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Journal of Orthopaedic Surgery and Research
Erschienen in: Journal of Orthopaedic Surgery and Research 1/2019

Open Access 01.12.2019 | Research article

Transferrin receptor-1 and VEGF are prognostic factors for osteosarcoma

verfasst von: Hongzeng Wu, Jinming Zhang, Ruoheng Dai, Jianfa Xu, Helin Feng

Erschienen in: Journal of Orthopaedic Surgery and Research | Ausgabe 1/2019

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Abstract

Background

Osteosarcoma is aggressive and prognostic biomarkers are important to predict the outcomes of surgery and chemotherapy. Here, we investigated the potential of transferrin receptor-1 (TfR1) and vascular endothelial growth factor (VEGF) as prognostic markers of osteosarcoma.

Methods

TfR1 and VEGF in osteosarcoma samples from a cohort of 53 osteosarcoma patients were detected by immunohistochemistry analysis. The correlation of TfR1 and VEGF levels with clinicopathological parameters was analyzed by Pearson chi-square and Spearman-rho tests. Overall patient survival was analyzed by the Kaplan-Meier method.

Results

We found that TfR1 and VEGF expression levels were low in 20.8% and 18.9%; modest in 35.8% and 35.8%; and high in 43.4% and 45.3% of osteosarcoma patients, respectively. TfR1 and VEGF expression was significantly correlated to histologic grade, Enneking stage, and distant metastasis. TfR1 expression was significantly correlated to VEGF expression and both TfR1 expression and VEGF expression were correlated to shorter overall survival.

Conclusions

TfR1 and VEGF are potential prognostic factors for osteosarcoma.
Hinweise

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Background

Primary bone tumors are uncommon and the incidence is low [1]. Osteosarcoma (OS) is a pleomorphic sarcoma of the bone in children and adult, and OS patients frequently develop metastasis [2]. With the recent development of adjuvant chemotherapy, the 5-year-free survival rate has improved to approximately 50% for patient with high-grade OS [3, 4]. The identification of new prognostic biomarkers in osteosarcoma has become increasingly important to predict the responsiveness of treatment [5].
Iron is an element essential to cellular activities such as DNA synthesis and cell proliferation [68]. Proteins involved in iron metabolism have been shown to promote lung cancer [911]. Recent studies have shown high expression of transferrin receptor-1 (TfR1) in a variety of tumors including lung, breast, and bladder cancer as well as malignant glioma, but the clinical significance of TfR1 in tumor remains to be confirmed [12, 13].
Angiogenesis plays an important role in tumor development. Vascular endothelial growth factor (VEGF) is known to promote neovascularization [14, 15]. Up to now, the association between TfR1 and VEGF expression and the prognosis of OS patients remains unclear. Therefore, this study aimed to examine TfR1 and VEGF expression in OS patients and analyze their prognostic significance for clinical outcomes of OS.

Methods

Subjects

Ethics Committees of the Fourth Hospital of Hebei Medical University (also named as Tumor Hospital of Hebei Province) approved this study and all patients signed written informed consent. This study enrolled 53 OS patients from 2002 to 2010 from the Fourth Hospital of Hebei Medical University, who had not received radiotherapy or chemotherapy. All patient data and follow-up information were collected, including the gender, age, tumor size, histological grade, Enneking stage, and distant metastasis.

Immunohistochemistry analysis

Immunohistochemistry (IHC) analysis was performed on OS tissues using antibodies for TfR1 (1:100; Biogot Tech) and VEGF (1:100; Santa Cruz Biotechnology), following a previously described protocol [16]. The results of IHC were judged using the following score system based on the percentage of stained cells, < 1% (0); 1–25% (1); 25–50% (2); 51–80% (3); and > 80% (4); and the intensity of staining, no staining (0); weak staining (1); strong staining (2); and very strong staining (3). The final score was the product of staining intensity and percentage and judged as low (0–3 points), mild (4–7 points), and high (> 7 points).

Statistical analysis

All data were analyzed by using SPSS software 25.0. The association of clinical variables was analyzed by the Pearson chi-square test or Spearman-rho test. Univariate and multivariate analyses were performed by using the Cox proportional hazard model. Survival was analyzed by the Kaplan-Meier method. P < 0.05 was considered significant.

