Multifunctional Role of Erk5 in Multiple Myeloma

Overview

Journal Blood

Publisher Elsevier

Specialty Hematology

Date 2005 Feb 5

PMID 15692064

Citations 41

Authors

Xonia Carvajal-Vergara

Soraya Tabera

Juan C Montero

Azucena Esparis-Ogando

Ricardo Lopez-Perez

Gema Mateo

Norma Gutierrez

Marisa Parmo-Cabanas

Joaquin Teixido

Jesus F San Miguel

Atanasio Pandiella

Affiliations

Soon will be listed here.

Abstract

Multiple myeloma is characterized by the accumulation of terminally differentiated B cells in the bone marrow, due to increased proliferation and restricted apoptosis of the myelomatous clone. Here we have studied the participation of a novel mitogen-activated protein kinase (MAPK) route, the extracellular signal-regulated kinase 5 (Erk5) pathway, in the regulation of myeloma cell proliferation and apoptosis. Erk5 was expressed in cells isolated from patients and in myeloma cell lines. The myeloma growth factor interleukin 6 (IL-6) activated Erk5, and this activation was independent of Ras and Src. Expression of a dominant-negative form of Erk5 restricted the proliferation of myeloma cells and inhibited IL-6-dependent cell duplication. This dominant-negative form also sensitized myeloma cells to the proapoptotic action of dexamethasone and PS341. The latter compound caused a profound decrease in the amount of endogenous Erk5 and was less effective in inducing apoptosis when the level of Erk5 was increased by transfection of Erk5. These results place the Erk5 route as a new regulatory signaling pathway that affects multiple myeloma proliferation and apoptosis.

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