ABSTRACT
ABSTRACT Background: Malfunctioning or damaged mitochondria result in altered energy metabolism, redox equilibrium, and cellular dynamics and is a central point in the pathogenesis of neurological disorders such as Alzheimer's disease, Parkinson's disease, Huntington's disease and Amyotrophic Lateral Sclerosis. Therefore, it is of utmost importance to identify mitochondrial genetic susceptibility markers for neurodegenerative diseases. Potential markers include the respiratory chain enzymes Riboflavin kinase (RFK), Flavin adenine dinucleotide synthetase (FAD), Succinate dehydrogenase B subunit (SDHB), and Cytochrome C1 (CYC1). These enzymes are associated with neuroprotection and neurodegeneration. Objective: To test if variants in genes RFK, FAD, SDHB and CYC1 deviate from Hardy-Weinberg Equilibrium (HWE) in different human mitochondrial haplogroups. Methods: Sequence variants in genes RFK, FAD, SDHB and CYC1 of 2,504 non-affected individuals of the 1,000 genomes project were used for mitochondrial haplogroup assessment and HWE calculations in different mitochondrial haplogroups. Results: We show that RFK variants deviate from HWE in haplogroups G, H, L, V and W, variants of FAD in haplogroups B, J, L, U, and C, variants of SDHB in relation to the C, W, and A and CYC1 variants in B, L, U, D, and T. HWE deviation indicates action of selective pressures and genetic drift. Conclusions: HWE deviation of particular variants in relation to global populational HWE, could be, at least in part, associated with the differential susceptibility of specific populations and ethnicities to neurodegenerative diseases. Our data might contribute to the epidemiology and diagnostic/prognostic methods for neurodegenerative diseases.
RESUMO Introdução: Mitocôndrias defeituosas ou danificadas resultam em alterações do metabolismo energético, equilíbrio redox e dinâmica celular e são, portanto, identificadas como o ponto central da patogênese em muitos distúrbios neurológicos, como a doença de Alzheimer, a doença de Parkinson, a doença de Huntington e a Esclerose Lateral Amiotrófica. Portanto, é de fundamental importância identificar marcadores de susceptibilidade genética mitocondrial para doenças neurodegenerativas. Entre os potenciais marcadores relevantes estão as enzimas da cadeia respiratória riboflavina quinase (RFK), flavina adenina dinucleotídeo sintetase (FAD), succinato desidrogenase subunidade B (SDHB) e citocromo C1 (CYC1). Estas enzimas estão associadas à neuroproteção e à neurodegeneração. Objetivo: Testar se variantes nas sequências dos genes RFK, FAD, SDHB e CYC1 desviam do Equilíbrio de Hardy-Weinberg (HWE) em diferentes haplogrupos mitocondriais humanos. Métodos: Neste trabalho utilizamos os variantes nos genes RFK, FAD, SDHB e CYC1 de sequências de 2.504 indivíduos não afetados do projeto de 1.000 genomas para o cálculo dos valores de HWE em diferentes haplogrupos mitocondriais. Resultados: As variantes de RFK desviam de HWE nos haplogrupos G, H, L, V e W, variantes de FAD nos haplogrupos B, J, L, U e C, variantes de SDHB em relação às variantes C, W e A e CYC1 em B, L, U, D e T. O desvio de HWE indica a ação de pressões seletivas e desvio genético. Conclusões: O desvio do HWE de variantes particulares em relação ao HWE populacional global poderia estar, pelo menos em parte, associado à suscetibilidade diferencial de populações e etnias específicas a doenças neurodegenerativas. Nossos dados podem contribuir para a epidemiologia e métodos diagnósticos/prognósticos para doenças neurodegenerativas.
