Large-scale circular RNA deregulation in T-ALL: unlocking unique ectopic expression of molecular subtypes

Circular RNAs (circRNAs) are stable RNA molecules that can drive cancer through interactions with microRNAs and proteins and by the expression of circRNA encoded peptides. The aim of the study was to define the circRNA landscape and potential impact in T-cell acute lymphoblastic leukemia (T-ALL). An...

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Veröffentlicht in:	Blood advances 2020-12, Vol.4 (23), p.5902-5914
Hauptverfasser:	Buratin, Alessia, Paganin, Maddalena, Gaffo, Enrico, Dal Molin, Anna, Roels, Juliette, Germano, Giuseppe, Siddi, Maria Teresa, Serafin, Valentina, De Decker, Matthias, Gachet, Stéphanie, Durinck, Kaat, Speleman, Frank, Taghon, Tom, te Kronnie, Geertruij, Van Vlierberghe, Pieter, Bortoluzzi, Stefania
Format:	Artikel
Sprache:	eng
Schlagworte:	Cell Line Ectopic Gene Expression Humans Lymphoid Neoplasia MicroRNAs Precursor T-Cell Lymphoblastic Leukemia-Lymphoma - genetics RNA, Circular
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container_title	Blood advances
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creator	Buratin, Alessia Paganin, Maddalena Gaffo, Enrico Dal Molin, Anna Roels, Juliette Germano, Giuseppe Siddi, Maria Teresa Serafin, Valentina De Decker, Matthias Gachet, Stéphanie Durinck, Kaat Speleman, Frank Taghon, Tom te Kronnie, Geertruij Van Vlierberghe, Pieter Bortoluzzi, Stefania
description	Circular RNAs (circRNAs) are stable RNA molecules that can drive cancer through interactions with microRNAs and proteins and by the expression of circRNA encoded peptides. The aim of the study was to define the circRNA landscape and potential impact in T-cell acute lymphoblastic leukemia (T-ALL). Analysis by CirComPara of RNA-sequencing data from 25 T-ALL patients, immature, HOXA overexpressing, TLX1, TLX3, TAL1, or LMO2 rearranged, and from thymocyte populations of human healthy donors disclosed 68 554 circRNAs. Study of the top 3447 highly expressed circRNAs identified 944 circRNAs with significant differential expression between malignant T cells and normal counterparts, with most circRNAs displaying increased expression in T-ALL. Next, we defined subtype-specific circRNA signatures in molecular genetic subgroups of human T-ALL. In particular, circZNF609, circPSEN1, circKPNA5, and circCEP70 were upregulated in immature, circTASP1, circZBTB44, and circBACH1 in TLX3, circHACD1, and circSTAM in HOXA, circCAMSAP1 in TLX1, and circCASC15 in TAL-LMO. Backsplice sequences of 14 circRNAs ectopically expressed in T-ALL were confirmed, and overexpression of circRNAs in T-ALL with specific oncogenic lesions was substantiated by quantification in a panel of 13 human cell lines. An oncogenic role of circZNF609 in T-ALL was indicated by decreased cell viability upon silencing in vitro. Furthermore, functional predictions identified circRNA-microRNA gene axes informing modes of circRNA impact in molecular subtypes of human T-ALL. •The circRNAome is dramatically deregulated in T-ALL compared with normal thymocytes, with most circRNAs upregulated in malignant cells.•CircRNA-miRNA gene networks and circZNF609 silencing suggest a functional role for ectopically expressed circRNAs in T-ALL disease biology. [Display omitted]
doi_str_mv	10.1182/bloodadvances.2020002337
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The aim of the study was to define the circRNA landscape and potential impact in T-cell acute lymphoblastic leukemia (T-ALL). Analysis by CirComPara of RNA-sequencing data from 25 T-ALL patients, immature, HOXA overexpressing, TLX1, TLX3, TAL1, or LMO2 rearranged, and from thymocyte populations of human healthy donors disclosed 68 554 circRNAs. Study of the top 3447 highly expressed circRNAs identified 944 circRNAs with significant differential expression between malignant T cells and normal counterparts, with most circRNAs displaying increased expression