Abstract

The Histology and Imaging core supports analysis of mutant ears and connectional defects at all levels in fixed tissue. The goal of this core is to provide the necessary training and certain services to process and image ears at all light and electron microscopic levels, including high resolution multiphoton imaging using multicolor labeling and 3D reconstruction to accelerate analysis of existing and soon to be analyzed mutants or otherwise manipulated ears, including samples of human ears as needed. To this end, the core provides expertise through the core personnel, including a full time RA expertly trained in all techniques needed to evaluate ears and neuronal connections at all stages of development. Reservation of the equipment in this core (three confocal systems, high resolution transmitted and epifluorescence microscopes and dissecting scopes, TEM and SEM, freezing microtomes, vibratomes and ultramicrotomes) will be handled on line.
The specific aims of the histology and imaging core are: (1) To provide a range of service (advice and/or assistance) for optimized and standardized histological processing at all levels of light and electron microscopy, including sophisticated multicolor immunocytochemical labeling followed by multiphoton analysis, or combinations of in situ hybridization and immunocytochemistry; (2) To improve data analysis through the availability and use of appropriate image processing and quantitative analysis software; (3) To provide expert training in these techniques to stimulate collaboration between members of the core grant as well as potential additional members currently funded through NIDCD. The histology core closely interacts with other cores such as the molecular core for the generation of in situ probes. The core will be driven by the needs of several researchers to achieve a standardized high resolution analysis of various mouse models generated by genetic or other manipulations. The scientific expertise of the core personnel will enhance the performance of all core related research. An annual workshop that provides overviews of the techniques available in this core and their potential usefulness for research of current and future members of the core will generate a vital interaction toward a hearing research related community at the Univ. of Iowa.

Public Health Relevance

The histology and imaging core provides centralized resources and facilities that are readily available to all NIDCD funded investigators at the University of Iowa (currently 19 R01 funded investigators) as well as to other NIH funded investigators at this University. The availability of this core will enhance ongoing NIDCD funded research.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Center Core Grants (P30)
Project #
5P30DC010362-03
Application #
8380794
Study Section
Special Emphasis Panel (ZDC1-SRB-Q)
Project Start
Project End
Budget Start
2012-09-01
Budget End
2013-08-31
Support Year
3
Fiscal Year
2012
Total Cost
$100,864
Indirect Cost
$34,067

  Institution

Name
University of Iowa
Department
Type
DUNS #
062761671
City
Iowa City
State
IA
Country
United States
Zip Code
52242

  Publications

Yang, Tian; Choi, Ji-Eun; Soh, Daniel et al. (2018) CaBP1 regulates Cav1 L-type Ca2+ channels and their coupling to neurite growth and gene transcription in mouse spiral ganglion neurons. Mol Cell Neurosci 88:342-352
Tuft, Bradley W; Xu, Linjing; Leigh, Braden et al. (2018) Photopolymerized micropatterns with high feature frequencies overcome chemorepulsive borders to direct neurite growth. J Tissue Eng Regen Med 12:e1392-e1403
Xu, Linjing; Seline, Alison E; Leigh, Braden et al. (2018) Photopolymerized Microfeatures Guide Adult Spiral Ganglion and Dorsal Root Ganglion Neurite Growth. Otol Neurotol 39:119-126
Leigh, Braden L; Truong, Kristy; Bartholomew, Reid et al. (2017) Tuning Surface and Topographical Features to Investigate Competitive Guidance of Spiral Ganglion Neurons. ACS Appl Mater Interfaces 9:31488-31496
Chagnaud, Boris P; Engelmann, Jacob; Fritzsch, Bernd et al. (2017) Sensing External and Self-Motion with Hair Cells: A Comparison of the Lateral Line and Vestibular Systems from a Developmental and Evolutionary Perspective. Brain Behav Evol 90:98-116
Li, Tongchao; Giagtzoglou, Nikolaos; Eberl, Daniel F et al. (2016) The E3 ligase Ubr3 regulates Usher syndrome and MYH9 disorder proteins in the auditory organs of Drosophila and mammals. Elife 5:
Li, Shufeng; Tuft, Bradley; Xu, Linjing et al. (2016) Intracellular calcium and cyclic nucleotide levels modulate neurite guidance by microtopographical substrate features. J Biomed Mater Res A 104:2037-48
Eyo, Ukpong B; Miner, Samuel A; Weiner, Joshua A et al. (2016) Developmental changes in microglial mobilization are independent of apoptosis in the neonatal mouse hippocampus. Brain Behav Immun 55:49-59
Kay, Alan R; Raccuglia, Davide; Scholte, Jon et al. (2016) Goggatomy: A Method for Opening Small Cuticular Compartments in Arthropods for Physiological Experiments. Front Physiol 7:398
Yang, Tian; Scholl, Elizabeth S; Pan, Ning et al. (2016) Expression and Localization of CaBP Ca2+ Binding Proteins in the Mouse Cochlea. PLoS One 11:e0147495

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