In vitro efficacy of isoflavonoids and terpenes against Leishmania (Leishmania) infantum and L. amazonensis.

The main form of control of leishmaniasis is the treatment, however various side effects and poor efficacy are associated with presently available drugs. The investigation of bioactive natural products for new antileishmanial drugs is a valid approach. The present study reports the in vitro efficacy of natural isoflavonoids and terpenes against Leishmania infantum and L. amazonensis and their cytotoxicity against HepG2 cells. L. infantum and L. amazonensis promastigotes were exposed to the terpenes kaurenoic acid, xylopic acid, and (-)-α-bisabolol and to the isoflavonoids (-)-duartin and (3R)-claussequinone for antileishmanial activity and to cytotoxicity to HepG2 cells. The most effective substance against both L. infantum and L. amazonensis species was (3R)-claussequinone (IC50 = 3.21 µg/mL and 2.47 µg/mL, respectively) that disclosed low cytotoxicity against HepG2 cells (CC50 = 387.79 µg/mL). The efficacy of (3R)-claussequinone against intracellular amastigotes of L. infantum and the externalization of phosphatidylserine in promastigotes of this isoflavanoid were investigated by infection of Raw 264.7 macrophages and marking with Annexin V-FITC and propidium Iodide for flow cytometry analysis. The results for amastigotes showed that (3R)-claussequinone was able to reduce the rate of infection with IC50 = 4.61 µg/mL and did not alter the externalization of phosphatidylserine. In conclusion it is presently reported, for the first time, the striking antileishmanial activity of (3R)-claussequinone against L. infantum and L. amazonensis associated to low cytotoxicity. Furthermore, these results suggest that (3R)-claussequinone is a new hit aiming to develop new therapeutic alternatives.

Efficacy of lapachol on treatment of cutaneous and visceral leishmaniasis.

Leishmaniasis is one of the most important neglected diseases worldwide. It is a life-threatening disease and causes significant morbidity, long-term disability, and early death. Treatment involves disease control or use of intervention measures, although the currently used drugs require long-lasting therapy, and display toxicity and reduced efficacy. The use of natural products isolated from plants, such as lapachol, an abundant naphthoquinone naturally occurring in South American Handroanthus species (Tabebuia, Bignoniaceae), is a promising option for the treatment of leishmaniasis. In this study, we investigated the leishmanicidal activity of lapachol in vitro and in vivo against Leishmania infantum and L. amazonensis, causative agents of visceral and cutaneous leishmaniasis, respectively. Low cytotoxicity in HepG2 cells (3405.8 ±â€¯261.33 µM), good anti-Leishmania activity, and favorable selectivity indexes (SI) against promastigotes of both L. amazonensis (IC50 = 79.84 ±â€¯9.10 µM, SI = 42.65) and L. infantum (IC50 = 135.79 ±â€¯33.04 µM, SI = 25.08) were observed. Furthermore, anti-Leishmania activity assays performed on intracellular amastigotes showed good activity for lapachol (IC50 = 191.95 µM for L. amazonensis and 171.26 µM for L. infantum). Flow cytometric analysis demonstrated that the cytotoxic effect of lapachol in Leishmania promastigotes was caused by apoptosis-like death. Interestingly, the in vitro leishmanicidal effect of lapachol was confirmed in vivo in murine models of visceral and cutaneous leishmaniasis, as lapachol (25 mg/kg oral route for 24 h over 10 days) was able to significantly reduce the parasitic load in skin lesions, liver, and spleen, similar to amphotericin B, the reference drug. These results reinforce the therapeutic potential of lapachol, which warrants further investigations as an anti-leishmaniasis therapeutic.

Phytochemical characterization and antioxidant, antibacterial and antimutagenic activities of aqueous extract from leaves of Alchornea glandulosa.

