Increased arginase levels contribute to impaired perfusion after cardiopulmonary resuscitation

Christian Jung; Felix Quitter; Michael Lichtenauer; Michael Fritzenwanger; Alexander Pfeil; Alexey Shemyakin; Marcus Franz; Hans R Figulla; Ruediger Pfeifer; John Pernow

doi:10.1111/eci.12330

Increased arginase levels contribute to impaired perfusion after cardiopulmonary resuscitation

Eur J Clin Invest. 2014 Oct;44(10):965-71. doi: 10.1111/eci.12330.

Authors

Christian Jung¹, Felix Quitter, Michael Lichtenauer, Michael Fritzenwanger, Alexander Pfeil, Alexey Shemyakin, Marcus Franz, Hans R Figulla, Ruediger Pfeifer, John Pernow

Affiliation

¹ Department of Medicine, Karolinska Institute, Stockholm, Sweden; Clinic of Internal Medicine I, Friedrich-Schiller-University, Jena, Germany.

PMID: 25186018
DOI: 10.1111/eci.12330

Abstract

Objectives: The postcardiac arrest syndrome occurs after global hypoxia leading to microcirculatory impairment. Nitric oxide (NO) is a key molecule regulating microvascular function. The enzyme arginase has been suggested to modulate microvascular function by regulating NO metabolism. Therefore, we investigated whether arginase increases following global hypoxia and resuscitation and tested whether arginase inhibition influences altered microcirculation in resuscitated patients.

Methods: To determine the effect of global hypoxia on circulating arginase levels, fourteen healthy subjects were exposed to hypoxia in a normobaric hypoxia chamber (FiO² = 9·9%). In addition, 31 resuscitated patients were characterized clinically, and arginase 1 was measured on days 1 and 3. In eight resuscitated patients, a microcirculatory analysis was performed using a sidestream darkfield microcirculation camera. Perfused capillary density (PCD) was recorded before and after sublingual incubation of N-omega-hydroxy-nor-l-arginine (nor-NOHA) alone or together with the NOS inhibitor NG-monomethyl-l-arginine (l-NMMA).

Results: Circulating arginase 1 levels increased in healthy volunteers following global hypoxia in the hypoxic chamber (P < 0·01). In addition, arginase 1 levels were higher on day 1 (69·1 ± 83·3 ng/mL) and on day 3 (44·2 ± 65·6 ng/mL) after resuscitation than in control subjects (P < 0·001). Incubation of the sublingual mucosa with nor-NOHA increased microcirculatory perfusion (P < 0·001). This effect was inhibited by co-incubation with K-NMMA.

Conclusions: Circulating arginase 1 levels are increased following exposure to global hypoxia and in patients who have been successfully resuscitated after cardiac arrest. Topical arginase inhibition improves microcirculatory perfusion following resuscitation. This is of potential therapeutic importance for the postcardiac arrest syndrome.

Keywords: Arginase; heart failure; intravital microscopy; microcirculation; sidestream darkfield.

Publication types

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

MeSH terms

Adult
Arginase / metabolism*
Arginine / analogs & derivatives
Arginine / pharmacology
Capillaries / physiology
Cardiopulmonary Resuscitation*
Enzyme Inhibitors / pharmacology
Female
Heart Arrest / enzymology*
Heart Arrest / therapy
Humans
Hypoxia / enzymology*
Male
Microcirculation / drug effects
Microcirculation / physiology*
Nitric Oxide / metabolism
omega-N-Methylarginine / pharmacology

Substances

Enzyme Inhibitors
N(omega)-hydroxynorarginine
omega-N-Methylarginine
Nitric Oxide
Arginine
ARG1 protein, human
Arginase