University of Illinois Urbana-Champaign

Neuronal Polarization and Axonal mRNA Localization on Microfabricated Substrates

Scharnweber, Rudi

This item is only available for download by members of the University of Illinois community. Students, faculty, and staff at the U of I may log in with your NetID and password to view the item. If you are trying to access an Illinois-restricted dissertation or thesis, you can request a copy through your library's Inter-Library Loan office or purchase a copy directly from ProQuest.

Permalink

https://hdl.handle.net/2142/82527

Description

Title
Neuronal Polarization and Axonal mRNA Localization on Microfabricated Substrates
Author(s)
Scharnweber, Rudi
Issue Date
2009
Doctoral Committee Chair(s)
Wheeler, Bruce C.
Department of Study
Neuroscience
Discipline
Neuroscience
Degree Granting Institution
University of Illinois at Urbana-Champaign
Degree Name
Ph.D.
Degree Level
Dissertation
Keyword(s)
Biology, Molecular
Language
eng
Abstract
Complex structures at both the gross and cellular levels endow the nervous system with its distinct function: the rapid processing of information via elaborate patterns of synaptic connectivity. Various arrangements of numerous growth factors, guidance cues, and other molecules influence both the interconnectivity of neurons and the subcellular makeup of individual neurons. This dissertation describes experiments that used an engineering-based approach to study the mechanisms that regulate neuronal behavior, both in small networks and at the subcellular level. The first half of this report shows that high-resolution protein patterns and cellular positioning systems may eventually be used to develop simple, reliable neuronal networks. Specifically, a PDMS stencil was used to restrict cellular positions at plating to specific regions on a micropatterned culturing substrate with the goal of regulating neurite outgrowth and neuronal network formation. Also, a variety of protein patterns were tested to determine their effects on the direction of axonal extension. Next, to look at subcellular events during axon outgrowth, the second half of the dissertation utilized a PDMS microdevice to isolate purified axonal mRNA transcripts for microarray analysis. The list of axonal mRNAs generated will facilitate further studies of protein synthesis within axons, which is now a recognized process in normal axon physiology.
Graduation Semester
2009
Type of Resource
text
Permalink
http://hdl.handle.net/2142/82527

Owning Collections

Graduate Dissertations and Theses at Illinois PRIMARY
Graduate Theses and Dissertations at Illinois
Dissertations - Neuroscience