Plant extracts exist as a complex matrix which serves as a source of numerous bioactive metabolites. The ultra performance liquid chromatography with diode-array detection-coupled electrospray ionization-mass spectrometry/mass spectrometry technique was used to characterize the aqueous extract from leaves of Alchornea glandulosa (EAG), a species popularly used to treat gastrointestinal problems as an antiulcer agent. Quantification of phenolic derivatives was determined using Folin-Ciocalteu and aluminum trichloride (AlCl3) methods. In addition, antioxidant (2,2-diphenyl-1-picrylhydrazyl [DPPH•] radical scavenging, ß-carotene-linoleic acid, and lipid peroxidation), antibacterial (agar well diffusion method and minimum inhibitory concentration), antimutagenic (Ames test), and antigenotoxic (plasmid cleavage) assays were also performed on this plant extract. The ellagitannin tris-galloyl-hexahydroxydiphenic acid-glucose was identified as the predominant compound along with tannins as majority metabolites. EAG showed high antioxidant activity accompanied by moderate antibacterial activity against Staphylococcus aureus. The highest antimutagenic activity was observed for TA97 strain without metabolic activation (S9) and with metabolic activation, TA100 and TA102 were completely inhibited. In addition, EAG exhibited potential signs of antigenotoxic action. The high antioxidant and antimutagenic activity observed for EAG suggests important therapeutic uses that still need to be verified in future studies.

Structure-based drug design studies of the interactions of ent-kaurane diterpenes derived from Wedelia paludosa with the Plasmodium falciparum sarco/endoplasmic reticulum Ca²âº-ATPase PfATP6.

Malaria is responsible for more deaths around the world than any other parasitic disease. Due to the emergence of strains that are resistant to the current chemotherapeutic antimalarial arsenal, the search for new antimalarial drugs remains urgent though hampered by a lack of knowledge regarding the molecular mechanisms of artemisinin resistance. Semisynthetic compounds derived from diterpenes from the medicinal plant Wedelia paludosa were tested in silico against the Plasmodium falciparum Ca2+-ATPase, PfATP6. This protein was constructed by comparative modelling using the three-dimensional structure of a homologous protein, 1IWO, as a scaffold. Compound 21 showed the best docking scores, indicating a better interaction with PfATP6 than that of thapsigargin, the natural inhibitor. Inhibition of PfATP6 by diterpene compounds could promote a change in calcium homeostasis, leading to parasite death. These data suggest PfATP6 as a potential target for the antimalarial ent-kaurane diterpenes.

Bioprospection for antiplasmodial activity, and identification of bioactive metabolites of native plants species from the Mata Atlântica biome, Brazil.

A total of 33 extracts of eleven different plants species from Mata Atlântica biome, Brazil, and different fractions of the bioactive extracts were evaluated against chloroquine-resistant Plasmodium falciparum W2 strain by PfLDH method and cytotoxicity to HepG2 cells by the MTT assay, and chemically characterized by LC-DAD-ESI-MS/MS analysis. The results allowed the identification of Alchornea glandulosa, Miconia latecrenata, and Psychotria suterella as the most active plant species. Different flavonoids and tannins in Alchornea glandulosa and Miconia latecrenata besides alkaloids in Psychotria suterella were identified. Bioguided fractionation of A. glandulosa and M. latecrenata leaves extracts led to fractions exhibiting high parasite growth inhibition. Seven known alkaloids were identified in the P. suterella extract, and of these, only 5-carboxystrictosidine had been assayed for antiplasmodial activity what points to this species as the most promising among the eleven one assayed.

Phytochemistry and antiplasmodial activity of Xylopia sericea leaves.

Aiming to investigate the antiplasmodial activity and the phytochemical composition of Xylopia sericea leaves, the essential oil and dichloromethane extract were analyzed by gas and liquid chromatography, respectively, both of them coupled to mass spectrometry, and were evaluated against the chloroquine-resistant Plasmodium falciparum strain (W2) and for cytotoxicity to HepG2 cells. Low growth inhibition of P. falciparum as well as low cytotoxicity to HepG2 cells were observed for the essential oil. The leaves dichloromethane extract showed moderate growth inhibition of P. falciparum and low cytotoxicity to HepG2 cells. Bioguided chromatographic fractionation of this extract led to fractions with increased antiplasmodial activity from which liriodenine (IC50 6.1 ± 0.1 µg/mL, CC50 > 1000.0 µg/mL, SI > 164), an aporphine alkaloid, and an acetogenin-rich fraction containing mainly isomers of annomontacin and 4-deoxy-annomontacin (IC50 22.7 ± 1.9 µg/mL, CC50 336.1 ± 15.5 µg/mL, SI = 15) might be highlighted for their antiplasmodial activity.

