Sound Production in Two Loricariid Catfishes

Webb, Amanda Lynn

01 August 2011

Many families of catfish produce sounds via pectoral spine stridulation and/or swim bladder compression using sonic muscles attached to the swim bladder. The sound production capabilities and characteristics in Loricariidae, the largest catfish family, have not been well examined. Sounds produced by two loricariid catfish species, Macrotocinclus affinis and Pterygoplichthys gibbiceps were recorded. Both species produce broad band calls via pectoral spine stridulation. These species produce sounds by rubbing the ridges of the dorsal process of the pectoral spine base against the groove of the pectoral girdle. Call duration was generally shorter in M. affinis (2-15 ms) as opposed to those produced by P. gibbiceps (20-200 ms). Mean dominant frequencies were approximately 4000 Hz for M. affinis and 1000 (abduction) and 4500 Hz (adduction) for P. gibbiceps. Light and scanning electron microscopy were used to examine the dorsal process of the pectoral spines from the largest and smallest M. affinis, and from a wide range of sizes from P. gibbiceps. Mean distances between dorsal process ridges of M. affinis and P. gibbicepswere approximately 50 and 160 microns, respectively. For P. gibbiceps, dominant frequency was an inverse function of total length and inter-ridge distance.

pectoral spine stridulation

bioacoustics

dominant frequency

dorsal process

inter-ridge distance

Pterygoplichthya gibbiceps

macrotocinclus affinis

Biology, general

Structural Biology

Συγκριτική μελέτη των φαρμακολογικών ιδιοτήτων του συμπλόκου του υποδοχέα GABAA/Βενζοδιαζεπινών μεταξύ του διαφραγματικού και κροταφικού ιπποκάμπου επίμυος

