Aberrations of the Wnt canonical pathway (WCP) are known to contribute to the pathogenesis of various types of cancer. We hypothesize that these defects may exist in mantle cell lymphoma (MCL). Both the upstream and downstream aspects of WCP were examined in MCL cell lines and tumors. Using WCP-specific oligonucleotide arrays, we found that MCL highly and consistently expressed Wnt3 and Wnt10. -catenin, a transcriptional factor that is a downstream target of WCP, is localized to the nucleus and transcriptionally active in all 3 MCL cell lines examined. By immunohistochemistry, 33 (52%) of 64 MCL tumors showed nuclear localization of -catenin, which significantly correlated with the expression of the phosphorylated/inactive form of GSK3 (p-GSK3; P ؍ .011, Fisher).
IntroductionMantle cell lymphoma (MCL) is a specific type of non-Hodgkin B-cell lymphoma recognized by the World Health Organization (WHO) Classification Scheme. 1 The genetic hallmark of this disease is the recurrent chromosomal abnormality, the t(11;14)(q13;q32), which brings the cyclin D1 gene under the influence of the enhancer of the immunoglobulin heavy chain (IgH) gene, leading to cyclin D1 overexpression. 2 Although cyclin D1 overexpression is likely to be pathogenetically important in MCL, evidence suggests that additional biochemical defects are necessary for lymphomagenesis. For instance, using Ecyclin D1 transgenic mice, 2 research groups have previously shown that enforced cyclin D1 expression in B cells is not sufficient to induce tumor formation. 3,4 Furthermore, large-scale cDNA microarray studies using frozen MCL tumors have revealed a relatively large number of biochemical abnormalities in MCL, with these defects frequently implicated in the regulation of apoptosis, cell cycle progression, and DNA repair. [5][6][7][8][9][10] Examination of specific cellular signaling pathways also provided additional insights into the biology of these tumors. For instance, a relatively recent study reported constitutive activation of the phosphatidylinositol 3-kinase (PI3K)/Akt signaling pathway in a subset of MCL tumors, particularly those with a blastoid morphology. 11 The Wnt canonical pathway (WCP) is important for normal cell growth and development. 12,13 Defects of this pathway have been shown to play roles in the pathogenesis of a variety of human cancers, particularly those of epithelial type. 14 Normally, WCP is activated via ligation of the Wnt proteins, which are secreted glycoproteins, to their respective dimeric cell surface receptors composed of the frizzled proteins and the low-density lipoprotein-receptor-related proteins (LRPs). 15 The binding of the Wnt proteins to their receptors is negatively regulated by the Wnt inhibitory factor and the sFRP proteins (sFRP1-5). Upon ligation to their receptors, the disheveled proteins (DvLs), a family of the upstream WCP signaling proteins, are phosphorylated. 16,17 In WCP, Wnt stimulation results in inactivation/phosphorylation of GSK3, as well as the dissociation of the "destruction comp...
