Exogenous vasopressin dose-dependently modulates gastric microcirculatory oxygenation in dogs via V1A receptor

Richard Truse; Steven Grewe; Anna Herminghaus; Jan Schulz; Andreas P M Weber; Tabea Mettler-Altmann; Inge Bauer; Olaf Picker; Christian Vollmer

doi:10.1186/s13054-019-2643-y

Exogenous vasopressin dose-dependently modulates gastric microcirculatory oxygenation in dogs via V1A receptor

Crit Care. 2019 Nov 12;23(1):353. doi: 10.1186/s13054-019-2643-y.

Authors

Richard Truse¹, Steven Grewe², Anna Herminghaus², Jan Schulz², Andreas P M Weber³, Tabea Mettler-Altmann³, Inge Bauer², Olaf Picker², Christian Vollmer²

Affiliations

¹ Department of Anesthesiology, Duesseldorf University Hospital, Moorenstr 5, 40225, Duesseldorf, Germany. Richard.Truse@med.uni-duesseldorf.de.
² Department of Anesthesiology, Duesseldorf University Hospital, Moorenstr 5, 40225, Duesseldorf, Germany.
³ Institute of Plant Biochemistry, Cluster of Excellence on Plant Sciences (CEPLAS), Heinrich-Heine-University Duesseldorf, Universitätsstr. 1, 40225, Duesseldorf, Germany.

Abstract

Background: Hypercapnia improves gastric microcirculatory oxygenation (μHbO₂) and increases vasopressin plasma levels, whereas V1A receptor blockade abolishes the increase of μHbO₂. The aim of this study was to evaluate the effect of exogenous vasopressin (AVP) in increasing doses on microcirculatory perfusion and oxygenation and systemic hemodynamic variables. Furthermore, we evaluated the role of the vasopressin V1A receptor in mediating the effects.

Methods: In repetitive experiments, six anesthetized dogs received a selective vasopressin V1A receptor inhibitor ([Pmp¹, Tyr (Me)²]-Arg⁸-Vasopressin) or sodium chloride (control groups). Thereafter, a continuous infusion of AVP was started with dose escalation every 30 min (0.001 ng/kg/min-1 ng/kg/min). Microcirculatory variables of the oral and gastric mucosa were measured with reflectance spectrometry, laser Doppler flowmetry, and incident dark field imaging. Transpulmonary thermodilution was used to measure systemic hemodynamic variables. AVP plasma concentrations were measured during baseline conditions and 30 min after each dose escalation.

Results: During control conditions, gastric μHbO₂ did not change during the course of experiments. Infusion of 0.001 ng/kg/min and 0.01 ng/kg/min AVP increased gastric μHbO₂ to 87 ± 4% and 87 ± 6%, respectively, compared to baseline values (80 ± 7%), whereas application of 1 ng/kg/min AVP strongly reduced gastric μHbO₂ (59 ± 16%). V1A receptor blockade prior to AVP treatment abolished these effects on μHbO₂. AVP dose-dependently enhanced systemic vascular resistance (SVR) and decreased cardiac output (CO). After prior V1A receptor blockade, SVR was reduced and CO increased (0.1 ng/kg/min + 1 ng/kg/min AVP).

Conclusions: Exogenous AVP dose-dependently modulates gastric μHbO₂, with an increased μHbO₂ with ultra-low dose AVP. The effects of AVP on μHbO₂ are abolished by V1A receptor inhibition. These effects are independent of a modulation of systemic hemodynamic variables.

Keywords: Gastric microcirculation; V1A receptor; Vasopressin.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Disease Models, Animal
Dogs
Dose-Response Relationship, Drug*
Gastrointestinal Tract / blood supply*
Gastrointestinal Tract / physiopathology
Hypercapnia / blood
Microcirculation / drug effects*
Vasopressins / analysis*
Vasopressins / blood
Vasopressins / pharmacology*

Substances

Vasopressins