HO-3867, a Safe STAT3 Inhibitor, Is Selectively Cytotoxic to Ovarian Cancer

Rath, Kellie S.; Naidu, Shan K.; Lata, Pushpa; Bid, Hemant K.; Rivera, Brian K.; McCann, Georgia A.; Tierney, Brent J.; ElNaggar, Adam C.; Bravo, Veronica; Leone, Gustavo; Houghton, Peter J.; Hideg, Kálmán; Kuppusamy, Periannan; Cohn, David E.; Selvendiran, Karuppaiyah

doi:10.1158/0008-5472.can-13-2433

Cited by 71 publications

(66 citation statements)

References 24 publications

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“…Furthermore, STAT3 activation is correlated with disease stage, lymph node metastasis, drug resistance and poor survival in ovarian cancer [27,28,29]. The expression of the phosphorylated form of STAT3, p-STAT3, is higher in ovarian cancer cell lines and in EOC tissues compared to benign ovarian tumors or normal ovarian tissues [27,30]. The nuclear localization of p-STAT3 has been detected in a significant proportion of ovarian cancer patients in association with poor prognosis [28,31].…”

Section: Discussionmentioning

confidence: 99%

MicroRNA-302b Suppresses Human Epithelial Ovarian Cancer Cell Growth by Targeting RUNX1

Yin

Yang

et al. 2014

Cell Physiol Biochem

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Background: The microRNA (miR)-302 family functions as a tumor suppressor in human cancer. However, its role in epithelial ovarian carcinoma (EOC) remains unknown. Here, we investigated the role of miR-302b and its target gene RUNX1 in EOC. Methods: The expression levels of miR-302b and RUNX1 were assessed by quantitative real-time PCR and western blotting. The effects of ectopic expression of miR-302b were evaluated by the MTT assay, colony forming assay and flow cytometry. RUNX1 was identified as a target of miR-302b and their interaction was confirmed by luciferase activity assays, RUNX1 silencing and overexpression of a RUNX1 mutant construct lacking the 3′UTR. The effect of miR-302b on the suppression of tumor growth was investigated in vivo in a xenograft mouse model. Results: MiR-302b levels were markedly decreased in EOC specimens. Ectopic expression of miR-302b in EOC cells inhibited cell proliferation and colony formation, induced G0/G1 arrest, and promoted apoptosis. RUNX1 was identified as a direct target of miR-302b, and knockdown of RUNX1 inhibited cell growth in a manner similar to miR-302b overexpression, whereas introduction of a 3′UTR mutant of RUNX1 reversed the suppressive effect of miR-302b. Furthermore, miR-302b overexpression led to the inactivation of the STAT3 signaling pathway in EOC cells and inhibited tumor growth in a xenograft mouse model. Conclusions: MiR-302b functions as a tumor suppressor in EOC by targeting RUNX1 and modulating the activity of the STAT3 signaling pathway.

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Section: Discussionmentioning

confidence: 99%

MicroRNA-302b Suppresses Human Epithelial Ovarian Cancer Cell Growth by Targeting RUNX1

Yin

Yang

et al. 2014

Cell Physiol Biochem

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“…Samples were diluted in 11 ml 1× PBS and filtered through a 0.2 μm pore filter and then followed the same protocol as described above for the cell culture medium. The resulting exosome pellet was re-suspended in 100μl of cold PBS or lysis buffer according to the downstream applications such as NTA, TEM and Western blotting as we previously described 41, 42 .…”

Section: Methodsmentioning

confidence: 99%

“…The resultant STAT3 knockdown cells were called as OVCAR-8 KD cells. A negative scrambled shRNA was used as a control 41 .…”

Section: Methodsmentioning

confidence: 99%

Hypoxia-induced exosomes contribute to a more aggressive and chemoresistant ovarian cancer phenotype: a novel mechanism linking STAT3/Rab proteins

et al. 2018

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Hypoxia-mediated tumor progression, metastasis, and drug resistance are major clinical challenges in ovarian cancer. Exosomes released in the hypoxic tumor microenvironment may contribute to these challenges by transferring signaling proteins between cancer cells and normal cells. We observed that ovarian cancer cells exposed to hypoxia significantly increased their exosome release by up-regulating Rab27a, down-regulating Rab7, LAMP1/2, NEU-1, and also by promoting a more secretory lysosomal phenotype. STAT3 knockdown in ovarian cancer cells reduced exosome release by altering the Rab family proteins Rab7 and Rab27a under hypoxic conditions. We also found that exosomes from patient-derived ascites ovarian cancer cell lines cultured under hypoxic conditions carried more potent oncogenic proteins - STAT3 and FAS that are capable of significantly increasing cell migration/invasion and chemo-resistance in vitro and tumor progression/metastasis in vivo. Hypoxic ovarian cancer cells derived exosomes (HEx) are proficient in re-programming the immortalized fallopian tube secretory epithelial cells (FT) to become pro-tumorigenic in mouse fallopian tubes. In addition, cisplatin efflux via exosomes was significantly increased in ovarian cancer cells under hypoxic conditions. Co-culture of HEx with tumor cells led to significantly decreased dsDNA damage and increased cell survival in response to cisplatin treatment. Blocking exosome release by known inhibitor Amiloride or STAT3 inhibitor and treating with cisplatin resulted in a significant increase in apoptosis, decreased colony formation and proliferation. Our results demonstrate that HEx are more potent in augmenting metastasis/chemotherapy resistance in ovarian cancer, and may serve as a novel mechanism for tumor metastasis, chemo-resistance and a point of intervention for improving clinical outcomes.

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“…Therefore, the traditional strategy of inhibiting STAT3 dimerization may not be an efficient strategy to eliminate functions in tumor cells. Recently, a curcumin-based STAT3 inhibitor HO-3867 was suggested to bind directly to the STAT3 DNA binding domain [44] unlike other STAT3 inhibitors. Meanwhile, only few studies have been accomplished in other STAT3 inhibition strategies or binding site verification, which all the more emphasizes the challenge to STAT3 inhibitor design.…”

Section: Discussionmentioning

confidence: 99%

An Integrated Computational and Experimental Binding Study Identifies the DNA Binding Domain as the Putative Binding Site of Novel Pyrimidinetrione Signal Transducer and Activator of Transcription 3 (STAT3) Inhibitors

Sun¹,

Yue²,

He³

et al. 2017

Drug Des

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HO-3867, a Safe STAT3 Inhibitor, Is Selectively Cytotoxic to Ovarian Cancer

Cited by 71 publications

References 24 publications

MicroRNA-302b Suppresses Human Epithelial Ovarian Cancer Cell Growth by Targeting RUNX1

MicroRNA-302b Suppresses Human Epithelial Ovarian Cancer Cell Growth by Targeting RUNX1

Hypoxia-induced exosomes contribute to a more aggressive and chemoresistant ovarian cancer phenotype: a novel mechanism linking STAT3/Rab proteins

An Integrated Computational and Experimental Binding Study Identifies the DNA Binding Domain as the Putative Binding Site of Novel Pyrimidinetrione Signal Transducer and Activator of Transcription 3 (STAT3) Inhibitors

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