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Antimalarial activity and cytotoxicity of some South African medicinal plants and their active constituentsSekhoacha, Mamello January 2008 (has links)
Includes bibliographical references (leaves 150-187).
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The interaction of verapamil with the human malaria parasite : Plasmodium falciparumVan Schalkwyk, Donelly Andrew January 2004 (has links)
Includes bibliographical references (leaves [129]-144).
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The antimalarial potential of Ugandan traditional medicines : a study of six plants used to treat malaria symptomsWaako, Paul January 2003 (has links)
Bibliography: leaves 102-122. / The study investigates the antimalarial potential of six Ugandan traditional medicinal plants Senecfo discifolius oliv, Senecio stuhlmannii, Indigofera emarginella steud. Ex A. Rich, Aspifia africana (Pers) C.D. Adams, Cardiospermum halicacabum L. and Momordica foetida Schumch. Et Thonn. Selection of the plants was based on ethnobotanical surveys of traditional treatment of malaria symptoms and reports from traditional healers practising in three different communities.
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Investigation of non-prostatic in vitro prostate-specific membrane antigen expression in MCF-7 and MDA-MB-231 breast tumour cellsTshabalala, Malvin Thabani January 2020 (has links)
Introduction
Breast and prostate cancer mutually represent the most commonly occurring malignancies worldwide in women and men, respectively. The mutative state, recurrence capacity, resistance to conventional chemotherapy, low success rate of surgery and risks associated with radiotherapy confound the management of both these malignancies. There are several similarities between breast and prostate cancer, like growth hormone dependence and similar chemotherapeutic interventions. Therapy based on radiopharmaceuticals targeting the prostate-specific membrane antigen (PSMA) is proving to be a cutting-edge theranostics intervention for prostate cancer. Clinical positron emission tomography (PET) scans have located anti-PMSA binding sites in breast cancer in vivo. This indicates possible non-prostatic expression of PSMA, therefore research focused on understanding the cellular kinetics, PSMA expression profiles using two breast cancer adenocarcinoma cell lines as breast cancer models. This approach was to assess PSMA as a biomarker molecule that can aid in development of more selective, effective and safe diagnostic and therapeutic alternatives for breast cancer. This study was aimed at evaluating PSMA expression of MCF-7 or MDA-MB-231 mammary adenocarcinoma cell lines in comparison to a known high PSMA expressing LNCaP prostate carcinoma and EA.hy926 hybrid vascular endothelial cell line.
Methods
In vitro cultures of LNCaP’s , a prostatic adenocarcinoma cell line, MCF-7 and MDA-MB-231 breast adenocarcinoma cell lines and endothelial EA.hy926 cells were tested for expression of PSMA by flow cytometry. The LNCaP cells were used a positive control. Cellular localisation of PSMA was achieved utilising confocal microscopy and fluorescently-tagged antibodies in all the cell lines tested. PSMA was quantified in all the cell lines utilising ELISA. Prior to experimentation, a pilot study was undertaken to optimise cell detachment methods. Trypsinisation was compared to mechanical scraping to evaluate a cell detachment method that allowed optimal downline experimentation.
Results
Findings from three supporting and complementary techniques demonstrate positive PSMA identification, localisation and quantification in all the probed cell lines despite three cell types not having a prostrate origin. Quantitatively, LNCaP cells reported the highest concentration of PSMA followed by the malignant MDA-MB-231 cells, then the MCF-7 cell line and least in EA.hy926 cells. The difference in fluorescence between LNCaP cells and all three investigational cell lines was statistically significant however the difference in fluorescence between the three investigational cell lines was not statistically significant. The PSMA antigen was localised on the cell membrane and diffused within the cytosol in LNCaP cells. The MDA-MB-231, MCF-7 and EA.hy926 cells all exhibited a differential expression pattern of PSMA. These cells showed diffuse cytosolic accumulation and intense circular region accumulation apparently bordering the cell membrane and the cell nucleus. The quantification of PSMA reported the highest concentration as being in LNCaP cells. The MDA-MB-231 cells were second, then the MCF-7 cells and the lowest concentration. Significant differences were seen between the positive control and the investigation cell lines. The difference in concentration between the investigational cell lines was not significant. Finally, cryotome sections of biopsies of tumours from two breast cancer patients were found to show detectable PSMA presence.
