| Literature DB >> 23321514 |
Y Li1, J Wu, W Zhang, N Zhang, H Guo.
Abstract
BACKGROUND: Early serum detection is of critical importance to improve the therapy for hepatocellular carcinoma (HCC), one of the most deadly cancers. Hepatitis infection is a leading cause of HCC.Entities:
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Year: 2013 PMID: 23321514 PMCID: PMC3553511 DOI: 10.1038/bjc.2012.494
Source DB: PubMed Journal: Br J Cancer ISSN: 0007-0920 Impact factor: 7.640
Figure 1Identification of CCL15 in HCC patient serum. (A) Differential expression of the SELDI peaks in the comparisons of four groups. a: the sample from mixture of healthy controls; b: the sample from mixture of benign diseases (liver cirrhosis or hepatitis); c: the sample from mixture of HBV-HCC; and d: the sample from mixture of HBV-HCC after immunodepression assay using CCL15 antibody. P1-P7 shows different peptides or proteins. (B) Isolation of the 7777.27 M/Z peak. Arrow indicates the band of 7777.27 M/Z protein. a: marker; b: sample from mixture of HCC. (C) The 7777.27 M/Z protein-matched CCL15 protein (MW=7773.10 M/Z, pI=9) with two consistent sequences (Score=61).
Comparative content of seven different proteins at M/Z in WCX-2
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| P1 | 6489.48 | 19.77±3.54 | 6.46±2.18 | 6.87±2.30 |
| P2 | 6662.34 | 22.82±4.15 | 9.96±2.93 | 8.06±2.47 |
| P3 | 7777.27 | 4.09±1.14 | 6.87±2.18 | 15.87±4.30 |
| P4 | 8593.75 | 11.45±2.73 | 2.13±0.89 | 3.21±1.21 |
| P5 | 8720.23 | 13.69±2.30 | 4.57±2.12 | 4.32±2.89 |
| P6 | 9250.00 | 4.51±1.32 | 4.87±1.82 | 23.15±3.81 |
| P7 | 16200.17 | 8.83±2.76 | 26.72±4.51 | 7.63±2.48 |
Abbreviations: HCC=hepatocellular carcinoma; WCX-2=weak cationic exchange.
Benign diseases include liver cirrhosis and hepatitis B.
This value was significantly higher than that in the other two groups (P<0.01).
Figure 2The expression of CCL15 in liver tissues and sera, and its comparison with AFP as a proteomic biomarker. (A) Immunohistochemical staining of CCL15 expression in HCC tissues and adjacent liver tissues. The positive signals for CCL15 were observed in brown. No positive signal of CCL15 was detected in adjacent normal liver tissues. (B) Western blotting analysis of CCL15 expression in HBV-HCC sera and liver cirrhosis sera. Arrow indicates that CCL15 were observed in HCC. a, b: sample from two batches of mixture of liver cirrhosis; c,d; sample from two batches of mixture of HCC; (C) Receiver operation characteristic (ROC) curves in patients with B-related HCC and B-hepatitis.
The expression of CCL15 in the liver tissues
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| Normal | 50 | 1 (2.00) | 0.12±0.13 |
| Adjacent cancer | 80 | 16 (20.00) | 0.55±1.23 |
| HCC | 80 | 64 (80.00) | 2.25±1.29 |
Abbreviation: CCL15=C-C motif chemokine 15.
Normal vs hepatocellular carcinoma (HCC); P<0.05.
Adjacent cancer vs normal, P>0.05.
Adjacent cancer vs HCC, P<0.05.
The relationship between clinicopathological data of patients with HCC and the serum levels of CCL15
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| Total (before treatment) (55) | 26.6±1.2 |
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| Poorly differentiated (15) | 30.3±2.2 |
| Moderately differentiated (20) | 24.3±0.6 |
| Well differentiated (20) | 19.1±0.6 |
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| ⩾3 cm (35) | 27.6±1.2 |
| <3 cm (20) | 19.6±2.1 |
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| Yes (30) | 27.9±3.6 |
| No (25) | 20.6±1.1 |
| After treatment | 9.7 ±1.2 |
| Operation (25) | 9.9±0.8 |
| Arterial embolization (20) | 10.0±1.4 |
| Percutaneous tumour ablation (10) | 9.0±1.6 |
| Healthy controls (60) | 1.2±0.1 |
Abbreviations: CCL15=C-C motif chemokine 15; HCC=hepatocellular carcinoma.
Showed P<0.05 between poorly differentiated and well differentiated.
Showed P<0.05 between tumour size ⩾3 and <3 cm.
Showed P<0.05 between patients with metastasis and without metastasis.
Showed P<0.05 between patients before and after treatments.
Differential levels of CCL15 in various groups
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| B-related HCC (55) | 26.6±1.2 |
| C-related HCC (25) | 23.9±3.1 |
| Lung cancer (15) | 4.3±1.7 |
| Gastric cancer (15) | 4.1±0.5 |
| Carcinoma of gallbladder (15) | 3.6±1.5 |
| Benign diseases (65) | 2.0±0.9 |
| Healthy controls (60) | 1.2±0.1 |
Abbreviations: CCL15=C-C motif chemokine 15; HCC=hepatocellular carcinoma.
Showed P>0.05 between B-related HCC and C-related HCC.
Showed P<0.05 between B-related HCC and lung cancer.
Showed P<0.05 between B-related HCC and gastric cancer.
Showed P<0.05 between B-related HCC and carcinoma of gallbladder.
Showed P<0.05 between B-related HCC and benign diseases.
Showed P>0.05 between benign diseases and healthy controls.
Showed P<0.05 between B-related HCC and healthy controls.
Figure 3Effects of CCL15 on hepatocarcinoma cells chemotaxis and migration. (A) Chemotaxis assay of three kinds of hepatocarcinoma cells with indicated amount of CCL15 as chemoattractant for 6 h. (B) RT–PCR and western blotting analysis of CCL15 in Huh-7, HLE and HepG2 cells. (C) Wound-healing assay of the three kind of hepatocarcinoma cells. Wound widths were recorded at indicated time points. ***P<0.0005. (D) Wound-healing assay of HLE cells with or without CCL15 (1 nℳ) treatment. ***P<0.005.
Figure 4Downregulation of CCL15 impaired HepG (A) Western blotting analysis of HepG2 cells and its clones with downregulation of CCL15. (B) Wound-healing assay of HepG2 cells and siCCL15/HepG2 cells at indicated time points. (C) Invasion assays of HepG2 cells and siCCL15/HepG2 cells. CCL15 coated in Matrigel-enhanced HepG2/siClone2 cells invasive ability, with pictures shown ( × 200; *P<0.05, **P<0.005).