Artículos de revistas
Altered gray matter morphometry and resting-state functional and structural connectivity in social anxiety disorder
Fecha
2011Registro en:
BRAIN RESEARCH, v.1388, p.167-177, 2011
0006-8993
10.1016/j.brainres.2011.03.018
Autor
LIAO, Wei
XU, Qiang
MANTINI, Dante
DING, Jurong
MACHADO-DE-SOUSA, Joao Paulo
HALLAK, Jaime E. C.
TRZESNIAK, Clarissa
QIU, Changjian
ZENG, Ling
ZHANG, Wei
CRIPPA, Jose Alexandre S.
GONG, Qiyong
CHEN, Huafu
Institución
Resumen
In social anxiety disorder (SAD), impairments in limbic/paralimbic structures are associated with emotional dysregulation and inhibition of the medial prefrontal cortex (MPFq. Little is known, however, about alterations in limbic and frontal regions associated with the integrated morphometric, functional, and structural architecture of SAD. Whether altered gray matter volume is associated with altered functional and structural connectivity in SAD. Three techniques were used with 18 SAD patients and 18 healthy controls: voxel-based morphometry; resting-state functional connectivity analysis; and diffusion tensor imaging tractography. SAD patients exhibited significantly decreased gray matter volumes in the right posterior inferior temporal gyrus (ITG) and right parahippocampal/hippocampal gyrus (PHG/HIP). Gray matter volumes in these two regions negatively correlated with the fear factor of the Liebowitz Social Anxiety Scale. In addition, we found increased functional connectivity in SAD patients between the right posterior ITG and the left inferior occipital gyrus, and between the right PHF/HIP and left middle temporal gyms. SAD patients had increased right MPFC volume, along with enhanced structural connectivity in the genu of the corpus callosum. Reduced limbic/paralimbic volume, together with increased resting-state functional connectivity, suggests the existence of a compensatory mechanism in SAD. Increased MPFC volume, consonant with enhanced structural connectivity, suggests a long-time overgeneralization of structural connectivity and a role of this area in the mediation of clinical severity. Overall, our results may provide a valuable basis for future studies combining morphometric, functional and anatomical data in the search for a comprehensive understanding of the neural circuitry underlying SAD. (C) 2011 Elsevier B.V. All rights reserved.