Discussion
Fluorescence is directly proportional to concentration. The high fluorescence of PSMA exhibited by LNCaP cells in the flow cytometry results can be equated to concentration. A fundamental point of departure from which PSMA expression in the breast carcinoma cell lines could be investigated was established. Expression of PSMA is associated with cancer aggression, metastatic progression and increased malignancy. These clinicopathological characteristics support the expression of PSMA seen in MDA-MB-231. Contrastingly, the same characteristics aren’t seen in MCF-7 cells but expression of PSMA was observed. The expression is not entirely dismissible as other luminal A cell lines have also been shown to express PSMA. The EA.hy926 cells are somatic hybrids that are made up of lung A549 cells and HUVEC’s. Lung cancer has been shown to also express PSMA when probed utilising histology. The expression of PSMA in EA.hy926 is the first of its kind but may be attributable to its lung carcinoma makeup. The pattern of expression in the LNCaP confocal microscopy images can be expected. The PSMA antigen is a transmembrane receptor and as such intense fluorescence was seen on the membrane. Expression of PSMA in the cytoplasm has been reported and was equally observed in the LNCaP cells. The investigation cell line showed accumulation of green fluorescence in vesicular bodies bordering the cell membrane and in juxtanuclear positions. The expression of PSMA has been reported in the mitochondria and the green fluorescence at the nucleus could be mitochondrial. The Golgi apparatus and endoplasmic reticulum have also been recognised as potential location of PSMA expression. The localisation of both these organelles at the nucleus along with the expression of PSMA seen close to the nucleus could be associated. Worth noting is the internalisation properties of PSMA. The antigen has an internalisation signal that can be induced by ligand binding or in the absence of a ligand. Upon internalisation the receptors are vesicled and transported either for degradation of for recycling. The vesicular expression seen close to the membrane in the investigational cell lines could be PSMA that is being trafficked for recycling or degradation upon internalisation. The ELISA quantification revealed the levels of PSMA in the positive control are 100-fold greater than those in the investigation cell lines. The ability to translate PSMA targeting in clinical settings is questionable when considering the difference in concentration values. The probing of PSMA in histological slices was positive and showed patterns that are similar to those seen in the monolayer cultures. This shows continuity between two-dimensional cultures and heterogeneous tissue samples. The premise for investigation of PSMA as a potential theranostic target was established through positive identification, localisation and quantification across three independents methods.
Conclusion
This study is the first of its kind to report reproducible expression of PSMA in the two-dimensional cultures of breast adenocarcinoma MDA-MB-231 and MCF-7 cell lines as well as in the hybrid endothelial EA.hy926 cell line. The results were confirmed by three different techniques where different antibodies were used for the ELISA showing reproducibility in the findings. Moreover, the generated results support the apparent localisation of PSMA in breast cancer patients utilising PSMA targeting radionuclides in PET imaging in a clinical setting. The potential application of this study’s result is stimulating. The success being realised in prostate cancer theranostics through PSMA targeting, may conceivably be realised in other carcinomas, particularly breast carcinoma theranostics. / Dissertation (MSc)--University of Pretoria, 2020. / https://doi.org/10.25403/UPresearchdata.14885454 / Pharmacology / MSc / Unrestricted
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A Pharmacological investigations of South Africa Lichens, Dessication-tolerant Plants and Medicinal Tree, Warburgia SalutarisKellermann, Tracy January 2010 (has links)
No description available.
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The therapeutic effectiveness of some local Nigerian plants used in the treatment of malariaMelariri, Paula E January 2010 (has links)
Includes abstract. / Includes bibliographical references (leaves 184-219). / In Nigeria most of the populace relies heavily on medicinal plants for the treatment of malaria. This thesis describes the investigation of the antiplasmodial properties of seven plants used in the traditional treatment of malaria in Nigeria. The seven plants include Mangifera indica L., Citrus limon L. Burm.f, Musa sapientum L., Psidium guajava L., Carica papaya L., Cymbopogon citratus Staph, and Vernonia amygdalina Delile. These plants are widely distributed in Nigeria and are used in Nigerian folk medicine to treat malaria and febrile illnesses. It is apparent that experimental evaluation of herbal drugs for the treatment of malaria is rather impressive, however, only few are in the market and very few have reached clinical trials. Researchers need to take more active interest in the investigation and standardization of herbal drugs with potent antimalarial activity.
