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11	Molecular authentication of Chinese medicinal herbs. January 1997 (has links) by Ngan Fai Ngor Karenda. / Thesis (M.Phil.)--Chinese University of Hong Kong, 1997. / Includes bibliographical references (leaves 128-134). / Acknowledgements --- p.i / Abstract --- p.ii / Table of Contents --- p.iii / Abbreviations --- p.viii / Chapter Chapter 1 --- Authentication of Chinese Medicinal Herbs / Chapter 1.1 --- Introduction --- p.1 / Chapter 1.2 --- Traditional Identification of Chinese Herbs / Chapter 1.2.1 --- Morphology --- p.3 / Chapter 1.2.2 --- Histology --- p.4 / Chapter 1.2.3 --- Chemical Analysis --- p.4 / Chapter 1.2.4 --- Proteins and Isozymes --- p.6 / Chapter 1.3 --- Molecular Technology in Authentication / Chapter 1.3.1 --- Restriction Fragment Length Polymorphism (RFLP) --- p.6 / Chapter 1.3.2 --- Polymerase Chain Reactions (PCRs) / Chapter 1.3.2.1 --- Random-Primed PCRs --- p.8 / Chapter 1.3.2.2 --- Simple Sequence Repeats --- p.10 / Chapter 1.3.2.3 --- Amplified Fragment Length Polymorphism (AFLP) --- p.11 / Chapter 1.4 --- Objectives and Strategies of the Study --- p.13 / Chapter Chapter 2 --- Materials and Methods / Chapter 2.1 --- Reagents and Buffers / Chapter 2.1.1 --- Buffers for Total DNA Extraction --- p.15 / Chapter 2.1.2 --- Reagents for Agarose Gel Electrophoresis --- p.16 / Chapter 2.1.3 --- Reagents for Polyacrylamide Gel Electrophoresis --- p.17 / Chapter 2.1.4 --- Reagents for Plasmid and Single-Stranded DNA Preparation --- p.17 / Chapter 2.1.5 --- Media for Bacterial Culture --- p.19 / Chapter 2.1.6 --- Reagents for Preparation of Competent Cells --- p.20 / Chapter 2.2 --- DNA Isolation / Chapter 2.2.1 --- Sample Preparation --- p.21 / Chapter 2.2.2 --- Cetyl triethylammonium bromide (CTAB) Extraction --- p.21 / Chapter 2.2.3 --- Cesium Chloride Gradient Ultracentrifugation --- p.21 / Chapter 2.3 --- Phenol/Chloroform Extraction --- p.22 / Chapter 2.4 --- Ethanol Precipitation --- p.23 / Chapter 2.5 --- DNA Concentration/Purity Estimation --- p.23 / Chapter 2.6 --- Random-Primed Polymerase Chain Reactions / Chapter 2.6.1 --- Random Amplified Polymorphic DNA (RAPD) --- p.24 / Chapter 2.6.2 --- Arbitarily-Primed Polymerase Chain Reaction (AP-PCR) --- p.24 / Chapter 2.7 --- rDNA Amplification --- p.24 / Chapter 2.8 --- Agarose Gel Electrophoresis of DNA --- p.25 / Chapter 2.9 --- Purification of rDNA / Chapter 2.9.1 --- from Agarose Gel using Geneclean II Kit (Bio 101 Inc.) --- p.25 / Chapter 2.9.2 --- using Microspin´ёØ Columns --- p.26 / Chapter 2.10 --- Preparation of Escherichia coli Competent Cells --- p.26 / Chapter 2.11 --- Ligation and Transformation of Escherichia coli --- p.27 / Chapter 2.12 --- Isolation of Plasmid DNA --- p.27 / Chapter 2.13 --- Screening of Plasmid DNA by Restriction Digestion --- p.28 / Chapter 2.14 --- Isolation of Plasmid DNA / Chapter 2.14.1 --- Minipreparation of Plasmid using Magic´ёØ Miniprep DNA Purification Kit from Promega --- p.28 / Chapter 2.14.2 --- Megapreparation of Plasmid using Qiagen-tip100 --- p.28 / Chapter 2.15 --- Single-Stranded DNA Preparation / Chapter 2.15.1 --- Transfection --- p.29 / Chapter 2.15.2 --- Single-Stranded DNA Isolation --- p.29 / Chapter 2.16 --- DNA Sequencing / Chapter 2.16.1 --- Plasmid Sequencing using T7 Sequencing Kit --- p.30 / Chapter 2.16.2 --- Cycle Sequencing from PCR Products --- p.30 / Chapter 2.16.3 --- Cycle Sequencing from PCR Products or Plasmid --- p.31 / Chapter 2.16.4 --- DNA Sequencing Electrophoresis --- p.31 / Chapter Chapter 3 --- Studies of Panax Species by Random-Primed PCRs / Chapter 3.1 --- Introduction --- p.34 / Chapter 3.2 --- Materials and Methods / Chapter 3.2.1 --- Plant Materials --- p.39 / Chapter 3.2.2 --- DNA Extraction and Random-Primed PCRs --- p.39 / Chapter 3.2.3 --- Data Analysis --- p.39 / Chapter 3.3 --- Results and Discussion / Chapter 3.3.1 --- DNA Isolation --- p.40 / Chapter 3.3.2 --- DNA Fingerprinting --- p.41 / Chapter 3.3.3 --- Relationship between the Six Panax Species --- p.45 / Chapter Chapter 4 --- Studies of Acorus by Random-Primed PCRs / Chapter 4.1 --- Introduction --- p.48 / Chapter 4.2 --- Materials and Methods / Chapter 4.2.1 --- Plant Materials --- p.49 / Chapter 4.2.2 --- DNA Extraction and Random-Primed PCRs --- p.50 / Chapter 4.3 --- Results and Discussion / Chapter 4.3.1 --- Acorus DNA --- p.50 / Chapter 4.3.2 --- Reproducibility of Random-Primed PCRs --- p.51 / Chapter 4.3.3 --- DNA Fingerprinting --- p.53 / Chapter Chapter 5 --- Studies of Epimedium by Random-Primed PCRs / Chapter 5.1 --- Introduction --- p.70 / Chapter 5.2 --- Materials and Methods / Chapter 5.2.1 --- Plant Materials --- p.71 / Chapter 5.2.2 --- DNA Extraction and Random-Primed PCRs --- p.71 / Chapter 5.3 --- Results and Discussion / Chapter 5.3.1 --- DNA Extraction --- p.71 / Chapter 5.3.2 --- DNA Fingerprinting --- p.72 / Chapter Chapter 6 --- Application of AP-PCR in Commercial Ginseng Products / Chapter 6.1 --- Introduction --- p.90 / Chapter 6.2 --- Materials and Methods / Chapter 6.2.1 --- Materials --- p.91 / Chapter 6.2.2 --- DNA Extraction and Random-Primed PCRs --- p.91 / Chapter 6.2.3. --- Data Analysis --- p.91 / Chapter 6.3 --- Results and Discussion / Chapter 6.3.1 --- DNA Isolation --- p.92 / Chapter 6.3.2 --- AP-PCR Analysis --- p.93 / Chapter Chapter 7 --- Ribosomal DNA as a Marker in Authentication of Panax Species / Chapter 7.1 --- Introduction --- p.99 / Chapter 7.2 --- Materials and Methods / Chapter 7.2.1 --- Plant Materials --- p.100 / Chapter 7.2.2 --- DNA Extraction and rDNA Amplification --- p.101 / Chapter 7.2.3 --- rDNA Sequencing --- p.101 / Chapter 7.2.4 --- Generation of Restriction Fragment Length Polymorphisms / Chapter 7.2.4.1 --- Restriction Digestion of rDNA Fragment --- p.102 / Chapter 7.2.4.2 --- Polyacrylamide Gel Electrophoresis (PAGE) --- p.103 / Chapter 7.2.4.3 --- Silver Staining for Nucleic Acids --- p.103 / Chapter 7.2.5 --- Data Analysis --- p.104 / Chapter 7.3 --- Results and Discussion / Chapter 7.3.1 --- rDNA Amplification and Plasmid Isolation --- p.104 / Chapter 7.3.2 --- rDNA Sequencing / Chapter 7.3.2.1 --- Sequence Comparison between the Six Panax species and the Two Adulterants --- p.107 / Chapter 7.3.3 --- Restriction Fragment Length Polymorphisms / Chapter 7.3.3.1 --- Restriction Profiles between Ginsengs and their Adulterants --- p.113 / Chapter 7.3.3.2 --- Restrciton Profiles of Ginsengs from Different Sources --- p.118 / Chapter 7.3.4 --- Panax Phylogeny --- p.121 / Chapter Chapter 8 --- General Discussion / Chapter 8.1 --- Advantages of Random-Primed PCRs --- p.124 / Chapter 8.2 --- Weaknesses of the Random-Primed PCRs --- p.125 / Chapter 8.3 --- Molecular Markers for Phylogenetic Studies --- p.126 / Chapter 8.4 --- Specific PCR-RFLP Patterns in Authentication --- p.126 / Chapter 8.5 --- Conclusions --- p.127 / References --- p.128 / Appendix --- p.135 Medicinal plants--Identification Ginseng--Identification Plants, Medicinal Medicine, Chinese Traditional Panax
12	Immunomodulatory and adjuvant effects of ginseng extracts : with emphasis on defence mechanisms of the bovine udder / Hu, Songhua. January 2002 (has links) (PDF) Diss. (sammanfattning) Uppsala : Sveriges lantbruksuniv., 2002. / Härtill 5 uppsatser.
