Adenosine Monophosphate-activated Protein Kinase (AMPK) Activators For the Prevention, Treatment and Potential Reversal of Pathological Pain

Price, Theodore J.; Das, Vaskar; Dussor, Gregory

doi:10.2174/1389450116666151102095046

Cited by 50 publications

(51 citation statements)

References 159 publications

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“…Our in vitro experiments on DRG neurons indicate the combination of resveratrol and metformin activate AMPK in at least an additive fashion. These data add to a growing body of evidence that AMPK activation can inhibit the development of acute mechanical hypersensitivity resulting from injury (Melemedjian et al, 2011, Tillu et al, 2012a, Russe et al, 2013, Bullon et al, 2015, Ma et al, 2015, Song et al, 2015, Maixner et al, 2016, Ling et al, 2017), reduce the excitability of nociceptors (Melemedjian et al, 2011, Tillu et al, 2012a, Melemedjian et al, 2013, Asiedu et al, 2017) and prevent the development of hyperalgesic priming (Price and Dussor, 2013, Price et al, 2015, Asiedu et al, 2016, Mejia et al, 2016). We conclude that topical resveratrol and co-treatment of various AMPK activators such as metformin are clinically relevant and could show utility as pain therapeutics in humans.…”

Section: Discussionmentioning

confidence: 58%

Pharmacological activation of AMPK inhibits incision-evoked mechanical hypersensitivity and the development of hyperalgesic priming in mice

et al. 2017

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New therapeutics to manage post-surgical pain are needed to mitigate the liabilities of opioid and other analgesics. Our previous work shows that key modulators of excitability in peripheral nociceptors, such as extracellular signal-regulated kinases (ERK) are inhibited by activation of adenosine monophosphate activated protein kinase (AMPK). We hypothesized that AMPK activation would attenuate acute incision-evoked mechanical hypersensitivity and the development of hyperalgesic priming caused by surgery in mice. Here we have used a variety of administration routes and combinations of AMPK activators to test this hypothesis. Topical administration of a resveratrol-based cream inhibited acute mechanical hypersensitivity evoked by incision and blocked the development of hyperalgesic priming. We also observed that systemic administration of metformin dose-dependently inhibited incision-evoked mechanical hypersensitivity and hyperalgesic priming. Interestingly, low doses of systemic metformin and local resveratrol that had no acute effect were able to mitigate development of hyperalgesic priming. Combined treatment with doses of systemic metformin and local resveratrol that were not effective on their own enhanced the acute efficacy of the individual AMPK activators for post-surgical mechanical pain alleviation and blocked the development of hyperalgesic priming. Finally, we used dorsal root ganglion (DRG) neurons in culture to show that resveratrol and metformin given in combination shift the concentration-response curve for AMPK activation to the left and increase the magnitude of AMPK activation. Therefore, we find that topical administration is an effective treatment route of administration and combining systemic and local treatments led to anti-nociceptive efficacy in acute mechanical hypersensitivity at doses that were not effective alone. Collectively our work demonstrates a specific effect of AMPK activators on post-surgical pain and points to novel therapeutic opportunities with potential immediate impact in the clinical setting.

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Section: Discussionmentioning

confidence: 58%

Pharmacological activation of AMPK inhibits incision-evoked mechanical hypersensitivity and the development of hyperalgesic priming in mice

et al. 2017

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“…Recent preclinical studies have suggested that metformin, a drug approved by the US Food and Drug Administration (FDA) for glycemic control in patients with type 2 diabetes, alleviates neuropathic and inflammatory pain in various models . We demonstrated that metformin also prevents cisplatin‐induced neuropathic pain, numbness, and loss of IENFs .…”

Section: Introductionmentioning

confidence: 81%

Beyond symptomatic relief for chemotherapy‐induced peripheral neuropathy: Targeting the source