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Variability in the pharmacokinetics of rifapentine in South African tuberculosis patients : a classical and population approachLangdon, Grant January 2004 (has links)
Includes bibliographical references (leaves 101-115). / Tuberculosis is recognised as one of the leading public health problems in sub-Saharan Africa. The treatment and control of the disease depends largely on a limited number of chemotherapeutic agents, most of which have been used for the past 30 years. Discovery and development of new antimycobacterial agents has been relatively stagnant. New impetus from the Global Alliance for Tuberculosis Drug Development aims to register a new faster-acting and affordable drug by 2010. Until such an agent is freely available, though, it is necessary to use the available means at our disposal. Treatment regimens based on rifapentine, with its less demanding schedule, lack of autoinduction and increased absorption following food intake could make it an excellent candidate to anchor an intermittent chemotherapy regimen. The studies thus far on patients receiving proven bioavailable preparations of rifapentine do not comment on the respective plasma levels but have concentrated on specific outcomes. As a result little is known as to the magnitude of variability in plasma levels amongst patients receiving rifapentine. This degree of variability may prove to be important as rifapentine continues to be investigated as an alternative to rifampicin. This thesis describes the pharmacokinetics of rifapentine in a South African tuberculosis patient population with special reference to variability in serum drug levels between patients and between occasions. Forty-five patients received rifapentine doses of 600, 750 and 900 mg based on body weight. Doses were administered on study days one and five. All patients had already received not less than four weeks and no more than six weeks of standard antimycobacterial therapy (isoniazid, rifampicin, pyrazinamide and ethambutol). In total, twenty blood samples were collected per patient from 0 - 168 hours. Rifapentine and 25desacetyl rifapentine concentrations were determined using validated high pressure liquid chromatography methods. Median peak plasma concentrations, time to reach this peak, plasma elimination half-lives and area under the concentration-time curve were calculated for both parent drug and metabolite on both occasions using non-compartmental methods. The pharmacokinetics of the parent drug was best described using a one-compartment model, with a lag time and first-order absorption and elimination. Estimated population parameters were absorption rate constant, lag time on absorption, clearance/bioavailability, and volume of distribution/bioavailability. Between subject and between occasion variability was below 25% for all parameters except KA which showed a between subject variability of 52%. The pharmacokinetics of the metabolite in this study were best described by a one-compartment model with no first-pass metabolism and a clearance value that declined in a non-linear fashion over time. Parameters estimated were, volume of distribution, induced metabolite clearance, baseline metabolite clearance, and slope of decline in clearance over time. In South African tuberculosis patients the 15 mg/kg dose of rifapentine was well absorbed and well tolerated. The variability observed between individuals and between occasions was small and similar to that seen in data from previous studies in healthy volunteers.
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Investigation of the phytochemistry and biological activity of isoquinoline alkaloids isolated from the South African medicinal plants, cyrtanthus sanguineus (Lindl.) walp. and cyrtanthus obliquus (L.f.)aitBrine, Natalie Dawn January 2001 (has links)
Bibliography: p. 128-140. / The term "traditional medicine" refers to the ways of protecting and restoring health that existed before the arrival of modern medicine. These approaches to health belong to the traditions of each country and have been handed down from generatio to generation.
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A study of the immune response in murine experimental malaria, with special reference to the effects of South African medicinal plants, artesunate and chloroquineGumede, Bonginkosi January 2003 (has links)
Bibliography: leaves 151-175.
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The isolation, characterization and antiplasmodial activity of two novel dimeric sesquiterpenes from Dicoma anomalaTselanyane, Malefa Lydia January 2006 (has links)
Includes bibliographical references (leaves 180-208). / The study investigates the antimalarial potential of a Southern African traditional medicinal plant, Dicoma anomala (Sond.). The plant is used to treat a variety of treatments including fevers. The extracts of the leaves and twigs have been reported to treat malaria and fever but the treatments with the roots are unrelated to malaria.
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