tatiana barichello,phd assistant professor department of ......tatiana barichello, phd department of...
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Tatiana Barichello,PhD
Assistant 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.�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 ofthe meninges affecting the pia mater, the arachnoid andsubarachnoid space (van de Beek et al., N Engl J Med, 2006).
� The mortality ranges are from 16 to 37% and neurologicalsequelae including, hearing loss, focal neurological deficits.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 withhigher depressive and anxiety symptoms, and increasedrisk 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 inlow-income countries.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
Mechanisms of Microbial Traversal of the BBB
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.
(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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Leukocyte Migration
Leukocytes migrate to sites of infection. Sialyl-Lewisx onleukocytes binds to selectins-P and -E on endothelial cells along agradient of chemoattractants substances.
(Barichello et al., Oximed, 2013)
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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.
Meningitis Induction
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.
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Cytokines
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Cytokines are produced in jugular venous blood
before arterial blood
Arterial plasma: CINC-1 increased at 6h after pneumococcal meningitis.
Jugular plasma: CINC-1 increased at 3 and 6h after pneumococcal
meningitis.
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Blood Brain Barrier Integrity
BBB breakdown between 12 and 24 h in the hippocampus and in the cortex at 12 and 18 h after pneumococcal meningitis induction.
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Long-term Cognitive Impairment
Step-down Inhibitory Avoidance Task
In the step-down latency, 10 days after meningitis induction, there was nosignificant difference between training and test in the meningitis group,suggesting impairment of aversive memory (Barichello et al., JNT, 2010).
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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100
200
300
400Training
Test
*
*
*
La
ten
cy (
se
c)
Control/ Control/ Meningitis/ Meningitis/0
IL-1Ra IL-1RaSaline 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 task
1. Training: 5 min.
2. Test: 5 min/24 h after.
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200
300
400
Training
Test
*
*
La
ten
cy (
se
c)
Sham Meningitis + Cefriaxone Meningitis + Daptomycin0
100
La
ten
cy (
se
c)
Daptomycin prevented impairment of aversive memory.
Step-down inhibitory avoidance task
1. Training: 5 min.
2. Test: 5 min/24 h after.
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100
200
300
400
Training
Test
* * *
La
ten
cy
(s
ec
)
Sham Sham/Inhibitor Meningitis Meningitis/Inhibitor0
100
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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100
150
200Training
Test
**
La
ten
cy (
se
c)
Sham Meningitis CBD 2.5 CBD 5 CBD 100
50
________________________________________________________
Menigitis
The cannabidiol prevented of aversive memory.
Step-down inhibitory avoidance task
1. Training: 5 min.
2. Test: 5 min/24 h after.
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1.5
2.0
Training
STM
LTM
* *
* *
Re
co
gn
itio
n I
nd
ex (
se
c)
Training: 2 identical objects.
Sham Meningitis + Cefriaxone Meningitis + Daptomycin0.0
0.5
1.0
Re
co
gn
itio
n I
nd
ex (
se
c)
LTM:24 h after training: familiar (A) and a new object (C).
STM:1.5h after training: familiar (A) and novel (B) object.
Demonstrating short- and long-term memoryimpairment for novel object recognition.They did not spend a significantly higher percentageof time exploring the novel object.Daptomycin reversed.
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0.5
1.0
1.5
2.0Training
Test* * *
Re
co
gn
itio
n i
nd
ex
IL-1Ra: Object Recognition task
Training: 2 identical objects.
Control/ Control/ Meningitis/ Meningitis/0.0
0.5
IL-1Ra IL-1RaSalineSaline
Re
co
gn
itio
n i
nd
ex
The meningitis/IL-1Ra groups showed differencebetween training and test sessions demonstratinglong-term memory for novel object recognition.
LTM:24 h after training: familiar (A) and a new object (C).
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.The rodents presented long-term cognitive impairment.
Kynurenine pathway, cytokines, non-bacteriolytic antibiotic
prevented memory impairment.
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20
40
60
80
100 *
#
Imm
ob
ilit
y (
se
c)
1. The training session: 5 min.
2. Test session after 24 h: 5 min.
Imipramine treatment reversed depressive like-behavior.
0
20
Control/sal Control/IMI Meningitis/sal Meningitis/IMI
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“Imipramine” Prevented Depressive-like Behavior
Treatment with imipramine reverted the reduction of sweet food consumption when compared to meningitis/saline.
Imipramine prevented anhedonia-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, PhDTatiana Barichello, PhD
Department of Psychiatryc and Behavioral Sciences