| Literature DB >> 26674738 |
Xiaotong Sun1, Zhongtian Jin2, Xiao Song3, Jingjing Wang4, Yan Li5, Xiaoping Qian6, Yu zhang7, Yanhui Yin8.
Abstract
BACKGROUND: KIF23 (kinesin family member 23) is a kinesin-like motor protein and plays an important role in cytokinesis. In search for genes associated with hepatocellular carcinoma (HCC) by cDNA microarray, we found that KIF23 was upregulated in HCC tissues. At present, much less is known about its expression and functions in tumor cells. In this work, we aimed to investigate the expression of KIF23 in HCC and the correlation between its expression and clinical features.Entities:
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Year: 2015 PMID: 26674738 PMCID: PMC4682286 DOI: 10.1186/s12885-015-1987-1
Source DB: PubMed Journal: BMC Cancer ISSN: 1471-2407 Impact factor: 4.430
Fig. 1Expressions of KIF23 V1 and KIF23 V2 mRNA in normal and malignant tissues. a Expressions of KIF23 V1 and KIF23 V2 mRNAs in normal tissues. Lane 1: heart; 2: liver; 3: skeletal muscle; 4: pancreas; 5: ovary; 6: colon; 7: PBMC; 8: placenta; 9: lung; 10: kindey; 11: spleen; 12: thymus; 13: prostate; 14: small intestine. b Representative positive expressions of KIF23 V1 and KIF23 V2 mRNA in some HCC tissues. T: cancerous tissues; A: adjacent noncancerous tissues. c Expressions of KIF23 V1 and KIF23 V2 mRNA in HCC cell lines. Lane 1: HLE; 2: SMMC-7721; 3: BEL-7402; 4: Huh7; 5: HepG2; N: negative control
Fig. 2Characterization of anti-KIF23 V1 antibody. a HEK293T cells were transiently transfected with pRK-FLAG-KIF23 V1, pRK-FLAG-KIF23 V2, or pRK-FLAG plasmids and the protein expression was detected by Western blotting employing anit-KIF23 V1 antibody. b Western blotting analysis of the same samples as in (a) was performed with commercial anti-KIF23 antibody. c HLE cells were transfected with either control or KIF23 V1 siRNAs and whole cell extracts were processed for immunoblotting with anti-KIF23 V1 antibody. d Western blotting analysis of the same samples as in (c) was performed with commercial anti-KIF23 antibody. All the membranes were reblotted for the expression of tubulin
Fig. 3Subcellular distribution of endogenous KIF23 V1 protein. a Localization of KIF23 V1 in HLE and Huh7 cells examined by immunofluorescence. Cells grown on coverslips were fixed and immunostained with polyclonal anti-KIF23 V1 antibody, followed by detection with FITC-conjugated anti-rabbit IgG secondary antibody. b Subcellular localization of KIF23 V1 examined by cell fractionation and Western blotting. HLE cells were separated into nuclear and cytoplasmic fractions. Equal amounts of proteins were loaded onto SDS-PAGE gels, and the protein expression was analyzed with anti-KIF23 V1, anti-tubulin (cytoplasmic marker), or anti-lamin B1 (nuclear marker) antibodies
Fig. 4Expressions of KIF23 V1 and KIF23 V2 protein in HCC tissues. a Representative images of KIF23 V1 staining in HCC tissues. i: A strong stained HCC sample (H-score of 290). ii: A moderately stained HCC sample (H-score of 130). iii: A weakly stained HCC sample (H-score of 60). iiii: A negative stained HCC sample (H-score of 0). Magnification: 1:200. b Representative images of KIF23 V2 staining in HCC tissues. i: A strong stained HCC sample (H-score of 260). ii: A moderately stained HCC sample (H-score of 125). iii: A weakly stained HCC sample (H-score of 40). iiii: A negative stained HCC sample (H-score of 0). Magnification: 1:200. c Histograms showing the distribution and frequency for KIF23 V1 expression in HCC tissues. d Histograms showing the distribution and frequency for KIF23 V2 expression in HCC tissues
Fig. 5Association between KIF23 V1 or KIF23 V2 protein expression and overall survival (OS) of HCC patients. Correlation of KIF23 V1 expression with 3-year (a) or 5-year (b) OS of HCC patients. Correlation of KIF23 V2 expression with 3-year (c) or 5-year (d) OS of HCC patients. The group with expression of KIF23 V1 showed significantly better survival than the group without expression of KIF23 V1 (p = 0.0052). Patients were categorized by the median H-scores of KIF23 V2 (60) or by KIF23 V1 expression or not
Prognostic factors for survival
| Variable | OS | ||
|---|---|---|---|
| Univariate | Multivariate | ||
| HR (95 % CI) | |||
| Gender (Male versus Female) | NS | NA | |
| Age (≤55 vs. >55) | NS | NA | |
| Size (≤5 cm vs. >5 cm) | 0.0186 | NS | |
| TNM stage (I, II vs. III, IV) | 0.0040 | 1.502 (1.121-2.014) | 0.0059 |
| KIF23 V2 (≤60 vs. >60) | NS | NA | |
| KIF23 V1 (negative vs. positive) | 0.0097 | NS | |
Univariate analysis: χ2 test
Multivariate analysis: Cox proportional hazards regression model
Abbreviations: OS Overall survival, HR Hazard Ratio, CI confidence interval, TNM tumor-node-metastasis, NA not adopted, NS not significant