Spared Nerve Injury Causes Sexually Dimorphic Mechanical Allodynia and Differential Gene Expression in Spinal Cords and Dorsal Root Ganglia in Rats

Ahlström, Fredrik; Mätlik, Kert; Viisanen, Hanna; Blomqvist, Kim; Liu, X.; Lilius, Tuomas; Sidorova, Yulia; Kalso, Eija; Rauhala, Pekka

doi:10.1007/s12035-021-02447-1

Cited by 36 publications

(35 citation statements)

References 102 publications

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“…Other male-prevalent RAGs included the AP-1 component c-Fos ( Fos ). RAGs were consistently upregulated at later stages of PNI, including sciatic nerve chronic constriction injury (CCI; Stephens et al, 2019 ; Ahlström et al, 2021 ). We suggest that their early activation and sustained long-term expression are indispensable for a robust response to injury.…”

Section: Resultsmentioning

confidence: 99%

“…Additional considerations were given to the timing of sexually dimorphic changes, which directly relate to the temporal coordination of biological and behavioral processes. Generally, male DRG displayed a significantly higher number of differentially expressed genes, both up- and downregulated, in response to PNI within 24 h, than on day 7 ( Ahlström et al, 2021 ) and day 14 PNI timepoints ( Stephens et al, 2019 ). By comparing the most prominent sexually dimorphic transcripts at the early and later stages of PNI response, we observed consistent regulation of genes related to immunological response, neuronal transmission, regeneration, and plasticity obtained on day 7 ( Ahlström et al, 2021 ) and day 14 PNI timepoints in rats ( Stephens et al, 2019 ).…”

Section: Discussionmentioning

confidence: 96%

“…Generally, male DRG displayed a significantly higher number of differentially expressed genes, both up- and downregulated, in response to PNI within 24 h, than on day 7 ( Ahlström et al, 2021 ) and day 14 PNI timepoints ( Stephens et al, 2019 ). By comparing the most prominent sexually dimorphic transcripts at the early and later stages of PNI response, we observed consistent regulation of genes related to immunological response, neuronal transmission, regeneration, and plasticity obtained on day 7 ( Ahlström et al, 2021 ) and day 14 PNI timepoints in rats ( Stephens et al, 2019 ). However, as outlined in the present study, many sexually dimorphic and monomorphic transcripts were specific for the early stages of PNI response.…”

Section: Discussionmentioning

confidence: 96%

“…Transcriptome RNA-sequencing (RNA-seq)-based analyses of human DRG at baseline ( Ray et al, 2019 ) and in patients with radicular/neuropathic pain ( North et al, 2019 ) highlighted DRG’s central role in sex-specific gene regulation. Likewise, emerging research has revealed sexual dimorphism in rodent DRG transcriptomes in response to peripheral nerve injury ( Stephens et al, 2019 ; Ahlström et al, 2021 ), hyperalgesic priming by interleukin 6 (Il-6; Paige et al, 2020 ), sciatic nerve injection of myelin basic protein (MBP) derived peptides ( Chernov et al, 2020 ), and other stimuli. Transcriptome differences in DRG have been implicated in female-prevalent hypersensitivity partly due to the activity of prostaglandin signaling and neuroendocrine mechanisms involving prolactin receptors ( North et al, 2019 ; Ray et al, 2019 ; Chernov et al, 2020 ; Mecklenburg et al, 2020 ; Paige et al, 2020 ; Tavares-Ferreira et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

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Sexual Dimorphism of Early Transcriptional Reprogramming in Dorsal Root Ganglia After Peripheral Nerve Injury

Chernov

Shubayev

2021

Front. Mol. Neurosci.

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Peripheral nerve injury induces genome-wide transcriptional reprogramming of first-order neurons and auxiliary cells of dorsal root ganglia (DRG). Accumulating experimental evidence suggests that onset and mechanistic principles of post-nerve injury processes are sexually dimorphic. We examined largely understudied aspects of early transcriptional events in DRG within 24 h after sciatic nerve axotomy in mice of both sexes. Using high-depth RNA sequencing (>50 million reads/sample) to pinpoint sexually dimorphic changes related to regeneration, immune response, bioenergy, and sensory functions, we identified a higher number of transcriptional changes in male relative to female DRG. In males, the decline in ion channel transcripts was accompanied by the induction of innate immune cascades via TLR, chemokine, and Csf1-receptor axis and robust regenerative programs driven by Sox, Twist1/2, and Pax5/9 transcription factors. Females demonstrated nerve injury-specific transcriptional co-activation of the actinin 2 network. The predicted upstream regulators and interactive networks highlighted the role of novel epigenetic factors and genetic linkage to sex chromosomes as hallmarks of gene regulation post-axotomy. We implicated epigenetic X chromosome inactivation in the regulation of immune response activity uniquely in females. Sexually dimorphic regulation of MMP/ADAMTS metalloproteinases and their intrinsic X-linked regulator Timp1 contributes to extracellular matrix remodeling integrated with pro-regenerative and immune functions. Lexis1 non-coding RNA involved in LXR-mediated lipid metabolism was identified as a novel nerve injury marker. Together, our data identified unique early response triggers of sex-specific peripheral nerve injury regulation to gain mechanistic insights into the origin of female- and male-prevalent sensory neuropathies.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Sexual Dimorphism of Early Transcriptional Reprogramming in Dorsal Root Ganglia After Peripheral Nerve Injury

