Isorhapontigenin (ISO) Inhibits Invasive Bladder Cancer Formation <i>In Vivo</i> and Human Bladder Cancer Invasion <i>In Vitro</i> by Targeting STAT1/FOXO1 Axis

Jiang, Guosong; Wu, Amy D.; Huang, Chao; Gu, Jiayan; Zhang, Liping; Huang, Haishan; Liao, Xin; Li, Jingxia; Zhang, Dongyun; Zeng, Xingruo; Jin, Honglei; Huang, Haojie

doi:10.1158/1940-6207.capr-15-0338

Cited by 57 publications

(72 citation statements)

References 51 publications

(81 reference statements)

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“…T24 is a non‐metastatic cell line, whereas T24T is a BC cell line with lung metastatic ability (Gildea et al ., ; Grossman et al ., ). Both cell lines were cultured in DMEM:F‐12 1 : 1 with 10% fetal bovine serum (FBS; ATLANTA, Flowery Branch, GA, USA) as described in our previous studies (Jiang et al ., ; Jin et al ., ), and cell lines will be authenticated every 6–12 months by Genetica DNA Laboratories (Burlington, NC 27215, CA, USA) and the results compared with the data in the ATCC STR database. The human mmp‐2 promoter‐driven luciferase reporter was a gift from Dr. Yi Sun (Michigan University, MI, USA) (Qin et al ., ).…”

Section: Methodsmentioning

confidence: 97%

“…Alterations of MMP‐2 are often associated with the metastasis of many other cancers, including colorectal cancer (Miao et al ., ), ovarian cancer (Zhuang et al ., ), and breast cancer (Miao et al ., ). Our recent study reveals that MMP‐2 overexpression is crucial for human BC invasion (Jin et al ., ), whereas inhibition of MMP‐2 expression by the anti‐cancer agent isorhapontigenin (ISO) dramatically attenuated both BC invasion in vitro and highly invasive BC formation in vivo (Jiang et al ., ) .…”

Section: Introductionmentioning

confidence: 99%

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RhoGDIβ promotes Sp1/MMP‐2 expression and bladder cancer invasion through perturbing miR‐200c‐targeted JNK2 protein translation

et al. 2017

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Our most recent studies demonstrate that RhoGDIβ is able to promote human bladder cancer (BC) invasion and metastasis in an X‐link inhibitor of apoptosis protein‐dependent fashion accompanied by increased levels of matrix metalloproteinase (MMP)‐2 protein expression. We also found that RhoGDIβ and MMP‐2 protein expressions are consistently upregulated in both invasive BC tissues and cell lines. In the present study, we show that knockdown of RhoGDIβ inhibited MMP‐2 protein expression accompanied by a reduction of invasion in human BC cells, whereas ectopic expression of RhoGDIβ upregulated MMP‐2 protein expression and promoted invasion as well. The mechanistic studies indicated that MMP‐2 was upregulated by RhoGDIβ at the transcriptional level by increased specific binding of the transcription factor Sp1 to the mmp‐2 promoter region. Further investigation revealed that RhoGDIβ overexpression led to downregulation of miR‐200c, whereas miR‐200c was able directly to target 3′‐UTR of jnk2 mRNA and attenuated JNK2 protein translation, which resulted in attenuation of Sp1 mRNA and protein expression in turn, inhibiting Sp1‐dependent mmp‐2 transcription. Collectively, our studies demonstrate that RhoGDIβ overexpression inhibits miR‐200c abundance, which consequently results in increases of JNK2 protein translation, Sp1 expression, mmp‐2 transcription, and BC invasion. These findings, together with our previous results showing X‐link inhibitor of apoptosis protein mediating mRNA stabilization of both RhoGDIβ and mmp‐2, reveal the nature of the MMP‐2 regulatory network, which leads to MMP‐2 overexpression and BC invasion.

