Diffusion MRI Anisotropy in the Cerebral Cortex is Determined by Unmyelinated Tissue Features

The diffusion of water molecules through the brain is constrained by tissue and cellular substructure, which imposes an anisotropy that can be measured through diffusion magnetic resonance imaging (dMRI). In the white matter, myelinated axons strongly shape diffusion anisotropy; however, in gray matter the determinants of dMRI signals remain poorly understood. Here we investigated the histological tissue properties underlying dMRI anisotropy and diffusivity in the cerebral cortex of the marmoset monkey. We acquired whole brain ex vivo dMRI data designed for high signal-to-noise at ultra-high (150μm) resolution. We compared the MRI to myelin- and Nissl-stained histological sections obtained from the scanned brain. We found that dMRI anisotropy corresponds most strongly not with cortical myelin content, but rather with the microscale anisotropy of tissue features, most notably those unmyelinated features highlighted by Nissl staining. The results suggest that dMRI anisotropy in gray matter derives from the organization of unmyelinated neurites, which are known to be affected by neurodegenerative diseases.

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Diffusion tensor imaging analysis of the brain in the canine model of Krabbe disease

The Neuroradiology Journal ◽

10.1177/1971400916665378 ◽

2016 ◽

Vol 29 (6) ◽

pp. 417-424 ◽

Cited By ~ 6

Author(s):

Allison Bradbury ◽

David Peterson ◽

Charles Vite ◽

Steven Chen ◽

N Matthew Ellinwood ◽

...

Keyword(s):

Diffusion Tensor Imaging ◽

White Matter ◽

Mr Imaging ◽

Gray Matter ◽

Diffusion Tensor ◽

Ex Vivo ◽

Small Animal ◽

Krabbe Disease ◽

Adc Values ◽

The Brain

Purpose The goal of this study was to compare the diffusion tensor imaging (DTI) metrics from an end-stage canine Krabbe brain evaluated by MR imaging ex vivo to those of a normal dog brain. We hypothesized that the white matter of the canine Krabbe brain would show decreased fractional anisotropy (FA) values and increased apparent diffusion coefficient (ADC) and radial diffusivity (RD) values. Methods An 11-week-old Krabbe dog was euthanized after disease progression. The brain was removed and was placed in a solution of 10% formalin. MR imaging was performed and compared to the brain images of a normal dog that was similarly fixed post-mortem. Both brains were scanned using similar protocols on a 7 T small-animal MRI system. For each brain, maps of ADC, FA, and RD were calculated for 11 white-matter regions and five control gray-matter regions. Results Large decreases in FA values, increases in ADC values, and increases in RD (consistent with demyelination) values, were seen in white matter of the Krabbe brain but not gray matter. ADC values in gray matter of the Krabbe brain were decreased by approximately 29% but increased by approximately 3.6% in white matter of the Krabbe brain. FA values in gray matter were decreased by approximately 3.3% but decreased by approximately 29% in white matter. RD values were decreased by approximately 27.2% in gray matter but increased by approximately 20% in white matter. Conclusion We found substantial abnormalities of FA, ADC, and RD values in an ex vivo canine Krabbe brain.

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Glutamatergic and GABAergic TCA Cycle and Neurotransmitter Cycling Fluxes in Different Regions of Mouse Brain

Journal of Cerebral Blood Flow & Metabolism ◽

10.1038/jcbfm.2013.114 ◽

2013 ◽

Vol 33 (10) ◽

pp. 1523-1531 ◽

Cited By ~ 31

Author(s):

Vivek Tiwari ◽

Susmitha Ambadipudi ◽

Anant B Patel

Keyword(s):