Antiplasmodial activity and cytotoxicity, isolation of active alkaloids, and dereplication of Xylopia sericea leaves ethanol extract by UPLC-DAD-ESI-MS/MS.

OBJECTIVES: To assess the antiplasmodial activity of the ethanol extract of Xylopia sericea leaves, Annonaceae, often associated with antimalarial use and to perform a bioguided isolation of active compounds. METHODS: Dereplication of ethanol extract by the UPLC-DAD-ESI-MS/MS technique allowed the identification of the major constituents, isolation and identification of alkaloids. The antiplasmodial and cytotoxic activity of the extract, fractions and isolated compounds was evaluated against the chloroquine-resistant W2 strain Plasmodium falciparum and HepG2 cells, respectively. KEY FINDINGS: Ethanol extract showed high reduction of parasitemia as well as moderate cytotoxicity (86.5 ± 3.0% growth inhibition at 50 µg/ml and CC50 72.1 ± 5.1 µg/ml, respectively). A total of eight flavonoids were identified, and two aporphine alkaloids, anonaine and O-methylmoschatoline, were isolated. Anonaine disclosed significant antiplasmodial effect and moderate cytotoxicity (IC50 23.2 ± 2.7 µg/ml, CC50 38.3 ± 2.3 µg/ml, SI 1.6) while O-methylmoschatoline was not active against P. falciparum and showed a low cytotoxicity (33.5 ± 1.9% growth inhibition at 50 µg/ml, CC50 274.4 ± 0.5 µg/ml). CONCLUSIONS: Characterization of Xylopia sericea leaves ethanol extract by UPLC-DAD-ESI-MS/MS as well as its antiplasmodial activity and the occurrence of anonaine and O-methylmoschatoline in this Xylopia species are reported by the first time.

Quinolinotriazole antiplasmodials via click chemistry: synthesis and in vitro studies of 7-Chloroquinoline-based compounds

Malaria is nowadays one of the most serious health concerns in a global scale and, although there is an evident increase in research studies in this area, pointed by the vast number of hits and leads, it still appears as a recurrent topic every year due to the drug resistance shown by the parasite exposing the urgent need to develop new antimalarial medications. In this work, 38 molecules were synthesized via copper(I)-catalyzed alkyne-azide cycloaddition (CuAAC) or "click" chemistry, following different routes to produce 2 different organic azides, obtained from a 4,7 dicholoquinoline, reacted with 19 different commercially available terminal alkynes. All those new compounds were evaluated for their in vitro activity against the chloroquine resistant malaria parasite Plasmodium falciparum (W2). The cytotoxicity evaluation was accomplished using Hep G2 cells and SI index was calculated for every molecule. Some of the quinoline derivatives have shown high antimalarial activity, with IC50 values in the range of 1.72-8.66 µM, low cytotoxicity, with CC50>1000 µM and selectivity index (SI) in the range of 20-100, with some compounds showing SI>800. Therefore, the quinolinotriazole hybrids could be considered a very important step on the development of new antimalarial drugs

Estudo químico e avaliação da atividade antimalárica dos galhos de Piranhea trifoliata / Chemical study and antimalarial activity evaluation of branches of Piranhea trifoliata

Este trabalho teve como objetivos realizar o estudo químico dos galhos de Piranhea trifoliata (Picrodendraceae) e avaliar o seu potencial antimalárico. Foram realizadas duas coletas no Estado do Pará. O material foi seco, moído e extraído com diclorometano (DCM), metanol (MeOH) e água (H2O). Os extratos DCM e MeOH foram submetidos à análise em cromatografia em camada delgada comparativa (CCDC), e apresentaram características principalmente de terpenos. Do estudo fitoquímico do extrato DCM da 2ª coleta, foi isolada: friedelan-3-ona e do extrato MeOH da 2ª coleta foi isolado: o triterpeno esqualeno, e mistura dos esteroides estigmasterol e ß-sitosterol. Quanto à atividade antimalárica, os extratos e as fases dos extratos MeOH foram avaliados in vitro frente ao Plasmodium falciparum, e os extratos MeOH da 1ª e 2ª coletas foram considerados ativos (CI50 = 13,7 µg/mL; CI50 = 5,8 µg/mL, respectivamente). Este trabalho contribuiu para o conhecimento biológico e químico da espécie Piranhea trifoliata e da família Picrodendraceae, sendo este o primeiro relato de atividades biológicas para a espécie em estudo.

