Neuropathies induites par chimiothérapie néo-adjuvante du cancer du sein : atteintes périphériques et centrales, mécanismes impliqués et perspectives thérapeutiques / Neuropathies induced by neo-adjuvant chemotherapy used against breast cancer : peripheral and central disorders, mechanisms and therapeutic prospects

Matta, Célia

20 September 2018

La chimiothérapie néoadjuvante (CNA) est une avancée majeure dans les traitements des cancers du sein. La CNA réduit nettement la tumeur primaire et permet une chirurgie conservatrice à tous les stades du cancer. Malheureusement, elle s’accompagne de dysfonctionnements neurologiques qui limitent le succès du traitement anti-tumoral. La prise en charge médicale de ces troubles neurologiques est problématique compte tenu de l’inefficacité des neuroprotecteurs disponibles. De plus, la recherche de nouvelles thérapeutiques est handicapée par l’absence de modèles expérimentaux reproduisant fidèlement les symptômes évoqués par la CNA séquentielle « épirubicine (EPI)/docétaxel (DO) » ou CNA-[EPI-DO] fréquemment utilisée. Ce travail de thèse a permis de caractériser pour la première fois un modèle animal pertinent de troubles neurologiques périphériques et centraux évoqués par la CNA-[EPI-DO]. Ce modèle préclinique a été utilisé pour révéler l’efficacité d’un traitement concomitant de duloxétine et d’alloprégnanolone contre la neuropathie périphérique douloureuse induite par la CNA-[EPI-DO]. Nos travaux montrent aussi que la duloxétine exerce une action bénéfique contre les déficits cognitifs évoqués par la CNA-[EPI-DO]. La thèse ouvre des perspectives prometteuses à explorer pour le développement de thérapies efficaces contre les altérations neurologiques CNA-induites. / Neoadjuvant chemotherapy (NAC) represents a major progress in breast cancer therapy. By shrinking significantly, the tumor volume, NAC allows conservative surgery at all stages of breast cancer. Unfortunately, NAC also induces neurological dysfunctions that jeopardize the chances of success of anti-tumor treatments. Therapeutic management of these neurological disorders remains a major concern because neuroprotective drugs currently available are not effective. Furthermore, investigations to characterize novel effective therapeutics are hampered by the lack of reliable experimental models mimicking the neurological symptoms evoked by the sequential epirubicin (EPI)/docetaxel (DO)-NAC or [EPI-DO]-NAC frequently used in humans. The present thesis work allowed the first characterization of a relevant animal model of [EPI-DO]-NAC-induced peripheral and central neurological disorders. This preclinical model has successfully been used to demonstrate the efficacy of duloxetine and allopregnanolone concomitant treatment against [EPI-DO]-NAC-evoked painful peripheral neuropathy. Our results also reveal a beneficial action of duloxetine against [EPI-DO]-NAC-induced cognitive deficits. The thesis opens promising perspectives to be explored for the development of effective therapies against [EPI-DO]-NAC-induced neurological alterations.

Allopregnanolone

Chimiothérapie néo-adjuvante

Duloxétine

Neuroprotection

Troubles cognitifs chimio-induits

Allopregnanolone

Neoadjuvant chemotherapy

Duloxetine

Neuroprotection

Chemo-induced cognitive disorders

615.7

616.99

Normalvärden och F-waves vid registrering på tibialis anterior vid undersökning av peroneus communis med elektroneurografi / Normal values and F-waves for registration on tibialis anterior for examination of peroneus communis with electroneurography

