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Endocrine,
Metabolic & Immune Disorders - Drug Targets
ISSN: 1871-5303
Endocrine, Metabolic &
Immune Disorders - Drug Targets
Volume 6, Number 2, June 2006
Contents
Sepsis: From the Bench to the Bedside
Editorial Pp. 125-126
Gender And Susceptibility To Sepsis Following Trauma
Pp. 127-135
M.A. Choudhry, K.I. Bland and I.H. Chaudry
[Abstract]
Neuro-Immune-Endocrine Mechanisms During Septic Shock:
Role For Nitric Oxide in Vasopressin and Oxytocin Release
Pp. 137-142
E.C. Carnio, V. Moreto, A. Giusti-Paiva and J. Antunes-Rodrigues
[Abstract]
Bacterial Translocation, Microcirculation Injury and
Sepsis Pp. 143-150
I.H.J. Koh, A.M.A. Liberatore, J.L. Menchaca-Diaz, M.
Ruiz-Silva, L. Vilela-Oliveira, A. Y. Watanabe, R. Salomao,
U. Fagundes-Neto and R.M. Silva
[Abstract]
Neutrophil Function in Severe Sepsis Pp.
151-158
J.C. Alves-Filho, B.M. Tavares-Murta, C. Barja-Fidalgo,
C.F. Benjamim, A. Basile-Filho, S.M. Arraes and F.Q. Cunha
[Abstract]
Redox Mechanisms of Vascular Cell Dysfunction in Sepsis
Pp. 159-164
L.C.P. Azevedo, M. Janiszewski, F.G. Soriano and F.R.M
Laurindo
[Abstract]
Nitric Oxide and Cardiovascular Dysfunction in Sepsis
Pp. 165-173
J. Assreuy
[Abstract]
Coagulation and sepsis Pp. 175-182
F.R. Machado and E. Silva
[Abstract]
Bacterial Recognition and Induced Cell Activation
in Sepsis Pp. 183-191
P.S. Martins, M.K.C. Brunialti, M. da Luz Fernandes, L.S.W.
Martos, N.E. Gomes, O. Rigato and R. Salomao
[Abstract]
Pathogenesis-Oriented Targets for Adjunctive Therapy
Pp. 193-200
O. Rigato, E. Silva and R. Salomao
[Abstract]
Mechanisms of Action of Hypertonic Saline Resuscitation
in Severe Sepsis and Septic Shock Pp. 201-206
L.F. Poli-de-Figueiredo, R.J. Cruz Jr., P. Sannomiya and
M. Rocha-e-Silva
[Abstract]
Epidemiology of Severe Sepsis Around the World
Pp. 207-212
D.C. Angus, C.A.P. Pereira and E. Silva
[Abstract]
The Lung in Sepsis: Guilty or Innocent? Pp.
213-216
E.L.V. Costa, I.A.L. Schettino and G.P.P. Schettino
[Abstract]
Surviving Sepsis Campaign: A Project to Change Sepsis
Trajectory Pp. 217-222
E. Silva, N. Akamine, R. Salomao, S.R. Townsend, R.P. Dellinger
and M. Levy
[Abstract]
Abstracts
[Back to top]
Editorial
Sepsis: From the Bench to the Bedside
The term sepsis derives from the Greek sêpsis,
which means putrefaction. The pathogenesis and clinical manifestations
of sepsis result from a complex interaction between the host
and the infecting microorganism. Evolving at different stages
of a continuum process it places the physician before a major
challenge, a medical emergency associated with high morbidity
and mortality [1-3].
Despite its importance and the progress of our understanding
of the sepsis pathogenesis, how to define and recognize sepsis
at the bedside, and how to use similar concepts in evaluating
new therapeutic strategies are still matters of debate. Bone
et al. have proposed a diagnostic system based on
progressive stages of the sepsis disease: bacteremia (presence
of positive blood cultures); sepsis (clinical evidence suggestive
of infection plus signs of a systemic response to infection);
sepsis syndrome (clinical diagnosis of sepsis plus the evidence
of an altered organ perfusion); and septic shock [4]. In a
consensus conference sponsored of the American College of
Chest Physicians and the Society of Critical Care it was recognized
that a wide range of insults could lead to a similar clinical
picture through common pathways. They proposed the term Systemic
Inflammatory Response Syndrome (SIRS) to encompass the clinical
manifestations following pancreatitis, burns, trauma and others,
with the term sepsis being restricted to the SIRS triggered
by infections [5, 6]. Recently, several intensive care societies
revisited the definitions for sepsis and related conditions.