13	Is ginseng effective against tiredness and fatigue? Mahmod, Chenar January 2019 (has links) Bakgrund: Ginseng klassas som ett traditionellt växtbaserat läkemedel som säljs inom egenvården på apotek samt hälsokostbutiker. Det påstås att ginseng har en uppiggande effekt och anses vara effektivt mot trötthet. Trötthet finns i olika former och grader samt beror på olika faktorer. Fatigue är också en typ av trötthet men beror på en bakomliggande sjukdom och anses vara mer utmattande än trötthet. Ordet används också för att skilja det från så kallad normal trötthet. Syfte: Syftet med detta arbete är att genom systematiska sammanställningar och meta-analyser analysera om det finns bevis som stödjer påståendet om att ginseng ska vara effektivt mot trötthet och fatigue.Mål: Hitta systematiska sammanställningar samt meta-analyser genom identifiering av relevant litteratur genom en databassökning, bedöma kvaliteten genom PRISMA och sammanställa resultat för att besvara syftets frågeställning.Metoder: Litteratursökning genom relevanta databaser samt värdera de med hjälp utav PRISMA. Slutligen ska litteraturen sammanställas. Resultat: 4 systematiska sammanställningar samt 1 meta-analys ingick i analysen. De bedömdes vara av medel till hög kvalitet enligt PRISMA. Resultaten variera beroende på vilken typ av ginseng som deltagarna fick. Majoriteten av resultaten från de enskilda studierna tyder på att amerikansk och asiatisk ginseng är effektivt mot fatigue. Röd ginseng är däremot inte lika effektiv. Nio utav de sammanlagda nitton studierna gjordes på friska individer och endast två utav studierna rapporterade att ginseng hade en signifikant förbättring på trötthet.Slutsats: Amerikansk ginseng, följt av asiatisk ginseng, visade sig vara bra mot fatigue. Däremot hade röd ginseng ingen effekt på fatigue i samma grad som amerikansk och asiatisk. Dock är det svårt att påstå hur det fungerar mot just trötthet, då trötthet har många grader och beror på olika faktorer samt att det inte finns tillräckligt med belägg av bra kvalitet som kan styrka påståendet om att det skulle fungera mot trötthet, som inte är orsakad av någon bakomliggande sjukdom som fatigue. / Background: Ginseng is classified as a traditional herbal medicine sold in the self-care section at pharmacies and health food stores. It is claimed that ginseng has a revitalizing effect and is considered effective against tiredness. Tiredness exists in various forms and degrees and depends on various factors. Fatigue is also a type of tiredness but depends on an underlying disease and is more exhausting than tiredness. The word is also used to distinguish it from so-called normal tiredness.Purpose: The aim of this work is to find systematic reviews and meta-analyzes to see if there is evidence supporting the claim that ginseng is effective against tiredness and fatigue.Objective: Find systematic reviews and meta analyzes by identifying relevant literature through a database search, assessing the value of the studies through PRISMA and compiling results to answer the purpose of this work. Method: Literature search through relevant databases and assess the studies based on PRISMA’s checklist. Finally the studies should be compiled.Results: 4 systematic reviews and 1 meta-analysis were obtained. They were to be of average to high quality according to the PRISMA checklist. The results vary depending on the type of ginseng that was given to the participants. Most of the studies indicate that American and Asian ginseng are effective against fatigue. However, the studies indicate that red ginseng is not effective. Conclusion: In conclusion ginseng is effective in people with fatigue, depending on the type of ginseng it is. American ginseng, followed by Asian ginseng, proved to be good against fatigue that’s caused by an underlying illness. However, red ginseng had no effect on fatigue to the same extent as American and Asian. Also, it is difficult to claim how it works against people who are only feeling tired, as normal tiredness has many degrees and depends on various factors and that there is not enough evidence of good quality that can substantiate the claim that it would work against tiredness that’s not caused by an underlying illness. Fatigue Ginseng Meta-analyzes Panax Systematic-review Tiredness Medical and Health Sciences Medicin och hälsovetenskap
14	Organelle movement in melanophores: Effects of <em>Panax ginseng</em>, ginsenosides and quercetin Eriksson, Therese January 2009 (has links) <p><em>Panax ginseng</em> is a traditional herb that has been used for over 2000 years to promote health and longevity. Active components of ginseng include ginsenosides, polysaccharides, flavonoids, polyacetylenes, peptides, vitamins, phenols and enzymes, of which the ginsenosides are considered to be the major bioactive constituents. Although widely used, the exact mechanisms of ginseng and its compounds remain unclear. In this thesis we use melanophores from <em>Xenopus laevis</em> to investigate the effects of <em>Panax ginseng</em> extract G115 and its constituents on organelle transport and signalling. Due to coordinated bidirectional movement of their pigmented granules (melanosomes), in response to defined chemical signals, melanophores are capable of fast colour changes and provide a great model for the study of intracellular transport. The movement is regulated by alterations in