Lundström, Malin

January 2019

För att undersöka misstänkt tillklämningsneuropati i peroneus communis (PC) används elektroneurografi, där elektrisk stimulering möjliggör undersökning av nervledningshastigheter, svarsamplitud och överledningstid. Vid opålitlig registrering på extensor digitorium brevis (EDB), görs registreringen på tibialis anterior (TA). I dagsläget finns dock inga normalvärden eller standardiserad metod för registrering på TA. Syftet med studien var därför att ta fram dessa normalvärden och utveckla en metod för TA-registrering, och samtidigt jämföra de båda registreringspunkterna gällande nervledningshastighet, undersöka sidoskillnaderna vid registrering på TA och undersöka hur kroppslängden påverkade överledningstiden. Det undersöktes om s.k. F-waves kunde påvisas vid registrering på TA och i så fall hur hög svarsandelen och svarslatensen var. 22 deltagare mellan 23-59 år gamla och 154-190 cm i kroppslängd undersöktes. TA undersöktes med den aktiva registreringselektroden på muskeln där den var som störst och med referenselektroden på fotleden. Stimuleringar gjordes på laterala poplitea fossa och 110 mm ned distalt om caput fibula. EDB undersöktes enligt metodbeskrivning. Normalvärdena för TA var 2,2-5,4 mV gällande amplitud, 55-73 m/s gällande nervledningshastighet och 3,8-5,9 ms gällande överledningstid. Sidoskillnaderna var 0-1,4 mV gällande amplitud, 0-8 m/s gällande hastighet och 0-0,8 ms gällande överledningstid. De beräknade gränsvärdena visar på de små sidoskillnaderna som krävs för en klinisk betydelse. Överledningstiden kunde till 23 % förklaras av kroppslängden. Resultaten var likvärdiga med tidigare studier. Jämförelsen av nervledningshastigheten mellan registrering på TA och EDB visade en statistiskt, men inte nödvändigtvis kliniskt signifikant skillnad, med bias + 5 m/s. F-waves återfanns hos samtliga deltagare, med svarsandelen 94-100 %. F-wave svarslatensen kunde till 41 % förklaras av kroppslängden. / Electroneurography is used to examine a suspected entrapmentneuropathy in peroneus communis (PC), where an electric stimulus enables the evaluation of nerve conduction velocity, muscle response amplitude and latency. If registration from the extensor digitorum brevis (EDB) provides unreliable results, the registration can be made from tibialis anterior (TA). Currently there are no normal values available in our laboratory and no standard method regarding the registration on TA. The purpose of this study was therefore to retrieve normal values for this registration and to develop and establish a method, and also compare the different registration sites, to examine the side differences from the registrations on TA, and how the height affected the latency. It was also examined if so called F-waves could be recorded from TA, and if so, determine the response rate and latency. 22 participants between 23-59 years an 154-190 cm were examined. TA was examined with the active registration electrode on the site where the muscle was the largest and the reference electrode on the ankle. Stimulations were made on lateral poplitea fossa and 110 mm lower on distal caput fibula. EDB were examined according to established methods. Normal values for the registration on TA were 2,2-5,4 mV regarding amplitude, 55-73 m/s regarding nerve conduction velocity and 3,8-5,9 ms regarding latency. Side differences were 0-1,4 mV regarding amplitude, 0-8 m/s regarding nerve conduction velocity and 0-0,8 ms regarding latency. The calculated limits show that it only takes small side differences to have a clinical significance. The method gave equivalent results to previous studies. 23 % of the latency could be explained by height. The comparing of the nerve conduction velocity from the different registrations showed a significant statistical, but not necessarily clinical, difference, with the bias 5 m/s. F-waves were retrieved from all participants with a response rate of 94-100 %. 41 % of the F-wave latency could be explained by height.

Peroneus communis

Tibialis anterior

Extensor digitorum brevis

Entrapment neuropathy

Normal values

F-waves

Peroneus communis

Tibialis anterior

Extensor digitorum brevis

Tillklämningsneuropati

Normalvärden

F-waves

Biomedical Laboratory Science/Technology

Mapping genetic diseases in northern Sweden

Einarsdottir, Elisabet

January 2005

The population of northern Sweden has previously been shown to be well suited for the mapping of monogenic diseases. In this thesis we have tested the hypothesis that this population could also be used for efficient identification of risk genes for common diseases. In Paper I we have hypothesised that despite the admixture of Swedish, Finnish and Sami, the northern Swedish population consists of sub-populations geographically restricted by the main river valleys running through the region. This geographic isolation, in combination with founder effects and genetic drift, could represent a unique resource for genetic studies. On the other hand, it also underlines the importance of accounting for this e.g. in genetic association studies. To test this hypothesis, we studied the patterns of marriage within and between river valley regions and compared allelic frequencies of genetic markers between these regions. The tendency to find a spouse and live in the river valley where one was born is strong, and allelic frequencies of genetic markers vary significantly between adjacent regions. These data support our hypothesis that the river valleys are home to distinct sub-populations and that this is likely to affect mapping of genetic diseases in these populations. In Paper II, we tested the applicability of the population in mapping HSAN V, a monogenic disease. This disease was identified in only three consanguineous individuals suffering from a severe loss of deep pain perception and an impaired perception of heat. A genome-wide scan combined with sequencing of candidate genes resulted in the identification of a causative point mutation in the nerve growth factor beta (NGFB) gene. In Paper III, a large family with multiple members affected by familial forms of type 1 diabetes mellitus (T1DM) and autoimmune thyroiditis (AITD) was studied. This syndrome was mapped to the IDDM12 region on 2q33, giving positive lodscores when conditioning on HLA haplotype. The linkage to HLA and to the IDDM12 region thus confirmed previous reports of linkage and/or association of T1DM and AITD to these loci and provided evidence that the same genetic factors may be mediating these diseases. This also supported the feasibility of mapping complex diseases in northern Sweden by the use of familial forms of these diseases. In Paper IV, we applied the same approach to study type 2 diabetes mellitus (T2DM). A non-parametric genome-wide scan was carried out on a family material from northern Sweden, and linkage was found to the calpain-10 locus, a previously described T2DM-susceptibility gene on 2q37. Together, these findings demonstrate that selecting for familial forms of even complex diseases, and choosing families from the same geographical region can efficiently reduce the genetic heterogeneity of the disease and facilitate the identification of risk genes for the disease.