Subject(s)
Humans , Neurodegenerative Diseases , Amyotrophic Lateral Sclerosis , Energy Metabolism , Neuroprotection , Mitochondria/chemistryABSTRACT
Mitochondria are central players in cell metabolism, responsible for the vast majority of ATP production in most cells. Although originally thought to be passive organelles focused only in keeping cellular ATP at adequate levels, complex interplay between mitochondrial function and cell signaling has been largely recognized over the last decades. Not surprisingly, given their role, changes in nutritional status promoted by chronic interventions like caloric restriction or short-term situations like fasting in animals or nutrient deprivation in cultured cells are one of the main factors that can activate those signaling mechanisms. One particular way in which this mitochondria-cell crosstalk can occur is through mitochondrial Ca2+ handling, a process in which Ca2+ signals generated by the cell are able to translate into elevations in mitochondrial matrix [Ca2+] due to the presence of the mitochondrial Ca2+ uniporter in the organelle. While the impact of mitochondrial Ca2+ handling on cellular function has been widely studied, the conditions which can modulate the process of mitochondrial Ca2+ handling itself are still not well characterized. In this work, we sought to test the effects of different interventions linked to nutritional status on mitochondrial Ca2+ handling. We found that caloric restriction, physiological fasting and modulations of mitochondrial dynamics resulted in modulation of mitochondrial Ca2+ handling through changes in their maximal Ca2+ retention capacity or Ca2+ uptake rates. These changes were, measured by following mitochondrial Ca2+ uptake using different strategies, employing the fluorescent Ca2+ probe Ca2+ Green 5N for experiments in isolated mitochondria and permeabilized cells and the cytosolic probe Fura2-AM in intact cells. Caloric restriction resulted in higher calcium uptake and retention in liver mitochondria, protecting against pathological conditions of Ca2+ overload during ischemia/reperfusion. On the other hand, overnight and short term fasting resulted in lower mitochondrial Ca2+ retention and oxidative phosphorylation capacity in the liver. Modulating mitochondrial morpholoy in C2C12 myoblasts showed that more fragmented mitochondria were less capable of taking up Ca2+, while more fusioned mitochondria showed the opposite phenotype. This modulation in Ca2+ handling through changes in mitochondrial morphology interfered with the process of Store-Operated Ca2+ entry in the cells, showing that these modulations can have impacts in physiological contexts as well. Overall, this work both establishes novel mechanisms of modulation of mitochondrial Ca2+ handling and demonstrates their relevance both in pathology and normal cellular physiology
Mitocôndrias possuem um papel central no metabolismo das células, sendo responsáveis pela maioria da produção de ATP na maioria dos tipos celulares. Embora originalmente se pensasse nas mitocôndrias como organelas estáticas, focadas somente em manter os níveis adequados de ATP na célula, a interação entre a função mitocondrial e a sinalização celular tem sido fortemente reconhecida nas ultimas décadas. Dado este papel, não é surpreendente que mudanças no estado nutricional, tanto crônicas como na restrição calórica quanto em situações como o jejum em animais e a privação de nutrientes em cultura de células foram demonstradas como sendo um dos principais fatores que podem ativar estes mecanismos de sinalização. Uma das formas em que esta interação entre a mitocôndria e a célula ocorre é através do manejo de Ca2+ mitocondrial, um processo em que sinais de Ca2+ gerados pela célula podem resultar em aumentos na [Ca2+] na matriz mitocondrial devido à presença do uniportador de Ca2+ mitocondrial na organelaEmbora o impacto do manejo de Ca2+ mitocondrial na função da célula tenha sido amplamente estudado, a regulação do processo de manejo de Ca2+ mitocondrial em si não é bem conhecida. Neste trabalho, nós nos propusemos a testar os efeitos de diferentes intervenções ligadas ao estado nutricional no manejo de Ca2+ mitocondrial e o possível impacto destas modulações nacapacidade de retenção e na taxa de captação de Ca2+ mitochondrial. As intervenções estudadas foram a restrição calórica, jejum e mudanças na dinâmica mitocondrial, e todas elas resultando em mudanças no manejo de Ca2+ mitocondrial, que foram medidos acompanhando a captação de Ca2+ em mitocôndrias isoladas ou células permeabilizadas utilizando a sonda Ca2+ Green 5N e em células intactas utilizando a sonda de Ca2+ citosólica Fura2-AM. Enquanto a restrição calórica resultou em uma maior capacidade de retenção de Ca2+ e em maiores taxas de captação, protegendo contra as condições patológicas de desregulação de Ca2+ observadas durante a