Cortical Thickness and Voxel-Based Morphometry of Classic Motor Regions of Interest in Autism Spectrum Disorder

Duffield, Tyler Cole

01 June 2016

Prior research has suggested that any cortical volume (CV) abnormalities in Autism Spectrum Disorder (ASD) need to be further explored by examination of the two determinants of CV, that being cortical thickness (CT) and pial surface area (PSA; Murphy, Beecham, Craig, & Ecker, 2011). The current study suggests that the two determinants of CV should be explored even in the presence of null CV findings, if structure-function analyses are significant (i.e., bi-lateral precentral gyrus and neuropsychological motor test) as demonstrated in the current sample (see Duffield et al., 2013). The only significant anatomic finding was reduced CT in the left frontal motor regions (primarily left precentral gyrus), which also corresponded to the only significant relationship between a motor variable (i.e., grooved pegboard test) and motor region-of-interest (ROI) where ASD had a stronger relationship than typically developing controls (TDC; ASD > TDC). Left hemisphere biased CT group differences has been shown to have the highest classification accuracy (i.e., designation of ASD versus TDC) of morphological parameters (Ecker et al., 2010), yet PSA has been shown to have far greater modulation of CV abnormalities. This is particularly true for subthreshold PSA (Ecker et al., 2013). These prior findings are not only consistent with the current motor ROI findings, but also provide an explanatory framework for the functional neuroanatomy of a generally worse left handed performance (i.e., non-dominant hand) for ASD compared to controls in a generally right handed dominant sample (no significant group differences on handedness). The only significant motor ROI finding was in the left hemisphere (i.e., ipsilateral to worse left handed performance), but subthreshold PSA findings in the right precentral were found and likely provide explanatory power of motor performances in the aggregate, despite a lack of significant statistical differences in a specific motor ROI individually.

