TY - JOUR
T1 - Direct synthesis of partially modified 2'-O-pivaloyloxymethyl RNAs by a base-labile protecting group strategy and their potential for prodrug-based gene-silencing applications
AU - Biscans, Annabelle
AU - Bos, Maxence
AU - Martin, Anthony R.
AU - Ader, Nicholas
AU - Sczakiel, Georg
AU - Vasseur, Jean Jacques
AU - Dupouy, Christelle
AU - Debart, Françoise
PY - 2014/10/24
Y1 - 2014/10/24
N2 - An original and straightforward synthesis of partially modified 2'-O-pivaloyloxymethyl-substituted (PivOM-substituted) oligori-bonucleotides has been achieved. The aim of this 2'-enzymola-bile modification was to enhance nuclease stability of RNA and transmembrane transport. To make these modified RNAs easily available we developed a base-labile protecting group strategy with standard protections for nucleobases (acyl) and phosphates (cyanoethyl), a Q-linker and two different acetalester protection groups for 2'-OH: propionyloxymethyl (PrOM) and PivOM. Interestingly, orthogonal deprotection conditions based on anhydrous butylamine in THF were found to remove propionyloxymethyl groups selectively, while preserving PivOM groups. Duplex stability, circular dichroism studies and nuclease resistance, as well as the ability to inhibit gene expression of modified 2'-O-PivOM RNA, were evaluated.
AB - An original and straightforward synthesis of partially modified 2'-O-pivaloyloxymethyl-substituted (PivOM-substituted) oligori-bonucleotides has been achieved. The aim of this 2'-enzymola-bile modification was to enhance nuclease stability of RNA and transmembrane transport. To make these modified RNAs easily available we developed a base-labile protecting group strategy with standard protections for nucleobases (acyl) and phosphates (cyanoethyl), a Q-linker and two different acetalester protection groups for 2'-OH: propionyloxymethyl (PrOM) and PivOM. Interestingly, orthogonal deprotection conditions based on anhydrous butylamine in THF were found to remove propionyloxymethyl groups selectively, while preserving PivOM groups. Duplex stability, circular dichroism studies and nuclease resistance, as well as the ability to inhibit gene expression of modified 2'-O-PivOM RNA, were evaluated.
UR - http://www.scopus.com/inward/record.url?scp=84915750429&partnerID=8YFLogxK
U2 - 10.1002/cbic.201402382
DO - 10.1002/cbic.201402382
M3 - Journal articles
C2 - 25346406
AN - SCOPUS:84915750429
SN - 1439-4227
VL - 15
SP - 2674
EP - 2679
JO - Chembiochem
JF - Chembiochem
IS - 18
ER -