Identification and Validation of Chromobox Family Members as Potential Prognostic Biomarkers and Therapeutic Targets for Human Esophageal Cancer

Fang, Xuefen; Wang, Junjun; Chen, Jiabing; Zhuang, Mingkai; Huang, Tao; Chen, Zhuo; Huang, Yanlei; Zheng, Biyun; Wang, Xiaozhong

doi:10.3389/fgene.2022.851390

Cited by 3 publications

(5 citation statements)

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“…In this study, we found that USP15 was highly expressed in breast cancer by searching the TCGA databases [ 32 , 54 ]. Then by searching the bioinformatics database UALCAN, GEPAI, Kaplan-Meier we.…”

Section: Discussionmentioning

confidence: 99%

A Regulatory Network Analysis of the Importance of USP15 in Breast Cancer Metastasis and Prognosis

Ling

Qin

et al. 2022

Journal of Oncology

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Background. Ubiquitin-specific protease15(USP15), is the 16th identified protease in the USP family and is a key protein in tumorigenesis. However, the predictive value and regulatory mechanism of USP15 in breast cancer are unclear. Methods. The GEPIA, UALCAN, GeneMANIA, and STRING databases were applied to explore the expression of USP15 in breast cancer and associated proteins. In addition, the TIMER database was evaluated for immune infiltration patterns. Moreover, protein immunoblotting assay, cell scratching assay, small compartment invasion assay, 3D stromal gel assay, immunoprecipitation assay, and immunohistochemistry (IHC) were used to USP15 regulatory mechanisms in breast cancer. Results. In BRCA, several databases, including GEPIA and UALCAN, describe the upregulation of total protein levels and USP15 phosphorylation. In addition, the expression of USP15 was significantly correlated with gender and clinical stage. Overall survival (OS) was lower in patients with high USP15 expression. Functional network analysis showed that USP15 is involved in tumor-associated pathways, DNA replication, and cell cycle signaling through TGFβRI. In addition, USP15 expression was positively correlated with immune infiltration, including immune score, mesenchymal score, and several tumor-infiltrating lymphocytes (TIL). In addition, IHC results further confirmed the high expression of USP15 in breast cancer and its prognostic potential. Conclusions. These findings demonstrate that high USP15 expression indicates poor prognosis in BRCA and reveal potential regulatory networks and the positive relationship with immune infiltration. Thus, USP15 may be an attractive predictor for BRCA.

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Section: Discussionmentioning

confidence: 99%

A Regulatory Network Analysis of the Importance of USP15 in Breast Cancer Metastasis and Prognosis

Ling

Qin

et al. 2022

Journal of Oncology

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“…Nowadays, it is well-established that the epigenetic dysregulation accelerates tumorigenesis, and at least partially, facilitates cancer stemness. Several reports suggest, that CBX family members possess the potential to become druggable targets in distinct tumor types, including breast, lung, ovarian, esophageal, and colon cancer [ 11 , 66 , 67 , 68 , 69 ]. However, these reports do not raise the question of therapeutic targeting of the stem cell-like phenotype of solid tumors and do not prove the engagement of CBX family members in molecular mechanism modulating cancer stemness.…”

Section: Discussionmentioning

confidence: 99%

Mining Transcriptomic Data to Uncover the Association between CBX Family Members and Cancer Stemness

Czerwińska

Maćkiewicz

2022

IJMS

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Genetic and epigenetic changes might facilitate the acquisition of stem cell-like phenotypes of tumors, resulting in worse patients outcome. Although the role of chromobox (CBX) domain proteins, a family of epigenetic factors that recognize specific histone marks, in the pathogenesis of several tumor types is well documented, little is known about their association with cancer stemness. Here, we have characterized the relationship between the CBX family members’ expression and cancer stemness in liver, lung, pancreatic, and uterine tumors using publicly available TCGA and GEO databases and harnessing several bioinformatic tools (i.e., Oncomine, GEPIA2, TISIDB, GSCA, UALCAN, R2 platform, Enrichr, GSEA). We demonstrated that significant upregulation of CBX3 and downregulation of CBX7 are consistently associated with enriched cancer stem-cell-like phenotype across distinct tumor types. High CBX3 expression is observed in higher-grade tumors that exhibit stem cell-like traits, and CBX3-associated gene expression profiles are robustly enriched with stemness markers and targets for c-Myc transcription factor regardless of the tumor type. Similar to high-stemness tumors, CBX3-overexpressing cancers manifest a higher mutation load. On the other hand, higher-grade tumors are characterized by the significant downregulation of CBX7, and CBX7-associated gene expression profiles are significantly depleted with stem cell markers. In contrast to high-stemness tumors, cancer with CBX7 upregulation exhibit a lower mutation burden. Our results clearly demonstrate yet unrecognized association of high CBX3 and low CBX7 expression with cancer stem cell-like phenotype of solid tumors.

