4.7 Article

Aptamers for Addressed Boron Delivery in BNCT: Effect of Boron Cluster Attachment Site on Functional Activity

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MDPI
DOI: 10.3390/ijms24010306

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cell-specific aptamers; boron clusters; boron neutron capture therapy; boron delivery agents; glioblastoma; cancer treatment

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Boron neutron capture therapy (BNCT) is a unique anti-cancer treatment strategy that improves treatment accuracy by precisely positioning a neutron beam and delivering boron compounds. This study demonstrates the feasibility of using cell-specific RNA aptamers for targeted delivery of boron clusters in BNCT. The results show that the amount of boron-loaded aptamer inside the cell exceeds 1 x 10^9 atoms/cell, and the efficacy of boron-loaded RNA conjugates is comparable to that of B-10-boronophenylalanine.
Among the great variety of anti-cancer therapeutic strategies, boron neutron capture therapy (BNCT) represents a unique approach that doubles the targeting accuracy due to the precise positioning of a neutron beam and the addressed delivery of boron compounds. We have recently demonstrated the principal possibility of using a cell-specific 2 '-F-RNA aptamer for the targeted delivery of boron clusters for BNCT. In the present study, we evaluated the amount of boron-loaded aptamer inside the cell via two independent methods: quantitative real-time polymerase chain reaction and inductive coupled plasma-atomic emission spectrometry. Both assays showed that the internalized boron level inside the cell exceeds 1 x 10(9) atoms/cell. We have synthesized closo-dodecaborate conjugates of 2 '-F-RNA aptamers GL44 and Waz, with boron clusters attached either at the 3 '- or at the 5 '-end. The influence of cluster localization was evaluated in BNCT experiments on U-87 MG human glioblastoma cells and normal fibroblasts and subsequent analyses of cell viability via real-time cell monitoring and clonogenic assay. Both conjugates of GL44 aptamer provided a specific decrease in cell viability, while only the 3 '-conjugate of the Waz aptamer showed the same effect. Thus, an individual adjustment of boron cluster localization is required for each aptamer. The efficacy of boron-loaded 2 '-F-RNA conjugates was comparable to that of B-10-boronophenylalanine, so this type of boron delivery agent has good potential for BNCT due to such benefits as precise targeting, low toxicity and the possibility to use boron clusters made of natural, unenriched boron.

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