cyclic adenosine 3’:5’-monophosphate (cAMP) concentration, where a high or low level induce anterograde (dispersion) or retrograde (aggregation) transport respectively, resulting in a dark or light cell. Here we demonstrate that <em>Panax ginseng</em> and its constituents ginsenoside Rc and Rd and flavonoid quercetin induce a concentration-dependent anterograde transport of melanosomes. The effect of ginseng is shown to be independent of cAMP changes and protein kinase A activation. Upon incubation of melanophores with a combination of Rc or Rd and quercetin, a synergistic increase in anterograde movement was seen, indicating cooperation between the ginsenoside and flavonoid parts of ginseng. Protein kinase C (PKC) inhibitor Myristoylated EGF-R Fragment 651-658 decreased the anterograde movement stimulated by ginseng and ginsenoside Rc and Rd. Moreover, ginseng, but not ginsenosides or quercetin, stimulated an activation of 44/42-mitogen activated protein kinase (MAPK), previously shown to be involved in both aggregation and dispersion of melanosomes. PKC-inhibition did not affect the MAPK-activation, suggesting a role for PKC in the ginseng- and ginsenoside-induced dispersion but not as an upstream activator of MAPK.</p> / <p><em>Panax ginseng </em>är ett av de vanligaste naturläkemedlen i världen och används traditionellt för att öka kroppens uthållighet, motståndskraft och styrka. Ginseng är ett komplext ämne bestående av ett antal olika substanser, inklusive ginsenosider, flavonoider, vitaminer och enzymer, av vilka de steroidlika ginsenosiderna anses vara de mest aktiva beståndsdelarna. Flavonoider (som finns i till exempel frukt och grönsaker) och ginseng har genom forskning visat sig motverka bland annat hjärt-och kärlsjukdomar, diabetes, cancer och demens. Trots den omfattande användningen är dock mekanismen för hur ginseng verkar fortfarande oklar. I den här studien har vi använt pigmentinnehållande celler, melanoforer, från afrikansk klogroda för att undersöka effekterna av <em>Panax ginseng</em> på pigment-transport och dess maskineri. Melanoforer har förmågan att snabbt ändra färg genom samordnad förflyttning av pigmentkorn fram och tillbaka i cellen, och utgör en utmärkt modell för studier av intracellulär transport. Förflyttningen regleras av förändringar i halten av cykliskt adenosin-monofosfat (cAMP) i cellen, där en hög eller låg koncentration medför spridning av pigment över hela cellen (dispergering) eller en ansamling i mitten (aggregering), vilket resulterar i mörka respektive ljusa celler. Här visar vi att <em>Panax ginseng</em>, ginsenosiderna Rc och Rd samt flavonoiden quercetin stimulerar en dispergering av pigmentkornen. När melanoforerna inkuberades med en kombination av ginsenosid Rc eller Rd och quercetin, kunde en synergistisk ökning av dispergeringen ses, vilket tyder på en samverkan mellan ginsenosid- och flavonoid-delarna av ginseng. Ett protein som tidigare visats vara viktigt för pigmenttransporten är mitogen-aktiverat protein kinas (MAPK), och här visar vi att också melanoforer stimulerade med ginseng, men dock inte med ginsenosider eller quercetin, innehåller aktiverat MAPK. Genom att blockera enzymet protein kinas C (PKC) (känd aktivator av dispergering), minskade den ginseng- och ginsenosid-inducerade dispergeringen, medan aktiveringen av MAPK inte påverkades alls. Detta pekar på en roll för PKC i pigment-transporten men inte som en aktivator av MAPK.</p> melanophores Panax ginseng ginsenosides quercetin organell anterograde transport endothelin-3 mitogen activated protein kinase protein kinase C MEDICINE MEDICIN
15	Organelle movement in melanophores: Effects of Panax ginseng, ginsenosides and quercetin Eriksson, Therese January 2009 (has links) Panax ginseng is a traditional herb that has been used for over 2000 years to promote health and longevity. Active components of ginseng include ginsenosides, polysaccharides, flavonoids, polyacetylenes, peptides, vitamins, phenols and enzymes, of which the ginsenosides are considered to be the major bioactive constituents. Although widely used, the exact mechanisms of ginseng and its compounds remain unclear. In this thesis we use melanophores from Xenopus laevis to investigate the effects of Panax ginseng extract G115 and its constituents on organelle transport and signalling. Due to coordinated bidirectional movement of their pigmented granules (melanosomes), in response to defined chemical signals, melanophores are capable of fast colour changes and provide a great model for the study of intracellular transport. The movement is regulated by alterations in cyclic adenosine 3’:5’-monophosphate (cAMP) concentration, where a high or low level induce anterograde (dispersion) or retrograde (aggregation) transport respectively, resulting in a dark or light cell. Here we demonstrate that Panax ginseng and its constituents ginsenoside Rc and Rd and flavonoid quercetin induce a concentration-dependent anterograde transport of melanosomes. The effect of ginseng is shown to be independent of cAMP changes and protein kinase A activation. Upon incubation of melanophores with a combination of Rc or Rd and quercetin, a synergistic increase in anterograde movement was seen, indicating cooperation between the ginsenoside and flavonoid parts of ginseng. Protein kinase C (PKC) inhibitor Myristoylated EGF-R Fragment 651-658 decreased the anterograde movement