Survivin as a target for new anticancer interventions

Zaffaroni, Nadia; Pennati, Marzia; Daidone, Maria Grazia

doi:10.1111/j.1582-4934.2005.tb00361.x

Cited by 228 publications

(190 citation statements)

References 65 publications

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“…Overexpression of survivin, a member of the IAP family of proteins, is attributed to the chemoresistance of tumor cells (Adida et al, 2000;Fukuda and Pelus, 2006;Ryan et al, 2009;Feng et al, 2013). On the contrary, different studies have shown that suppression of survivin expression can sensitize tumor cells to anti-cancer drugs (Zaffaroni et al, 2005). In the current study to investigate whether down-regulation of survivin affects chemosensitivity in AML cells, we examined the effect of survivin specific siRNA and etoposide alone or in combination on HL-60 AML cells.…”

Section: Discussionmentioning

confidence: 99%

“…Furthermore, survivin is required for stabilization of spindle microtubules and accurate chromosome segregation during mitosis. However, the exact roles of survivin in regulation of cell division and apoptosis are still unclear (Zaffaroni and Daidone, 2002;Zaffaroni et al, 2005;Kelly et al, 2011;Church and Talbot, 2012).…”

Section: Discussionmentioning

confidence: 99%

“…Because of this overexpression in cancer, its important role in apoptosis as well as cell division, and its association with drug resistance, survivin has been considered as an attractive therapeutic target in malignancies (Ryan et al, 2009;Feng et al, 2013). Various studies have shown that suppression of survivin expression with dominant negative mutants, ribozymes, antisense oligonucleotides (ASOs) and small interfering RNAs (siRNAs) increased spontaneous apoptosis and sensitized tumor cells to chemotherapy and ionizing radiation (Zaffaroni et al, 2005;Ryan et al, 2009). Yet, a study on whether the siRNA targeting of survivin could enhance the sensitivity of AML cells to antileukemic agent etoposide has not been investigated until now.…”

Section: Sirna-mediated Silencing Of Survivin Inhibits Proliferation mentioning

confidence: 99%

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siRNA-mediated Silencing of Survivin Inhibits Proliferation and Enhances Etoposide Chemosensitivity in Acute Myeloid Leukemia Cells

Karami¹,

Baradaran²,

Esfahani³

et al. 2013

Asian Pacific Journal of Cancer Prevention

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Background: Overexpression of survivin, a known inhibitor of apoptosis, is associated with tumor progression and drug resistance in numerous malignancies, including leukemias. The aim of this study was to investigate the effect of a specific survivin small interference RNA (siRNA) on proliferation and the sensitivity of HL-60 acute myeloid leukemia (AML) cells to the chemotherapeutic drug etoposide. Materials and Methods: The cells were transfected with siRNAs using Lipofectamine™2000 transfection reagent. Relative survivin mRNA and protein levels were measured by quantitative real-time PCR and Western blotting, respectively. Trypan blue exclusion assays were performed to monitor tumor cell proliferation after siRNA transfection. The cytotoxic effects of etoposide and survivin siRNA, alone and in combination, on leukemic cells were determined using MTT assay. Apoptosis was assessed by ELISA cell death assay. Results: Survivin siRNA markedly reduced both mRNA and protein expression levels in a time-dependent manner, leading to distinct inhibition of cell proliferation and increased spontaneous apoptosis. Surprisingly, survivin siRNA synergistically increased the cell toxic effects of etoposide. Moreover, survivin down-regulation significantly enhanced its induction of apoptosis. Conclusions: Our study suggests that down-regulation of survivin by siRNA can trigger apoptosis and overcome drug resistance of leukemia cells. Therefore, survivin siRNA may be an effective adjuvant in AML chemotherapy

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Sirna-mediated Silencing Of Survivin Inhibits Proliferation mentioning

confidence: 99%

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siRNA-mediated Silencing of Survivin Inhibits Proliferation and Enhances Etoposide Chemosensitivity in Acute Myeloid Leukemia Cells

Karami¹,

Baradaran²,

Esfahani³

et al. 2013

Asian Pacific Journal of Cancer Prevention

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“…In fact, Survivin that is suppressed by p53 is highly expressed in various cancer tissues and specific inhibitors for it are developed for clinical application (Zaffaroni et al, 2005). Since we have been analysing gene expression profiles of various cancer tissues using cDNA microarray, we compared the gene expression profile data for cells in which p53 gene was exogenously introduced and those for various clinical cancers.…”

