Distribution of Systemic Macrolides to Gingiva Crevicular Fluid: Effect on Crevicular Fluid Flow

Ho, Weiting

15 July 2009

No description available.

Dental Care

Azithromycin

Anti-inflammatory

Gingival Crevicular Fluid

Comparison of the Effects of Deracoxib, Buffered Aspirin, and Placebo on the Gastric Mucosa of Healthy Dogs

Sennello, Kathleen Ann

04 May 2005

This study tested the hypothesis that administration of deracoxib, a cyclooxygenase-2 specific (COX-2) inhibitor, would result in lower gastric lesion scores than administration of buffered aspirin and gastric lesion scores similar to placebo when administered to healthy dogs for 28 days. Twenty-four, healthy, random source dogs were divided into three groups. Group I received buffered aspirin, 23.6 mg/kg PO q 8h, group II received deracoxib, 1.6 mg/kg PO q 24h and placebo twice daily PO q 8h after deracoxib administration, and group III received placebo PO q 8h. Gastroscopy was performed on days -7, 6, 14, and 28 of treatment. Four regions of the stomach (pylorus, incisura, cardia, and body) were evaluated separately and lesions scored on a scale of 1 (mucosal hemorrhage) to 12 (perforating ulcer) by an observer unaware of which treatments the dogs received. Dogs were observed every 8 hours for vomiting, diarrhea and anorexia. Feces were scored from 1-5 (scores <4 were considered diarrhea). Lesion scores for each group, at each location, and total scores, at each time period, were evaluated for the effects of time and treatment using a Kruskal-Wallis test. Total dog days of vomiting and dog days of diarrhea in each group were compared using a Wilcoxon rank sums test. Significance was determined at p<0.05. Significantly higher median total gastric lesion scores were found in the aspirin group compared to the deracoxib or placebo groups on days 6, 14, and 28. There were no significant differences in median total gastric lesion scores between the deracoxib or placebo groups at any time during the study. There was no location effect on gastric lesion scores and there was no significant change in gastric lesion scores over time in any of the groups during treatment. Significantly more dog-days of vomiting occurred in the aspirin group as compared to the deracoxib group. No significant differences were found between groups for dog-days of diarrhea. In this study, the administration of deracoxib to healthy dogs resulted in significantly lower gastric lesion scores compared to dogs receiving aspirin and lesion scores similar to those receiving placebo. / Master of Science

gastroscopy

cyclooxygenase

gastric ulceration

non-steroidal anti-inflammatory drugs

canine

A pivotal role for interleuking-4 in Atorvastatin-associated neuroprotection in rat brain.

Clarke, R.M., Lyons, A., O'Connell, F., Deighan, B.F., Barry, C.E., Anyakoha, Ngozi G., Nicolaou, Anna, Lynch, M.A.

January 2008

No / Inflammatory changes, characterized by an increase in pro-inflammatory cytokine production and up-regulation of the corresponding signaling pathways, have been described in the brains of aged rats and rats treated with the potent immune modulatory molecule lipopolysaccharide (LPS). These changes have been coupled with a deficit in long-term potentiation (LTP) in hippocampus. The evidence suggests that anti-inflammatory agents, which attenuate the LPS-induced and age-associated increase in hippocampal interleukin-1ß (IL-1ß) concentration, lead to restoration of LTP. Here we report that atorvastatin, a member of the family of agents that act as inhibitors of 3-hydroxy-3-methylglutaryl-CoA reductase, exerts powerful anti-inflammatory effects in brain and that these effects are mediated by IL-4 and independent of its cholesterol-lowering actions. Treatment of rats with atorvastatin increased IL-4 concentration in hippocampal tissue prepared from LPS-treated and aged rats and abrogated the age-related and LPS-induced increases in pro-inflammatory cytokines, interferon-¿ (IFN¿) and IL-1ß, and the accompanying deficit in LTP. The effect of atorvastatin on the LPS-induced increases in IFN¿ and IL-1ß was absent in tissue prepared from IL-4¿/¿ mice. The increase in IL-1ß in LPS-treated and aged rats is associated with increased microglial activation, assessed by analysis of major histocompatibility complex II expression, and the evidence suggests that IFN¿ may trigger this activation. We propose that the primary effect of atorvastatin is to increase IL-4, which antagonizes the effects of IFN¿, the associated increase in microglial activation, and the subsequent cascade of events.

