Characterization of Mechanical Allodynia and Skin Innervation in a Mouse Model of Type-2 Diabetes Induced by Cafeteria-Style Diet and Low-Doses of Streptozotocin

Castañeda-Corral, Gabriela; Velázquez-Salazar, Norma B; A, Martínez-Martínez; Taboada-Serrano, Juanita N; Núñez-Aragón, Pablo Noé; González-Palomares, Laura; Acosta-González, Rosa Issel; Petricevich, Vera L.; Acevedo-Fernández, Juan José; Montes, Sergio; Jiménez-Andrade, Juan Miguel

doi:10.3389/fphar.2020.628438

Cited by 5 publications

(3 citation statements)

References 61 publications

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“…It is possible that the initial phase of hypersensitivity was not replicated in these studies due to the acute period of T2DM induction. In contrast to the absence of hypoesthesia in female mice in this study, another study reported long-term allodynia using the same T2DM induction protocol as this study, although their study examined female C57BL/6 mice (Castañeda-Corral et al, 2021).…”

Section: Discussionmentioning

confidence: 65%

Artificial light at night alters progression of cold neuropathy in a sex-dependent manner in a mouse model of type II diabetes mellitus

Bumgarner,

White,

Brown

et al. 2024

Front. Photon.

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Artificial light at night (ALAN) is a pervasive circadian rhythm disruptor. Exposure to ALAN is associated with detrimental effects on physiology and behavior, including disrupted metabolism, immune function, endocrine function, and pain behavior. Given the detrimental effects of ALAN and other circadian rhythm disruptors on pain, we sought to understand how ALAN may alter the progression and severity of diabetic neuropathy. To do this, we used a previously reported high-fat diet and streptozotocin injection protocol to induce a type II diabetic phenotype in ∼8 week old female and male mice and then exposed the mice to either control or ALAN lighting conditions in 14:10 h light-dark cycles for 4 weeks. Male mice housed in control conditions exhibited reduced responsiveness to cold pain; in contrast, ALAN blunted this effect in male mice. ALAN exposure also elevated blood glucose and altered body mass loss in male mice. These effects were not present in female mice. The results of this study highlight the need to consider and study ALAN exposure and sex as a biological variable as risk factors in the treatment and mitigation of pain.

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Section: Discussionmentioning

confidence: 65%

Artificial light at night alters progression of cold neuropathy in a sex-dependent manner in a mouse model of type II diabetes mellitus

Bumgarner,

White,

Brown

et al. 2024

Front. Photon.

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“…The doses were selected based on those used in previous studies on pregabalin (Bardin et al, 2010;Chen et al, 2001;Eutamene et al, 2000;Goncalves & Dickenson, 2012;Kiso et al, 2008;Peng et al, 2012), duloxetine (Bardin et al, 2010;Iyengar et al, 2004;Kiso et al, 2008) and diclofenac (Granados-Soto et al, 2004;Khan et al, 2018;Sukriti & Pandhi, 2004). However, we cannot rule out the possibility that different doses could produce different results, specifically in the case of diclofenac as varied doses were used in other studies (Allchorne et al, 2012;Castaneda-Corral et al, 2020).…”

Section: Discussionmentioning

confidence: 95%

Response profile in a rat model of exercise‐induced hypoalgesia is associated with duloxetine, pregabalin and diclofenac effect on constriction‐induced neuropathy

Khan

Wang

Korczeniewska

et al. 2022

European Journal of Pain

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Background Exercise is a known trigger of the inhibitory pain modulation system and its analgesic effect is termed exercise‐induced hypoalgesia (EIH). Previous studies have demonstrated that rats with deficient analgesic response following exercise develop more significant hypersensitivity following nerve injury compared to rats with substantial analgesic response following exercise. Objectives A rat model of EIH as an indicator of the pain inhibitory system's efficiency was used to explore the association between EIH profiles and the effect of pharmacotherapy on rat's neuropathic pain. Methods EIH profiles were assessed by evaluating paw responses to mechanical stimuli before and after exercise on a rotating rod. Rats with a reduction of ≤33% in responses were classified as low EIH and those with ≥67% as high EIH. Low and high EIH rats underwent sciatic nerve chronic constriction injury (CCI). Paw responses to mechanical stimuli were measured at baseline, following CCI, and after treatment with diclofenac, duloxetine or pregabalin. In a different group of low and high EIH rats, EIH was measured before and following treatment with the same medications. Results Low EIH rats developed more significant hypersensitivity following CCI. Duloxetine and pregabalin successfully reduced hypersensitivity, although significantly more so in low EIH rats. Diclofenac had limited effects, and only on low EIH rats. Four days of duloxetine administration transformed low EIH rats' profiles to high EIH. Conclusions The findings of this study suggest that EIH profiles in rats can not only predict the development of hypersensitivity following injury but may also support targeted pharmacological treatment. Significance Exercise is a known trigger of the inhibitory pain modulation. Rats with deficient analgesic response following exercise develop more significant hypersensitivity following nerve injury. Pain modulation profiles in rats can also support targeted pharmacological treatment; rats with deficient analgesic response following exercise benefit more from treatment with duloxetine and gabapentin. Treatment with duloxetine can improve pain modulation profile.

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“…Moreover, chronic pain has also been investigated in metabolic disorder neuropathies [ 52 , 53 ]. Preclinical models of chronic pain induced by metabolic disorder neuropathies are based on chemical and surgical approaches, genetic, and diet alterations.…”

Section: Sexual Dimorphism Of Pain In Pre-clinical Studiesmentioning

confidence: 99%

Sexual Dimorphism in the Mechanism of Pain Central Sensitization

Barcelon

Chung

Lee

et al. 2023

Cells

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It has long been recognized that men and women have different degrees of susceptibility to chronic pain. Greater recognition of the sexual dimorphism in chronic pain has resulted in increasing numbers of both clinical and preclinical studies that have identified factors and mechanisms underlying sex differences in pain sensitization. Here, we review sexually dimorphic pain phenotypes in various research animal models and factors involved in the sex difference in pain phenotypes. We further discuss putative mechanisms for the sexual dimorphism in pain sensitization, which involves sex hormones, spinal cord microglia, and peripheral immune cells. Elucidating the sexually dimorphic mechanism of pain sensitization may provide important clinical implications and aid the development of sex-specific therapeutic strategies to treat chronic pain.

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Characterization of Mechanical Allodynia and Skin Innervation in a Mouse Model of Type-2 Diabetes Induced by Cafeteria-Style Diet and Low-Doses of Streptozotocin

Cited by 5 publications

References 61 publications

Artificial light at night alters progression of cold neuropathy in a sex-dependent manner in a mouse model of type II diabetes mellitus

Artificial light at night alters progression of cold neuropathy in a sex-dependent manner in a mouse model of type II diabetes mellitus

Response profile in a rat model of exercise‐induced hypoalgesia is associated with duloxetine, pregabalin and diclofenac effect on constriction‐induced neuropathy

Sexual Dimorphism in the Mechanism of Pain Central Sensitization

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