They concluded that “the concepts of sepsis, severe
sepsis, and septic shock remain useful to clinicians and researchers”,
and expanded the list of signs and symptoms of sepsis. They
proposed, however, a developing staging system for sepsis,
similar to others used in clinical medicine, stratifying patients
by their baseline risk and potential to respond to therapy.
The classification is called PIRO, for predisposition
conditions, the nature and extend of the insult,
the nature and magnitude of the host response and
the degree of the organ dysfunction [7].
The pathogenesis of sepsis is a fascinating area of investigation,
and our understanding of its underlying mechanisms has improved
markedly in recent years [1, 8, 9], specially in bacterial
recognition and cellular signaling [10,11]. Perhaps in no
other disease, even infectious, are the protective and deleterious
responses so closely related. Indeed, they are part of the
same process, and as such may not fit into a good or bad dychotomic
response. Certainly, this is an important reason for the failure
of many pathogenesis-oriented target adjunctive therapies
[12]. It is interesting to note that the host-response to
bacteria and their products is modulated by the ongoing septic
process. In this context, it has been proposed that an anti-inflammatory
response should proceed the initial inflammatory response
[13], or that both would occur at a different balance in different
tissues [14] during sepsis.
The experimental work has been fundamental for the development
and testing of sepsis concepts. From the chemical studies
of LPS, its biological activities, the importance of the host-response
in mediating its activity, which ultimately led to discovery
of the LPS-gene, much of what we know from about sepsis derives
from seminal experimental work. However, a great task has
been to translate the basic knowledge into the clinical setting
that is, by nature, much more complex.
Our therapeutic approach to sepsis has improved in the recent
years. While the appropriate use of antibiotics remains the
main stone of the therapy, supportive therapy has gained renewed
importance and new strategies based on pathophysiology are
in use nowadays. Surely, as our understanding of pathogenesis
improves, new targets will be identified. It is important
to emphasize the existence of a number of time-dependent interventions
that reduce mortality from sepsis. A surviving sepsis campaign
was launched few years ago aiming to increase awareness and
improve outcome in severe sepsis, by using education and monitoring
of the standards of care as strategy [15].
In this issue of the Endocrine, Metabolic & Immune Disorders
– Drug Targets we aimed to provide a comprehensive overview
of sepsis, from the bench to the bedside. I thank the invited
authors that brought excellent reviews, mostly based on their
own data, offering a wide scope of experimental and clinical
work, covering the pathogenesis of sepsis and its clinical
therapy.
REFERENCES
[1] Salomao, R.; Rigato, O.; Pignatari, A. C.; Freudenberg,
M. and Galanos, C. (1999) Infection, 27,
1-11.
[2] Angus, D.C.; Linde-Zwirble, W.T.; Lidicker, J.; Clermont,
G.; Carcillo, J. and Pinsky, M.R. (2001) Crit. Care Med.,
29(7),1303-10.
[3] Martin, G.S.; Mannino, D.M.; Eaton, S. and Moss, M. (2003)
N. Engl. J. Med., 348(16),1546-54.
[4] Bone, R.C. (1991) Ann. Intern. Med., 114(4),
332-3.
[5] Bone, R.C.; Sibbald, W.J. and Sprung, C.L. (1992) Chest,
101(6),1481-3.
[6] Bone, R.C.; Sprung, C.L. and Sibbald, W.J. (1992) Crit.
Care Med., 20(6), 724-6.
[7] Levy, M.M.; Fink, M.P.; Marshall, J.C.; Abraham, E.; Angus,
D.; Cook, D., Cohen, J.; Opal, S.M.; Vincent, J.L. and Ramsay,
G. (2003) Intens. Care Med., 29(4),
530-8.
[8] Hotchkiss, R.S. and Karl I.E. (2003) N. Engl. J. Med.,
348(2), 138-50
[9] Cohen, J. (2002) Nature, 420,
885-91.
[10] Aderem. A. and Ulevitch, R.J. (2000) Nature,
406(6797), 782-7.
