Inhibition of iNOS as a novel effective targeted therapy against triple-negative breast cancer

Granados-Principal, Sergio; Liu, Yi; Guevara, María L.; Blanco, Elvin; Choi, Dong Soon; Qian, Wei; Patel, Tejal; Rodriguez, Angel Augusto; Cusimano, Joseph; Weiss, Heidi L.; Zhao, Hong; Landis, Melissa D.; Dave, Bhuvanesh; Gross, Steven S.; Chang‐Claude, Jenny

doi:10.1186/s13058-015-0527-x

Cited by 182 publications

(164 citation statements)

References 48 publications

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“…In vitro, iNOS inhibition diminished cell proliferation, cancer stem cell self-renewal, and cell migration in TNBC cell lines. These effects have been replicated in corresponding cell lines in in vivo xenografts (16). In addition, mutations in RPL39 (A14V) and MLF2 (R158W) have been shown to enhance migration in in vitro experiments (17).…”

Section: Introductionmentioning

confidence: 82%

“…Regimen treatment design followed three, 2-week cycles of docetaxel (20 or 33 mg/kg intraperitoneal on day 1) and NOS inhibition therapy from days 2 to 6 and 9 to 13 [L-NMMA (400 mg/kg oral gavage on days 2 and 9, 200 mg/kg on days 3 to 6 and 10 to 13) þ amlodipine (10 mg/ kg intraperitoneal injection on days 2 to 6 and 9 to 13]. A Caþ channel blocker, amlodipine, was administrated to counteract the effects of NOS inhibition on blood pressure as previously described (16).…”

Section: In Vivo Experimentsmentioning

confidence: 99%

“…NO and reactive NO-derived species have been implicated in the modulation of carcinogenesis and as a critical determinant of oxidative stress in cells (12,13). In TNBC, increased iNOS expression is related to tumor grade, aggressiveness, and poor prognosis (14)(15)(16). In vitro, iNOS inhibition diminished cell proliferation, cancer stem cell self-renewal, and cell migration in TNBC cell lines.…”

Section: Introductionmentioning

confidence: 99%

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Pharmacological Inhibition of NOS Activates ASK1/JNK Pathway Augmenting Docetaxel-Mediated Apoptosis in Triple-Negative Breast Cancer

Dávila‐González

Choi

Rosato

et al. 2018

Clinical Cancer Research

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Purpose: Chemoresistance in triple-negative breast cancer (TNBC) is associated with the activation of a survival mechanism orchestrated by the endoplasmic reticulum (EnR) stress response and by inducible nitric oxide synthase (iNOS). Our aim was to determine the effects of pharmacologic NOS inhibition on TNBC.Experimental Design: TNBC cell lines, SUM-159PT, MDA-MB-436, and MDA-MB-468, were treated with docetaxel and NOS inhibitor (L-NMMA) for 24, 48, and 72 hours. Apoptosis was assessed by flow cytometry using Annexin-V and propidium iodide. Western blot was used to assess ER stress and apoptosis, and rtPCR was used to evaluate s-XBP1. TNBC patient-derived xenografts (PDX) were treated either with vehicle, docetaxel, or combination therapy (NOS inhibition þ docetaxel). Mouse weight and tumor volumes were recorded twice weekly. Docetaxel concentration was determined using mass spectrometry. To quantify proliferation and apoptosis, PDX tumor samples were stained using Ki67 and TUNEL assay.Results: In vitro, L-NMMA ameliorated the iNOS upregulation associated with docetaxel. Apoptosis increased when TNBC cells were treated with combination therapy. In TNBC PDXs, combination therapy significantly reduced tumor volume growth and increased survival proportions. In the BCM-5998 PDX model, intratumoral docetaxel concentration was higher in mice receiving combination therapy. Coupling docetaxel with NOS inhibition increased EnR-stress response via coactivation of ATF4 and CHOP, which triggered the pASK1/JNK proapoptotic pathway, promoting cleavage of caspases 3 and 9.Conclusions: iNOS is a critical target for docetaxel resistance in TNBC. Pharmacologic inhibition of NOS enhanced chemotherapy response in TNBC PDX models. Combination therapy may improve prognosis and prevent relapse in TNBC patients who have failed conventional chemotherapy.

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Section: Introductionmentioning

confidence: 82%

Section: In Vivo Experimentsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Pharmacological Inhibition of NOS Activates ASK1/JNK Pathway Augmenting Docetaxel-Mediated Apoptosis in Triple-Negative Breast Cancer

Dávila‐González

Choi

Rosato

et al. 2018

Clinical Cancer Research

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“…Since in several human diseases the NOS activity and pH are altered and affect a variety of processes including tumour cells metabolism [1,3,4,11,12,14], and expression and activity of H + exchangers (mainly NHE1) are increased in tumour cells [4][5][6][7][8], we propose that human ovarian cancer cells will show a potential functional link between increase in NO synthesis and low pHo, but higher pHi (Figure 1). The role of NHE1 seems crucial in this phenomenon, which also generates a pro-inflammatory environment maintaining elevated iNOS expression and NO synthesis.…”

mentioning

confidence: 99%

“…To date, expression of the inducible NOS (iNOS) isoform is upregulated and correlates with poor prognosis in breast cancer [11]. Other reports show that NO promotes human ovarian cancer cell growth and inhibits mitochondrial oxidative phosphorylation [12].…”

mentioning

confidence: 99%

Are NHE1 and inducible nitric oxide synthase involved in human ovarian cancer?

Sanhueza

Araos

Naranjo

et al. 2016

Pharmacological Research

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The EMT spectrum and therapeutic opportunities

et al. 2017

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Carcinomas are phenotypically arrayed along an epithelial–mesenchymal transition (EMT) spectrum, a developmental program currently exploited to understand the acquisition of drug resistance through a re‐routing of growth factor signaling. This review collates the current approaches employed in developing therapeutics against cancer‐associated EMT, and provides an assessment of their respective strengths and drawbacks. We reflect on the close relationship between EMT and chemoresistance against current targeted therapeutics, with a special focus on the epigenetic mechanisms that link these processes. This prompts the hypothesis that carcinoma‐associated EMT shares a common epigenetic pathway to cellular plasticity as somatic cell reprogramming during tissue repair and regeneration. Indeed, their striking resemblance suggests that EMT in carcinoma is a pathological adaptation of an intrinsic program of cellular plasticity that is crucial to tissue homeostasis. We thus propose a revised approach that targets the epigenetic mechanisms underlying pathogenic EMT to arrest cellular plasticity regardless of upstream cancer‐driving mutations.

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Inhibition of iNOS as a novel effective targeted therapy against triple-negative breast cancer

Cited by 182 publications

References 48 publications

Pharmacological Inhibition of NOS Activates ASK1/JNK Pathway Augmenting Docetaxel-Mediated Apoptosis in Triple-Negative Breast Cancer

Pharmacological Inhibition of NOS Activates ASK1/JNK Pathway Augmenting Docetaxel-Mediated Apoptosis in Triple-Negative Breast Cancer

Are NHE1 and inducible nitric oxide synthase involved in human ovarian cancer?

The EMT spectrum and therapeutic opportunities

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