isquemia/reperfusão, o jejum curto ou pela duração da noite resultou em uma diminuição na capacidade de retenção de Ca2+ e na oxidação fosforilativa mitocondriais. As mudanças observadas modulando a dinâmica mitocôndria (feitas utilizando-se mioblastos da linhagem C2C12) revelaram que mitocôndrias mais fragmentadas são menos capazes de captar Ca2+, enquanto mitocôndrias mais fusionadas possuem o fenótipo oposto. Essas mudanças no manejo de Ca2+ mitocondrial interferem com o processo de Store-Operated Ca2+ entry nestas células, demonstrando que essas modulações da captação de Ca2+ mitocondrial também podem ser relevantes em contextos fisiológicos. Em resumo, este trabalho ajudou a estabelecer novos mecanismos de modulação do manejo de Ca2+ mitocondrial que podem ser relevantes tanto em condições patológicas quanto na fisiologia normal das células
Subject(s)
Calcium/analysis , Nutritional Status , Mitochondrial Dynamics , Cell Death/immunology , Myoblasts/classification , Mitochondria/chemistryABSTRACT
Introduction: Photodynamic therapy (PDT) using 5-aminolevulinic acid-induced protoporphyrin IX (ALA-PpIX) constitutes an interesting alternative for cutaneous leishmaniasis treatment. Objective: To evaluate the production of PpIXbased on the administration of ALA and MAL and the effect of ALA-PDTat cellular level on non-infected and infected THP-1 cells using Leishmania ( Viannia ) panamensis or Leishmania ( Leishmania ) infantum (syn Leishmania chagasi ) parasites. Materials and methods: Protoporphyrin IX (PpIX) production and mitochondrial colocalization were evaluated by confocal microscopy. Cell toxicities were evaluated after treatment with the compounds, followed by light irradiation (597-752 nm) at 2.5 J/cm 2 fluency using a colorimetric MTT assay for THP-1 cells and a standard microscopic analysis of parasites. Results were expressed as compound concentration activity against 50% of cells or parasites (CC 50 or IC 50 ). Results: ALA or MAL induced an endogenous PpIX with a red fluorescence localized mainly in the mitochondria inside human cells. ALA and MAL-PDT induced a similar range of toxicities on THP-1 cells (CC 50 0.16±0.01mM and 0.33±0.019 mM, respectively) without any apparent inhibition of intracellular parasites in the infected cells as compared to untreated controls. Exogenous PpIX-PDT was toxic to THP-1 cells (CC 50 0.00032±0.00002 mM), L. (L.) infantum (IC 50 0.003±0.0001 mM) and L. (V.) panamensis (IC 50 0.024±0.0001 mM) promastigotes. Conclusions: Despite the effectiveness of exogenous PpIX on promastigotes and the production of PpIX by human infected cells, treatment with ALA or MAL before irradiation was unable to completely destroy L. (L.) infantum or L. (V.) panamensis intracellular amastigotes.
Introducción. El tratamiento fotodinámico con ácido 5-aminolevulínico como inductor de la protoporfirina IX (ALA-PpIX) constituye una alternativa interesante en el tratamiento de la leishmaniasis cutánea. Objetivo. Evaluar la producción de protoporfirina IX (PpIX) a partir de la administración de ALA o MAL y el efecto de la PDT con ALA a nivel celular en células THP-1 no infectadas e infectadas con Leishmania ( Viannia ) panamensis o Leishmania ( Leishmania ) infantum (syn. Leishmania chagasi ). Materiales y métodos. La producción de protoporfirina IX y su colocalización´ mitocondrial se evaluaron mediante microscopía confocal´. Se evaluó la toxicidad celular después del tratamiento con los compuestos y la aplicación de irradiación de luz (597-752 nm) en una fluencia de 2,5 J/cm 2 mediante el empleo de la prueba colorimétrica con metil-tiazol-tetrazolio (MTT) en las células, y de métodos microscópicos estándar en los parásitos. Los resultados se expresaron como la concentración del compuesto activo en el 50 % de las células o parásitos (CC 50 o CI 50 ). Resultados. El ácido aminolevulínico o el metil-5-aminolevulinato indujeron la protoporfirina IX endógena en células humanas, y se observó fluorescencia de color rojo en las mitocondrias. La actividad del ácido aminolevulínico y del metil-5-aminolevulinato utilizados con terapia fotodinámica fue similar en las células THP-1 (CC 50 0,16±0,01 mM y 0,33±0,019 mM, respectivamente) y, aparentemente, no inhibió los parásitos en las células infectadas, en comparación con los controles. El tratamiento exógeno con protoporfirina IX y terapia fotodinámica fue tóxico para las células THP-1 (CC 50 0,00032 ±0,00002 mM) y para los promastigotes de L. (L .) infantum (IC 50 0,003±0,0001 mM) y L. ( V .) panamensis (CI 50 0,024±0,0001 mM). Conclusiones. A pesar de la fotoactividad´ del tratamiento con protoporfirina IX en promastigotes y de su producción después del tratamiento con ácido aminolevulínico y metil-5-aminolevulinato en las células infectadas con Leishmania , no se observó daño en los amastigotes presentes en las células de L. ( L .) infantum o L . ( V .) panamensis .
