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Current
Pharmaceutical Design
ISSN: 1381-6128
Current Pharmaceutical Design
Volume 14, Number 19, 2008
Contents
Sepsis: Evolving Concepts and Therapeutic Strategies
Executive Editors: T.J. Standiford and M. Moss
Editorial: Pp. 1832
The Epidemiology of Sepsis Pp. 1833-1839
K.E. Hodgin and M. Moss
[Abstract]
Sepsis: Links between Pathogen Sensing and Organ
Damage Pp. 1840-1852
E. Crouser, M. Exline, D. Knoell and M.D. Wewers
[Abstract]
Apoptosis in Sepsis: Mechanisms, Clinical Impact
and Potential Therapeutic Targets Pp. 1853-1859
A. Ayala, M. Perl, F. Venet, J. Lomas-Neira, R. Swan and
C-S. Chung
[Abstract]
The Coagulation Cascade in Sepsis Pp.
1860-1869
L. Wang, J.A. Bastarache and L.B. Ware
[Abstract]
Immunosuppression in Sepsis Pp. 1870-1881
K. Lyn-Kew and T.J. Standiford
[Abstract]
Adrenal Insufficiency in Sepsis Pp.
1882-1886
D. Annane
[Abstract]
Glucose Metabolism and Insulin Resistance in
Sepsis Pp. 1887-1899
S.J. Van Cromphaut, I. Vanhorebeek and G. Van den Berghe
[Abstract]
Genetic Insights into Sepsis: What have we Learned
and How will it Help? Pp. 1900-1911
M.M. Wurfel
[Abstract]
New Developments in Antimicrobial Use
in Sepsis Pp. 1912-1920
D.R. Kaul, C.D. Collins and R.C. Hyzy
[Abstract]
Abstracts
[Back to top]
Editorial: Sepsis: Evolving Concepts
and Therapeutic Strategies
Sepsis is a common and devastating syndrome that causes over
200,000 deaths per year in the United States, and the incidence
of sepsis is increasing at an alarming rate. The manifestations
of sepsis result from the complex interaction between microbe
and host. Microbial invasion triggers a robust but tightly
regulated host inflammatory response. However, when this response
becomes amplified and dysregulated, a cascade of maladaptive
events ensue, culminating in tissue hypoperfusion, multiple
organ failure, and even death. Past clinical trials targeting
either selected microbial products or host inflammatory responses
have produced disappointing results. However, exciting new
research has provided novel insights into disease pathogenesis
in sepsis, opening the door to the development of innovative
therapeutic strategies in the treatment of patients with this
syndrome.
In this Special Issue, we will review clinical manifestations
and pathogenic mechanisms in sepsis, with a particular emphasis
on novel mediators and pathways involved. Drs. Hodgin and
Moss [1] will discuss the changing epidemiology of sepsis
and how these changes have impacted both causes of sepsis
and clinical outcomes. Dr. Crouser and colleagues [2] provide
an introduction to novel inflammatory targets in sepsis, including
host derived molecules that activate toll receptor signaling
cascades. These authors highlight the importance of other
fundamental processes in disease pathogenesis, including mechanistic
links between sepsis-induced inflammation, mitochondrial dysfunction,
and multiple organ failure. Dr. Ayala and associates [3] discuss
the critical role of apoptosis in sepsis, including effects
on organ function and immunity. Activation of the coagulation
cascade is a hallmark of sepsis, and compelling evidence indicates
that microvascular thrombosis contributes to pathophysiologic
events in sepsis. Wang and colleagues [4] outline mechanisms
of abnormal coagulation in sepsis and review the findings
of clinical trials aimed at disrupting coagulation cascades.
