Influence of drug release rate on systemic timolol absorption from polymeric ocular inserts in the pigmented rabbit.

V H Lee, S Y Li, H Sasaki, M F Saettone, P Chetoni
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引用次数: 17

Abstract

There is an expectation that ocular inserts, regardless of the nature of the polymer, will faithfully reduce systemic drug absorption. This may not necessarily be so, however, since not all polymers would release drug at the same rate and to the same extent. The objective of the present study was to determine how drug release rate from various polymeric ocular inserts may influence systemic timolol absorption in the pigmented rabbit. The inserts tested were made of polyvinyl alcohol (PVA), hydroxypropylcellulose (HPC), or partial ethyl ester of poly(vinyl methyl ether/maleic anhydride) (PVMMA), approximately 89.4% w/w in all cases. Some polyvinyl alcohol inserts contained timolol in salt form with Carbopol 940 (PVA-C940), 8.6% w/w. The time course of timolol in plasma over 6 hr was monitored using reversed phase HPLC. While all inserts reduced the peak timolol concentration in plasma (Cmax), only the PVA and HPC inserts, which released timolol rapidly in vitro, reduced the extent of systemic timolol absorption (AUC). On the other hand, both PVA-C940 and PVMMA inserts, which released timolol relatively slowly in vitro, increased the extent of systemic timolol absorption. Moreover, the time at which peak timolol concentration was achieved in the plasma was much delayed, raising the possibility of delayed timolol absorption until discharge of the presumably viscous and/or mucoadhesive solutions of PVA-C940 and PVMMA inserts into the nasal cavity. It may be concluded that not all polymeric ocular inserts reduce systemic timolol absorption. Whether an insert would do so depends on the interplay of residence time in the conjunctival sac and rate of drug release from the insert.

药物释放速度对有色家兔聚合物眼植入物对噻洛尔全身吸收的影响。
人们期望眼内植入物,无论聚合物的性质如何,都能忠实地减少全身药物吸收。然而,这可能并不一定如此,因为并非所有的聚合物都会以相同的速度和程度释放药物。本研究的目的是确定各种聚合物眼植入物的药物释放速度如何影响铁莫洛尔在色素家兔体内的全身吸收。测试的插入件由聚乙烯醇(PVA)、羟丙基纤维素(HPC)或聚乙烯基甲基醚/马来酸酐部分乙酯(PVMMA)制成,在所有情况下,w/w均约为89.4%。一些聚乙烯醇插入物含有卡波波尔940盐态噻莫洛尔(PVA-C940), 8.6% w/w。用反相高效液相色谱法监测替马洛尔在血浆中6小时的时间过程。虽然所有植入物都降低了噻洛尔的血浆峰值浓度(Cmax),但只有PVA和HPC植入物在体外快速释放噻洛尔,降低了噻洛尔的全身吸收程度(AUC)。另一方面,PVA-C940和PVMMA植入物在体外释放替洛尔相对缓慢,增加了替洛尔的全身吸收程度。此外,在血浆中达到噻洛尔浓度峰值的时间大大延迟,增加了噻洛尔吸收延迟的可能性,直到PVA-C940和PVMMA插入物的可能粘性和/或黏性溶液排出鼻腔。由此可以得出结论,并不是所有的聚合物眼植入物都能减少全身噻洛尔的吸收。插入物是否会这样做取决于在结膜囊中停留时间和药物从插入物释放速度的相互作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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