Plantas leishmanicidas da Amazônia Brasileira: uma revisão / Leishmanicidal plants from Brazilian Amazonia: a review

As leishmanioses constituem grave problema de saúde pública, ocorrendo em 98 países. O Brasil é responsável pela, quase, totalidade dos casos notificados de Leishmaniose Visceral (LV) nas Américas, e a doença está em processo de urbanização. A Leishmaniose Tegumentar (LT) também apresenta ampla distribuição mundial. No Brasil, a região Norte possui o maior número de casos confirmados, a maioria deles causados por Leishmania (L.) amazonensis. Os fármacos de primeira escolha para o tratamento das leishmanioses são derivados do antimônio pentavalente (Sb5+), como o glucantime, o mais utilizado no Brasil. Fármacos antimoniais apresentam vários efeitos adversos, além disso, nos últimos anos, o problema agravou com o surgimento de resistência dos parasitos a estes medicamentos. A necessidade de novos fármacos leishmanicidas eficazes vem despertando o interesse em pesquisas de plantas utilizadas para este fim em países endêmicos, levando ao reconhecimento de produtos naturais ativos, os quais podem representar marcadores químico-biológicos para o desenvolvimento de fitoterápicos eficazes e seguros, novos fármacos ou protótipos para a síntese de substâncias químicas potencialmente ativas. O objetivo da presente revisão é destacar os trabalhos publicados sobre plantas leishmanicidas da Amazônia Brasileira e motivar um maior interesse para pesquisas na área.

Estudo farmacobotânico das folhas de Aspidosperma excelsum Benth. (Apocynaceae) / Pharmacobotanical study of the leaves of Aspidosperma excelsum Benth. (Apocynaceae)

Aspidosperma excelsum Benth. (Apocynaceae) é uma planta nativa da Amazônia brasileira, usada na medicina tradicional à base de plantas, especialmente para o tratamento de malária. Neste trabalho foram realizadas análises anatômicas, histoquímicas, fitoquímicas, fisícas e físico-químicas com as folhas de A. excelsum, visando auxiliar em sua distinção taxonômica, além de fornecer parâmetros de qualidade para futuros estudos farmacognósticos com a espécie. Amostras de folhas foram coletadas em Santa Bárbara, Estado do Pará. Para as análises estruturais e histoquímicas foram utilizadas técnicas usuais em anatomia vegetal. Algumas classes de metabólitos secundários foram detectadas a partir de Cromatografia de Camada Delgada. Os parâmetros físicos e físico-químicos foram avaliados a partir de análises de granulometria, teor de cinzas totais, cinzas insolúveis em ácido, umidade e pH. A folha de A. excelsum possui face abaxial com cutícula ornamentada, tricomas tectores, laticíferos articulados ramificados e idioblastos com conteúdo cristalífero e acidófilo. A análise histoquímica revelou que os idioblastos apresentam composição heterogênea, como compostos fenólicos, taninos, alcaloides e lipídeos. A análise fitoquímica confirmou uma presença destas substâncias, além de heterosídeos flavônicos e esteroides. Os testes físicos e físico-químicos são dados inéditos para as folhas de A. excelsum.

Bioguided isolation of an antiviral compound from Xylophragma myrianthum (Cham.) Sprague (Bignoniaceae Juss.)

Espécies do gênero Xylophragma Sprague são trepadeiras pertencentes à família Bignoniaceae Juss. (tribo Bignonieae Dumort.) e algumas tem um amplo espectro de usos medicinais, incluindo o tratamento de infecções. No presente artigo relatamos o fracionamento do extrato etanólico de caules de Xylophragma myrianthum (Cham.) Sprague biomonitorado por testes de atividade contra Human herpesvirus 1 (HSV-1), Dengue virus 2 (DENV-2), Encephalomyocarditis virus murino (EMCV) e Vaccinia vírus (VACV), o que levou ao isolamento de uma substância ativa, XM-1. Análises espectroscópicas permitiram a identificação desta como sendo o triterpeno ácido arjúnico, cuja atividade anti-DENV-2 e ocorrência em Bignoniaceae são relatadas pela primeira vez. X. myrianthum revela-se, portanto, como fonte de uma substância e frações antivirais.