[11] Medzhitov, R. and Janeway Jr., C.A. (1998) Semin.
Immunol., 10(5), 351-3.
[12] Rigato, O.; Silva. E.; Kallas, E.G.; Brunialti, M.K.;
Martins, P.S. and Salomao, R. (2001) Curr. Drug Targets
Immune Endocr. Metabol. Disord., 1(1),
13-30.
[13] Oberholzer, A.; Oberholzer, C. and Moldawer, L.L. (2001)
Shock, 16(2), 83-96.
[14] Cobb, J.P. and O'Keefe, G.E. (2004) Lancet,
363(9426), 2076-83.
[15] Dellinger, R.P.; Carlet, J.M.; Masur, H.; Gerlach, H.;
Calandra, T.; Cohen, J.; Gea-Banacloche, J.; Keh, D.; Marshall,
J.C.; Parker, M.M.; Ramsay, G.; Zimmerman, J.L.; Vincent,
J.L. and Levy, M.M. (2004) Crit. Care Med. 32(3),
858-73.
R. Salomao, MD, PhD
Immunology Laboratory,
Division of Infectious Diseases,
Escola Paulista de Medicina,
Universidade Federal de Sao Paulo – UNIFESP
Rua Pedro de Toledo 781, 15o andar
Brasil
[Back to top]
Gender And Susceptibility To Sepsis Following Trauma
M.A. Choudhry, K.I. Bland and I.H. Chaudry
An analysis of current literature on sexual dimorphism in
response to trauma-hemorrhage revealed conflicting reports
on the role of gender in outcomes of trauma patients. In contrast,
results obtained from experimental studies clearly support
the suggestion that gender plays a significant role in post
injury pathogenesis. As discussed in this review, experimental
studies suggest that the suppression of immune and cardiac
function is severe in males and ovariectomized females; however,
both immune and cardiac functions are maintained in proestrus
females. Furthermore, findings from a number of studies have
shown that the depletion of male sex hormones by castration
or by blocking the interaction between male sex steroids and
their receptors in males prevented the suppression of both
immune and cardiac functions following trauma-hemorrhage.
Moreover, administration of estrogen in males and ovariectomized
females also prevented the suppression of immune and cardiac
functions following trauma-hemorrhage. Thus, these experimental
findings collectively suggest that female sex hormones (i.e.,
estrogen) produce salutary effects following trauma-hemorrhage
whereas male sex steroids (i.e. 5α
-dihydrotestosterone, 5α
-DHT) are suppressive to immune and cardiac functions
under those conditions. Such dramatic differences in the outcome
of trauma-hemorrhage in proestrus females and males clearly
suggest that the prevailing sex hormonal levels at the time
of injury play a critical role in shaping the host response
to trauma-hemorrhage. While a definitive cause for the conflicting
data obtained in the clinical setting remains to be established,
the discrepancy could be due to the differences in the hormonal
levels at the time of injury. Since there is no information
on hormonal status in the clinical studies, it is difficult
to ascertain the role of sex hormones in post trauma pathogenesis.
Therefore, in order to establish the role of gender in the
outcome of trauma patients, more planned studies are needed
in which the levels of sex hormones should be measured at
the time of hospital admission. Furthermore, more studies,
both in the clinical and experimental settings, should be
performed to determine the mechanism by which the sex hormones
improve immune and organ functions following trauma-hemorrhage.
The findings obtained from these studies will help in designing
innovative therapeutic approaches for the treatment of trauma
patients.
[Back to top]
Neuro-Immune-Endocrine Mechanisms During Septic Shock:
Role For Nitric Oxide in Vasopressin and Oxytocin Release
E.C. Carnio, V. Moreto, A. Giusti-Paiva and J. Antunes-Rodrigues
Fos-like immunoreactivity in the organum vasculosum of
the lamina terminalis (OVLT), subfornical organ (SFO), dorsal
median preoptical nucleus (MnPO); and paraventricular nucleus
(PVN) 1 hour after i.v. injection of saline (top) or LPS (1,5
mg/kg; bottom).
Septic shock is a major cause of death following trauma and
a persistent problem in surgical patients. It is a challenge
to the critical care medicine specialist and carries an unacceptably
high mortality rate, despite adequate antibiotic and vasopressor
therapy.
