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Blood, 15 October 2006, Vol. 108, No. 8, pp. 2500-2501. This Article Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Alert me to new issues of the journal Download to citation manager Rights and Permissions Citing Articles Citing Articles via CrossRef Citing Articles via Google Scholar Google Scholar Articles by Morris, S. W. Search for Related Content PubMed Articles by Morris, S. W. Related Collections Related Articles in Blood Online Social Bookmarking                   What's this?  Previous Article  |  Table of Contents  |  Next Article  NEOPLASIA Comment on Han et al, page 2796, and comment on Fawal et al, page 2780 ALK-mediated oncogenesis: mechanisms that matter Stephan W. Morris ST JUDE CHILDREN'S RESEARCH HOSPITAL Two reports in this issue of Blood provide new insights into the lymphomagenic mechanisms used by ALK fusions, one highlighting the effects of loss of expression of the tyrosine phosphatase SHP1 that occurs in the majority of ALK-positive lymphomas and the other describing a heretofore unappreciated role for ALK fusions in the enhancement of mRNA stability. Primary systemic anaplastic large cell lymphoma (ALCL) can be subdivided into 2 biologic subtypes based on the presence or absence of oncogenically transforming fusions of the anaplastic lymphoma kinase (ALK), a receptor tyrosine kinase truncated and fused to a variety of N-terminal, activating partner proteins—the most common chimeric form being nucleophosmin (NPM)-ALK—in these lymphomas.1 The distinction between the so-called ALK-negative and ALK-positive ALCLs (the latter colloquially known as ALKomas) is relevant both from basic research and clinical standpoints. For example, a substantial body of basic research data suggest ALK-positive ALCLs to be "ALK addicts" that are exquisitely dependent upon the continuous growth-promoting cellular signals conferred by chimeric ALK proteins, making ALK a very attractive target for the development of directed therapies for future clinical use such as small molecules analogous to the BCR-ABL inhibitors imatinib and dasatinib that have revolutionized chronic myeloid leukemia treatment. Two articles published in this issue of Blood report important basic research data that help to further elucidate the downstream cellular signaling mechanisms that modulate oncogenic transformation by ALK fusions and that may ultimately permit identification of additional targets for therapeutic intervention in the clinic for ALK-positive ALCLs. View larger version (145K): [in this window] [in a new window]   Anti-ALK immunostain of a typical NPM-ALK-positive anaplastic large-cell lymphoma. Illustration by Dr Mihaela Onciu, St Jude Children's Research Hospital.   Han and colleagues report studies that follow up on earlier data from this group showing that almost all ALK-positive ALCLs experience silencing of the nonreceptor tyrosine phosphatase SHP1 due to methylation of the SHP1 gene promoter. SHP1 phosphatase is normally abundant in hematopoietic cells, but is silenced in many hematologic cancers; the biologic importance of SHP1 is exemplified by the phenotype of so-called moth-eaten mice, in which absent or markedly reduced Shp1 expression causes abnormal myeloid cell development and function as well as a propensity for lymphomagenesis.2 Using ALK-positive ALCL cell lines and primary tumor samples, Han et al show that reintroduction of SHP1 expression into lymphoma cells that had silenced the gene produces marked reductions in the phosphorylation and activation of JAK3 (a known dephosphorylation target for SHP1) and STAT3 and down-regulation of the STAT3 transcriptional targets cyclin D3, MCL1, and BCL2. Intriguingly, re-establishment of SHP1 expression in ALCL tumor cells also resulted in marked decreases in the levels of both JAK3 and NPM-ALK, an effect due to enhanced proteasome-mediated protein degradation by a yet-to-be defined mechanism. The biologic consequences of SHP1 re-expression were noteworthy: Karpas-299 and SU-DHL-1 ALCL cells experienced significant cell-cycle arrest and impaired growth upon introduction of exogenous SHP1. These data, as well as recent corroborating results from others,3 demonstrate that SHP1 loss contributes to the growth of ALK-positive ALCLs by allowing enhanced, unregulated phosphorylation and activation of JAK3/STAT3 and by permitting increased levels of JAK3 and NPM-ALK protein expression due to decreased proteasome degradation. Taken collectively, these