Palmer W K, Emeson E E, Johnston T P
Exercise Research Division, School of Kinesiology, University of Illinois at Chicago 60608, USA.
Atherosclerosis. 1998 Jan;136(1):115-23. doi: 10.1016/s0021-9150(97)00193-7.
Poloxamer 407 (P-407) induces hyperlipidemia in the rat. It was the purpose of this investigation to determine if chronic P-407 administration would produce atherogenic arterial lesions in the C57BL/6 mouse, a strain reported to be susceptible to hyperlipidemia-induced atherosclerotic plaque formation. One injection (i.p.) of P-407 (0.5g/kg) produced hypercholesterolemia in the mouse that peaked at 24 h and returned to control levels by 96 h following treatment. Four groups of mice were maintained: (1) saline injected (C); (2) P-407-injected (0.5g/kg every 3rd day) (P); (3) P-407 injected plus cholic acid in the diet (PC); and (4) mice fed a high cholesterol (CHOL) diet containing cholic acid (HF). Mice from each group were sacrificed following 90, 145, 200, or 300 days of treatment. Plasma lipid concentrations, hepatic CHOL concentrations (145 and 300 day), and aortic atherogenic lesion areas were measured. Plasma CHOL and triglyceride remained at control levels throughout the 300 days in the C group. CHOL of the HF animals plateaued at approximately 225 mg/dl. P-407 produced CHOL concentrations of 600 mg/dl in P mice and 1000-1500 mg/dl in PC animals. There was no lesion formation in C mice. However, by 90 days lesions were present in the three other groups. Size of the lesions progressed through day 300 with the largest lesions (184.33 + 27.99 mu2 x 10(-3)) being present in the PC mice. HF and P animals had lesions of 70.50 + 11.35 and 43.33 + 7.88 mu2 x 10(-3), respectively. This study provides an animal model where atherogenesis has been produced with hyperlipidemia induced using a chemical agent.
泊洛沙姆407(P - 407)可在大鼠中诱发高脂血症。本研究的目的是确定长期给予P - 407是否会在C57BL / 6小鼠中产生动脉粥样硬化性病变,据报道该品系小鼠易患高脂血症诱导的动脉粥样硬化斑块形成。单次腹腔注射P - 407(0.5g / kg)可使小鼠产生高胆固醇血症,在治疗后24小时达到峰值,并在96小时后恢复到对照水平。将小鼠分为四组:(1)注射生理盐水(C组);(2)注射P - 407(每3天0.5g / kg)(P组);(3)注射P - 407并在饮食中添加胆酸(PC组);(4)喂食含胆酸的高胆固醇(CHOL)饮食的小鼠(HF组)。在治疗90、145、200或300天后处死每组小鼠。测量血浆脂质浓度、肝脏胆固醇浓度(第145天和300天)以及主动脉粥样硬化病变面积。在C组中,血浆胆固醇和甘油三酯在整个300天内均保持在对照水平。HF组动物的胆固醇水平稳定在约225mg / dl。P组小鼠中P - 407产生的胆固醇浓度为600mg / dl,PC组动物中为1000 - 1500mg / dl。C组小鼠未形成病变。然而,到90天时,其他三组出现了病变。病变大小在第300天持续进展,PC组小鼠中出现最大病变(184.33 + 27.99μm²×10⁻³)。HF组和P组动物的病变面积分别为70.50 + 11.35和43.33 + 7.88μm²×10⁻³。本研究提供了一种动物模型,其中通过化学试剂诱导高脂血症产生了动脉粥样硬化。