stimulated by ginseng and ginsenoside Rc and Rd. Moreover, ginseng, but not ginsenosides or quercetin, stimulated an activation of 44/42-mitogen activated protein kinase (MAPK), previously shown to be involved in both aggregation and dispersion of melanosomes. PKC-inhibition did not affect the MAPK-activation, suggesting a role for PKC in the ginseng- and ginsenoside-induced dispersion but not as an upstream activator of MAPK. / Panax ginseng är ett av de vanligaste naturläkemedlen i världen och används traditionellt för att öka kroppens uthållighet, motståndskraft och styrka. Ginseng är ett komplext ämne bestående av ett antal olika substanser, inklusive ginsenosider, flavonoider, vitaminer och enzymer, av vilka de steroidlika ginsenosiderna anses vara de mest aktiva beståndsdelarna. Flavonoider (som finns i till exempel frukt och grönsaker) och ginseng har genom forskning visat sig motverka bland annat hjärt-och kärlsjukdomar, diabetes, cancer och demens. Trots den omfattande användningen är dock mekanismen för hur ginseng verkar fortfarande oklar. I den här studien har vi använt pigmentinnehållande celler, melanoforer, från afrikansk klogroda för att undersöka effekterna av Panax ginseng på pigment-transport och dess maskineri. Melanoforer har förmågan att snabbt ändra färg genom samordnad förflyttning av pigmentkorn fram och tillbaka i cellen, och utgör en utmärkt modell för studier av intracellulär transport. Förflyttningen regleras av förändringar i halten av cykliskt adenosin-monofosfat (cAMP) i cellen, där en hög eller låg koncentration medför spridning av pigment över hela cellen (dispergering) eller en ansamling i mitten (aggregering), vilket resulterar i mörka respektive ljusa celler. Här visar vi att Panax ginseng, ginsenosiderna Rc och Rd samt flavonoiden quercetin stimulerar en dispergering av pigmentkornen. När melanoforerna inkuberades med en kombination av ginsenosid Rc eller Rd och quercetin, kunde en synergistisk ökning av dispergeringen ses, vilket tyder på en samverkan mellan ginsenosid- och flavonoid-delarna av ginseng. Ett protein som tidigare visats vara viktigt för pigmenttransporten är mitogen-aktiverat protein kinas (MAPK), och här visar vi att också melanoforer stimulerade med ginseng, men dock inte med ginsenosider eller quercetin, innehåller aktiverat MAPK. Genom att blockera enzymet protein kinas C (PKC) (känd aktivator av dispergering), minskade den ginseng- och ginsenosid-inducerade dispergeringen, medan aktiveringen av MAPK inte påverkades alls. Detta pekar på en roll för PKC i pigment-transporten men inte som en aktivator av MAPK. melanophores Panax ginseng ginsenosides quercetin organell anterograde transport endothelin-3 mitogen activated protein kinase protein kinase C MEDICINE MEDICIN
16	Desenvolvimento de néctares mistos de frutas tropicais adicionados de Ginkgo biloba e Panax ginseng / Development of tropical fruit mixed nectars with addition of Ginkgo biloba e Panax ginseng Sousa, Paulo Henrique Machado de 06 November 2006 (has links) Submitted by Reginaldo Soares de Freitas (reginaldo.freitas@ufv.br) on 2016-11-11T16:46:37Z No. of bitstreams: 1 texto completo.pdf: 682521 bytes, checksum: 869569e287896b20f5fe279b28aee120 (MD5) / Made available in DSpace on 2016-11-11T16:46:37Z (GMT). No. of bitstreams: 1 texto completo.pdf: 682521 bytes, checksum: 869569e287896b20f5fe279b28aee120 (MD5) Previous issue date: 2006-11-06 / Conselho Nacional de Desenvolvimento Científico e Tecnológico / Com o apelo da mudança para hábitos saudáveis, observa-se o aumento do consumo de fruta fresca em todo o mundo, que se estende aos sucos processados. Bebidas com novos sabores e aromas estão sendo elaboradas, sendo as bebidas mistas de frutas mais uma opção para os consumidores e uma tendência do mercado internacional. A adição de componentes funcionais também vem sendo feita, e os extratos de Ginkgo biloba e Panax ginseng vêm como uma nova opção, por apresentarem inúmeros benefícios à saúde, agregando valor aos produtos de frutas. Diante do exposto, o presente trabalho objetivou a elaboração de néctares mistos à base de caju, manga e acerola, adicionados de extratos de Ginkgo biloba e Panax ginseng e a mistura dos dois extratos, além de estudar a estabilidade dos produtos por um período de seis meses. Foram formulados néctares mistos de frutas tropicais, a partir de 35% de polpa e sólidos solúveis totais padronizados a 11 °Brix. Os teores de polpas variaram segundo um delineamento de misturas: caju (12,25%-21,00%); acerola (1,75%-10,50%); e manga (12,25%-21,00%). A formulação com 12,25% de caju, 21,00% de manga e 1,75% de acerola foi a mais aceita pelos provadores, e apresentou 49,9 mg de vitamina C/100mL de néctar. As respostas sensoriais também foram avaliadas através de análise de agrupamento e os grupos obtidos foram submetidos à análise de componentes principais, revelando a existência de três grupos distintos entre os provadores, indicando claramente a segmentação dos consumidores que preferiam formulações diferenciadas. A adição de extratos de Ginkgo biloba, Panax ginseng e a mistura de ambos em concentrações 15, 20, 25 e 30mg/100mL de néctar foi testada nos néctares, observando-se diminuição das notas de aceitação com o aumento da concentração dos extratos. Foram selecionados os néctares com adição de 15 mg de extrato de Ginkgo biloba/100 mL, 20 mg de extrato de Panax ginseng / 100 mL e a