The Wnt Signaling Pathway Regulates Nalm-16 B-cell Precursor Acute Lymphoblastic Leukemic Cell Line Survival and Etoposide Resistance

Overview

Journal Biomed Pharmacother

Specialties Biology
General Medicine
Pharmacology

Date 2009 Oct 30

PMID 19864107

Citations 14

Authors

L S Thiago

E S Costa

D V Lopes

I B Otazu

A E Nowill

F A Mendes

D M Portilho

J G Abreu

C S Mermelstein

A Orfao

M I D Rossi

R Borojevic

Affiliations

Soon will be listed here.

Abstract

B-cell precursor acute lymphoblastic leukemia (BCP-ALL) is the most common malignancy in children. The Wnt signaling pathway has been found to be extensively involved in cancer onset and progression but its role in BCP-ALL remains controversial. We evaluate the role of the Wnt pathway in maintenance of BCP-ALL cells and resistance to chemotherapy. Gene expression profile revealed that BCP-ALL cells are potentially sensitive to modulation of Wnt pathway. Nalm-16 and Nalm-6 cell lines displayed low levels of canonical activation, as reflected by the virtually complete absence of total beta-catenin in Nalm-6 and the beta-catenin cell membrane distribution in Nalm-16 cell line. Canonical activation with Wnt3a induced nuclear beta-catenin translocation and led to BCP-ALL cell death. Lithium chloride (LiCl) also induced a cytotoxic effect on leukemic cells. In contrast, both Wnt5a and Dkk-1 increased Nalm-16 cell survival. Also, Wnt3a enhanced the in vitro sensitivity of Nalm-16 to etoposide (VP-16) while treatment with canonical antagonists protected leukemic cells from chemotherapy-induced cell death. Overall, our results suggest that canonical activation of the Wnt pathway may exerts a tumor suppressive effect, thus its inhibition may support BCP-ALL cell survival.

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