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“…Compared with normal tissues or paracancerous tissues, the expression of all or some of the CBX1/2/3/4/5/8 members is upregulated in most cancer tissues, including glioma (67-69), tongue squamous cell carcinoma (TSCC) (70), head and neck squamous cell carcinoma (HNSCC) (71), breast cancer (BC) (15,(72)(73)(74)(75)(76)(77)(78)(79)(80), non-small cell lung cancer (NSCLC) (81)(82)(83)(84)(85), esophageal cancer (EC) (86)(87)(88)(89)(90), gastric cancer (GC) (91)(92)(93)(94)(95)(96)(97)(98), pancreatic adenocarcinoma (PAAD) (99,100), colorectal cancer (CRC) (101-104), urinary bladder cancer (UBC) (105), sarcoma (106) and osteosarcoma (107,108). As a tumor suppressor, CBX7 is expressed at low levels in most tumors, such as glioma, HNSCC (71), EC (87,88), GC (93)(94)(95)(96)(97)(98), PAAD (109), CRC (103,104), clear cell renal cell carcinoma (ccRCC) …”

Section: Expression Of Cbxs In Cancers and The Relationship Between C...mentioning

confidence: 99%

“…CBX3 is a poor prognostic factor in as many as 13 tumor types (67,69-71,80 ,81,84,86-88,101,106,110,111,114,116,122,123). CBX4 is of prognostic value in BC (76,80), LUAD (85), EC (86)(87)(88), GC (92,94,95,98), HCC (11) and ccRCC (110). In addition, patients with BC (80), LUAD (84), GC (94)(95)(96)(97)(98), CRC (103), sarcoma (106), SKCM (113) with upregulated CBX5 and HNSCC (71) and ccRCC (110) with downregulated CBX5 have poor prognosis.…”

Section: Othersmentioning

confidence: 99%

“…CBX7 acts as a tumor suppressor in glioma (68), BC (15,77), LUAD (83,84,125), HCC (114,119), PAAD (99,109), ccRCC (110), CCA (112), sarcoma (106) and SKCM (113). When the expression of CBX7 is low, the OS of patients is shorter, but its relationship to survival in EC (86)(87)(88) and GC (94-98) is controversial. High expression of CBX8 in patients with glioma (67), BC (79), HCC (120,121), CRC (102), ccRCC (110) and UBC (105) lead to unfavorable prognosis, but patients with LUAD (84) with low CBX8 expression exhibit a shorter OS.…”

Section: Othersmentioning

confidence: 99%

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Chromobox proteins in cancer: Multifaceted functions and strategies for modulation (Review)

et al. 2023

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Chromobox (CBX) proteins are important epigenetic regulatory proteins and are widely involved in biological processes, such as embryonic development, the maintenance of stem cell characteristics and the regulation of cell proliferation and apoptosis. Disorder and dysfunction of CBXs in cancer usually lead to the blockade or ectoptic activation of developmental pathways, promoting the occurrence, development and progression of cancer. In the present review, the characteristics and functions of CBXs were first introduced. Subsequently, the expression of CBXs in cancers and the relationship between CBXs and clinical characteristics (mainly cancer grade, stage, metastasis and relapse) and prognosis were discussed. Finally, it was described how CBXs regulate cell proliferation and self-renewal, apoptosis and the acquisition of malignant phenotypes, such as invasion, migration and chemoresistance, through mechanisms involving epigenetic modification, nuclear translocation, noncoding RNA interactions, transcriptional regulation, posttranslational modifications, protein-protein interactions, signal transduction and metabolic reprogramming. The study also focused on cancer therapies targeting CBXs. The present review provides new insight and a comprehensive basis for follow-up research on CBXs and cancer. Contents1. Introduction 2. Constituent members of CBXs 3. Characteristics and functions of PcG family CBXs 4. Characteristics and functions of HP1 family CBXs 5. Expression of CBXs in cancers and the relationship between CBXs and clinical characteristics and prognosis 6. CBXs regulate biological tumor processes through epigenetic modification, nuclear translocation, ncRNA interactions, transcriptional regulation, PTMs, proteinprotein interactions, signal transduction and metabolic reprogramming 7. Cancer therapies targeting CBXs 8. Conclusion and prospects

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Identification and Validation of Chromobox Family Members as Potential Prognostic Biomarkers and Therapeutic Targets for Human Esophageal Cancer

Cited by 3 publications

References 56 publications

A Regulatory Network Analysis of the Importance of USP15 in Breast Cancer Metastasis and Prognosis

A Regulatory Network Analysis of the Importance of USP15 in Breast Cancer Metastasis and Prognosis

Mining Transcriptomic Data to Uncover the Association between CBX Family Members and Cancer Stemness

Chromobox proteins in cancer: Multifaceted functions and strategies for modulation (Review)

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