Cancer/Testis Antigens: “Smart” Biomarkers for Diagnosis and Prognosis of Prostate and Other Cancers

Kulkarni, Prakash; Uversky, Vladimir N.

doi:10.3390/ijms18040740

Cited by 31 publications

(26 citation statements)

References 152 publications

(206 reference statements)

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“…Cancer testis antigens (CTAs) have been extensively studied in a variety of cancers of diverse histological origin and germinal cells (Lim et al, 2012;Zajac et al, 2017). However, the majority of these studies focused on the correlative expression data and/or on evaluating their immunotherapeutic targeting or tumor biomarker values, with limited studies on their gene expression regulation and even fewer on their cellular function in cancer cells (Lim et al, 2012;Kulkarni and Uversky, 2017).…”

Section: Introductionmentioning

confidence: 99%

MAGEA1 inhibits the expression of BORIS via increased promoter methylation

Zhao

Wang

Liang

et al. 2018

Journal of Cell Science

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Melanoma-associated antigen A1 (MAGEA1) and BORIS (also known as CTCFL) are members of the cancer testis antigen (CTA) family. Their functions and expression-regulation mechanisms are not fully understood. In this study, we reveal new functions and regulatory mechanisms of MAGEA1 and BORIS in breast cancer cells, which we investigated in parental and genetically manipulated breast cancer cells via gene overexpression or siRNA-mediated downregulation. We identified the interaction between MAGEA1 and CTCF, which is required for the binding of MAGEA1 to the BORIS promoter and is critical for the recruitment of DNMT3a. A protein complex containing MAGEA1, CTCF and DNMT3a was formed before or after conjunction with the BORIS promoter. The binding of this complex to the BORIS promoter accounts for the hypermethylation and repression of BORIS expression, which results in cell death in the breast cancer cell lines tested. Multiple approaches were employed, including co-immunoprecipitation, glutathione S-transferase pull-down assay, co-localization and cell death analyses using annexin V-FITC/ propidium iodide double-staining and caspase 3 activation assays, chromatin immunoprecipitation and bisulfite sequencing PCR assays for methylation. Our results have implications for the development of strategies in CTA-based immune therapeutics.

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Section: Introductionmentioning

confidence: 99%

MAGEA1 inhibits the expression of BORIS via increased promoter methylation

Zhao

Wang

Liang

et al. 2018

Journal of Cell Science

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“…The procedure of germ cell formation and tumorigenesis has significant similarities, involving cell immortalization, migration and invasion, induction of meiosis . CT genes have been known as prospective cancer markers and objectives for therapy . The activation of CT gene expression in various types of tumours was observed .…”

Section: Discussionmentioning

confidence: 99%

“…7 CT genes have been known as prospective cancer markers and objectives for therapy. 20 The activation of CT gene expression in various types of tumours was observed. 21,22 Previous study found that the activation frequency of CT gene is much changeful depending on cancer type, the melanomas, the liver and lung cancers could show a high rate of recurrence.…”

Section: Discussionmentioning

confidence: 99%

Hypomethylation‐activated cancer‐testis gene SPANXC promotes cell metastasis in lung adenocarcinoma

Wang

Chen

et al. 2019

J Cellular Molecular Medi

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Many studies have shown that there were similarity between tumorigenesis and gametogenesis. Our previous work found that cancer‐testis (CT) genes could serve as a novel source of candidate of cancer. Here, by analysing The Cancer Genome Atlas (TCGA) database, we characterized a CT gene, SPANXC, which is expressed only in testis. The SPANXC was reactivated in lung adenocarcinoma (LUAD) tissues. And the expression of SPANXC was associated with prognosis of LUAD. We also found that the activation of SPANXC was due to the promoter hypomethylation of SPANXC. Moreover, SPANXC could modulate cell metastasis both in vitro and in vivo. Mechanistically, we found that SPANXC could bind to ROCK1, a metastasis‐related gene, and thus SPANXC may regulate cell metastasis partly through interaction with ROCK1 in LUAD. Together, our results demonstrated that the CT expression pattern of SPANXC served as a crucial role in metastasis of LUAD. And these data further corroborated the resemblance between processes of germ cell development and tumorigenesis, including migration and invasion.

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“…CTAs by definition are normally expressed in testis and other developmentally regulated tissues (e.g., placenta) but are aberrantly expressed in many types of cancers [19]. This unique pattern of expression makes these genes attractive candidates as biomarkers and, together with their immunogenic capacity, also good targets for the development of cancer immunotherapy [20][21][22]. The aberrant expression of CTAs in different cancer types is associated with phenotypic changes that confer cancer cells added advantages for proliferation and survival [23,24].…”

Section: Introductionmentioning

confidence: 99%

Cancer/Testis Antigens Differentially Expressed in Prostate Cancer: Potential New Biomarkers and Targets for Immunotherapies

Kagohara

Carleton

Takahashi

et al. 2019

Preprint

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Current clinical tests for prostate cancer (PCa), such as the PSA test, are not fully capable of discerning patients that are highly likely to develop metastatic prostate cancer (MPCa). Hence, more accurate prediction tools are needed to provide treatment strategies that are focused on the different risk groups. Cancer/testis antigens (CTAs) are expressed during embryonic development and present aberrant expression in cancer making them ideal tumor specific biomarkers. Here, the potential use of a panel of CTAs as a biomarker for PCa detection as well as metastasis prediction is explored. We initially identified eight CTAs (CEP55, NUF2, PAGE4, PBK, RQCD1, SPAG4, SSX2 and TTK) that are differentially expressed in MPCa when compared to local disease and used this panel to compare the gene and protein expression profiles in paired PCa and normal adjacent prostate tissue. We identified differential expression of all eight CTAs at the protein level when comparing 80 paired samples of PCa and the adjacent non-cancer tissue. Using multiple logistic regression we also show that a panel of these CTAs present high accuracy to discriminate normal from tumor samples. In summary, this study provides evidence that a panel of CTAs, differentially expressed in aggressive PCa, is a potential biomarker for diagnosis and prognosis to be used in combination with the current clinically available tools and is also a potential target for immunotherapy development. PRÉCISA panel of eight cancer/testis antigens aberrantly expressed in prostate cancer presents high accuracy to discriminate local from metastatic tumors. This signature includes potential biomarker and immunotherapy targets for aggressive prostate cancer. expression profiles; the next step is to evaluate the expression of CEP55, NUF2, PAGE4, PBK, RQCD1, SPAG4, SSX2 and TTK in larger cohorts with follow-up data right from screening to the development of MPCa.Also, the development of less invasive approaches (liquid biopsies) to measure CTAs expression in circulating tumor cells, and even the presence of antibodies against these immunogenic biomarkers would be beneficial for early detection of primary tumors as well as metastasis prediction.

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Cancer/Testis Antigens: “Smart” Biomarkers for Diagnosis and Prognosis of Prostate and Other Cancers

Cited by 31 publications

References 152 publications

MAGEA1 inhibits the expression of BORIS via increased promoter methylation

MAGEA1 inhibits the expression of BORIS via increased promoter methylation

Hypomethylation‐activated cancer‐testis gene SPANXC promotes cell metastasis in lung adenocarcinoma

Cancer/Testis Antigens Differentially Expressed in Prostate Cancer: Potential New Biomarkers and Targets for Immunotherapies

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