cortical thickness

voxel-based morphometry

motor

autism spectrum disorder

Psychology

Linking structure and function of complex cortical networks

Zamora-López, Gorka

January 2009

The recent discovery of an intricate and nontrivial interaction topology among the elements of a wide range of natural systems has altered the manner we understand complexity. For example, the axonal fibres transmitting electrical information between cortical regions form a network which is neither regular nor completely random. Their structure seems to follow functional principles to balance between segregation (functional specialisation) and integration. Cortical regions are clustered into modules specialised in processing different kinds of information, e.g. visual or auditory. However, in order to generate a global perception of the real world, the brain needs to integrate the distinct types of information. Where this integration happens, nobody knows. We have performed an extensive and detailed graph theoretical analysis of the cortico-cortical organisation in the brain of cats, trying to relate the individual and collective topological properties of the cortical areas to their function. We conclude that the cortex possesses a very rich communication structure, composed of a mixture of parallel and serial processing paths capable of accommodating dynamical processes with a wide variety of time scales. The communication paths between the sensory systems are not random, but largely mediated by a small set of areas. Far from acting as mere transmitters of information, these central areas are densely connected to each other, strongly indicating their functional role as integrators of the multisensory information. In the quest of uncovering the structure-function relationship of cortical networks, the peculiarities of this network have led us to continuously reconsider the stablished graph measures. For example, a normalised formalism to identify the “functional roles” of vertices in networks with community structure is proposed. The tools developed for this purpose open the door to novel community detection techniques which may also characterise the overlap between modules. The concept of integration has been revisited and adapted to the necessities of the network under study. Additionally, analytical and numerical methods have been introduced to facilitate understanding of the complicated statistical interrelations between the distinct network measures. These methods are helpful to construct new significance tests which may help to discriminate the relevant properties of real networks from side-effects of the evolutionary-growth processes. / Die jüngste Entdeckung einer komplexen und nicht-trivialen Interaktionstopologie zwischen den Elementen einer großen Anzahl natürlicher Systeme hat die Art und Weise verändert, wie wir Komplexität verstehen. So bilden zum Beispiel die Nervenfasern, welche Informationen zwischen Regionen des Kortex übermitteln, ein Netzwerk, das weder vollkommen regelmäßig noch völlig zufallig ist. Die Struktur dieser Netzwerke scheint Funktionsprinzipien zu folgen, die ein Gleichgewicht zwischen Segregation (funktionale Spezialisierung) und Integration (Verarbeitung von Informationen) halten. Die Regionen des Kortex sind in Module gegliedert, welche auf die Verarbeitung unterschiedlicher Arten von Informationen, wie beispielsweise Visuelle oder Auditive, spezialisiert sind. Um eine umfassende Vorstellung von der Realität zu erzeugen, muss das Gehirn verschiedene Informationsarten kombinieren (integrieren). Wo diese Integration jedoch geschieht, ist noch ungeklärt. In dieser Dissertation wurde eine weitreichende und detaillierte graphen- theoretische Analyse der kortiko-kortikalen Organisation des Katzengehirns durchgeführt. Dabei wurde der Versuch unternommen, individuelle sowie kollektive topologische Eigenschaften der Kortexareale zu ihrer Funktion in Beziehung zu setzen. Aus der Untersuchung wird geschlussfolgert, dass der Kortex eine äußerst reichhaltige Kommunikationsstruktur aufweist, die aus einer Mischung von parallelen und seriellen übertragungsbahnen besteht, die es ermöglichen dynamische Prozesse auf vielen verschiedenen Zeitskalen zu tragen. Die Kommunikationsbahnen zwischen den sensorischen Systemen sind nicht zufällig verteilt, sondern verlaufen fast alle durch eine geringe Anzahl von Arealen. Diese zentralen Areale agieren nicht allein als übermittler von Informationen. Sie sind dicht untereinander verbunden, was auf ihre Funktion als Integrator hinweist. Bei der Analyse der Struktur-Funktions-Beziehungen kortikaler Netzwerke wurden unter Berucksichtigung der Besonderheiten des untersuchten Netzwerkes die bisher verwandten Graphenmaße überdacht und zum Teil überarbeitet. So wurde beispielsweise ein normalisierter Formalismus vorgeschlagen, um die funktionalen Rollen der Knoten in Netzwerken mit einer Community-Struktur zu identifizieren. Die für diesen Zweck entwickelten Werkzeuge ermöglichen neue Methoden zur Erkennung dieser Strukturen, die möglicherweise auch die überlappung von Modulen beschreiben. Das Konzept der Integration wurde revidiert und den Bedürfnissen des untersuchten Netzwerkes angepasst. Außerdem wurden analytische und numerische Methoden eingeführt, um das Verständnis des komplizierten statistischen Zusammenhangs zwischen den verschiedenen Netzwerkmaßen zu erleichtern. Diese Methoden sind hilfreich für die Konstruktion neuer Signifikanztests, die relevante Eigenschaften realer Netzwerke von Nebeneffekten ihrer evolutionären Wachstumsprozesse unterscheiden können.

komplexe Netzwerke

kortikale Netzwerke

complex networks

cortical networks

Physics

Mitofusin 1 and Mitofusin 2 Function in the Context of Brain Development

Hamze, Carmen

01 November 2011

Mitofusin 1 and 2 are outer-mitochondrial membrane proteins that have been shown to be involved in fusion. Mitofusin 2 has also been associated with apoptosis and development. When Mfn1 and Mfn2 were each conditionally knocked out from the cerebellum, Purkinje cells in Mfn2 deficient cerebellum during development had undergone neurodegeneration. Mutations in Mfn2 have also been associated with the Charcot Marie Tooth Type 2A (CMT2A). We want to asses the effect Mfn2 and Mfn1 might have on the development of other regions of the brain such as the telencephalon. We generated Mfn1 and Mfn2 conditional knockouts in the telencephalon by crossing them with Foxg1 Cre - a cre expressed in the telencephalon. We found that Mfn1 deficient mice have lost their corpus callosum at the midline, but survive over 6 months with a decrease in progenitor cells postnatally. Mfn2 deficient mice die between P9 and P12 with a decrease in progenitor cells postnatally and a decrease in number of neurons in the cortex. Therefore, our results suggest that Mfn1 and Mfn2 play a significant role in the development of the telencephalon.