Cerebral Cortex ◽

Mouse Brain ◽

Ex Vivo ◽

Tca Cycle ◽

Metabolic Model ◽

Nmr Studies ◽

Inhibitory Function ◽

The Tca Cycle ◽

The Brain ◽

C Nmr

The 13C nuclear magnetic resonance (NMR) studies together with the infusion of 13C-labeled substrates in rats and humans have provided important insight into brain energy metabolism. In the present study, we have extended a three-compartment metabolic model in mouse to investigate glutamatergic and GABAergic tricarboxylic acid (TCA) cycle and neurotransmitter cycle fluxes across different regions of the brain. The 13C turnover of amino acids from [1,6-13C2]glucose was monitored ex vivo using qH-[13C]-NMR spectroscopy. The astroglial glutamate pool size, one of the important parameters of the model, was estimated by a short infusion of [2-13C]acetate. The ratio Vcyc/VTCA was calculated from the steady-state acetate experiment. The 13C turnover curves of [4-13C]/[3-13C]glutamate, [4-13C]glutamine, [2-13C]/[3-13C]GABA, and [3-13C]aspartate from [1,6-13C2]glucose were analyzed using a three-compartment metabolic model to estimate the rates of the TCA cycle and neurotransmitter cycle associated with glutamatergic and GABAergic neurons. The glutamatergic TCA cycle rate was found to be highest in the cerebral cortex (0.91±0.05 μmol/g per minute) and least in the hippocampal region (0.64±0.07 μmol/g per minute) of the mouse brain. In contrast, the GABAergic TCA cycle flux was found to be highest in the thalamus-hypothalamus (0.28±0.01 μmol/g per minute) and least in the cerebral cortex (0.24±0.02 μmol/g per minute). These findings indicate that the energetics of excitatory and inhibitory function is distinct across the mouse brain.

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Volumetric Alterations of the Cerebral Cortex in Eating Disorders

Journal of Clinical Medicine ◽

10.3390/jcm10235480 ◽

2021 ◽

Vol 10 (23) ◽

pp. 5480

Author(s):

Laura Vidal ◽

Miguel A Ortega ◽

Miguel Angel Alvarez-Mon ◽

Melchor Álvarez-Mon ◽

Guillermo Lahera

Keyword(s):

Eating Disorders ◽

Cerebral Cortex ◽

Eating Disorder ◽

Binge Eating ◽

Cortical Thickness ◽

Gray Matter ◽

Binge Eating Disorder ◽

Gray Matter Volume ◽

The Right ◽

The Brain

Eating disorders are relatively frequent psychiatric disorders that can produce serious consequences at the brain level. In an effort to clarify the neurobiological mechanisms of their pathogenesis, some studies have suggested the existence of modifications of the cortical architecture in eating disorders, but it is unknown whether the alterations described are a cause or consequence of eating disorders. The main objective of this systematic review is to collect the evidence available about the volumetric alterations of the cerebral cortex in eating disorders in adults and their apparent relationship with the pathogenesis of the disease. Initially, 91 articles were found by a search that included the terms anorexia nervosa (AN), bulimia nervosa (BN), binge eating disorder, gray matter, cortical thickness (CT), and brain volume. To pare down the articles, the following inclusion criteria were applied: (1) cortical thickness and/or gray matter volume (GMV) in patients with anorexia, bulimia nervosa, or binge-eating disorder was the main measure of the study; and (2) the sample was adult patients aged 18–65. The exclusion criteria were as follows: (1) articles that did not analyze cortical thickness or gray matter volume; (2) studies with patients with comorbidities; and (3) studies in patients who did not meet the DSM-IV/DSM-V criteria. In the first phase of selection, we proceeded to read the titles and abstracts as a first screen, thereby excluding 62 studies, followed by a complete critical reading of the 29 remaining articles. In this last phase, nine studies were excluded because they did not specify the eating disorder subtype, they included adolescents, or they did not measure GMV or CT. Finally, after the above systematic selection process, 20 articles were included in this review. Despite the methodological heterogeneity of the studies, there was some agreement between them. They showed an overall reduction in GMV in eating disorders, as well as alterations in certain regions of the cerebral cortex. Some of the most often mentioned cortical areas were the frontal, cingulate, and right orbitofrontal cortices, the precuneus, the right insula, and some temporoparietal gyri in cases of AN, with greater cortical involvement in frontotemporal and medial orbitofrontal regions in BN and binge eating disorder. Likewise, certain cortical regions, such as the left inferior frontal gyrus, the precuneus, the right superior motor area, the cingulate cortex, the insula, and the medial orbitofrontal sulcus, often remained altered after recovery from AN, making them potential cortical areas involved in the etiopathogenesis of AN. A reduction in GMV in specific areas of the CNS can inform us about the neurobiological mechanisms that underlie eating disorders as well as give us a better understanding of their possible consequences at the brain level.

