| Literature DB >> 24886074 |
Nelma Pértega-Gomes, José R Vizcaíno, Jan Attig, Sarah Jurmeister, Carlos Lopes, Fátima Baltazar1.
Abstract
BACKGROUND: In a malignant tumour, cancer cells are embedded in stromal cells, namely cancer-associated fibroblasts (CAFs). These CAFs are now accepted as important players in cancer dynamics, being involved in tumour growth and progression. Although there are various reports on the interaction between tumour and stromal cells, the clinico-pathological significance of this cross-talk is still largely unknown. In this study, we aimed to characterise the expression of key metabolic proteins involved in glucose transport, pyruvate/lactate shuttle system, glycolytic metabolism and fatty acid oxidation in CAFs and tumour cells in different stages of malignant transformation. We further aimed to contextualise the clinico-pathological significance of these protein expression profiles with reference to known prognostic indicators, including biochemical recurrence in pT stage.Entities:
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Year: 2014 PMID: 24886074 PMCID: PMC4039335 DOI: 10.1186/1471-2407-14-352
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Details of the immunohistochemical procedure used to analyze the expression of the different proteins
| sc-50329 | Santa Cruz Biotechnology | 1:500 | Colon tumor | Overnight | R.T.U. Vectastain Universal Elite ABC Kit, Vector, EUA | |
| ab 15309 | Abcam | 1:2000 | Head and neck tumor | 2 hours | Ultravision Detection System Anti-polyvalent, HRP, Labvision Corporation, Freemont, CA | |
| ab 15086 | Abcam | 1:2000 | Stomach | |||
| sc-365501 | Santa Cruz Biotechnology | 1:500 | Colon tumor | Overnight | R.T.U. Vectastain Universal Elite ABC Kit, Vector, EUA | |
| ab 75441 | Abcam | 1:500 | Kidney | Overnight | | |
| ab 53010 | Abcam | 1:1000 | Colon tumor | | | |
| ab 110025 | Abcam | 1:500 | Stomach | | | |
| 504R-16 | Cell Marque | 1:50 | Kidney | | | |
| sc-135435 | Santa Cruz Biotechnology | 1:250 | Liver | 2 hours | Ultravision Detection System Anti-polyvalent, HRP, Labvision Corporation, Freemont, CA | |
| DBP antibody was a gift from Dr. Gabriele Moller from HelmholtzZentrum mÜnchen | Ready to use | Kidney | ||||
Figure 1Comparison between metabolism-related proteins expression in tumour cells and cancer associated fibroblasts (CAFs).
Figure 2Stacked bar graph according to one protein column within each fibroblast group for MCT4, PDK1 and CAIX expression. The stronger expression (3) is represented by the more intense colour.
Figure 3Immunohistochemical staining for MCT1, MCT4, PDK1 and CAIX expression in non-neoplastic tissue (NNT), PIN lesions (PIN), tumour tissue (TT) and the surrounding stroma for each case. Strong expression of MCT4, PDK1 and CAIX in stromal cells is evident, in contrast with MCT1, which is present only in the epithelial cells of the glands.
Correlations between the key metabolic-related proteins MCT4, PDK1 and CAIX expressions in CAFs and clinico-pathological data
| | | ||||||||
|---|---|---|---|---|---|---|---|---|---|
| | | 0.296 | | 0.451 | | 0.250 | | 0.525 | |
| ≤ 5.0 | 245 | 47.9 | | 16.2 | | 85.9 | | 27.1 | |
| >5.0 | 123 | 44.0 | | 17.5 | | 82.2 | | 27.5 | |
| | | 0.445 | | 0.258 | | 0.522 | | ||
| 2 | 359 | 40.2 | | 18.7 | | 86.4 | | 20.8 | |
| 3 | 99 | 41.7 | | 15.2 | | 86.9 | | 33.3 | |
| | | | | | | | | | |
| | | 0.155 | | 0.069 | | 0.399 | | 0.255 | |
| Absent | 119 | 45.4 | | 13.4 | | 85.8 | | 26.9 | |
| Present | 327 | 39.4 | | 19.8 | | 87.2 | | 23.3 | |
| | | | | | | | | | |
| | | 0.104 | | 0.176 | | | 0.052 | ||
| Absent | 410 | 40.2 | | 18.5 | | 75.4 | | 22.6 | |
| Present | 69 | 49.3 | 13.0 | 89.0 | 32.8 | ||||
The correlation between MCT1/MCT4 expression (*MCT1 expression in prostate tumour cells with concomitant expression of MCT4 in CAFs) and the clinico-pathological data is also presented.
Figure 4Schematic representation of the lactate shuttle system between malignant cells and cancer associated fibroblasts (CAFs). The expression of MCT4 in CAFs together with the expression of MCT1 in tumour cells is associated with biochemical recurrence after surgery and pT3 stage of the tumour.