Mfn1

Mfn2

progenitor cells

post-mitotic cortical neurons

development

telencephalon

Molecular Mechanisms Regulating Embryonic Cerebral Cortex Development

Paquin, Annie

03 March 2010

Cerebral cortex development is a complex process that integrates both extrinsic and intrinsic mechanisms. The surrounding cellular environment triggers receptor activation, which in turn initiates components of different signalling cascades and subsequently gene transcription, influencing cell survival, proliferation, and differentiation. Genetic mutations causing a loss-of-function or gain-of-function of signalling pathways elements can lead to cortical abnormalities and result in cognitive dysfunctions. In this thesis, I examined the receptor tyrosine kinase (RTK) TrkB and TrkC, the small GTPase Ras, and the C/EBP family of transcription factors, investigating their roles during cerebral cortex development. First, I looked at the role of C/EBPs during cortical cell fate determination. I determined that inhibition of C/EBPs decrease neurogenesis, keeping precursors in an undifferentiated state and later promoting their differentiation into astrocytes, while expression of an activated form of C/EBP promoted neurogenesis and reduced astrogenesis. Moreover, the inhibition of MEK, a mediator of C/EBPβ phosphorylation, also caused a decrease in neurogenesis. Thus, activation of the MEK-C/EBP pathway biases precursor cells to become neurons rather than astrocytes, thereby acting as a differentiation switch. Second, I examined the involvement of Trk signalling during cortical development. I showed that genetic knockdown using shRNA, or inhibition using dominant negative of TrkB and TrkC lead to a decrease in proliferation and later to postnatal precursor cells depletion. Moreover, it caused a reduction in number of neurons combined with mislocalization of the generated neurons to the different cortical layers. Thus, Trk signalling plays an essential role in the regulation of cortical precursor cell proliferation and differentiation during embryonic development. Third, I elucidated the effect of Costello syndrome H-Ras mutations during cerebral cortex formation. I determined that these mutations promoted cell proliferation and astrogenesis, while reducing neurogenesis. Together, these data support a model where proper Trks/Ras/MEK/C/EBP signalling is essential for normal genesis of neurons and astrocytes and show that cortical development perturbations can ultimately lead to cognitive dysfunction as seen in Costello syndrome patients.

cerebral cortex development

cellular differentiation

in utero electroporation

cortical precursors

0317

The development of a small animal model for assessing the 3D implications of loading on bone microarchitecture

Britz, Hayley M

09 September 2011

It is well established that bone is capable of adapting to changes in its environment; however, little is known regarding how environmental stimuli, specifically loading, are associated with the internal 3D microarchitecture of cortical bone. The aim of this thesis was to develop a small animal model that can be used to experimentally test hypotheses regarding bone adaptation. High resolution micro-CT was validated and employed as a novel method for the visualization and quantification of rat cortical bone microarchitecture in 3D. The use of this imaging method allowed for the measurement of primary vascular canal orientation in 3D, which had never been achieved before. Using this measure along with an immobilization model for unloading allowed me to test how loading is associated with the orientation of these vascular canals. Normally ambulating rat bones (from 10 female rats) had a canal structure that was 9.9° more longitudinal than their immobilized counterparts. This finding that loading has an effect on primary canal orientation brought to light the need to induce remodeling and therefore, secondary vascular canals, in the rat to increase its novelty as a model for looking at bone adaptation. Remodeling was induced by increasing the calcium demands of female rats, either through a calcium restricted diet (n=2) or pregnancy and lactation coupled with a calcium restricted diet (n=2). Mean cortical thickness for the calcium restricted rats and the pregnant and lactating rats that were on a calcium restricted diet were 622 µm and 419 µm, respectively. The mean BMU count for calcium restricted rats seemed to be higher than that of the pregnant and lactating rats; however, the calcium restricted rats seemed to have a lower BMU density. Once this full-scale study is executed the rat will provide a more representative model for studying human bone adaptation.