mistura com 10 mg de extrato de Ginkgo biloba e 10 mg de extrato de Panax ginseng/100 mL para avaliação da estabilidade durante 180 dias de armazenamento em condições similares às de comercialização. O tratamento térmico de 90 oC / 60s, conjuntamente com a adição de benzoato de sódio e metabissulfito foram suficientes para garantir a estabilidade microbiológica dos néctares formulados à temperatura ambiente. Os valores de pH, sólidos solúveis, acidez, e açúcares redutores apresentaram pouca variação ao longo dos 180 dias de armazenamento a temperatura ambiente. Os teores de vitamina C foram os que apresentaram maiores variações em todos os néctares mistos de frutas no decorrer de armazenamento. O tempo de armazenamento não afetou a qualidade sensorial dos produtos; sendo que a adição de extrato de Ginkgo biloba ao néctar misto de frutas alterou a aceitação pelos consumidores, sendo a aceitação destes produtos menores. Os resultados sensoriais foram avaliados através da metodologia de Mapa de Preferência Interno, que permitiu identificar a segmentação dos consumidores no aroma, sabor e impressão global, podendo ser feita uma identificação e caracterização de preferências e grupos consumidores. Os néctares sem adição de extrato (controle) e com adição de Panax ginseng foram os mais aceitos pelos consumidores em todos os atributos testados. / With the appealing of changes to healthy habits, it is observed that the consumption of fresh fruit has increased all over the world, and processed juices are an extension of that. Beverages presenting new flavors and aromas are being elaborated; being the mixed fruit drinks one more option to consumers and a trend to international market. The addition of functional components can also be noticed, and extracts of Ginkgo biloba e Panax ginseng are new options, once they present large benefits to human s health and aggregate value to fruit products. According to what was quoted, the actual work had as objective to develop mixed nectars based on cashew apple, mango and acerola, added to extracts of Ginkgo biloba e Panax ginseng and the mix of both extracts, as well as to study the stability of the developed products for six months. They were developed mixed nectars of tropical fruit formulated with at least 35% of pulp and total soluble solids, with 11°Brix. The values of pulp varied according to design of the mixtures: cashew apple (12.25%-21.00%); acerola (1.75%-10.50%); and mango (12.25%-21.00%). The formulation containing 12.25% of cashew apple, 21.00% of mango and 1.75% of acerola was best accepted among the panelists, and it showed 49.9mg of vitamin C/100mL of nectar. The sensorial responses were also evaluated trough cluster analyses and the obtained groups were submitted to main components analyses, showing the existence of three distinct groups among the panelists, indicating clearly consumer s segmentation that preferred different formulations. The addition of Ginkgo biloba and Panax ginseng extracts and the mixture of both in concentrations of 15, 20, 25 and 30mg/100ml nectar were tested at nectars; it was observed that values decreased as the concentration of the extract was being enhanced. They was selected the nectars with addition of 15mg of Ginkgo biloba extract/100 mL, 20 mg of Panax ginseng extract/100 mL and the mixture containing 10 mg of de Ginkgo biloba extract and 10 mg of Panax ginseng extract/100 mL for stability evaluation for the period of 180 days of storage in similar conditions of commercialization. The thermal treatment of 90 o C / 60s, combined to the addition of sodium benzoate and sodium metabisulfite were sufficient to guarantee microbiological stability of the formulated nectars at room temperature. The values of pH, soluble solids, acidity and reducing sugar showed little variation during 180 days of storage at room temperature. The contents of vitamin C were the ones that presented the highest variations in all mixed fruit nectars during the storage. The storage period did not affect the sensorial quality of the products, besides that, the addition of Ginkgo biloba extract to the mixed fruit nectar altered the consumers acceptance, being these products acceptance the lowest ones. The sensorial results were evaluated trough internal preference mapping methodology, which allowed an identification of the consumers segmentation of aroma, flavor and global impression, being possible an identification of characterization of preferences and consumers groups. The nectars without the addition of extract (control) and addition of Panax ginseng were preferred by consumers in all tested attributes. Polpa de frutas - Composição Polpa de frutas - Avaliação sensorial Alimentos - Microbiologia Alimentos - Conservação Ginkgo biloba Panax ginseng Ciências Agrárias
17	Mycorrhizal Symbiosis in Forest-Grown American Ginseng (Panax quinquefolius), and the Effect of Mycorrhizal Colonization on Root Ginsenoside Concentrations Filyaw, Tanner R. 19 September 2017 (has links) No description available. Agriculture Alternative Medicine Biochemistry Biology Botany Ecology Environmental Studies Pharmacology Plant Biology Plant Sciences American ginseng ginseng Panax quinquefolius mycorrhizae arbuscular mycorrhizal fungi ginsenosides wild-simulated forest-grown
