Neuroimmune Activation Drives Multiple Brain States

Tchessalova, Daria; Posillico, Caitlin K.; Tronson, Natalie C.

doi:10.3389/fnsys.2018.00039

Cited by 38 publications

(38 citation statements)

References 115 publications

(165 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Although we did not observe microglial activation, it is likely that more subtle neuroimmune changes persist long after a subchronic immune challenge (Tchessalova et al, 2018). For example, persistent microglial priming persists to adulthood after early life immune challenge (Hoeijmakers, Heinen, van Dam, Lucassen, & Korosi, 2016;Williamson & Bilbo, 2013).…”

Section: Discussionmentioning

confidence: 53%

“…Together, these findings demonstrate progressive changes in neural function and sex-specific patterns of memory deficits emerging over the weeks and months following a mild, subchronic immune challenge. The delayed emergence of memory deficits in the absence of ongoing overt microglial activation suggests that the transient immune response exerts lasting indirect effects on neural function (Tchessalova, Posillico, & Tronson, 2018).…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Memory deficits in males and females long after subchronic immune challenge

Tchessalova

Tronson

2018

Preprint

Self Cite

View full text Add to dashboard Cite

Memory impairments and cognitive decline persist long after recovery from major illness or injury, and correlate with increased risk of later dementia. Here we developed a subchronic peripheral immune challenge model to examine delayed and persistent memory impairments in females and in males. We show that intermittent injections of either lipopolysaccharide or Poly I:C cause memory decline in both sexes that are evident eight weeks after the immune challenge. Importantly, we observed sex-specific patterns of deficits.Females showed impairments in object recognition one week after challenge that persisted for at least eight weeks. In contrast, males had intact memory one week after the immune challenge but exhibited broad impairments in memory tasks including object recognition, and both context and tone fear conditioning several months later. The differential patterns of memory deficits in males and in females were observed without sustained microglial activation or changes in blood-brain barrier permeability. Together, these data suggest that transient neuroimmune activity results in differential vulnerabilities of females and males to memory decline after immune challenge. This model will be an important tool for determining the mechanisms in both sexes that contribute to memory impairments that develop over the weeks and months after recovery from illness. Future studies using this model will provide new insights into the role of chronic inflammation in the pathogenesis of long-lasting memory decline and dementias.

show abstract

Section: Discussionmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 99%

Memory deficits in males and females long after subchronic immune challenge

Tchessalova

Tronson

2018

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…In contrast, females previously exposed to a subchronic immune challenge showed markedly different patterns of gene expression after an acute injection compared with previously naïve mice. Together with the sexspecific changes in baseline gene expression, where males but not females showed changes 12 weeks later, these findings suggest that males and females have different patterns of vulnerability and resilience to future stressors, immune challenge, and other environmental events (Tchessalova et al, 2018).…”

Section: Discussionmentioning

confidence: 74%

“…Here, females previously exposed to a subchronic immune challenge showed greater dysregulation of transcriptional response after an acute LPS injection, whereas males showed similar patterns of gene expression whether or not they had previously experienced a subchronic challenge. Thus both males and females show changes in transcriptional processes in the brain that persist long after a subchronic immune challenge, but the patterns of dysregulation show striking sex specificity, and suggest that males and females have different patterns of vulnerability and resilience to future stressors, including immune challenge, and other environmental events (Tchessalova et al, 2018).…”

Section: Discussionmentioning

confidence: 99%

“…The neuroimmune system, and its regulation by peripheral immune states, plays an important regulatory role for behavioral, affective, and cognitive functions (Raison et al, 2006;Tchessalova et al, 2018). In addition to their central role in behavioral and physiological changes during illness and injury (Dantzer et al, 1998), neuroimmune cells and cytokines are activated as a consequence of physical and psychological stressors (Bekhbat and Neigh, 2017), and are critical for normal neural functions including synaptic plasticity and memory (Avital et al, 2003;Yirmiya and Goshen, 2011;del Rey et al, 2013;Adamsky et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Enduring and sex-specific changes in hippocampal gene expression after a subchronic immune challenge

