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Inhibition and brain work

Buzsaki, Gyorgy; Kaila, Kai; Raichle, Marcus
The major part of the brain's energy budget ( approximately 60%-80%) is devoted to its communication activities. While inhibition is critical to brain function, relatively little attention has been paid to its metabolic costs. Understanding how inhibitory interneurons contribute to brain energy consumption (brain work) is not only of interest in understanding a fundamental aspect of brain function but also in understanding functional brain imaging techniques which rely on measurements related to blood flow and metabolism. Herein we examine issues relevant to an assessment of the work performed by inhibitory interneurons in the service of brain function
PMCID:2266612
PMID: 18054855
ISSN: 0896-6273
CID: 148925

Generation of uniform fly retinas [Letter]

Wernet, Mathias F; Celik, Arzu; Mikeladze-Dvali, Tamara; Desplan, Claude
PMID: 18054757
ISSN: 0960-9822
CID: 1694682

Cerebellum morphogenesis: the foliation pattern is orchestrated by multi-cellular anchoring centers

Sudarov, Anamaria; Joyner, Alexandra L
BACKGROUND: The cerebellum has a striking morphology consisting of folia separated by fissures of different lengths. Since folia in mammals likely serve as a broad platform on which the anterior-posterior organization of the sensory-motor circuits of the cerebellum are built, it is important to understand how such complex morphology arises. RESULTS: Using a combination of genetic inducible fate mapping, high-resolution cellular analysis and mutant studies in mouse, we demonstrate that a key event in initiation of foliation is the acquisition of a distinct cytoarchitecture in the regions that will become the base of each fissure. We term these regions 'anchoring centers'. We show that the first manifestation of anchoring centers when the cerebellar outer surface is smooth is an increase in proliferation and inward thickening of the granule cell precursors, which likely causes an associated slight invagination of the Purkinje cell layer. Thereafter, granule cell precursors within anchoring centers become distinctly elongated along the axis of the forming fissure. As the outer cerebellar surface begins to fold inwards, Bergmann glial fibers radiate in towards the base of the immature fissure in a fan shape. Once the anchoring center is formed, outgrowth of folia seems to proceed in a self-sustaining manner driven by granule cell migration along Bergmann glial fibers. Finally, by analyzing a cerebellum foliation mutant (Engrailed 2), we demonstrate that changing the timing of anchoring center formation leads to predictable changes in the shape and size of the surrounding folia. CONCLUSION: We present a new cellular model of the initial formation of cerebellar fissures with granule cells providing the driving physical force. Both the precise timing of the appearance of anchoring centers at the prospective base of each fissure and the subsequent coordinated action of granule cells and Bergmann glial fibers within the anchoring centers dictates the shape of the folia
PMCID:2246128
PMID: 18053187
ISSN: 1749-8104
CID: 96756

Statistical modeling of images with fields of Gaussian scale mixtures

Chapter by: Lyu, Siwei; Simoncelli, Eero P.
in: Advances in Neural Information Processing Systems by
[S.l.] : Neural information processing systems foundation, 2007
pp. 945-952
ISBN: 9780262195683
CID: 2873012

Learning to be Bayesian without supervision

Chapter by: Raphan, Martin; Simoncelli, Eero P.
in: Advances in Neural Information Processing Systems by
[S.l.] : Neural information processing systems foundation, 2007
pp. 1145-1152
ISBN: 9780262195683
CID: 2873002

Lateralized caudate metabolic abnormalities in adolescent major depressive disorder: a proton MR spectroscopy study