The septic response is associated with a profound state of
immune suppression, which is temporally associated with reprogramming
of leukocyte immune responses. Putative mediators of leukocyte
reprogramming in sepsis include inhibitors of pathogen recognition
receptors, anti-inflammatory cytokines, ligands of nuclear
hormone receptors, pro-apoptotic molecules, and epigenetic
changes of key regulatory genes. Drs. Lyn-Kew and Standiford
[5] discuss molecular mechanisms of impaired innate and acquired
immunity in sepsis, and explore novel approaches to reverse
these deleterious events in both animal models and patients
with sepsis. Sepsis-induced alterations in corticosteroid
responses are common and of substantial clinical importance.
Dr. Annane [6] reviews causes of abnormal corticosteroid responses
in sepsis, and discusses the merits of glucocorticoid therapy
in this patient population. Patients with sepsis also have
marked impairment in glucose metabolism, which is partially
attributable to a relative state of insulin resistance. Implications
of hyperglycemia include persistent inflammation, cellular
toxicity, and impairment in leukocyte antimicrobial function.
Dr. Van Cromphaut and colleagues [7] define mechanisms involved,
and discuss the impact of insulin therapy on cellular responses
and clinical outcomes in critically ill patients, including
patients with sepsis. The influence of genetic variations
on gene expression patterns in sepsis is an intense area of
research. Dr. Wurfel [8] provides an informative summary of
common sequence variations in genes involved in innate immunity,
inflammation, and coagulation, and how these genetic factors
influence disease susceptibility and expression in sepsis.
In the final article of this Issue, Drs. Kaul, Collins, and
Hyzy [9] address the important topic of antimicrobial therapy
in sepsis, including an overview of evolving patterns of antimicrobial
resistance and the status of new classes of antimicrobial
agents in development. Collectively, this Special Issue of
Current Pharmaceutical Design provides a timely and
comprehensive update of new directions in sepsis research
that may ultimately fuel a real paradigm shift in our approach
to the treatment of this deadly disease.
References
[1] Hodgin KE, Moss M. The Epidemiology of Sepsis. Curr Pharm
Des 2008; 14(19): 1833-1839.
[2] Crouser E, Exline M, Knoell D, Wewers MD. Sepsis: Links
Between Pathogen Sensing and Organ Damage. Curr Pharm Des
2008; 14(19): 1840-1852.
[3] Ayala A, Perl M, Venet F, Lomas-Neira J, Swan R, Chung
C-S. Apoptosis in Sepsis: Mechanisms, Clinical Impact and
Potential Therapeutic Targets. Curr Pharm Des 2008; 14(19):
1853-1859.
[4] Wang L, Bastarache JA, Ware LB.The Coagulation Cascade
in Sepsis. Curr Pharm Des 2008; 14(19): 1860-1869.
[5] Lyn-Kew K.L, Standiford TJ. Immunosuppression in Sepsis.
Curr Pharm Des 2008; 14(19): 1870-1881.
[6] Annane D. Adrenal Insufficiency in Sepsis. Curr Pharm
Des 2008; 14(19): 1882-1886.
[7] Van Cromphaut SJ, Vanhorebeek I, Van den Berghe G. Glucose
Metabolism and Insulin Resistance in Sepsis. Curr Pharm Des
2008; 14(19): 1887-1899.
[8] Wurfel MM. Genetic Insights into Sepsis: What Have We
Learned and How Will It Help? Curr Pharm Des 2008; 14(19):
1900-1911.
[9] Kaul DR, Collins C, Hyzy RC. New Development in Antimicrobial
Use in Sepsis. Curr Pharm Des 2008; 14(19): 1912-1920.
Theodore J. Standiford
Professor of Medicine
Division of Pulmonary and Critical Care Medicine
University of Michigan Medical Center
109 Zina Pitcher Place
4065 BSRB
Ann Arbor, MI. 48109
USA
Marc Moss
Professor of Medicine
Chief, Division of Critical Care Medicine
University of Colorado Health Sciences Center
4200 E 9th Ave C272 Rm 5525
Denver, Colorado 80262-0001
USA
[Back to top]
The Epidemiology of Sepsis
K.E. Hodgin and M. Moss
Sepsis is a common and devastating syndrome that represents
a significant healthcare burden worldwide. The average annual
cost to care for patients with sepsis has been estimated to
being $16.7 billion. Uniform definitions have been developed
for the spectrum of sepsis syndrome, including the systemic
inflammatory response syndrome (SIRS), sepsis, severe sepsis
and septic shock. SIRS describes the clinical manifestations
derived from an acute yet nonspecific illness, whereas an
infectious etiology is required for the diagnosis of sepsis.