Subject(s)
Humans , Aminolevulinic Acid/analogs & derivatives , Aminolevulinic Acid/pharmacology , Leishmania guyanensis/drug effects , Leishmania infantum/drug effects , Monocytes/drug effects , Photochemotherapy , Photosensitizing Agents/pharmacology , Protoporphyrins/analysis , Subcellular Fractions/drug effects , Aminolevulinic Acid/radiation effects , Amphotericin B/pharmacology , Cell Line, Tumor , Colorimetry , Leukemia, Monocytic, Acute/pathology , Lysosomes/chemistry , Microscopy, Fluorescence , Mitochondria/chemistry , Monocytes/parasitology , Monocytes/ultrastructure , Photosensitizing Agents/radiation effects , Species Specificity , Subcellular Fractions/chemistryABSTRACT
A restrição calórica (RC) é uma intervenção dietética capaz de estender a longevidade de vários organismos. O modelo para RC em Saccharomyces cerevisiae consiste da diminuição da concentração de glicose no meio de cultura e mostra um aumentado tanto do tempo de vida cronológico quanto replicativo. Nosso objetivo foi investigar experimentalmente a ação da RC, focando principalmente nas causas e consequências das modificações de geração de EROs mitocondriais e como estas estão associadas ao processo de envelhecimento. Em um primeiro período de estudos, verificamos quais as fontes mitocondriais de EROs, e comprovamos que uma quantidade significativa se origina de proteínas da matriz mitocondrial, e não da cadeia de transporte de elétrons. Nós estudamos a participação de glicose e de outras fontes de carbono sobre o tempo de vida cronológico em leveduras e mostramos que o aumento da longevidade promovida pela RC está associado à uma mudança de metabolismo fermentativo para respiratório, com participação da via de sinalização de glicose. No estágio realizado no laboratório do Professor Francis Sluse na Université de Liegè, Bélgica, estudamos a ação da RC em leveduras focando nas consequências das modificações no proteoma mitocondrial. Em nosso estudo proteômico, encontramos grandes modificações em proteínas envolvidas com o metabolismo de aminoácidos. Monitoramos a atividade de enzimas relacionadas ao metabolismo de aminoácidos e o tempo de vida cronológico de S. cerevisiae e as mutantes nulas bat2Δ, gdh1Δ, gdh2Δ e gdh3Δ, que codificam a aminotransferase de aminoácidos de cadeia ramificada citosólica, NADP glutamato desidrogenase citosólica, a NAD glutamato desidrogenase mitocondrial, e a NADP glutamato desidrogenase mitocondrial, respectivamente. A atividade da NAD glutamato desidrogenase é aumentada em RC, mas a de NADP glutamato desidrogenase decresce em células controle. Aumentos do tempo de vida cronológico foram observados nas mutantes...