The prevalent hypothesis regarding its mechanism is that the
syndrome is caused by an excessive defensive and inflammatory
response.
During the acute phase some signalling mechanisms are activated,
particularly hormone release, which function to restore the
host homeostasis that has been disturbed by the infection.
Since the neuroendocrine and immune systems are functionally
related, so the exposure to antigens induces a synchronized
response, which allows the organism to successfully endure
immunology changes. An important characteristic of this communication
includes the appearance of proteins released into the circulation
by activated immune cells. These proteins, called cytokines
can enter the circulation and reach neuroendocrine organs,
where they act either themselves or through the release of
intermediates such as prostaglandin, catecholamines and nitric
oxide. The synthesis of nitric oxide may be induced in brain
as a consequence of infection and may alter the function of
the hypothalamic-pituitary axis. In this review we discuss
the physiologic roles of the nitric oxide in central nervous
system controlling the regulation of vasopressin and oxytocin
during the pathophysiology of sepsis.
[Back to top]
Bacterial Translocation, Microcirculation Injury and
Sepsis
I.H.J. Koh, A.M.A. Liberatore, J.L. Menchaca-Diaz, M.
Ruiz-Silva, L. Vilela-Oliveira, A. Y. Watanabe, R. Salomao,
U. Fagundes-Neto and R.M. Silva
Aspects of mesenteric microcirculation captured by intra-vital
technique in control animal and following bacterial translocation.
Sepsis is the result from a complex bacterial-host interaction,
which is an often-fatal response when host protective molecular
mechanisms designed to fight invading bacteria surpass the
beneficial intensity to the point of causing injury to the
host. Increasing evidences have implicated the bacterial translocation
(BT) as the main source for the induction of sepsis, although
the beneficial effect of BT process has been related to the
development of the intestinal immune response by physiological
interaction between bacteria and host. In this article, we
examined evolving concepts concerning to BT and discussed
about its potential role in the promotion of microcirculation
injury, moreover, its possible participation in the sepsis
induction.
According to our data obtained from in-vivo BT animal-model,
both bacterial overgrowth and bacterial pathogenic determinants
seem to be major predisposing factors for the induction of
BT. Besides, translocation of luminal bacteria through the
lymphatic via elicits the activation of the GALT
inflammatory response contributing to microcirculation injuries,
and the haematological via of BT was responsible
to the systemic bacterial spread. On other hand, the combination
of BT process to the pre-existing host systemic infection
played a crucial role in the worsening of the clinical outcome.
In our understanding, studies concerning to intestinal immune
response and the pathophysiology of bacterial-host interaction,
under normal and disease conditions, seems to be the key elements
to the development of therapeutic approaches towards sepsis.
[Back to top]
Neutrophil Function in Severe Sepsis
J.C. Alves-Filho, B.M. Tavares-Murta, C. Barja-Fidalgo,
C.F. Benjamim, A. Basile-Filho, S.M. Arraes and F.Q. Cunha
iNOS and rolling and adhesion of neutrophils in sub-lethal
and lethal CLP.
Sepsis and septic shock continue to be a major cause
of morbidity and mortality in critically ill patients. During
the onset of sepsis, several inflammatory mediators, including
cytokines, chemokines and nitric oxide are released systemically
and mediate most of the pathophysiological events present
in sepsis and septic shock, such as cardiovascular dysfunction
and target-organ lesions. Polymorphonuclear leukocytes are
critical effector cells during the inflammatory process and
their migration to the infection focus is extremely important
for the local control of bacterial growth and consequently
for the prevention of bacterial dissemination. In experimental
models and in human sepsis a profound failure of neutrophil
migration to the infection focus is observed. It seems that
the failure of neutrophil migration is dependent on toll-like
receptor 4 (TLR4) and mediated by cytokines and chemokines,
which induce the production of nitric oxide that inhibits
neutrophil adhesion to venular endothelium and also the neutrophil
chemotactic ability.
