Academic literature on the topic 'Geranial'

ABSTRACTCastellaniella defragransis aBetaproteobacteriumcapable of coupling the oxidation of monoterpenes with denitrification. Geraniol dehydrogenase (GeDH) activity was induced during growth with limonene in comparison to growth with acetate. The N-terminal sequence of the purified enzyme directed the cloning of the corresponding open reading frame (ORF), the first bacterial gene for a GeDH (geoA, forgeranioloxidation pathway). TheC. defragransgeraniol dehydrogenase is a homodimeric enzyme that affiliates with the zinc-containing benzyl alcohol dehydrogenases in the superfamily of medium-chain-length dehydrogenases/reductases (MDR). The purified enzyme most efficiently catalyzes the oxidation of perillyl alcohol (kcat/Km= 2.02 × 106M−1s−1), followed by geraniol (kcat/Km= 1.57 × 106M−1s−1). ApparentKmvalues of <10 μM are consistent with anin vivotoxicity of geraniol above 5 μM. In the genetic vicinity ofgeoAis a putative aldehyde dehydrogenase that was namedgeoBand identified as a highly abundant protein during growth with phellandrene. Extracts ofEscherichia coliexpressinggeoBdemonstratedin vitroa geranial dehydrogenase (GaDH) activity. GaDH activity was independent of coenzyme A. The irreversible formation of geranic acid allows for a metabolic flux from β-myrcene via linalool, geraniol, and geranial to geranic acid.

ABSTRACT Geraniol is one of the important aromatic ingredients in alcoholic beverages. Bioconversions of geraniol to other terpenoids and genes involved in the oxidation of geraniol were investigated. Geranic acid and citronellic acid were detected in yeast culture, where geraniol or nerol was added. Addition of citral, a mixture of geranial and neral, resulted in the production of geranic acid and citronellic acid, whereas the addition of citral or citronellal resulted in the production of citronellic acid, suggesting that citronellic acid might be produced through the conversion of citral to citronellal followed by the oxidation of citronellal. Consumption of geraniol and production of geranic acid, citronellic acid, and citronellol were affected in adh1Δ, adh3Δ, adh4Δ, and sfa1Δ yeast strains, which possess single deletion of a gene encoding alcohol dehydrogenase. This is the first report of the bioconversion of monoterpene alcohols, geraniol and nerol, to geranic acid and citronellic acid in yeast culture.

Mini-Tn5-induced mutants with defects in utilization of linear terpenes such as citronellol, geraniol, citronellate and/or geranylate were isolated from Pseudomonas aeruginosa. One mutant was unable to utilize geraniol but showed wild-type growth with the three other acyclic terpenes tested. The Tn5 insertion site of the mutant was determined by DNA sequencing. Comparison with the P. aeruginosa genome sequence revealed that PA3028, an ORF with high similarity on the amino acid level to molybdenum cofactor biosynthesis protein A2 (encoded by moeA2), was the target of mini-Tn5 in the mutant. Disruption of moeA2 in P. aeruginosa PAO1 wild-type by insertion mutagenesis resulted in the same geraniol-minus phenotype. The ability to utilize geraniol was restored to the mutant by conjugative transfer of PCR-cloned wild-type moeA2 on a broad-host-range plasmid. Growth of P. aeruginosa PAO1 on geraniol and geranial, but not on citronellol, citronellate or geranylate, was inhibited by the presence of 10 mM tungstate, a molybdenum-specific inhibitor. Inhibition by tungstate was prevented by addition of molybdate. The results indicate that at least one step in the oxidation of geraniol to geranic acid (geranial oxidation) is a molybdenum-dependent reaction in P. aeruginosa and is different from the molybdenum-independent oxidation of citronellol to citronellate.

Hydro-distilled essential oils from fresh and dry leaves and fresh and dry flowers of `Sweet Dani', a new ornamental lemon basil (Ocimum basilicum) cultivar with potential as a source of natural citral, were analyzed by GC and GC/MS. The essential oil contents were 0.18%, 0.19%, 0.30%, 0.28% w/w on a fresh weight basis of fresh and dry leaves, and fresh and dry flowers, respectively. Oils from leaves and flowers differed significantly in content and composition. The major constituents in dry leaf oil were neral 21.8% and geranial 33.5%. The major constituents in dry flower oil included: nerol 11.5%, neral 12.9%, geraniol 7.6%, and geranial 17.7%. Nerol (1.6%), and geraniol (0.4%) were very low in dry leaf oil. As citral is a combination of neral and geranial, the relative leaf and flower citral content is 55.3% and 30.6% of the total oil, respectively. Linalool and octanol were detected in flower oils only.

The chemical composition of the essential oil from the rhizome of ginger ( Zingiber officinale Roscoe), collected from Nahan, Himachal Pradesh, India, was determined by gas chromatography and GC-MS. Fifty-one compounds, representing 95.1% of the oil, were identified. The oil was characterized by relatively large amounts of the monoterpenoids 1,8-cineole (10.9%), linalool (4.8%), borneol (5.6%), α-terpineol (3.6%), neral (8.1%), geraniol (14.5%), geranial (9.5%), trans-dimethoxy citral (5.0%) and geranyl acetate (6.3%). Five compounds, namely trans-linalool oxide, trans-linalool oxide acetate, ( Z)-dimethoxycitral, ( E)-dimethoxy citral and epi-zingiberenol are reported for the first time in oil of ginger.