Genetics

isolated populations

linkage disequilibrium

linkage analysis

genome-wide scan

type 1 diabetes mellitus

type 2 diabetes mellitus

autoimmune thyroid disease

Genetik

Clinical genetics

Klinisk genetik

Caractérisation clinique et génétique d’une famille canadienne-française atteinte de la neuropathie héréditaire sensitive avec rétinite pigmentaire et ataxie

Putorti, Maria Lisa

04 1900

La complexité de l’étude des neuropathies héréditaires provient de leur hétérogénéité clinique et génétique et de la diversité des fibres composant les nerfs périphériques. Cette complexité se reflète dans les nombreuses classifications différentes. Les neuropathies héréditaires se classifient entre autres selon leur mode de transmission et leur atteinte sensitive, autonomique et motrice. Les neuropathies héréditaires sensitives et autonomiques (NHSA) se présentent avec une perte de la sensation distale aux membres, accompagnée d’autres manifestations selon le type de NHSA. L’étude des NHSA est facilitée lorsqu’il existe des grappes de familles originaires de régions du Québec où des effets fondateurs pour des maladies récessives ont déjà été identifiés. Nous avons recruté une grande famille canadienne-française originaire de Paspébiac dans la Baie-des-Chaleurs dans laquelle nous avons identifié quatre cas atteints d’une neuropathie héréditaire sensitive avec rétinite pigmentaire et ataxie (NHSRPA). Nous avons émis l’hypothèse que nous étions en présence d’une nouvelle forme de neuropathie héréditaire sensitive récessive à effet fondateur. Afin d’identifier la position chromosomique du gène muté responsable de la NHSRPA, nous avons tout d’abord complété un criblage du génome en génotypant des marqueurs microsatellites «single tandem repeat» (STR) sur des individus clés et nous avons ensuite procédé à une analyse de liaison génétique paramétrique. Ces études nous ont permis de lier cette famille au chromosome 1 et de définir un premier intervalle candidat de 6,7 Mb. Grâce à un génotypage de marqueurs «single nucleotide polymorphism» (SNP), nous avons réduit l’intervalle candidat à 5,3 Mb au locus 1q32,2-q32,3. Cette région contient 44 gènes candidats. Une revue plus fine de la littérature a fait ressortir qu’une famille espagnole et une américaine de souche hollandaise souffrant de la même maladie avaient déjà été liées au même locus. L’origine possiblement basque de notre famille gaspésienne nous a poussé à comparer l’haplotype porteur avec celui de la famille espagnole qui, quoi que gitane, provient du pays basque espagnol. Ces travaux ont démontré le partage d’une région de 203 kb. Afin de rétrécir davantage notre intervalle candidat, nous avons comparé les haplotypes des cas entre les deux familles et nous avons identifié un dernier intervalle candidat de 60 SNP au locus 1q32,3. Cette région ne contient que quatre gènes candidats dont le plus intéressant est le gène «activating transcription factor» (ATF3). À ce jour, aucune mutation n’a été trouvée dans le gène ATF3 et les gènes FAM71A, BATF3 et NSL1. Des expériences supplémentaires sont nécessaires afin d’identifier le gène muté responsable de la NHSRPA. / Hereditary neuropathies study’s complexity comes from their clinical and genetic heterogeneity and the peripheral nerves fibers’ diversity. This complexity leads to numerous different classifications. Hereditary neuropathies are classified based on the transmission mode and the sensitive, autonomic and motor affection. Hereditary sensory and autonomic neuropathies (HSAN) present themselves with members’ distal loss and other manifestations depending on the HSAN type. HSAN study can be facilitated when there are existing family grapes originating from Quebec regions where recessive diseases founder effects have been identified. We have recruited a large French-Canadian family originating from Paspébiac in the Baie-des-Chaleurs in which we have identified four cases affected by a hereditary sensory neuropathy with retinitis pigmentosa and ataxia (HSNRPA). We have hypothesized that we were in presence of a new form of recessive hereditary sensitive neuropathy with founder effect. In order to identify the HSNRPA causing mutated gene chromosomal position, we first completed a genome wide scan by genotyping microsatellite single tandem repeat (STR) markers on informative individuals and we have then proceeded to a parametric genetic linkage analysis. These studies allowed us to link this family to chromosome 1 and define a first candidate interval of 6.7 Mb. Second to the single nucleotide polymorphism (SNP) markers genotyping, we have reduced the candidate interval at 5.3 Mb on locus 1q32.2-q32.3. This region contains 44 genes. A finer literature review made us realize that a Spanish family and an American from Dutch origin suffering from the same disease had already been linked to the same locus. The possible Gaspesian family’s Basque origins brought us to compare their carrier haplotype with the Spanish family’s, although Gypsy but coming from the Spanish Basque country. This work has demonstrated a shared region of 203 kb. In order to further refine our candidate interval, we have compared the haplotypes of the cases between the two families and we have identified a last candidate interval of 60 SNP at locus 1q32.3. This region contains only four candidate genes, the activating transcription factor (ATF3) gene being the most interesting one. Until today, no mutation has been found in the ATF3 gene and in the FAM71A, BATF3 and NSL1 genes. Further experiments will be necessary in order to identify the HSNRPA causing mutated gene.

