Is the ADHD brain wired differently? A review on structural and functional connectivity in attention deficit hyperactivity disorder

Kerstin Konrad, Simon B. Eickhoff
2010 Human Brain Mapping  
In recent years, a change in perspective in etiological models of attention deficit hyperactivity disorder (ADHD) has occurred in concordance with emerging concepts in other neuropsychiatric disorders such as schizophrenia and autism. These models shift the focus of the assumed pathology from regional brain abnormalities to dysfunction in distributed network organization. In the current contribution, we report findings from functional connectivity studies during resting and task states, as well
more » ... as from studies on structural connectivity using diffusion tensor imaging, in subjects with ADHD. Although major methodological limitations in analyzing connectivity measures derived from noninvasive in vivo neuroimaging still exist, there is convergent evidence for white matter pathology and disrupted anatomical connectivity in ADHD. In addition, dysfunctional connectivity during rest and during cognitive tasks has been demonstrated. However, the causality between disturbed white matter architecture and cortical dysfunction remains to be evaluated. Both genetic and environmental factors might contribute to disruptions in interactions between different brain regions. Stimulant medication not only modulates regionally specific activation strength but also normalizes dysfunctional connectivity, pointing to a predominant network dysfunction in ADHD. By combining a longitudinal approach with a systems perspective in ADHD in the future, it might be possible to identify at which stage during development disruptions in neural networks emerge and to delineate possible new endophenotypes of ADHD. Hum Brain Mapp 31:904-916, in Wiley InterScience (www. V C 2010 Wiley-Liss, Inc. r Structural and Functional Connectivity in ADHD r r 905 r r Konrad and Eickhoff r r 906 r r Structural and Functional Connectivity in ADHD r r 909 r r Konrad and Eickhoff r r 914 r
doi:10.1002/hbm.21058 pmid:20496381 fatcat:r66d27bujncm3md2mv7tngc3li