Tchessalova

Tronson

2019

Preprint

Self Cite

View full text Add to dashboard Cite

Acknowledgements:We would like to acknowledge the University of Michigan Bioinformatics core for their expertise and data analysis of differentially expressed genes and the University of Michigan DNA sequencing core for their processing of samples. We would like to sincerely thank Dr. Shigeki Iwase and Christina Vallianatos for their advice, support, and assistance with prepping of the RNA samples. We would also very much like to thank them for allowing us to use their laboratory equipment for RNA extraction.We thank Ms. Brynne Raines, Ms. Melanie Gil, and Ms. Caitlin Posillico for their extensive feedback on this manuscript. ABSTRACTMajor illnesses, including major surgery, heart attack, and sepsis, can cause long-lasting cognitive impairments, depression, and progressive memory decline that persist well after recovery from the original illness. Similarly, in animal models, immune challenge results in impairments of learning and memory as well as increased depression-like behaviors. Although neuroimmune signaling is now well established as playing a crucial role in the modulation of neural functions, how transient immune signaling mediates enduring changes in cognition, memory, and emotion remains unknown. We have recently demonstrated that a series of intermittent injections of lipopolysaccharides over a two-week period resulted in sex-specific patterns of memory deficits that persist at least several months after the end of the immune challenge. Here, we examined the persistent changes in hippocampal gene expression three months after this subchronic systemic immune challenge in males and in females. We used RNA-sequencing as a large-scale, unbiased approach to identify both persistent changes in gene expression long after an immune challenge, and changes in transcriptional response to a subsequent immune challenge. Males and females differed in number and patterns of gene expression in the hippocampus. In males, we observed enduring dysregulation of gene expression three months after the end of a subchronic immune challenge, in the absence of an additional insult. In contrast, females showed few persistent changes under basal conditions, but striking dysregulation of gene expression in response to an additional acute LPS injection. Striking sex differences in the specific genes, pathways, and biological processes affected were observed both after subchronic immune challenge and after a subsequent insult. Thus, subchronic systemic immune activation has enduring and sex-specific consequences for gene expression and response to subsequent stimuli. Such persistent changes in neural functions further suggest that in both males and females, neuroimmune signaling during illness contributes to subsequent vulnerability or resilience to cognitive decline, memory impairments, and affective disorders.

show abstract

Autocrine positive feedback of tumor necrosis factor from activated microglia proposed to be of widespread relevance in chronic neurological disease

Clark,

Vissel

2023

Pharmacology Res & Perspec

View full text Add to dashboard Cite

Over a decade's experience of post‐stroke rehabilitation by administering the specific anti‐TNF biological, etanercept, by the novel perispinal route, is consistent with a wide range of chronically diminished neurological function having been caused by persistent excessive cerebral levels of TNF. We propose that this TNF persistence, and cerebral disease chronicity, largely arises from a positive autocrine feedback loop of this cytokine, allowing the persistence of microglial activation caused by the excess TNF that these cells produce. It appears that many of these observations have never been exploited to construct a broad understanding and treatment of certain chronic, yet reversible, neurological illnesses. We propose that this treatment allows these chronically activated microglia to revert to their normal quiescent state, rather than simply neutralizing the direct harmful effects of this cytokine after its release from microglia. Logically, this also applies to the chronic cerebral aspects of various other neurological conditions characterized by activated microglia. These include long COVID, Lyme disease, post‐stroke syndromes, traumatic brain injury, chronic traumatic encephalopathy, post‐chemotherapy, post‐irradiation cerebral dysfunction, cerebral palsy, fetal alcohol syndrome, hepatic encephalopathy, the antinociceptive state of morphine tolerance, and neurogenic pain. In addition, certain psychiatric states, in isolation or as sequelae of infectious diseases such as Lyme disease and long COVID, are candidates for being understood through this approach and treated accordingly. Perispinal etanercept provides the prospect of being able to treat various chronic central nervous system illnesses, whether they are of infectious or non‐infectious origin, through reversing excess TNF generation by microglia.

show abstract

Neuroimmune Activation Drives Multiple Brain States

Cited by 38 publications

References 115 publications

Memory deficits in males and females long after subchronic immune challenge

Memory deficits in males and females long after subchronic immune challenge

Enduring and sex-specific changes in hippocampal gene expression after a subchronic immune challenge

Autocrine positive feedback of tumor necrosis factor from activated microglia proposed to be of widespread relevance in chronic neurological disease

Contact Info

Product

Resources

About