波洛沙姆407介导大鼠腹腔注射后血浆胆固醇和甘油三酯的变化。

Z G Wout, E A Pec, J A Maggiore, R H Williams, P Palicharla, T P Johnston
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摘要

Poloxamer (Pluronic)非离子表面活性剂载体是一系列化学相关的嵌段共聚物,广泛用于肠外配方,作为传统的低分子量有机药物分子的增溶剂和润湿剂,以及蛋白质和多肽药物的稳定剂。我们报道了poloxam407 (Pluronic F-127)对大鼠血浆胆固醇和甘油三酯浓度的影响。给大鼠腹腔注射波洛沙姆407(剂量为1.5 gm/kg)可导致持续(大于96小时)高胆固醇血症和高甘油三酯血症。提高血浆甘油三酯相对于总胆固醇的比值需要更大剂量的poloxam407。在对照组(没有注射波洛沙姆)动物中,摄入商业大鼠食物对血浆胆固醇和甘油三酯水平的影响可以忽略不计,但腹腔注射波洛沙姆407 (30% w/w)的动物摄入食物导致血浆胆固醇和甘油三酯水平显著(p < 0.05)高于禁食给予波洛沙姆407的动物。研究发现,与泊洛沙莫介导的血浆甘油三酯升高相比,泊洛沙莫407给药途径(即肌肉注射与腹腔注射)是泊洛沙莫诱导的血浆胆固醇升高的更重要因素。我们的研究结果还提供了提示性证据,表明大鼠腹腔注射poloxam407溶液(30% w/w)后血浆胆固醇升高的机制可能是由于poloxamer载体刺激肝脏中3-羟基-3-甲基戊二酰辅酶a (HMG-CoA)还原酶活性。(摘要删节250字)
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Poloxamer 407-mediated changes in plasma cholesterol and triglycerides following intraperitoneal injection to rats.

Poloxamer (Pluronic) nonionic surfactant vehicles are a series of chemically-related block copolymers finding widespread use in parenteral formulations as solubilizing and wetting agents for traditional, low-molecular weight organic drug molecules, as well as stabilizing agents for proteins and polypeptide drugs. We report the effects of poloxamer 407 (Pluronic F-127) on plasma cholesterol and triglyceride concentrations in rats. Poloxamer 407 injected into rats by intraperitoneal injection (dose = 1.5 gm/kg) resulted in sustained (greater than 96 hour) hypercholesterolemia and hypertriglyceridemia. A larger dose of poloxamer 407 was required to elevate plasma triglyceride relative to total cholesterol. Ingestion of commercial rat chow had a negligible effect on plasma cholesterol and triglycerides levels in control (no poloxamer injection) animals, but consumption of food by animals that received an intraperitoneal injection of poloxamer 407 (30% w/w) resulted in significantly (p < .05) greater elevations in plasma cholesterol and triglycerides than in fasted animals administered poloxamer 407. The route of poloxamer 407 administration, namely intramuscular vs. intraperitoneal injection, was observed to be a more important factor for poloxamer-induced elevations in plasma cholesterol than poloxamer-mediated elevations in plasma triglycerides. Our results also provide suggestive evidence that the mechanism responsible for the elevation of plasma cholesterol following intraperitoneal injection of a poloxamer 407 solution (30% w/w) to rats may be due to stimulation of 3-hydroxy-3-methylglutaryl-co-enzyme A (HMG-CoA) reductase activity in the liver by the poloxamer vehicle.(ABSTRACT TRUNCATED AT 250 WORDS)

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Evaluating out-of-specification laboratory results. Simplifying and improving process validation. Depyrogenation of pharmaceutical solutions using submicron and ultrafilters. USP perspectives on particle contamination of injectable products. Moisture measurement: a new method for monitoring freeze-drying cycles.
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