Female gonadal hormone effects on microglial activation and functional outcomes in a mouse model of moderate traumatic brain injury

Umeano, Odera; Wang, Haichen; Dawson, Hana N.; Lei, Beilei; Umeano, Afoma; Kernagis, Dawn; James, Michael L.

doi:10.5492/wjccm.v6.i2.107

Cited by 5 publications

(2 citation statements)

References 45 publications

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“…As such, our analysis with fibrinogen demonstrated acute sex-specific neuroprotection to BBB compromise. The above is corroborated by Umeano and colleagues in which following a closed-head injury model, the effect of BBB protection in females was diminished with the absence of sex hormones as a result of ovariectomy [43]. Together with our behavioral data, this finding implies that it is not necessarily the injury parameters that are responsible for inducing sex-specific effects of TBI-induced neuroinflammation, but rather the sex-specific biological response to injury that can account for differences observed.…”

Section: Discussionsupporting

confidence: 87%

Reward and immune responses in adolescent females following experimental traumatic brain injury

Cannella

Andrews

Razmpour

et al. 2020

Behavioural Brain Research

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The pathology of traumatic brain injury (TBI) adversely affects many brain regions, often resulting in the development of comorbid psychiatric disorders including substance use disorders (SUD). Although traditionally thought to be an epidemic that predominantly affects males, recent clinical studies report females have higher rates of concussions and longer recovery times than males. Yet, how neurotrauma, particularly deep within the brain, between the sexes is differentially manifested remains largely unknown. The risk of TBI peaks during adolescence when neuronal networks that regulate reward behaviors are not fully developed. Previously, using the conditioned place preference (CPP) assay, we found that adolescent TBI increased susceptibility to the rewarding effects of cocaine in male mice. Further, we observed augmented inflammatory profiles, increased microglial phagocytosis of neuronal proteins, and decreased neuronal spine density in the NAc. Notably, the extent of sex differences in SUD susceptibility following TBI has not be investigated. Thus, here we ask the central question of whether the adolescent TBI-induced neuroinflammatory profile at reward centers is divergent in a sex-dependent manner. Using the CPP assay, we found that female mice with high levels of female sex hormones at the time of adolescent TBI demonstrated neuroprotection against increased sensitivity to the rewarding effects of cocaine. These studies also provide evidence of significantly reduced microglial activation and phagocytosis of neuronal proteins within the NAc of females. Overall, our results offer crucial insight into how adolescent TBI impacts the reward pathway in a sex depending manner that could explain a vulnerability to addiction-like behavior.

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Section: Discussionsupporting

confidence: 87%

Reward and immune responses in adolescent females following experimental traumatic brain injury

Cannella

Andrews

Razmpour

et al. 2020

Behavioural Brain Research

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“…The finding that female DAGL-b + / + mice showed high TBI survival rates is consistent with female rodents being generally protected from TBI-induced mortality compared with males. 39,40 The high rate of survival in female mice indicates that DAGL-b plays a sex-dependent role. Although the mechanisms underlying female protection from TBI mortality remain unclear, in this study, we consider several possibilities.…”

Section: Discussionmentioning

confidence: 99%

Diacylglycerol Lipase-β Knockout Mice Display a Sex-Dependent Attenuation of Traumatic Brain Injury-Induced Mortality with No Impact on Memory or Other Functional Consequences

O'Brien

Smith

Donvito

et al. 2021

Cannabis and Cannabinoid Research

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Background: The endogenous cannabinoid system modulates inflammatory signaling in a variety of pathological states, including traumatic brain injury (TBI). The selective expression of diacylglycerol lipase-b (DAGL-b), the 2-arachidonylglycerol biosynthetic enzyme, on resident immune cells of the brain (microglia) and the role of this pathway in neuroinflammation, suggest that this enzyme may contribute to TBI-induced neuroinflammation. Accordingly, we tested whether DAGL-b À/À mice would show a protective phenotype from the deleterious consequences of TBI on cognitive and neurological motor functions. Materials and Methods: DAGL-b À/À and -b + / + mice were subjected to the lateral fluid percussion model of TBI and assessed for learning and memory in the Morris water maze (MWM) Fixed Platform (reference memory) and Reversal (cognitive flexibility) tasks, as well as in a cued MWM task to infer potential sensorimotor/motivational deficits. In addition, subjects were assessed for motor behavior (Rotarod and the Neurological Severity Score assays) and in the light/dark box and the elevated plus maze to infer whether these manipulations affected anxietylike behavior. Finally, we also examined whether brain injury disrupts the ceramide/sphingolipid lipid signaling system and if DAGL-b deletion offers protection. Results: TBI disrupted all measures of neurological motor function and reduced body weight, but did not affect body temperature or performance in common assays used to infer anxiety. TBI also impaired performance in MWM Fixed Platform and Reversal tasks, but did not affect cued MWM performance. Although no differences were found between DAGL-b À/À and -b + / + mice in any of these measures, male DAGL-b À/À mice displayed an unexpected survival-protective phenotype, which persisted at increased injury severities. In contrast, TBI did not elicit mortality in female mice regardless of genotype. TBI also produced significant changes in sphingolipid profiles (a family of lipids, members of which have been linked to both apoptotic and antiapoptotic pathways), in which DAGL-b deletion modestly altered levels of select species. Conclusions: These findings indicate that although DAGL-b does not play a necessary role in TBI-induced cognitive and neurological function, it appears to contribute to the increased vulnerability of male mice to TBIinduced mortality, whereas female mice show high survival rates irrespective of DAGL-b expression.

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Effects of sex and pro-inflammatory cytokines on context discrimination memory

McNaughton

Williamson

2023

Behavioural Brain Research

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Female gonadal hormone effects on microglial activation and functional outcomes in a mouse model of moderate traumatic brain injury

Cited by 5 publications

References 45 publications

Reward and immune responses in adolescent females following experimental traumatic brain injury

Reward and immune responses in adolescent females following experimental traumatic brain injury

Diacylglycerol Lipase-β Knockout Mice Display a Sex-Dependent Attenuation of Traumatic Brain Injury-Induced Mortality with No Impact on Memory or Other Functional Consequences

Effects of sex and pro-inflammatory cytokines on context discrimination memory

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