Your search keyword '"Broccardo C"' showing total 4 results

1. RET fusion genes are associated with chronic myelomonocytic leukemia and enhance monocytic differentiation.

Author

Ballerini, P, Struski, S, Cresson, C, Prade, N, Toujani, S, Deswarte, C, Dobbelstein, S, Petit, A, Lapillonne, H, Gautier, E-F, Demur, C, Lippert, E, Pages, P, Mansat- De Mas, V, Donadieu, J, Huguet, F, Dastugue, N, Broccardo, C, Perot, C, and Delabesse, E

Subjects

MYELOPROLIFERATIVE neoplasms, PROTEIN-tyrosine kinases, CHRONIC myeloid leukemia, CLONING, GENETIC mutation

Abstract

Myeloproliferative neoplasms are frequently associated with aberrant constitutive tyrosine kinase (TK) activity resulting from chimaeric fusion genes or point mutations such as BCR-ABL1 or JAK2 V617F. We report here the cloning and functional characterization of two novel fusion genes BCR-RET and FGFR1OP-RET in chronic myelomonocytic leukemia (CMML) cases generated by two balanced translocations t(10;22)(q11;q11) and t(6;10)(q27;q11), respectively. The two RET fusion genes leading to the aberrant activation of RET, are able to transform hematopoietic cells and skew the hematopoietic differentiation program towards the monocytic/macrophage lineage. The RET fusion genes seem to constitutively mimic the same signaling pathway as RAS mutations frequently involved in CMML. One patient was treated with Sorafenib, a specific inhibitor of the RET TK function, and demonstrated cytological and clinical remissions. [ABSTRACT FROM AUTHOR]

Published

2012

2. B-cell regulator of immunoglobulin heavy-chain transcription (Bright)/ARID3a is a direct target of the oncomir microRNA-125b in progenitor B-cells.

Author

Puissegur, M P, Eichner, R, Quelen, C, Coyaud, E, Mari, B, Lebrigand, K, Broccardo, C, Nguyen-Khac, F, Bousquet, M, and Brousset, P

Subjects

B cells, IMMUNOGLOBULINS, MICRORNA, LYMPHOBLASTIC leukemia, GENE expression, CHROMOSOMAL translocation, CASPASES regulation

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) is often associated with chromosomal translocations leading to the deregulation of proto-oncogenes. MicroRNAs can also be affected by chromosomal alterations and thus contribute to carcinogenesis. The microRNA, miR-125b-1, is overexpressed in B-ALL cases with the t(11;14)(q24;q32) translocation; therefore, we sought to determine the role of this microRNA in B-cell fate. We used murine pre-BI cells alongside murine and human leukemic B-cell lines to show that miR-125b expression enhances proliferation by targeting B-cell regulator of immunoglobulin heavy-chain transcription (Bright)/ARID3a, an activator of immunoglobulin heavy-chain transcription. Accordingly, this target gene was downregulated in B-ALL patients with the t(11;14)(q24;q32) translocation. Repression of Bright/ARID3a blocked differentiation and conferred a survival advantage to Ba/F3 cells under interleukin-3 starvation. In addition, overexpression of miR-125b protected pre-BI and leukemic B-cell lines from apoptosis by blockade of caspase activation by a mechanism that was independent of p53 and BAK1. In summary, miR-125b can act as an oncogene in B-ALL by targeting ARID3a and mediating its repression, thus leading to a blockage in differentiation, increased proliferation and inhibition of apoptosis. [ABSTRACT FROM AUTHOR]

Published

2012

3. Comparative analysis of the promoter structure and genomic organization of the human and mouse ABCA7 gene encoding a novel ABCA transporter.

Author

Broccardo, C., Osorio, J., Luciani, M. -F., Schriml, L. M., Prades, C., Shulenin, S., Arnould, I., Naudin, L., Lafargue, C., Rosier, M., Jordan, B., Mattei, M. G., Dean, M., Denèfle, P., and Chimini, G.

Subjects

GENE mapping, HUMAN chromosomes, MICE, THYMUS, HEMATOPOIETIC system, GENOMICS

Abstract

We report here the genomic and transcriptional characterization in mouse and man of a novel transporter of the ABCA subclass,named ABCA7.As it is the case for other ABCA genes,the predicted protein encoded by ABCA7 is a full symmetric transporter,highly conserved across species.The ABCA7 gene maps to human chromosome 19 and to the homologous region at band B4-C1 on mouse chromosome 10. The preferential expression of ABCA7 in the spleen,thymus, and fetal liver is consistent with the finding,in both human and mouse promoter,of sites targeted by lymphomyeloid-specific transcription factors.This suggests that ABCA7 may play a pivotal role in the developmental specification of hematopoiet- ic cell lineages. [ABSTRACT FROM AUTHOR]

Published

2001

4. Invito alla lettura.

Author

Broccardo, C.

Published

2012