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Journal article

Tracking neuronal marker expression inside living differentiating cells using molecular beacons

From

Department of Micro- and Nanotechnology, Technical University of Denmark1

Surface Physics and Catalysis, Department of Physics, Technical University of Denmark2

Silicon Microtechnology, Department of Micro- and Nanotechnology, Technical University of Denmark3

Fluidic Array Systems and Technology, Department of Micro- and Nanotechnology, Technical University of Denmark4

Monitoring gene expression is an important tool for elucidating mechanisms of cellular function. In order to monitor gene expression during nerve cell development, molecular beacon (MB) probes targeting markers representing different stages of neuronal differentiation were designed and synthesized as 2'-O-methyl RNA backbone oligonucleotides.

MBs were transfected into human mesencephalic cells (LUHMES) using streptolysin-O-based membrane permeabilization. Mathematical modeling, simulations and experiments indicated that MB concentration was equal to the MB in the transfection medium after 10 min transfection. The cells will then each contain about 60,000 MBs.

Gene expression was detected at different time points using fluorescence microscopy. Nestin and NeuN mRNA were expressed in approximately 35% of the LUHMES cells grown in growth medium, and in 80-90% of cells after differentiation. MAP2 and tyrosine hydroxylase mRNAs were expressed 2 and 3 days post induction of differentiation, respectively.

Oct 4 was not detected with MB in these cells and signal was not increased over time suggesting that MB are generally stable inside the cells. The gene expression changes measured using MBs were confirmed using qRT-PCR. These results suggest that MBs are simple to use sensors inside living cell, and particularly useful for studying dynamic gene expression in heterogeneous cell populations.

Language: English
Publisher: Frontiers Media S.A.
Year: 2013
Pages: 266
ISSN: 16625102
Types: Journal article
DOI: 10.3389/fncel.2013.00266
ORCIDs: Hansen, Ole and Dufva, Martin

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