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舌下免疫治疗片剂治疗过敏性鼻炎的临床疗效不太可能源自过敏原释放数据。

Clinical efficacy of sublingual immunotherapy tablets for allergic rhinitis is unlikely to be derived from allergen-release data.

机构信息

Department of Internal Medicine, Humanitas University and Research Hospital ICH , Milan , Italy.

UPRES EA220, Foch Hospital, University Versailles Saint-Quentin, University Paris-Saclay , Suresnes , France.

出版信息

Expert Rev Clin Immunol. 2019 Sep;15(9):921-928. doi: 10.1080/1744666X.2019.1649597. Epub 2019 Aug 12.

Abstract

: Allergen bioavailability underpins the efficacy and safety of SLIT tablets. Three product-related factors are likely to influence this: tablet potency, formulation and sublingual holding time. : Tablet formulation determines the rate and extent of solubilized allergen release. Using validated dissolution assays, the two licensed grass pollen SLIT tablets are shown to release ≥85% of their total allergenic activity within several minutes. Sublingual holding time affects the contact duration between solubilized allergens and sublingual tissue. Maximal uptake of allergens by sublingual tissue requires ~5 minutes, with little uptake occurring within the first minute. A higher potency tablet with longer sublingual holding time would provide higher bioavailability, while faster rates of allergen release are unlikely to translate to a greater increase in bioavailability. Differences in dissolution times cannot serve as a surrogate of bioavailability, and are not related to differences in efficacy at the marketed tablet dosages. Rapid dissolution is likely not a key requirement for inducing a potent immune response. : dissolution cannot predict the clinical efficacy of SLIT tablets but could be important in immune tolerance and safety. In addition, a discontinuous administration regimen may have benefits for adherence and cost without compromising efficacy.

摘要

过敏原生物利用度是 SLIT 片剂疗效和安全性的基础。有三个与产品相关的因素可能会影响这一点:片剂效力、配方和舌下保持时间。

片剂配方决定了过敏原溶解释放的速度和程度。使用经过验证的溶解测定法,两种已批准的草花粉 SLIT 片剂在数分钟内释放出其总过敏原活性的≥85%。舌下保持时间影响溶解的过敏原与舌下组织之间的接触持续时间。过敏原被舌下组织最大吸收需要约 5 分钟,在最初的 1 分钟内几乎没有吸收。效力更高、舌下保持时间更长的片剂将提供更高的生物利用度,而过敏原释放速度的提高不太可能转化为生物利用度的更大增加。溶解时间的差异不能作为生物利用度的替代指标,并且与上市片剂剂量的疗效差异无关。快速溶解不太可能是诱导有效免疫反应的关键要求。

溶解不能预测 SLIT 片剂的临床疗效,但在免疫耐受和安全性方面可能很重要。此外,不连续给药方案可能在不影响疗效的情况下提高顺应性和降低成本方面具有优势。

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