April 2014
Volume 55, Issue 13
Free
ARVO Annual Meeting Abstract  |   April 2014
Comparison of fMRI measurements in LGN and Primary Visual Cortex with visual deficits in Glaucoma
Author Affiliations & Notes
  • Joanne Powell
    University of Liverpool, Liverpool, United Kingdom
  • Anshoo Choudhary
    University of Liverpool, Liverpool, United Kingdom
    Royal Liverpool University Hospital., Liverpool, United Kingdom
  • Laura Parkes
    University of Manchester, Manchester, United Kingdom
  • Sophie Wuerger
    University of Liverpool, Liverpool, United Kingdom
  • Footnotes
    Commercial Relationships Joanne Powell, None; Anshoo Choudhary, None; Laura Parkes, None; Sophie Wuerger, None
  • Footnotes
    Support None
Investigative Ophthalmology & Visual Science April 2014, Vol.55, 3013. doi:
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      Joanne Powell, Anshoo Choudhary, Laura Parkes, Sophie Wuerger; Comparison of fMRI measurements in LGN and Primary Visual Cortex with visual deficits in Glaucoma. Invest. Ophthalmol. Vis. Sci. 2014;55(13):3013.

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      © ARVO (1962-2015); The Authors (2016-present)

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Abstract
 
Purpose
 

Primary open angle glaucoma (POAG) is a major cause of visual morbidity and blindness. Experimental primate glaucoma demonstrates that the retinal ganglion cell (RGC) loss is also associated with atrophies in the lateral geniculate nucleus (LGN) and the primary visual cortex (V1). The purpose of our study was to determine whether, in glaucoma patients, selective behavioural deficits in the three main visual pathways are associated with selective changes in the neural activity in LGN and V1.

 
Methods
 

A POAG group (n=20) and a matched control group (n=20) were examined using the following tests: Visual field loss was assessed using standard automated perimetry (SAP); the Cambridge Colour Vision test (CCT) was used to assess colour deficiencies; visual detection thresholds along the three cardinal directions of colour space were measured (achromatic - BW; red-greenish - RG; yellowish-violet - YV). For a subset of the participants (n=9 in either groups), functional Magnetic Resonance Imaging (fMRI) was used to obtain BOLD (Blood-oxygen-level dependent) signals in the LGN and V1 in response to supra-threshold modulations along the cardinal directions.

 
Results
 

(1) There are significant visual threshold differences between patients with Glaucoma and controls, in particular along the yellowish-violet (YV) cardinal direction. This is confirmed by the Cambridge Colour Vision Test (CCT) which shows differential deficits along the tritanopic confusion line. (2) The average BOLD signal in primary visual cortex (V1) is lower in the Glaucoma group compared to the control group. Within the glaucoma group, high visual thresholds along the yellowish-violet colour direction are associated with low V1 activity. (3) In contrast, the BOLD signal in the lateral geniculate nucleus (LGN) is higher in Glaucoma patients compared to the controls. Within the Glaucoma group, more severe visual field defects are associated with higher LGN activity.

 
Conclusions
 

The BOLD signal in V1 is reduced in patients with POAG, consistent with their loss in visual sensitivity along the cardinal colour directions. Contrary to our expectations, the LGN signal is increased in POAG patients. We speculate that this may reflect feedback from primary visual cortex.

 
 
V1 BOLD signal as a function of colour modulation for patients and controls
 
V1 BOLD signal as a function of colour modulation for patients and controls
 
 
LGN BOLD signal as a function of colour modulation in patients and controls
 
LGN BOLD signal as a function of colour modulation in patients and controls
 
Keywords: 471 color vision • 759 visual impairment: neuro-ophthalmological disease • 755 visual cortex  
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