Σαράντης, Κωνσταντίνος

30 July 2007

Η ΒΥΠ διαθέτει αντίτυπο της διατριβής σε έντυπη μορφή στο βιβλιοστάσιο διδακτορικών διατριβών που βρίσκεται στο ισόγειο του κτιρίου της. / Ο ιππόκαμπος στον αρουραίο είναι μια δομή σε C-σχήμα που εκτείνεται από τον διαφραγματικό πυρήνα προσθιοραχιαία έως τον κροταφικό λοβό οπισθιοκοιλιακά. Παρόλο που από παλιά θεωρείτο ως ομοιογενής δομή, έχουν παρατηρηθεί πολλές διαφορές σε όλα τα επίπεδα οργάνωσης μεταξύ του διαφραγματικού και του κροταφικού ιππόκαμπου. Οι βενζοδιαζεπίνες δρουν στις θέσεις δέσμευσης των βενζοδιαζεπινών, οι οποίες είναι αλλοστερικά συνδεδεμένες με το σύμπλοκο του GABAA, όπου ενισχύουν την δράση του GABA στους GABAA υποδοχείς, αυξάνοντας τη συχνότητα ανοίγματος του διαύλου των ιόντων χλωρίου (Cl-) και έχοντας μικρή μόνο επίδραση στο χρόνο ανοίγματος ή στην αγωγιμότητα του διαύλου. Προηγούμενη μελέτη υποδεικνύει ότι η έκφραση των α1-, β2- και γ2-υπομονάδων ήταν μικρότερη, ενώ αντίθετα η έκφραση των α2-, α5- και β1-υπομονάδων ήταν μεγαλύτερη στον κροταφικό ιπποκάμπο σε σύγκριση με τον διαφραγματικό ιππόκαμπο. Σύμφωνα με προηγούμενες μελέτες που αφορούν την συνέκφραση των υπομονάδων στο σύμπλοκο του GABAA υποδοχέα τα αποτελέσματα μας υποδηλώνουν ότι ο α1β2-υποτύπος του GABAA υποδοχέα επικρατεί στον διαφραγματικό ιππόκαμπο (ΔΙ), ενώ ο α2β1-υπότυπος κυριαρχεί στον κροταφικό ιππόκαμπο (ΚΙ). Επιπλέον, φαρμακολογικές μελέτες έχουν δείξει ότι η καταπραϋντική δράση της diazepam πραγματοποιείται μέσω των GABAA υποδοχέων, που περιέχουν την α1-υπομονάδα, ενώ η αγχολυτική δράση της πραγματοποιείται μέσω των υποδοχέων που φέρουν την α2-υπομονάδα. Επομένως, η μελέτη των φαρμακολογικών ιδιοτήτων των υποτύπων του GABAΑ υποδοχέα δίνει την δυνατότητα στο να σχεδιαστούν ειδικά φάρμακα τα οποία θα βελτιώνουν το κλινικό προφίλ ασθενειών, όπως το άγχος, η αϋπνία ή η επιληψία, δρώντας σε εξειδικευμένους υποτύπους του GABAΑ υποδοχέα. Ο στόχος της συγκεκριμένης εργασίας ήταν να μελετηθούν οι φαρμακολογικές ιδιότητες των υποτύπων του συμπλόκου του GABAA υποδοχέα/βενζοδιαζεπινών στον διαφραγματικό σε σύγκριση με τον κροταφικό ιππόκαμπο επίμυος. Έτσι, για τη μελέτη των θέσεων δέσμευσης των βενζοδιαζεπινών μεταξύ του διαφραγματικού και κροταφικού ιπποκάμπου χρησιμοποιήθηκε ο ευρέως φάσματος αγωνιστής των θέσεων δέσμευσης των βενζοδιαζεπινών, [3H]-flunitrazepam, σε μια αυτοραδιογραφική μελέτη. Επιπλέον, χρησιμοποιήθηκαν εξειδικευμένα φάρμακα, που δεσμεύονται σε συγκεριμένους υποτύπους του GABAA υποδοχέα, όπως το zolpidem (ειδικός αγωνιστής των GABAA υποδοχέων, που περιέχουν την α1-υπομονάδα), το etomidate (ειδικός θετικός αλλοστερικός ρυθμιστής των GABAA υποδοχέων, που περιέχουν τη β2-υπομονάδα) και το L-655,708 (ειδικός αντίστροφος αγωνιστής των GABAA υποδοχέων, που περιεχούν την α5-υπομονάδα) σε μια αυτοραδιγραφική κινητική μελέτη. Τα αποτελέσματα μας έδειξαν ότι οι τομές που προέρχονταν από τον ΚΙ συγκρινόμενες με αυτές από τον ΔΙ είχαν: Α) μειωμένη δέσμευση της [3H]-flunitrazepam στις CA1, CA3 και DG περιοχές, Β) μικρότερη χημική συγγένεια της δέσμευση της [3H]-flunitrazepam στη CA1 περιοχή, Γ) καμία διαφορά στον αριθμό των θέσεων δέσμευσης, Δ) μεγαλύτερες τιμές IC50 και EC50 για το zolpidem και το etomidate, αντίστοιχα και Ε) μικρότερες τιμές IC50 για το L-655,708. Συμπερασματικά, τα αποτελέσματά μας υποδεικνύουν διαφορετικές φαραμκολογικές ιδιότητες των υποτύπων του GABAΑ/ΒΖ υποδοχέα μεταξύ του ΔΙ και ΚΙ, ενώ επιβεβαιώνεται και ενισχύεται προηγούμενη μελέτη που υποδηλώνει ότι ο α1β2-υποτύπος του GABAA υποδοχέα επικρατεί στον διαφραγματικό ιππόκαμπο (ΔΙ), ενώ ο α2β1-υπότυπος κυριαρχεί στον κροταφικό ιππόκαμπο (ΚΙ). Η μελέτη αυτή είναι πιθανό να τυγχάνει ιδιαίτερης κλινικής αξίας, στην κατεύθυνση της ακριβέστερης ρύθμισης των αποτελεσματικών δόσεων των διάφορων μορίων που δρουν στις θέσεις δέσμευσης των βενζοδιαζεπινών των α1- και α2-υποτύπων του GABAA υποδοχέα. / The hippocampus in the rat appears grossly as an elongated structure with its long axis bending in a C-shaped manner from the septal nuclei rostrodorsally to the incipient temporal lobe caudoventrally. The long axis of the hippocampal formation is referred as the dorsoventral axis. Although hippocampus has been traditionally thought as a homogeneous structure, several studies have been demonstrated differences at several organization levels (from the behavioural to the cellular) between its dorsal (DH) and ventral (VH) pole. Pharmacological studies have shown that the α1-GABAA receptor subtype is associated with the sedative and anticonvulsant effects of benzodiazepines (BZs), whereas the α2-subtype is associated with the anxiolytic effects of BZs. Recent data have demonstrated a differential distribution of the GABAA receptor subunits between DH and VH, with the α1/β2 GABAA receptor subtype dominating in the DH and the α2/β1 subtype prevailing in the VH. We therefore study possible differences in the pharmacological properties and receptor binding parameters of the GABAA/BZ receptor subtypes between DH and VH, by examining: 1a) the specific binding of [3H]-flunitrazepam (BZ sites agonist), by using quantitative autoradiography, b) the kinetic parameters of [3H]-flunitrazepam specific binding, by using the “wipe off” technique and 2) the competitive displacement of [3H]-flunitrazepam binding by using zolpidem (a specific agonist of α1-subtype) and L-655,708 (a specific inverse agonist of α5-subtype) and the enhancement of [3H]-flunitrazepam binding by using etomidate (a selective positive modulator of β2- subunit), in an autoradiographical saturation kinetic study. Our results showed in VH compared to the DH: A) lower level of [3H]-flunitrazepam binding in CA1, CA3 and DG regions, B) higher KD value for [3H]-flunitrazepam specific binding in CA1 region and no differences in the Bmax value, C) higher IC50 and EC50 values for zolpidem and etomidate, respectively and D) lower IC50 values for L-655,708. In conclusion, the lower affinity of GABAA receptors for [3H]-flunitrazepam binding, the higher IC50 and EC50 values for zolpidem and etomidate, respectively, as well as the lower IC50 values for L-655,708 observed in VH compared to DH, support the evidence that the α1/β2-GABAA receptor subtype dominates in DH and the α2/β1-subtype prevails in VH and suggest differential pharmacological effects of the benzodiazepines in DH compared to VH, which could be of clinical relevence for the more accuate adjustment of the effective dose of α1- and α2-subtype specific BZ binding sites’ ligands.

GABAA

Υπότυποι

Βενζοδιαζεπίνες

Zolpidem

Etomidate

L-655,708

612.825

Dorsal hippocampus

Ventral hippocampus

GABAA

Subtypes

Benzodiazepines

Zolpidem

Etomidate

L-655,708

The effect of long-term interleukin-1 beta exposure on sensory neuron electrical membrane properties: implications for neuropathic pain

Stemkowski, Patrick

Unknown Date

No description available.

sensory neurons

dorsal root ganglion

interleukin-1 beta

neuropathic pain

electrophysiology

cell culture

excitability

ion channels

peripheral nerve injury

central sensitization

Aspects spatial et temporel de l'intégration visuelle au niveau de la voie dorsale du système visuel du chat : le cortex suprasylvien latéral comme modèle

Ouellette, Brian G.

