Sepsis Clinical Trial
Official title:
The Effect of rHuEPO on Microcircualtory Alteration in ICU Patients With Severre Sepsis and Septic Shock
The objective of this study is to determine if observations the investigators made in an animal model of sepsis can be translated to clinical practice. Specifically, the investigators will use the noninvasive Orthogonal Polarization Spectral (OPS) microscope and venous oxygen saturation to test the hypothesis that recombinant human erythropoietin(rHuEPO) will acutely improve the microcircualtion in septic patients in the ICU.
Sepsis is a systemic inflammatory response to a bacterial infection and is a common
complication during the course of treatment of patients with multiple trauma and major
surgery. In severe sepsis, the inflammatory response leads to multiple organ failure that can
result in death. Multiple organ dysfunction in sepsis is now considered the most common cause
of death in non-coronary critical care units. In fact, sepsis is one of the top 10 or 12
causes of death in the general population. Approximately 150,000 people die annually.1 On a
microscopic level there is impairment in the relationship between oxygen delivery (DO2) and
consumption (VO2) suggestive of defects in microcirculatory perfusion during septic
shock.2,3,4 These alterations include a decrease in the proportion of perfused vessels
smaller than 20 μm, which mostly are capillaries whereas flow in the larger perfusion vessels
is preserved. As the micro-circulation alteration persists then multiple organ failure and
death ensues,4 thus interventions able to improve the microcirculation may reduce tissue
dysoxia. De Backer et. al.3 reported that topical application of acetylcholine can restore a
normal microcirculatory flow pattern in patients with septic shock, indicating an important
role for the micro-vascular endothelium, and that these alterations can be manipulated. Other
experimental studies of several vasodilatory compounds have been shown to improve
micro-vascular perfusion5,6,7,8,9 and even be associated with improved outcomes.7,10 In a
human study, Spronk et. al.11 observed that intravenous administration of nitroglycerin
resulted in a marked improvement in capillary perfusion, but this intervention may produce
severe arterial hypotension and also increase some nitric oxide mediated cytoxic
effects.12,13 In another human study, De Baker et. al.14 demonstrated that the administration
of 5 μg/kg-min dobutamine can improve but not restore capillary perfusion in patients with
septic shock and that these changes are independent of changes in systemic hemodynamic
variables. The concomitant decrease in blood lactate level suggested the changes in the
micro-vascular perfusion were associated with improved cellular metabolism. However,
dobutamine may also produce hypotension in patients with hypovolemia.
Erythropoietin (EPO), a sialoglycoprotein hormone produced by the adult kidney, is a major
regulator of red blood cell production but more recently has been suggested to have
favourable effects on tissue injury and vascular function. It stimulates the proliferation of
committed erythroid progenitor cells and their development into mature erythrocytes.15 Thus,
the potential benefit of erythropoietin therapy in patients with anemia secondary to chronic
renal failure has long been recognized.16 Recombinant Human EPO (rh-EPO) is indicated for the
treatment of anemia associated with chronic renal failure, non-myeloid malignancies due to
the effect of concomitantly administered chemotherapy, zidovudine treated HIV infected
patients and patients under going major elective surgery to facilitate autologous blood
collection thus to reduce allogenic blood exposure.
In critically ill adults and specifically those with sepsis, EPO levels have been shown to be
relatively low with respect to the level of anemia present.17,18 As well, correlations were
found between erythropoietin concentration and biological markers of tissue hypoperfusion
i.e. lactate level or PCO2 gap.19 A common adverse effect of rh-EPO therapy in renal patients
is the development of hypertension. The acute effects of rh-EPO on arterial vasoactivity
suggest direct and indirect actions that occur prior to any effect on erythropoeisis. In
addition to its hematopoietic effect, rh-EPO also has significant cardiovascular
effects,20,21 including a direct vasopressor effect.22 In a rat splanchnic artery occlusion
shock model, treatment with rh-EPO inhibited inducible nitric oxide synthase (iNOS) activity
and prevented the overproduction of NO in vivo restoring responsiveness to
Phenylephrine.23,24 Rh-EPO has direct vasopressor effects on smooth muscle cells, which
express EPO receptors, modulating intracellular Ca++.25 An increase in the plasma levels of
the endothelium derived vasoconstrictor endothelin-1 can occur after rh-EPO
treatment.26,27,28 Indirect effects of EPO treatment may also increase the activity of the
autonomic nervous system and increase sensitivity to angiotensin II, which is a potent
vasoconstrictor.29 We recently reported that rh-EPO in a septic mouse model produces an
immediate increase in the perfused capillary density with a concomitant decrease in NADH
fluorescence, an indirect measure indicating improvement in mitochondical oxidative
phosphorylation, in skeletal muscle. Thus, rh-EPO appears to improve tissue bioenergetics in
this septic mouse model in part by maintaining DO2 via increased perfused capillary
density.30 The recently developed, noninvasive orthogonal polarization spectral (OPS) imaging
technique can be applied to investigate the human vasculature.34 Polarized light of defined
wavelength (548 nm) is emitted to illuminate the area of interest, is reflected by the
background but absorbed by hemoglobin, producing high-contrast images of the
micro-circulation. This technique is particularly convenient for studying tissues protected
by a thin epithelial layer, such as the mucosal surface35 and has been validated as an
effective method of micro-vascular imaging in animals34, 36,37 and in humans.38 The OPS
technique has been used to observe major micro-vascular blood flow alterations in patients
with severe sepsis3 including a decreased vascular density, especially of the small vessels;
a large number of non-perfused and intermittently perfused small vessels; and a marked
perfusion heterogeneity between areas.39 These alterations were more severe in non-survivors
than in survivors but were not affected by the global hemodynamic state or vasopressor
agents.39 The persistence of micro-vascular alterations in patients with poor outcomes
further emphasize the potential role of micro-circulatory disturbances in the pathophysiology
of sepsis-induced multiple organ failure. In this study, we will use the OPS imaging
technique to investigate the sublingual microcirculation in patients with septic shock after
treatment with a single dose of rh-EPO. We hypothesize that rh-EPO will improve the
sepsis-related alterations in micro-circulatory perfusion, independent of any systemic
hemodynamic effects.
;
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