| Literature DB >> 34188681 |
Zhenyu Zhang1, Minghui Chang1, Xingguo Song1, Kangyu Wang1, Wenjuan Sun2, Hongxin Ma1, Xiaohui Yan3, Yuhong Sun4, Xianrang Song1,5, Li Xie1.
Abstract
TIPE1, a newly identified member in TIPE (TNFAIP8) family, plays an important role in tumorigenesis and immune regulation, but its role in ovarian cancer, especially in tumor metastasis, remains unknown. In the current study, we aimed to reveal the protein expression spectrum of TIPE1 in normal human tissues and explored its relationship with metastasis in ovarian cancer. The results of IHC staining showed that TIPE1 protein was not only detected in cytoplasm in most human tissues but also expressed in both cytoplasm and nucleus in squamous epithelium and some epithelial-derived cells with secretory functions, such as esophagus, cervix uteri and ovary, and thyroid gland. Moreover, TIPE1 protein was downregulated in ovarian cancer tissues compared with that in the paracancerous. More importantly, TIPE1 suppressed tumorigenesis and metastasis of ovarian cancer in vitro and in vivo, as evidence shows its ability to suppress growth, colony formation, migration, and epithelial-mesenchymal transition (EMT) of ovarian cancer. Taken together, our results demonstrate the suppressor role of TIPE1 in ovarian cancer metastasis, indicating TIPE1 might be a metastasis predictor and a novel therapeutic target for ovarian cancer.Entities:
Year: 2021 PMID: 34188681 PMCID: PMC8195659 DOI: 10.1155/2021/5538911
Source DB: PubMed Journal: J Oncol ISSN: 1687-8450 Impact factor: 4.375
TIPE1 protein expression in normal human tissues.
| Tissues | Positive cells | TIPE1 expression | |
|---|---|---|---|
| Cytoplasm | Nucleus | ||
| Esophagus | Stratified squamous epithelium | +++ | ++ |
| Stomach | Simple columnar epithelium | + | ± |
| Parietal cells | ++ | + | |
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| |||
| Duodenum | Simple columnar epithelium | + | ± |
| Jejunum | Simple columnar epithelium | + | ± |
| Ileum | Simple columnar epithelium | + | ± |
| Appendix | Simple columnar epithelium | + | ± |
| Colon | Simple columnar epithelium | + | ± |
| Plasma cells | ++ | ± | |
|
| |||
| Rectum | Simple columnar epithelium | + | ± |
| Liver | Hepatocytes | ++ | ± |
| Bile canaliculus | +++ | ± | |
|
| |||
| Pancreas | Islet cells | +++ | ± |
| Trachea | Pseudostratified ciliated columnar epithelium | ++ | ++ |
| Lung | Alveolar epithelial cells | + | + |
| Dust cells | ++ | ± | |
| Myocardium | Myocardial cells | ++ | ± |
| Artery wall | Smooth muscle cells | ± | ± |
| Skeletal muscle | Skeletal muscle cells | ++ | ± |
| Telencephalon | Neurons | + | + |
| Medulla oblongata | Neurons | + | + |
| Cerebellum | Neurons | ± | ± |
| Testis | Spermatogenic epithelium | + | ± |
| Seminal vesicle | Pseudostratified columnar epithelium | ++ | +++ |
| Prostate | Epithelium | + | ± |
| Cervix uteri | Stratified squamous epithelium | ++ | ++ |
| Endometrium | Uterine gland | + | + |
| Ovary | Corpus luteum | +++ | +++ |
| Skin | Stratified squamous epithelium | ++ | ++ |
| Urinary bladder | Transitional epithelium | ++ | ± |
| Spleen | Lymphoid tissue | ± | ± |
| Thyroid gland | Follicular epithelial cells | + | + |
| Breast | Acinar cells | ++ | ++ |
Figure 1TIPE1 was significantly decreased in ovarian cancer and negatively correlated with tumor metastasis. (a) Relative mRNA levels of TIPE1 in ovarian cancer tissues (n = 18) and non-cancer tissues (n = 10). (b) Immunohistochemistry score analysis of TIPE1 expression in ovarian cancer tissues (n = 281) and non-cancer tissues (n = 89). (c) Immunohistochemistry score analysis of TIPE1 expression in metastatic ovarian cancer tissues (n = 179) and non-metastatic ovarian cancer tissues (n = 102). (d) Representative photographs of TIPE1 IHC staining in ovarian cancer tissues and ovarian stroma tissues. Scale bar = 50 μm. (e) Representative photographs of TIPE1 IHC staining in metastatic ovarian cancer tissues and non-metastatic ovarian cancer tissues. Scale bar = 50 μm.