calcium

rat

immobilization

micro-CT

cortical bone microarchitecture

The development of a small animal model for assessing the 3D implications of loading on bone microarchitecture

Britz, Hayley M

09 September 2011

It is well established that bone is capable of adapting to changes in its environment; however, little is known regarding how environmental stimuli, specifically loading, are associated with the internal 3D microarchitecture of cortical bone. The aim of this thesis was to develop a small animal model that can be used to experimentally test hypotheses regarding bone adaptation. High resolution micro-CT was validated and employed as a novel method for the visualization and quantification of rat cortical bone microarchitecture in 3D. The use of this imaging method allowed for the measurement of primary vascular canal orientation in 3D, which had never been achieved before. Using this measure along with an immobilization model for unloading allowed me to test how loading is associated with the orientation of these vascular canals. Normally ambulating rat bones (from 10 female rats) had a canal structure that was 9.9° more longitudinal than their immobilized counterparts. This finding that loading has an effect on primary canal orientation brought to light the need to induce remodeling and therefore, secondary vascular canals, in the rat to increase its novelty as a model for looking at bone adaptation. Remodeling was induced by increasing the calcium demands of female rats, either through a calcium restricted diet (n=2) or pregnancy and lactation coupled with a calcium restricted diet (n=2). Mean cortical thickness for the calcium restricted rats and the pregnant and lactating rats that were on a calcium restricted diet were 622 µm and 419 µm, respectively. The mean BMU count for calcium restricted rats seemed to be higher than that of the pregnant and lactating rats; however, the calcium restricted rats seemed to have a lower BMU density. Once this full-scale study is executed the rat will provide a more representative model for studying human bone adaptation.

calcium

rat

immobilization

micro-CT

cortical bone microarchitecture

Molecular Mechanisms Regulating Embryonic Cerebral Cortex Development

Paquin, Annie

03 March 2010

Cerebral cortex development is a complex process that integrates both extrinsic and intrinsic mechanisms. The surrounding cellular environment triggers receptor activation, which in turn initiates components of different signalling cascades and subsequently gene transcription, influencing cell survival, proliferation, and differentiation. Genetic mutations causing a loss-of-function or gain-of-function of signalling pathways elements can lead to cortical abnormalities and result in cognitive dysfunctions. In this thesis, I examined the receptor tyrosine kinase (RTK) TrkB and TrkC, the small GTPase Ras, and the C/EBP family of transcription factors, investigating their roles during cerebral cortex development. First, I looked at the role of C/EBPs during cortical cell fate determination. I determined that inhibition of C/EBPs decrease neurogenesis, keeping precursors in an undifferentiated state and later promoting their differentiation into astrocytes, while expression of an activated form of C/EBP promoted neurogenesis and reduced astrogenesis. Moreover, the inhibition of MEK, a mediator of C/EBPβ phosphorylation, also caused a decrease in neurogenesis. Thus, activation of the MEK-C/EBP pathway biases precursor cells to become neurons rather than astrocytes, thereby acting as a differentiation switch. Second, I examined the involvement of Trk signalling during cortical development. I showed that genetic knockdown using shRNA, or inhibition using dominant negative of TrkB and TrkC lead to a decrease in proliferation and later to postnatal precursor cells depletion. Moreover, it caused a reduction in number of neurons combined with mislocalization of the generated neurons to the different cortical layers. Thus, Trk signalling plays an essential role in the regulation of cortical precursor cell proliferation and differentiation during embryonic development. Third, I elucidated the effect of Costello syndrome H-Ras mutations during cerebral cortex formation. I determined that these mutations promoted cell proliferation and astrogenesis, while reducing neurogenesis. Together, these data support a model where proper Trks/Ras/MEK/C/EBP signalling is essential for normal genesis of neurons and astrocytes and show that cortical development perturbations can ultimately lead to cognitive dysfunction as seen in Costello syndrome patients.

