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Polyamidoamine-Carbon Nanodot Conjugates with Bioreducible Building Blocks: Smart Theranostic Platforms for Targeted siRNA Delivery

Salvatore Emanuele Drago, Mara Andrea Utzeri, Nicolò Mauro, Gennara Cavallaro

2024Biomacromolecules10 citationsDOIOpen Access PDF

Abstract

High Resolution Image Download MS PowerPoint Slide This study focuses on designing hybrid theranostic nanosystems, utilizing gadolinium-doped carbon nanodots decorated with bioreducible amphoteric polyamidoamines (PAAs). The objective is to synergize the exceptional theranostic properties of gadolinium-doped carbon nanodots (CDs) with the siRNA complexation capabilities of PAAs. Linear copolymeric polyamidoamines, based on N, N ′-bis(acryloyl)cystamine, arginine, and agmatine, were synthesized, resulting in three distinct amphoteric copolymers. Notably, sulfur bridges within the PAA repeating units confer pronounced susceptibility to glutathione-mediated degradation─a key attribute in the tumor microenvironment. This pathway enables controlled and stimuli-responsive siRNA release, theoretically providing precise spatiotemporal control over therapeutic interventions. The selected PAA, conjugated with CDs using the redox-sensitive spacer cystamine, formed the CDs-Cys-PAA conjugate with superior siRNA complexing capacity. Stable against polyanion exchange, the CDs-Cys-PAA/siRNA complex released siRNA in the presence of GSH. In vitro studies assessed cytocompatibility, internalization, and gene silencing efficacy on HeLa, MCF-7, and 16HBE cell lines.

Topics & Concepts

CystamineNanodotChemistryInternalizationGene silencingConjugateSmall interfering RNANanotechnologyBiophysicsCombinatorial chemistryMaterials scienceBiochemistryTransfectionCellBiologyMathematical analysisGeneMathematicsGraphene and Nanomaterials ApplicationsRNA Interference and Gene DeliveryAdvanced biosensing and bioanalysis techniques
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