[Back to top]
Redox Mechanisms of Vascular Cell Dysfunction in Sepsis
L.C.P. Azevedo, M. Janiszewski, F.G. Soriano and F.R.M
Laurindo
Sepsis remains one of the leading causes of death in intensive
care units, despite recent acquired knowledge on pathophysiology
and treatment. Several mediators of inflammation and cellular
damage have been implicated in the complex host-pathogen interaction
underlying organ damage and multisystem organ failure , which
are hallmarks of sepsis and common causes of death. Among
such mediators, reactive oxygen/nitrogen species have been
increasingly studied in the context of direct cytotoxicity
as well as altered cell signaling. While the generation of
reactive oxygen species by inflammatory cells in sepsis is
well known, recent studies have shown that vascular cells
are able to release reactive oxygen intermediates that may
be associated with endothelial dysfunction of sepsis. These
compounds can activate transcription factors such as NF-κB
that sustain inflammatory process or enzymatic systems like
poly(ADP-ribose) polymerase-1, which are involved in apoptosis
and cytotoxicity of sepsis. Our laboratory recently showed
that platelet-derived exosomes from septic patients carry
components of a superoxide-producing NADPH oxidase and can,
at least in vitro, induce apoptosis of endothelial
and vascular smooth muscle cells by a ROS-dependent pathway.
Taken together, these data show that reactive oxygen species
are involved in cell signaling and organ injury in sepsis.
Efforts must be made to identify the precise contribution
of these factors in septic process, in order to clarify the
mechanisms associated with the disease. This will certainly
lead to discovery of therapeutic strategies that can help
us to mitigate vascular dysfunction of sepsis.
[Back to top]
Nitric Oxide and Cardiovascular Dysfunction in Sepsis
J. Assreuy
There is a wealth of data implicating NO as a key player
in all cardiac, vascular, renal and pulmonary derangements
of sepsis and septic shock. Clinical assays trying to improve
sepsis by inhibiting NO formation by NO synthases have met
with failure, probably due to the lack of selectivity of inhibitors
towards NOS isoforms. Notwithstanding the search for selective
inhibitors, a better understanding of the NO molecular effector
mechanisms may provide new opportunities for therapy development.
Sepsis and septic shock are the major causes of morbidity
and mortality in critically ill patients. During the onset
of sepsis, a massive inflammatory reaction involving chemical
mediators such as cytokines and chemokines and inflammatory
cells such as the polymorphonuclear neutrophil and macrophage
takes place. In addition to this systemic inflammatory process,
sepsis and septic shocks cause a profound decrease in the
peripheral vasomotor tone leading to a great decrease in the
peripheral resistance. This event is central to derangement
of hemodynamic and perfusional parameters. Nitric oxide (NO)
is produced by several cell types and has been implicated
in a wide range of physiological and pathological processes,
with both detrimental and beneficial effects. There is a wealth
of data implicating NO as a key player in all cardiac, vascular,
renal and pulmonary derangements of sepsis and septic shock.
Clinical assays trying to improve sepsis by inhibiting NO
formation by NO synthases have met with failure, probably
due to the lack of selectivity of inhibitors towards NOS isoforms.
Notwithstanding the search for selective inhibitors, a better
understanding of the NO molecular effector mechanisms may
provide new opportunities for therapy development. Some of
these NO effector mechanisms are discussed, including guanylate
cyclase, nitrosothiols, potassium channels, reactive oxygen
species and gene expression in the context of sepsis. Thus,
more research on the relationship between NO and sepsis is
clearly needed and warranted and may provide new therapeutic
targets to treat sepsis and septic shock.
[Back to top]
Coagulation and sepsis
F.R. Machado and E. Silva
The inflammatory storm is ultimately responsible for
coagulation derangements. It is characterized by exacerbated
coagulation, impaired anticoagulation and decreased fibrin
removal. These derangements are implicated in the generation
of microcirculation thrombosis, with deposition of microclots
and obstruction of circulation, impairing blood flow and contributing
to tissue hypoperfusion and consequently, organ dysfunction.
There is a tight and interdependent link between inflammation
and coagulation, which is responsible for the maintenance
of this state. The ensuing vicious cycle can ultimately lead
to death.
Sepsis is a complex disease and coagulation derangements are
part of this context. The inflammatory storm is ultimately
responsible for coagulation derangements. It is characterized
by exacerbated coagulation, impaired anticoagulation and decreased
fibrin removal. These derangements are implicated in the generation
of microcirculation thrombosis, with deposition of microclots
and obstruction of circulation, impairing blood flow and contributing
to tissue hypoperfusion and consequently, organ dysfunction.