results provide impetus for additional preclinical studies to examine the feasibility of therapeutic efforts for the clinical management of ALCL (and other SHP1-silenced cancers) that are designed to reawaken SHP1 expression by the inhibition of SHP1 promoter methylation.4 In a second ALK-related study, Fawal and colleagues report a novel oncogenic signaling mechanism— enhancement of mRNA stability by a fusion tyrosine kinase. These investigators discovered the physical interaction of NPM-ALK with AUF1/hnRNPD, one of the family of AU-binding proteins (AU-BPs) that regulates the half-lives of many mRNAs by directly interacting with A+U-rich elements (AREs) found in their 3' untranslated regions.5,6 AUF1/hnRNPD was shown to be hyperphosphorylated due to its association with NPM-ALK, and this phosphorylation correlated with the increased stability of a number of mRNAs encoding critical growth-promoting proteins such as c-MYC and cyclins A2, B1, D1, and D3. Biologically, this posttranscriptional enhancement of mRNA stability was associated with an increased survival of cells in which transcription had been experimentally arrested by actinomycin D. These data are consistent with recent results from a number of investigators indicating that the mRNA-binding properties of AU-BPs including AUF1/hnRNPD can be modified by various posttranslational modifications such as ubiquitinylation, methylation, and phosphorylation. The observations of Fawal et al show that NPM-ALK increases the stability of otherwise short-lived mRNAs, thus contributing to enhanced proliferation, survival, and oncogenesis. Now established for NPM-ALK, it will be important to examine other oncogenic kinases and AU-BPs for a similar functional interplay; if identified, such a mechanistic relationship could represent an important, heretofore unrecognized, paradigm underlying oncogenic transformation in not only hematopoietic but perhaps other malignancies as well. References Pulford K, Morris SW, Turturro F. Anaplastic lymphoma kinase proteins in growth control and cancer. J Cell Physiol. 2004;199: 330-358.[CrossRef][Medline] [Order article via Infotrieve] Wu C, Sun M, Liu L, Zhou GW. The function of the protein tyrosine phosphatase SHP-1 in cancer. Gene. 2003;306: 1-12.[CrossRef][Medline] [Order article via Infotrieve] Honorat J, Ragab A, Lamant L, Delsol G, Ragab-Thomas J. SHP1 tyrosine phosphatase negatively regulates NPM-ALK tyrosine kinase signaling. Blood. 2006;107: 4130-4138.[Abstract/Free Full Text] Han Y, Amin HM, Frantz C, et al. Restoration of shp1 expression by 5-AZA-2'-deoxycytidine is associated with downregulation of JAK3/STAT3 signaling in ALK-positive anaplastic large cell lymphoma. Leukemia. Prepublished on July 27, 2006, as DOI 10.1038/sj.leu.2404323. Bevilacqua A, Ceriani MC, Capaccioli S, Nicolin A. Post-transcriptional regulation of gene expression by degradation of messenger RNAs. J Cell Physiol. 2003;195: 356-372.[CrossRef][Medline] [Order article via Infotrieve] Gouble A, Grazide S, Meggetto F, Mercier P, Delsol G, Morello D. A new player in oncogenesis: AUF1/hnRNPD overexpression leads to tumorigenesis in transgenic mice. Cancer Res. 2002;62: 1489-1495.[Abstract/Free Full Text] CiteULike    Connotea    Del.icio.us    Digg    Reddit    Technorati    What's this? Related Articles in Blood Online: A "liaison dangereuse" between AUF1/hnRNPD and the oncogenic tyrosine kinase NPM-ALK Mohamad Fawal, Florence Armstrong, Severine Ollier, Henri Dupont, Christian Touriol, Bernard Monsarrat, Georges Delsol, Bernard Payrastre, and Dominique Morello Blood 2006 108: 2780-2788. [Abstract] [Full Text] [PDF] Loss of SHP1 enhances JAK3/STAT3 signaling and decreases proteosome degradation of JAK3 and NPM-ALK in ALK+ anaplastic large-cell lymphoma Yajun Han, Hesham M. Amin, Bevin Franko, Christine Frantz, Xinzhe Shi, and Raymond Lai Blood 2006 108: 2796-2803. [Abstract] [Full Text] [PDF] This Article Full Text (PDF) Alert me when this article is cited Alert me if a correction is posted Services Email this article to a friend Similar articles in this journal Alert me to new issues of the journal Download to citation manager Rights and Permissions Citing Articles Citing Articles via CrossRef Citing Articles via Google Scholar Google Scholar Articles by Morris, S. W. Search for Related Content PubMed Articles by Morris, S. W. Related Collections Related Articles in Blood Online Social Bookmarking                   What's this?

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