Cerebral cortex
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Recent studies have revealed spatial and functional relations in the temporal dynamics of resting-state functional magnetic resonance imaging (rs-fMRI) or electroencephalography (EEG) signals recorded in the adult brain. By modeling the frequency power spectrum of resting-state brain signals with a power-law function 0(f)α1/fα, the power-law exponent α has been shown to relate to the connectivity patterns of spontaneous brain activity that forms so-called rs-fMRI networks in the human adult brain. ⋯ We show that the spatial segregation of resting-state dynamics of intrinsic fMRI signals in terms of the power-law exponent α is closely related to previously delineated resting-state neuronal architecture that encompasses primary sensory cortices and associate cortex in newborns. Moreover, the spatial profiles of differences in temporal dynamics for rs-fMRI signals could also be observed in EEG measurements in the newborn brain, albeit at a coarser spatial scale, with larger power-law exponents in occipital and parietal cortices compared with signals from the frontal brain.
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The neuron-specific K-Cl cotransporter, KCC2, is highly expressed in the vicinity of excitatory synapses in pyramidal neurons, and recent in vitro data suggest that this protein plays a role in the development of dendritic spines. The in vivo relevance of these observations is, however, unknown. Using in utero electroporation combined with post hoc iontophoretic injection of Lucifer Yellow, we show that premature expression of KCC2 induces a highly significant and permanent increase in dendritic spine density of layer 2/3 pyramidal neurons in the somatosensory cortex. ⋯ In contrast, no effect on spine density was observed following in utero electroporation of a point mutant of KCC2 (KCC2-C568A) where both the cotransporter function and the interaction with the cytoskeleton are disrupted. Transfection of the C-terminal domain of KCC2, a region involved in the interaction with the dendritic cytoskeleton, also increased spine density. Collectively, these results demonstrate a role for KCC2 in excitatory synaptogenesis in vivo through a mechanism that is independent of its ion transport function.
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Functional magnetic resonance imaging signals, in addition to reflecting neuronal response, also contain physiological variances. These factors may introduce variability into blood oxygen level-dependent (BOLD) activation results, particularly in different population groups. In this study, we hypothesized that the amplitude as well as the spatial extent of BOLD activation could be improved after minimizing the variance caused by the neurovascular and anatomical factors. ⋯ Whole-brain analyses were conducted to regress out the anatomical and neurovascular information. Differential maps (obtained using t-test) indicated that the adjustment tended to suppress activation in regions that were near vessels such as midline cingulate gyrus, bilateral anterior insula, and posterior cerebellum. These results suggest that voxelwise adjustment using GMV and neurovascular parameters can minimize structural and physiological variances among individuals and be used for quantitative comparisons.
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Recent magnetic resonance imaging (MRI) studies suggest that abnormalities in Huntington's disease (HD) extend to white matter (WM) tracts in early HD and even in presymptomatic stages. Thus, changes of the corpus callosum (CC) may reflect various aspects of HD pathogenesis. We recruited 17 HD patients, 17 pre-HD subjects, and 34 healthy age-matched controls. ⋯ At this disease stage, both myelin and axonal damage are detectable. Supplementary multiple regression analyses revealed that WM reduction density in the isthmus as well as Disease Burden scores allowed to predict the "HD development" index. While callosal changes seem to proceed in a posterior-to-anterior direction as the diseases progresses, this observation requires validation in future longitudinal investigations.
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Randomized Controlled Trial
Repeatedly pairing vagus nerve stimulation with a movement reorganizes primary motor cortex.
Although sensory and motor systems support different functions, both systems exhibit experience-dependent cortical plasticity under similar conditions. If mechanisms regulating cortical plasticity are common to sensory and motor cortices, then methods generating plasticity in sensory cortex should be effective in motor cortex. Repeatedly pairing a tone with a brief period of vagus nerve stimulation (VNS) increases the proportion of primary auditory cortex responding to the paired tone (Engineer ND, Riley JR, Seale JD, Vrana WA, Shetake J, Sudanagunta SP, Borland MS, Kilgard MP. 2011. ⋯ Rats receiving identical motor training without VNS pairing did not exhibit motor cortex map plasticity. These results suggest that pairing VNS with specific events may act as a general method for increasing cortical representations of those events. VNS movement pairing could provide a new approach for treating disorders associated with abnormal movement representations.