January 2008

Thèse numérisée par la Division de la gestion de documents et des archives de l'Université de Montréal

Mouvement

Movement

Vision

Électrophysiologie

Electrophysiology

Hiérarchie corticale

Cortical hierarchy

Chat

Cat

Voie dorsale

Dorsal stream

PMLS

Latence

Latency

Lésion

Lesion

Profils spatio-temporel

Spatio-temporal profiles

Pesquisa etiológica da Miopatia Dorsal Cranial em frangos de corte

Zimermann, Francielli Cordeiro

January 2011

A indústria avícola brasileira representa uma atividade econômica muito importante para o país. Recentemente, uma lesão muscular localizada cranialmente no dorso de frangos de corte, vem causando grandes perdas econômicas devido à condenação de carcaças. Machos de linhagens pesadas, com as maiores médias de peso e idade de abate apresentam as maiores freqüências de condenação devido à referida lesão. As lesões são caracterizadas por amarelamento e inchaço da pele que recobre o músculo lesado. Após abertura da pele, pode-se notar edema subcutâneo, hemorragia muscular superficial, palidez, aderência, aumento da espessura e consistência envolvendo sempre o músculo anterior latissimus dorsi. Histologicamente a lesão é polifásica e inclui variação no tamanho e partição das fibras (splitting), degeneração hialina, necrose, regeneração e intensa fibrose com presença de adipócitos e infiltrado linfohistiocitário. A etiologia desta miopatia é desconhecida e não há publicações detalhadas a respeito na literatura consultada. Os objetivos do presente trabalho foram detectar a etiologia da miopatia dorsal cranial através da realização de alguns experimentos, bem como, verificar se a lesão apresenta um potencial risco à saúde pública Para atender esses objetivos foram conduzidos experimentos de avaliação da associação entre a miopatia dorsal cranial e a síndrome ascítica; de ausência de inclusão de vitamina E e selênio na dieta de frangos de corte na tentativa de reproduzir a lesão; quantificação de vitamina E (alfa tocoferol) e selênio em músculos lesados e músculos normais; avaliação do papel do exercício na indução da miopatia dorsal cranial bem como sua associação com a miopatia peitoral profunda e também foram realizadas pesquisas de bactérias de interesse em saúde pública em músculos com lesão. Não há risco de intoxicação através do consumo do músculo Anterior latissimus dorsi lesado ou normal em relação às bactérias Sthaphylococcus aureus, Escherichia coli, Salmonella enteritidis Enteritidis, Listeria monocytogenes, Pasteurella multocida, Yersinia enterocolitica, Campylobacter coli e Campylobacter jejuni subsp. jejuni. Os níveis médios de alfa tocoferol e selênio nos músculos anterior latissimus dorsi lesados ou normais são compatíveis com os níveis de carcaças usualmente suplementadas. Músculos com lesão apresentaram níveis mais elevados de selênio do que músculos sem lesão. Pode-se constatar também, a ausência de associações entre a miopatia dorsal cranial e a síndrome ascítica, bem como, à miopatia peitoral profunda. O protocolo de exercício que induziu à frequências altas (96,9%) de miopatia peitoral profunda não reproduziu à miopatia dorsal cranial. A causa ou as causas da miopatia dorsal cranial não puderam ser esclarecidas com base nos experimentos realizados, porém os mesmos permitem concluir que e a ingestão de baixos níveis de vitamina E não está envolvida na etiologia desta miopatia. / The Brazilian poultry industry is a very important economic activity to this country. Recently, a dorsal cranial muscular lesion has been occurring in increasing frequency in broilers causing heavy economic losses due to downgrading of carcasses. Males of heavy strains with higher average weight at slaughter had the highest frequency of downgrading due to this lesion. Gross lesions are characterized by yellowish discoloration of the skin and swelling on the dorsal cranial region. When the skin is sectioned, subcutaneous edema, muscular superficial hemorrhage, pallor, adherence, increased thickness and density involving always the anterior latissimus dorsi muscle are seen. Microscopical features include a polyphasic lesion with size variation and fiber splitting, hyaline, necrotic, regenerating fibers and extensive fibrosis and adipose tissue. Lymphohistiocytic infiltration is seen. The etiology of this myopathy is unknown and no detailed report is available in the world literature. The aims of this study were to detect the etiology of the dorsal cranial myopathy by some experiments, as well as to verify if this lesion may pose a potential public health risk. One experiment was designed to assess the association between dorsal cranial myopathy and ascitic syndrome; other experiment attempt to reproduce the lesion with the lack of inclusion of vitamin E and selenium in the diet of broiler chickens; other study was the quantification of vitamin E (alpha tocopherol) and selenium in injured and normal muscles; the evaluation of the role of exercise in inducing the dorsal cranial myopathy and its association with the deep pectoral myopathy; and microbiological studies were done to clarify if infectious agents are present in the affected muscles. There is no risk of poisoning through the consumption of the injured or normal anterior latissimus dorsi muscle in relation to the bacteria Staphylococcus aureus, Escherichia coli, Salmonella enteritidis Enteritidis, Listeria monocytogenes, Pasteurella multocida, Yersinia enterocolitica, Campylobacter coli e Campylobacter jejuni subsp. jejuni. Average levels of alpha tocopherol and selenium in the damaged or normal anterior latissimus dorsi muscle are consistent with carcasses usually supplemented. Injured muscles showed higher levels of selenium than uninjured muscles. The absence of associations between dorsal cranial myopathy and ascitic syndrome, as well as the deep pectoral myopathy was observed. The exercise protocol that induced a high frequency (96.9%) of deep pectoral myopathy did not reproduce the dorsal cranial myopathy. The cause or causes of dorsal cranial myopathy could not be clarified based on these experiments, but is possible to conclude that low intake of vitamin E is not involved in the etiology of this myopathy.

