同时双光子激发荧光和相干拉曼成像揭示小鼠肝细胞和巨噬细胞对反义寡核苷酸摄取的差异。

IF 4 2区医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Nucleic acid therapeutics Pub Date : 2022-06-01 Epub Date: 2021-11-19 DOI:10.1089/nat.2021.0059

Prabuddha Mukherjee, Edita Aksamitiene, Aneesh Alex, Jindou Shi, Kajari Bera, Chi Zhang, Darold R Spillman, Marina Marjanovic, Michael Fazio, Punit P Seth, Kendall Frazier, Steve R Hood, Stephen A Boppart

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引用次数: 7

摘要

反义寡核苷酸(ASOs)通过结合互补的信使RNA (mRNA)序列来调节细胞基因表达，是现代治疗中的一种新范式。虽然ASO药物化学的进步大大提高了细胞摄取的效率，但很难实现特定细胞类型的选择性摄取。为了更有效和选择性地摄取，ASOs通常与对跨膜受体具有高结合亲和力的分子结合。三天线n -乙酰半乳糖胺偶联硫代磷酸酯ASOs (GalNAc-PS-ASOs)是一种通过肝细胞特异性asialal糖蛋白受体(ASGR)增强ASO靶向递送到肝脏的药物。我们在J774A中评估了AlexaFluor 488 (AF488)标记的PS-ASOs和GalNAc-PS-ASOs的摄取动力学和随后的细胞内分布。1小鼠巨噬细胞和原代小鼠或大鼠肝细胞采用同步相干抗斯托克斯拉曼散射(CARS)和双光子荧光(2PF)成像。CARS模式捕获了细胞的动态脂质分布和整体形态;双光子荧光(2PF)测量了悬浮细胞改良处理后ASOs的时间和剂量依赖性定位。我们的研究结果表明，巨噬细胞对PS-ASOs的摄取率与GalNAc-PS-ASOs的摄取率无显著差异。然而，在肝细胞中，GalNAc-PS-ASOs表现为外周摄取分布，而在巨噬细胞中则表现为极性摄取分布。与PS-ASOs相比，外周分布与内化GalNAc-PS-ASOs的数量显著增加相关。这项工作证明了多模态成像在阐明肝细胞中不同ASO的摄取机制、积累和命运方面的相关性，可以进一步用于复杂的体外模型和肝组织，以评估ASO的分布和活性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Differential Uptake of Antisense Oligonucleotides in Mouse Hepatocytes and Macrophages Revealed by Simultaneous Two-Photon Excited Fluorescence and Coherent Raman Imaging.

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Differential Uptake of Antisense Oligonucleotides in Mouse Hepatocytes and Macrophages Revealed by Simultaneous Two-Photon Excited Fluorescence and Coherent Raman Imaging.

Antisense oligonucleotides (ASOs), a novel paradigm in modern therapeutics, modulate cellular gene expression by binding to complementary messenger RNA (mRNA) sequences. While advances in ASO medicinal chemistry have greatly improved the efficiency of cellular uptake, selective uptake by specific cell types has been difficult to achieve. For more efficient and selective uptake, ASOs are often conjugated with molecules with high binding affinity for transmembrane receptors. Triantennary N-acetyl-galactosamine conjugated phosphorothioate ASOs (GalNAc-PS-ASOs) were developed to enhance targeted ASO delivery into liver through the hepatocyte-specific asialoglycoprotein receptor (ASGR). We assessed the kinetics of uptake and subsequent intracellular distribution of AlexaFluor 488 (AF488)-labeled PS-ASOs and GalNAc-PS-ASOs in J774A.1 mouse macrophages and primary mouse or rat hepatocytes using simultaneous coherent anti-Stokes Raman scattering (CARS) and two-photon fluorescence (2PF) imaging. The CARS modality captured the dynamic lipid distributions and overall morphology of the cells; two-photon fluorescence (2PF) measured the time- and dose-dependent localization of ASOs delivered by a modified treatment of suspension cells. Our results show that in macrophages, the uptake rate of PS-ASOs did not significantly differ from that of GalNAc-PS-ASOs. However, in hepatocytes, GalNAc-PS-ASOs exhibited a peripheral uptake distribution compared to a polar uptake distribution observed in macrophages. The peripheral distribution correlated with a significantly larger amount of internalized GalNAc-PS-ASOs compared to the PS-ASOs. This work demonstrates the relevance of multimodal imaging for elucidating the uptake mechanism, accumulation, and fate of different ASOs in liver cells that can be used further in complex in vitro models and liver tissues to evaluate ASO distribution and activity.

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来源期刊

Nucleic acid therapeutics BIOCHEMISTRY & MOLECULAR BIOLOGY-CHEMISTRY, MEDICINAL

CiteScore

7.60

自引率

7.50%

发文量

审稿时长

>12 weeks

期刊介绍： Nucleic Acid Therapeutics is the leading journal in its field focusing on cutting-edge basic research, therapeutic applications, and drug development using nucleic acids or related compounds to alter gene expression. The Journal examines many new approaches for using nucleic acids as therapeutic agents or in modifying nucleic acids for therapeutic purposes including: oligonucleotides, gene modification, aptamers, RNA nanoparticles, and ribozymes.