Results

Association of TfR1 and VEGF with clinicopathological parameters

Typical staining of TfR1 and VEGF in OS tissues was presented in Fig. 1. TfR1 expression was low in 20.8%, mild in 35.8% and high in 43.4% of OS tissues, whereas VEGF expression was low in 18.9%, mild in 35.8%, and high in 45.3% of OS tissues. As shown in Table 1, TfR1 and VEGF expression was significantly associated with histological grade, Enneking stage and distant metastasis (all P < 0.05). In addition, TfR1 and VEGF expression showed a significantly positive correlation (P < 0.01, Table 2).
Table 1
Clinicopathological variables and the expression of TfR1 and VEGF
 
TfR1
P
VEGF
P
Low(%)
Mild(%)
High(%)
Low(%)
Mild(%)
High(%)
Sex
Female
25
3(12.0)
10(40.0)
12(48.0)
0.332
5(20.0)
11(44.0)
9(36.0)
0.405
 
Male
28
8(28.6)
9(32.1)
11(39.3)
5(17.8)
8(28.6)
15(53.6)
Age
≥ 20 years
18
4(22.2)
4(22.2)
10(55.6)
0.306
3(16.7)
9(50.0)
6(33.3)
0.293
 
< 20 years
35
7(20.0)
15(42.9)
13(37.1)
7(20.0)
10(28.6)
18(51.4)
Tumor size
< 5 cm
27
6(22.2)
10(37.0)
11(40.8)
0.919
6(22.2)
10(37.0)
11(40.7)
0.741
 
≥ 5 cm
26
5(19.2)
9(34.6)
12(46.2)
4(15.4)
9(34.6)
13(50.0)
Histologic grade*
I
15
4(26.7)
8(53.3)
3(20.0)
0.04
4(26.7)
9(60.0)
2(13.3)
0.02
 
II
25
5(20.0)
10(40.0)
10(40.0)
5(20.0)
8(32.0)
12(48.0)
 
III
13
2(15.4)
1(7.7)
10(76.9)
1(7.7)
2(15.4)
10(76.9)
Distant metastasis*
Yes
23
1(4.2)
11(47.8)
11(47.8)
0.029
1(4.4)
13(56.5)
9(39.1)
0.008
 
No
30
10(33.3)
8(26.7)
12(40.0)
9(30.0)
6(20.0)
15(50.0)
Enneking staging*
I
12
8 (66.7)
3 (25.0)
7(36.9)
< 0.001
6(50.0)
4(33.3)
2(16.7)
0.004
 
II
19
2 (10.5)
10(52.6)
21(43.8%)
 
2(10.5)
10(52.6)
7(36.9)
 
 
III
22
1 (4.5)
6 (27.3)
15 (68.2)
 
2(9.1)
5(22.7)
15(68.2)
 
Pearson’s chi-squared test was used. *P < 0.05
Table 2
The correlation of TfR1 and VEGF expression
Characteristics
TfR1
P (Spearman)
Low(%)
Mild(%)
High(%)
VEGF*
Low
10
6(11.3)
3(5.7)
1(1.9)
= 0.001
Mild
19
2(3.7)
10(18.9)
7(13.2)
High
24
3(5.7)
6(11.3)
15(28.3)
  
53
11
19
23
 
Spearman-rho test was used. *P < 0.05

TfR1 and VEGF were correlated with poor overall survival of OS patients

Table 3 showed the results of univariate Cox hazard analysis of overall survival of OS patients. Kaplan-Meier survival curve showed that the gender, age, tumor size, and histologic grade had no significance in predicting overall survival, but Enneking staging and distant metastasis predicted a poor overall survival (Fig. 2). Moreover, TfR1 and VEGF were significantly correlated with poor overall survival (Table 3, Fig. 2).
Table 3
Clinicopathological factors associated with overall survival based on univariate Cox proportional regression analysis
Characteristics
Overall survival
P
HR
95% CI
Sex
Female
25
1
 