Imunologia veterinaria

Síndrome Ascítica : Aves

Vitamina E

Selenio

Anterior latissimus dorsi muscle

Ascitic syndrome

Exercise

Deep pectoral myopathy

Vitamin E and selenium and public health

Reversão dos efeitos reforçadores da morfina através do prejuízo da reconsolidação da memória do condicionamento de preferência por local e da sensibilização locomotora

Boos, Flávia Zacouteguy

January 2016

A dependência de drogas é um transtorno multifatorial complexo que se desenvolve em uma minoria de indivíduos que fazem uso dessas substâncias. Memórias associativas entre a droga e o contexto funcionam como gatilho para disparar comportamentos não adaptativos de busca e consumo, além de recaídas após períodos de abstinência. Subjacentes a essas mudanças comportamentais, existem modificações nas subunidades de receptores glutamatérgicos do tipo AMPA em estruturas envolvidas com memória (Hipocampo) e recompensa (Núcleo Accumbens). Por isso, estratégias que enfraqueçam a associação do contexto com a droga e que aprofundem o conhecimento dos circuitos envolvidos nesses comportamentos são de extrema relevância terapêutica. A memória quando evocada pode passar por dois processos pós-evocação: a extinção, em que uma nova memória é formada inibindo uma prévia associação, e a reconsolidação, em que a memória original entra em um estado lábil e suscetível a modificações, em que é possível enfraquecê-la através da inibição de sua reconsolidação. A reconsolidação da memória mostra-se uma estratégica mais eficaz e duradoura em relação à extinção, já que a memória original é modificada. Como modelo animal para o estudo da memória na dependência de drogas, o condicionamento de preferência por local (CPL) é bastante utilizado e sabe-se que é possível enfraquecer a preferência através do bloqueio da reconsolidação. Porém, são escassos os estudos que investigaram a existência da reconsolidação no modelo de sensibilização locomotora, que parece ocorrer, na maioria dos casos, em condição dependente do contexto de aquisição do comportamento, embora existam exemplos que demonstrem sua independência. As questões a serem respondidas neste trabalho são (a) se é possível reverter conjuntamente a preferência por local e a sensibilização locomotora à morfina (5 mg/kg) em ratos Wistar adultos machos, inibindo-se a síntese proteica com cicloheximida (CHX) i.p. logo após uma sessão de reativação contextual da memória no CPL, (b) se a reversão dos comportamentos reflete alterações (já descritas por outros autores) em GluA1, GluA1p (Ser845) e GluA2, no Hipocampo dorsal (HPCd) e no Núcleo Accumbens (NAc), e (c) se o mesmo tratamento em ambas estruturas reverte os dois parâmetros avaliados – comportamental e neuroquímico – de forma diferente ou igual. Nossos resultados mostraram ser possível reverter a preferência por local e a sensibilização locomotora por inibição sistêmica de síntese proteica, e que o condicionamento com exposição à morfina induz alterações nas subunidades analisadas de AMPA, conforme verificado no HPCd e NAc, embora a CHX não tenha produzido um efeito tão bem definido. Os animais que receberam infusões centrais no HPCd e NAc (central) não exibiram preferência por local, nem sensibilização. Em conjunto, nossos resultados mostraram, pela primeira vez em um mesmo desenho experimental, que é possível reverter diferentes aspectos da memória de recompensa (preferência e sensibilização) por meio do bloqueio da reconsolidação. / Drug addiction is a complex and multifactorial disorder that develops in a few people who use these substances. Associative memories between the drug and context of use act as a trigger for maladaptive behavior such as drug seeking and drug use, in addition to relapse after an extended period of withdrawal. Underlying these behavioral changes are modifications in glutamatergic reception (AMPA) in structures involved with memory (Hippocampus) and reward (Nucleus Accumbens). Therefore, strategies that weaken the drug and context association and deepen knowledge of circuits involved in these behaviors are extremely relevant therapeutically. When retrieved, a memory can undergo two distinct processes post-retrieval: extinction, in which a new memory inhibiting a previous association is generated, and reconsolidation, in which the original memory can enter a labile state and is susceptible to modifications, when it can be weakened by inhibition of its reconsolidation. Reconsolidation of memory has been shown to be a more effective and long lasting strategy in relation to extinction, since the original memory is modified. An animal model for studying drug addiction, conditioned place preference (CPP) is largely used and it is well known that it is possible to weaken preference by disrupting reconsolidation. However, there are few studies that investigate the existence of reconsolidation in a locomotor sensitization paradigm, which seems to occur in a condition dependent on context of acquisition, although some works report its independence. The questions answered in this work were (a) if it is possible to reverse both, context preference and locomotor sensitization to morphine (5mg/kg) by protein synthesis inhibition (CHX) after a contextual memory reactivation session in CPP, (b) if the disruption of behaviors reflects a reversal of changes of GluA1, GluA1p (Ser845) e GluA2 in dorsal Hippocampus (dHPC) and Nucleus Accumbens (NAc) and (c) if the same treatment in these structures differentially reverts the two parameters assessed. Our results indicate that it is possible to revert context preference and locomotor sensitization via systemic disruption of protein synthesis and that morphine conditioning induces changes in AMPA subunits in dHPC and NAc, although CHX did not have an evident effect on molecular reversal. Animals cannulated in dHPC and NAc core did not induce preference or sensitization. Taken together, our results demonstrated, for the first time, using the same experimental design that is possible to revert different aspects of reward memory (preference and sensitization) by disrupting the reconsolidation process.

