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FAT1 expression in T-cell acute lymphoblastic leukemia (T-ALL) modulates proliferation and WNT signaling

FAT atypical cadherin 1 (FAT1), a transmembrane protein, is frequently mutated in various cancer types and has been described as context-dependent tumor suppressor or oncogene. The FAT1 gene is mutated in 12–16% of T-cell acute leukemia (T-ALL) and aberrantly expressed in about 54% of T-ALL cases co...

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Published in:	Scientific reports 2023-01, Vol.13 (1), p.972-12, Article 972
Main Authors:	Liebig, Sven, Neumann, Martin, Silva, Patricia, Ortiz-Tanchez, Jutta, Schulze, Veronika, Isaakidis, Konstandina, Schlee, Cornelia, Schroeder, Michael P., Beder, Thomas, Morris, Luc G. T., Chan, Timothy A., Bastian, Lorenz, Burmeister, Thomas, Schwartz, Stefan, Gökbuget, Nicola, Mochmann, Liliana H., Baldus, Claudia D.
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Language:	English
Subjects:	692/4028/67/1990/283/2125 692/4028/67/68 692/4028/67/68/2486 Acute lymphoblastic leukemia Adult Cadherins Cadherins - genetics Cadherins - metabolism Cell Line, Tumor Cell Proliferation - genetics DNA methylation E-cadherin Gene expression Humanities and Social Sciences Humans Leukemia Leukemogenesis Lymphocytes T Methylation multidisciplinary Myc protein Precursor T-Cell Lymphoblastic Leukemia-Lymphoma - genetics Science Science (multidisciplinary) Signal transduction T-Lymphocytes - metabolism Tlx1 protein Tumor suppressor genes Tumors Wnt protein Wnt Signaling Pathway
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description	FAT atypical cadherin 1 (FAT1), a transmembrane protein, is frequently mutated in various cancer types and has been described as context-dependent tumor suppressor or oncogene. The FAT1 gene is mutated in 12–16% of T-cell acute leukemia (T-ALL) and aberrantly expressed in about 54% of T-ALL cases contrasted with absent expression in normal T-cells. Here, we characterized FAT1 expression and profiled the methylation status from T-ALL patients. In our T-ALL cohort, 53% of patient samples were FAT1 positive (FAT1pos) compared to only 16% FAT1 positivity in early T-ALL patient samples. Aberrant expression of FAT1 was strongly associated with FAT1 promotor hypomethylation, yet a subset, mainly consisting of TLX1-driven T-ALL patient samples showed methylation-independent high FAT1 expression. Genes correlating with FAT1 expression revealed enrichment in WNT signaling genes representing the most enriched single pathway. FAT1 knockdown or knockout led to impaired proliferation and downregulation of WNT pathway target genes ( CCND1 , MYC , LEF1) , while FAT1 overexpressing conveyed a proliferative advantage. To conclude, we characterized a subtype pattern of FAT1 gene expression in adult T-ALL patients correlating with promotor methylation status. FAT1 dependent proliferation and WNT signaling discloses an impact on deeper understanding of T-ALL leukemogenesis as a fundament for prospective therapeutic strategies.
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In our T-ALL cohort, 53% of patient samples were FAT1 positive (FAT1pos) compared to only 16% FAT1 positivity in early T-ALL patient samples. Aberrant expression of FAT1 was strongly associated with FAT1 promotor hypomethylation, yet a subset, mainly consisting of TLX1-driven T-ALL patient samples showed methylation-independent high FAT1 expression. Genes correlating with FAT1 expression revealed enrichment in WNT signaling genes representing the most enriched single pathway. FAT1 knockdown or knockout led to impaired proliferation and downregulation of WNT pathway target genes ( CCND1 , MYC , LEF1) , while FAT1 overexpressing conveyed a proliferative advantage. To conclude, we characterized a subtype pattern of FAT1 gene expression in adult T-ALL patients correlating with promotor methylation status. 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Here, we characterized FAT1 expression and profiled the methylation status from T-ALL patients. In our T-ALL cohort, 53% of patient samples were FAT1 positive (FAT1pos) compared to only 16% FAT1 positivity in early T-ALL patient samples. Aberrant expression of FAT1 was strongly associated with FAT1 promotor hypomethylation, yet a subset, mainly consisting of TLX1-driven T-ALL patient samples showed methylation-independent high FAT1 expression. Genes correlating with FAT1 expression revealed enrichment in WNT signaling genes representing the most enriched single pathway. FAT1 knockdown or knockout led to impaired proliferation and downregulation of WNT pathway target genes ( CCND1 , MYC , LEF1) , while FAT1 overexpressing conveyed a proliferative advantage. To conclude, we characterized a subtype pattern of FAT1 gene expression in adult T-ALL patients correlating with promotor methylation status. 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T.</au><au>Chan, Timothy A.</au><au>Bastian, Lorenz</au><au>Burmeister, Thomas</au><au>Schwartz, Stefan</au><au>Gökbuget, Nicola</au><au>Mochmann, Liliana H.</au><au>Baldus, Claudia D.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>FAT1 expression in T-cell acute lymphoblastic leukemia (T-ALL) modulates proliferation and WNT signaling</atitle><jtitle>Scientific reports</jtitle><stitle>Sci Rep</stitle><addtitle>Sci Rep</addtitle><date>2023-01-18</date><risdate>2023</risdate><volume>13</volume><issue>1</issue><spage>972</spage><epage>12</epage><pages>972-12</pages><artnum>972</artnum><issn>2045-2322</issn><eissn>2045-2322</eissn><abstract>FAT atypical cadherin 1 (FAT1), a transmembrane protein, is frequently mutated in various cancer types and has been described as context-dependent tumor suppressor or oncogene. The FAT1 gene is mutated in 12–16% of T-cell acute leukemia (T-ALL) and aberrantly expressed in about 54% of T-ALL cases contrasted with absent expression in normal T-cells. Here, we characterized FAT1 expression and profiled the methylation status from T-ALL patients. In our T-ALL cohort, 53% of patient samples were FAT1 positive (FAT1pos) compared to only 16% FAT1 positivity in early T-ALL patient samples. Aberrant expression of FAT1 was strongly associated with FAT1 promotor hypomethylation, yet a subset, mainly consisting of TLX1-driven T-ALL patient samples showed methylation-independent high FAT1 expression. Genes correlating with FAT1 expression revealed enrichment in WNT signaling genes representing the most enriched single pathway. FAT1 knockdown or knockout led to impaired proliferation and downregulation of WNT pathway target genes ( CCND1 , MYC , LEF1) , while FAT1 overexpressing conveyed a proliferative advantage. 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subjects	692/4028/67/1990/283/2125 692/4028/67/68 692/4028/67/68/2486 Acute lymphoblastic leukemia Adult Cadherins Cadherins - genetics Cadherins - metabolism Cell Line, Tumor Cell Proliferation - genetics DNA methylation E-cadherin Gene expression Humanities and Social Sciences Humans Leukemia Leukemogenesis Lymphocytes T Methylation multidisciplinary Myc protein Precursor T-Cell Lymphoblastic Leukemia-Lymphoma - genetics Science Science (multidisciplinary) Signal transduction T-Lymphocytes - metabolism Tlx1 protein Tumor suppressor genes Tumors Wnt protein Wnt Signaling Pathway
title	FAT1 expression in T-cell acute lymphoblastic leukemia (T-ALL) modulates proliferation and WNT signaling
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