Tatiana Barichello,PhD Assistant Professor Department of Psychiatry and Behavioral Sciences.
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Transcript of Tatiana Barichello,PhD Assistant Professor Department of Psychiatry and Behavioral Sciences.
![Page 1: Tatiana Barichello,PhD Assistant Professor Department of Psychiatry and Behavioral Sciences.](https://reader035.fdocuments.us/reader035/viewer/2022070410/56649f265503460f94c3d300/html5/thumbnails/1.jpg)
Tatiana Barichello,PhDAssistant Professor
Department of Psychiatry and Behavioral Sciences
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Today I’ll talk about:Bacterial traversal of the BBB.Recognition receptors.Second messenger systems.Rodent model of bacterial meningitis.BBB integrity.Cytokines/chemokines.Cognitive impairment.Depressive-like behavior.
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Meningitis is characterized by acute purulent infection of the meninges affecting the pia mater, the arachnoid and subarachnoid space (van de Beek et al., N Engl J Med, 2006).
The mortality ranges are from 16 to 37% and neurological sequelae including, hearing loss, focal neurological deficits.
Cognitive impairment is estimated to occur in 30 to 52% of surviving patients from pneumococal meningitis (Mook-Kanamori et al., Clin Microbiol Rev, 2011; Nau et al., Expert Rev Anti Infect Ther, 2015).
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Bacterial meningitis during early life was associated with higher depressive and anxiety symptoms, and increased risk of psychotic experiences; risk ratio 2.22 (Avon Longitudinal Study of Parents and Children (ALSPAC), Khandaker et al., Ann Epidemiol, 2015).
The risk of impairment from bacterial meningitis is greater in low-income countries.
Africa (25.1%), South Asia (21.6%), compared with Europe (9.4%) (Liechti et al., Fut. Microb. 2015).
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Transcellular traversal, the pathogens cross the BBB without any evidence of intercellular tight-junction disruption.
Paracellular traversal involves microbial penetration between BBB cells with and/or without evidence of tight-junction disruption.
The Trojan-horse mechanism involves microbial penetration of BBB cells using transmigration within infected phagocytes.
Mechanisms of Microbial Traversal of the BBB
(Kim, Nat Rev Microbiol, 2010).
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(Barichello et al., Oximed, 2013).
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Second messenger systems
(Barichello et al., J Med Microbiol, 2013)
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Leukocytes migrate to sites of infection. Sialyl-Lewisx on leukocytes binds to selectins-P and -E on endothelial cells along a gradient of chemoattractants substances.
(Barichello et al., Oximed, 2013)
Leukocyte Migration
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Microorganisms are cultured overnight in 10 ml of Todd Hewitt
broth. The culture is centrifuged and re-suspended in sterile saline to the
concentration of 5x109cfu/ml.
The anesthesia, consists of an intraperitoneal administration of ketamine,
xylazine. Rodents receiving via cisterna magna either 10 µl of artificial CSF as a placebo or an equivalent volume of bacterial suspension.
Meningitis Induction
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Cytokines
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Arterial plasma: CINC-1 increased at 6h after pneumococcal meningitis.
Jugular plasma: CINC-1 increased at 3 and 6h after pneumococcal
meningitis.
Cytokines are produced in jugular venous blood before arterial blood
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BBB breakdown between 12 and 24 h in the hippocampus and in the cortex at 12 and 18 h after pneumococcal meningitis induction.
Blood Brain Barrier Integrity
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In the step-down latency, 10 days after meningitis induction, there was no significant difference between training and test in the meningitis group, suggesting impairment of aversive memory (Barichello et al., JNT, 2010).
Long-term Cognitive ImpairmentStep-down Inhibitory Avoidance Task
1. Training: Immediately after step down on the grid, rodents received a foot shock.
2. In test session: 24 h after training, no foot shock was given and the step-down latency was used as a measure of retention.
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Control/ Control/ Meningitis/ Meningitis/0
100
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400Training
Test
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*
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IL-1Ra IL-1Ra
La
ten
cy (
sec)
Saline Saline
The meningitis/IL-Ra groups there were difference between training and test session preserving the aversive memory in this group.
Step-down inhibitory avoidance task1. Training: 5 min.2. Test: 5 min/24 h after.
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Sham Meningitis + Cefriaxone Meningitis + Daptomycin0
100
200
300
400
Training
Test
*
*
Late
ncy
(sec
)
Daptomycin prevented impairment of aversive memory.
Step-down inhibitory avoidance task1. Training: 5 min.2. Test: 5 min/24 h after.
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Sham Sham/Inhibitor Meningitis Meningitis/Inhibitor0
100
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400
Training
Test
* * *
Late
ncy
(sec
)
Step-down inhibitory avoidance task 10 days after the induction of meningitis. The indoleamine 2,3-dioxygenase inhibitor prevented of aversive memory.
1. Training: Immediately after stepping down on the grid, rodents received a foot shock.
2. In test session: 24 h after training, no foot shock was given and the step-down latency was used as a measure of retention.
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Sham Meningitis CBD 2.5 CBD 5 CBD 100
50
100
150
200Training
Test
**
________________________________________________________ Menigitis
La
ten
cy (
sec)
The cannabidiol prevented of aversive memory.
Step-down inhibitory avoidance task1. Training: 5 min.2. Test: 5 min/24 h after.
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Sham Meningitis + Cefriaxone Meningitis + Daptomycin0.0
0.5
1.0
1.5
2.0
Training
STM
LTM
* *
* *
Rec
ogni
tion
Inde
x (s
ec)
LTM:24 h after training: familiar (A) and a new object (C).
Training: 2 identical objects.
STM:1.5h after training: familiar (A) and novel (B) object.
Demonstrating short- and long-term memory impairment for novel object recognition.They did not spend a significantly higher percentage of time exploring the novel object. Daptomycin reversed.
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Control/ Control/ Meningitis/ Meningitis/0.0
0.5
1.0
1.5
2.0Training
Test* * *
IL-1Ra IL-1RaSalineSaline
Re
cog
nit
ion
in
de
x
The meningitis/IL-1Ra groups showed difference between training and test sessions demonstrating long-term memory for novel object recognition.
IL-1Ra: Object Recognition task
LTM:24 h after training: familiar (A) and a new object (C).
Training: 2 identical objects.
STM:1.5h after training: familiar (A) and novel (B) object.
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Summary of Part I
The cytokines increase prior of BBB disruption.
The rodents presented long-term cognitive impairment.
Kynurenine pathway, cytokines, non-bacteriolytic antibiotic
prevented memory impairment.
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1. The training session: 5 min. 2. Test session after 24 h: 5 min.
Imipramine treatment reversed depressive like-behavior.
0
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#
Control/sal Control/IMI Meningitis/sal Meningitis/IMI
Immo
bility
(sec
)
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Treatment with imipramine reverted the reduction of sweet food consumption when compared to meningitis/saline.
Imipramine prevented anhedonia-like behavior.
“Imipramine” Prevented Depressive-like Behavior
1.Trials: 5 days sessions/3 min. 2.Test: 2 test sessions/3 min.
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“Imipramine” decreased Corticosterone and ACTH levels
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Summary of Part II
In the present research we showed experimental
bacterial meningitis during childhood presented with
depressive-like behaviour in adulthood.
The rodents also demonstrated pathophysiological
findings similar to patients with depression.
They improved their behaviour in response to
imipramine treatment.
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New treatment options: a perspective from rodent model
Barichello et al., J Neuroimmunol, 2015
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Tatiana Barichello, PhDDepartment of Psychiatryc and Behavioral Sciences
[email protected]@unesc.net