Modulation of the Biological Activity of microRNA-210 with Peptide Nucleic Acids (PNAs)

Modulation of the Biological Activity of microRNA-210 with Peptide Nucleic Acids (PNAs)

Herein we describe the activity of a peptide nucleic acid (PNA) that targets microRNA‐210 (miR‐210), which is associated with hypoxia and is modulated during erythroid differentiation. PNAs directed against miR‐210 were designed to bind with high affinity to the target RNA strand and to undergo effi...

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Bibliographic Details
Published in:ChemMedChem Vol. 6; no. 12; pp. 2192 - 2202
Main Authors: Fabbri, Enrica, Manicardi, Alex, Tedeschi, Tullia, Sforza, Stefano, Bianchi, Nicoletta, Brognara, Eleonora, Finotti, Alessia, Breveglieri, Giulia, Borgatti, Monica, Corradini, Roberto, Marchelli, Rosangela, Gambari, Roberto
Format: Journal Article
Language:English
Published: Weinheim WILEY-VCH Verlag 09-12-2011
WILEY‐VCH Verlag
Subjects:
Base Sequence
Cell Line, Tumor
drug delivery
erythroid differentiation
gamma-Globins - genetics
gamma-Globins - metabolism
hemoglobin
Humans
microRNAs
MicroRNAs - metabolism
peptide nucleic acids
Peptide Nucleic Acids - chemical synthesis
Peptide Nucleic Acids - chemistry
Peptide Nucleic Acids - pharmacology
Peptides - chemistry
Phase Transition
Ultraviolet Rays
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Summary:Herein we describe the activity of a peptide nucleic acid (PNA) that targets microRNA‐210 (miR‐210), which is associated with hypoxia and is modulated during erythroid differentiation. PNAs directed against miR‐210 were designed to bind with high affinity to the target RNA strand and to undergo efficient uptake in target cells. A polyarginine–PNA conjugate directed against miR‐210 (Rpep‐PNA‐a210) showed both very high affinity for RNA and efficient uptake into target cells without the need for transfection reagents. An unmodified PNA of the same sequence displayed the ability to bind RNA, but cellular uptake was very poor. Consistent with this, only Rpep‐PNA‐a210 strongly inhibited miR‐210 activity, as evaluated by assays on undifferentiated K562 cells and on cells treated with mithramycin, which was found to induce erythroid differentiation and miR‐210 overexpression. Targeting miR‐210 by Rpep‐PNA‐a210 resulted in: 1) a decrease in miR‐210 levels as measured by RT‐PCR, 2) up‐regulation of raptor mRNA, 3) a decrease in γ‐globin mRNA, and 4) decreased expression of differentiated functions (i.e., proportion of benzidine‐positive cells, content of embryo‐fetal hemoglobins). The efficient delivery of anti‐miR PNAs through a suitable peptide carrier (Rpep‐PNA‐a210) leads to the inhibition of miR‐210 activity, altering the expression of miR‐210‐regulated erythroid functions. R8‐conjugated PNAs for uptake! A polyarginine–PNA conjugate that targets microRNA‐210 (Rpep‐PNA‐a210, or miR‐210) shows high affinity for RNA, efficient uptake into target cells without the need for transfection reagents, and potent inhibitory effects toward the biological activity of microRNA‐210.
Bibliography:istex:55888FD6AF80803EB10D0E43EED3D56EF7E713D3
ArticleID:CMDC201100270
ark:/67375/WNG-X84K1VHX-V
ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
content type line 23
ISSN:1860-7179
1860-7187
DOI:10.1002/cmdc.201100270