Expression Patterns of Cancer-Testis Antigens in Human Embryonic Stem Cells and Their Cell Derivatives Indicate Lineage Tracks

Pluripotent stem cells can differentiate into various lineages but undergo genetic and epigenetic changes during long-term cultivation and, therefore, require regular monitoring. The expression patterns of cancer-testis antigens (CTAs) MAGE-A2, -A3, -A4, -A6, -A8, -B2, and GAGE were examined in undifferentiated human embryonic stem (hES) cells, their differentiated derivatives, teratocarcinoma (hEC) cells, and cancer cell lines of neuroectodermal and mesodermal origin. Undifferentiated hES cells and embryoid body cells expressed MAGE-A3, -A6, -A4, -A8, and GAGEs while later differentiated derivatives expressed only MAGE-A8 or MAGE-A4. Likewise, mouse pluripotent stem cells also express CTAs of Magea but not Mageb family. Despite similarity of the hES and hEC cell expression patterns, MAGE-A2 and MAGE-B2 were detected only in hEC cells but not in hES cells. Moreover, our analysis has shown that CTAs are aberrantly expressed in cancer cell lines and display low tissue specificity. The identification of CTA expression patterns in pluripotent stem cells and their derivatives may be useful for isolation of abnormally CTA-expressing cells to improve the safety of stem-cell based therapy.

• Publication year

  2011

• Venue

  Stem Cells International

• Publication date

  2011-07-18

• Fields of study

  Biology, Medicine

• Identifiers
  DOI 10.4061/2011/795239PMID 21785609PMCID 3140037
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar, PubMed

• No claims are published for this paper.

• No concepts are published for this paper.

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  2011influential reference
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• Lab-specific gene expression signatures in pluripotent stem cells.

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• Chromatin structure and gene expression programs of human embryonic and induced pluripotent stem cells.

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• Identification and classification of chromosomal aberrations in human induced pluripotent stem cells.

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• The SSX Family of Cancer-Testis Antigens as Target Proteins for Tumor Therapy

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• Cancer/testis (CT) antigens: Potential targets for immunotherapy

  2009cited by this paper
• Induced pluripotent stem cells and embryonic stem cells are distinguished by gene expression signatures.

  2009cited by this paper
• Genome-wide analysis of cancer/testis gene expression

  2008cited by this paper
• Distinct GAGE and MAGE-A expression during early human development indicate specific roles in lineage differentiation.

  2008influential reference
• Derivation of Euploid Human Embryonic Stem Cells from Aneuploid Embryos

  2008influential reference
• Characterization of human embryonic stem cell lines by the International Stem Cell Initiative

  2007influential reference
• Global gene expression profiling reveals similarities and differences among mouse pluripotent stem cells of different origins and strains.

  2007influential reference
• Generation of germline-competent induced pluripotent stem cells

  2007influential reference
• Global Epiproteomic Signatures Distinguish Embryonic Stem Cells from Differentiated Cells

  2007cited by this paper
• Expression of cancer-testis (CT) antigens in placenta.

  2007cited by this paper
• Directly reprogrammed fibroblasts show global epigenetic remodeling and widespread tissue contribution.

  2007influential reference
• MAGE-A1, GAGE and NY-ESO-1 cancer/testis antigen expression during human gonadal development.

  2007cited by this paper
• Genome wide profiling of human embryonic stem cells (hESCs), their derivatives and embryonal carcinoma cells to develop base profiles of U.S. Federal government approved hESC lines

  2006influential reference
• Induction of pluripotent stem cells from mouse embryonic and adult fibroblast cultures by defined factors.

  2006influential reference
• Chromosomal integrity maintained in five human embryonic stem cell lines after prolonged in vitro culture

  2006cited by this paper
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  2006influential reference
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  2006cited by this paper
• Gene Expression Signatures of Seven Individual Human Embryonic Stem Cell Lines

  2005influential reference
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  2005cited by this paper
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  2005influential reference
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  2005influential reference
• Cancer/testis antigen expression in human mesenchymal stem cells: down-regulation of SSX impairs cell migration and matrix metalloproteinase 2 expression.

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  2005influential reference
• MAGE-A1 interacts with adaptor SKIP and the deacetylase HDAC1 to repress transcription.

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  2003influential reference
• hMAGE-A1 overexpression reduces TNF-alpha cytotoxicity in ME-180 cells.

  2002cited by this paper
• Monoallelic expression and methylation of imprinted genes in human and mouse embryonic germ cell lineages

  2002cited by this paper
• Cancer/testis antigens: an expanding family of targets for cancer immunotherapy

  2002cited by this paper
• Expression patterns of cancer testis antigens in testicular germ cell tumors and adjacent testicular tissue.

  2001cited by this paper
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  2001cited by this paper
• The melanoma antigen genes--any clues to their functions in normal tissues?

  2001influential reference
• Isolation of pluripotent embryonic stem cells from reprogrammed adult mouse somatic cell nuclei.

  2000influential reference
• Mage-b4, a novel melanoma antigen (MAGE) gene specifically expressed during germ cell differentiation.

  2000cited by this paper
• Expression of cancer testis genes in human brain tumors.

  2000cited by this paper
• A new family of mouse genes homologous to the human MAGE genes.

  1999cited by this paper
• Expression of MAGE and GAGE in high-grade brain tumors: a potential target for specific immunotherapy and diagnostic markers.

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• DNA Methylation Is the Primary Silencing Mechanism for a Set of Germ Line- and Tumor-Specific Genes with a CpG-Rich Promoter

  1999influential reference
• Derivation of pluripotent stem cells from cultured human primordial germ cells.

  1998influential reference
• Embryonic stem cell lines derived from human blastocysts.

  1998influential reference
• Molecular detection of tumor-associated antigens shared by human cutaneous melanomas and gliomas.

  1997cited by this paper
• Methylated CpG points identified within MAGE‐1 promoter are involved in gene repression

  1996influential reference
• Structure, chromosomal location, and expression pattern of three mouse genes homologous to the human MAGE genes.

  1995cited by this paper
• Derivation of Pluripotential Embryonic Stem Cells from Murine Primordial Germ Cells in Culture.

  1993influential reference
• Derivation of pluripotential embryonic stem cells from murine primordial germ cells in culture.

  1992cited by this paper
• Expression of necdin, an embryonal carcinoma-derived nuclear protein, in developing mouse brain.

  1992cited by this paper
• Establishment in culture of pluripotential cells from mouse embryos

  1981influential reference

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  2018cites this paper
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  2018cites this paper
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  2017cites this paper
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  2017cites this paper
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