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Selective Imaging of APIs in Powdered Blends with Common Excipients Utilizing TPE-UVF and UV-SONICC

机译:在粉末共混物与常用的赋形剂利用TpE-UVF和UV-sONICC的apI选择性成像

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摘要

Second order nonlinear optical imaging of chiral crystals (SONICC) and two-photon excited fluorescence measurements [both autofluorescence and two-photon excited UV-fluorescence (TPE-UVF)] were assessed for the selective detection of APIs relative to common pharmaceutical excipients. Active pharmaceutical ingredients (APIs) compose only a small percentage of most tabulated formulations, yet the API distribution within the tablet can affect drug release and tablet stability. Complementary measurements using either UV-SONICC (266 nm detection) or TPE-UVF were shown to generate signals >50-fold more intense for a model API (griseofulvin) than those produced by common pharmaceutical excipients. The combined product of the measurements produced signals >104-fold greater than the excipients studied. UV-SONICC or TPE-UVF produced greater selectivity than analogous measurements with visible-light detection, attributed to the presence of aromatic moieties within the API exhibiting strong one and two photon absorption at ~266 nm. Complementary SONICC and fluorescence measurements allowed for the sensitive detection of the three-dimensional distribution of tadalafil within a Cialis® tablet to a depth of >140 µm.
机译:对手性晶体(SONICC)和双光子激发荧光测量的二阶非线性光学成像进行评估相对于普通药物赋形剂的选择性检测API的选择性检测。活性药物成分(API)仅组成小百分比的大多数列表制剂,但片剂内的API分布可以影响药物释放和片剂稳定性。示出了使用UV-SONICC(266nm检测)或TPE-UVF的互补测量以产生比普通药物赋形剂产生的模型API(Griseofulvin)更强烈的信号> 50倍。测量的组合产物产生的信号> 10 4 - 大于所研究的赋形剂的折叠。 UV-SonicC或TPE-UVF产生的选择性比具有可见光检测的类似测量的选择性,归因于API内的芳族部分存在于〜266nm处的强烈的一个和两个光子吸收。互补的Sonicc和荧光测量允许敏感检测Cialis ®平板电脑内塔达拉非的三维分布,深度>140μm。

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