Criteria for developing active cellular targeting miRNA oligonucleotide therapeutics with a peptide nucleic acid backbone: Combating cardiometabolic pandemics

Marc Thibonnier
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Abstract

Oligonucleotide therapeutics (ONTs) represent a growing new class of therapeutic agents aimed at addressing chronic diseases that remain untreatable by small molecules and antibodies. Our goal was to establish a selection of several criteria to design and develop miRNA-based ONTs, focusing on improved chemistry, pharmacokinetics/pharmacodynamics (PK/PD) profiles, and safety characteristics to combat cardiometabolic pandemics. By leveraging our own experimental data obtained from experiments involving miR-22-3p antagomirs and a careful review of the literature, we established a set of seven criteria to optimize the design of miRNA ONTs. These criteria prioritize simplified drug synthesis, optimized PK/PD properties, and reduced potential toxicities. This proposed set of seven criteria represents a novel strategy for developing active cellular targeting miRNA ONTs for various therapeutic indications.
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开发以肽核酸为骨架的活性细胞靶向 miRNA 寡核苷酸疗法的标准:抗击心脏代谢大流行病
寡核苷酸疗法(ONTs)是一类不断发展的新型治疗药物,旨在解决小分子药物和抗体仍无法治疗的慢性疾病。我们的目标是建立设计和开发基于 miRNA 的 ONTs 的若干标准选择,重点是改进化学、药代动力学/药效学(PK/PD)特征和安全性特征,以防治心脏代谢大流行病。通过利用我们从 miR-22-3p 抗凝集素实验中获得的实验数据以及对文献的仔细研究,我们建立了一套七项标准来优化 miRNA ONTs 的设计。这些标准优先考虑简化药物合成、优化 PK/PD 特性和减少潜在毒性。这套拟议的七项标准代表了一种新策略,可用于开发针对各种治疗适应症的活性细胞靶向 miRNA ONTs。
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