Neuropathie héréditaire sensitive

Sensory hereditary neuropathy

rétinite pigmentaire

retinitis pigmentosa

effet fondateur

founder effect

ataxie

ataxia

criblage génomique

genome-wide scan

cartographie de l’homozygosité

homozygosity mapping

identité par la descendance

identity by descent

Inter and intra-specific differences in medicinal plant use for the treatment of type II diabetes symptoms by the Cree Elders of Eeyou Istchee (QC)

Downing, Ashleigh A.

07 1900

Au Canada, nous remarquons une prédominance du diabète de type 2 au sein des communautés autochtones. Une approche ethnobotanique est utilisée en collaboration avec la Nation Crie de Eeyou Istchee afin de déterminer quels traitements à base de plantes peuvent être utilisés pour contrer les différentes conditions qui, collectivement, forment le diabète. Les pharmacopées de deux communautés cries, soit celles de Waskaganish et de Nemaska, ont été établies puis comparées à celles de étudiées antérieurement : communautés Whapmagoostui et Mistissini. Malgré les différences géographiques de ces groupes, leurs utilisations sont majoritairement semblables, avec pour seule exception le contraste entre les communautés de Nemaska et de Whapmagoostui. De plus, nous avons complété l’évaluation du taux cytoprotecteur des aiguilles, de l’écorce et des cônes de l’épinette noire (Picea mariana). Les extraits provenant de tous les organes des plantes démontrent une protection qui dépend de la concentration. La réponse spécifique d’organes peut varier selon l’habitat; ainsi, les plantes poussant dans les tourbières ou dans les forêts, sur le littoral ou à des terres l’intérieur démontrent des différences quant à leur efficacité. Bref, l’écorce démontre une relation dose-effet plus forte dans la forêt littorale, tandis que les aiguilles n’indiquent pas de changements significatifs selon leur environnement de croissance. La bioactivité observée démontre une corrélation avec le contenu phénolique et non avec l’activité de l’agent antioxydant. Ces résultats contribuent à péciser les activités antidiabétiques des plantes de la forêt boréale canadienne, telles qu’identifiées au niveau cellulaire par les guérisseurs Cries. / In Canada there is an overwhelming prevalence of type II diabetes in First Nations communities. Here an ethnobotanical approach has been used in cooperation with the Cree Nation of Eeyou Istchee to focus on finding plant based treatments for the conditions which collectively make up the symptoms of diabetes. The pharmacopoeias of two Cree communities (Waskaganish and Nemaska) are elucidated then compared with previously studied populations (Whapmagoostui and Mistissini). Despite differences in north-south east-west geography, plant ranking and use matrices were similar with the exception of Nemaska/Whapmagoostui. We have also completed the evaluation of Black spruce (Picea mariana) needle, bark and cone cytoprotectivity. Extracts from all organs exhibited concentration-dependent protection. Organ-specific response was habitat and growth environment dependent with plants grown either in bog or forest habitats in coastal or inland environments exhibiting differences in efficacy. Observed bioactivity correlated with total phenolic content but not with antioxidant activity. Together, these results contributed to the understanding of antidiabetic activity of Canadian boreal forest plants identified by the Cree of Eeyou Istchee healers at the cellular level.

plantes médicinales

diabète de Type II

neuropathie

Picea mariana

ethnobotanique

agent antioxydant

phénol

cytoprotection

Autochtones

cellules PC12-AC

medicinal plants

type II diabetes

neuropathy

Picea mariana

ethnobotany

antioxidant

phenolics

cytoprotection

Aboriginal

PC12-AC cells

Neuroprotection and axonal regeneration after peripheral nerve injury

Welin, Dag,

January 2010

Diss. (sammanfattning) Umeå : Umeå universitet, 2010.

Impact de l'hypoxie intermittente chronique sur la rétine et le nerf optique du rat : aspects vasculaire et inflammatoire. / Chronic intermittent hypoxia impact on rat retina and optic nerve : vascular and inflammatory aspects.

