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首页> 外文期刊>International Journal of Pharmaceutics >Sodium lauryl sulfate impedes drug release from zinc-crosslinked alginate beads: Switching from enteric coating release into biphasic profiles.
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Sodium lauryl sulfate impedes drug release from zinc-crosslinked alginate beads: Switching from enteric coating release into biphasic profiles.

机译:月桂基硫酸钠可阻止药物从锌交联的藻酸盐微珠中释放:从肠溶包衣释放转变为两相分布。

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摘要

The aim of this research is to investigate the effects of sodium lauryl sulfate (SLS) on ionotropically cross-linked alginate beads. Different levels of SLS were mixed with sodium alginate and chlorpheniramine maleate (as loaded model drug). The resulting viscous solutions were dropped onto aqueous solutions of zinc or calcium ions for ionotropic curing. The generated beads were assessed by their drug releasing profiles, infrared and differential scanning colorimetery (DSC) traits. SLS was found to exert profound concentration-dependent impacts on the characteristics of zinc-crosslinked alginate beads such that moderate modifications in the levels of SLS switched drug release from enteric coating-like behavior to a biphasic release modifiable to sustained-release by the addition of minute amounts of xanthan gum. Calcium cross-linking failed to reproduce the same behavior, probably due to the mainly ionic nature of calcium-carboxylate bonds compared to the coordinate character of their zinc-carboxylate counterparts. Apparently, moderate levels of SLS repel water penetration into the beads, and therefore minimize chlorpheniramine release. However, higher SLS levels seem to discourage polymeric cross-linking and therefore allow biphasic drug release.
机译:这项研究的目的是研究十二烷基硫酸钠(SLS)对离子交联的藻酸盐珠的影响。将不同水平的SLS与海藻酸钠和马来酸氯苯那敏混合(作为上样药物)。将所得的粘性溶液滴到锌或钙离子的水溶液上以进行离子固化。通过其药物释放曲线,红外和差示扫描比色法(DSC)特性评估产生的珠子。发现SLS对锌交联的藻酸盐微珠的特性产生深远的浓度依赖性影响,使得SLS含量的适度变化可通过添加SLS将药物释放从肠溶样行为转变为可转变为持续释放的双相释放。微量的黄原胶。钙交联未能重现相同的行为,这可能是由于羧酸钙键的主要离子性质与其羧酸锌对应物的配位特征相比所致。显然,适度的SLS可以抑制水渗透到微珠中,从而使氯苯那敏的释放降至最低。但是,较高的SLS含量似乎不鼓励聚合物交联,因此允许两相药物释放。

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