Pharmacology, pharmacokinetics, and metabolism of the DNA-decoy AYX1 for the prevention of acute and chronic post-surgical pain

Mamet, Julien; Harris, Scott M.; Klukinov, Michael; Yeomans, David C.; Donahue, Renée R.; Taylor, Bradley K.; Eddinger, Kelly A.; Yaksh, Tony L.; Manning, Donald C.

doi:10.1177/1744806917703112

Cited by 11 publications

(12 citation statements)

References 47 publications

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“…This approach, in its simple or complex form, has been tested with various TFs involved in cancers or immunological disorders, including E2F (Ahn et al, 2003), NF-kB (Takahashi et al, 2009), CRE (Liu et al, 2004), AP1 (Cho et al, 2006), SP1 (Park et al, 2009), andSTAT1 (H€ olschermann et al, 2006), and also with those involved in viral infections, for example, HIV-1 (Li et al, 2005), HCV (Zhang et al, 2005), STAT3 (Zhang et al, 2010), Myc/Oct4/Sox2 (Wang et al, 2013), Myc (El-Andaloussi et al, 2005, Johari et al, 2017, Nanog/Oct4 (Rad et al, 2015), SOX18 (Klaus et al, 2016), and AYX1 (Mamet et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Simultaneous targeted inhibition of Sox2‐Oct4 transcription factors using decoy oligodeoxynucleotides to repress stemness properties in mouse embryonic stem cells

Johari

Zargan

2017

Cell Biology International

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Transcriptional master regulators like Sox2 and Oct4, which are expressed in various human tumors, have been shown to cause tumor growth promotion as well as epithelial dysplasia by means of interfering with progenitor cell differentiation. In order to investigate the potential of Sox2-Oct4 transcription factor decoy (TFD) strategy for differentiation therapy, mouse embryonic stem cells (mESCs) were used in this study as a model of cancer stem cells (CSCs). Sox2-Oct4 complex decoy ODNs (cd-ODNs) were designed according to their elements in the promoter region of Sox2 gene. DNA-protein interactions between decoy ODNs and their corresponding proteins were examined by electrophoretic mobility shift assay (EMSA). Then, decoy and scrambled ODNs were transfected into mESCs with lipofectamine under 2 inhibitors (2i) conditions. Fluorescence and confocal microscopy, cell viability, cell cycle and apoptosis analysis, alkaline phosphatase, embryoid body formation assay, and real-time PCR were used to conduct further investigations. EMSA data showed that Sox2-Oct4 decoy ODNs bound specifically to their recombinant proteins. The results revealed that the synthesized complex decoy can concomitantly target Sox2 and Oct4, which subsequently represses the stemness properties of mESCs compared to controls through decreasing cell viability, arresting cell cycle in G /G phases, inducing apoptosis, and modulating differentiation in mESCs despite the presence of 2i/LIF in cell culture. While cd-ODN strategy seems to offer great promise for cancer therapy, further studies are still required to put this powerful investigative tool in practice for a wide range of human cancers.

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Section: Introductionmentioning

confidence: 99%

Simultaneous targeted inhibition of Sox2‐Oct4 transcription factors using decoy oligodeoxynucleotides to repress stemness properties in mouse embryonic stem cells

Johari

Zargan

2017

Cell Biology International

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“…To date, there are few reports regarding pathological pain hypersensitivity relevant to oral mucosal injury, although previous studies have shown that post-traumatic pain hypersensitivity was induced in a traumatic injury model (Kumar, Sarumathi, Veerabahu, & Raman, 2013;Liu et al, 2017;Mamet et al, 2017). Clinically, it has long been known that the oral mucosa is unique in its mechanical and thermal sensitivity compared with that of the skin, suggesting that the mechanical and thermal sensory mechanisms in the oral mucosa are different from those of the body's surface (Green & Gelhard, 1987;Komiyama & De Laat, 2005).…”

Section: Discussionmentioning

confidence: 99%

Involvement of transient receptor potential vanilloid 2 in intra‐oral incisional pain

et al. 2018

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“…Transcription factor decoys function as inhibitors of transcription factor activity. Such decoys were tested and led to the inhibition of Kruppel-like transcription factors (KLF), resulting in a reduction of mechanical hypersensitivity in animal models [12]. The company's website communicates that AYX2 is specifically designed to target multiple transcription factors that sustain chronic pain due to inflammatory and/or neuropathic insult.…”

Section: Example Of Pharmacotherapy For Lbp In Research or Developmenmentioning

confidence: 99%

Is there an unmet pharmacological need in chronic lower back pain?

Hesselink¹

2017

J Med Therap

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Lower Back Pain (LBP) is a heterogeneous indication based on many different etiopathogeneses. Placebo response and natural course in LBP are complicating the outcome of drug trials. Non-drug treatments are effective and recommended as first choice in most guidelines. Pharmacological treatments are thus not first choice for the treatment of LBP. Expensive new drugs therefore are discouraged by opinion leaders and by the field itself. Drug effects in general are seen as only moderate to weak, and are often complicated by troublesome side effect issues. LBP, although a huge market, is segmented in many sub-indications, such as arthritic induced pain, sciatic pain, lumbar stenosis and Chronic Discogenic Low Back Pain. Drug development of New Chemical Entities (NCE's) in indications linked to LBP remains a risky business, given the situation above. Most therapies under evaluation for LBP are non-pharmacological, such as acupuncture, progressive relaxation, electromyography biofeedback, low-level laser therapy, operant therapy and cognitive-behavioral therapy. There is no consensus on what are currently promising NCE's in the pipeline (apart from what the companies themselves communicate). It seems that there is no unmet pharmacological need in this segment of the chronic pain market.

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Pharmacology, pharmacokinetics, and metabolism of the DNA-decoy AYX1 for the prevention of acute and chronic post-surgical pain

Cited by 11 publications

References 47 publications

Simultaneous targeted inhibition of Sox2‐Oct4 transcription factors using decoy oligodeoxynucleotides to repress stemness properties in mouse embryonic stem cells

Simultaneous targeted inhibition of Sox2‐Oct4 transcription factors using decoy oligodeoxynucleotides to repress stemness properties in mouse embryonic stem cells

Involvement of transient receptor potential vanilloid 2 in intra‐oral incisional pain

Is there an unmet pharmacological need in chronic lower back pain?

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