Calorie restriction (CR) is a dietary intervention capable of extending lifespans in a wide range of organisms. A yeast model of CR has been developed in which limiting the concentration of glucose in growth media of Saccharomyces cerevisiae leads to enhanced chronological and replicative life spans. Our aim was to experimentally investigate the effects of CR, focusing mainly on the causes and consequences of changes in mitochondrial reactive oxygen species (ROS) generation and how these are associated with the aging process. Initially, we looked for sources of mitochondrial ROS, and found that a significant amount of ROS comes from mitochondrial matrix enzymes and not from the electron transport chain. We studied the participation of glucose and other carbon sources in chronological lifespan and show that increased longevity promoted by CR is associated with a metabolism change from fermentation to respiration, with participation of glucose repression pathway. During studies performed in the laboratory of Professor Francis Sluse at the Université de Liège, Belgium, we studied the effect of CR in yeast with focus on the consequences of changes in the mitochondrial proteome. We found large proteomic changes in proteins involved in amino acid metabolism. We monitored the activity of enzymes related to amino acid metabolism and chronological life span of S. cerevisiae null mutants bat2Δ, gdh1Δ, gdh2Δ, and gdh3Δ, which encode for the cytosolic branched-chain amino acid aminotransferase, cytosolic NADP glutamate dehydrogenase, mitochondrial NAD glutamate dehydrogenase and mitochondrial NADP glutamate dehydrogenase, respectively. The activity of NAD glutamate dehydrogenase is increased in CR, but NADP glutamate dehydrogenase decreases in control cells. Increases in chronological life span due to RC were observed in bat2Δ and gdh1Δ mutants, but no significant difference was found in Gdh2p and Gdh3p null mutants in the stationary phase
La restriction calorique (RC) est une intervention diététique capable de prolonger la durée de vie dans divers organismes. Un modèle de RC pour la levure a été developpé dans lequel limiter la concentration de glucose dans le milieu de culture de Saccharomyces cerevisiae a montré une augmentation de vieillessement chronologique et réplicative. Notre objectif était détudierexpérimentalement leffet de la RC, en se concentrant principalement sur les causes et les conséquences des changements dans la production des espèces doxygène réactive (ROS) mitochondriales et de la façon dont elles sont associée au processus de vieillessement. Dans une première période détudes, qui a trouvé la source de ROS mitochondriale, nous montrons quune quantité importante vient denzyme de la matrice et pas de la chaîne de transport délectrons. Nous avons étudié la participation de glucose et dautres sources de carbone sur le vieillissement chronologique dans la levure et nous avons montré que laugmentation de la longévité promure par RC est associée à un changement du métabolisme fermentaire à respiratoire, avec la participation de la voie de signalisation du glucose. Dans le laboratoire du professeur Francis Sluse à lUniversité de Liège, en Belgique, nous avons étudié leffet du RC dans la levure en se concentrant sur les conséquences des changements du protéome mitochondrial. Dans notre étude, nous avons constaté de grands changements des protéines impliquées dans le métabolisme des acides amines. Nous avons surveillé lactivité des enzymes liées au métabolisme des acides aminés et le vieillissement chronologique de S. cerevisiae et des mutants nul bat2Δ, gdh1Δ, gdh2Δ et gdh3Δ, qui codent aminotransférase pour les acides aminés à chaîne ramifiée cytosolique, NADP glutamate déshydrogénase cytologique, NAD glutamate déshydrogénase mitochondriale et NADP glutamate déshydrogénase mitochondriale, respectivement. Lactivité de la NAD glutamate...