As sepsis progresses, organ system dysfunction becomes apparent
(severe sepsis) with the final development of fluid refractory
cardiovascular dysfunction (septic shock). Pulmonary, gastrointestinal,
genitourinary, and primary bloodstream infections account
for the majority of infectious sources in septic patients.
Since 1987, gram positive bacteria have become the most common
organisms responsible for the development of sepsis. Several
risk factors for the development of sepsis have been identified
including male sex, race, age, comorbid medical conditions,
alcohol abuse, and a lower socioeconomic status. Seasonal
variations also exist, with sepsis being more common in the
winter months. Fortunately, the case fatality rates for both
sepsis and severe sepsis have diminished over the last two
decades. However, patients who survive their episode of sepsis
continue to have increased morbidity and mortality up to five
years after their initial illness.
[Back to top]
Sepsis: Links between Pathogen Sensing and Organ Damage
E. Crouser, M. Exline, D. Knoell and M.D. Wewers
The host’s inflammatory response to sepsis can
be divided into two phases, the initial detection and response
to the pathogen initiated by the innate immune response, and
the persistent inflammatory state characterized by multiple
organ dysfunction syndrome (MODS). New therapies aimed at
pathogen recognition receptors (PRRs) particularly the TLRs
and the NOD-like receptors offer hope to suppress the initial
inflammatory response in early sepsis and to bolster this
response in late sepsis. The persistence of MODS after the
initial inflammatory surge can also be a determining factor
to host survival. MODS is due to the cellular damage and death
induced by sepsis. The mechanism of this cell death depends
in part upon mitochondrial dysfunction. Damaged mitochondria
have increased membrane permeability prompting their autophagic
removal if few mitochondria are involved but apoptotic cell
death may occur if the mito-chondrial losses are more extensive.
In addition. severe loss of mitochondria results in low cell
energy stores, necrotic cell death, and increased inflammation
driven by the release of cell components such as HMGB1. Therapies,
which aim at improving cellular energy reserves such as the
promotion of mitochondrial biogenesis by insulin, may have
a role in future sepsis therapies. Finally, both the inflammatory
responses and the susceptibility to organ failure may be modulated
by nutritional status and micronutrients, such as zinc, Therapies
aimed at micronutrient repletion may further augment approaches
targeting PRR function and mitochondrial viability.
[Back to top]
Apoptosis in Sepsis: Mechanisms, Clinical Impact and Potential
Therapeutic Targets
A. Ayala, M. Perl, F. Venet, J. Lomas-Neira, R. Swan and
C-S. Chung
The inability of present therapies to mitigate the devastating
effects of sepsis and multiple organ failure in the critically
ill patient indicates that more knowledge of the pathophysiology
of sepsis is needed if we are to develop better, more effective
interventions. This review will examine the concept that a
portion of the immune and organ dysfunctions encountered in
the septic rodent/ patient is a reflection of not only the
types of cells stimulating/ mediating the apoptotic response,
but also the varying capacity of the target cell in a given
tissue/ organ to perceive these death receptor stimuli as
either an apoptotic, inflammatory and/or necrotic signal.
We hope the discussion of such studies provides not only new
insight into the pathobiology of sepsis, but also suggests
possible therapeutic targets for the management of this devastating
condition.