Kavelaars

Dougherty

et al. 2018

Cancer

123

111

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Chemotherapy-induced peripheral neuropathy (CIPN) is a serious adverse side effect of many chemotherapeutic agents, affecting >60% of patients with cancer. Moreover, CIPN persists long into survivorship in approximately 20% to 30% of these patients. To the authors' knowledge, no drugs have been approved to date by the US Food and Drug Administration to effectively manage chemotherapy-induced neuropathic pain. The majority of the drugs tested for the management of CIPN aim at symptom relief, including pain and paresthesia, yet are not very efficacious. The authors propose that there is a need to acquire a more thorough understanding of the etiology of CIPN so that effective, mechanism-based, disease-modifying interventions can be developed. It is important to note that such interventions should not interfere with the antitumor effects of chemotherapy. Mitochondria are rod-shaped cellular organelles that represent the powerhouses of the cell, in that they convert oxygen and nutrients into the cellular energy "currency" adenosine triphosphate. In addition, mitochondria regulate cell death. Neuronal mitochondrial dysfunction and the associated nitro-oxidative stress represent crucial final common pathways of CIPN. Herein, the authors discuss the potential to prevent or reverse CIPN by protecting mitochondria and/or inhibiting nitro-oxidative stress with novel potential drugs, including the mitochondrial protectant pifithrin-μ, histone deacetylase 6 inhibitors, metformin, antioxidants, peroxynitrite decomposition catalysts, and anti-inflammatory mediators including interleukin 10. This review hopefully will contribute toward bridging the gap between preclinical research and the development of realistic novel therapeutic strategies to prevent or reverse the devastating neurotoxic effects of chemotherapy on the (peripheral) nervous system. Cancer 2018;124:2289-98. © 2018 American Cancer Society.

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“…Indeed, there are indications that these agents may mediate their effects through other cellular signaling pathways including those that involve pro-inflammatory cytokines, protein kinases, growth factors, and reactive oxygen species (ROS). 15,73,121,142,143 …”

Section: Second Messenger Pathwaysmentioning

confidence: 99%

Ion channels and neuronal hyperexcitability in chemotherapy-induced peripheral neuropathy

Aromolaran

Goldstein

2017

Mol Pain

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Cancer is the second leading cause of death worldwide and is a major global health burden. Significant improvements in survival have been achieved, due in part to advances in adjuvant antineoplastic chemotherapy. The most commonly used antineoplastics belong to the taxane, platinum, and vinca alkaloid families. While beneficial, these agents are frequently accompanied by severe side effects, including chemotherapy-induced peripheral neuropathy (CPIN). While CPIN affects both motor and sensory systems, the majority of symptoms are sensory, with pain, tingling, and numbness being the predominant complaints. CPIN not only decreases the quality of life of cancer survivors but also can lead to discontinuation of treatment, thereby adversely affecting survival. Consequently, minimizing the incidence or severity of CPIN is highly desirable, but strategies to prevent and/or treat CIPN have proven elusive. One difficulty in achieving this goal arises from the fact that the molecular and cellular mechanisms that produce CPIN are not fully known; however, one common mechanism appears to be changes in ion channel expression in primary afferent sensory neurons. The processes that underlie chemotherapy-induced changes in ion channel expression and function are poorly understood. Not all antineoplastic agents directly affect ion channel function, suggesting additional pathways may contribute to the development of CPIN Indeed, there are indications that these drugs may mediate their effects through cellular signaling pathways including second messengers and inflammatory cytokines. Here, we focus on ion channelopathies as causal mechanisms for CPIN and review the data from both pre-clinical animal models and from human studies with the aim of facilitating the development of appropriate strategies to prevent and/or treat CPIN.

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Adenosine Monophosphate-activated Protein Kinase (AMPK) Activators For the Prevention, Treatment and Potential Reversal of Pathological Pain

Cited by 50 publications

References 159 publications

Pharmacological activation of AMPK inhibits incision-evoked mechanical hypersensitivity and the development of hyperalgesic priming in mice

Pharmacological activation of AMPK inhibits incision-evoked mechanical hypersensitivity and the development of hyperalgesic priming in mice

Beyond symptomatic relief for chemotherapy‐induced peripheral neuropathy: Targeting the source

Ion channels and neuronal hyperexcitability in chemotherapy-induced peripheral neuropathy

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