Mentek, Marielle

14 December 2015

Le syndrome d’apnées obstructives du sommeil (SAOS) est associé à la survenue de neuropathies optiques, en particulier la neuropathie optique ischémique antérieure aigue non artéritique (NOIAA-NA). Parmi les mécanismes d’apparition de cette neuropathie et potentiellement associés au SAOS, la dysrégulation et l’inflammation vasculaires pourraient jouer un rôle. Il n’existe aucune donnée dans la littérature sur l’effet de l’hypoxie intermittente (HI) chronique sur la fonction vasculaire de l’œil.Le but de ce travail était de développer des techniques d’évaluation de la fonction vasculaire oculaire chez le rat et de les appliquer à l’étude des conséquences vasculaires oculaires de l’HI. Ainsi, deux approches complémentaires ont été développées : 1) un prototype de fluxmètre laser Doppler (LDF) adapté au rongeur pour l’évaluation in vivo de la perfusion sanguine rétinienne et de la tête du nerf optique (TNO) et 2) le modèle d’étude de l’artère ophtalmique (AO) du rat par myographie vasculaire, in vitro.La mise au point du LDF chez le rat sain a permis de valider la pertinence du signal provenant des artères rétiniennes. A l’inverse, nos données invalident l’intérêt de la mesure au niveau de la TNO. En réponse à l’inhalation d’oxygène pur, nous observons une diminution de 17,0 ± 13,7 % de la vélocité artérielle rétinienne (VelART). Nous n’observons pas de variation significative de VelART lors d’injection intra-carotidienne d’endothéline 1 (ET-1) malgré une forte vasoconstriction des vaisseaux rétiniens. Les perspectives consistent à associer une caméra de haute résolution à un système bidirectionnel de LDF. L’étude de la réactivité de l’AO par myographie chez le rat soumis à 14 jours d’HI a mis en évidence une augmentation de la contraction à l’ET-1, associée à une augmentation de la réponse médiée par les récepteurs de type A (ETRA)et à une surexpression des ETRA au sein de l’AO. La relaxation NO-dépendante était diminuée chez le rat HI, et associée à un effet prédominant des produits vasoconstricteurs du cytochrome P450. Ces réponses étaient associées à une augmentation de la présence d’anions superoxyde dans la paroi de l’AO. Des études complémentaires sont nécessaires pour explorer les mécanismes à l’origine des ces altérations vasculaires, en particulier le rôle du stress oxydant. / Obstructive sleep apnea (OSA) has recently been associated with the occurrence of optic neuropathies, especially acute non-arteritic anterior ischemic optic neuropathy (NAION). Among the mechanisms of NAION onset potentially associated with OSA, vascular dysregulation and inflammation may play a role. There is still no data on the effect of chronic intermittent hypoxia (IH) on vascular function of the eye. The purpose of this work was to develop techniques for assessing rat ocular vascular function and apply them to the study of the ocular vascular consequences of IH. Thus, two complementary models have been developed: 1) a laser Doppler flowmeter (LDF) prototype adapted for rodents, to evaluate in vivo retinal and optic nerve head (ONH) blood perfusion and 2) in vitro model of rat ophthalmic artery (OA) study by myography. Preliminary work on healthy rat enabled us to validate the relevance of retinal arteries LDF signal, but not that of the ONH. Retinal blood velocity (VelART) dropped by 17.0 ± 13.7% in response to pure oxygen inhalation. We did not observe any significant change in VelART signal after intracarotidian endothelin 1 (ET -1) injection, despite strong vasoconstriction of retinal vessels. OA reactivity study by myography in rats exposed to a 14-day IH showed increased contraction to ET-1, associated with an increased endothelin receptor A-mediated (ETRA) response and ETRA overexpression within the AO. NO-dependent relaxation is reduced in IH rats, and associated with a shift towards vasoconstrictive effects of cytochrome P450 products. These responses were associated with an increase in superoxide anions in the OA wall. Further studies are needed to explore the underlying mechanisms of these vascular changes, particularly the role of oxidative stress. Understanding of the LDF signal is partial and should be further explored to permit application to the study of IH rat.

Syndrome apnées du sommeil

Hypoxie intermittente

Rétine

Nerf optique

Flowmétrie laser Doppler

Obstructive sleep apnea syndrome

Intermittent hypoxia

Non arteritic ischemic optic neuropathy

Retina

Optic nerve

Laser Doppler flowmetry

Identificação de herpesvírus bovino em amostras de cérebro / Identification of bovine herpesvirus in brain samples