cerebral cortex development

cellular differentiation

in utero electroporation

cortical precursors

0317

Mitofusin 1 and Mitofusin 2 Function in the Context of Brain Development

Hamze, Carmen

01 November 2011

Mitofusin 1 and 2 are outer-mitochondrial membrane proteins that have been shown to be involved in fusion. Mitofusin 2 has also been associated with apoptosis and development. When Mfn1 and Mfn2 were each conditionally knocked out from the cerebellum, Purkinje cells in Mfn2 deficient cerebellum during development had undergone neurodegeneration. Mutations in Mfn2 have also been associated with the Charcot Marie Tooth Type 2A (CMT2A). We want to asses the effect Mfn2 and Mfn1 might have on the development of other regions of the brain such as the telencephalon. We generated Mfn1 and Mfn2 conditional knockouts in the telencephalon by crossing them with Foxg1 Cre - a cre expressed in the telencephalon. We found that Mfn1 deficient mice have lost their corpus callosum at the midline, but survive over 6 months with a decrease in progenitor cells postnatally. Mfn2 deficient mice die between P9 and P12 with a decrease in progenitor cells postnatally and a decrease in number of neurons in the cortex. Therefore, our results suggest that Mfn1 and Mfn2 play a significant role in the development of the telencephalon.

Mfn1

Mfn2

progenitor cells

post-mitotic cortical neurons

development

telencephalon

異方性と損傷を考慮した皮膚骨の非弾性構成式の定式化

岩本, 正実, IWAMOTO, Masami, 田中, 英一, TANAKA, Eiichi, 伝田, 耕平, DENDA, Kohei, 山本, 創太, YAMAMOTO, Sota

05 1900

No description available.

Biomechanics

Constitutive Equation

Anisotropy

Cortical Bone

Damage Mechanics

Approche micromécanique du remodelage osseux

Devulder, Anne

29 June 2009

Dans le cadre de la prédiction du risque fracturaire associée à diverses pathologies, comme l'ostéoporose, cette étude vise à une meilleure compréhension du comportement mécanique de l'os cortical humain, notamment à l'échelle de la microstructure, et, en particulier, du processus biologique de remodelage osseux. Ce phénomène permet, en effet, le renouvellement continuel de la microstructure au cours du temps et contribue ainsi à une diminution de l'endommagement de l'os et, par conséquent, des risques de fracture. Les facteurs déterminants et les conséquences sur les champs mécaniques locaux au sein de la microstructure sont ici recherchés. Une approche couplée, expérimentale et numérique, est proposée. Huit spécimens de fémurs humains, de sexes féminins, âgés de 74 à 101 ans sont analysés. L'analyse expérimentale est réalisée à différentes échelles. A l'échelle macroscopique, le module de Young et les paramètres à la rupture sont déterminés via des essais de compression et les relations potentielles avec les caractéristiques morphométriques, que sont l'âge, la porosité et la densité minérale, sont évaluées. L'analyse de l'évolution des champs de déformations locaux au cours de ces essais de compression et des essais de nanoindentation permet d'accéder à des échelles plus fines (micro- et nanoscopique) afin d'apprécier l'hétérogénéité de la microstructure. On s'intéresse plus particulièrement à l'endommagement de l'os et à l'étape d'initiation de microfissures ainsi qu'à l'hétérogénéité du module de Young. Macroscopiquement, le paramètre le plus influent semble être la porosité. Microscopiquement, les paramètres mécaniques recueillis, notamment les valeurs de déformations pour lesquelles l'os commence à se fissurer, sont intégrés dans les simulations numériques. Un scénario simplifié du remodelage osseux est alors mis en place au sein des microstructures étudiées expérimentalement et, par ailleurs, supposées endommageables. Une loi d'évolution de l'endommagement est introduite et fait l'objet d'un travail d'homogénéisation temporelle afin de considérer l'endommagement par fatigue. Les facteurs d'activation du remodelage et l'évolution des champs mécaniques au cours du processus sont, en particulier, étudiés. L'interaction du phénomène biologique et du comportement mécanique, à l'échelle de l'ostéon, est ainsi mise en évidence.

[SPI] Engineering Sciences

os cortical

remodelage osseux

simulation numérique du remodelage