Structure-based drug design studies of the interactions of ent-kaurane diterpenes derived from Wedelia paludosa with the Plasmodium falciparum sarco/endoplasmic reticulum Ca2+-ATPase PfATP6

Malaria is responsible for more deaths around the world than any other parasitic disease. Due to the emergence of strains that are resistant to the current chemotherapeutic antimalarial arsenal, the search for new antimalarial drugs remains urgent though hampered by a lack of knowledge regarding the molecular mechanisms of artemisinin resistance. Semisynthetic compounds derived from diterpenes from the medicinal plant Wedelia paludosa were tested in silico against the Plasmodium falciparum Ca2+-ATPase, PfATP6. This protein was constructed by comparative modelling using the three-dimensional structure of a homologous protein, 1IWO, as a scaffold. Compound 21 showed the best docking scores, indicating a better interaction with PfATP6 than that of thapsigargin, the natural inhibitor. Inhibition of PfATP6 by diterpene compounds could promote a change in calcium homeostasis, leading to parasite death. These data suggest PfATP6 as a potential target for the antimalarial ent-kaurane diterpenes.

Genotoxicity of lapachol evaluated by wing spot test of Drosophila melanogaster

This study investigated the genotoxicity of Lapachol (LAP) evaluated by wing spot test of Drosophila melanogaster in the descendants from standard (ST) and high bioactivation (HB) crosses. This assay detects the loss of heterozygosity of marker genes expressed phenotypically on the fly's wings. Drosophila has extensive genetic homology to mammals, which makes it a suitable model organism for genotoxic investigations. Three-day-old larvae from ST crosses (females flr³/TM3, Bd s x males mwh/mwh), with basal levels of the cytochrome P450 and larvae of high metabolic bioactivity capacity (HB cross) (females ORR; flr³/TM3, Bd s x males mwh/mwh), were used. The results showed that LAP is a promutagen, exhibiting genotoxic activity in larvae from the HB cross. In other words, an increase in the frequency of spots is exclusive of individuals with a high level of the cytochrome P450. The results also indicate that recombinogenicity is the main genotoxic event induced by LAP.

Estudo farmacognóstico comparativo das folhas de Davilla elliptica A. St.-Hil. e D. rugosa Poir., Dilleniaceae / Comparative pharmacognostic study of leaves of Davilla elliptica A. St.-Hil. e D. rugosa Poir., Dilleniaceae

As características farmacognósticas das folhas de Davilla elliptica A. St.-Hil. e D. rugosa Poir., Dilleniaceae, foram determinadas com objetivo de auxiliar na identificação taxonômica e no controle de qualidade das drogas vegetais e de produtos fitoterápicos. A espécie D. elliptica é um arbusto ereto, que ocorre naturalmente no cerrado e D. rugosa é um trepadeira lenhosa de beira de mata. Ambas são conhecidas popularmente como lixeirinha, sambaibinha e cipó-caboclo, empregadas na medicina tradicional como antiinflamatória e antiúlcera. As características microscópicas observadas em D. rugosa tais como tricomas estrelados e esclereídes no mesofilo e em D. elliptica de idioblastos contendo mucilagem e endoderme, são parâmetros que poderão ser utilizados na diferenciação das espécies. Os teores obtidos nos ensaios de pureza e nos doseamentos de taninos (9,4 por cento e 7,2 por cento), flavonoides (0,46 por cento e 0,9 por cento) e mucilagens (2,2 por cento e 4,1 por cento) de ambas as espécies, podem contribuir no controle de qualidade das drogas vegetais uma vez que são usadas indistintamente na produção de fitoterápicos.

