Lipoprotein lipase (LPL) and hepatic triglyceride lipase (HTGL) have an important role in
lifestyle-related diseases. To evaluate species differences, we compared LPL and HTGL
activities in different animal models of lifestyle-related diseases using the same assay
kit. Normal animals (JW rabbits, ICR mice, and SD rats), a hypercholesterolemic animal
model (WHHLMI rabbits), and obese animal models (KK-
A
y
mice
and Zucker fatty rats) fed standard chow were used in this study. Plasma was prepared
before and after an intravenous injection of heparin sodium under fasting and feeding. LPL
and HTGL activities were measured with the LPL/HTGL activity assay kit (Immuno-Biological
Laboratories) using an auto-analyzer. Only in mice, high HTGL activity was observed in
pre-heparin plasma. In normal animals, LPL and HTGL activities were high in ICR mice and
SD rats but low in JW rabbits. Compared to normal animals, LPL activity was high in Zucker
fatty rats and WHHLMI rabbits at both fasting and feeding, while LPL activity after
feeding was low in KK-
A
y
mice. HTGL activity was higher in
fasted and fed WHHLMI rabbits and fasted Zucker fatty rats, but was lower in fed
KK-
A
y
mice. Gender difference was observed in HTGL
activity in SD rats and LPL activity in WHHLMI rabbits but not in ICR mice. In conclusion,
this simple assay method was effective for measuring LPL and HTGL activities of
experimental animals, and the activities are highly regulated depending on animal species,
animal models, feeding/fasting conditions and genders.
In WHHLMI rabbits, arterial lesions develop spontaneously in various arteries even with
standard chow. Here, we examined the development of arterial lesions in various arteries
to demonstrate standard characteristics of arterial lesions in WHHLMI rabbits. For WHHLMI
rabbits at 6, 12, 20, and 30 months of age, lesion areas and areas of arterial lumen
surfaces were measured using image analysis software. Histopathological sections of
arterial lesions were stained with elastic van Gieson staining. Arterial lesions developed
around bifurcations and expanded with aging. In the aorta, atheromatous lesions were
severe in the thoracic aorta but were mild in the distal part of the abdominal aorta.
Carotid artery lesions progressed in the proximal region and at bifurcations, and the
histopathological features were similar to those of coronary lesions. Pulmonary artery
lesions contained many foam cells. Fibrous lesions were observed in the proximal and
distal areas of the renal arteries, at the bifurcation of the iliac-femoral artery and
mesenteric artery, and around the anastomosis of vertebral arteries. Lesions in the celiac
artery contained foam cells and/or lipid droplets within fibrous lesions. In a pair of
right and left arteries, the arterial lesions tended to progress more in the right artery.
Gender did not affect analysis of arterial lesions. In conclusion, the arterial lesions
expanded from bifurcations, and the morphological features of the arterial lesions varied
depending on the type of artery. These results serve as reference data for arterial
lesions in studies using WHHLMI rabbits.
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