STI571 sensitizes breast cancer cells to 5-fluorouracil, cisplatin and camptothecin in a cell type-specific manner

Sims, Jonathan T.; Ganguly, Sourik S.; Fiore, Leann S.; Holler, Chris; Park, Eun-Sil; Plattner, Rina

doi:10.1016/j.bcp.2009.04.007

Cited by 23 publications

(22 citation statements)

References 33 publications

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“…Some reports have shown that the inhibition of STAT3 could sensitize tumor cells to cisplatin-induced cell death [Sims et al, 2009;Liu et al, 2010;Yilmaz et al, 2010]. Therefore, we postulate that arctigenin may promote chemosensitivity of tumor cells to cisplatin through inhibition of STAT3 activity.…”

Section: Discussionmentioning

confidence: 78%

Arctigenin enhances chemosensitivity of cancer cells to cisplatin through inhibition of the STAT3 signaling pathway

et al. 2011

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Arctigenin is a dibenzylbutyrolactone lignan isolated from Bardanae fructus, Arctium lappa L, Saussureamedusa, Torreya nucifera, and Ipomea cairica. It has been reported to exhibit anti-inflammatory activities, which is mainly mediated through its inhibitory effect on nuclear transcription factor-kappaB (NF-κB). But the role of arctigenin in JAK-STAT3 signaling pathways is still unclear. In present study, we investigated the effect of arctigenin on signal transducer and activator of transcription 3 (STAT3) pathway and evaluated whether suppression of STAT3 activity by arctigenin could sensitize cancer cells to a chemotherapeutic drug cisplatin. Our results show that arctigenin significantly suppressed both constitutively activated and IL-6-induced STAT3 phosphorylation and subsequent nuclear translocation in cancer cells. Inhibition of STAT3 tyrosine phosphorylation was found to be achieved through suppression of Src, JAK1, and JAK2, while suppression of STAT3 serine phosphorylation was mediated by inhibition of ERK activation. Pervanadate reversed the arctigenin-induced downregulation of STAT3 activation, suggesting the involvement of a protein tyrosine phosphatase. Indeed, arctigenin can obviously induce the expression of the PTP SHP-2. Furthermore, the constitutive activation level of STAT3 was found to be correlated to the resistance of cancer cells to cisplatin-induced apoptosis. Arctigenin dramatically promoted cisplatin-induced cell death in cancer cells, indicating that arctigenin enhanced the sensitivity of cancer cells to cisplatin mainly via STAT3 suppression. These observations suggest a novel anticancer function of arctigenin and a potential therapeutic strategy of using arctigenin in combination with chemotherapeutic agents for cancer treatment.

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Section: Discussionmentioning

confidence: 78%

Arctigenin enhances chemosensitivity of cancer cells to cisplatin through inhibition of the STAT3 signaling pathway

et al. 2011

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“…83 , and active c-Abl was localized in the cytoplasm, similar to BCRAbl and v-Abl. 84,85 Significantly, c-Abl/ Arg activities (assessed by phosphorylation of substrates, Crk/CrkL) were dramatically elevated in primary melanomas relative to benign nevi or normal skin. 83,79 We showed that constitutively active IGF-1R, Her-2, EGFR, and/or SFKs contributed to c-Abl/Arg activation in melanoma and breast cancer lines, ruling out mutation as the method of activation and uncovering a novel activation mechanism in solid tumors (Fig.…”

Section: Mechanisms Of C-abl and Arg Activation In Solid Tumorsmentioning

confidence: 99%

Activation of Abl Family Kinases in Solid Tumors

Ganguly

Plattner

2012

Genes & Cancer

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Although c-Abl and Arg non-receptor tyrosine kinases are well known for driving leukemia development, their role in solid tumors has not been appreciated until recently. Accumulating evidence now indicates that c-Abl and/or Arg are activated in some solid tumor cell lines via unique mechanisms that do not involve gene mutation/translocation, and c-Abl/Arg activation promotes matrix degradation, invasion, proliferation, tumorigenesis, and/ or metastasis, depending on the tumor type. However, some data suggest that c-Abl also may suppress invasion, proliferation, and tumorigenesis in certain cell contexts. Thus, c-Abl/Arg may serve as molecular switches that suppress proliferation and invasion in response to some stimuli (e.g., ephrins) or when inactive/regulated, or as promote invasion and proliferation in response to other signals (e.g., activated growth factor receptors, loss of inhibitor expression), which induce sustained activation. Clearly, more data are required to determine the extent and prevalence of c-Abl/Arg activation in primary tumors and during progression, and additional animal studies are needed to substantiate in vitro findings. Furthermore, c-Abl/ Arg inhibitors have been used in numerous solid tumor clinical trials; however, none of these trials were restricted to patients whose tumors expressed highly activated c-Abl/Arg (targeted trial). Targeted trials are critical for determining whether c-Abl/Arg inhibitors can be effective treatment options for patients whose tumors are driven by c-Abl/Arg.

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“…The reason for increased efficacy of imatinib in combination with cisplatin in chordoma is not clear yet. However, there is increasing preclinical evidence in favor of a synergic activity of these two agents in other cancers and, in particular, that imatinib can sensitize tumor cells to cisplatin [90][91][92][93], at least in some tumors. These data are somehow encouraging and surely deserve further investigation.…”

Section: Imatinib In Combination With Cisplatinmentioning

confidence: 99%

Systemic Therapy Options for Unresectable and Metastatic Chordomas

Stacchiotti

Casali

2011

Curr Oncol Rep

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Chordoma is an exceedingly rare tumor, marked by a slow growth rate. Surgery is the treatment of choice, but the most frequent sites of origin (spine and skull base) make treatment of primary disease challenging. Local relapses affect more than 50% of cases, with a minority of patients being cured by further surgery. Furthermore, metastases occur in at least 20% of patients. For residual or recurrent disease, high-dose radiation therapy may be indicated. Radiation therapy is currently the preferred local treatment when surgery is problematic, exploiting most recent techniques, including proton beams and carbon ions. However, systemic therapy is needed in patients non-amenable to surgery and/or radiation therapy. We reviewed systemic treatments currently available, and targets possibly druggable in the future in this orphan disease.

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STI571 sensitizes breast cancer cells to 5-fluorouracil, cisplatin and camptothecin in a cell type-specific manner

Cited by 23 publications

References 33 publications

Arctigenin enhances chemosensitivity of cancer cells to cisplatin through inhibition of the STAT3 signaling pathway

Arctigenin enhances chemosensitivity of cancer cells to cisplatin through inhibition of the STAT3 signaling pathway

Activation of Abl Family Kinases in Solid Tumors

Systemic Therapy Options for Unresectable and Metastatic Chordomas

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