18	Avaliação dos aspectos toxicológicos dos fitoterápicos: um estudo comparativo / Evaluation of toxicological aspects of the herbal medicines:a comparative study Turolla, Monica Silva dos Reis 13 April 2004 (has links) Esta Dissertação apresenta informações gerais sobre os medicamentos fitoterápicos e os aspectos toxicológicos de uma amostra de dez plantas medicinais comercializadas como medicamentos fitoterápicos no Brasil, pesquisados junto aos principais bancos de dados e fontes públicas de informação. A análise dos medicamentos fitoterápicos cobre as dimensões histórica, econômica e farmacêutica. No tocante aos aspectos toxicológicos, foram avaliados os dados de toxicidade pré-clínica de dez plantas selecionadas, e realizado um levantamento das informações publicadas para Hypericum perforatum e Piper methysticum, relacionadas ao termo toxicidade, segundo três importantes bancos de dados. Adicionalmente, este trabalho aborda as propostas para realização de ensaios de toxicidade pré-clínica para os fitoterápicos segundo a OMS e legislação brasileira, e as normas para avaliação de substâncias químicas segundo a OECD. / This thesis presents general information on herbal medicines and on the toxicological aspects of a sample of ten medicinal plants traded as herbal medicines in Brazil. The survey was carried out in the main databases and public sources of information. The analysis on the herbal medicines encompasses the historical, economic and pharmaceutical dimensions. In what concerns toxicological aspects, data on pre-clinical toxicity were evaluated for Hypericum perforatum and Piper methysticum, these keywords being related to toxicity in three important databases. In addition, this study discusses the proposals for pre-clinical toxicity trials on herbal medicines according to WHO and the Brazilian legislation, and the standards for evaluation of chemical substances according to OECD. aesculus hippocastanum aesculus hippocastanum cimicifuga racemosa cimicifuga racemosa ginkgo biloba ginkgo biloba herbal medicines hypericum perforatum hypericum perforatum medicamentos fitoterápicos medicinal plants panax ginseng panax ginseng passiflora incarnata passiflora incarnata piper methysticum piper methysticum plantago ovata plantago ovata plantas medicinais rhamnus purshiana Rhamnus purshiana toxicological aspects Valeriana officinalis Valeriana officinalis
19	Avaliação dos aspectos toxicológicos dos fitoterápicos: um estudo comparativo / Evaluation of toxicological aspects of the herbal medicines:a comparative study Monica Silva dos Reis Turolla 13 April 2004 (has links) Esta Dissertação apresenta informações gerais sobre os medicamentos fitoterápicos e os aspectos toxicológicos de uma amostra de dez plantas medicinais comercializadas como medicamentos fitoterápicos no Brasil, pesquisados junto aos principais bancos de dados e fontes públicas de informação. A análise dos medicamentos fitoterápicos cobre as dimensões histórica, econômica e farmacêutica. No tocante aos aspectos toxicológicos, foram avaliados os dados de toxicidade pré-clínica de dez plantas selecionadas, e realizado um levantamento das informações publicadas para Hypericum perforatum e Piper methysticum, relacionadas ao termo toxicidade, segundo três importantes bancos de dados. Adicionalmente, este trabalho aborda as propostas para realização de ensaios de toxicidade pré-clínica para os fitoterápicos segundo a OMS e legislação brasileira, e as normas para avaliação de substâncias químicas segundo a OECD. / This thesis presents general information on herbal medicines and on the toxicological aspects of a sample of ten medicinal plants traded as herbal medicines in Brazil. The survey was carried out in the main databases and public sources of information. The analysis on the herbal medicines encompasses the historical, economic and pharmaceutical dimensions. In what concerns toxicological aspects, data on pre-clinical toxicity were evaluated for Hypericum perforatum and Piper methysticum, these keywords being related to toxicity in three important databases. In addition, this study discusses the proposals for pre-clinical toxicity trials on herbal medicines according to WHO and the Brazilian legislation, and the standards for evaluation of chemical substances according to OECD. aesculus hippocastanum cimicifuga racemosa ginkgo biloba hypericum perforatum medicamentos fitoterápicos panax ginseng passiflora incarnata piper methysticum plantago ovata plantas medicinais Rhamnus purshiana Valeriana officinalis aesculus hippocastanum cimicifuga racemosa ginkgo biloba herbal medicines hypericum perforatum medicinal plants panax ginseng passiflora incarnata piper methysticum plantago ovata rhamnus purshiana toxicological aspects Valeriana officinalis
