Abstract
Arginine vasopressin (AVP), a hormone secreted by the posterior pituitary, plays a vital role in maintaining vasomotor tone during acute blood loss. We hypothesized that decompensated hemorrhagic shock is associated with decreased AVP stores and supplementation during resuscitation would improve both blood pressure and renal function. Using a decompensated hemorrhagic shock model, male Long-Evans rats were bled to mean arterial blood pressure (MAP) of 40mmHg and maintained until the MAP could not be sustained without fluid. Once 40% of the shed volume was returned in lactated Ringer’s (Severe Shock), animals were resuscitated over 60 minutes with 4x the shed volume in lactated Ringer’s (LR) or the same fluids with AVP (0.5 units/kg+ 0.03 units/kg/min). Animals (n = 6-9/group) were sacrificed before hemorrhage (Sham), at Severe Shock, following resuscitation (60R, 60R with AVP) or 18 hours post-resuscitation (18hr, 18hr with AVP). Blood samples were taken to measure AVP levels and renal function. Pituitaries were harvested and assayed for AVP. Kidney samples were taken to assess mitochondrial function, histology, and oxidative damage. Baseline pituitary AVP stores (30,364 ± 5311 pg/mg) decreased with severe shock and were significantly depressed post-resuscitation (13,910 ± 3016 pg/ml. p<0.05) and at 18hr (15,592 ±1169 pg/ml, p<0.05). Resuscitation with LR+AVP led to higher serum AVP levels at 60R (31±8 vs 79±12; p<0.01) with an improved MAP both at 60R (125±3 vs 77±7mmHg; p<0.01) and 18hr (82±6 vs 69±5mmHg;p<0.05). AVP supplementation preserved complex I respiratory capacity at 60R and both complex I and II function at 18hr (p<0.05). AVP was also associated with decreased reactive oxygen species at 60R (856±67 vs 622±48F RFU) and significantly decreased oxidative damage as measured by mitochondrial lipid peroxidation (0.9±0.1 vs 1.7±0.1 fold change, p<0.01) and nitrosylation (0.9±0.1 vs 1.4±0.2 fold change, p<0.05). With AVP, renal damage was mitigated at 60R and histologic architecture was conserved at 18 hours. In conclusion, pituitary and serum AVP levels decrease during severe hemorrhage and may contribute to the development of decompensated hemorrhagic shock. Supplementing exogenous AVP during resuscitation improves blood pressure, preserves renal mitochondrial function, and mitigates acute kidney injury.
Highlights
130,000 people die of unintentional injury annually in the United States.[1]
In animals lacking arginine vasopressin (AVP), even minor blood loss results in significant hypotension and low levels during prolonged hemorrhagic shock have been associated with the development of catecholamineresistant hypotension.[11,12,13,14,15]
Severely injured trauma patients demonstrate a high incidence of AVP deficiency with an increased need for vasopressor support, blood product transfusions and prolonged ICU care.[9, 16, 17]
Summary
130,000 people die of unintentional injury annually in the United States.[1] Of those who survive the initial trauma, hemorrhagic shock accounts for the majority of potentially preventable deaths.[2] intense vasoconstriction is the normal response to hemorrhagic shock, it cannot be maintained indefinitely. Arginine vasopressin (AVP) has been investigated as an adjunct during the resuscitation of severe trauma.[5,6,7,8,9,10] Secreted by the posterior pituitary in response to hypotension, AVP is essential for maintaining vasomotor tone during hemorrhagic shock. In animals lacking AVP, even minor blood loss results in significant hypotension and low levels during prolonged hemorrhagic shock have been associated with the development of catecholamineresistant hypotension.[11,12,13,14,15] Clinically, severely injured trauma patients demonstrate a high incidence of AVP deficiency with an increased need for vasopressor support, blood product transfusions and prolonged ICU care.[9, 16, 17]
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