Subject(s)
Caloric Restriction , Mitochondria/chemistry , Saccharomyces cerevisiae/genetics , Time Factors , Amino Acids/metabolism , Dihydrouracil Dehydrogenase (NADP) , Reactive Oxygen Species , Proteome/analysisABSTRACT
Apoptosis within the placenta is increased in pregnancies complicated by pre-eclampsia [PE].This study aimed at evaluating the mitochondrial pathway of apoptosis in placenta of pregnant women with pre-eclampsia and correlate it with severity and pregnancy outcome. Apoptosis was assessed by measuring DNA fragmentation%,Bcl-2, p53 and caspase-9 in placental tissues from 25 pregnancies complicated by pre-eclampsia, and 25 placentas of normal pregnancy [NP]. DNA fragmentation, p53 and caspase-9, were significantly increased while, Bcl-2 was significantly decreased in the placenta of pre-eclampsia group compared to control. No significant difference between mild and severe pre-eclampsia subgroups regarding these parameters could be found. DNA fragmentation was negatively correlated with Bcl-2 in PE group. Moreover, DNA fragmentation was negatively correlated with maternal age in both PE and control groups. A significant positive correlation between placental DNA fragmentation and gestational age in the NP group was observed. A significant negative correlation between caspase9 activity, and fetal weight in PE group was found. It can be concluded that Hypoxia and ischemia induced by pre-eclampsia, up regulate p53 and reduce Bcl-2 expression with activation of caspase-9 and increasing DNA fragmentation in placental tissue. These results implicate the mitochondrial pathway in enhancing apoptosis in preeclamptic placenta and affecting fetal outcome but not the severity
Subject(s)
Humans , Female , Apoptosis , Mitochondria/chemistry , DNA Fragmentation , Caspase 9 , FemaleABSTRACT
Aluminium has a unique combination of physical and chemical properties which has enabled man to put this metal to very wide and varied use. However, prolonged exposure to aluminium ions may lead to adverse health effects. In this study, we evaluated the effects of dietary aluminium on the protein composition and the intrinsic activity of cytochrome oxidase (COX) for brain mitochondria. New Zealand white rabbits were maintained on a diet of commercial rabbit pellets and distilled water for a period of 12 weeks. For the experimental group, AlCl3, 330mg/kg/L was added to the drinking water. When compared to the control, mitochondria isolated from the brains of the AlCl3 fed rabbits showed no change in Km but an approximate 35% decrease in both the low and high affinity Vmax values. Also, whereas the protein composition of the mitochondria from both sources appeared to be normal, isolation of highly purified COX proved to be difficult and for the AICI3 fed rabbits, a number of the enzyme's low molecular weight subunits were absent. These results appear to confirm a relationship between long term aluminium consumption and low brain COX activity; they further suggest that an altered COX structure may be the cause of the low enzymic activity.
El aluminio posee una combinación única de las propiedades físicas y químicas que ha permitido al ser humano hacer un uso amplio y variado de este metal. Sin embargo, un número de estudios recientes, sugiere que la exposición prolongada a los iones de aluminio puede tener efectos nocivos sobre la salud. En el presente estudio, evaluamos los efectos del aluminio dietético sobre la composición proteínica y la actividad intrínseca de la oxidasa citocrómica (COX) para la mitocondria cerebral. Conejos blancos de Nueva Zelanda, fueron mantenidos con una dieta de alimento para conejos y agua destilada por un período de 12 semanas. Para el grupo experimental AlCl3, 330mg/kg/L fueron añadidos al agua potable. En comparación con el grupo de control, las mitocondrias aisladas de los cerebros de los conejos alimentados con AlCl3 no mostraron cambios en Km pero hubo una disminución de aproximadamente 35% tanto en los valores Vmax de baja y alta afinidad. Por otro lado, mientras que la composición proteica de las mitocondrias de ambas fuentes parecía ser normal, resultó difícil aislar el COX altamente purificado y un número de enzimas de subunidades de bajo peso molecular MMMM estuvieron ausentes. Estos resultados parecen confirmar una relación entre el consumo de aluminio a largo plazo y la baja actividad del COX del cerebro. Asimismo, sugieren que una alteración de la estructura del COX puede ser la causa de una baja actividad enzimática.
Subject(s)
Animals , Rabbits , Aluminum Compounds/toxicity , Brain/metabolism , Chlorides/toxicity , Electron Transport Complex IV/drug effects , Electron Transport Complex IV/metabolism , Mitochondria/enzymology , Administration, Oral , Aluminum Compounds/administration & dosage , Astringents/administration & dosage , Astringents/toxicity , Brain Chemistry/drug effects , Brain/enzymology , Chlorides/administration & dosage , Mitochondria/chemistryABSTRACT
Partial cytochrome b DNA sequences for 62 Triatoma infestans were analyzed to determine the degree of genetic variation present in populations of this insect in the northwest region of Chuquisaca, Bolivia. A total of seven haplotypes were detected in the localities sampled. The phylogenetic relationship and population genetic structure of the haplotypes found in this region, indicate that there is greater variation in this relatively small region of Bolivia than what has been previously reported by studies using the same gene fragment, for more distant geographic areas of this country. In addition, a comparison of rural and peri-urban localities, indicate that there is no difference in the genetic variation of T. infestans between these two environments.