The biological activity and composition of the essential oil of the aerial flowering parts of D. moldavica have been investigated. The oil analysis was performed by GC and GC-MS. Thirteen compounds were identified, representing 99.8% of the oil. Oxygenated monoterpenes (96.3%) were found to be the principal group of compounds, of which neral, geranial, geranyl acetate and geraniol with 32.1, 21.6, 19.9 and 17.6% of the total oil were the main constituents, respectively. The in vitro antimicrobial activity of the essential oil and its main components, citral, geraniol and geranyl acetate, showed that all of the tested microorganisms were highly inhibited by the essential oil with inhibition zones ranged from 15 – 41 mm for bacteria and 29 – 30 mm for fungi. The most sensitive microorganisms were Bacillus subtilis, Staphylococcus aureus and S. epidermidis with the lowest MIC values of 0.9 mg/mL. Considering sensitivity screening, it is conceivable that the activity of the oil from D. moldavica could be attributed mainly to the presence of citral.

The present study aimed to chemically characterize 31 accessions and seven cultivars of basil. The percentage composition of the essential oils of the accessions and cultivars was based on the 14 most abundant constituents: 1,8-cineole, linalool, methyl chavicol, neral, nerol, geraniol, geranial, methyl cinnamate,β-bourbonene, methyl eugenol,α-trans-bergamotene, germacrene-D,epi-α-cadinol, andδ-cadinene. The genetic materials were classified into eight clusters according to the chemical composition of the essential oils: Cluster 1—mostly linalool and 1,8-cineole; Cluster 2—mostly linalool, geraniol, andα-trans-bergamotene; Cluster 3—mostly linalool, methyl chavicol, methyl cinnamate, andβ-bourbonene; Cluster 4—mostly linalool, methyl chavicol,epi-α-cadinol, andα-trans-bergamotene; Cluster 5—mainly linalool, methyl eugenol,α-trans-bergamotene, andepi-α-cadinol; Cluster 6—mainly linalool, geraniol, andepi-α-cadinol; Cluster 7—mostly linalool and methyl chavicol; Cluster 8—mainly geranial and neral.

Ginger production in Paraná State, Brazil, has predominated in Morretes Municipality, with around 300 ha cultivated area. The aim of this work was to evaluate the essential oil yield and composition of ginger rhizomes produced in Morretes and subjected to different drying periods at room temperature. Experimental design was completely randomized, in a 5x5 factorial arrangement, with four replicates (four plants each), five origins and five drying periods at room temperature (0, 15, 30, 45 and 60 days). The essential oil was extracted by hydrodistillation in a Clevenger-type device for 3h and the constituents were analyzed by gas chromatography-mass spectrometry (GC/MS). The drying of ginger rhizomes at room temperature for up to 60 days decreased the essential oil yield in most origins. Geranial and neral levels were higher in all origins and as drying periods were longer. Geraniol and geranyl acetate levels decreased after drying in all origins, as well as eucalyptol, camphene, zingiberene and β-bisabolene in most origins.

Cell suspension cultures of Petroselinum crispum (Mill) Nyman cultivars “Paramount” and “Plain-leaved” were capable of biotransforming exogenously supplied geraniol largely into nerol and minor quantities of neral and geranial. Maximal conversions into nerol (32-36%); and neral: < 1% (cult. “Plain-leaved”), <5% (cult. “Paramount”) were usually recorded by 24 h. Over the incubation period a low proportion of the substrate, 32-40% was involved in biotransformation. Cyclic and other acyclic monoterpenoids were not biotransformed.

Aphrodisiac and anti-aphrodisiac pheromone production and composition in the green-veined white butterfly Pieris napi L. were investigated. Aphrodisiac pheromone biosynthesis had different time constraints in butterflies from the diapausing and directly developing generations. Effects of stable isotope incorporation in adult butterfly pheromone, in the nectar and flower volatiles of  host plants from labeled substrates were measured by solid phase microextraction and gas chromatography–mass spectrometry. A method to fertilize plants with stable isotopes was developed and found to be an effective method to investigate the transfer of pheromone building blocks from flowering plants to butterflies. The anti-aphrodisiac methyl salicylate was not biosynthesized from phenylalanine in flowers of Alliaria petiolata. Both aphrodisiac and anti-aphrodisiac pheromones in P.napi are produced not only from resources acquired in the larval stage, but also from nutritional resources consumed intheadult stage. Males of P. napi produce the anti-aphrodisiac pheromone from both the essential amino acid L-phenylalanine and from common flower fragrance constituents.