The characters pharmacognostics of leaves of Davilla elliptica St. Hil. and Davilla rugosa Poir. of Dilleniaceae family were determinated for aiming in taxonomic and quality control of vegetable drugs and phytotherapic produtcs. The specie of D. elliptica is an erect shrub, that occurs naturally in cerrado and D. rugosa is a scandent shrub of forest edge. Both are populary known as "lixeirinha", "sambaibinha" and "cipó-caboclo" and used in popular medicine as anti-inflammatory and antiulcer. The microscopic characteristics observed like strellate trichomes and sclereids in the mesophyll in D. rugosa and the idioblasts with mucilage and endodermis in D. elliptica are parameter that will be used to differentiate the species. The content obtained in tests of purity and the tannins (9.4 percent and 7.2 percent), flavonoids (0.46 percent and 0.9 percent) and mucilage (2.2 percent and 4.1 percent) of both species help in quality control of vegetable drugs since they are indistinctly used in production of phytotherapics.

Antiviral activities of plants occurring in the state of Minas Gerais, Brazil: Part 2. Screening Bignoniaceae species / Atividade antiviral de extratos de plantas coletadas no estado de Minas Gerais: Parte 2. Triagem de Bignoniaceae

Ethanol extracts of eighteen Bignoniaceae species have been evaluated by the MTT assay for cytotoxicity in Vero cells and for antiviral activity against Human herpes virus type 1, Vaccinia virus and murine Encephalomyocarditis virus. Among such species, seven are reported to be of traditional medicinal use No cytotoxicity was observed for most of the extracts up to the concentration of 500 μg/mL. Fourteen (50 percent) of the 28 extracts assayed have disclosed antiviral activity with EC50 values in the range of 4.6+0.3 to 377.2+17.7 μg/mL. Only two species, Arrabidaea samydoides and Callichlamys latifolia, have shown activity against all the three viruses. The extracts were chemically characterized by their TLC and HPLC-DAD profiles. Mangiferin is the major constituent of A. samydoides but the isolated compound has been less active than the crude extract. This is the first report on the antiviral evaluation of the eighteen Bignoniaceae species assayed.

Extratos etanólicos de dezoito espécies vegetais pertencentes à família Bignoniaceae, das quais sete são descritas como de uso medicinal, foram avaliados, pelo ensaio colorimétrico do MTT, para atividades citotóxica, em células Vero, e antiviral, frente aos vírus herpes simplex-tipo 1, vaccinia e encefalomiocardite murina. A maior parte dos extratos não apresentou citotoxicidade até a concentração de 500 μg/mL. Dos 28 extratos testados quatorze (50 por cento) apresentaram atividade antiviral com valores de CE50 na faixa de 4,6+03 a 377,2+17,7 μg/mL. Somente duas espécies, Arrabidaea samydoides e Callichlamys latifolia, foram ativas frente aos três vírus. Os extratos foram caracterizados pelos seus perfís cromatográficos em CCD e CLAE-FR. Análises por CLAE-FR mostraram que a mangiferina é o constituinte majoritário em A. samydoides mas a substância isolada foi menos ativa do que o extrato bruto. Esta é a primeira vez que se relata a atividade antiviral de extratos das dezoito espécies avaliadas.

Anatomia e histoquímica dos órgãos vegetativos de Polygonum hydropiperoides Michx., Polygonaceae / Anatomical and histochemical characters of Polygonum hydropiperoides Michaux, Polygonaceae

Polygonum hydropiperoides Michaux é uma espécie conhecida popularmente como "erva-de-bicho", amplamente utilizada na medicina tradicional como anti-hemorroidal, antiinflamatória e antidiarréica. O presente trabalho tem como objetivo a caracterização anatômica e histoquímica da folha, caule e raiz, que constituem a droga vegetal, visando estabelecer parâmetros para o controle de qualidade. O material vegetal foi fixado e submetido às técnicas usuais de microscopia de luz e aos testes histoquímicos. A folha é anfiestomática, dorsiventral e com estômatos paracíticos e anisocíticos. É comum a presença de estruturas secretoras como: tricomas glandulares capitados e glândulas epidérmicas e subepidérmicas em ambas as faces da lâmina foliar e também no caule. O material secretado pelas glândulas apresenta composição heterogênea de lipídios e flavonóides, segundo análises histoquímicas. Cristais de oxalato de cálcio e grãos de amido são freqüentes em células parenquimáticas da folha e do caule. Compostos fenólicos estão presentes na folha (parênquima paliçádico), no caule (parênquima cortical e floema) e na raiz (parênquima cortical).