This review will address the main issues regarding coagulation
disorders in the context of sepsis.
[Back to top]
Bacterial Recognition and Induced Cell Activation
in Sepsis
P.S. Martins, M.K.C. Brunialti, M. da Luz Fernandes, L.S.W.
Martos, N.E. Gomes, O. Rigato and R. Salomao
TNF-α
production by monocytes in whole blood from septicpatients.
The pathogenesis of sepsis involves complex interaction
between the host and the infecting microorganism. Recognition
and processing of microorganism antigens are essential functions
of the cells of innate immune systems, and will ultimately,
through the antigen presentation to the cells of adaptive
immunity and the synthesis and secretions of mediators, such
as cytokines, drive a coordinated immune response. Neutrophils
and monocytes will therefore function as sensing and effectors
cells. Fundamental in this process is the ability to discriminate
self from non-self molecules. Of major interest in sepsis
is that the protective and damaging host responses are part
of the same process, that is, the inflammatory response that
controls the infection process also underscores many of the
pathophysiological events of sepsis. Moreover, this is a dynamic
process according to the continuum of sepsis and its complications;
up and down regulation of cellular activities may be differently
regulated in different tissues, different cells and even in
different functions of the same cell. This review will focus
on microorganism recognition and signalization in sepsis,
with emphasis on the neutrophils and monocytes adaptation
during the ongoing disease.
[Back to top]
Pathogenesis-Oriented Targets for Adjunctive Therapy
O. Rigato, E. Silva and R. Salomao
Several strategies have been applied as adjunctive therapy
including neutralizing LPS/lipid A, blocking its binding to
macrophages and inhibiting the release or action of cytokines,
such as TNF-α
and IL-1 and cytokine-induced mediators thereof, such as nitric
oxide and tissue factor. The better understanding of the coagulation
dysfunction along with its influence on outcomes has prompt
investigators to conduct clinical trials to interfere with
the coagulation cascade in sepsis.
The outcome of patients with sepsis arises from multiple factors
affecting both the host and the invading microorganisms. Even
within the setting of adequate antimicrobial use, patients
still die of sepsis. Thus, strategies focusing on further
therapy targets are an important area of interest for basic
and clinical research. Although such adjunctive sepsis therapy
has failed to achieve consistent better survival rates so
far, the progress in understanding of the pathophysiology
of sepsis seen in recent years is so profound, that the possibility
that a new and effective treatment may arise should be warmly
considered. Indeed, it may be considered that efficacious
interventions, such as early and vigorous fluid replacement,
strict blood glucose control, low-dose corticosteroid reposition,
protective mechanical ventilation and activated-protein C
are pathogenic-oriented targets of therapy. In this paper
we aim to review some aspects of the pathogenesis of sepsis,
focusing on possible targets for adjunctive therapy. Published
clinical trials and experimental data supporting such trials
are commented on.
[Back to top]
Mechanisms of Action of Hypertonic Saline Resuscitation
in Severe Sepsis and Septic Shock
L.F. Poli-de-Figueiredo, R.J. Cruz Jr., P. Sannomiya and
M. Rocha-e-Silva
Cardiac index in experimental septic shock induced by
lethal intravenous dose of live E. coli in dogs. B0
(baseline), IF15 (after 6 x 10 9cfu/Kg
over 15 minutes); S45-S105 (shock: 45 to
105 minutes after B0); R135-R165 (resuscitation
period).
Small volumes of 7.5% NaCl (2400mOsm/L) have been extensive
evaluated in animal models of hemorrhagic shock and in clinical
trials of post-traumatic hypotension and as volume support
for complex cardiovascular procedures. Hypertonic solutions
promote immediate blood volume expansion, restore cardiac
output and regional blood flows, improve microcirculation
and modulate immune responses, thereby decreasing inflammatory
responses triggered by shock and trauma. A large number of
very interesting in vivo and in vitro experiments
highlighted that hypertonic saline resuscitation may decrease
susceptibility to post-traumatic sepsis, modulate trauma and
sepsis-induced immune dysfunction, inflammatory response and
apoptosis. All those long-term benefits associated with hypertonic
resuscitation may be of potential relevance for the management
of severe sepsis and septic shock In this review, we describe
the mechanisms of action of hypertonic saline based on experimental
studies as well as its efficacy and safety based on its clinical
use. We believe those studies support the need for additional
experimental and clinical studies before the widespread use
of hypertonic solutions for the treatment of severe sepsis
and septic shock.