SILVA, Duanne Alves da

24 February 2011

Made available in DSpace on 2014-07-29T15:07:43Z (GMT). No. of bitstreams: 1 Dissertacao Duanne A da Silva.pdf: 1367420 bytes, checksum: 2450c56c8175888ad1aaa259e17f1059 (MD5) Previous issue date: 2011-02-24 / Herpetic meningoencephalitis is an infection of the central nervous system caused by bovine herpesvirus 5 (BoHV-5) despite BoHV-1 also being associated with this pathology. The course of the disease is usually fatal. Meningoencephalitis has caused significant economic burden to the Brazilian cattle industry due to its high mortality rate, especially in young animals. Because of cross-reactivity and the absence of an effective serological test that differentiates types 1 and 5 of herpesvirus, the actual prevalence of infection with both viruses is unknown. It is estimated that some animals, supposedly infected with type 1, may be seropositive for type 5. For a better understanding of the molecular epidemiology of this virus in Goiás, 110 brain samples of young cattle, that died with neurological signs, referred to the reference laboratory of the State of Goiás for rabies diagnosis in 2008, were analyzed by multiplex PCR to amplify the glycoprotein C (gC) region of the BoHV-1 and -5 DNA. Of the 110 samples, 53.6% were positive for bovine herpesvirus. Of these, 22.0% were positive for BoHV-1, whereas 52.5% were positive for BoHV-5. Furthermore, 13.6% of samples showed co-infection for types 1 and 5. Among these, one sample came from a buffalo. Positivity for both bovine herpesvirus and rabies virus was observed in 53.3% of samples. This study showed that BoHV-1 and -5 are circulating among cattle in the State of Goiás and that herpesvirus type 1 can also be encephalitogenic. Although there was no evidence of viral replication, after inoculation of all 20 brain samples in cell culture, the possibility of viruses being associated with neurological disease cannot be ruled out. This was the first study to demonstrate the presence of BoHV-1 and BoHV-5 in samples obtained from herds in Goiás. / A meningoencefalite herpética é uma infecção do sistema nervoso central de curso geralmente fatal causada pelo herpesvírus bovino tipo 5 (BoHV-5), todavia, também o BoHV-1 pode estar associado a essa patologia. A enfermidade tem gerado muitos prejuízos à pecuária brasileira por apresentar elevada letalidade, principalmente, entre animais jovens. Devido a reatividade cruzada e a falta de um teste sorológico eficaz que diferencie os tipos 1 e 5 de herpesvírus bovino, não se sabe a real prevalência das infecções por ambos os vírus. Estima-se que uma parcela dos animais supostamente infectados pelo tipo 1 possa ser soropositiva para o tipo 5. Para um melhor entendimento da epidemiologia molecular desses vírus em Goiás, 110 amostras de cérebro de bovinos jovens que vieram a óbito com sinais neurológicos, encaminhadas ao laboratório de referência do Estado para diagnóstico de raiva no ano de 2008, foram analisadas por PCR multiplex para amplificação da região da glicoproteína C (gC) do DNA do BoHV-1 e -5. Das 110 amostras, 53,6% foram positivas para herpesvírus bovino. Destas, 22,0% foram positivas para o BoHV-1, enquanto 52,5% foram positivas para o BoHV-5. Além disso, encontrou-se 13,6% de coinfecção para os tipos 1 e 5. Entre estas, uma amostra foi proveniente de um bubalino. Foi observada positividade simultânea para herpesvírus bovino e o vírus da raiva em 53,3% das amostras. Este estudo permitiu concluir que o BoHV-1 e o -5 circulam no Estado de Goiás e que o BoHV-1 apresenta potencial encefalitogênico. Apesar de não ter ocorrido multiplicação viral em nenhuma das 20 amostras de cérebro inoculadas em cultura de célula, não se pode descartar a possibilidade da doença neurológica estar associada aos vírus nas outras amostras analisadas. Este foi o primeiro estudo com amostras de Goiás a comprovar a presença dos dois vírus nos rebanhos do Estado.

gado

infecção viral

letalidade

neuropatia

PCR multiplex

reatividade cruzada

cattle

viral infection

lethality

neuropathy

multiplex PCR

cross-reactivity

Atividade da proteína quinase dependente de RNA (PKR) no sistema nociceptivo em um modelo experimental de neuropatia periférica de origem viral / Double stranded RNA-activated protein kinase (PKR) activity in the nociceptive system in an experimental model of peripheral neuropathy of viral origin

