Propagação in vivo e in vitro de Cissus sicyoides, uma planta medicinal.

O estudo da propagação de espécies utilizadas na medicina popular tem sido intensificado nos últimos anos devido ao crescente investimento em pesquisas para a descoberta de novos fármacos e da utilização da fitoterapia como um meio alternativo. O objetivo do trabalho foi a propagação in vivo e in vitro (estabelecimento e multiplicação) de Cissus sicyoides. Plantas mantidas em casa de vegetação forneceram estacas com 10 e 20 cm de comprimento, as quais foram tratadas com 0, 80 ou 160 mg/l de AIB, com ou sem sacarose + ácido bórico, por duas horas. Para o estabelecimento in vitro, após desinfestação, segmentos nodais com 10 mm de comprimento foram inoculados em meio de cultura sólido (MS), com diferentes concentrações de cinetina, BAP e ANA. Para a multiplicação in vitro, segmentos nodais com 10 mm foram inoculados em meio MS, suplementado com diferentes concentrações de BAP e ANA, e ANA e cinetina. Na propagação in vivo as estacas com 10 cm de comprimento apresentaram maior eficiência no enraizamento quando tratadas com 160 mg/l de AIB. In vitro os explantes foram melhor estabelecidos e multiplicados em meio de cultura suplementado com cinetina e ANA, que proporcionaram maior indução de gemas, crescimento em altura e ausência de calos na base das plântulas

Robust constrained model predictive control based on parameter-dependent Lyapunov functions

The problem of robust constrained model predictive control (MPC) of systems with polytopic uncertainties is considered in this paper. New sufficient conditions for the existence of parameter-dependent Lyapunov functions are proposed in terms of linear matrix inequalities (LMIs), which will reduce the conservativeness resulting from using a single Lyapunov function. At each sampling instant, the corresponding parameter-dependent Lyapunov function is an upper bound for a worst-case objective function, which can be minimized using the LMI convex optimization approach. Based on the solution of optimization at each sampling instant, the corresponding state feedback controller is designed, which can guarantee that the resulting closed-loop system is robustly asymptotically stable. In addition, the feedback controller will meet the specifications for systems with input or output constraints, for all admissible time-varying parameter uncertainties. Numerical examples are presented to demonstrate the effectiveness of the proposed techniques

Influence of nitrogen and phosphorus in the biomass production and induction of mucilage in insulina plants

The influence of nitrogen and phosphorus fertilization on production of biomass and mucilage in Cissus sicyoides plants was evaluated. 45-day old plants obtained from cuttings were planted in pots with capacity for 5 Kg of soil, having as substrate allic cambisol soil, medium texture from Nazareno (Brazil). Basic fertilization with macro and micronutrients was done. Nitrogen doses (0; 40; 80; 160 and 200 mg of N/Kg of soil) and phosphorus doses (50 and 150 mg of P/Kg of soil) were evaluated. The experiment was laid out in a complete randomised factorial scheme of 5 x 2, with four replications. The research was carried out in a greenhouse during 90 days, being evaluated the dry matter of leaves, stalks and roots; chemicals characteristics and mucilage were determined. Between nitrogen and phosphorus doses and the production of dry matter of leaves was observed interaction. Higher biomass gain occurred with higher nitrogen dose of 150 mg P/Kg of soil. The mucilage production increased with increasing doses of nitrogen and phosphorus, reaching a higher content at the same conditions that gave a higher leaves biomass gain and total aerial part.Foi verificada a influência da adubação com nitrogênio e fósforo na produção de biomassa e de mucilagem em plantas de Cissus sicyoides. Plantas com 45 dias, formadas pelo método de estaquia, foram plantadas em vasos com capacidade para 5 kg de solo, contendo como substrato um Cambissolo álico, textura média, do município de Nazareno-MG. Foi realizada uma adubação básica com macro e micronutrientes, variando apenas as concentrações de nitrogênio e fósforo. O experimento consistiu de 5 doses de N (0; 40; 80; 160 e 200 mg de N/kg de solo) e duas doses de P (50 e 150 mg de P/kg de solo), com 4 repetições. O delineamento foi inteiramente casualizado, em esquema fatorial de 5 x 2. O experimento foi conduzido em casa de vegetação por 90 dias, onde avaliou-se o peso de matéria seca de folha, caule e raiz; características químicas e mucilagem da parte aérea. Houve interação entre as concentrações de nitrogênio e fósforo para a produção de matéria seca foliar, sendo que os maiores ganhos de biomassa ocorreram nas maiores doses de N com 150 mg de P/kg solo. A produção de mucilagem respondeu positivamente ao aumento das concentrações de nitrogênio e fósforo, atingindo o maior conteúdo nas mesmas concentrações que proporcionaram o maior ganho de biomassa foliar e de parte aérea total.53654