[Back to top]
Epidemiology of Severe Sepsis Around the World
D.C. Angus, C.A.P. Pereira and E. Silva
Sepsis is an on-going challenge for clinicians and health-care
administrators around the world. Recent studies have reported
a high population-based incidence of sepsis in different countries
and sepsis prevalence in intensive care units (ICU) remains
extremely common. Moreover, the associated mortality rate,
ranging from 30% to 60%, is very high compared to other common
diseases, such as myocardial infarction or breast cancer.
Severe sepsis is an ongoing challenge for clinicians and health-care
administrators mainly because is associated with a high incidence,
mortality rate and costs. In recent years, several epidemiological
studies about the incidence of sepsis have come out in different
and prestigious journals. However, it is not advisable to
draw direct conclusions from those studies considering methodological
flaws or even different approaches. Hence, we have to be familiar
with those obstacles and know how to overcome them. This review
paper highlights the methods which have been used in these
studies and depicts the results of occurrence rate or incidence
of sepsis in countries and in intensive care units.
[Back to top]
The Lung in Sepsis: Guilty or Innocent?
E.L.V. Costa, I.A.L. Schettino and G.P.P. Schettino
The lung is the most frequently identified organ to fail
in sepsis and is also the most frequent primary site of infection.
The current understanding of the pathogenesis of ARDS suggests
that the degree of inflammatory response and its sustained
leukocyte activation may determine the clinical evolution
of ARDS.
The mortality rate of severe sepsis is still high (20 to 65%)
despite the advances in critical care. The most important
determinant of the prognosis in this condition is the occurrence
of multiple organ dysfunction syndrome (MODS). The lung is
the most frequently identified organ to fail in sepsis and
is also the most frequent primary site of infection. The development
of acute respiratory distress syndrome (ARDS) is common in
those cases. The current understanding of the pathogenesis
of ARDS suggests that the degree of inflammatory response
and its sustained leukocyte activation may determine the clinical
evolution of ARDS. The way that mechanical ventilation is
delivered is responsible for the start and/or the perpetuation
of a pro-inflammatory cascade activation that, due to the
loss of the alveolar compartmentalization in ARDS, can reach
the bloodstream and induce MODS. On the other hand, during
sepsis, the alveolar compartmentalization is lost, allowing
the passage of cytokines, released to the bloodstream by any
other organ, to the pulmonary endothelium. These cytokines,
especially IL-1, TNF-α
and IL-8, have important roles in the lung dysfunction.
Experimental and clinical studies have been demonstrated that
ventilation strategies using low tidal volumes and limitation
of airway pressures can block cytokines and reduce mortality
of patients with respiratory failure. The studies are still
insufficient to determine the role of pharmacological therapies
in those patients.
[Back to top]
Surviving Sepsis Campaign: A Project to Change Sepsis
Trajectory
E. Silva, N. Akamine, R. Salomao, S.R. Townsend, R.P. Dellinger
and M. Levy
Survey for hospital ability to implement SSC recommendations.
Sepsis is an acute and severe disease associated with early
and late high mortality, high and growing prevalence, and
impressive costs. In October 2002, during the European Society
of Intensive Care Medicine annual congress, the Surviving
Sepsis Campaign was launched through a “Barcelona Declaration”
– a document calling critical care providers, governments,
health agencies and lay people to join the fight against sepsis.
The aim of the campaign was to reduce the sepsis mortality
rate by 25% within 5 years (actually, this deadline has been
ended from 2007 to 2009). In 2003, a group of international
critical care and infectious disease experts in the diagnosis
and management of infection and sepsis met to develop guidelines
that the bedside clinician could use to improve the outcome
of severe sepsis and septic shock. A comprehensive document
created from the committee’s deliberations was published
in prestigious journals. Thus, the SSC is a global, multi-organizational
initiative to fight sepsis and undoubtedly, this campaign
is a historic step for critical care medicine. This paper
highlights the recommendations and the strategies proposed
by SSC to implement them in intensive care units.
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