Subject(s)
Animals , Cytochromes b/genetics , Genetic Variation , Haplotypes/genetics , Mitochondria/chemistry , Triatoma/genetics , Bolivia , Cytochromes b/analysis , DNA, Protozoan/genetics , Phylogeny , Sequence Analysis, DNA , Triatoma/chemistryABSTRACT
The use of chemical pesticides and herbicides has increased environmental pollution and affected ichthyofauna in the watersheds where they are used.We studied the effect of an herbicide, triazine, on the kidneys of two species (Caquetaia kraussii and Colossoma macropomum )widely found in Caribbean and South American rivers.In Venezuela,these species are abundant and have a high aquaculture potential because they may be cultured and reproduced in captivity.Four kidney samples from juveniles of each species exposed to the herbicide were examined by Transmission Electron Microscopy.Kidney tubule alterations included loss of plasmalemma and cell interdigitations, misshaped mitochondria,decrease in rough endoplasmic reticulum and free polysomes,and the presence of autophagic vacuoles and primary lysosomes.These alterations at the cellular level may explain fish behaviour in terms of kidney tubule pathology,and relative amounts and conditions of organelles within affected cells
Subject(s)
Animals , Atrazine/toxicity , Fisheries , Fishes , Herbicides/toxicity , Kidney/drug effects , Water Pollutants, Chemical/toxicity , Atrazine/analysis , Biomarkers/analysis , Cichlids , Herbicides/analysis , Kidney Tubules/chemistry , Kidney Tubules/drug effects , Kidney/chemistry , Kidney/ultrastructure , Mitochondria/chemistry , Mitochondria/drug effects , VenezuelaABSTRACT
Epilepsy affects more than 0.5% of the world population and is known to be associated with a large genetic component eliciting an electrical hyperexcitability in the central nervous system. However, its pathogenic mechanisms remain poorly understood. In order to gain greater molecular incite in the pathogenesis in epilepsy, we analyzed proteomes of human cerebral cortices. Quantitative proteome analysis was used to compare signals corresponding to individual proteins between epileptic cerebral cortices from patients with temporal lobe epilepsy and age-matched non-epileptic subjects. To minimize individual variations, gender and age of the patients were matched. Changes of several spots were consistent among 6 pairs of epileptic patients and nonepileptic subjects. One of the spots was identified as the mitochondrial type Mn-superoxide dismutase (Mn-SOD) confirmed by Western blot analysis with Mn-SOD antibody and enzyme activity assay. Such results were agreeable with chemical and physical parameters given by the 2-dimensional electrophoresis (2-DE) gel. Mn-SOD was consistently down-regulated in epileptic cerebral cortices compared with those of nonepileptic subjects. Our results demonstrate a clear link between pathogenesis of epilepsy and SOD. Additionally, we identified four proteins that were consistently over-expressed in all epileptic temporal neocortices specimens and the other four proteins that were found to be expressed less than non-epileptic control subjects. These proteomic data provide cellular markers in the understanding mechanism of the epilepsy pathogenesis.
Subject(s)
Adult , Female , Humans , Male , Middle Aged , Biomarkers/analysis , Brain Chemistry , Case-Control Studies , Cerebral Cortex/chemistry , Down-Regulation , Electrophoresis, Gel, Two-Dimensional , Epilepsy/genetics , Mitochondria/chemistry , Nerve Tissue Proteins/chemistry , Proteomics , Superoxide Dismutase/analysis , Up-RegulationABSTRACT
Apoptosis is regulated by interaction of antiapoptotic Bcl-2 family proteins with various proapoptotic proteins, several of which are also members of the Bcl-2 family. BNIP3 (formerly NIP3) is a proapoptotic mitochondrial protein classified in the Bcl-2 family based on limited sequence homology-3 (BH3) domain and COOH-terminal transmembrane domain. Sequence comparison of BNIP3 has indicated that there are several BNIP3 human homologs of this protein, like BNIP3L, Nix and BNIP3. We have cloned a new member of BNIP3 family from the cDNA library prepared from human dermal papilla cells and designated as BNIP3h. BNIP3h shows substantial homology with other BNIP3 family proteins. BNIP3h induced apoptosis from 24 hours after transfection in MCF7 cell lines and its apoptosis inducing activity is extended until 72 hours after transfection.