Memória

Hipocampo

Núcleo accumbens

Locomoção

Morfina

Morphine

Conditioned place preference

Locomotor sensitization

Memory

Reconsolidation

Dorsal hippocampus

Nucleus accumbens

Cicloheximide

GluA1

GluA2

Modélisation théorique du développement tumoral sous fenêtre dorsale : Vers un outil clinique d'individualisation et d'optimisation de la thérapie / Theoretical modelisation of tumour development on dorsal skinfold chamber : towards a clinical tool to individualize and optimize therapies.

Lesart, Anne-Cécile

13 November 2013

Le travail réalisé durant cette thèse a eu pour objectif de développer un modèle théorique spécifiquement dédié au contexte du développement tumoral tel qu'il peut être observé sous une fenêtre dorsale implantée sur une souris. Le modèle développé est un modèle hybride multi-physique et multi-échelle qui couple deux modules principaux. Le premier module modélise la croissance tumorale par un automate cellulaire qui permet de différencier l'état de chaque cellule en fonction de son histoire (cycle cellulaire), et de son environnement (espace disponible pour proliférer, présence d'oxygène). Le second module modélise le réseau vasculaire et le flux sanguin et rend compte de l'angiogenèse (apparition de nouveaux vaisseaux) et de l'adaptation du diamètre des vaisseaux, en fonction de l'évolution des contraintes hémodynamiques, nettement visible sous la fenêtre dorsale. L'ensemble des processus diffusifs (diffusion de l'oxygène et des facteurs de croissance vasculaire) sont décrits par des équations aux dérivées partielles, couplées à des automates cellulaires qui permettent de localiser à chaque instant pour chaque équation les termes sources (production) et les termes puits (consommation) pour chaque entité diffusive. Les simulations numériques réalisées montrent dans quelle mesure il est possible de rendre compte des observations expérimentales sur le plan qualitatif, qui nécessite la neutralisation des biais numériques ; et sur le plan quantitatif, pour reproduire la cinétique de croissance tumorale et l'évolution de la densité vasculaire. Le modèle numérique de l'évolution tumorale sous fenêtre dorsale est ensuite utilisé pour tester les effets de deux types de molécules : cytotoxiques et anti-vasculaires. Les simulations numériques de ces deux types de traitement explorent différents protocoles, définis par le mode d'action de la molécule, la dose administrée et la fréquence d'administration. Les résultats montrent comment il est alors possible de définir un protocole optimum pour une tumeur donnée en direction d'une individualisation de la thérapie. Ce modèle intégré a permis de poser de façon satisfaisante les bases d'un clone numérique du modèle expérimental d'évolution tumorale sous fenêtre dorsale même si certains aspects nécessitent encore quelques améliorations. La validation des aspects thérapeutiques restera encore à accomplir avant de pouvoir envisager à terme le remplacement (au moins partiel) de l'animal par l'ordinateur. / The work realised during this thesis had for objective to develop a theoretical model dedicated to the context of tumour development as observed on a dorsal skinfold chamber on a mouse. The model developed is hybrid, multi-physic and multi-scale, and associate two main modules. The first module model tumour growth with a cellular automaton which permit to differentiate the state of each cell regarding its history (cell cycle), its environment (available space to proliferate, oxygen availability). The second module model vascular network and blood flow, and accounts for angiogenesis (apparition of new vessels) and diameter adaptation of vessels, regarding hemodynamical constraints evolution which is distinctly visible on dorsal chamber. The diffusive processes (oxygen diffusion and vascular growth factors) are described by partiel differential equations, coupled with cellular automata which permit to localize at each time for each equation the source terms (production) and the well terms (consumption) for each diffusive entity. The numerical simulations realised show in which regard it is possible to accounts for the experimental observations on the qualitative basis, which require numerical bias neutralisation; and on the quantitative basis, to reproduce tumour growth kinetic and evolution of vascular density. The numerical model of tumour evolution on dorsal chamber is then used to test the effects of two types of molecules: cytotoxic and anti-vascular. Numerical simulation of these two types of treatment explore different protocols, defined by the action mode of the molecule, the dose administrated, and the administration frequency. Results show how it is possible to define an optimum protocol for a given tumour in direction of therapy individualisation. This integrated model has permitted to put in place in a satisfactory way the bases of a numerical clone of the experimental model of tumour growth on dorsal chamber, even if several aspects still necessitate some improvements. The validation of these theoretical aspects has yet to be accomplished before considering in term the replacement (at least partiallly) of animals by computers.

Fenêtre dorsale

Modélisation multi-échelle

Modèle computationnel

Croissance tumorale

Angiogénèse

Couplage et optimisation des thérapies

Dorsal skinfold chamber

Multi-scale modelling

Computational model

Tumour growth

Angiogenesis

Therapies' coupling and optimisation

Investiga??o do papel dos receptores 5-HT3 da subst?ncia cinzenta periaquedutal dorsal na modula??o dos comportamentos relativos ? ansiedade no labirinto em cruz elevado e no campo aberto em ratos