QC 20140311

Submitted by Leonardo Cavalcante (leo.ocavalcante@gmail.com) on 2018-07-17T18:53:07Z No. of bitstreams: 1 Arquivototal.pdf: 3232624 bytes, checksum: 559aa25bbe9205467b3fdd737354219e (MD5)
Made available in DSpace on 2018-07-17T18:53:07Z (GMT). No. of bitstreams: 1 Arquivototal.pdf: 3232624 bytes, checksum: 559aa25bbe9205467b3fdd737354219e (MD5) Previous issue date: 2016-02-29
The high incidence of pain in the general population has encouraged research about this theme. Products derived from plant species have been widely used in the pharmacological treatment of pain relief. Recent studies have reported the important role of monoterpenes, active compounds found in the essential oils of aromatic plants, having relevant analgesic and anti-inflammatory potential. The geraniol (GER) is a monoterpenic alcohol, found in >160 essential oil of plant species, especially Cymbopogon gender. In the literature consulted, several biochemical and pharmacological properties are shown of GER: antitumor, antimicrobial, antiinflammatory, antioxidant, gastric and intestinal protector, neuroprotective and antiarrhythmic. In this study was evaluated the antinociceptive activity of GER, not yet reported, by animal behavioral and electrophysiological in vitro models. Male and female adult Swiss mice were used. Initially the acute toxicity of GER was investigated by calculating the lethal dose 50 (LD50) by intraperitoneal (i.p.) (= 199.9 mg/kg) and oral (p.o.) (> 1 g/kg). In psychopharmacological screening, after the administration of single doses of GER (i.p. and p.o.), behavioral changes were observed indicating a depressant profile on the central nervous system (CNS) and/or peripheral nervous system (SNP), and relevant antinociceptive effect of geraniol. Therefore, more specific antinociceptive property evaluation tests were performed. The GER (12.5, 25 or 50 mg/kg i.p. and 50 or 200 mg/kg p.o.) decreased (p<0.001) the number of abdominal contractions induced by i.p. injection of acetic acid, when compared with the control. The opioid antagonist naloxone (5 mg/kg) administered subcutaneously (s.c.) in mice, subsequently treated with GER (25 mg/kg i.p.), did not reverse its antinociceptive activity. The GER (12.5, 25 and 50 mg/kg i.p.) reduced (p<0.001) paw licking time in the second phase (15-30 min, inflammatory phase) of the formalin test. Also, in the glutamate test was reduced (p<0.01) paw licking time when GER 50 mg/kg i.p. administered. In a subsequent step, it was investigated the effect of GER on the excitability of peripheral nerve fibers through extracellular recording in the sciatic nerve in mice. The GER presented depressant effect of the compound action potential (CAP), which was reversed after washing and recovery period. The GER blocked components of the CAP concentration-dependent manner and exposure time to the drug: 1 mM after 120 min for the first component (Aγ and Aβ fibers) and 0.6 mM after 90 min for the second (Aγ and Aδ fibers). The concentration, which induces 50% inhibition of the peak-to-peak amplitude of the PAC (IC50) for the GER was calculated, being equal to 0.48±0.04 mM. The conduction velocity was also reduced by exposure to GER from the 0.3 mM concentration, for the 1st component [46.18±2.60 m/s to 36.04±1.60 m/s; p<0.05 (n=7)] and the 2nd component [18.37±1.31 m/s to 12.71±0.56 m/s; p<0.001 (n=7)]. In conclusion, the results obtained show that GER has antinociceptive activity, mainly in pain related to inflammation. Participation of the opioid pathway in its mechanism of action is unlikely, but the modulation of glutamatergic neurotransmission in a dose-dependent manner is a possible mechanism. Its antinociceptive activity is also related to the reduction in peripheral neuronal excitability, firstly in thinner fibers Aδ, which are directly connected to the conduction pain.
A elevada incidência da dor na população em geral tem incentivado as pesquisas entorno desse tema. Produtos oriundos de espécies vegetais têm sido amplamente utilizados no tratamento farmacológico de alívio da dor. Estudos recentes têm relatado o importante papel dos monoterpenos, princípios ativos encontrados nos óleos essenciais de plantas aromáticas, tendo relevante potencial analgésico e anti-inflamatório. O geraniol (GER) é um álcool monoterpênico, encontrado no óleo essencial de >160 espécies vegetais, especialmente do gênero Cymbopogon. Na literatura consultada, pesquisas apontam várias propriedades bioquímicas e farmacológicas para o GER: antitumoral, antimicrobiana, anti-inflamatória, antioxidante, de proteção gástrica e intestinal, neuroprotetora e antiarrítmica. Neste estudo foi avaliada a atividade antinociceptiva do GER, ainda não relatada, mediante modelos animais comportamentais e eletrofisiológicos in vitro. Foram utilizados camundongos machos e fêmeas Swiss adultos. Inicialmente, foi investigada a toxicidade aguda do GER mediante cálculo da dose letal 50 (DL50) pela via intraperitoneal (i.p.) (=199,9 mg/kg) e oral (v.o.) (>1 g/kg). Na triagem psicofarmacológica, após a subministração de doses únicas de GER (i.p. e v.o.) foram observadas alterações comportamentais que indicaram perfil depressor do sistema nervoso central (SNC) e/ou periférico (SNP), e relevante efeito antinociceptivo do geraniol. Portanto, foram realizados testes comportamentais de avaliação de propriedade antinociceptiva mais específicos. O GER (12,5; 25 e 50 mg/kg i.p. e 50 ou 200 mg/kg v.o.) reduziu (p<0,001) o número de contorções abdominais induzidas por injeção i.p. de ácido acético, quando comparado com o controle. O antagonista opióide naloxona (5 mg/kg) administrado pela via subcutânea (s.c.) em camundongos, subsequentemente tratados com GER (25 mg/kg i.p.), não reverteu sua atividade antinociceptiva. O GER (12,5; 25 e 50 mg/kg i.p.) reduziu (p<0,001) o tempo de lambida da pata na segunda fase (15-30 min, fase inflamatória) do teste da formalina. Também, no teste do glutamato houve redução (p<0,01) do tempo de lambida da pata quando administrado GER 50 mg/kg i.p. Em uma etapa subsequente, investigou-se o efeito do GER sobre a excitabilidade de fibras nervosas periféricas, mediante registro extracelular em nervo ciático de camundongo. O GER apresentou efeito depressor do potencial de ação composto (PAC), o qual foi parcialmente revertido após lavagem durante o período de recuperação. O GER bloqueou as componentes do PAC, de maneira dependente da concentração e do tempo de exposição à droga: 1 mM aos 120 min para a primeira componente (fibras Aγ e Aβ) e 0,6 mM aos 90 min para a segunda (fibras Aγ e Aδ). Foi calculada para o GER, a concentração que induz 50% de inibição da amplitude pico-a-pico do PAC (CI50), sendo igual a 0,48±0,04 mM. A velocidade de condução também, foi reduzida pela exposição ao GER, a partir da concentração de 0,3 mM para a 1ª componente [46,18±2,60 m/s para 36,04±1,60 m/s; p<0,05 (n=7)] e para a 2ª componente [18,37±1,31 m/s para 12,71±0,56 m/s; p<0,001 (n=7)]. Em conclusão, os resultados obtidos mostram que o GER tem atividade antinociceptiva, principalmente na dor relacionada à inflamação. A participação da via opióide no seu mecanismo de ação é pouco provável, mas a modulação da neurotransmissão glutamatérgica de maneira dependente da dose é um mecanismo possível. Sua atividade antinociceptiva tambèm, está relacionada à redução da excitabilidade neuronal periférica, primeiramente de fibras mais finas como Aδ, ligadas diretamente à condução da dor.