Subject(s)
Humans , Amino Acid Sequence , Apoptosis/physiology , Base Sequence , Cells, Cultured , Cloning, Molecular , Dermis/chemistry , Membrane Proteins/chemistry , Mitochondria/chemistry , Molecular Sequence Data , Multigene Family , Sequence Alignment , Tissue Distribution , Transfection , Tumor Cells, CulturedABSTRACT
Purification of mitochondria and mitochondrial protein complexes from green tissues is often severely impaired by the presence of chloroplasts and their proteins. Here we present a method which allows analysis of respiratory protein complexes from potato leaves. The procedure includes the preparation of an organellar fraction specifically enriched in mitochondria and the separation of organellar protein complexes by blue-native polyacrylamide gel electrophoresis (BN-PAGE). For the first time mitochondrial and chloroplast protein complexes have been resolved simultaneously in a native gel. BN-PAGE allowed the separation of eleven bands, including the mitochondrial NADH-dehydrogenase, the bc1 complex and the mitochondrial F1-ATP synthase as well as the chloroplast F1-ATP synthase, the cytochrome b6f complex, the two photosystems and the light harvesting complex. The resolution of the protein complexes in the first dimension was good enough to allow identification of all subunits of individual complexes in the second dimension under denaturing conditions. Thus, BN-PAGE offers an opportunity to analyze mitochondrial and chloroplast protein complexes from a single preparation from very small amounts of tissue. The implications of our findings, for studies on protein expression and turnover in different tissues and developmental stages, are discussed.
Subject(s)
Chloroplasts/chemistry , Electrophoresis, Gel, Two-Dimensional , Membrane Proteins/chemistry , Mitochondria/chemistry , Plant Leaves/chemistry , Plant Proteins/chemistry , Solanum tuberosum/chemistryABSTRACT
The two developmental stages of human malarial parasite Plasmodium falciparum, asexual and sexual blood stages, were continuously cultivated in vitro. Both asexual and sexual stages of the parasites were assayed for mitochondrial oxygen consumption by using a polarographic assay. The rate of oxygen consumption by both stages was found to be relatively low, and was not much different. Furthermore, the mitochondrial oxygen consumption by both stages was inhibited to various degrees by mammalian mitochondrial inhibitors that targeted each component of complexes I- IV of the respiratory system. The oxygen consumption by both stages was also affected by 5-fluoroorotate, a known inhibitor of enzyme dihydroorotate dehydrogenase of the pyrimidine pathway and by an antimalarial drug atovaquone that acted specifically on mitochondrial complex III of the parasite. Moreover, antimalarials primaquine and artemisinin had inhibitory effects on the oxygen consumption by both stages of the parasites. Our results suggest that P. falciparum in both developmental stages have functional mitochondria that operate a classical electron transport system, containing complexes I-IV, and linked to the pyrimidine biosynthetic pathway.
Subject(s)
Animals , Dose-Response Relationship, Drug , Electron Transport/drug effects , Enzyme Inhibitors/pharmacology , Humans , Life Cycle Stages/drug effects , Mitochondria/chemistry , Oxygen Consumption/drug effects , Plasmodium falciparum/growth & development , ThailandABSTRACT
Se presenta la prevalencia de hipocausia neurosensoriales en 24 familiares ubicados en diferentes poblados del estado Nva. Esparta. De 329 individuos estudiados, 27 (8,9 por ciento) mostraron diferentes grados de transtornos auditivos, 16 de los cuales se asociaron a complejos sindromáticos, siendo el más frecuente la renitis pigmentosa correspondiente clínicamente al síndrome de Usher