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Sepsis (and the kidney): what’s new? What’s hot?
Vincenzo Cantaluppi
SCDU Nefrologia e Trapianto Renale,
Dipartimento di Medicina Traslazionale,Università del Piemonte Orientale,
AOU Maggiore della Carità,Novara
University of Eastern Piedmont- Center for Experimental
UPO Medical Research-UNITO
EUROPE400 cases of sepsis per 100,000 habitants annually
ITALYIn Italy there are
about 60,000 deaths due to sepsis every year
Sepsis, Septic Shock, Refractory Septic Shock(different severity = different outcomes)
Insult
Acute Renal Failure and Sepsis
Robert W. Schrier, M.D., and Wei Wang, M.D 1999
Acute renal failure occurs in approximately 19 percent of patients with
moderate sepsis, 23 percent with severe sepsis, and 51 percent with
septic shock when blood cultures are positive
Sepsis Septic ShockHealthy individual
Insult
Mort
alit
y
Refractory Septic Shock
NEP+EP requirement≥ 0.25 μg/kg/min
Refractory Septic Shock
Sepsis Septic ShockHealthy
Mo
rtality
Refractory Septic Shock
NEP+EP ≥ 0.25 mcg/kg/min
Three cornerstones of Sepsis Therapy
• Antibiotics and
Source Control
• Supportive Therapy
• Specific Therapy
– Immuno-modulation
Hemodynamic monitoring and support for prevention
and management of AKI
In patients in the ICU, use of either 4
percent albumin or normal saline for
fluid resuscitation results in similar
outcomes at 28 days.
Il primo grande studio randomizzato effettuato su pazienti settici e stato condotto
confrontando HES 200/0.60 a 0,66 con una gelatina e ha dimostrato una maggiore
incidenza di AKI.
Punti critici dello studio: SCr basale piu elevata nel gruppo HES, piccola dimensione
campionaria, breve durata del follow-up (34 giorni).
Kidney Liver
Bone marrow
84 studi inclusi
37 studi sull’uomo (tot 635 pz)
11 studi su animali
Storage occurrs within 30 min of infusion
HES deposits may last 8-10 ys (skin, kidney)
• Children with
severe febrile
illness and
impaired perfusion
20-40 ml/kg
of 5%
Albumin
0.9% saline
No bolus
• Primary endpoint
was 48h mortality
• Secondary
endpoints:
pulmonary edema,
increased
intracranial
pressure, and
mortality or
neurologic
sequelae at 4
weeks
Mortality (%) 10.6 vs 10.5 vs 7.3
Multicenter RCT, double-blind, placebo-
controlled trial
•251 patients to receive 50 mg of intravenous
hydrocortisone
Or
•248 patients to receive placebo every 6
hours for 5 days
A genomic storm: Refining the immune, inflammatory paradigm in trauma.
Immunosupression in Sepsis and Impaired Immunity
No New Genes or Pathways Activated
Sepsis is considered to induce immune
suppression, leading to increased susceptibility to
secondary infections with associated late
mortality
ICU–acquired infections occurred more
commonly in patients with sepsis with higher
disease severity, but such infections contributed
only modestly to overall mortality.
The genomic response of patients with sepsis
was consistent with immune suppression at the
onset of secondary infection.
Presepsin levels may have useful prognostic information for patients with severe sepsis
or septic shock.
Circulating sCD40L levels are increased in septic patients and are independently
associated with mortality
Numerous promising therapies targeting the maladaptive host immune response to sepsis are under investigation.
Importantly, these potential treatments can have an effect on the three different levels we have discussed earlier: the
number of immune cells; the proportion of cell subtypes with the modification of the leucocyte surface markers
expression; and the cell expression and function.
Multistep evaluation of immune cell activation, suppression, and homeostasis.
Endotoxin is an important mediator of septic shock and supports efforts to develop anti-endotoxin
therapies for treating patients with this disease.