20	Recherche de nouvelles substances naturelles d'intérêt dans la prévention de la fibrose rénale d'origine médicamenteuse / Research of new natural substances of interest in the prevention of drug induced renal fibrosis Bunel, Valérian 03 November 2014 (has links) Les reins sont les organes cibles de nombreuses molécules toxiques. Les cellules épithéliales du tubule proximal rénal sont particulièrement vulnérables vis-à-vis de xénobiotiques utilisés comme médicaments ou non. Ces agressions peuvent être corrélées à une augmentation du stress oxydatif et induire la mort cellulaire. Elles peuvent également mener à la perte des caractéristiques phénotypiques des cellules épithéliales, initiant leur dédifférenciation en cellules mésenchymateuses et éventuellement en fibroblastes, principaux responsables de la fibrose rénale.<p>Les stratégies de protection – notamment implémentées en clinique lors de l'administration de médicaments néphrotoxiques – reposant sur une approche pharmacologique restent rares.<p>A partir de données de médecines traditionnelles, nous avons sélectionné une série de plantes considérées utiles pour le traitement ou la prévention de troubles associés aux maladies rénales :Angelicae sinensis radix, Eleutherococci radix, Ginseng radix, Schisandrae chinensis fructus et Silybi mariani fructus.<p>A l'aide d'un modèle in vitro reposant sur l'emploi de la lignée cellulaire HK-2, nous avons examiné si ces produits pouvaient apporter une protection efficace vis-à-vis de 3 xénobiotiques néphrotoxiques :les acides aristolochiques, le cisplatine et la ciclosporine. Cinq phénomènes impliqués dans la néphrotoxicité et couramment retrouvés lors du développement de la fibrose rénale ont été investigués :(i) la mortalité cellulaire et l'apoptose ;(ii) la génération de stress oxydatif ;(iii) la modulation des capacités de régénération ;(iv) la production de matrice extracellulaire ;et (v) l'activation de la voie de signalisation de la β-caténine. <p>Parmi les 5 plantes étudiées sur ce modèle, celle présentant l'activité la plus intéressante vis-à-vis de l'un des 3 toxiques a été investiguée plus en détails afin d'identifier le(s) composé(s) responsable(s) de sa bioactivité. Les résultats ont indiqué que l'extrait méthanolique d'Angelica sinensis était le plus efficace pour réduire la néphrotoxicité induite par le cisplatine. Ces principes actifs – l'acide férulique, le Z-ligustilide et le E-ligustilide – ont été testés selon la même méthodologie. <p>L'acide férulique a été le plus efficace pour améliorer la survie cellulaire et diminuer l'apoptose induite par le cisplatine. Il a également permis de réduire la production de matrice extracellulaire, de stimuler les capacités de régénération de cellules saines et d'inhiber partiellement la voie de signalisation de la β-caténine. Il n'a toutefois pas été capable de limiter la génération de stress oxydatif induite par le traitement au cisplatine. <p>L'acide férulique semble être un candidat prometteur pour protéger les tubules rénaux vis-à-vis du cisplatine et pourrait contribuer à limiter l'initiation et le développement de la fibrose rénale. <p>/<p>The kidneys are targets of numerous toxic compounds. Proximal tubular epithelia cells are particularly vulnerable to xenobiotics used as drugs or not. These injuries can be associated with an increased oxidative stress and can trigger cell death. They can also lead to the loss of phenotypic characteristics of epithelial cells and initiate their dedifferentiation in mesenchymal cells, eventually evolving in fibroblasts, major actors responsible for renal fibrosis. <p>Protective strategies – including those implemented in clinical practice during the administration of nephrotoxic drugs – relying on a pharmacological approach remain seldom.<p>By means of data issuing from traditional medicines, we selected a series of herbs potentially useful for the treatment or prevention of troubles associated with kidney diseases: Angelicae sinensis radix, Eleutherococci radix, Ginseng radix, Schisandrae chinensis fructus and Silybi mariani fructus.<p>Using an in vitro model based on HK-2 cell line, we examined if these herbal products could bring an effective protection towards 3 nephrotoxic drugs: aristolochic acids, cisplatin and ciclosporin. Five phenomena involved in nephrotoxicity and regularly occurring during the progression of renal fibrosis were investigated: (i) cell death and apoptosis; (ii) oxidative stress generation; (iii) modulation of regeneration capacities; (iv) extracellular matrix production; and (v) β-catenin pathway activation.<p>Among the 5 herbs that were studied, the one presenting the most interesting effects towards one of the 3 toxicants has been investigated in details in order to identify the compound(s) responsible for its bioactivity. Results indicated that the crude methanolic extract of Angelica sinensis was the most potent for reducing cisplatin-induced nephrotoxicity. Its active principles – ferulic acid, Z-ligustilide and E-ligustilide – were tested according to the same methods.<p>Ferulic acid was the most potent compound for improving cell survival and for alleviating cisplatine-induced apoptosis. It also allowed to restrain the extracellular matrix production, enhanced the regeneration capacities of healthy cells and partially inhibited the activation of the β-catenin pathway. It was however ineffective in preventing the generation of oxidative stress induced during cisplatin treatment. <p>Ferulic acid appears as a promising candidate for protecting renal tubules against cisplatin's nephrotoxicity and could contribute to limit the onset and progression of renal fibrosis. / Doctorat en Sciences biomédicales et pharmaceutiques / info:eu-repo/semantics/nonPublished Sciences pharmaceutiques Kidneys -- Fibrosis Xenobiotics -- Metabolism Oxidative stress Reins -- Fibrose Xénobiotiques -- Métabolisme Stress oxydatif Panax ginseng néphroprotection matrice extracellulaire collagen cisplatin cell survival & apoptosis Angelica sinensis in vitro HK-2 découverte de médicament fibrose rénale collagène

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