0.837
 
Male
28
1.064
0.590–1.919
Age
≥ 20 years
18
1
 
0.777
 
< 20 years
35
1.093
0.591–2.022
Tumor size
< 5 cm
27
1
 
0.940
 
≥ 5 cm
26
1.024
0.556–1.884
Histologic grade*
I
15
1
 
0.412
 
II
25
1.267
0.634–2.534
0.503
 
III
13
1.738
0.771–3.917
0.183
Distant metastasis*
Yes
23
1
 
< 0.001
 
No
30
0.161
0.073–0.356
Enneking staging*
I
12
1
 
< 0.001
 
II
19
8.605
2.942–25.169
 
III
22
26.039
7.679–88.293
TfR1*
Low
11
1
 
< 0.001
 
Moderate
19
0.158
0.063–0.398
 
High
23
0.300
0.143–0.629
VEGF*
Low
10
1
 
0.021
 
Moderate
19
0.114
0.043–0.303
 
High
24
0.422
0.202–0.880
HR, hazard ratio; 95% CI, 95% confidence interval. *P < 0.05

TfR1 and VEGF are prognostic factors for OS patients

Table 4 showed the results of multivariate Cox hazard analysis of univariate factors listed in Table 3. Enneking staging, TfR1 expression, and VEGF expression were identified as independent prognostic factors of OS patients. Higher TfR1 and VEGF expression, higher Enneking staging, and distance metastasis were associated with significantly higher mortality risk (Plogrank < 0.001) (Fig. 2).
Table 4
Clinicopathological factors associated with overall survival based on multivariate Cox regression analysis
 
Overall survival
 
HR
95% CI
P
Enneking stage
4.622
2.541–8.406
< 0.001
TfR1
2.514
1.445–4.372
0.001
VEGF
2.882
1.203–8.217
0.002
HR, hazard ratio; 95% CI, 95% confidence interval. *P < 0.05

Discussion

As a common malignant bone tumor, OS accounts for 30% of all bone malignancies and 3–4% of pediatric tumors [17]. OS has been reported to be the third most common cancer in adolescence [18]. Therefore, it is important to identify novel biomarkers and therapeutic targets for OS.
Abnormal iron metabolism is associated with tumorigenesis [1921]. Iron homeostasis is maintained by the balance of iron uptake, usage, and storage [22]. TfR1 is the main protein responsible for iron absorption. Strong immunohistochemical staining of TfR1 could indicate high cancer cell proliferation and poor prognosis of cancer patients [2325]. Tumor cells with high TfR1 expression exhibited a high rate of iron absorption and cell proliferation [26].
To our knowledge, our study was the first to report high expression of TfR1 and VEGF in OS tissues. Moreover, we found that high TfR1 and VEGF expression was significantly correlated to histological grade, Enneking staging, and distant metastasis. Furthermore, high TfR1 and VEGF expression was significantly correlated to poor overall survival, and both TfR1 and VEGF were independent prognostic indicators of OS patients.
Our study has several limitations. First, immunohistochemistry analysis is only semi-quantitative, and bias may affect the evaluation of staining score although we analyzed all samples in a blind manner. Second, our sample size is limited. Third, our study is a single-center study.

Conclusions

In summary, TfR1 and VEGF expression is high in OS tissues and is correlated to malignancy grade of OS patients. TfR1 and VEGF are potential prognostic factors of OS patients.

Acknowledgements

N/A
Ethics Committees of the Fourth Hospital of Hebei Medical University approved this study and all patients signed written informed consent.
Yes

Competing interests

All authors declare no conflicts of interest.
Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://​creativecommons.​org/​licenses/​by/​4.​0/​), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://​creativecommons.​org/​publicdomain/​zero/​1.​0/​) applies to the data made available in this article, unless otherwise stated.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
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Metadaten
Titel
Transferrin receptor-1 and VEGF are prognostic factors for osteosarcoma
verfasst von
Hongzeng Wu
Jinming Zhang
Ruoheng Dai
Jianfa Xu
Helin Feng
Publikationsdatum
01.12.2019
Verlag
BioMed Central
Erschienen in
Journal of Orthopaedic Surgery and Research / Ausgabe 1/2019
Elektronische ISSN: 1749-799X
DOI
https://doi.org/10.1186/s13018-019-1301-z

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