No presente estudo avaliou-se a atividade quimiopreventiva do farnesol (FR) e geraniol (GR), isoprenóides presentes em frutas e ervas, quando administrados a ratos Wistar durante as etapas de iniciação e/ou seleção/promoção do modelo de hepatocarcinogênese do \"hepatócito resistente\" (RH). No Protocolo Experimental 1, os animais receberam durante 8 semanas consecutivas, continuamente durante as etapas de iniciação e seleção/promoção, por entubação gástrica e dissolvido em óleo de milho (OM): FR (25 mg/100 g de peso corpóreo [p.c.]; grupo FR) ou GR (25 mg/100 g de p.c.; grupo GR). Além disso, 1 grupo recebeu durante o mesmo período, por entubação gástrica, apenas OM (0,25 mL/100 g de p.c.; grupo OM; controle). Duas semanas após o início dos tratamentos, todos os grupos foram submetidos ao modelo do RH. Esse consistiu na aplicação intraperitoneal de uma dose do agente iniciante dietilnitrosamina (DEN, 20 mg/100 g de p.c.), seguida, 2 semanas após, da aplicação de 4 doses consecutivas de 2-acetilaminofluoreno (2-AAF; 2,5 mg/100 g de p.c.) e de uma hepatectomia parcial (HP) a 70%, acrescida de 2 doses de 2-AAF (2 mg/100 g de p.c.) 2 e 4 dias após a cirurgia. Decorridas 6 semanas após a iniciação com DEN, os animais foram sacrificados administrando-se, entretanto, 2 h. antes desse procedimento 5-bromo-2-desoxiuridina (BrdU) (10 mg/100 g de p.c.). De acordo com a análise macroscópica dos fígados, e em comparação ao grupo OM, verificou-se que o FR inibiu a incidência (p<0,05) e número médio (p<0,05) de lesões pré-neoplásicas (LPN) hepáticas visíveis à macroscopia. No caso do grupo GR, observou-se apenas sugestão de redução da incidência e número médio dessas LPN visíveis à macroscopia. Em relação à análise morfométrica das LPN hepáticas positivas para a enzima glutationa S-transferase forma placentária (GST-P) totais (persistentes + em remodelação), observou-se que em comparação ao grupo OM, o FR reduziu o tamanho (p<0,05) e área do corte ocupada (p<0,05) por essas lesões. O GR, por sua vez, reduziu o tamanho (p<0,05) das LPN GST-P positivas totais, observando-se, também, sugestão de redução pelo isoprenóide da área do corte ocupada pelas mesmas. Em comparação ao grupo OM, o FR e o GR foram capazes de inibir (p<0,05) a proliferação celular nas LPN, enquanto apenas o GR induziu (p<0,05) a apoptose nas mesmas. Além disso, danos no DNA hepático foram menores (p<0,05) nos animais tratados com FR ou GR, em comparação aos tratados com OM (controles). O tratamento com FR, mas não com GR, resultou em inibição (p<0,05) das concentrações plasmáticas de colesterol total. A análise, por \"western blot\", da expressão hepática do receptor nuclear ativado pelo farnesóide X (FXR) não revelou diferenças (p>0,05) entre os diferentes grupos. No Protocolo Experimental 2, os ratos receberam apenas durante 2 semanas consecutivas na fase de iniciação, e por entubação gástrica, FR (25 mg/100 g p.c.; grupo FRi), GR (25 mg/100 g p.c.; grupo GRi) ou OM (0,25 mL/00 g p.c.; grupo OMi, controle), sendo então submetidos ao modelo do RH, conforme descrito para o Protocolo Experimental 1. O sacrifício dos animais ocorreu 6 semanas após iniciação com DEN. De acordo com a análise macroscópica dos fígados, não foram constatadas diferenças entre os diferentes grupos (p>0,05) quanto à incidência de LPN hepáticas visíveis à macroscopia. Em comparação ao grupo OMi (controle), observou-se nos grupos FRi e GRi sugestão de maior número de LPN hepáticas visíveis à macroscopia. Também em comparação ao grupo OMi (controle), observou-se no grupo GRi menor (p<0,05) número de LPN hepáticas GST-P positivas totais (persistentes + em remodelação), e no grupo FRi sugestão de menor número dessas LPN GST-P positivas totais. Além disso, foram observadas nos grupos FRi e GRi, em comparação ao grupo OMi, LPN hepáticas GST-P positivas totais (persistentes + em remodelação) maiores (p<0,05), bem como sugestão de maior área do corte ocupada por essas LPN GST-P positivas. Não foram observadas diferenças (p>0,05) entre os diferentes grupos quanto à concentração hepática de DNA. No Protocolo Experimental 3, os ratos receberam inicialmente uma dose de DEN (20 mg/100 g de p.c.). Duas semanas após, os animais passaram a receber por entubação gástrica, durante 6 semanas consecutivas em período compreendendo a etapa de seleção/promoção: FR (25 mg/100 g p.c.; grupo FRs/p), GR (25 mg/100 g p.c.; grupo GRs/p) ou OM (0,25 mL/100 g p.c.; grupo Oms/p; controle). Nesse experimento, as administrações de 2-AAF e a realização da HP ocorreram 4 semanas após a iniciação com DEN. O sacrifício dos animais ocorreu após 8 semanas da iniciação com DEN. Em comparação ao grupo OMs/p (controle), observou-se nos grupos FRs/p e GRs/p sugestão de menor número médio de LPN hepáticas visíveis à macroscopia. Não foram constatadas diferenças (p>O,05) entre os diferentes grupos quanto à incidência de LPN hepáticas visíveis à macroscopia; quanto ao número, tamanho e área do corte ocupada por LPN hepáticas GST-P positivas totais (persistentes + em remodelação); e quanto à concentração hepática de DNA. De acordo com os resultados do estudo, considerou-se pronunciada a atividade quimiopreventiva do FR quando administrado a ratos Wistar continuamente durante as etapas de iniciação e seleção/promoção do modelo de hepatocarcinogênese do RH (Protocolo Experimenta! 1). Nessas mesmas condições, considerou-se moderada a atividade quimiopreventiva do GR. Inibições da proliferação celular e de danos no DNA parecem estar envolvidas com as ações anticarcinogênicas do FR e GR, enquanto que a indução da apoptose parece ser mecanismo de ação específico do GR. Além disso, as ações protetoras do FR e GR não parecem envolver alterações na expressão do receptor nuclear FXR. Finalmente, quando administrados especificamente durante a etapa de iniciação (Protocolo Experimental 2) ou de seleção/promoção (Protocolo Experimental 3), ambos os isoprenóides não foram capazes de apresentar atividades quimiopreventivas efetivas. Dessa forma, em ratos Wistar submetidos ao modelo do RH, é necessária a administração contínua de FR ou GR durante as etapas de iniciação e seleção/promoção para a ocorrência de atividades quimiopreventivas.