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Differences in the molecular structure of the blood-brain barrier in the cerebral cortex and white matter: an in silico, in vitro, and ex vivo study

AJP Heart and Circulatory Physiology ◽

10.1152/ajpheart.00774.2015 ◽

2016 ◽

Vol 310 (11) ◽

pp. H1702-H1714 ◽

Cited By ~ 19

Author(s):

Ádám Nyúl-Tóth ◽

Maria Suciu ◽

Judit Molnár ◽

Csilla Fazakas ◽

János Haskó ◽

...

Keyword(s):

Endothelial Cells ◽

Cerebral Cortex ◽

White Matter ◽

Blood Brain Barrier ◽

In Silico ◽

Grey Matter ◽

Ex Vivo ◽

Cortical Grey Matter ◽

The Brain

The blood-brain barrier (BBB) is the main interface controlling molecular and cellular traffic between the central nervous system (CNS) and the periphery. It consists of cerebral endothelial cells (CECs) interconnected by continuous tight junctions, and closely associated pericytes and astrocytes. Different parts of the CNS have diverse functions and structures and may be subject of different pathologies, in which the BBB is actively involved. It is largely unknown, however, what are the cellular and molecular differences of the BBB in different regions of the brain. Using in silico, in vitro, and ex vivo techniques we compared the expression of BBB-associated genes and proteins (i.e., markers of CECs, brain pericytes, and astrocytes) in the cortical grey matter and white matter. In silico human database analysis (obtained from recalculated data of the Allen Brain Atlas), qPCR, Western blot, and immunofluorescence studies on porcine and mouse brain tissue indicated an increased expression of glial fibrillary acidic protein in astrocytes in the white matter compared with the grey matter. We have also found increased expression of genes of the junctional complex of CECs (occludin, claudin-5, and α-catenin) in the white matter compared with the cerebral cortex. Accordingly, occludin, claudin-5, and α-catenin proteins showed increased expression in CECs of the white matter compared with endothelial cells of the cortical grey matter. In parallel, barrier properties of white matter CECs were superior as well. These differences might be important in the pathogenesis of diseases differently affecting distinct regions of the brain.

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Biochemische Untersuchungen an experimentell chronisch epileptischen Tieren / Biochemical Investigations of Experimental Chronic Epileptic Animals

Zeitschrift für Naturforschung B ◽

10.1515/znb-1971-1116 ◽

1971 ◽

Vol 26 (11) ◽

pp. 1158-1167 ◽

Cited By ~ 2

Author(s):

Eberhard Riedel ◽

Eugen Wamsiedler

Keyword(s):

Cerebral Cortex ◽

Gray Matter ◽

Brain Metabolism ◽

Tissue Respiration ◽

Good Reproducibility ◽

Chronic Epilepsy ◽

Alumina Gel ◽

Gel Injection ◽

The Brain

In the brain-metabolism of experimental chronic epileptic cats (modificated Kopeloffmethod of intracerebrale alumina-gel injection) some alterations were observed in the lesioned cortical hemisphere. An increase of tissue-respiration in vitro (gray-matter of the cerebral cortex), increase of the activities of alkaline (E.C. 3.1.3.1) and acid phosphomonoesterases (E.C. 3.1.3.2) and a decrease of K-Na-stimulated, Ouabain-inhibited adenosintriphosphatase (E.C. 3.6.1.3) were determined. Postconvulsive (one to six hours after seizures) these changes were found to be more extensive than one or more days after discharge. They couldn’t be found in brain tissues of cats only with mechanical lesions without injection of aluminagel2 which didn’t have convulsions. Because the good reproducibility the communicated method for experimental chronic epilepsy is proposed for pharmacological investigations.

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Glucuronyl 3-sulfate occurs exclusively on distal unmyelinated terminals of selected sensory neurons in the peripheral nervous system

Proceedings, annual meeting, Electron Microscopy Society of America ◽

10.1017/s0424820100141160 ◽

1995 ◽

Vol 53 ◽

pp. 958-959

Author(s):

S.S. Spicer ◽

B.A. Schulte

Keyword(s):

