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LNP/AAV 封装核酸的电泳表征:优势与不足

Electrophoretic characterization of LNP/AAV-encapsulated nucleic acids: Strengths and weaknesses.

作者信息

Hutanu Andrei, Ferreiro Miriam López, van Haasteren Joost, Höcker Oliver, Montealegre Cristina, Mäser Marina, Keresztfalvi Alex, Monti Jose, Schwarz Maria Anna

机构信息

Pharma Technical Development, Cell and Gene Therapy Unit, F. Hoffmann-La Roche AG, Basel, Switzerland.

Department of Chemistry, University of Basel, Basel, Switzerland.

出版信息

Electrophoresis. 2023 Oct;44(19-20):1595-1606. doi: 10.1002/elps.202300127. Epub 2023 Aug 25.

Abstract

The use of nucleic acids (NAs) has revolutionized medical approaches and ushered in a new era of combating various diseases. Accordingly, there is an increasing demand for accurate identification, localization, quantification, and characterization of NAs encapsulated in nonviral or viral vectors. The vast spectrum of molecular dimensions and intra- and intermolecular interactions presents a formidable obstacle for NA analytical development. Typically, the comprehensive analysis of encapsulated NAs, free NAs, and their spatial distribution poses a challenge that is seldom tackled in its complete complexity. The identification of appropriate physicochemical methodologies for large nonencapsulated or encapsulated NAs is particularly intricate and necessitates an evaluation of the analytical outcomes and their appropriateness in addressing critical quality attributes. In this work, we examine the analytics of non-encapsulated or encapsulated large NAs (>500 nucleotides) utilizing capillary electrophoresis (CE) and liquid chromatography (LC) methodologies such as free zone CE, gel CE, affinity CE, and ion pair high-performance liquid chromatography (HPLC). These methodologies create a complete picture of the NA's critical quality attributes, including quantity, identity, purity, and content ratio.

摘要

核酸(NAs)的应用彻底改变了医学方法,开创了抗击各种疾病的新时代。因此,对非病毒或病毒载体中封装的核酸进行准确鉴定、定位、定量和表征的需求日益增加。分子尺寸的广泛范围以及分子内和分子间的相互作用给核酸分析的发展带来了巨大障碍。通常,对封装的核酸、游离核酸及其空间分布进行全面分析是一项极具挑战性的任务,很少有人能完全应对其复杂性。确定适用于大型非封装或封装核酸的物理化学方法尤为复杂,需要评估分析结果及其在解决关键质量属性方面的适用性。在这项工作中,我们利用毛细管电泳(CE)和液相色谱(LC)方法,如自由区CE、凝胶CE、亲和CE和离子对高效液相色谱(HPLC),研究非封装或封装的大型核酸(>500个核苷酸)的分析。这些方法全面呈现了核酸的关键质量属性,包括数量、身份、纯度和含量比例。

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