ROS + RNS
Role of endotoxin in septic shock
LPS neutralization failed to save
patients with sepsis
Patients early severe sepsis or septic shock2:1 eritoran:placebo ratio
Eritoran is synthetic analog of lipid A/inhibits lipid A binding toMD2
Implications of lower mortality
• As long as lower mortality has been detected in
control arms of studies addressing new therapies in
sepsis, much larger sample size will be needed
• If sepsis associated mortality decreases because of
better standard of care, increase the likelihood that
therapies aimed to modulate innate immune
response result less effective
Compartmentalization of the inflammatory response in
sepsis and SIRS Cavaillon JM et al.
AKI Etiology
From an international study including >29,000 critically ill patients
48%
34%
27% 26%
19%
6%3%
12%
0
10
20
30
40
50
Sep
tic S
hock
Major
Sur
gery
Car
dioge
nic Sho
ck
Hyp
ovo
lemia
Dru
g-induc
ed
Hep
atore
nal S
yndro
me
Obs
truc
tive Uro
pathy
Oth
er
Uchino S, et al. JAMA. 2005;294:813-818.
% o
f P
ati
en
tsUchino S et al.
San Giovanni Battista Molinette Hospital Turin: AKI in ICU
RIFLE
Mortality (day 28)
TOTAL
1584 PATIENTS
13210 RRT
AKI 11,3%
Liver Tx (151/1335)
AKI 25% Lung Tx (22/88)
AKI 26,2 % Heart Tx (60/229)
Main cause of AKI in solid organ transplant recipients : sepsis (43,6%)
AKI in solid organ transplantation (liver, lung and heart)
SEPSIS AND AKI: THE “ENTANGLEMENT” QUESTION
Entanglement is a physical phenomenon that occurs when pairs or groups of particles are generated or interact in ways such that the quantum state of each particle cannot be described independently.
First defined by Erwin Schrodinger in
1935 as “something that can not be
separated”……..
AKI
SEPSI AND AKI: ENTANGLEMENT
AKI
1
2
AKI
SEPSIS: FREQUENT AFTER AKI
INCREASE MORTALITY AND HOSPITALIZATION
(PICARD STUDY)
PREDOMINANT PARADIGM
Septic AKI is associated with
reduced renal perfusion
-) loss of GFR by ischemia
-) Tubular ischemic injury
-) Acute tubular necrosis
… the hemodynamic hallmark of sepsis is generalized arterial
vasodilatation
E coli bolus E coli bolus
LA VASODILATAZIONE DELLA
ARTERIOLA EFFERENTE CAUSA
PERDITA DEL GFR.
PRESENZA DI SHUNT.
DISSOCIAZIONE FLUSSO – FUNZIONE RENALE IN CORSO DI SEPSI
Insufficienza renale acuta può complicare la sepsi anche in presenza di una
flusso renale normale, se non addirittura aumentato
Ang II riduce flusso renale
Migliora la funzione renale
Angiotensin II: effective
rescue vasopressor
agent in patients with
distributive shock
requiring multiple
vasopressors.
The initiation of an ATII
infusion in patients
receiving norepinephrine
for septic shock resulted
in a marked decrease
in norepinephrine doses.
ATII may be effective as a
novel pressor agent in
the treatment of high-
output shock.
Initial dosing ranges:
between 2 and 10
ng/kg/min. In the pilot
study, the drug appears
to be welltolerated.
No significant difference in the rate of death between
patients with shock who were treated with dopamine
or norepinephrine as the first-line vasopressor agent,
the use of dopamine was associated with a greater
number of adverse events such as arrhythmias.
Vasopressor therapy is safe and probably beneficial from a renal,
and probably general, point of view.
In hypotensive vasodilated patients with AKI, restoration of blood
pressure within autoregulatory values should occur promptly with
noradrenaline and be sustained until such vasodilatation dissipates.
The addition of vasopressin may be helpful in individual patients,
but widespread use is not supported by evidence.
Alpha-dose dopamine has no advantages over noradrenaline and is
not as reliably effective in restoring blood pressure and urine
output. Its widespread use cannot be supported in patients with
vasodilatation and acute kidney injury.
Terlipressin: useful in patients with AKI secondary to hepatorenal
syndrome.
