Activating mutations of N- and K-ras in multiple myeloma show different clinical associations: analysis of the Eastern Cooperative Oncology Group Phase III Trial

Liu, P; Leong, Traci; Quam, Lois; Billadeau, Daniel D.; Kay, NE; Greipp, PR; Kyle, RA; Oken, MM; Ness, Brian Van

doi:10.1182/blood.v88.7.2699.bloodjournal8872699

Cited by 195 publications

(66 citation statements)

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“…Also, along with hTERT, in MM permitted bypass of senescence, a substantial extension of lifespan, and possibly immortalization. KRAS is an oncogene involved in various malignancies, including MM [84]. It is implicated in telomere maintenance by the stimulation of telomere-telomere fusions (T-TFs) [85], demonstrating a high degree of genomic instability [86].…”

Section: Discussionmentioning

confidence: 99%

Expression profile of telomere‐associated genes in multiple myeloma

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Panero

et al. 2012

J Cellular Molecular Medi

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To further contribute to the understanding of multiple myeloma, we have focused our research interests on the mechanisms by which tumour plasma cells have a higher survival rate than normal plasma cells. In this article, we study the expression profile of genes involved in the regulation and protection of telomere length, telomerase activity and apoptosis in samples from patients with monoclonal gammopathy of undetermined significance, smouldering multiple myeloma, multiple myeloma (MM) and plasma cell leukaemia (PCL), as well as several human myeloma cell lines (HMCLs). Using conventional cytogenetic and fluorescence in situ hybridization studies, we identified a high number of telomeric associations (TAs). Moreover, telomere length measurements by terminal restriction fragment (TRF) assay showed a shorter mean TRF peak value, with a consistent correlation with the number of TAs. Using gene expression arrays and quantitative PCR we identified the hTERT gene together with 16 other genes directly involved in telomere length maintenance: HSPA9, KRAS, RB1, members of the Small nucleolar ribonucleoproteins family, A/B subfamily of ubiquitously expressed heterogeneous nuclear ribonucleoproteins, and 14-3-3 family. The expression levels of these genes were even higher than those in human embryonic stem cells (hESCs) and induced pluripotent stem cells (iPSCs), which have unlimited proliferation capacity. In conclusion, the gene signature suggests that MM tumour cells are able to maintain stable short telomere lengths without exceeding the short critical length, allowing cell divisions to continue. We propose that this could be a mechanism contributing to MM tumour cells expansion in the bone marrow (BM).

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Section: Discussionmentioning

confidence: 99%

Expression profile of telomere‐associated genes in multiple myeloma

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Catalina

Panero

et al. 2012

J Cellular Molecular Medi

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“…In parallel, the MEK/ ERK signalling cascade tightly regulates cytokine and growth factor secretion within the BM milieu, which can further augment MM growth, survival, and drug resistance (Giuliani et al, 2004;Menu et al, 2004;Hideshima et al, 2007). Importantly, the key components of the Ras/Raf/MEK/ERK signalling pathway frequently mediate constitutive activation of downstream effectors in late stage MM and plasma cell leukaemia (PCL) (Corradini et al, 1993;Liu et al, 1996;Bezieau et al, 2002;Intini et al, 2007;Tiedemann et al, 2008).…”

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confidence: 99%

“…In these indications, the presence of the BRAF V600E mutation was suggested to predict responses to MEK inhibition (Davies et al, 2002;Solit et al, 2006;Pratilas & Solit, 2007;Friday & Adjei, 2008). RAS mutations, either NRAS or KRAS but not HRAS, were found in MM patients with increasing frequency in relapsed (45-67%) versus newly diagnosed (25%) diseases, correlating with more aggressive disease features (Portier et al, 1992;Liu et al, 1996;Rasmussen et al, 2005;Chng et al, 2008). RAS mutations have been rarely detected (<7%) in pre-malignant monoclonal gammopathy of undetermined significance (MGUS) (Rasmussen et al, 2005;Chng et al, 2008), suggesting an important role of mutated RAS in malignant transformation of clonal plasma cells and MM pathogenesis.…”

