in breast cancer could be predictable by measuring a novel serum apoptosis product, caspase-cleaved cytokeratin 18: a prospective pilot study. Cancer Invest 24:669–676PubMedCrossRef
10.
Ueno T, Toi M, Bivén K, Bando H, Ogawa T, Linder S (2003) Measurement of an apoptotic product in the sera of breast cancer patients. Eur J Cancer 39:769–774PubMedCrossRef
11.
Ulukaya E, Yilmaztepe A, Akgoz S, Linder S, Karadag M (2007) The levels of caspase-cleaved cytokeratin 18 are elevated in serum from patients with lung cancer, helpful to predict the survival. Lung Cancer 56:399–404PubMedCrossRef
12.
Olofsson MH, Ueno T, Pan Y et al (2007) Cytokeratin-18 is a useful serum biomarker for early determination of response of breast carcinomas to chemotherapy. Clin Cancer Res 13:3198–3206PubMedCrossRef
13.
Ozturk B, Coskun U, Sancak B, Yaman E, Buyukberber S, Benekli M (2009) Elevated serum levels of M30, M65 in patients with locally advanced head, neck tumors. Int Immunopharmacol 9:645–648PubMedCrossRef
14.
Ausch C, Buxhofer-Ausch V, Olszewski U, Hinterberger W, Ogris E, Schiessel R, Hamilton G (2009) Caspase-cleaved cytokeratin 18 fragment (M30) as marker of postoperative residual tumor load in colon cancer patients. Eur J Surg Oncol 35:1164–1168PubMed
15.
Dive C, Smith RA, Garner E et al (2010) Considerations for the use of plasma cytokeratin 18 as a biomarker in pancreatic cancer. Br J Cancer 102:577–582PubMedCrossRef
16.
de Haas EC, di Pietro A et al (2008) Simpson KL,Clinical evaluation of M30, M65 ELISA cell death assays as circulating biomarkers in a drug-sensitive tumor, testicular cancer. Neoplasia 10:1041–1048PubMed
17.
Jemal A, Siegel R, Ward E, Hao Y, Xu J, Thun MJ (2009) Cancer statistics 2009. CA Cancer J Clin 59:225–249PubMedCrossRef
18.
Desai AM, Pareek M, Nightingale PG, Fielding JW (2004) Improving outcomes in gastric cancer over 20 years. Gastric Cancer 7:196–201PubMedCrossRef
19.
Galizia G, Lieto E, Orditura M et al (2007) Epidermal growth factor receptor (EGFR) expression is associated with a worse prognosis in gastric cancer patients undergoing curative surgery. World J Surg 31:1458–1468PubMedCrossRef
20.
Kim JG, Sohn SK, Chae YS et al (2007) Vascular endothelial growth factor gene polymorphisms associated with prognosis for patients with gastric cancer. Ann Oncol 18:1030–1036PubMedCrossRef
21.
Abe T, Fukumoto M, Tsuchiya K et al (1989) Human monoclonal antibodies against cytokeratin 18 generated from patients with gastric cancer. Jpn J Cancer Res 80:271–276PubMed
22.
Xu W, Zhang MW, Huang J, Wang X, Xu SF, Li Y, Wang SJ (2005) Correlation between CK18 gene, gastric carcinoma micrometastasis. World J Gastroenterol 11:6530–6534PubMed
23.
Greene FLPD, Fleming ID (2002) American joint committee on cancer staging manual, 6th edn. Springer, Philadelphia
24.
Wu YX, Wang JH, Wang H, Yang XY (2003) Study on expression of Ki-67, early apoptotic protein M30 in endometrial carcinoma, their correlation with prognosis (article in Chinese). Zhonghua Bing Li Xue Za Zhi 32:314–318 (article in Chinese)PubMed
25.
Hou JM, Greystoke A, Lancashire L et al (2009) Evaluation of circulating tumor cells, serological cell death biomarkers in small cell lung cancer patients undergoing chemotherapy. Am J Pathol 175:808–816PubMedCrossRef
26.
Ausch C, Buxhofer-Ausch V, Olszewski U, Schiessel R, Ogris E, Hinterberger W, Hamilton G (2009) Circulating cytokeratin 18 fragment m65-a potential marker of malignancy in colorectal cancer patients. J Gastrointest Surg 13:2020–2026PubMedCrossRef
Metadata
Title
Is there any impact of plasma M30 and M65 levels on progression-free survival of patients with advanced gastric cancer?
Authors
Ahmet Bilici
Bala Basak Oven Ustaalioglu
Serif Ercan
Asuman Orcun
Mesut Seker
Taflan Salepci
Mahmut Gumus
Publication date
01-08-2011
Publisher
Springer-Verlag
Published in
Cancer Chemotherapy and Pharmacology / Issue 2/2011
Print ISSN: 0344-5704
Electronic ISSN: 1432-0843
DOI
https://doi.org/10.1007/s00280-010-1480-0

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