Search on website
chevron-left-black Keywords

Sepsis: Vasopressin

Vasopressin (also, anti-diuretic hormone (ADH) or arginine vasopressin (AVP)) has been shown to be a very effective vasopressor, especially in circumstances where patients are vasopressin depleted and have become reliant on catecholamines for blood pressure regulation. Concerns for the use vasopressin tend to center on how it compares to other vasopressors, especially norepinephrine, and risks of digital and mesenteric ischemia.

Vasopressin has a very short half-life. In cases of prolonged shock, vasopressin is rapidly released and then depleted, thereby suggesting that, especially in early shock states, vasopressin is a useful adjunct to norepinephrine. Furthermore, vasopressin maintains its potency in the setting of acidosis and hypoxia, while catecholamines may not. Vasopressin may be particularly beneficial in acidotic states as it may inhibit KATP channels more effectively than catecholamines. However, these effects have been observed only in animal models. These rationales have formed the basis for large randomized controlled studies in patients with shock. In general, vasopressin has been shown to be a safe and appropriate alternative to norepinephrine in septic, cardioplegic, and hemorrhagic shock states.

Septic shock:

Vasopressin can be a safe substitute for norepinephrine in the setting of septic shock. VASST was a multicenter, randomized double blinded trial in 778 patients with septic shock. Patients were randomized to either receive Vasopressin (0.01- 0.03 units/min) or norepinephrine (5-15 ug/min), plus open-label vasopressors to maintain MAPs 65-75mmHg. The primary endpoint was death within 28 days after beginning infusions. In patients with “less severe” shock, vasopressin was superior to norepinephrine (mortality 26.5% vs 35.7%, NNT=10.7). This benefit was not demonstrated in those with more severe septic shock. There were no statistically significant differences in serious adverse events including cardiac complications, life threatening arrhythmias, mesenteric ischemia, hyponatremia, digital ischemia, and CVA.

Vasoplegic shock:

The VASST results mirror those of the VANCS trial, a randomized double blinded control study of 300 cardiac surgery patients. Subjects resistant to fluid challenge were randomized to either norepinephrine (10-60 ug/min) or vasopressin (0.01-0.06 units/min) to maintain MAPS > 65mmHg. The primary endpoint was composite mortality or severe complications (stroke, mechanical ventilation > 48h, sternal wound infection, reoperation, acute renal failure) within 30 days. Mortality occurred in 32% of vasopressin group and 49% norepinephrine group (NNT=5.9). Atrial fibrillation was found in 63.8% of vasopressin group and 82.1% norepinephrine group (NNT=5.5). No statistically significant difference between groups of digital ischemia, mesenteric ischemia, hyponatremia, and myocardial infarction. However, concerns regarding the statistical methods and potential for bias of this study have been raised.

Hemorrhagic & Hypovolemic shock:

The argument for early use of vasopressin in the setting of hemorrhagic shock is to decrease the size of the vascular compartment while adding volume . Blood loss requiring massive fluid resuscitation can be complicated by intravascular extravasation. Blood products are often not able to keep pace with blood counts and coagulopathy. Vasopressin has the advantage of maintaining potency in acidic and hypoxic conditions, whereas catecholamines lose their potency. Given a concern for neuroprotection following trauma, a systematic review found that vasopressin and hypertonic-hyperoncotic solution strategy was better able to increase cerebral perfusion pressure and cerebral oxygenation compared to norepinephrine and hypertonic-hyperoncotic solution in the first 10 minutes. A vasopressin analogue (Terlipressin) had a similar effect over Lactated Ringers. Unfortunately, most studies in hemorrhagic and hypovolemic shock are based on animal models of hemorrhage. There is a need for future trials as to the effects of vasopressin in us humans.

Concerns for the use of vasopressin is usually due to its association with digital and mesenteric ischemia. These studies are often limited by lack of randomization and use of concurrent norepinephrine, among other inotropes and vasopressors. In Van Haren et al., 13 patients with septic shock were prospectively given vasopressin after fluid bolus, dobutamine, and norepinephrine to maintain MAPs > 50mmHg. These patients were not randomized. Gastric tonometry was used to determine gut perfusion which was found to be decreased in the study population, but again this study was not randomized and there was no control group . Dunser et al. retrospectively analyzed the incidence and risk factors for skin lesions in 63 critically ill patients receiving arginine vasopressin with catecholamine-resistant vasodilatory shock. Catecholamine resistance was defined failing effect of increasing norepinephrine 0.2ug/kg/min over 2 hours for maintenance of MAPs >60mmHg. Vasopressin doses were given 4-6 units/hour. 30% of patients developed skin lesions. But again, this was a retrospective study without randomization, and there was no control or matched group making generalization of the effects of vasopressin very difficult.


  1. Gkisioti S, Mentzelopoulos SD. Vasogenic shock physiology. Open access emergency medicine : OAEM 2011; 3: 1-6. PubMed Link
  2. Landry DW, Oliver JA. The ATP-sensitive K+ channel mediates hypotension in endotoxemia and hypoxic lactic acidosis in dog. J Clin Invest 1992; 89: 2071-4. PubMed Link
  3. Wakatsuki T, Nakaya Y, Inoue I. Vasopressin modulates K(+)-channel activities of cultured smooth muscle cells from porcine coronary artery. Am J Physiol 1992; 263: H491-6. PubMed Link
  4. Russell JA, Walley KR, Singer J, et al. Vasopressin versus Norepinephrine Infusion in Patients with Septic Shock. New England Journal of Medicine 2008; 358: 877-87. PubMed Link
  5. Anand T, Skinner R. Arginine vasopressin: the future of pressure-support resuscitation in hemorrhagic shock. J Surg Res 2012; 178: 321-9. PubMed Link
  6. Nistor M, Behringer W, Schmidt M, Schiffner R. A Systematic Review of Neuroprotective Strategies during Hypovolemia and Hemorrhagic Shock. Int J Mol Sci 2017; 18. PubMed Link
  7. van Haren FM, Rozendaal FW, van der Hoeven JG. The effect of vasopressin on gastric perfusion in catecholamine-dependent patients in septic shock. Chest 2003; 124: 2256-60. PubMed Link
  8. Dunser MW, Mayr AJ, Tur A, et al. Ischemic skin lesions as a complication of continuous vasopressin infusion in catecholamine-resistant vasodilatory shock: incidence and risk factors. Crit Care Med 2003; 31: 1394-8. PubMed Link

Other References

  1. Hajjar LA, Vincent JL, Barbosa Gomes Galas FR, et al. Vasopressin versus Norepinephrine in Patients with Vasoplegic Shock after Cardiac Surgery: The VANCS Randomized Controlled Trial. Anesthesiology: The Journal of the American Society of Anesthesiologists 2017; 126: 85-93. Link
  2. James A, Amour J. Vasopressin versus Norepinephrine in Patients with Vasoplegic Shock after Cardiac Surgery: A Discussion of the Level of Evidence. Anesthesiology: The Journal of the American Society of Anesthesiologists 2018; 128: 228-. Link