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confidence: 99%

Blockade of the MEK/ERK signalling cascade by AS703026, a novel selective MEK1/2 inhibitor, induces pleiotropic anti‐myeloma activity in vitro and in vivo

et al. 2010

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Summary This study investigated the cytotoxicity and mechanism of action of AS703026, a novel, selective, orally bioavailable MEK1/2 inhibitor, in human multiple myeloma (MM). AS703026 inhibited growth and survival of MM cells and cytokine‐induced osteoclast differentiation more potently (9‐ to 10‐fold) than AZD6244. Inhibition of proliferation induced by AS703026 was mediated by G0‐G1 cell cycle arrest and was accompanied by reduction of MAF oncogene expression. AS703026 further induced apoptosis via caspase 3 and Poly ADP ribose polymerase (PARP) cleavage in MM cells, both in the presence or absence of bone marrow stromal cells (BMSCs). Importantly, AS703026 sensitized MM cells to a broad spectrum of conventional (dexamethasone, melphalan), novel or emerging (lenalidomide, perifosine, bortezomib, rapamycin) anti‐MM therapies. Significant tumour growth reduction in AS703026‐ vs. vehicle‐treated mice bearing H929 MM xenograft tumours correlated with downregulated pERK1/2, induced PARP cleavage, and decreased microvessels in vivo. Moreover, AS703026 (<200 nmol/l) was cytotoxic against the majority of tumour cells tested from patients with relapsed and refractory MM (84%), regardless of mutational status of RAS and BRAF genes. Importantly, BMSC‐induced viability of MM patient cells was similarly blocked within the same dose range. Our results therefore support clinical evaluation of AS703026, alone or in combination with other anti‐MM agents, to improve patient outcome.

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“…Activation of RAS is a common feature in a wide spectrum of tumours. In multiple myeloma (MM), RAS mutations have been observed at variable incidences with most of them >40% and showing generally more common N-than K-RAS mutations in western studies (Neri et al, 1989;Portier et al, 1992;Corradini et al, 1993;Liu et al, 1996;Feinman et al, 1997;Bezieau et al, 2001). However, data on Chinese patients with MM have been lacking.…”

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Alterations of RAS signalling in Chinese multiple myeloma patients: absent BRAF and rare RAS mutations, but frequent inactivation of RASSF1A by transcriptional silencing or expression of a non‐functional variant transcript

Lau

Wong

et al. 2003

Br J Haematol

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Summary. The methylation status, mutation and expression of RASSF1A, and mutations of RAS and BRAF were studied in 52 patients with multiple myeloma (MM), one plasma cell leukaemia (PCL) patient and four MM-derived cell lines. Aberrant methylation of RASSF1A was found in nine of 32 MM patients and in one of four MM cell lines (U266), where the associated loss of transcription was reversible by demethylation treatment. RASSF1A transcription was further investigated on anti-CD138-sorted plasma cell-enriched bone marrow samples from 10 MM, one PCL and three reactive plasmacytosis patients. While the wild-type RASSF1A transcript was detected in all three reactive plasmacytosis and the PCL samples, we found no detectable wild-type transcripts in six of 10 MM samples studied. In two MM samples, only the non-functional variant transcript was detected, whereas the other four showed loss of transcription. In great contrast to western data, RAS mutations were identified in only four of 31 (13%) MM patients. While no RASSF1A or BRAF mutation (V599E) was detected in any of the primary MM studied (n ¼ 21), the latter was found in the U266 cell line. Taken together, these data indicate that alterations of RAS signalling are critical in MM pathogenesis. In our current studies of Chinese MM patients, these alterations involved frequent RASSF1A inactivation (60%) as a result of transcriptional silencing or expression of a non-functional variant transcript.

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Activating mutations of N- and K-ras in multiple myeloma show different clinical associations: analysis of the Eastern Cooperative Oncology Group Phase III Trial

Cited by 195 publications

References 23 publications

Expression profile of telomere‐associated genes in multiple myeloma

Expression profile of telomere‐associated genes in multiple myeloma

Blockade of the MEK/ERK signalling cascade by AS703026, a novel selective MEK1/2 inhibitor, induces pleiotropic anti‐myeloma activity in vitro and in vivo

Alterations of RAS signalling in Chinese multiple myeloma patients: absent BRAF and rare RAS mutations, but frequent inactivation of RASSF1A by transcriptional silencing or expression of a non‐functional variant transcript

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