Gabbay, Vilma; Hess, David A; Liu, Songtao; Babb, James S; Klein, Rachel G; Gonen, Oded
OBJECTIVE: Proton magnetic resonance spectroscopy ((1)H-MRS) has been increasingly used to examine striatal neurochemistry in adult major depressive disorder. This study extends the use of this modality to pediatric major depression to test the hypothesis that adolescents with major depression have elevated concentrations of striatal choline and creatine and lower concentrations of N-acetylaspartate. METHOD: Fourteen adolescents (ages 12-19 years, eight female) who had major depressive disorder for at least 8 weeks and a severity score of 40 or higher on the Children's Depression Rating Scale-Revised and 10 healthy comparison adolescents (six female) group-matched for gender, age, and handedness were enrolled. All underwent three-dimensional 3-T (1)H-MRS at high spatial resolution (0.75-cm(3) voxels). Relative levels of choline, creatine, and N-acetylaspartate in the left and right caudate, putamen, and thalamus were scaled into concentrations using phantom replacement, and levels were compared for the two cohorts. RESULTS: Relative to comparison subjects, adolescents with major depressive disorder had significantly elevated concentrations of choline (2.11 mM versus 1.56 mM) and creatine (6.65 mM versus 5.26 mM) in the left caudate. No other neurochemical differences were observed between the groups. CONCLUSIONS: These findings most likely reflect accelerated membrane turnover and impaired metabolism in the left caudate. The results are consistent with prior imaging reports of focal and lateralized abnormalities in the caudate in adult major depression
PMCID:2774821
PMID: 18056244
ISSN: 0002-953x
CID: 75716

Interleukin-11 potentiates oligodendrocyte survival and maturation, and myelin formation [Meeting Abstract]

Zhang, YT; Taveggia, C; Melendez-Vasquez, CV; Einheber, S; Salzer, JL; Raine, CS; Brosnan, CF; John, G
ISI:000251708800341
ISSN: 1740-925x
CID: 87174

Tetanus toxin C fragment-conjugated nanoparticles for targeted drug delivery to neurons

Townsend, Seth A; Evrony, Gilad D; Gu, Frank X; Schulz, Martin P; Brown, Robert H; Langer, Robert
The use of nanoparticles for targeted drug delivery is often facilitated by specific conjugation of functional targeting molecules to the nanoparticle surface. We compared different biotin-binding proteins (avidin, streptavidin, or neutravidin) as crosslinkers to conjugate proteins to biodegradable nanoparticles prepared from poly(lactic-co-glycolic acid) (PLGA)-polyethylene glycol (PEG)-biotin polymers. Avidin gave the highest levels of overall protein conjugation, whereas neutravidin minimized protein non-specific binding to the polymer. The tetanus toxin C fragment (TTC), which is efficiently retrogradely transported in neurons and binds to neurons with high specificity and affinity, retained the ability to bind to neuroblastoma cells following amine group modifications. TTC was conjugated to nanoparticles using neutravidin, and the resulting nanoparticles were shown to selectively target neuroblastoma cells in vitro. TTC-conjugated nanoparticles have the potential to serve as drug delivery vehicles targeted to the central nervous system.
PMID: 17854886
ISSN: 0142-9612
CID: 3332462

The role of impaired neuronal communication in neurological disorders

He, Biyu J; Shulman, Gordon L; Snyder, Abraham Z; Corbetta, Maurizio
PURPOSE OF REVIEW: Basic and translational neuroscience findings indicate that normal brain function depends on activity synchronization within distributed brain networks. This conclusion suggests a view of how brain injury causes behavioral deficits that differs from traditional localizationist views. RECENT FINDINGS: Novel functional neuroimaging methods demonstrate coherent activity in large-scale networks not only during task performance but also, surprisingly, at rest (i.e. in the absence of stimuli, tasks, or overt responses). Furthermore, breakdown of activity coherence at rest, even in regions of the brain that are structurally intact, correlates with behavioral deficits and their recovery after injury. Breakdown of functional connectivity appears to occur not just after local injury but also in other conditions that affect large-scale neural communication. SUMMARY: A network perspective is fundamental to appreciating the pathophysiology of brain injury at the systems level and the underlying mechanisms of recovery, and for developing novel strategies of rehabilitation.
PMID: 17992085
ISSN: 1350-7540
CID: 1781282

Type III Neuregulin-1 promotes oligodendrocyte myelination [Meeting Abstract]

Taveggia, C; Thaker, P; Caporas, GL; Toews, A; Einheber, S; Salzer, JL
ISI:000251708800079
ISSN: 1740-925x
CID: 87172