Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
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Target Concepts:
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Query: EC:3.1.1.34 (
lipoprotein lipase
)
7,025
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We have previously shown that transgenic expression of catalytically inactive
lipoprotein lipase
(
LPL
) in muscle (Mck-N-
LPL
) enhances triglyceride hydrolysis as well as whole particle lipoprotein and selective cholesterol ester uptake. In the current study, we have examined whether these functions can be performed by inactive
LPL
alone or require the presence of active
LPL
expressed in the same tissue. To study inactive
LPL
in the presence of active
LPL
in the same tissue, the Mck-N-
LPL
transgene was bred onto the heterozygous
LPL
-deficient (
LPL1
) background. At 18 h of age, Mck-N-
LPL
reduced triglycerides by 35% and markedly increased muscle lipid droplets. In adult mice, it reduced triglycerides by 40% and increased lipoprotein particle uptake into muscle by 60% and cholesterol ester uptake by 110%. To study inactive
LPL
alone, the Mck-N-
LPL
transgene was bred onto the
LPL
-deficient (LPL0) background. These mice die at approximately 24 h of age. At 18 h of age, in the absence of active
LPL
, inactive
LPL
expression did not diminish triglycerides nor did it result in the accumulation of muscle lipid droplets. To study inactive
LPL
in the absence of active
LPL
in the same tissue in adult animals, the Mck-N-
LPL
transgene was bred onto mice that only expressed active
LPL
in the heart (LPL0/He-
LPL
). In this case, Mck-N-
LPL
did not reduce triglycerides or increase the uptake of lipoprotein particles but did increase muscle uptake of chylomicron and very low density lipoprotein cholesterol ester by 40%. Thus, in the presence of active
LPL
in the same tissue, inactive
LPL
augments triglyceride hydrolysis and increases whole particle triglyceride-rich lipoprotein and selective cholesterol ester uptake. In the absence of active
LPL
in the same tissue, inactive
LPL
only mediates selective cholesterol ester uptake.
...
PMID:Inactive lipoprotein lipase (LPL) alone increases selective cholesterol ester uptake in vivo, whereas in the presence of active LPL it also increases triglyceride hydrolysis and whole particle lipoprotein uptake. 1175 82
Both hyperglycemia and hyperlipidemia have been postulated to increase atherosclerosis in patients with diabetes mellitus. To study the effects of diabetes on lipoprotein profiles and atherosclerosis in a rodent model, we crossed mice that express human apolipoprotein B (HuB), mice that have a heterozygous deletion of
lipoprotein lipase
(
LPL1
), and transgenic mice expressing human cholesteryl ester transfer protein (CETP). Lipoprotein profiles due to each genetic modification were assessed while mice were consuming a Western type diet. Fast-protein liquid chromatography analysis of plasma samples showed that HuB/
LPL1
mice had increased VLDL triglyceride, and HuB/
LPL1
/CETP mice had decreased HDL and increased VLDL and IDL/LDL. All strains of mice were made diabetic using streptozotocin (STZ); diabetes did not alter lipid profiles or atherosclerosis in HuB or HuB/
LPL1
/CETP mice. In contrast, STZ-treated HuB/
LPL1
mice were more diabetic, severely hyperlipidemic due to increased cholesterol and triglyceride in VLDL and IDL/LDL, and had more atherosclerosis.
...
PMID:Lipoprotein lipase deficiency and CETP in streptozotocin-treated apoB-expressing mice. 1203 61
To investigate the nutritional regulation of lipid metabolism in fish, molecular characterization of lipases was conducted in red sea bream Pagrus major, and the effects of fasting and refeeding on their gene expression was examined. Together with data from a previous study, a total of four lipase genes were identified and characterized as
lipoprotein lipase
(
LPL
), hepatic lipase (HL) and pancreatic lipase (PL). These four lipase genes, termed
LPL1
, LPL2, HL and PL, share a high degree of similarity.
LPL1
and LPL2 genes were expressed in various tissues including adipose tissue, gill, heart and hepatopancreas. HL gene was exclusively expressed in hepatopancreas. PL gene expression was detected in hepatopancreas and adipose tissue. Red sea bream
LPL1
and LPL2 gene expression levels in hepatopancreas were increased during 48 h of fasting and decreased after refeeding, whereas no significant change in the expression levels of
LPL1
and LPL2 was observed in adipose tissue, indicating that
LPL1
and LPL2 gene expression is regulated in a tissue-specific manner in response to the nutritional state of fish. HL and PL gene expression was not affected by fasting and refeeding. The results of this study suggested that
LPL
, HL and PL gene expression is under different regulatory mechanisms in red sea bream with respect to the tissue-specificities and their nutritional regulation.
...
PMID:Molecular characterization of lipoprotein lipase, hepatic lipase and pancreatic lipase genes: effects of fasting and refeeding on their gene expression in red sea bream Pagrus major. 1690 58