Central Nervous System ◽

Nervous System ◽

Cerebral Cortex ◽

Peripheral Nervous System ◽

Sensory Neurons ◽

Sensory Nerves ◽

Tissue Antigens ◽

The Central Nervous System ◽

The Brain ◽

Leu 7

Generation of monoclonal antibodies (MAbs) against tissue antigens has yielded several (VC1.1, HNK- 1, L2, 4F4 and anti-leu 7) which recognize the unique sugar epitope, glucuronyl 3-sulfate (Glc A3- SO4). In the central nervous system, these MAbs have demonstrated Glc A3-SO4 at the surface of neurons in the cerebral cortex, the cerebellum, the retina and other widespread regions of the brain.Here we describe the distribution of Glc A3-SO4 in the peripheral nervous system as determined by immunostaining with a MAb (VC 1.1) developed against antigen in the cat visual cortex. Outside the central nervous system, immunoreactivity was observed only in peripheral terminals of selected sensory nerves conducting transduction signals for touch, hearing, balance and taste. On the glassy membrane of the sinus hair in murine nasal skin, just deep to the ringwurt, VC 1.1 delineated an intensely stained, plaque-like area (Fig. 1). This previously unrecognized structure of the nasal vibrissae presumably serves as a tactile end organ and to our knowledge is not demonstrable by means other than its selective immunopositivity with VC1.1 and its appearance as a densely fibrillar area in H&E stained sections.

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Neurotransmitter systems of female mouse brain during growth of malignant melanoma modeled on the background of chronic pain

Nauchno-prakticheskii zhurnal «Patogenez» ◽

10.25557/gm.2018.4.9749 ◽

2018 ◽

pp. 49-55

Author(s):

О.И. Кит ◽

И.М. Котиева ◽

Е.М. Франциянц ◽

И.В. Каплиева ◽

Л.К. Трепитаки ◽

...

Keyword(s):

Chronic Pain ◽

Cerebral Cortex ◽

Malignant Melanoma ◽

Sciatic Nerve ◽

Female Mouse ◽

Combined Effects ◽

Malignant Growth ◽

Course Of Disease ◽

The Brain ◽

Melanoma Growth

Известно, что биогенные амины (БА) участвуют в злокачественном росте, их уровень изменяется в ЦНС при болевом воздействии, однако исследований о сочетанном влиянии хронической боли (ХБ) и онкопатологии на динамику БА в головном мозге не проводилось. Цель: изучить особенности баланса БА в коре головного мозга в динамике роста меланомы, воспроизведенной на фоне ХБ. Материалы и методы. Работа выполнена на 64 мышах-самках, весом 21-22 г. Животным основной группы меланому В16/F10 перевивали под кожу спины через 2 недели после перевязки седалищных нервов. Группой сравнения служили мыши с меланомой без боли. Уровни БА: адреналина, норадреналина, дофамина (ДА), серотонина (5-НТ), гистамина, а также 5-ОИУК определяли методом иммуноферментного анализа. Результаты. У мышей с ХБ уменьшается содержание большинства БА, однако уровень ДА не изменяется. Метаболизм 5-НТ происходит с участием МАО. Развитие меланомы сопровождается увеличением содержания ДА и 5-НТ, тогда как МАО - ингибируется. Направленность сдвигов БА при развитии меланомы на фоне ХБ оказалась практически такой же, как и без неё. В то же время ХБ ограничивает накопление 5-НТ в коре мозга при меланоме, что сопровождается более агрессивным её течением. Выводы. ХБ ограничивает включение стресс-лимитирующих механизмов в головном мозге при развитии меланомы у мышей, что приводит к более агрессивному течению злокачественного процесса. Biogenic amines (BA) are known to be involved in malignant growth, and their CNS levels change in pain; however, there are no studies of combined effects of chronic pain (CP) and cancer on BA dynamics in the brain. Aim: To study features of BA balance in the cerebral cortex during melanoma growth associated with CP. Material and methods. The study included 64 female mice weighing 21-22 g. In the main groups, B16/F10 melanoma was transplanted under the skin of the back two weeks following sciatic nerve ligation. Mice with melanoma without pain were used as the control. Concentrations of BA: adrenaline, noradrenaline, dopamine (DA), serotonin (5-HT), histamine and 5-HIAA were measured with ELISA. Results. Concentrations of BAs decreased in mice with CP although DA levels did not change. 5-HT metabolism involved MAO. The development of melanoma was accompanied by increases in DA and 5-HT whereas MAO was inhibited. The direction of BA changes during the development of melanoma was the same with and without CP. At the same time, CP with melanoma limited accumulation of 5-HT in the cerebral cortex, which resulted in even more aggressive course of cancer. Conclusion. CP restricted the activation of cerebral stress-limiting mechanisms during the development of melanoma in mice, which resulted in a more aggressive course of disease.

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