Blood ammonia concentration measurement - effects of sampling site and cirrhosis during induced hyperammonaemia

Lars Djernes; Hendrik Vilstrup; Peter Ott; Peter Lykke Eriksen

doi:10.1007/s11011-024-01442-4

Blood ammonia concentration measurement - effects of sampling site and cirrhosis during induced hyperammonaemia

Lars Djernes
, Hendrik Vilstrup
, Peter Ott
, Peter Lykke Eriksen

Research output: Contribution to journal/Conference contribution in journal/Contribution to newspaper › Journal article › Research › peer-review

1 Citation (Scopus)

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Abstract

Background: Ammonia is implicated in hepatic encephalopathy (HE) and prognostic in cirrhosis. Venous ammonia concentration, yielding similar correlation with HE grades as arterial, has become the preferred practise but comparative data are limited. Aim: To quantify effect of sampling site on ammonia concentration in healthy persons and patients with cirrhosis. Methods: Ammonia concentrations were measured by arterial and femoral venous blood sampling in ten healthy men and ten male patients with cirrhosis before and during hyperammonaemia induced by ammonia infusion. Cubital vein samples were included during the infusion. Results: At baseline, arterial-venous concentration gaps were similar (p = 0.15) in healthy persons [14 (10–19) and 8 (4–12) µmol/L] and patients with cirrhosis [53 (32–74) and 40 (23–57) µmol/L]. Ammonia infusion increased arterial-venous concentration gaps in both groups [115 (97–133) and 61 (31–90) vs. 175 (123–227) and 134 (65–203) µmol/L]. Mean ammonia concentration difference between groups during hyperammonaemia was 72 (42–103) µmol/L (p < 0.001) and independent of sampling site. Cubital and femoral vein concentrations were comparable (p = 0.26). In cirrhosis, calculated upper limit normal values (ULN) were comparable for arterial and venous blood at baseline [2.0 (1.2–2.8) and 2.1 (1.2–3.0), p = 0.74] and during hyperammonaemia [6.7 (4.7–8.7) and 6.2 (4.4– 8.1), p = 0.44]. Conclusions: We found clinically meaningful intra-individual arterial-venous concentration gaps in both healthy persons and patients with cirrhosis at any ammonia concentration. Inter-group concentration differences after induced hyperammonaemia were relatively constant across sampling sites which supports clinical use of venous sampling. ULN-normalised ammonia concentrations were valid for both arterial and venous sampling.

Original language	English
Article number	21
Journal	Metabolic Brain Disease
Volume	40
Issue	1
ISSN	0885-7490
DOIs	https://doi.org/10.1007/s11011-024-01442-4
Publication status	Published - Jan 2025

Keywords

Adult
Aged
Ammonia/blood
Hepatic Encephalopathy/blood
Humans
Hyperammonemia/blood
Liver Cirrhosis/blood
Male
Middle Aged
Sampling site
Ammonia
Cirrhosis
Arterial-venous concentration differences
Upper limit normal

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@article{54a364f1e4b444a599a4d3cdfd75005f,

title = "Blood ammonia concentration measurement - effects of sampling site and cirrhosis during induced hyperammonaemia",

abstract = "Background: Ammonia is implicated in hepatic encephalopathy (HE) and prognostic in cirrhosis. Venous ammonia concentration, yielding similar correlation with HE grades as arterial, has become the preferred practise but comparative data are limited. Aim: To quantify effect of sampling site on ammonia concentration in healthy persons and patients with cirrhosis. Methods: Ammonia concentrations were measured by arterial and femoral venous blood sampling in ten healthy men and ten male patients with cirrhosis before and during hyperammonaemia induced by ammonia infusion. Cubital vein samples were included during the infusion. Results: At baseline, arterial-venous concentration gaps were similar (p = 0.15) in healthy persons [14 (10–19) and 8 (4–12) µmol/L] and patients with cirrhosis [53 (32–74) and 40 (23–57) µmol/L]. Ammonia infusion increased arterial-venous concentration gaps in both groups [115 (97–133) and 61 (31–90) vs. 175 (123–227) and 134 (65–203) µmol/L]. Mean ammonia concentration difference between groups during hyperammonaemia was 72 (42–103) µmol/L (p < 0.001) and independent of sampling site. Cubital and femoral vein concentrations were comparable (p = 0.26). In cirrhosis, calculated upper limit normal values (ULN) were comparable for arterial and venous blood at baseline [2.0 (1.2–2.8) and 2.1 (1.2–3.0), p = 0.74] and during hyperammonaemia [6.7 (4.7–8.7) and 6.2 (4.4– 8.1), p = 0.44]. Conclusions: We found clinically meaningful intra-individual arterial-venous concentration gaps in both healthy persons and patients with cirrhosis at any ammonia concentration. Inter-group concentration differences after induced hyperammonaemia were relatively constant across sampling sites which supports clinical use of venous sampling. ULN-normalised ammonia concentrations were valid for both arterial and venous sampling.",

keywords = "Adult, Aged, Ammonia/blood, Hepatic Encephalopathy/blood, Humans, Hyperammonemia/blood, Liver Cirrhosis/blood, Male, Middle Aged, Sampling site, Ammonia, Cirrhosis, Arterial-venous concentration differences, Upper limit normal",

author = "Lars Djernes and Hendrik Vilstrup and Peter Ott and Eriksen, \{Peter Lykke\}",

note = "{\textcopyright} 2024. The Author(s).",

year = "2025",

month = jan,

doi = "10.1007/s11011-024-01442-4",

language = "English",

volume = "40",

journal = "Metabolic Brain Disease",

issn = "0885-7490",

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number = "1",

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Blood ammonia concentration measurement - effects of sampling site and cirrhosis during induced hyperammonaemia. / Djernes, Lars; Vilstrup, Hendrik; Ott, Peter et al.
In: Metabolic Brain Disease, Vol. 40, No. 1, 21, 01.2025.