Atorvastatin

Brain

Inflamation

Anti-inflammatory effects

Rat model

Interleukin-4

In Vitro and in Vivo Evaluation Of Pharmacological Activites of Pouzolzia Sanguinea

Ahsan, M.Q., Alam, M.T., Chowdhury, M.M.U., Nasim, Md. Talat, Islam, S.M.S.

13 November 2024

Yes / Pouzolzia sanguinea grows in tropical and sub-tropical regions of Bangladesh, used for a variety of purposes including pain, rheumatoid kidney diseases in traditional medicine. The crude ethanolic leaf extract of P. sanguinea with its different fractions (ethanol, n-hexane, and chloroform) was investigated for phytochemical constituents, in vitro antioxidant, anti-inflammatory effects, in-vivo analgesic and antipyretic activities. Preliminary phytochemical constituents were identified by chemical group test. P. sanguinea fractionated extracts contain alkaloids, glycosides, tannins, flavonoids, saponins, gums, and amides. Antioxidant activity test was performed by both qualitative (TLC and Rf value) and quantitative tests (inhibition of DPPH free radical scavenging). Extracts exhibited significant (p <0.001, p <0.0001) inhibition of DPPH free radical scavenging activity as compared to the standard drug ascorbic acid at similar doses. In vitro anti-inflammatory activity was determined by protein denaturation of egg albumin method. The percent inhibition of protein denaturation in the experiment of ethanol extract was found significantly higher (p <0.0001) compared with chloroform and n-hexane extracts. In addition, in vivo analgesic and antipyretic effects were determined in mice by acetic acid-induced writhing and yeast-induced pyrexia methods. The ethanol extracts of P. sanguinea exhibited inhibition of writhing reflex on mice by 71.58% at the dose of 500 mg/kg body weight which had greater analgesic activity than other n-hexane and chloroform extracts. In the anti-pyretic test, fractional extracts ethanol, chloroform, and n-hexane at a dose of 500 mg/kg body weight significantly (p <0.05) decreased pyrexia in mice up to 3 h as compared with the positive control paracetamol drug at a dose of 150 mg/kg body weight. In our in vitro and in vivo study models, it is evident that Pouzolzia sanguinea fractionated extracts showed significant antioxidant, anti-inflammatory, analgesic, and antipyretic activities.

Analgesic

Antipyretic

Anti-inflammatory

Phytochemical screening

Pouzolzia sanguinea

Estudo fitoquímico e potencial biológico de cactos da Mata Atlântica do gênero Rhipsalis Gärtner (Cactaceae) /

Kamikawachi, Renan Canute.

January 2019

Orientador: Wagner Vilegas / Resumo: Apesar dos diversos relatos do uso de Rhipsalis Gaërtn (Cactaceae) por populações tradicionais no tratamento de uma gama de enfermidades, há pouquíssimos estudos fitoquímicos com esse grupo de cactos e por vezes estes são superficiais, apenas indicando a possível presença de algumas classes de produtos naturais. Ademais, estudos avaliando a atividade biológica de Rhipsalis são escassos. Neste viés, este trabalho objetivou investigar a composição química do gênero Rhipsalis e avaliar possíveis atividades ligadas à sua composição, subsidiando desta forma seu uso popular. Esta dissertação foi dividida e organizada da seguinte forma: a primeira parte apresenta uma introdução geral sobre plantas medicinais e sua importância, assim como uma revisão sobre estudos fitoquímicos em Cactaceae. Em seguida, foram redigidas três seções: na primeira, investigamos a composição química de Rhipsalis teres (Vell.) Steud identificando 5 saponinas derivadas do ácido oleanólico, 2 flavonoides C-glicosilados derivados da apigenina e 2 ácidos fenólicos; na segunda, investigamos a composição química do gênero Rhipsalis identificando 28 saponinas cujo core é o ácido oleanólico e 8 flavonoides, também sugerimos fingerprints para cada espécie avaliada com base nas substâncias majoritárias, os resultados quantitativos obtidos por UPLC-MS foram eficientes na identificação das espécies com base na filogenia; na terceira, avaliamos as atividades antioxidante, antifúngica e anti-inflamatória de espécies de R... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Despite the several reports of the use of Rhipsalis Gaërtn (Cactaceae) by traditional populations in the treatment of a range of diseases, there are very few phytochemical studies with this group and sometimes these are superficial, only indicating the possible presence of some classes of natural products. In addition, there are very few studies evaluating the biological activity of Rhipsalis. Therefore, this work aimed to investigate the chemical composition of the genus Rhipsalis and to evaluate possible activities related to its composition, thus subsidizing its popular use. This dissertation was divided and organized as follows: the first part presents a general introduction on medicinal plants and their importance as well as a review on phytochemical studies in Cactaceae. Then, three sections were written: in the first one, we investigated the chemical composition of Rhipsalis teres, identifying 5 saponins derived from oleanolic acid, 2 C-glycosilated flavonoids derived from apigenin and 2 phenolic acids; in the second section, we investigate the chemical composition of the genus Rhipsalis identifying 28 saponins whose core is oleanolic acid and 8 flavonoids, we also suggested fingerprints for each species evaluated on the basis of the majority compounds, the quantitative results obtained by UPLC-MS were efficient in the identification of the species based on the phylogeny; in the third, we evaluated the antioxidant, antifungal and anti-inflammatory activities of Rhipsal... (Complete abstract click electronic access below) / Mestre

