Expression of scinderin in megakaryoblastic leukemia cells induces differentiation, maturation, and apoptosis with release of plateletlike particles and inhibits proliferation and tumorigenesis

Zunino, Rodolfo; Li, Qinggang; Rosé, Sergio Daniel; Romero-Benítez, María Margarita Itatí; Lejen, Tatiana; Brandan, Nora Cristina; Trifaró, José-María

Artículos de revistas

Fecha

2001-10

Registro en:

Zunino, Rodolfo; Li, Qinggang; Rosé, Sergio Daniel; Romero-Benítez, María Margarita Itatí; Lejen, Tatiana; et al.; Expression of scinderin in megakaryoblastic leukemia cells induces differentiation, maturation, and apoptosis with release of plateletlike particles and inhibits proliferation and tumorigenesis; American Society of Hematology; Blood; 98; 7; 10-2001; 2210-2219

0006-4971

http://hdl.handle.net/11336/60914

1528-0020

CONICET Digital

CONICET

http://repositorioslatinoamericanos.uchile.cl/handle/2250/1871646

Autor

Zunino, Rodolfo

Li, Qinggang

Rosé, Sergio Daniel

Romero-Benítez, María Margarita Itatí

Lejen, Tatiana

Brandan, Nora Cristina

Trifaró, José-María

Institución

Consejo Nacional de Investigaciones Científicas y Tecnológicas (Argentina)

Resumen

Rapid proliferation of atypical megakaryoblasts is a characteristic of megakaryoblastic leukemia. Cells from patients with this disorder and cell lines established from this type of leukemia showed the presence of gelsolin but the absence of scinderin expression, 2 filamentous actin-severing proteins present in normal megakaryocytes and platelets. Vector-mediated expression of scinderin in the megakaryoblastic cell line MEG-01 induced a decrease in both F-actin and gelsolin. This was accompanied by increased Rac2 expression and by activation of the PAK/MEKK.SEK/JNK/c-jun, c-fos transduction pathway. The Raf/MEK/ERK pathway was also activated in these cells. Transduction pathway activation was followed by cell differentiation, polyploidization, maturation, and apoptosis with release of platelet-like particles. Particles expressed surface CD41a antigen (glycoprotein IIb/IIIa or fibrinogen receptor), had dense bodies, high-affinity serotonin transport, and circular array of microtubules. Treatment of particles with thrombin induced serotonin release and aggregation that was blocked by CD41a antibodies. PAC-1 antibodies also blocked aggregation. Exposure of cells to PD98059, a blocker of MEK, inhibited antigen CD41a expression, increases in cell volume, and number of protoplasmic extensions. Cell proliferation and cell ability to form tumors in nude mice were also inhibited by the expression of scinderin. MEG-01 cells expressing scinderin had the same fate in vivo as in culture. Thus, when injected into nude mice, they entered apoptosis and released platelet-like particles. The lack of scinderin expression in megakaryoblastic leukemia cells seems to be responsible for their inability to enter into differentiation and maturation pathways characteristic of their normal counterparts. © 2001 by The American Society of Hematology.

Materias

MEG-01 cell line

PAK/MEKK.SEK/JNK/c-jun, c-fos pathway

Raf/MEK/ERK pathway

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