[Back to top]
The Coagulation Cascade in Sepsis
L. Wang, J.A. Bastarache and L.B. Ware
Intravascular and extravascular fibrin formation are
characteristic findings in patients with sepsis, suggesting
that the activation of coagulation and the inhibiton of fibrinolysis
are important in the pathogenesis of sepsis. Activation of
coagulation during sepsis is primarily driven by the tissue
factor (TF) pathway, while inhibition of fibrinolysis is primarily
due to increases in plasminogen activator inhibitor -1(PAI-1).
Downregulation of the anticoagulant Protein C pathway also
plays an important role in the modulation of coagulation and
inflammation in sepsis. Recent advances in the understanding
of pathogenetic mechanisms of coagulation and fibrinolysis
in sepsis may have therapeutic implications. Recombinant human
activated protein C (rhAPC) is currently the only pharmacologic
therapy that has been shown to reduce mortality in adults
with severe sepsis, highlighting the importance of coagulation
and fibrinolysis as a therapeutic target in sepsis. This review
summarizes recent basic and clinical findings with regard
to the role of the coagulation cascade in sepsis and explores
potential therapeutic targets in the coagulation and fibrinolytic
pathways in the management of sepsis.
[Back to top]
Immunosuppression in Sepsis
K. Lyn-Kew and T.J. Standiford
The often fatal sepsis syndrome is characterized by the
systemic release of inflammatory mediators, which is regulated
and counterbalanced by the coordinated expression of anti-inflammatory
molecules. The magnitude of sepsis-induced tissue injury and
sub-sequent risk of infectious complications is dictated by
the balance between the expression of pro- and anti-inflammatory
mediators. As our understanding of the pathophysiology of
sepsis continues to evolve, we have gained a greater appreciation
for the profound effects that sepsis and similar states of
overwhelming stress have on host innate and adaptive immunity.
Impaired leukocyte function in sepsis has important clinical
consequences, as high mortality rates have been observed in
patients who display evidence of sepsis-induced immune dysregulation.
Functional defects in leukocytes isolated from patients with
sepsis include diminished expression of important cell surface
molecules, dysregulated cytokine production, alterations in
antigen-presenting ability, and accelerated apoptosis. In
this article, we review the current literature supporting
the notion that dysregulation of host immunity occurs during
sepsis syndrome, and describe novel therapeutic interventions
directed at augmenting host immunity during sepsis.
[Back to top]
Adrenal Insufficiency in Sepsis
D. Annane
The role of the hypothalamic-pituitary adrenal axis in
the host response to infection is crucial. The initial inflammatory
response to sepsis activates the endogenous release of cortisol,
which in turn modulates the synthesis and release of both
pro- and anti-inflammatory mediators to restrict inflammation
in infected tissues. However, a number of factors, including
vascular or ischemic damage, inflammation and apoptosis within
the hypothalamic-pituitary adrenal axis, as well as use of
drugs that alter cortisol metabolism, may cause adrenal insufficiency.
One major problem ICU physicians are faced with is the diagnosis
of sepsis-induced adrenal insufficiency at the bedside. A
multidisciplinary international task force has recently recommended
that sepsis induced adrenal insufficiency is best recognized
by basal cortisol of less than 10μg/dl
or change in cortisol of less than 9μg/dl
after administration of corticotrophin. The diagnostic value
of measuring salivary free cortisol in this setting remains
to be investigated. While sepsis adrenal insufficiency is
un-doubtedly associated with a poor prognosis, the indication
and practical modalities of corticosteroids therapy remained
controversial. Based on the two largest randomised, placebo-controlled
trials, many investigators, myself included, contend that
septic shock patients with hypotension poorly responsive to
fluid replacement and vasopressors should receive a seven
day treatment with the combination of hydrocortisone at a
dose of 200 mg per day and fludrocortisone at the dose of
50 μg
per day.