In the present study, the chemopreventive activity of farnesol (FR) and geraniol (GR), isoprenoids present in fruits and herbs, was evaluated when administered to Wistar rats during the initiation and/or selection/promotion phases of the \"resistant hepatocyte\" (RH) model of hepatocarcinogenesis. In Experimental Protocol 1, animals received during 8 consecutive weeks, continuously during the initiation and selection/promotion phases, by gavage and dissolved in corn oil (CO): FR (25 mg/100g9 body weight [b.w.]; FR group) or GR (25 mg/100 g de b.w.; GR group). Moreover, 1 group received during the same period, by gavage, only CO (0,25 mL/100 g de b.w.; CO group; controls). Two weeks after the beginning of the treatments, all groups were submitted to the RH model. Initiation was obtained by administration of a single intraperitoneal dose of diethylnitrosamine (DEN; 20 mg/100 g b.w.) followed, 2 weeks after, by the administration of 4 consecutive doses of 2-acetylaminofluorene (2-AAF; .2.5 mg/100 b.w.) and by a partial (70%) hepatectomy (PH). Finally, 2 and 4 days after PH, 2 additional 2-AAF doses (2 mg/100 g b.w.) were administered. Six weeks after initiation with DEN, the animals were anesthetized and sacrificed by exsanguination. Two hours before sacrifice, the rats received 5-bromo-2\'-deoxyuridine (10 mg/100 g b.w.). According to the macroscopic examination of the livers, and compared to CO group, FR inhibited the incidence (P<0.05) and mean number (P<0.05) of visible hepatic preneoplastic lesions (PNL). Regarding GR group, only a suggestion of inhibition of visible PNL incidence and mean number was observed. Morphometrical analysis of total (persitent and remodeling) glutathione S-transferase (GST-P) positive PNL showed that compared to CO group, FR group presented with smaller total GST-P positive PNL (p<0.05) that occupied a smaller area of the liver section (p<0.05). Also compared to CO group, GR group presented with smaller total GST-P positive PNL (p<0.05) and a suggestion of reduction of the liver section area occupied by these LPN was observed. Compared to CO group, FR and GR inhibited (p<0.05) PNL cell proliferation, whereas only GR induced (p<0.05) apoptosis in these PNL. Furthermore, hepatic DNA damage was lower (p<0.05) in FR or GR treated animals, compared to CO treated ones (controls). Animal treatment with FR, but not with GR, inhibited (p<0,05) total plasma cholesterol levels. Farnesoid X activated receptor (FXR) expression analysis by western blot did not reveal differences (p>0,05) between the different groups. In the Experimental Protocol 2, rats received only for 2 consecutive weeks during the initiation phase, and by gavage: FR (25 mg/100 g body weight b.w.; FRi group), GR (25 mg/100 g de b.w.; GRi group) or CO (0,25 mL/100 g de b.w.; COi group; controls) being submitted to the RH model as described for Experimental Protocol 1. Six weeks after initiation with DEN, the animals were sacrificed. According to the macroscopic examination of the livers, no differences (p>0.05) were observed among the different groups regarding the incidence of visible PNL. In FRi and GRi groups a suggestion of higher number of visible PNL was observed, when compared to COi group (controls). Also compared to COi group, GRi group presented with smaller (p<0.05) number of total (persistente + remodeling) GST-P positive PNL, whereas in FRi group a suggestion of smaller number of these visible PNL was observed. Moreover, compared to COi group, FRi and GRi groups presented with total (persistent + remodelling) GST-P positive PNL with greater (p<0,05) size, and a suggestion of greater area of the liver section occupied by these GST -P positive PNL was observed. No differences (p>0.05) among the different groups were observed regarding hepatic DNA concentration. In Experimental Protocol 3, rats were first initiated with DEN (20 mg/100 g de b.w.). After 2 weeks, animals received by gavage for 6 consecutive weeks during the selection/promotion phase: FR (25 mg/100 g body weight b.w.; FRs/p group), GR (25 mg/100 g de b.w.; GRs/p group) or CO (0,25 Ml/100 g de b.w.; COs/p group; controls). In this experiment animals received 2-AAF doses and were submitted to PH 4 weeks after initiation with DEN. Six weeks after initiation with DEN, the animals were sacrificed. Compared to COs/p group (controls), a suggestion of smaller visible PNL mean number was observed in FRs/p e GRs/p groups. No differences (p>0.05) among the different groups were observed regarding visible PNL incidence; regarding number, size and liver section occupied by total (persistent + remodeling) GST-P positive PNL; and regarding hepatic DNA concentration. According to the results of the study, FR chemopreventive activity was considered pronounced when administered to Wistar rats continuously during the initiation and selection/promotion phases of the RH model of hepatocarcinogenesis (Experimental Protocol 1). In these same conditions, GR chemopreventive activity was considered moderate. Cell proliferation and DNA damage inhibition seem to be involved with FR and GR anticarcinogenic actions, whereas apoptosis induction seems to represent a GR specific mechanism. Furthermore, FR and GR protective actions do not seem to involve alterations in FXR expression. Finally, when administered specifically during the initiation (Experimental Protocol 2) or selection/promotion (Experimental Protocol 3) phase, both isoprenoids did not present effective chemopreventive activity. Thus, in Wistar rats submitted to the RH model, FR or GR should be administered continuously during the initiation and selection/promotion phases in order to obtain chemopreventive activities.

