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Selasa, 20 Desember 2011
septic shock
SEPTIC SHOCK
SEPTIC SHOCK PREDISPOSING FACTORS
Disseminated malignancy - Hyperalimentation
Biliary tract surgery - Genital tract surgery
Extended hospitalization - Advanced age
Debilitating illness - Immunodeficiency disorder
Ventilator > 48 h - Disseminated malignancy
Hyperalimentation - Biliary tract surgery
Genital tract surgery
SEPTIC SHOCK MORTALITY SEPTIC SHOCK MICROBIOLOGY
Underlying Illness Mortality %
Rapidly fatal 80
Ultimately fatal 40
Non-fatal <10
SEPTIC SHOCK PATHOPHYSIOLOGY
Endotoxinàstimulation of humoral and cellular immune systemsàactivation of complement sequence and coagulation cascade
Activation of coagulation cascadeà activation of fibrinolytic systemà DIC
Complement activationàchemotaxis of PMNs, degranulation of mast cells, and release of histamine and inflammatory mediatorsàincreased capillary permeability
INFLAMMATIONà release of catecholamines and prostaglandinsà generalized vasoconstriction
VASOCONSTRICTIONà decreased perfusion of vital organsà tissue hypoxiaà metabolic acidosis
METABOLIC ACIDOSISà capillary poolingà decreased circulating blood volumeà decreased venous returnà decreased cardiac output
DECREASED CARDIAC OUTPUTà decreased coronary and cerebral blood flowà intractable hypotension, coma, multiorgan failureà DEATH
SEPTIC SHOCK CLINICAL MANIFESTATIONS
Altered mental status - Thermal instability
Cardiac dysfunction - Respiratory compromise
Bleeding - Jaundice
Ileus - Skin changes
SEPTIC SHOCK DIFFERENTIAL DIAGNOSIS
Cardiogenic shock - Hypovolemic shock
Venous or AF embolism - Cardiac tamponade
Hemorrhagic pancreatitis - Diabetic ketoacidosis
Aortic dissection
SEPTIC SHOCK DIAGNOSTIC TESTS
Laboratory Test Result
WBC Decreased, then increased
HCT Variable
PLT Decreased with DIC
Fibrinogen Decreased with DIC
Fibrin degradation products Increased with DIC
PT, PTT, TT Prolonged with DIC
pH Decreased
Lactic acid Increased (poor prognostic factor)
pO2 Decreased
pCO2 Increased
HCO3 Decreased
K+ Increased
SEPTIC SHOCK MICROBIOLOGY STUDIES
Urine culture - Blood culture
Culture of peritoneal fluid - Culture of abscess
Sputum culture - Chest x-ray
Abdominal films - IVP
CT - MRI
Ultrasound - ECG
Right heart catheterization
SEPTIC SHOCKMANAGEMENT
Monitoring --> CO , PCWP, BP, ABGs, Urine output
Restore circulating blood volume Packed red blood cells; Maintain hemoglobin of 7 to 9 g/l ; Crystalloid ; Ringer’s lactate ; Normal saline
“7 – 3 rule” for fluid replacement
Infuse 150-200 ml/10 minutes
If PCWP increases > 7mm Hg, discontinue infusion temporarily
If PCWP increases < 3 mm Hg, infuse a second increment
SEPTIC SHOCK GOALS OF FLUID RESUSCITATION
Central venous pressure of 8 to 12 mm Hg
Mean arterial pressure > 65 mm Hg
Urine output > 0.5 ml/kg/h
Central venous or mixed venous oxygen saturation > 70%
SEPTIC SHOCK VASOPRESSORS
Dopamine
Starting dose 1-3 mcg/kg/min
Norepinephrine
5 to 15 mcg/min
Vasopressin
0.01 to 0.03 U/min
In patients with septic shock, there is no difference in mortality in patients treated with dopamine vs norepinephrine vs vasopressin
Dopamine is associated with more arrhythmic events than norepinephrine
Events serious enough to require discontinuation of medication
SEPTIC SHOCK INOTROPIC THERAPY
Dobutamine - first choice inotrope for patients with low CO in the presence of adequate LV filling pressure
Dose
0.5 to 1 mcg/kg/min
Maximum – 40 mcg/kg/min
SEPTIC SHOCK TREATMENT WITH HYDROCORTISONE
Dose – 200-300 mg/day for 7 days in 3 or 4 divided doses or by continuous infusion
Reverses shock more rapidly
Variable effect on mortality
Increases frequency of superinfection
SEPTIC SHOCK SURGICAL INTERVENTION
Drainage of abscess
Debridement of infected wound
Removal of infected organ
SEPTIC SHOCK ANTIBIOTIC THERAPY
Antibiotics should be started within one hour of diagnosis of sepsis/hypotensionà improved survival
Initial empiric regimen should target most likely pathogens, e
Reassess regimen after 48-72 hours
Total duration of treatment- 7 to 10 days
SEPTIC SHOCK SPECIALIZED ANTIBIOTICS
Anti-staphylococcal agents
Linezolid
Quinupristin plus dalfopristin
Vancomycin
Anti-fungal agents
SEPTIC SHOCK
POSSIBLE MODIFICATIONS IN ANTIBIOTIC ADMINISTRATION
Prolong the intravenous infusion to 3 to 4 hours
For ventilator-related infections, administer nebulized antibiotics
SEPTIC SHOCK
MINIMIZING INFLAMMATION
Recombinant human activated protein C (rhAPC)
Inflammatory response is integrally linked to procoagulant activity and endothelial activation
rhAPC is an endogenous anticoagulant with anti-inflammatory properties
Recombinant human activated protein C
Inhibits thrombin
Inhibits neutrophil recruitment
Inhibits apoptosis
Improves survival in patients with multi-organ dysfunction
Dose - 24 micrograms/kg/min x 96 hours
SEPTIC SHOCK RESPIRATORY SUPPORT
Administer oxygen
Monitor ABGs
Initiate mechanical ventilation early
Avoid barotrauma
Use PEEP as indicated
EFFECT OF ARDS ON MORTALITY IN SEPTIC SHOCK
Condition Mortality %
Septic shock without ARDS 50
Septic shock with ARDS 90
MANAGEMENT OF SEPTIC SHOCK OTHER SUPPORTIVE MEASURES
Maintain normal temperature
Correct coagulation abnormalities
Maintain glucose < 150 mg/dl
Administer WBC transfusion
DVT prophylaxis
SEPTIC SHOCK PREVENTIVE MEASURES
Stabilize pre-existing illnesses prior to surgery
Avoid unnecessary preoperative hospitalization
Diagnose and treat operative site infections immediately
Be ever vigilant
SEPTIC SHOCK CONCLUSIONS
Predisposing factors
Microbiology
Fluid resuscitation
Surgical intervention
Antibiotic therapy
Importance of early intervention
REFERENCES
Dellinger RP, et al. Surviving sepsis campaign guidelines for management of severe sepsis and septic shock. Crit Care Med 2004; 32: 858-73.
Russell JA. Management of sepsis. N Engl J Med 2007: 355:1699-713.
Sprung CL, et al. Hydrocortisone therapy for patients with septic shock. N Engl J Med 2008; 358:111-24.
Parrillo JE. Septic shock – vasopressin, norepinephrine, and urgency. N Engl J Med 2008; 358: 954-55
DeBacker D, et al. Comparison of dopamine and norepinephrine in the treatment of shock. N Engl J Med 2010; 362:779-89.
Peleg AY, Hooper DC. Hospital-acquired infections due to gram-negative bacteria. N Engl J Med 2010; 362:1804-13.
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