An increasing body of evidence suggests that AKI can occur in the
absence of hypoperfusion.
Sepsis induces profound alterations in microcirculatory flow in the
entire organism, and the kidney is not the exception
Sepsis is associated with the release of damage and pathogen
associated molecular patterns (DAMPs and PAMPs) into the
circulation.
Circulating plasma factors induce tubular and glomerular
alterations in septic burns patientsFilippo Mariano,# Vincenzo Cantaluppi,# Maurizio Stella, Giuseppe Mauriello Romanazzi, Barbara
Assenzio, Monica Cairo, Luigi Biancone, Giorgio Triolo, V Marco Ranieri, and Giovanni Camussi
CIRCULATING ENDOTOXINS REDUCE RENAL OXYGENATION AND MODULATE MITOCHONDRIAL FUNCTION.
PGC-1 alpha REPRESENTS ONE OF THE MAIN REGULATORS OF MYTOCHONDRIAL BIOGENESIS AND ITS
EXPRESSION IS SUPPRESSED IN PROPORTION WITH RENAL FUNCTION IMPAIRMENT.
PGC-1 alpha LEVELS ARE ALSO REDUCED IN RELATIONSHIP WITH TNF-alpha ACTIVITY
Cell polarity/ tight junction dysfunction in MOF
Fink MP et al. RL.Epithelial barrier
dysfunction: a unifying theme to
explain the pathogenesis of multiple
organ dysfunction at the cellular
level.
Crit Care Clin. 2005 Apr;21(2):177-96.
Sepsis: tight junction injury
in lung, liver and bowel
epithelium. control sepsis
Sepsis modulates the tubular regulation of ion, glucose,
urea and water transport and acid–base homeostasis in the
kidney.
Recent discoveries on changes in epithelial transport under
septic and endotoxemic conditions as well as the
mechanisms that link inflammation with impaired tubular
membrane transport.
Tubular dysfunction that is mediated by inflammation in
sepsis ultimately leads to increased sodium and chloride
delivery to the distal tubule and macula densa, contributing
to tubuloglomerular feedback and GFR decrease.
Systemic inflammation is known to
target tubular epithelial cells (TECs),
leading to acute kidney injury.
Tubular cells have been implicated in
the response to inflammatory
mediators in
ischaemic and septic renal damage.
Loss of tubular cells by apoptosis or
epithelial-to-mesenchymal transition
may ingenerate conditions that lead
to progression towards
chronic kidney disease.
TECs may actively contribute to the
production of inflammatory
mediators that may propagate the
injury locally or in distant organs.
Prof. Peter Higgs
The Higgs’ boson or “the God’s particle”
AKI
What’s new in the
STANDARD MODEL?
PRODUCTION OF MICROVESICLES
Shedding vesicles are usually larger than exosomes with sizeranging from 100nm to 1mm.
Formation of shedding vesicles takes place from the buddingof small cytoplasmic protrusions followed by their detachmentfrom the cell surface dependent on calcium influx, calpain andcytoskeleton reorganization.
The intra-cellular levels of calcium ions modify the asymmetricphospholipids distribution of plasmamembranes by specificenzymes named flippase, floppase and scramblase.
The increase of calcium ions inhibits translocase and inducesactivation of scramblase that translocates phosphatydilserinefrom the inner leaflet of the cell membrane bilayer to theouter with changes in curvature-mediated lateralredistribution of membrane components with the formationof membrane nanodomains.
Calcium ions by activation of calpain which cleaves tallin andactivin, and of gelsolin which cleaves actin-capping proteinsalso favor the reorganization of cytoskeleton.
MICROVESICLES
James E. Rothman Randy W. Schekman Thomas C. Südhof
A mechanism of cell-to-cell communication…….