Research output: Contribution to journal/Conference contribution in journal/Contribution to newspaper › Journal article › Research › peer-review

TY - JOUR

T1 - Blood ammonia concentration measurement - effects of sampling site and cirrhosis during induced hyperammonaemia

AU - Djernes, Lars

AU - Vilstrup, Hendrik

AU - Ott, Peter

AU - Eriksen, Peter Lykke

PY - 2025/1

Y1 - 2025/1

N2 - Background: Ammonia is implicated in hepatic encephalopathy (HE) and prognostic in cirrhosis. Venous ammonia concentration, yielding similar correlation with HE grades as arterial, has become the preferred practise but comparative data are limited. Aim: To quantify effect of sampling site on ammonia concentration in healthy persons and patients with cirrhosis. Methods: Ammonia concentrations were measured by arterial and femoral venous blood sampling in ten healthy men and ten male patients with cirrhosis before and during hyperammonaemia induced by ammonia infusion. Cubital vein samples were included during the infusion. Results: At baseline, arterial-venous concentration gaps were similar (p = 0.15) in healthy persons [14 (10–19) and 8 (4–12) µmol/L] and patients with cirrhosis [53 (32–74) and 40 (23–57) µmol/L]. Ammonia infusion increased arterial-venous concentration gaps in both groups [115 (97–133) and 61 (31–90) vs. 175 (123–227) and 134 (65–203) µmol/L]. Mean ammonia concentration difference between groups during hyperammonaemia was 72 (42–103) µmol/L (p < 0.001) and independent of sampling site. Cubital and femoral vein concentrations were comparable (p = 0.26). In cirrhosis, calculated upper limit normal values (ULN) were comparable for arterial and venous blood at baseline [2.0 (1.2–2.8) and 2.1 (1.2–3.0), p = 0.74] and during hyperammonaemia [6.7 (4.7–8.7) and 6.2 (4.4– 8.1), p = 0.44]. Conclusions: We found clinically meaningful intra-individual arterial-venous concentration gaps in both healthy persons and patients with cirrhosis at any ammonia concentration. Inter-group concentration differences after induced hyperammonaemia were relatively constant across sampling sites which supports clinical use of venous sampling. ULN-normalised ammonia concentrations were valid for both arterial and venous sampling.

AB - Background: Ammonia is implicated in hepatic encephalopathy (HE) and prognostic in cirrhosis. Venous ammonia concentration, yielding similar correlation with HE grades as arterial, has become the preferred practise but comparative data are limited. Aim: To quantify effect of sampling site on ammonia concentration in healthy persons and patients with cirrhosis. Methods: Ammonia concentrations were measured by arterial and femoral venous blood sampling in ten healthy men and ten male patients with cirrhosis before and during hyperammonaemia induced by ammonia infusion. Cubital vein samples were included during the infusion. Results: At baseline, arterial-venous concentration gaps were similar (p = 0.15) in healthy persons [14 (10–19) and 8 (4–12) µmol/L] and patients with cirrhosis [53 (32–74) and 40 (23–57) µmol/L]. Ammonia infusion increased arterial-venous concentration gaps in both groups [115 (97–133) and 61 (31–90) vs. 175 (123–227) and 134 (65–203) µmol/L]. Mean ammonia concentration difference between groups during hyperammonaemia was 72 (42–103) µmol/L (p < 0.001) and independent of sampling site. Cubital and femoral vein concentrations were comparable (p = 0.26). In cirrhosis, calculated upper limit normal values (ULN) were comparable for arterial and venous blood at baseline [2.0 (1.2–2.8) and 2.1 (1.2–3.0), p = 0.74] and during hyperammonaemia [6.7 (4.7–8.7) and 6.2 (4.4– 8.1), p = 0.44]. Conclusions: We found clinically meaningful intra-individual arterial-venous concentration gaps in both healthy persons and patients with cirrhosis at any ammonia concentration. Inter-group concentration differences after induced hyperammonaemia were relatively constant across sampling sites which supports clinical use of venous sampling. ULN-normalised ammonia concentrations were valid for both arterial and venous sampling.

KW - Adult

KW - Aged

KW - Ammonia/blood

KW - Hepatic Encephalopathy/blood

KW - Humans

KW - Hyperammonemia/blood

KW - Liver Cirrhosis/blood

KW - Male

KW - Middle Aged

KW - Sampling site

KW - Ammonia

KW - Cirrhosis

KW - Arterial-venous concentration differences

KW - Upper limit normal

UR - https://www.scopus.com/pages/publications/85209723785

U2 - 10.1007/s11011-024-01442-4

DO - 10.1007/s11011-024-01442-4

M3 - Journal article

C2 - 39565434

SN - 0885-7490

VL - 40

JO - Metabolic Brain Disease

JF - Metabolic Brain Disease

IS - 1

M1 - 21

ER -

Blood ammonia concentration measurement - effects of sampling site and cirrhosis during induced hyperammonaemia

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