in T-ALL. Next, we defined subtype-specific circRNA signatures in molecular genetic subgroups of human T-ALL. In particular, circZNF609, circPSEN1, circKPNA5, and circCEP70 were upregulated in immature, circTASP1, circZBTB44, and circBACH1 in TLX3, circHACD1, and circSTAM in HOXA, circCAMSAP1 in TLX1, and circCASC15 in TAL-LMO. Backsplice sequences of 14 circRNAs ectopically expressed in T-ALL were confirmed, and overexpression of circRNAs in T-ALL with specific oncogenic lesions was substantiated by quantification in a panel of 13 human cell lines. An oncogenic role of circZNF609 in T-ALL was indicated by decreased cell viability upon silencing in vitro. Furthermore, functional predictions identified circRNA-microRNA gene axes informing modes of circRNA impact in molecular subtypes of human T-ALL. •The circRNAome is dramatically deregulated in T-ALL compared with normal thymocytes, with most circRNAs upregulated in malignant cells.•CircRNA-miRNA gene networks and circZNF609 silencing suggest a functional role for ectopically expressed circRNAs in T-ALL disease biology. 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The aim of the study was to define the circRNA landscape and potential impact in T-cell acute lymphoblastic leukemia (T-ALL). Analysis by CirComPara of RNA-sequencing data from 25 T-ALL patients, immature, HOXA overexpressing, TLX1, TLX3, TAL1, or LMO2 rearranged, and from thymocyte populations of human healthy donors disclosed 68 554 circRNAs. Study of the top 3447 highly expressed circRNAs identified 944 circRNAs with significant differential expression between malignant T cells and normal counterparts, with most circRNAs displaying increased expression in T-ALL. Next, we defined subtype-specific circRNA signatures in molecular genetic subgroups of human T-ALL. In particular, circZNF609, circPSEN1, circKPNA5, and circCEP70 were upregulated in immature, circTASP1, circZBTB44, and circBACH1 in TLX3, circHACD1, and circSTAM in HOXA, circCAMSAP1 in TLX1, and circCASC15 in TAL-LMO. Backsplice sequences of 14 circRNAs ectopically expressed in T-ALL were confirmed, and overexpression of circRNAs in T-ALL with specific oncogenic lesions was substantiated by quantification in a panel of 13 human cell lines. An oncogenic role of circZNF609 in T-ALL was indicated by decreased cell viability upon silencing in vitro. Furthermore, functional predictions identified circRNA-microRNA gene axes informing modes of circRNA impact in molecular subtypes of human T-ALL. •The circRNAome is dramatically deregulated in T-ALL compared with normal thymocytes, with most circRNAs upregulated in malignant cells.•CircRNA-miRNA gene networks and circZNF609 silencing suggest a functional role for ectopically expressed circRNAs in T-ALL disease biology. 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Backsplice sequences of 14 circRNAs ectopically expressed in T-ALL were confirmed, and overexpression of circRNAs in T-ALL with specific oncogenic lesions was substantiated by quantification in a panel of 13 human cell lines. An oncogenic role of circZNF609 in T-ALL was indicated by decreased cell viability upon silencing in vitro. Furthermore, functional predictions identified circRNA-microRNA gene axes informing modes of circRNA impact in molecular subtypes of human T-ALL. •The circRNAome is dramatically deregulated in T-ALL compared with normal thymocytes, with most circRNAs upregulated in malignant cells.•CircRNA-miRNA gene networks and circZNF609 silencing suggest a functional role for ectopically expressed circRNAs in T-ALL disease biology. 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subjects	Cell Line Ectopic Gene Expression Humans Lymphoid Neoplasia MicroRNAs Precursor T-Cell Lymphoblastic Leukemia-Lymphoma - genetics RNA, Circular
title	Large-scale circular RNA deregulation in T-ALL: unlocking unique ectopic expression of molecular subtypes
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