Clarissa Maria Dias Mota

25 February 2016

A proteína quinase dependente de RNA (PKR) é uma molécula sentinela ativada em situações de estresse celular, incluindo infecções virais. A ativação de PKR por meio de sua fosforilação aciona cascatas de sinalização intracelular envolvidas em respostas inflamatórias e inibição da síntese protéica. Dados prévios do nosso laboratório sugerem que PKR está envolvida na hiperalgesia térmica de origem inflamatória. No presente estudo, foi investigado o papel da PKR na hiperalgesia térmica induzida pelo vírus da herpes simples tipo 1 (HSV1), durante as fases herpética e pós-herpética, combinando métodos comportamentais, genéticos, farmacológicos e moleculares. Camundongos C57bl/6, PKR+/+ e PKR-/- machos foram inoculados com HSV1. Os grupos controle foram inoculados com HSV1 inativo. Alodínia mecânica e hiperalgesia térmica foram monitoradas antes da inoculação do vírus e 8, 14, 21 e 28 dias após a inoculação. A curva dose e temporesposta e o teste da capsaicina foram realizados no 8º e 21º dias após a inoculação do vírus. Também nos períodos herpético e pós-herpético, foi investigado o perfil de expressão de proteínas envolvidas nas vias de sinalização de PKR (PKR, eIF2?, PACT, IKK e PP2A?), assim como o efeito da inibição de PKR pelo monitoramento da fosforilação de PKR, IKK?/?, P38, JNK, ERK1,2 e STAT3, e expressão de CaMKII? e TRPV1 nos GRD (L3-L6) ipsilateralmente à pata inoculada. Alodínia mecânica e hiperalgesia térmica ficaram evidentes até 28 dias após a inoculação. Camundongos PKR-/- desenvolveram alodínia mecânica, mas não hiperalgesia térmica, quando comparados com animais PKR+/+. A inibição sistêmica de PKR reverteu a hiperalgesia térmica de modo tempo- e dose-dependente e preveniu o comportamento nocifensivo induzido por capsaicina, enquanto PKR-/- apresentaram resposta nocifensiva praticamente ausente em ambas as fases herpética e pósherpética. Houve aumento da expressão de PP2A? e da fosforilação de PKR, IKK?/? e eIF2?, durante os períodos herpético e pós-herpético, e de PACT na fase pósherpética. A inibição de PKR promoveu o aumento da fosforilação de P38 em ambas as fases, e redução da fosforilação de PLC?1 acompanhada do retorno da fosforilação de Akt e STAT3 ao nível do grupo controle e o aumento da expressão de Ca-MKII? na fase herpética. Já na fase pós-herpética, reduziu a fosforilação de JNK e Akt e a expressão de Ca-MKII?, retornou a fosforilação de ERK1,2, PLC?1 e STAT3 ao nível do grupo controle e aumentou a expressão de TRPV1. Nossos resultados indicam que a atividade de PKR desempenha papel essencial na hiperalgesia térmica induzida por infecção pelo HSV1 / Double stranded RNA-activated protein kinase (PKR) is a sentinel molecule activated by cellular stress conditions, including viral infections. PKR activation by phosphorylation triggers cascades involved in inflammatory response and protein synthesis suppression. Our previous data suggest that PKR is involved in the inflammatory thermal hyperalgesia. Here we investigated the role played by PKR on thermal hyperalgesia induced by herpes simplex virus type-1 (HSV-1), during herpetic and post-herpetic phases, by combining behavioral, genetic, pharmacological, and molecular methods. Adult male C57bl/6, PKR+/+ and PKR-/- mice were inoculated with HSV-1. Control groups were inoculated with inactive (mock) HSV1. Mechanical allodynia and thermal hyperalgesia were monitored before virus inoculation and 8, 14, 21, and 28 days post-inoculation. The dose- and timeresponse curve and the capsaicin test were performed at 8th and 21st days post virus inoculation. Also in the herpetic and post-herpetic periods, was investigated the expression profile of proteins involved in the PKR signaling pathways (PKR, eIF2?, PACT, IKK and PP2A?), and the effect of PKR inhibition by monitoring PKR, IKK?/?, P38, JNK, ERK1,2, and STAT3 phosphorylation, and Ca-MKII? and TRPV1 expression in the dorsal root ganglia (L3-L6) ipsilaterally to the inoculated paw. Mechanical allodynia and thermal hyperalgesia became evident until 28 days postinnoculation. PKR-/- mice developed mechanical allodynia but not thermal hyperalgesia, when compared with PKR+/+ mice. Systemic PKR inhibition reversed thermal hyperalgesia in a dose and time-dependent manner, and prevented the capsaicin-induced nocifensive behavior, whereas PKR-/- showed no nocifensive behavior almost absent in both herpetic and post-herpetic phases. There was increased expression of PP2A? and the phosphorylation of PKR, IKK?/?, and eIF2?, during herpetic and post-herpetic periods, and PACT in the post-herpetic phase. PKR inhibition increased P38 phosphorylation in both phases, and reduction of PLC?1 phosphorylation together with the return of the Akt and STAT3 phosphorylation to the control group level, and enhanced Ca-MKII? expression in the herpetic phase. At the post-herpetic phase, suppressed JNK and Akt, and Ca-MKII? expression returned ERK1,2, PLC?1 and STAT3 phosphorylation to control group level and increased TRPV1 expression. The data indicate that PKR activity plays an essential role in the HSV-1 infection-induced thermal hyperalgesia

Dor crônica

Neuralgia herpética

Neuralgia pós-herpética

Neuropatia periférica

PKR

Vírus herpes simples tipo 1

Chronic pain

Herpes simplex virus type-1

Herpetic neuralgia

Peripheral neuropathy

PKR

Post-herpetic neuralgia

Catalytic core of respiratory chain NADH-ubiquinone oxidoreductase:roles of the ND1, ND6 and ND4L subunits and mitochondrial disease modelling in <em>Escherichia coli</em>

Pätsi, J. (Jukka)