Garcia, Jarmilla Bow Ltaif

25 June 2015

Submitted by Automa??o e Estat?stica (sst@bczm.ufrn.br) on 2016-05-10T22:31:40Z No. of bitstreams: 1 JarmillaBowLtaifGarcia_DISSERT.pdf: 1132092 bytes, checksum: 73425ef0ae6509211c5362da756e1308 (MD5) / Approved for entry into archive by Arlan Eloi Leite Silva (eloihistoriador@yahoo.com.br) on 2016-05-17T19:56:28Z (GMT) No. of bitstreams: 1 JarmillaBowLtaifGarcia_DISSERT.pdf: 1132092 bytes, checksum: 73425ef0ae6509211c5362da756e1308 (MD5) / Made available in DSpace on 2016-05-17T19:56:28Z (GMT). No. of bitstreams: 1 JarmillaBowLtaifGarcia_DISSERT.pdf: 1132092 bytes, checksum: 73425ef0ae6509211c5362da756e1308 (MD5) Previous issue date: 2015-06-25 / Coordena??o de Aperfei?oamento de Pessoal de N?vel Superior (CAPES) / A ansiedade ? um estado emocional caracterizado por altera??es fisiol?gicas e psicol?gicas que oferecem uma sensa??o desagrad?vel ao indiv?duo. No entanto esse comportamento tem grande valor adaptativo, uma vez que alerta o indiv?duo sobre os poss?veis perigos que determinada situa??o possa oferecer. J? foram identificadas v?rias regi?es encef?licas relacionadas ao substrato neural da ansiedade e dentre elas pode-se citar a subst?ncia cinzenta periaquedutal (SCP). Al?m disso, diversos estudos demonstraram o envolvimento do sistema seroton?rgico da por??o dorsal da SCP (SCPD) na modula??o de comportamentos relativos ? ansiedade. Tendo em vista isso, o objetivo desse trabalho foi avaliar o papel dos receptores 5-HT3 da SCPD na modula??o de comportamentos relacionados ? ansiedade e locomo??o em ratos testados no labirinto em cruz elevado (LCE) e no campo aberto (CA). Ratos Wistar receberam a microinje??o do antagonista do receptor 5-HT3 dolasetron (100ng, 500ng e 1000ng) (experimento 1), do agonista do receptor 5-HT3m-Chlorophenylbiguanide (mCPBG) (2,5?g, 05?g e 10?g) (experimento 2) ou de salina a 0,9% na SCPD. Ap?s 10 minutos (experimento 1) ou 5 minutos (experimento 2), os ratos foram colocados no LCE e seus comportamentos foram avaliados durante 5 minutos. Vinte e quatro horas depois, os animais receberam as mesmas doses com que foram microinjetados no dia anterior na SCPD e ap?s 10 minutos (experimento 1) ou 5 minutos (experimento 2) foram colocados no CA e seus comportamentos foram avaliados durante 15 minutos. No experimento 1 a microinje??o do dolasetron n?o alterou os par?metros de ansiedade e locomo??o no LCE e CA. J? no experimento 2, o mCPBG nas doses de 5?g e de 10?g produziu efeito ansiol?tico no LCE sem promover altera??o locomotora no animal. Esses resultados sugerem que a ativa??o dos receptores 5-HT3 da SCPD favorece um efeito ansiol?tico em ratos avaliados no LCE. / Anxiety is an emotional state characterized by physiological and psychological changes that provide an unpleasant feeling to the individual. However this behavior has great adaptive value, since it alerts the individual about possible dangers that particular situation can offer. It has been identified various brain regions related to neural substrate of anxiety and, among them, it is the periaqueductal gray matter (PAG). Several studies have demonstrated the involvement of serotonergic system of the dorsal portion of PAG (DPAG) in the modulation of behaviors related to anxiety. In view of this, the objective of this study was to evaluate the role of 5-HT3 receptors of the DPAG in the modulation of behaviors related to anxiety and locomotion in rats tested in the elevated plus maze (EPM) and open field (OF). Wistar rats received microinjection of 5-HT3 receptor antagonist dolasetron (100ng, 500ng and 1000ng) (experiment 1), 5-HT3 receptor agonist m-Chlorophenylbiguanide (mCPBG) (2,5?g, 5?g and 10mg) (Experiment 2) or saline 0.9% in the DPAG. After 10 minutes (experiment 1) or 5 minutes (Experiment 2), the rats were placed in the EPM and their performances were evaluated during 5 minutes. Twenty-four hours later the animals received the same doses that were microinjected on the previous day in the DPAG and after 10 minutes (experiment 1) or 5 minutes (experiment 2) were placed in OF and their behaviors were assessed for 15 minutes. In experiment 1 microinjection of dolasetron did not change the parameters of anxiety and locomotion in EPM and OF. In the experiment 2, the mCPBG at doses of 5?g and 10mg produced anxiolytic effect in EPM without changes in locomotor behavior. These results suggest that activation of 5-HT3 receptors in the SCPD eliciate an anxiolytic effect in rats evaluated in EPM.

CNPQ::CIENCIAS BIOLOGICAS

Ansiedade

Subst?ncia cinzenta periaquedutal dorsal

Serotonina

Receptor 5-HT3

Dolasetron

m-Chlorophenylbiguanide (mCPBG)

Labirinto em cruz elevado

Campo aberto

Medium change monitoring using ambient seismic noise and coda wave interferometry: examples from intraplate NE Brazil and the Mid-Atlantic Ridge