Effects of Inhibiting CoQ10 Biosynthesis with 4-nitrobenzoate in Human Fibroblasts

Coenzyme Q10 (CoQ10) is a potent lipophilic antioxidant in cell membranes and a carrier of electrons in the mitochondrial respiratory chain. We previously characterized the effects of varying severities of CoQ10 deficiency on ROS production and mitochondrial bioenergetics in cells harboring genetic defects of CoQ10 biosynthesis. We observed a unimodal distribution of ROS production with CoQ10 deficiency: cells with <20% of CoQ10 and 50–70% of CoQ10 did not generate excess ROS while cells with 30–45% of CoQ10 showed increased ROS production and lipid peroxidation. Because our previous studies were limited to a small number of mutant cell lines with heterogeneous molecular defects, here, we treated 5 control and 2 mildly CoQ10 deficient fibroblasts with varying doses of 4-nitrobenzoate (4-NB), an analog of 4-hydroxybenzoate (4-HB) and inhibitor of 4-para-hydroxybenzoate:polyprenyl transferase (COQ2) to induce a range of CoQ10 deficiencies. Our results support the concept that the degree of CoQ10 deficiency in cells dictates the extent of ATP synthesis defects and ROS production and that 40–50% residual CoQ10 produces maximal oxidative stress and cell death

Impaired Nuclear Nrf2 Translocation Undermines the Oxidative Stress Response in Friedreich Ataxia

BACKGROUND: Friedreich ataxia originates from a decrease in mitochondrial frataxin, which causes the death of a subset of neurons. The biochemical hallmarks of the disease include low activity of the iron sulfur cluster-containing proteins (ISP) and impairment of antioxidant defense mechanisms that may play a major role in disease progression. METHODOLOGY/PRINCIPAL FINDINGS: We thus investigated signaling pathways involved in antioxidant defense mechanisms. We showed that cultured fibroblasts from patients with Friedreich ataxia exhibited hypersensitivity to oxidative insults because of an impairment in the Nrf2 signaling pathway, which led to faulty induction of antioxidant enzymes. This impairment originated from previously reported actin remodeling by hydrogen peroxide. CONCLUSIONS/SIGNIFICANCE: Thus, the defective machinery for ISP synthesis by causing mitochondrial iron dysmetabolism increases hydrogen peroxide production that accounts for the increased susceptibility to oxidative stress

Idebenone and Resveratrol Extend Lifespan and Improve Motor Function of HtrA2 Knockout Mice

Heterozygous loss-of-function mutation of the human gene for the mitochondrial protease HtrA2 has been associated with increased risk to develop mitochondrial dysfunction, a process known to contribute to neurodegenerative disorders such as Huntington's disease (HD) and Parkinson's disease (PD). Knockout of HtrA2 in mice also leads to mitochondrial dysfunction and to phenotypes that resemble those found in neurodegenerative disorders and, ultimately, lead to death of animals around postnatal day 30. Here, we show that Idebenone, a synthetic antioxidant of the coenzyme Q family, and Resveratrol, a bioactive compound extracted from grapes, are both able to ameliorate this phenotype. Feeding HtrA2 knockout mice with either compound extends lifespan and delays worsening of the motor phenotype. Experiments conducted in cell culture and on brain tissue of mice revealed that each compound has a different mechanism of action. While Idebenone acts by downregulating the integrated stress response, Resveratrol acts by attenuating apoptosis at the level of Bax. These activities can account for the delay in neuronal degeneration in the striata of these mice and illustrate the potential of these compounds as effective therapeutic approaches against neurodegenerative disorders such as HD or PD

