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Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2
Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2
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Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2
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Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2
Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2

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Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2
Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2
Journal Article

Linking retinotopic fMRI mapping and anatomical probability maps of human occipital areas V1 and V2

2005
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Overview
Using functional MRI, we characterized field sign maps of the occipital cortex and created three-dimensional maps of these areas. By averaging the individual maps into group maps, probability maps of functionally defined V1 or V2 were determined and compared to anatomical probability maps of Brodmann areas BA17 and BA18 derived from cytoarchitectonic analysis (Amunts, K., Malikovic, A., Mohlberg, H., Schormann, T., Zilles, K., 2000. Brodmann's areas 17 and 18 brought into stereotaxic space—where and how variable? NeuroImage 11, 66–84). Comparison of areas BA17/V1 and BA18/V2 revealed good agreement of the anatomical and functional probability maps. Taking into account that our functional stimulation (due to constraints of the visual angle of stimulation achievable in the MR scanner) only identified parts of V1 and V2, for statistical evaluation of the spatial correlation of V1 and BA17, or V2 and BA18, respectively, the a priori measure κ was calculated testing the hypothesis that a region can only be part of functionally defined V1 or V2 if it is also in anatomically defined BA17 or BA18, respectively. κ = 1 means the hypothesis is fully true, κ = 0 means functionally and anatomically defined visual areas are independent. When applying this measure to the probability maps, κ was equal to 0.84 for both V1/BA17 and V2/BA18. The data thus show a good correspondence of functionally and anatomically derived segregations of early visual processing areas and serve as a basis for employing anatomical probability maps of V1 and V2 in group analyses to characterize functional activations of early visual processing areas.

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