Your search keyword '"Narducci, Maria Grazia"' showing total 3 results

1. TCL1 participates in early embryonic development and is overexpressed in human seminomas.

Author

Narducci, Maria Grazia, Fiorenza, Maria Teresa, Sang-Moo Kang, Bevilacqua, Arturo, Giacomo, Monica Di, Remotti, Daniele, Picchio, Maria Cristina, Fidanza, Vincenzo, Cooper, Max D., Croce, Carlo Maria, Mangia, Franco, and Russo, Giandomenico

Subjects

*ONCOGENES, *LEUKEMIA, *T cells, *EMBRYOLOGY

Abstract

Overexpression of the TCL1 oncogene has been shown to play a causative role in T cell leukemias of humans and mice. The characterization of Tcl1-deficient mice in these studies indicates an important developmental role for Tcl1 in early embryogenesis. In wild-type embryos, Tcl1 is abundant in the first three mitotic cycles, during which it shuttles between nuclei and the embryo cortical regions in a cell-cycle-dependent fashion. The absence of this protein in early embryogenesis results in reduced fertility of female mice. The present studies elucidate the mechanism responsible for the reduced female fertility through analysis of the oogenesis stages and early embryo development in Tcl1-deficient mice. Even though Tcl1[sup -l-] females display normal oogenesis and rates of oocyte maturation/ovulation and fertilization, the lack of maternally derived Tcl1 impairs the embryo's ability to undergo normal cleavage and develop to the morula stage, especially under in vitro culture conditions. Beyond this crisis point, differentiative traits of zygotic genome activation and embryo compaction can take place normally. In contrast with this unanticipated role in early embryogenesis, we observed an overexpression of TCL1 in human seminomas. This finding suggests that TCL1 dysregulation could contribute to the development of this germinal cell cancer as well as lymphoid malignancies. [ABSTRACT FROM AUTHOR]

Published

2002

2. The murine Tcl1 oncogene: embryonic and lymphoid cell expression.

Author

Narducci, Maria Grazia, Virgilio, Laura, Engiles, Julie B, Buchberg, Arthur M, Billips, Linda, Facchiano, Antonio, Croce, Carlo M, Russo, Giandomenico, and Rothstein, Jay L

Subjects

*ONCOGENES, *LYMPHOMAS, *CANCER cell proliferation

Abstract

In human leukemias and lymphomas nonrandom chromosomal rearrangements cause changes in cell growth and/or survival in such a way as to promote malignancy. The detailed study of the biochemical and genetic pathways altered in human cancer requires the identification or development of models to allow the study and manipulation of cancer gene function. Recently, the breakpoint gene TCL1, involved in chromosome translocations observed mostly in mature T-cell proliferations and chronic lymphocytic leukemias (CLL), was isolated and characterized, and showed to be part of a new gene family of proteins involved in these tumors. The murine Tcl1 gene, is similar in sequence to the murine and human MTCP1 gene also involved in T cell leukemias. The murine Tcl1 gene was shown to reside on mouse chromosome 12 in a region syntenic to human chromosome 14. Furthermore, we show that the murine Tcl1 gene is expressed early in mouse embryonic development and demonstrates expression in fetal hematopoietic organs as well as in immature T and B cells. Characterization of the murine Tcl1 gene will help in developing a mouse model of CLL and would provide the best opportunity to study and decipher the role of TCL1 in malignant transformation. [ABSTRACT FROM AUTHOR]

Published

1997

3. Deregulated expression of TCL1 causes T cell leukemia in mice.

Author

Virgilio, Laura, Lazzeri, Cristina, Bichi, Roberta, Nibu, Ken-Ichi, Narducci, Maria Grazia, Russo, Giandomenico, Rothstein, Jay L., and Croce, Carlo M.

Subjects

T cells, ONCOGENES

Abstract

Focuses on a study of the TCL1 oncogene on human chromosome 14q32.1, which is involved in the development of T cell leukemia in humans. Methodology used; Implication of the development of mature T cell leukemia in overexpression of the TCL1 gene in humans; Results and discussion.

Published

1998