Made available in DSpace on 2014-06-11T19:25:25Z (GMT). No. of bitstreams: 0 Previous issue date: 2012-02-29Bitstream added on 2014-06-13T20:13:51Z : No. of bitstreams: 1 carvalho_kim_me_botib.pdf: 473702 bytes, checksum: cf335e6c7efaff94811da0dd6fc60b36 (MD5)
Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES)
A úlcera péptica é causada por um desequilíbrio entre os fatores protetores e lesivos da mucosa. A expansão global no consumo de álcool e DAINEs têm contribuído para um aumento da incidência da doença na população. Um dos maiores problemas relativo à úlcera péptica consiste na recidiva da mesma após a terapêutica, justificando-se a busca por novos tratamentos mais eficazes. Relatos científicos mostram que os óleos essenciais derivados das plantas possuem uma variedade de atividades biológicas, tais como ansiolíticos, antioxidantes, antiinflamatórios e antiulcerogênicos. Baseando-se nessa premissa resolvemos avaliar a atividade gastroprotetora do monoterpeno geraniol. Os resultados do estudo mostraram que o geraniol na dose de 7,5 mg/Kg foi efetivo no modelo de úlcera induzida por etanol absoluto com 70% de proteção. Essa ação gastroprotetora mostrou-se dependente da presença de óxido nítrico, dos grupamentos sulfidrilas e do aumento na produção de muco gástrico. No modelo de úlcera gástrica induzida por indometacina o geraniol não teve ação antiulcerogênica, sugerindo-se que a proteção desse monoterpeno esteja associada à metabólitos da via da COX, tais como: as prostaglandinas. No modelo de úlcera induzida por etanol em ratos pré-tratados com indometacina, os resultados indicaram que a gastroproteção do geraniol está relacionada com as PGs, uma vez que na presença de um inibidor da COX, ele perdeu sua proteção. Os dados apontam ainda para uma atividade antioxidante, comprovada no modelo de isquemia e reperfusão, onde o geraniol conferiu uma proteção à mucosa gástrica de 71%, e no modelo de úlcera duodenal induzida por cisteamina cuja proteção observada foi de 68%. No modelo de ligadura de piloro observou-se a ausência de atividade antisecretória gástrica e verificou-se...
A peptic ulcer is caused by an imbalance between the protective and the agressive factors of the mucosa. The global expansion in the consumption of alcohol and NSAIDs have contributed to an increased incidence of disease in the population. One of the biggest problems relative on peptic ulcer is recurrence of it after the treatment, justifying the search for new more effective treatments. Scientific reports show that essential oils derived from plants have a variety of biological activities, such as anxiolytics, antioxidants, anti-inflammatory and antiulcerogenics. Based on this assumption we decided to evaluate the gastroprotective activity of the monoterpene geraniol. The study results showed that geraniol at a dose of 7.5 mg/Kg was effective in the model of ulcer induced by absolute ethanol with 70% protection. This gastroprotective action was dependent on the presence of nitric oxide, sulfhydryl groups (SHs) and increased production of gastric mucus. In the model of gastric ulcer indomethacin-induced geraniol (7.5 mg / kg) did not had antiulcerogenic action, suggesting that protection this monoterpene is associated with metabolites of the COX pathway, such as prostaglandins. In the model of ethanol-induced ulcer in rats pretreated with indomethacin the results indicated that the geraniol's gastroprotection is related to the prostaglandins, since in the presence of a COX inhibitor, it lost its protection. The results also point to an antioxidant activity, proven in the model of ischemia and reperfusion, where geraniol gave a protection to the gastric mucosa of 71% and the model of duodenal ulcer cysteamine-induced whose protection observed was 68%. In the pylorus ligation model was observed the absence of gastric antisecretory activity and was verified through the model of activated charcoal that this monoterpene... (Complete abstract click electronic access below)