[Back to top]
Glucose Metabolism and Insulin Resistance in Sepsis
S.J. Van Cromphaut, I. Vanhorebeek and G. Van den Berghe
Hyperglycemia is a common feature of the critically ill
in general and of patients with sepsis in particular. Even
a moderate degree of hyperglycemia appears detrimental for
the outcome of critically ill patients, since maintenance
of normoglycemia (blood glucose levels =110 mg/dL) with intensive
insulin therapy has shown to improve survival and reduce morbidity
in prolonged critically ill patients in both surgical and
medical intensive care units, as revealed by two large randomized
controlled studies. Subsequently, questions have been raised
regarding the efficacy and safety of this intervention, above
all in the major subpopulation of intensive care patients
presenting with sepsis, who are particularly susceptible to
hypoglycemia as well. Adequately powered and executed randomized
controlled trials addressing explicitly the impact of hyperglycemia,
tight blood glucose control and the inherently increased risk
of hypoglycemia on mortality and morbidity in patients with
sepsis are presently lacking. However, the available literature
suggests a causal link between hyperglycemia and adverse outcome
in sepsis and a benefit of intensive insulin therapy in sepsis
equal to the benefit found in critical illness without sepsis
and critical illness in general. Though a high frequency of
hypoglycemia may be noted during insulin treatment of patients
with sepsis, the present observations define hypoglycemia
as a marker of disease severity rather than a harmful treatment
side-effect. Prevention of cellular glucose toxicity by strict
glycemic control appears to play a predominant role, but other
metabolic and non-metabolic, anti-inflammatory effects of
insulin seem to contribute to the clinical benefits realized.
[Back to top]
Genetic Insights into Sepsis: What have we Learned and How
will it Help?
M.M. Wurfel
Sepsis and septic shock, are complex disorders that are a
major cause of mortality in the intensive care unit. In spite
of major advances in our understanding of the pathophysiology
of sepsis, accurate prediction of susceptibility to sepsis,
multi-organ dysfunction, and death, even in the setting of
a seemingly similar burden of infection, continues to challenge
critical care clinicians. Evidence from family-based studies
and recent gene-association studies suggest that a significant
portion of the apparent variability in susceptibility is due
to genetic factors. Common sequence variations in genes coding
for innate immune effectors, inflammatory mediators, and modulators
of coagulation have received particular attention. This review
will summarize and integrate the results of studies testing
for associations between sequence variations in genes from
these functional classes and susceptibility to sepsis and
related clinical outcomes. The important insights on sepsis
pathophysiology provided by these studies will be discussed
along with the relevance of these findings to the design of
future diagnostic approaches and therapeutic trials.
[Back to top]
New Developments in Antimicrobial Use in Sepsis
D.R. Kaul, C.D. Collins and R.C. Hyzy
Over the past decade, trends in antimicrobial resistance,
epidemiology, and drug development have occurred that affect
both the empiric and definite selection of antimicrobials
in the septic patient. The rapid spread of highly pathogenic
community-associated methicillin resistant Staph aureus
(MRSA) requires clinicians to consider the inclusion of empiric
coverage for MRSA even in community-acquired sepsis. Moreover,
vancomycin appears to be losing its effectiveness, and while
a number of new agents with broad gram positive activity have
been licensed, none have emerged as clearly superior. An alarming
increase in the number of hospital-acquired infections due
to multi-drug resistant gram negative bacteria has also occurred,
and few new gram negative drugs are in development. Clinicians,
faced with Pseudomonas aeruginosa or Acinetobacter baumanii
isolates resistant to all commonly used drugs, must resort
to toxic older drugs such as colistin or therapy combining
drugs not effective as monotherapy. Based on a desire to limit
overall antimicrobial use, a re-evaluation of older data in
both the neutropenic and non-neutropenic host has called into
question the common practice of using combination therapy
for some gram negative infections. An emerging consensus advocates
emphasizing local unit specific antimicrobial sensitivity
data in selecting empiric therapy and determining if combination
therapy is required. New antifungal drugs and a better understanding
of the risk factors for infection with Candida spp.
has altered the approach to empiric and definitive treatment
of Candida infections in the septic patient.
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