31 May 2011

Abstract NADH-ubiquinone oxidoreductase (complex I) is one of the largest enzymes in mammals. Seven (ND1-ND6 and ND4L) of its 45 subunits are encoded in mitochondrial DNA, mutations of which are usually behind mitochondrial diseases such as Leber hereditary optic neuropathy (LHON) and MELAS-syndrome. The rest of the genes are located in the nucleus. Bacterial homologs of complex I (NDH-1) consist of only 13&#8211;14 subunits, comprising the catalytic core of the enzyme. These complexes are simpler but perform a similar function. Escherichia coli NDH-1 was employed here to generate amino acid replacements at conserved sites in NuoH, NuoJ and NuoK, counterparts of ND1, ND6 and ND4L, to elucidate their role in complex I. Consequences of homologous amino acid substitutions brought about by ND1-affecting LHON/MELAS-overlap syndrome-associated m.3376G&gt;A and m.3865A&gt;G mutations and the ND6-affecting m.14498T&gt;C substitution associated with LHON were also studied to validate their pathogenicity. Effects of the site-directed mutations were evaluated on the basis of enzyme activity, inhibitor sensitivity and growth phenotype. Highly conserved glutamate-residues 36 and 72 within transmembrane helices of NuoK in positions similar to proton translocating transmembrane proteins were found essential for electron transfer to ubiquinone and growth on medium necessitating normal proton transfer by NDH-1. NuoH and NuoJ replacements at sites corresponding to targets of m.3376G&gt;A and m.14498T&gt;C decreased ubiquinone reductase activity and altered the ubiquinone binding site, while the counterpart of m.3865A&gt;G was without a major effect. Other NuoH and NuoJ mutations studied also affected the interactions of ubiquinone and inhibitors with NDH-1. The results corroborate the pathogenicity of the m.14498T&gt;C and m.3376G&gt;A mutations and demonstrate that the overlap syndrome-associated modification affects complex I in a pattern which appears to combine the effects of separate mutations responsible for LHON and MELAS. Change in ubiquinone binding affinity is a likely pathomechanism of all LHON-associated mutations. Effects of the NuoH, NuoJ and NuoK subunit substitutions also indicate that ND1 and ND6 subunits contribute to the ubiquinone-interacting site of complex I and the site is located in the vicinity of the membrane surface, while ND4L is likely involved in proton pumping activity of the enzyme. / Tiivistelmä 45 alayksiköstä muodostuva NADH-ubikinoni oksidoreduktaasi (kompleksi I) on nisäkkäiden suurimpia entsyymejä. Sen mitokondriaalisessa DNA:ssa koodattujen alayksiköiden ND1-ND6 ja ND4L geeneihin liittyvät mutaatiot ovat yleisiä mitokondriosairauksien, kuten Leberin perinnöllisen näköhermoatrofian (LHON) ja MELAS-oireyhtymän, syitä. Bakteerien vastaava entsyymi (NDH-1) koostuu vain 13&#8211;14 alayksiköstä. Tästä huolimatta sen katalysoima reaktio on samankaltainen kuin kompleksi I:n. NDH-1:n katsotaankin edustavan entsyymin katalyyttistä ydintä. Tässä työssä tutkittiin ND1, ND6 ja ND4L alayksiköiden tehtävää kompleksi I:ssä niiden Escherichia coli bakteerissa olevien vastineiden (NuoH, NuoJ ja NuoK) kohdennetun mutageneesin avulla. Samaa lähestymistapaa käytettiin LHON/MELAS-oireyhtymässä todettujen ND1 alayksikön mutaatioiden, m.3376G&gt;A ja m.3865A&gt;G, ja LHON:ssa havaitun ND6:n m.14498T&gt;C mutaation aiheuttamien aminohappomuutosten seurauksien selvittämiseen. Tehtyjen mutaatioiden vaikutuksia arvioitiin entsyymiaktiivisuus-mittauksin ja kasvukokein. NuoK:n solukalvon läpäisevissä rakenteissa olevien kahden glutamaatti-aminohappotähteen sijainti muistuttaa protoneita kalvon läpi kuljettavissa proteiineissa todettua. NuoK:n glutamaattien havaittiinkin olevan tärkeitä elektronien ja protonien kuljetukselle kompleksi I:ssä. m.3376G&gt;A ja m.14498T&gt;C mutaatioiden aiheuttamien aminohappomuutosten vastineet NDH-1:ssä alensivat NDH-1:n elektroninsiirtoaktiivisuutta ja heikensivät ubikinonin sitoutumista, kun taas m.3865A&gt;G mutaatiolla ei ollut vaikutusta. Muut NuoH ja NuoJ alayksiköihin tehdyt aminohappovaihdokset johtivat huonontuneeseen ubikinonin ja kompleksi I:n inhibiittoreiden sitoutumiseen. Saadut tulokset vahvistavat m.3376G&gt;A ja m.14498T&gt;C mutaatioiden patogeenisyyden. Ne myös osoittavat, että LHON/MELAS-oireyhtymään liitetyn mutaation biokemiallisissa vaikutuksissa yhdistyvät sekä LHON:ssa että MELAS-oireyhtymässä todettujen mutaatioiden seuraukset. Esitetyt tulokset tukevat näkemystä siitä, että ubikinonin ja kompleksi I:n välisessä vuorovaikutuksessa tapahtuva muutos on kaikille LHON:aan liitetyille mutaatioille yhteinen vaikutusmekanismi. NuoH:n, NuoJ:n ja NuoK:n kohdennetusta mutageneesista saatujen tulosten perusteella ND1 ja ND6 alayksiköt ovat osa ubikinonin sitoutumispaikkaa entsyymikompleksissa, kun taas ND4L osallistuu protoninkuljetukseen.

Leber hereditary optic neuropathy

MELAS syndrome

NADH-ubiquinone oxidoreductase

mitochondrial DNA

mitochondrial diseases

oxidative phosphorylation

site-directed mutagenesis

ubiquinone

Leberin hereditaarinen optikusneuropatia

MELAS-oireyhtymä

NADH-ubikinoni oksidoreduktaasi

mitokondrio-DNA

mitokondriotaudit

oksidatiivinen fosforylaatio

suunnattu mutageneesi

ubikinoni