MICROVESCICOLE:L’ULTIMA FRONTIERA
Camussi G, Cantaluppi V et al Kidney Int 2010
Bioanalyzer RNA
profilingSmall RNAs
MicroRNAs
(RT-PCR)
FACS
Healthy Septic
0
1
2
3
4
5
6
7
8
9
10
1 2 3 4 5 6
Nr.
of
faile
d o
rgan
sNr. of failed organs
MICROVESICLES IN EXPERIMENTAL MODELS OF SEPSIS
i.p.LPS injection
Cecal ligation
and puncture
0
1
2
3
4
5
6
7
8
9
Control LPS CLP
MV
/ml
(10^
8)
Tubular epithelial
cells
Recently, two small phase II clinical trials
demonstrated beneficial renal effects of
bovine-derived alkaline phosphatase
administration in critically ill patients with
sepsis-associated AKI.
Rationale: related to dephosphorylation and
thereby detoxification of detrimental
molecules involved in the pathogenesis of
sepsis-associated AKI.
Potential target of alkaline phosphatase:
adenosine triphosphate, (proinflammatory
mediator released during cellular stress) and
endotoxin (LPS)
recAP can attenuate LPS-induced cytokine
production in a human renal cell line,
whereas recAP improves renal blood flow
and vascular resistance and inhibits various
parameters of renal inflammation and tissue
damage during AKI induced by ischemia-
reperfusion or by LPS injection in vivo.
Interestingly, recAP tends to also exert renal
protective effects during cisplatin- or
gentamicin-induced AKI, which may indicate
a broader use for recAP treatment than
sepsis-associated AKI alone (fig. 1
To evaluate whether
alkaline phosphatase (AP)
treatment improves renal
function in sepsis-induced
AKI, a prospective,
double-blind, randomized,
placebo-controlled study
in critically ill patients
with severe sepsis or
septic shock with evidence
of AKI was performed
The improvements in
renal function suggest
alkaline phosphatase is a
promising new treatment
for patients with severe
sepsis or septic shock with
AKI.
Start extracorporeal therapies?
MODALITY OF RRT
Renal replacement therapy for acute kidney injury: let's follow the
evidence.Ronco C.
LA DOSE DIALITICA
OTTIMALE PER AKI E’
CONTROVERSA
NON SI OTTIENE BENEFICIO
DA DOSI DIALITICHE MOLTO
ALTE
The dilemma of whether and
when to start RRT among
critically ill patients with AKI
in the absence of conventional
indications has long been a
vexing challenge for
clinicians.
Recently, two randomized
trials (ELAIN and AKIKI)
reported specifically on the
issue of the timing of initiation
of RRT in critically ill patients
with AKI
Their fundamental differences
in trial design, sample size,
and widely discrepant findings
are considered in context.
While both trials are
important contributions
towards
informing practice on this
issue, additional evidence from
large multicenter randomized
trials is needed.
Possible biological effects of different drugs and of extracorporeal blood purification
therapies on immune system activation, suppression,
and homeostasis
According to II law od
thermodynamics, spontaneous
chemical and biological reactions are
always accompained by a decrease in
free energy.
Natural course of entropy is distrupted
by the effects of kidney disease and
uremia
Polymyxin B hemoperfusion added to conventional therapy
significantly improved hemodynamics and organ
dysfunction and reduced 28-day mortality in a targeted
population with severe sepsis and/or septic shock from
intra-abdominal gram-negative infections.
Evaluating the Use of PMX-B Hemoperfusion in a Randomized controlled trial of Adults Treated for
Endotoxemia and Septic Shock
Severe sepsis and septic shock
(14000 pts/year Italy)
Endotoxins
septic shock
(9000 pts/year )
EUPHAS patients
What makes EUPHRATES unique?
Biomarkers and AKI: personalized
therapies
Septic AKI
-AKI to CKD-MOF
-Death
Kidney regenerationFunctional improvement -Wrong therapy
-Wrong timing
CRRT
M.O.S.T
Multiple Organ Support therapy
Ronco C et al, Blood Purification, 2005
UF systems
VAD
MARS
Prometheus BAL
CO2 removal
Islet encapsulation
Artifical pancreas
The “entanglement” between sepsis and AKI…..
Grazie
vincenzo.cantaluppi@med.uniupo.it
University of Eastern Piedmont- Center for Experimental
UPO Medical Research-UNITO
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