Orientador: Clélia Akiko Hiruma-Lima
Banca: Marcos José Salvador
Banca: Luiz Claudio Di Stasi
Resumo: A úlcera péptica é causada por um desequilíbrio entre os fatores protetores e lesivos da mucosa. A expansão global no consumo de álcool e DAINEs têm contribuído para um aumento da incidência da doença na população. Um dos maiores problemas relativo à úlcera péptica consiste na recidiva da mesma após a terapêutica, justificando-se a busca por novos tratamentos mais eficazes. Relatos científicos mostram que os óleos essenciais derivados das plantas possuem uma variedade de atividades biológicas, tais como ansiolíticos, antioxidantes, antiinflamatórios e antiulcerogênicos. Baseando-se nessa premissa resolvemos avaliar a atividade gastroprotetora do monoterpeno geraniol. Os resultados do estudo mostraram que o geraniol na dose de 7,5 mg/Kg foi efetivo no modelo de úlcera induzida por etanol absoluto com 70% de proteção. Essa ação gastroprotetora mostrou-se dependente da presença de óxido nítrico, dos grupamentos sulfidrilas e do aumento na produção de muco gástrico. No modelo de úlcera gástrica induzida por indometacina o geraniol não teve ação antiulcerogênica, sugerindo-se que a proteção desse monoterpeno esteja associada à metabólitos da via da COX, tais como: as prostaglandinas. No modelo de úlcera induzida por etanol em ratos pré-tratados com indometacina, os resultados indicaram que a gastroproteção do geraniol está relacionada com as PGs, uma vez que na presença de um inibidor da COX, ele perdeu sua proteção. Os dados apontam ainda para uma atividade antioxidante, comprovada no modelo de isquemia e reperfusão, onde o geraniol conferiu uma proteção à mucosa gástrica de 71%, e no modelo de úlcera duodenal induzida por cisteamina cuja proteção observada foi de 68%. No modelo de ligadura de piloro observou-se a ausência de atividade antisecretória gástrica e verificou-se... (Resumo completo, clicar acesso eletrônico abaixo)
Abstract: A peptic ulcer is caused by an imbalance between the protective and the agressive factors of the mucosa. The global expansion in the consumption of alcohol and NSAIDs have contributed to an increased incidence of disease in the population. One of the biggest problems relative on peptic ulcer is recurrence of it after the treatment, justifying the search for new more effective treatments. Scientific reports show that essential oils derived from plants have a variety of biological activities, such as anxiolytics, antioxidants, anti-inflammatory and antiulcerogenics. Based on this assumption we decided to evaluate the gastroprotective activity of the monoterpene geraniol. The study results showed that geraniol at a dose of 7.5 mg/Kg was effective in the model of ulcer induced by absolute ethanol with 70% protection. This gastroprotective action was dependent on the presence of nitric oxide, sulfhydryl groups (SHs) and increased production of gastric mucus. In the model of gastric ulcer indomethacin-induced geraniol (7.5 mg / kg) did not had antiulcerogenic action, suggesting that protection this monoterpene is associated with metabolites of the COX pathway, such as prostaglandins. In the model of ethanol-induced ulcer in rats pretreated with indomethacin the results indicated that the geraniol's gastroprotection is related to the prostaglandins, since in the presence of a COX inhibitor, it lost its protection. The results also point to an antioxidant activity, proven in the model of ischemia and reperfusion, where geraniol gave a protection to the gastric mucosa of 71% and the model of duodenal ulcer cysteamine-induced whose protection observed was 68%. In the pylorus ligation model was observed the absence of gastric antisecretory activity and was verified through the model of activated charcoal that this monoterpene... (Complete abstract click electronic access below)
Mestre