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Section: Methodsmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

RhoGDIβ promotes Sp1/MMP‐2 expression and bladder cancer invasion through perturbing miR‐200c‐targeted JNK2 protein translation

et al. 2017

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“…The foxo1 promoter contains STATs binding sites, and it has been shown that STAT3 can bind to these sites in immune system T cells (48). We recently showed that phosphorylated STAT1 can bind to the foxo1 promoter to inhibit its transcription in BC cells (49). In the present study, we found that miR-145 suppressed STAT3 activation and increased foxo1 promoter transcriptional activity, which overcame its inhibition on foxo1 mRNA 3′UTR activation, and subsequently upregulated FOXO1 expression and suppressed anchorage-independent growth of non-metastatic T24 cells.…”

Section: Disscussionmentioning

confidence: 99%

Role of STAT3 and FOXO1 in the Divergent Therapeutic Responses of Non-metastatic and Metastatic Bladder Cancer Cells to miR-145

Jiang

Huang

et al. 2017

Molecular Cancer Therapeutics

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Although miR-145 is the most frequently down-regulated miRNA in bladder cancer (BC), its exact stage-association and downstream effector have not been defined. Here, we found that miR-145 was upregulated in human BC patients with lymph node metastasis and in metastatic T24T cell line. Forced expression of miR-145 promoted anchorage-independent growth of T24T cells accompanied by the down-regulation of forkhead box class O1 (FOXO1). In contrast, in non-metastatic T24 cells, miR-145 overexpression inhibited cell growth with upregulation of FOXO1 and the knockdown of FOXO1 abolished the miR-145-mediated inhibition of cell growth. Mechanistic studies revealed that miR-145 directly bound to and attenuated 3′UTR activity of foxo1 mRNA in both T24 and T24T cells. Interestingly, miR-145 suppressed STAT3 phosphorylation at Tyr705 and increased foxo1 promoter transcriptional activity in T24 cells, but not in T24T cells, suggesting a role of STAT3 in the divergent responses to miR-145. Supporting this was our finding that STAT3 knockdown mimicked miR-145-mediated upregulation of FOXO1 in T24T cells and inhibition of anchorage-independent growth. Consistently, ectopic expression of miR-145 promoted tumor formation of xenograft T24T cells, whereas such promoting effect became inhibitory due to specific knockdown of STAT3. Together, our findings demonstrate the stage-specific association and function of miR-145 in BCs, and provide novel insights into the therapeutic targeting of miR-145.

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“…The human invasive BC cell line UMUC3 was provided by Dr. Xue-Ru Wu (Department of Urology and Pathology, New York University School of Medicine, New York, NY), and was used in our previous studies [52]. The human metastatic BC cell line T24T, which is a lineage-related metastatic lung variant of the invasive BC cell line T24 [53], was kindly provided by Dr. Dan Theodorescu [54] and used in our previous studies [55].…”

Section: Methodsmentioning

confidence: 99%

“…In vitro migration and invasion assays were conducted using transwell chambers (for migration assays) or transwell chambers pre-coated with Matrigel (for invasion assays) according to the manufacturer's protocol (BD Biosciences, Bedford, MA), as described previously [52]. Briefly, 700 μl of medium containing 10% FBS (for UMUC3 and T24T cells with different transfectants) was added to the lower chambers, while homogeneous single cell suspensions (5×10 4 cells/well) in 0.1% FBS medium as indicated were added to the upper chambers.…”

Section: Methodsmentioning

confidence: 99%

Interaction of BIR2/3 of XIAP with E2F1/Sp1 Activates MMP2 and Bladder Cancer Invasion by Inhibiting Src Translation

Huang¹,

Xu²,

Hua³

et al. 2018

Preprint

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Isorhapontigenin (ISO) Inhibits Invasive Bladder Cancer Formation In Vivo and Human Bladder Cancer Invasion In Vitro by Targeting STAT1/FOXO1 Axis

Cited by 57 publications

References 51 publications

RhoGDIβ promotes Sp1/MMP‐2 expression and bladder cancer invasion through perturbing miR‐200c‐targeted JNK2 protein translation

RhoGDIβ promotes Sp1/MMP‐2 expression and bladder cancer invasion through perturbing miR‐200c‐targeted JNK2 protein translation

Role of STAT3 and FOXO1 in the Divergent Therapeutic Responses of Non-metastatic and Metastatic Bladder Cancer Cells to miR-145

Interaction of BIR2/3 of XIAP with E2F1/Sp1 Activates MMP2 and Bladder Cancer Invasion by Inhibiting Src Translation

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