Treatment of CoQ10 Deficient Fibroblasts with Ubiquinone, CoQ Analogs, and Vitamin C: Time- and Compound-Dependent Effects

Background: Coenzyme Q(10) (CoQ(10)) and its analogs are used therapeutically by virtue of their functions as electron carriers, antioxidant compounds, or both. However, published studies suggest that different ubiquinone analogs may produce divergent effects on oxidative phosphorylation and oxidative stress.Methodology/Principal Findings: To test these concepts, we have evaluated the effects of CoQ(10), coenzyme Q(2) (CoQ(2)), idebenone, and vitamin C on bioenergetics and oxidative stress in human skin fibroblasts with primary CoQ(10) deficiency. A final concentration of 5 mu M of each compound was chosen to approximate the plasma concentration of CoQ(10) of patients treated with oral ubiquinone. CoQ(10) supplementation for one week but not for 24 hours doubled ATP levels and ATP/ADP ratio in CoQ(10) deficient fibroblasts therein normalizing the bioenergetics status of the cells. Other compounds did not affect cellular bioenergetics. In COQ2 mutant fibroblasts, increased superoxide anion production and oxidative stress-induced cell death were normalized by all supplements.Conclusions/Significance: These results indicate that: 1) pharmacokinetics of CoQ(10) in reaching the mitochondrial respiratory chain is delayed; 2) short-tail ubiquinone analogs cannot replace CoQ(10) in the mitochondrial respiratory chain under conditions of CoQ(10) deficiency; and 3) oxidative stress and cell death can be counteracted by administration of lipophilic or hydrophilic antioxidants. The results of our in vitro experiments suggest that primary CoQ(10) deficiencies should be treated with CoQ(10) supplementation but not with short-tail ubiquinone analogs, such as idebenone or CoQ(2). Complementary administration of antioxidants with high bioavailability should be considered if oxidative stress is present

Mitochondrial genome deletions and minicircles are common in lice (Insecta: Phthiraptera)

Background The gene composition, gene order and structure of the mitochondrial genome are remarkably stable across bilaterian animals. Lice (Insecta: Phthiraptera) are a major exception to this genomic stability in that the canonical single chromosome with 37 genes found in almost all other bilaterians has been lost in multiple lineages in favour of multiple, minicircular chromosomes with less than 37 genes on each chromosome. Results Minicircular mt genomes are found in six of the ten louse species examined to date and three types of minicircles were identified: heteroplasmic minicircles which coexist with full sized mt genomes (type 1); multigene chromosomes with short, simple control regions, we infer that the genome consists of several such chromosomes (type 2); and multiple, single to three gene chromosomes with large, complex control regions (type 3). Mapping minicircle types onto a phylogenetic tree of lice fails to show a pattern of their occurrence consistent with an evolutionary series of minicircle types. Analysis of the nuclear-encoded, mitochondrially-targetted genes inferred from the body louse, Pediculus, suggests that the loss of mitochondrial single-stranded binding protein (mtSSB) may be responsible for the presence of minicircles in at least species with the most derived type 3 minicircles (Pediculus, Damalinia). Conclusions Minicircular mt genomes are common in lice and appear to have arisen multiple times within the group. Life history adaptive explanations which attribute minicircular mt genomes in lice to the adoption of blood-feeding in the Anoplura are not supported by this expanded data set as minicircles are found in multiple non-blood feeding louse groups but are not found in the blood-feeding genus Heterodoxus. In contrast, a mechanist explanation based on the loss of mtSSB suggests that minicircles may be selectively favoured due to the incapacity of the mt replisome to synthesize long replicative products without mtSSB and thus the loss of this gene lead to the formation of minicircles in lice