Stuttgart, Universiẗat, Diss., 2008.
Aus: Appl. Environ. Microbiol. 2006 Jul;72(7):4819-28, FEMS Microbiol. Lett. 2006 Nov;264(2):220-5, Microbiology. 2008 Mar;154(Pt 3):789-96, FEMS Microbiol. Lett. 2005 May 1;246(1):25-31.

Submitted by Maike Costa (maiksebas@gmail.com) on 2017-09-12T12:28:26Z No. of bitstreams: 1 arquivototal.pdf: 1665261 bytes, checksum: dbe5fa1dfafb0bc226838e2bdf4e396e (MD5)
Made available in DSpace on 2017-09-12T12:28:26Z (GMT). No. of bitstreams: 1 arquivototal.pdf: 1665261 bytes, checksum: dbe5fa1dfafb0bc226838e2bdf4e396e (MD5) Previous issue date: 2017-01-18
Currently, throughout the globe, there has been an increase in the frequency of cases of candidiasis, an opportunistic infection commonly treated with fluconazole. With the indiscriminate use of this and other antifungals cases of candidiasis by multiresistant strains have emerged, making it necessary to search for new drugs. Several natural products such as monoterpene geraniol have demonstrated antimicrobial activity to various microorganisms. The present study aimed to evaluate the antifungal activity of geraniol against strains of Candida albicans, C. glabrata and C. krusei resistant to fluconazole by means of microdilution techniques, evaluating the minimum inhibitory concentration - CIM, minimum fungicidal concentration - CFM, cell wall effect (sorbitol assay), binding to membrane ergosterol, effect of association of this monoterpene with fluconazole and amphotericin B antifungal agents by the checkeboard technique and modulation assay. Pharmacological, toxicological and possible spectra of geraniol activity were also verified by in silico assays using the Osiris, Molinspiration and Pass online software. The analysis showed that geraniol showed excellent antifungal activity against all multiresistant strains with a 512μg/mL CIM90, and a fungicidal effect dependent concentration after 8 hours of exposure with the CFM90 of 512μg/mL. Fungal wall and did not interact with the ergosterol of the cell membrane, nor did it show a synergistic, antagonistic or modulating effect of this phytoconstituent on fluconazole and amphotericin B. The in silico tests showed that geraniol has a good theoretical oral bioavailability, as well as numerous Although it presents the risk of an irritant effect, it does not present mutagenic, tumorigenic or reproductive effects, which leads to the conclusion that geraniol is a good candidate in the fight against multidrug resistant strains of Candida.
Atualmente, em todo globo terrestre tem ocorrido o aumento da frequência dos casos de candidíase, infecção oportunista comumente tratada com fluconazol. Com o uso indiscriminado deste e outros antifúngicos tem se emergido casos de candidíase por cepas multirresistentes tornando-se necessário a busca por novos fármacos. Vários produtos naturais a exemplo do monoterpeno geraniol têm demonstrado atividade antimicrobiana frente a diversos micro-organismos. Buscando alternativas para o tratamento da candidíase o presente estudo objetivou-se avaliar a atividade antifúngica do geraniol frente a cepas de Candida albicans, C. glabrata e C. krusei resistentes ao fluconazol por meio de técnicas de microdiluição, avaliando-se a concentração inibitória mínima – CIM, concentração fungicida mínima – CFM, efeito na parede celular (ensaio de sorbitol), ligação ao ergosterol da membrana, efeito de associação deste monoterpeno com antifúngicos fluconazol e anfotericina B pelo técnica de checkeboard e ensaio de modulação. Verificou-se também a os parâmetros farmacológicos, toxicológicos e possíveis espectros de atividade do geraniol por meio de ensaios in silico utilizando-se os softwares Osiris, Molinspiration e Pass online. As análises realizadas revelaram que o geraniol apresentou uma excelente atividade antifúngica frente a todas as cepas multirresistentes com uma CIM90 512μg/mL, além de um efeito fungicida concentração dependente após 8 horas de exposição com a CFM90 de 512μg/mL, este não apresentou atividade na parede fúngica e nem interagiu com o ergosterol da membrana celular, também não se evidenciou efeito sinérgico, antagônico ou modulador deste fitoconstituinte sobre o fluconazol e a anfotericina B. Os ensaios in silico mostraram que o geraniol tem uma boa biodisponibilidade oral teórica, além de inúmeras atividades farmacológicas e que embora apresente o risco de efeito irritante, não apresenta efeitos mutagênicos, tumorigênicos e nem danos ao aparelho reprodutor, o que permite sugerir que o geraniol é um bom candidato no combate a cepas de Candida multirresistentes.

Comparative research has been conducted to allow us to determine the content of heavy metals and chemical composition of lemon balm oils, as well as to identify the possibility of lemon balm growth on soils contaminated by heavy metals. The experimental plots were situated at different distances of 0.5 km, and 15 km, respectively, from the source of pollution the Non-Ferrous-Metal Works (MFMW) near Plovdiv, Bulgaria. On reaching the flowering stage the lemon balm plants were gathered. The content of heavy metals in leaves of lemon balm was determined by ICP. The essential oils of the lemon balm were obtained by steam distillation in laboratory conditions which were analyzed for heavy metals and chemical composition was determined. Lemon balm is a plant that is tolerant to heavy metals and can be grown on contaminated soils. Heavy metals do not affect the development of lemon balm and the quality and quantity of oil obtained from it. Forty components were identified in the oils. The quantity of identified compounds corresponds to 98.82-98.83% of the total oil content. Among the detected compounds, beta-citral (neral) (19.31-20.78%), alfa-citral (geranial) (18,65-19,12%), β-caryophyllene (14.76-16.28%), α-cadinol (3.88-4.74%), geranyl acetate (3.49-3.59%), trans-geraniol (3.40-3.51%), germacrene (3.18-3.28%), citronellal (2.94-3.03%), nerol (2.63-2.71%), neryl acetate (2.42 -2.49%) were the major compounds. The essential oil of Melissa officinalis L. can be a valuable product for farmers from polluted regions.

The bovine opsin protein, 6PGS, is present in the eye of the Bos taurus species, and has activity throughout the period of development of the retina, remaining until its adult stage. The interaction of the geraniol ligand, which has anti-inflammatory, antimicrobial and antioxidant activities, with the active site of the protein was studied through theoretical calculations using Density Functional Theory. The molecular structure results show that in the interaction process of geraniol with the active site of 6PGS there is a distortion in the geometry of the ligand. Through the UV-Vis spectra, a shift of the wavelength maximum value in relation to the free geraniol is observed, of the order of 50 nm.

The microbial oxidation of geranyl-N-phenylcarbamate by fungus Beauveria bassiana was investigated. Oxidation of the C3 – C4 double bond of the parent molecule leads to regioselective formation of O-3,4-epoxyheranyl-N-phenylcarbamate in 30 % yield