D'hour, Virginie

01 September 2015

Submitted by Automa??o e Estat?stica (sst@bczm.ufrn.br) on 2016-08-09T23:00:00Z No. of bitstreams: 1 VirginieD'hour_TESE.pdf: 8753386 bytes, checksum: 2e3e6a55a73239c9eeac2c8def85eb39 (MD5) / Approved for entry into archive by Arlan Eloi Leite Silva (eloihistoriador@yahoo.com.br) on 2016-08-13T00:23:12Z (GMT) No. of bitstreams: 1 VirginieD'hour_TESE.pdf: 8753386 bytes, checksum: 2e3e6a55a73239c9eeac2c8def85eb39 (MD5) / Made available in DSpace on 2016-08-13T00:23:12Z (GMT). No. of bitstreams: 1 VirginieD'hour_TESE.pdf: 8753386 bytes, checksum: 2e3e6a55a73239c9eeac2c8def85eb39 (MD5) Previous issue date: 2015-09-01 / Conselho Nacional de Desenvolvimento Cient?fico e Tecnol?gico (CNPq) / Nesta tese s?o apresentados e discutidos os resultados de correla??o do ru?do s?smico em dois contextos: regi?o intraplaca e Dorsal Meso-oce?nica. O m?todo de interferometria de cauda de onda (coda wave interferometry?CWI) tamb?m foi utilizado para os dados da regi?o intraplaca. A correla??o do ru?do permite recuperar a fun??o de Green emp?rica entre dois receptores , como se uma das esta??es atuasse como uma fonte (virtual). Esta t?cnica ?amplamente utilizado em sismologia para a imagem do subsolo e para monitorar mudan?as estruturais associadas principalmente com erup??es vulc?nicas e terremotos grandes (mb > 6.0). No estudo da regi?o intraplaca, fomos capazes de detectar mudan?as estruturais localizadas relacionadas com esta pequena sequ?ncia de terremotos, cujo evento principal ? de mR 3.7, no Nordeste do Brasil. N?s tamb?m mostramos que a normaliza??o de 1-bit de e o branqueamento spectral provoca perdas de detalhes na forma de onda e que a auto- correla??o de fase, que ? pouco sens?vel ? amplitude , parece ser mais sens?vel e robusta para a nossa an?lise. A an?lise de 6 meses de dados usando correla??es cruzadas detecta claramente altera??es do meio logo ap?s do evento principal, enquanto que as auto- correla??es essencialmente detectam altera??es ap?s 1 m?s. Estas mudan?as na correla??o cruzada e na auto-correla??o podem serexplicadas pela redistribui??o da press?o do fluido ocasionadas mudan?as hidromec?nicas e novos caminhos preferenciais para difus?o de press?o e fuidos , devido a terramotos que ocorrem mais tarde. No estudo da Dorsal Meso-oce?nica, investigamos as mudan?as estruturais associadas a um terremoto de mb 4,9 aolongo da falha transformante de S?o Paulo. Os dados foram registrados por a ?nica esta??o s?smica localizada a menos de 200 km da Dorsal Meso-oce?nica. Os resultados da auto-correla??o de fase por um per?odo de 5 meses, mostram uma forte mudan?a de meio co-s?smica seguido por uma recupera??o p?s-s?smica relativamente r?pida. Esta mudan?a do meio provavelmente est? relacionada aos danos causados pelo terremoto de mb 4.9. O processo de cicatriza??o (enchimento das novas fissuras) que durou 60 dias pode ser decomposto em duas fases, uma recupera??o r?pida na fase p?s-s?smica (de 70% em ~ 30 dias) precoce e uma recupera??o relativamente lenta depois (de 30% em ~ 30 dias) No estudo de interferometria de cauda de onda, monitoramos mudan?as temporais da subsuperf?cie causada pela sequ?ncia de pequenos terremotos intraplaca mencionado anteriormente. O m?todo foi validado com dados sint?ticos. Fomos capazes de detectar uma mudan?a da fonte de 2.5% e uma redu??o de 15% da quantidade dos espalhadores. A partir dos dados reais, observamos uma r?pida diminui??o da correla??o da cauda da onda ap?s do evento s?smico mR 3.7. Isso indica uma mudan?a r?pida do subsolo na regi?o da falha induzida pelo terremoto. / This thesis presents and discusses the results of ambient seismic noise correlation for two different environments: intraplate and Mid-Atlantic Ridge. The coda wave interferometry method has also been tested for the intraplate data. Ambient noise correlation is a method that allows to retrieve the structural response between two receivers from ambient noise records, as if one of the station was a virtual source. It has been largely used in seismology to image the subsurface and to monitor structural changes associated mostly with volcanic eruptions and large earthquakes. In the intraplate study, we were able to detect localized structural changes related to a small earthquake swarm, which main event is mR 3.7, North-East of Brazil. We also showed that the 1-bit normalization and spectral whitening result on the loss of waveform details and that the phase auto-correlation, which is amplitude unbiased, seems to be more sensitive and robust for our analysis of a small earthquake swarm. The analysis of 6 months of data using cross-correlations detect clear medium changes soon after the main event while the auto-correlations detect changes essentially after 1 month. It could be explained by fluid pressure redistribution which can be initiated by hydromechanical changes and opened path ways to shallower depth levels due to later occurring earthquakes. In the Mid-Atlantic Ridge study, we investigate structural changes associated with a mb 4.9 earthquake in the region of the Saint Paul transform fault. The data have been recorded by a single broadband seismic station located at less than 200 km from the Mid-Atlantic ridge. The results of the phase auto-correlation for a 5-month period, show a strong co-seismic medium change followed by a relatively fast post-seismic recovery. This medium change is likely related to the damages caused by the earthquake?s ground shaking. The healing process (filling of the new cracks) that lasted 60 days can be decomposed in two phases, a fast recovery (70% in ~30 days) in the early post-seismic stage and a relatively slow recovery later (30% in ~30 days). In the coda wave interferometry study, we monitor temporal changes of the subsurface caused by the small intraplate earthquake swarm mentioned previously. The method was first validated with synthetics data. We were able to detect a change of 2.5% in the source position and a 15% decrease of the scatterers? amount. Then, from the real data, we observed a rapid decorrelation of the seismic coda after the mR 3.7 seismic event. This indicates a rapid change of the subsurface in the fault?s region induced by the earthquake.

