GLDH

Glutamate déshydrogénase

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9,01

7,45 (hors 21% TVA)

uniquement par le vétérinaire

Description

La GLDH est une enzyme principalement localisée dans la matrice mitochondriale. Elle joue un rôle clé dans l’oxydation des acides aminés et la production d’urée. Dans le sang, la GLDH provient essentiellement du foie, un organe où prédominent les mitochondries riches en matrice. C’est un marqueur sérique sensible des lésions des cellules hépatiques, dans certains cas plus sensible que d’autres enzymes hépatiques telles que l’ALT, l’AST et l’ALP.

Espèce cible et races

Rat

Prélèvement

Sérum

Délai

même jour

Catégorie

Foie

Code

T0750

Analyses

GLDH

Litérature

2002

O'Brien, P J; Slaughter, Mark R; Polley, S R; Kramer, K

Advantages of glutamate dehydrogenase as a blood biomarker of acute hepatic injury in rats Article de journal

Dans: Lab Anim, vol. 36, no. 3, p. 313–321, 2002, ISSN: 0023-6772.

Résumé | Liens | BibTeX

@article{pmid12144742,

title = {Advantages of glutamate dehydrogenase as a blood biomarker of acute hepatic injury in rats},

author = {P J O'Brien and Mark R Slaughter and S R Polley and K Kramer},

doi = {10.1258/002367702320162414},

issn = {0023-6772},

year  = {2002},

date = {2002-07-01},

urldate = {2002-07-01},

journal = {Lab Anim},

volume = {36},

number = {3},

pages = {313--321},

abstract = {In a recent study in rats, alanine aminotransferase (ALT), the preferred plasma biomarker of hepatocellular injury in rats, was ineffective at detecting marked hepatic necrosis produced by acetaminophen (Human and Experimental Toxicology 19, 277-83, 2000). In contrast, glutamate dehydrogenase (GLDH) was markedly elevated. Accordingly, these enzymes were comprehensively evaluated as plasma biomarkers of hepatocellular injury in rats using several other models of hepatic injury, including partial hepatectomy and exposure to methapyrilene, dexamethasone, cyproterone, isoniazid, lead nitrate, and Wyeth-14643. Other enzymes also evaluated were aspartate aminotransferase (AST), sorbitol dehydrogenase (SDH), and the hepatobiliary marker alkaline phosphatase (ALP). Compared to plasma ALT increases, plasma GLDH increases were up to 10-fold greater, up to 3-fold more persistent, and occurred at times following hepatocellular injury when plasma ALT was not increased. Plasma GLDH activity was not inhibited by the test compounds, whereas ALT was substantially inhibited by both isoniazid and lead nitrate. While plasma GLDH activity was unaffected by induction, ALT was induced by cyproterone and dexamethasone, and ALP was induced by Wyeth-14643 and partial hepatectomy. GLDH was concluded to be a more effective biomarker of acute hepatic injury than ALT, AST, SDH or ALP in the rat, based primarily on the large increase following hepatocellular injury, prolonged persistence in the blood following injury, high sensitivity for detection of injury (including pre-necrotic injury), high tissue specificity, and lower susceptibility to inhibition or induction.},

keywords = {},

pubstate = {published},

tppubtype = {article}

}

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