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Cited 25 time in webofscience Cited 27 time in scopus
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Anti-miR delivery strategies to bypass the blood-brain barrier in glioblastoma therapyopen access

Authors
Kim, Dong GeonKim, Kang HoSeo, Yun JeeYang, HeekyoungMarcusson, Eric G.Son, EunjuLee, KyoungminSa, Jason K.Lee, Hye WonNam, Do-Hyun
Issue Date
May-2016
Publisher
Impact Journals
Keywords
anti-miR; glioblastoma; intratumoral injection; intraventricular injection; delivery efficiency
Citation
Oncotarget, v.7, no.20, pp 29400 - 29411
Pages
12
Indexed
SCIE
SCOPUS
Journal Title
Oncotarget
Volume
7
Number
20
Start Page
29400
End Page
29411
URI
https://scholarworks.korea.ac.kr/kumedicine/handle/2020.sw.kumedicine/6442
DOI
10.18632/oncotarget.8837
ISSN
1949-2553
Abstract
Small non-coding RNAs called miRNAs are key regulators in various biological processes, including tumor initiation, propagation, and metastasis in glioblastoma as well as other cancers. Recent studies have shown the potential for oncogenic miRNAs as therapeutic targets in glioblastoma. However, the application of antisense oligomers, or anti-miRs, to the brain is limited due to the blood-brain barrier (BBB), when administered in the traditional systemic manner. To induce a therapeutic effect in glioblastoma, anti-miR therapy requires a robust and effective delivery system to overcome this obstacle. To bypass the BBB, different delivery administration methods for anti-miRs were evaluated. Stereotaxic surgery was performed to administer anti-Let-7 through intratumoral (ITu), intrathecal (ITh), and intraventricular (ICV) routes, and each method's efficacy was determined by changes in the expression of anti-Let-7 target genes as well as by immunohistochemical analysis. ITu administration of anti-miRs led to a high rate of anti-miR delivery to tumors in the brain by both bolus and continuous administration. In addition, ICV administration, compared with ITu administration, showed a greater distribution of the miR across entire brain tissues. This study suggests that local administration methods are a promising strategy for anti-miR treatment and may overcome current limitations in the treatment of glioblastoma in preclinical animal models.
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