Section: Introductionmentioning

confidence: 99%

CDC20, a potential cancer therapeutic target, is negatively regulated by p53

et al. 2007

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The p53 protein inhibits malignant transformation through direct and indirect regulation of transcription of many genes related to cell cycle, apoptosis and cellular senescence. A number of genes induced by p53 have been well characterized, but biological significance of genes whose expression was suppressed by p53 is still largely undisclosed. To clarify the roles of p53-suppressive genes in carcinogenesis, we analysed two data sets of wholegenome expression profiles, one for cells in which wildtype p53 was exogenously introduced and the other for a large number of clinical cancer tissues. Here, we identified CDC20 that was frequently upregulated in many types of malignancies and remarkably suppressed by ectopic introduction of p53. CDC20 expression was suppressed by genotoxic stresses in p53-and p21-dependent manners through CDE-CHR elements in the CDC20 promoter. Furthermore, small interference RNA (siRNA)-mediated silencing of p53 induced CDC20 expression in normal human dermal fibroblast cells. As we expected, treatment of cancer cells with siRNA against CDC20 induced G 2 /M arrest and suppressed cell growth. Our results indicate that p53 inhibits tumor cell growth through the indirect regulation of CDC20 and that CDC20 might be a good potential therapeutic target for a broad spectrum of human cancer.

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“…However, several reports have demonstrated its expression in human tumors and enhanced survivin levels have been correlated with tumor progression. 6 Besides, it has been recently shown that Akt may regulate survivin expression in neuroblastoma. 7 Hyaluronan (HA) is a large, linear glycosaminoglycan with a molecular weight ranging from 10 5 to 10 7 Da.…”

mentioning

confidence: 99%

Hyaluronan oligosaccharides sensitize lymphoma resistant cell lines to vincristine by modulating P‐glycoprotein activity and PI3K/Akt pathway

Russo

Garcı́a

Alaniz

et al. 2007

Intl Journal of Cancer

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Multidrug resistance (MDR) is one of the main reasons for failure of cancer therapy. It may be mediated by overexpression of ATPdependent efflux pumps or by alterations in survival or apoptotic pathways. Fragments generated by enzymatic degradation of hyaluronan (oHA) were able to modulate growth and cell survival and sensitize MDR breast cancer cells to cytotoxic drugs. In this work the relationship between oHA and MDR in lymphoid malignancies was analyzed using murine lymphoma cell lines resistant to doxorubicin (LBR-D160) or vincristine (LBR-V160) and a sensitive line (LBR-). After oHA treatment, higher apoptosis levels were observed in the resistant cell lines than in the sensitive one. Besides, oHA sensitized LBR-D160 and LBR-V160 to vincristine showing increased apoptosis induction when used in combination with vincristine. Native hyaluronan failed to increase apoptosis levels. As different survival factors could be modulated by hyaluronan, we investigated the PI3K/Akt pathway through PIP3 production and phosphorylated Akt (p-Akt) and survivin expression was also evaluated. Our results showed that oHA decreased p-Akt in the 3 cell lines while anti-CD44 treatment abolished this effect. Besides, survivin was downregulated only in LBR-V160 by oHA. When Pgp function was evaluated, we observed that oHA were able to inhibit Pgp efflux in murine and human resistant cell lines in a CD44-dependent way. In summary, we report for the first time that oHA per se modulate MDR in lymphoma cells by decreasing p-Akt as well as Pgp activity, thus suggesting that oHA could be useful in combination with classical chemotherapy in MDR hematological malignancies. ' 2007 Wiley-Liss, Inc.

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Survivin as a target for new anticancer interventions

Cited by 228 publications

References 65 publications

siRNA-mediated Silencing of Survivin Inhibits Proliferation and Enhances Etoposide Chemosensitivity in Acute Myeloid Leukemia Cells

siRNA-mediated Silencing of Survivin Inhibits Proliferation and Enhances Etoposide Chemosensitivity in Acute Myeloid Leukemia Cells

CDC20, a potential cancer therapeutic target, is negatively regulated by p53

Hyaluronan oligosaccharides sensitize lymphoma resistant cell lines to vincristine by modulating P‐glycoprotein activity and PI3K/Akt pathway

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