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全氟碳基血液替代品的药代动力学及副作用

Pharmacokinetics and side effects of perfluorocarbon-based blood substitutes.

作者信息

Flaim S F

机构信息

Alliance Pharmaceutical Corp., San Diego, CA 92121.

出版信息

Artif Cells Blood Substit Immobil Biotechnol. 1994;22(4):1043-54. doi: 10.3109/10731199409138801.

Abstract

Perfluorochemicals are fluorine-saturated carbon-based molecules which demonstrate utility in the areas of imaging and oxygen delivery. In general, these molecules are biologically inert and, therefore, do not pose toxicologic risk from metabolic degradation. Intravenous (i.v.) perfluorocarbon (PFC) emulsions are cleared from the blood through a process involving phagocytosis of emulsion particles by reticuloendothelial macrophages (RES) and ultimate elimination through the lung in expired air. RES phagocytosis of PFC emulsion particles leads to characteristic, predictable, and reversible biological effects that are a consequence of a normal host-defense mechanism. This mechanism is characterized by dose-related stimulation of macrophages and subsequent release of intracellular products (particularly metabolites of the arachidonic acid cascade and cytokines) which are responsible for most of the biological effects associated with i.v. PFC emulsions (i.e., cutaneous flushing and fever at lower doses, and macrophage hypertrophy and recruitment at higher doses). These biological effects are reversible, and do not result in any permanent tissue alteration, even with prolonged exposure at relatively high doses. The rate of PFC elimination from the RES is proportional to the vapor pressure of the PFC, inversely proportional to molecular weight and positively influenced by lipophilicity. This dose-dependent respiratory excretion occurs with no evidence of metabolic products. Repeated administration of high doses of PFC emulsion may lead to a saturation of the RES-mediated clearance capacity, resulting in a redistribution of PFC to non-RES tissues and ingestion by resident or mobile macrophages. This condition is benign with respect to the integrity of the surrounding parenchyma, as well as to the macrophages themselves. Increased pulmonary residual volume (IPRV) due to pulmonary gas (air) trapping, a reversible side effect, has been observed with i.v. doses of PFC emulsion in some animal species. The gross morphological change associated with IPRV is not accompanied by any histological alteration other than the appearance of vacuolated macrophages (characteristic of the normal clearance mechanism) and some minor, increased interalveolar cellularity. Animal lungs affected by IPRV have a normal, pale pink appearance with no visible lesions or signs of edema. The degree of IPRV is dependent on species, PFC dose, and type of PFC administered; PFCs with higher vapor pressures produce the most severe cases of IPRV in sensitive species. Species sensitivity depends upon physiological and morphological characteristics. There is no evidence indicating that IPRV occurs in humans. Although i.v. PFC emulsions may elicit minor untoward effects, these effects are reversible and, at clinically relevant doses, do not pose a toxicologic risk.

摘要

全氟化合物是氟饱和的碳基分子,在成像和氧气输送领域具有应用价值。一般来说,这些分子具有生物惰性,因此不会因代谢降解而带来毒理学风险。静脉注射全氟碳(PFC)乳剂可通过网状内皮巨噬细胞(RES)对乳剂颗粒的吞噬作用从血液中清除,并最终通过肺部以呼出气体的形式排出体外。RES对PFC乳剂颗粒的吞噬作用会导致特征性、可预测且可逆的生物学效应,这是正常宿主防御机制的结果。这种机制的特点是与剂量相关地刺激巨噬细胞,并随后释放细胞内产物(特别是花生四烯酸级联反应的代谢产物和细胞因子),这些产物是与静脉注射PFC乳剂相关的大多数生物学效应(即低剂量时的皮肤潮红和发热,高剂量时的巨噬细胞肥大和募集)的原因。这些生物学效应是可逆的,即使在相对高剂量下长时间暴露也不会导致任何永久性组织改变。PFC从RES中的清除速率与PFC的蒸气压成正比,与分子量成反比,并受到亲脂性的正向影响。这种剂量依赖性的呼吸排泄过程中没有代谢产物的证据。重复给予高剂量的PFC乳剂可能导致RES介导的清除能力饱和,从而导致PFC重新分布到非RES组织,并被驻留或游走的巨噬细胞摄取。这种情况对于周围实质组织以及巨噬细胞本身的完整性而言是良性的。在一些动物物种中,静脉注射PFC乳剂会观察到由于肺气体(空气)滞留导致的肺残余容积增加(IPRV),这是一种可逆的副作用。与IPRV相关的大体形态变化除了出现空泡化巨噬细胞(正常清除机制的特征)和一些轻微的肺泡间细胞增多外,没有任何组织学改变。受IPRV影响的动物肺外观正常,呈淡粉色,没有可见病变或水肿迹象。IPRV的程度取决于物种、PFC剂量和所施用的PFC类型;蒸气压较高的PFC在敏感物种中会导致最严重的IPRV病例。物种敏感性取决于生理和形态特征。没有证据表明IPRV会在人类中发生。虽然静脉注射PFC乳剂可能会引起轻微的不良影响,但这些影响是可逆的,并且在临床相关剂量下不会带来毒理学风险。

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