Tetraspanins stimulate protein synthesis in myeloma cell lines

Zismanov, Victoria; Drucker, Liat; Attar-Schneider, Oshrat; Matalon, Shay; Pasmanik‐Chor, Metsada; Lishner, Michael

doi:10.1002/jcb.24126

Cited by 18 publications

(17 citation statements)

References 50 publications

(91 reference statements)

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“…Recently, dosage effects of protein translation and transport genes are reported for plasma cell leukemia, a cancer closely related to myeloma [31]. Overdrive of translation machines is a feature of cancer cell proliferation [32-34]. Dosage sensitivity of the genes in translation processes indicates their expression levels are not subject to tightly controlled dosage compensation and are susceptible to the influence of copy number alteration.…”

Section: Discussionmentioning

confidence: 99%

The shaping and functional consequences of the dosage effect landscape in multiple myeloma

et al. 2013

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BackgroundMultiple myeloma (MM) is a malignant proliferation of plasma B cells. Based on recurrent aneuploidy such as copy number alterations (CNAs), myeloma is divided into two subtypes with different CNA patterns and patient survival outcomes. How aneuploidy events arise, and whether they contribute to cancer cell evolution are actively studied. The large amount of transcriptomic changes resultant of CNAs (dosage effect) pose big challenges for identifying functional consequences of CNAs in myeloma in terms of specific driver genes and pathways. In this study, we hypothesize that gene-wise dosage effect varies as a result from complex regulatory networks that translate the impact of CNAs to gene expression, and studying this variation can provide insights into functional effects of CNAs.ResultsWe propose gene-wise dosage effect score and genome-wide karyotype plot as tools to measure and visualize concordant copy number and expression changes across cancer samples. We find that dosage effect in myeloma is widespread yet variable, and it is correlated with gene expression level and CNA frequencies in different chromosomes. Our analysis suggests that despite the enrichment of differentially expressed genes between hyperdiploid MM and non-hyperdiploid MM in the trisomy chromosomes, the chromosomal proportion of dosage sensitive genes is higher in the non-trisomy chromosomes. Dosage-sensitive genes are enriched by genes with protein translation and localization functions, and dosage resistant genes are enriched by apoptosis genes. These results point to future studies on differential dosage sensitivity and resistance of pro- and anti-proliferation pathways and their variation across patients as therapeutic targets and prognosis markers.ConclusionsOur findings support the hypothesis that recurrent CNAs in myeloma are selected by their functional consequences. The novel dosage effect score defined in this work will facilitate integration of copy number and expression data for identifying driver genes in cancer genomics studies. The accompanying R code is available at http://www.canevolve.org/dosageEffect/.

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Section: Discussionmentioning

confidence: 99%

The shaping and functional consequences of the dosage effect landscape in multiple myeloma

et al. 2013

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“…The hypermethylation of their gene promoters contributes to the silencing [32]. Overexpression of CD81-GFP and CD82-GFP fusions in MM cells causes massive autophagic, nonapoptotic death [33,34] by attenuating Akt/mTOR signaling [35], activating the unfolded protein response [34], and stimulating protein synthesis [36]. Notably, overexpression of GFP-CD81 and GFP-CD82 fusions in MM cells reduces cell-matrix adhesion and cell movement [33].…”

Section: Cd82 Solid Tumors and Hematopoietic Malignanciesmentioning

confidence: 98%

Tetraspanin CD82: a suppressor of solid tumors and a modulator of membrane heterogeneity

Feng

Huang

Wren

et al. 2015

Cancer Metastasis Rev

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Tetraspanin CD82 suppresses the progression and metastasis of a wide range of solid malignant tumors. However, its roles in tumorigenesis and hematopoietic malignancy remain unclear. Ubiquitously expressed CD82 restrains cell migration and cell invasion by modulating both cell-matrix and cell-cell adhesiveness and confining outside-in pro-motility signaling. This restraint at least contributes to, if not determines, the metastasis-suppressive activity and, also likely, the physiological functions of CD82. As a modulator of cell membrane heterogeneity, CD82 alters microdomains, trafficking, and topography of the membrane by changing the membrane molecular landscape. The functional activities of membrane molecules and the cytoskeletal interaction of the cell membrane are subsequently altered, followed by changes in cellular functions. Given its pathological and physiological importance, CD82 is a promising candidate for clinically predicting and blocking tumor progression and metastasis and also an emerging model protein for mechanistically understanding cell membrane organization and heterogeneity.

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“…CD81 is a transmembrane cell surface protein. Some studies have revealed that CD81 expression predicts a poor prognosis for PCM patients . In this study, CD117 and CD81 expression was analyzed in 131 patients who received initial treatment for PCM, and the relationship between CD117/CD81 expression and patient prognosis was further evaluated.…”

Section: Introductionmentioning

confidence: 99%

Expression of CD81 and CD117 in plasma cell myeloma and the relationship to prognosis

Chen

Wang

et al. 2018

Cancer Medicine

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In this study, the immunophenotype was retrospectively analyzed in 131 patients who received initial treatment for plasma cell myeloma (PCM) and the relationships of CD81 and CD117 with the clinicopathologic characteristics and prognosis were further evaluated. The Kaplan and Meier method and Cox regression survival analysis model were used to determine whether CD117 and CD81 were factors affecting the overall survival (OS) and progression‐free survival (PFS) of PCM patients. CD117 and CD81 positivity was demonstrated in 35.88% and 40.46% of the 131 patients, respectively. Kaplan‐Meier analysis showed that CD117 and CD81 were potential predictors of a patient's prognosis. Specifically, CD117(+) patients had longer PFS (P = 0.033) and OS (P = 0.002), while CD81(+) patients had shorter PFS (P = 0.001) and OS (P = 0.002). CD117(+) and CD81(−) patients had the longest PFS [P = 0.0183 compared to the CD117(−)CD81(−)/CD117(+)CD81(+) group; P = 0.0007 compared to the CD117(−)CD81(+) group] and the longest OS [P = 0.0331 compared to the CD117(−)CD81(−)/CD117(+)CD81(+) group; P = 0.0005 compared to the CD117(−)CD81(+) group]. Our results show that CD81 is an independent factor affecting the OS and PFS of PCM patients, and CD117 is an independent factor affecting the OS of PCM patients. CD117‐positive and CD81‐negative patients with PCM have a better prognosis.

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Tetraspanins stimulate protein synthesis in myeloma cell lines

Cited by 18 publications

References 50 publications

The shaping and functional consequences of the dosage effect landscape in multiple myeloma

The shaping and functional consequences of the dosage effect landscape in multiple myeloma

Tetraspanin CD82: a suppressor of solid tumors and a modulator of membrane heterogeneity

Expression of CD81 and CD117 in plasma cell myeloma and the relationship to prognosis

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