Chernov

Shubayev

2021

Front. Mol. Neurosci.

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“…In the periphery, naïve female rats were shown to have fewer CGRP-immunoreactive dorsal root ganglion (DRG) neurons than their male counterparts, though ovariectomy produced a significant increase in immunoreactive neurons (Yang et al, 1998 ). A recent study reported no significant sex differences in CGRP-immunostaining cells in the DRG 7 days after the induction of neuropathic pain using the spared nerve injury (SNI) model (Ahlström et al, 2021 ). To our knowledge, this study is the first to report neuropathic pain stage-specific sex differences in mRNA expression levels of CGRP and its receptor components within the brain.…”

Section: Discussionmentioning

confidence: 99%

Sex Differences in CGRP Regulation and Function in the Amygdala in a Rat Model of Neuropathic Pain

Presto

Neugebauer

2022

Front. Mol. Neurosci.

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The amygdala has emerged as a key player in the emotional response to pain and pain modulation. The lateral and capsular regions of the central nucleus of the amygdala (CeA) represent the “nociceptive amygdala” due to their high content of neurons that process pain-related information. These CeA divisions are the targets of the spino-parabrachio-amygdaloid pain pathway, which is the predominant source of calcitonin gene-related peptide (CGRP) within the amygdala. Changes in lateral and capsular CeA neurons have previously been observed in pain models, and synaptic plasticity in these areas has been linked to pain-related behavior. CGRP has been demonstrated to play an important role in peripheral and spinal mechanisms, and in pain-related amygdala plasticity in male rats in an acute arthritis pain model. However, the role of CGRP in chronic neuropathic pain-related amygdala function and behaviors remains to be determined for both male and female rats. Here we tested the hypothesis that the CGRP1 receptor is involved in neuropathic pain-related amygdala activity, and that blockade of this receptor can inhibit neuropathic pain behaviors in both sexes. CGRP mRNA expression levels in the CeA of male rats were upregulated at the acute stage of the spinal nerve ligation (SNL) model of neuropathic pain, whereas female rats had significantly higher CGRP and CGRP receptor component expression at the chronic stage. A CGRP1 receptor antagonist (CGRP 8-37) administered into the CeA in chronic neuropathic rats reduced mechanical hypersensitivity (von Frey and paw compression tests) in both sexes but showed female-predominant effects on emotional-affective responses (ultrasonic vocalizations) and anxiety-like behaviors (open field test). CGRP 8-37 inhibited the activity of CeA output neurons assessed with calcium imaging in brain slices from chronic neuropathic pain rats. Together, these findings may suggest that CGRP1 receptors in the CeA are involved in neuropathic pain-related amygdala activity and contribute to sensory aspects in both sexes but to emotional-affective pain responses predominantly in females. The sexually dimorphic function of CGRP in the amygdala would make CGRP1 receptors a potential therapeutic target for neuropathic pain relief, particularly in females in chronic pain conditions.

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Indirect involvement of α2-adrenoceptors in the mechanical antihypersensitivity effect induced by the spinally administered imidazoline I1 receptor ligand LNP599 in a rat model of experimental neuropathy

Wei,

Vuorenpää,

Laurila

et al. 2024

Brain Research Bulletin

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Spared Nerve Injury Causes Sexually Dimorphic Mechanical Allodynia and Differential Gene Expression in Spinal Cords and Dorsal Root Ganglia in Rats

Cited by 36 publications

References 102 publications

Sexual Dimorphism of Early Transcriptional Reprogramming in Dorsal Root Ganglia After Peripheral Nerve Injury

Sexual Dimorphism of Early Transcriptional Reprogramming in Dorsal Root Ganglia After Peripheral Nerve Injury

Sex Differences in CGRP Regulation and Function in the Amygdala in a Rat Model of Neuropathic Pain

Indirect involvement of α2-adrenoceptors in the mechanical antihypersensitivity effect induced by the spinally administered imidazoline I1 receptor ligand LNP599 in a rat model of experimental neuropathy

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