Ru?do s?smico

Auto-correla??o

Correla??o cruzada

Interferometria de cauda da onda

Intraplaca

Dorsal Meso-Oce?nica

Reversão dos efeitos reforçadores da morfina através do prejuízo da reconsolidação da memória do condicionamento de preferência por local e da sensibilização locomotora

Boos, Flávia Zacouteguy

January 2016

A dependência de drogas é um transtorno multifatorial complexo que se desenvolve em uma minoria de indivíduos que fazem uso dessas substâncias. Memórias associativas entre a droga e o contexto funcionam como gatilho para disparar comportamentos não adaptativos de busca e consumo, além de recaídas após períodos de abstinência. Subjacentes a essas mudanças comportamentais, existem modificações nas subunidades de receptores glutamatérgicos do tipo AMPA em estruturas envolvidas com memória (Hipocampo) e recompensa (Núcleo Accumbens). Por isso, estratégias que enfraqueçam a associação do contexto com a droga e que aprofundem o conhecimento dos circuitos envolvidos nesses comportamentos são de extrema relevância terapêutica. A memória quando evocada pode passar por dois processos pós-evocação: a extinção, em que uma nova memória é formada inibindo uma prévia associação, e a reconsolidação, em que a memória original entra em um estado lábil e suscetível a modificações, em que é possível enfraquecê-la através da inibição de sua reconsolidação. A reconsolidação da memória mostra-se uma estratégica mais eficaz e duradoura em relação à extinção, já que a memória original é modificada. Como modelo animal para o estudo da memória na dependência de drogas, o condicionamento de preferência por local (CPL) é bastante utilizado e sabe-se que é possível enfraquecer a preferência através do bloqueio da reconsolidação. Porém, são escassos os estudos que investigaram a existência da reconsolidação no modelo de sensibilização locomotora, que parece ocorrer, na maioria dos casos, em condição dependente do contexto de aquisição do comportamento, embora existam exemplos que demonstrem sua independência. As questões a serem respondidas neste trabalho são (a) se é possível reverter conjuntamente a preferência por local e a sensibilização locomotora à morfina (5 mg/kg) em ratos Wistar adultos machos, inibindo-se a síntese proteica com cicloheximida (CHX) i.p. logo após uma sessão de reativação contextual da memória no CPL, (b) se a reversão dos comportamentos reflete alterações (já descritas por outros autores) em GluA1, GluA1p (Ser845) e GluA2, no Hipocampo dorsal (HPCd) e no Núcleo Accumbens (NAc), e (c) se o mesmo tratamento em ambas estruturas reverte os dois parâmetros avaliados – comportamental e neuroquímico – de forma diferente ou igual. Nossos resultados mostraram ser possível reverter a preferência por local e a sensibilização locomotora por inibição sistêmica de síntese proteica, e que o condicionamento com exposição à morfina induz alterações nas subunidades analisadas de AMPA, conforme verificado no HPCd e NAc, embora a CHX não tenha produzido um efeito tão bem definido. Os animais que receberam infusões centrais no HPCd e NAc (central) não exibiram preferência por local, nem sensibilização. Em conjunto, nossos resultados mostraram, pela primeira vez em um mesmo desenho experimental, que é possível reverter diferentes aspectos da memória de recompensa (preferência e sensibilização) por meio do bloqueio da reconsolidação. / Drug addiction is a complex and multifactorial disorder that develops in a few people who use these substances. Associative memories between the drug and context of use act as a trigger for maladaptive behavior such as drug seeking and drug use, in addition to relapse after an extended period of withdrawal. Underlying these behavioral changes are modifications in glutamatergic reception (AMPA) in structures involved with memory (Hippocampus) and reward (Nucleus Accumbens). Therefore, strategies that weaken the drug and context association and deepen knowledge of circuits involved in these behaviors are extremely relevant therapeutically. When retrieved, a memory can undergo two distinct processes post-retrieval: extinction, in which a new memory inhibiting a previous association is generated, and reconsolidation, in which the original memory can enter a labile state and is susceptible to modifications, when it can be weakened by inhibition of its reconsolidation. Reconsolidation of memory has been shown to be a more effective and long lasting strategy in relation to extinction, since the original memory is modified. An animal model for studying drug addiction, conditioned place preference (CPP) is largely used and it is well known that it is possible to weaken preference by disrupting reconsolidation. However, there are few studies that investigate the existence of reconsolidation in a locomotor sensitization paradigm, which seems to occur in a condition dependent on context of acquisition, although some works report its independence. The questions answered in this work were (a) if it is possible to reverse both, context preference and locomotor sensitization to morphine (5mg/kg) by protein synthesis inhibition (CHX) after a contextual memory reactivation session in CPP, (b) if the disruption of behaviors reflects a reversal of changes of GluA1, GluA1p (Ser845) e GluA2 in dorsal Hippocampus (dHPC) and Nucleus Accumbens (NAc) and (c) if the same treatment in these structures differentially reverts the two parameters assessed. Our results indicate that it is possible to revert context preference and locomotor sensitization via systemic disruption of protein synthesis and that morphine conditioning induces changes in AMPA subunits in dHPC and NAc, although CHX did not have an evident effect on molecular reversal. Animals cannulated in dHPC and NAc core did not induce preference or sensitization. Taken together, our results demonstrated, for the first time, using the same experimental design that is possible to revert different aspects of reward memory (preference and sensitization) by disrupting the reconsolidation process.

Memória

Hipocampo

Núcleo accumbens

Locomoção

Morfina

Morphine

Conditioned place preference

Locomotor sensitization

Memory

Reconsolidation

Dorsal hippocampus

Nucleus accumbens

Cicloheximide

GluA1

GluA2