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Insights from 'Endosomal Escape and Nuclear Localization: Critical Barriers for Antisense Therapeutics

Insights from 'Endosomal Escape and Nuclear Localization: Critical Barriers for Antisense Therapeutics
Antisense oligonucleotides (ASOs) struggle with endosomal entrapment and inefficient nuclear localization, limiting their therapeutic impact. Researchers explore solutions like endosomal escape agents, peptide-based transport, lipid nanoparticles (LNPs), and nuclear localization signals (NLS) to enhance delivery. Combining non-toxic endosomal escape mechanisms with NLS-enhanced strategies could significantly improve ASO therapies, making them more effective for disease treatment.
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Endosomal Escape and Nuclear Localization: Critical Barriers for Antisense Therapeutics

Endosomal Escape and Nuclear Localization: Critical Barriers for Antisense Therapeutics
Antisense oligonucleotides (ASOs) are promising gene-targeting therapies, but endosomal escape and nuclear localization limit their effectiveness. Only 1-2% of ASOs reach their target mRNA. Strategies like lipid nanoparticles, pH-responsive materials, and membrane-destabilizing agents aim to improve ASO delivery. Enhancing nuclear localization is also critical for splice-switching oligonucleotides (SSOs). Overcoming these barriers is essential for making ASO-based therapies viable in clinical settings.
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