SAGE analysis demonstrates increased expression of TOSO contributing to Fas-mediated resistance in CLL

PROTO-SIQUEIRA, Rodrigo; PANEPUCCI, Rodrigo A.; CARETA, Francisco P.; LEE, Abigail; CLEAR, Andrew; MORRIS, Kelly; OWEN, Carolyn; RIZZATTI, Edgar G.; SILVA JR., Wilson A.; FALCAO, Roberto R.; ZAGO, Marco A.; GRIBBEN, John G.

Artículos de revistas

Fecha

2008

Registro en:

BLOOD, v.112, n.2, p.394-397, 2008

0006-4971

http://producao.usp.br/handle/BDPI/24996

10.1182/blood-2007-11-124065

http://dx.doi.org/10.1182/blood-2007-11-124065

http://repositorioslatinoamericanos.uchile.cl/handle/2250/1621722

Autor

PROTO-SIQUEIRA, Rodrigo

PANEPUCCI, Rodrigo A.

CARETA, Francisco P.

LEE, Abigail

CLEAR, Andrew

MORRIS, Kelly

OWEN, Carolyn

RIZZATTI, Edgar G.

SILVA JR., Wilson A.

FALCAO, Roberto R.

ZAGO, Marco A.

GRIBBEN, John G.

Institución

Universidade de São Paulo (Brasil)

Resumen

To identify novel genes involved in the molecular pathogenesis of chronic lymphocytic leukemia (CLL) we performed a serial analysis of gene expression (SAGE) in CLL cells, and compared this with healthy B cells (nCD19(+)). We found a high level of similarity among CLL subtypes, but a comparison of CLL versus nCD19(+) libraries revealed 55 genes that were over-represented and 49 genes that were down-regulated in CLL. A gene ontology analysis revealed that TOSO, which plays a functional role upstream of Fas extrinsic apoptosis pathway, was over-expressed in CLL cells. This finding was confirmed by real-time reverse transcription-polymerase chain reaction in 78 CLL and 12 nCD19(+) cases (P <.001). We validated expression using flow cytometry and tissue microarray and demonstrated a 5.6-fold increase of TOSO protein in circulating CLL cells (P =.013) and lymph nodes (P =.006). Our SAGE results have demonstrated that TOSO is a novel overexpressed antiapoptotic gene in CLL.

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