Characteristics of 281 ovarian cancer patients.
| Clinical characteristics | No. of cases | TIPE1 expression (median ± SD) |
|
|---|---|---|---|
|
| |||
| <60 years | 203 | 112.4 ± 26.43 | 0.9617 a |
| ≥60 years | 74 | 111.7 ± 27.22 | |
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| ≤5 cm | 55 | 104.3 ± 30.00 | 0.0833 a |
| >5 cm | 187 | 114.2 ± 26.44 | |
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| Serous | 186 | 111.5 ± 27.00 | 0.5528 b |
| Mucinous | 52 | 113.5 ± 27.96 | |
| Endometrioid | 21 | 118.0 ± 26.63 | |
| Clear cell | 19 | 113.5 ± 23.29 | |
| Squamous | 3 | 123.8 ± 19.81 | |
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| Absent | 179 | 116.1 ± 24.08 | <0.0001 b |
| Present | 102 | 102.2 ± 28.75 | |
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| Well | 42 | 115.7 ± 24.72 | 0.2968 b |
| Moderate | 78 | 110.3 ± 31.83 | |
| Poor | 161 | 112.8 ± 24.6 | |
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| Stage I | 17 | 109.1 ± 20.53 | 0.3252 b |
| Stage II | 45 | 112.1 ± 30.40 | |
| Stage III | 109 | 112.2 ± 27.48 | |
| Stage IV | 37 | 115.1 ± 20.09 | |
aUnpaired t-test (two-tailed). bOne-way ANOVA test.
Figure 2TIPE1 inhibited migration of ovarian cancer cells. (a) The expression of TIPE1 was detected by western blot in ES2 and SKOV3 cells after transfecting lentivirus as indicated. (b) EMT related proteins including E-cadherin, N-cadherin, Slug, and Snail were detected by western blot in ES2 and SKOV3 cells after transfecting lentivirus as indicated. (c) Wound healing assay was performed to determine the migration properties of ES2 and SKOV3 cells. Transwell assay was performed to determine the migration properties of ES2 and SKOV3 cells. Scale bar = 200 μm.
Figure 3TIPE1 inhibited growth of ovarian cancer cells in vitro. (a) Real-time PCR was performed to detected mRNA level of TIPE1 after transfecting lentivirus as indicated. (b) Cell growth curve of A2780, ES2, and SKOV3 cells transfected with TIPE1 and control lentivirus. (c) Colony formation analysis of A2780, ES2, and SKOV3 cells transfected with TIPE1 and control lentivirus. (d) Caspase3, cl-Caspase9, and cl-Caspase3 were detected by western blot in ES2 and SKOV3 cells after transfecting lentivirus as indicated. The results are presented as mean ± SD; p < 0.05, p < 0.01, p < 0.001.
Figure 4TIPE1 inhibited growth of ovarian cancer in vivo. (a) Photograph of tumors in mice that were injected subcutaneously with SKOV3 cells stably transfected with TIPE1 lentivirus or control lentivirus. (b, c) The average tumor weight and tumor volume in each group over a period of 19 days. The results are presented as mean ± SD; p < 0.001.