P. hydropiperoides is popularly known as "erva-de-bicho", and it is used in traditional medicine as anti-hemorroidal, anti-inflammatory and antidiarrhoeic. The present work has as objective the anatomical and histochemical characterization of leaf, stem and root that are used as drug in order to offer elements for quality control. The botanical material was prepared for the usual optical and histochemical microtechniques. The leaf is amphistomatic, dorsiventral and paracytic and anisocytic stomata. It is common to find the presence of secretory structures as: capitate glandular trichomes and secretory glands on both epidermis, that are also present in stem. The secretion material is heterogeneous composition of lipids and flavonoids. Druses of calcium oxalate and starch are common in parenchyma cells of leaf and stem. Phenolic compounds are present in leaf (palisade parenchyma), in stem (cortical parenchyma and phloem) and root (cortical parenchyma).

In vitro antiplasmodial activity of extract and constituents from Esenbeckia febrifuga, a plant traditionally used to treat malaria in the Brazilian Amazon

Esenbeckia febrifuga (Rutaceae) is a plant traditionally used to treat malaria in the Brazilian Amazon region. Ethanol extract of stems displayed a good antiplasmodial activity against Plasmodium falciparum strains W-2 (IC(50) 15.5+/-0.71mug/ml) and 3 D7 (IC(50) 21.0+/-1.4mug/ml). Two coumarins (bergaptene 1 and isopimpinellin 2), five alkaloids (flindersiamine 3, kokusaginine 4, skimmiamine 5, gamma-fagarine 6 and 1-hydroxy-3-methoxy-N-methylacridone, 7), besides a limonoid (rutaevine 8), have been isolated for the first time from this species. Antiplasmodial activity of compounds 3, 5-8 has been evaluated in vitro against P. falciparum strains (W-2 and 3D7) and the furoquinolines 5 and 6 were the most potent displaying IC(50) values <50mug/ml; flindersiamine (3) showed a weak activity while alkaloid 7 and rutaevine (8) were inactive (IC(50)>100mug/ml)...(AU)

Antimicrobial activity of Trembleya laniflora, Xyris platystachia and Xyris pterygoblephara

Trembleya laniflora (D. Don) Cogn. (Melastomataceae), Xyris platystachia Alb. Nilss. (Xyridaceae) and Xyris pterygoblephara Kunth., Brazilian species collected from a biodiversity hotspot for conservation priority, had their antimicrobial activity evaluated against standardized strains of Staphylococcus aureus and Micrococcus luteus, by the agar diffusion assay. All extracts, assayed in the concentration of 2000 µg/disc, were active against M. luteus, whereas S. aureus growth was inhibited only by T. laniflora leaves and X. platystachia aerial parts. Fractionation of the extracts by partition between immiscible solvents resulted in active fractions from extracts originally inactive against S. aureus. Activity was mainly found in low and medium polar fractions. The extract of T. laniflora leaves was also fractionated by silica gel column chromatography and both the HPLC fingerprint and antimicrobial activity of the obtained fractions were distinct of those originated from the partition process.

As espécies Trembleya laniflora (Melastomataceae), Xyris platystachia (Xyridaceae) e Xyris pterygoblephara foram coletadas na Serra do Cipó, região considerada hotspot para conservação de biodiversidade. A atividade antimicrobiana dessas espécies foi avaliada em ensaios in vitro de difusão em ágar frente a linhagens padronizadas de Staphylococcus aureus e Micrococcus luteus. Todos os extratos, avaliados na concentração de 2000 µg/disco, foram ativos contra M. luteus, enquanto a inibição de crescimento de S. aureus somente foi observada para os extratos de T. laniflora (folhas) e X. platystachia (partes aéreas). A partição dos extratos brutos entre solventes imiscíveis resultou na obtenção de frações ativas, oriundas de extratos originalmente inativos frente a S. aureus, observando-se atividade principalmente para as frações de baixa e média polaridade. O extrato de folhas de T. laniflora foi adicionalmente fracionado por cromatografia em coluna de sílica gel e as frações resultantes apresentaram atividade antimicrobiana e perfis por CLAE distintos daquelas obtidas pela partição entre solventes imiscíveis.