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Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection

From a cohort of 36 patients presenting apperceptive tactile agnosia after first cortical ischemic stroke, 14 showed temporary impairment at admission. A previous multi-voxel analysis of the cortical lesions, using as explanatory variable the course of tactile object recognition performance over the...

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Autores principales: Missimer, John H., Abela, Eugenio, Pastore-Wapp, Manuela, Wiest, Roland, Weder, Bruno J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9486662/
https://www.ncbi.nlm.nih.gov/pubmed/36126517
http://dx.doi.org/10.1016/j.nicl.2022.103193
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author Missimer, John H.
Abela, Eugenio
Pastore-Wapp, Manuela
Wiest, Roland
Weder, Bruno J.
author_facet Missimer, John H.
Abela, Eugenio
Pastore-Wapp, Manuela
Wiest, Roland
Weder, Bruno J.
author_sort Missimer, John H.
collection PubMed
description From a cohort of 36 patients presenting apperceptive tactile agnosia after first cortical ischemic stroke, 14 showed temporary impairment at admission. A previous multi-voxel analysis of the cortical lesions, using as explanatory variable the course of tactile object recognition performance over the recovery period of 9 months, partitioned the cohort into three subgroups. Of the 14 patients constituting two of the subgroups, 7 recovered from their impairment whereas 7 did not. These two subgroups could not be distinguished at admission. The primary aim of the present study is to present two assessments that can do so. The first assessment comprises a pattern of behavioral measures, determined via principal component analysis, encoded in three tests: picking small objects, macrogeometrical discrimination and tactile object recognition. The receiver operating characteristic curve derived from permutation of the behavioral test scores yielded an 80% probability of correct identification of the patient subgroup and an 8% probability for false identification. As done with the permuted scores, the pattern could predict the persistence of affliction of new stroke patients with tactile agnosia. The second predictive assessment extends our previous evaluation of cortical MRI lesion maps to include subcortical regions. Confirming our previous study, the lesions of the persistently impaired subgroup disrupted significantly the anterior arcuatus fasciculus and associated superior longitudinal fasciculus III in the ipsilesional hemisphere, impeding reciprocal information transfer between supramarginal gyrus and both the ventral premotor cortex and Brodmann area 44. Due to the importance of interhemispheric information transfer in tactile agnosia, we performed a supplementary analysis of tactile object recognition scores. It showed that haptic information transfer from the non-affected to the affected hands in the persistent cases partly restored function during the nine months, possibly following restoration of functional interhemispheric haptic information transfer at the border of posterior corpus callosum and splenium. In conclusion, the combined findings of the cortical lesion at subarea PFt of the inferior parietal lobule and the associated subcortical tract lesions permit almost perfect prediction of persistent impairment of tactile object recognition. The study substantiates the need for combined analysis of both cortical lesions and white matter tract disconnections.
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spelling pubmed-94866622022-09-21 Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection Missimer, John H. Abela, Eugenio Pastore-Wapp, Manuela Wiest, Roland Weder, Bruno J. Neuroimage Clin Regular Article From a cohort of 36 patients presenting apperceptive tactile agnosia after first cortical ischemic stroke, 14 showed temporary impairment at admission. A previous multi-voxel analysis of the cortical lesions, using as explanatory variable the course of tactile object recognition performance over the recovery period of 9 months, partitioned the cohort into three subgroups. Of the 14 patients constituting two of the subgroups, 7 recovered from their impairment whereas 7 did not. These two subgroups could not be distinguished at admission. The primary aim of the present study is to present two assessments that can do so. The first assessment comprises a pattern of behavioral measures, determined via principal component analysis, encoded in three tests: picking small objects, macrogeometrical discrimination and tactile object recognition. The receiver operating characteristic curve derived from permutation of the behavioral test scores yielded an 80% probability of correct identification of the patient subgroup and an 8% probability for false identification. As done with the permuted scores, the pattern could predict the persistence of affliction of new stroke patients with tactile agnosia. The second predictive assessment extends our previous evaluation of cortical MRI lesion maps to include subcortical regions. Confirming our previous study, the lesions of the persistently impaired subgroup disrupted significantly the anterior arcuatus fasciculus and associated superior longitudinal fasciculus III in the ipsilesional hemisphere, impeding reciprocal information transfer between supramarginal gyrus and both the ventral premotor cortex and Brodmann area 44. Due to the importance of interhemispheric information transfer in tactile agnosia, we performed a supplementary analysis of tactile object recognition scores. It showed that haptic information transfer from the non-affected to the affected hands in the persistent cases partly restored function during the nine months, possibly following restoration of functional interhemispheric haptic information transfer at the border of posterior corpus callosum and splenium. In conclusion, the combined findings of the cortical lesion at subarea PFt of the inferior parietal lobule and the associated subcortical tract lesions permit almost perfect prediction of persistent impairment of tactile object recognition. The study substantiates the need for combined analysis of both cortical lesions and white matter tract disconnections. Elsevier 2022-09-13 /pmc/articles/PMC9486662/ /pubmed/36126517 http://dx.doi.org/10.1016/j.nicl.2022.103193 Text en © 2022 The Author(s) https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Regular Article
Missimer, John H.
Abela, Eugenio
Pastore-Wapp, Manuela
Wiest, Roland
Weder, Bruno J.
Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection
title Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection
title_full Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection
title_fullStr Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection
title_full_unstemmed Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection
title_short Distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – Behavioral and neuroimaging evidence for white matter disconnection
title_sort distinguishing transient from persistent tactile agnosia after partial anterior circulation infarcts – behavioral and neuroimaging evidence for white matter disconnection
topic Regular Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9486662/
https://www.ncbi.nlm.nih.gov/pubmed/36126517
http://dx.doi.org/10.1016/j.nicl.2022.103193
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