espectrometria de massas

Saponinas.

Datiloscopia.

anti-inflamatória

mass spectrometry

saponins

anti-inflammatory

Controlled nanoparticle production by flash nanoprecipitation using a multi-inlet vortex mixer: comparative assessment with two profens of different physicochemical properties. / CUHK electronic theses & dissertations collection

January 2013

研究目的：本論文之研究主要旨在採用兩種非甾體抗炎藥--布洛芬（IBP）及氟比洛芬（FBP）來考察一項新型的納米粒子製備技術--瞬時納米沉澱技術（FNP）。IBP和FBP具有不同理化性質，但其親油性屬大部分藥物所具的典型親油性 （log P = 2-5）。研究證實IBP和FBP有治療阿爾茨海默氏病的潛在藥效，但在血液中廣泛與血漿蛋白結合，導致其腦血管通透性很低。因此，本研究的另一目的為考察FNP製備的納米處方是否能改善此類藥物的大腦遞送。 / 方法：應用FNP，用多入口渦旋混合器（MIVM）將藥物載入聚乙二醇-聚乳酸（PEG-PLA）的納米粒中。通過改變關鍵工藝流程變量考察了變量對納米粒物理性質及穩定性的影響。使用動態光散射儀測定了納米粒粒徑和粒徑分佈，使用zeta 電位分析測定了粒子表面電荷，使用原子力顯微鏡（AFM）確定了納米粒形態，使用x射線光電子能譜（XPS）分析了粒子表面化學成分，使用高效液相色譜測定了的處方載藥量和包封率。使用MDCK和Caco-2細胞株評估了優化後納米處方的細胞通透性，使用健康小鼠進行了優化后纳米處方的体内腦攝取實驗。 / 結果：IBP和FBP納米粒的粒徑均在30-100 nm的範圍內，粒徑分佈均低於或接近0.2。AFM結果顯示，納米粒具有近球狀形態。由多次線性回歸分析各工藝流程變量對IBP納米粒粒徑的影響所得相對重要性的結果為：PLA對PEG之分子量比 > 過飽和比 > 藥物對聚合物比 > 雷諾數。用相同統計方法分析FBP樣品所得結果顯示，PLA對PEG之分子量比亦為影響粒子粒徑的最重要變量。最穩定的IBP納米處方可以在懸浮液狀態下穩定超過1個月，而FBP納米處方為2天。IBP和FBP納米粒的載藥量和包封率均分別超過25%和70%。XPS，AFM和zeta電位測定結果共同表明納米粒中的PEG均偏重位於粒子表面，而相比之下，IBP納米粒中的PEG較FBP納米粒更加偏向於分佈於粒子表面。優化後的IBP納米粒由聚山梨醇酯80包裹後，與IBP溶液相比，顯著增加了IBP的健康小鼠腦攝取量。 / 結論：應用FNP及MIVM製備的聚合物IBP和FNP納米粒，粒徑小，粒徑分佈窄，重現性高，且有較高的載藥量和包封率。納米粒的粒徑主要取決於所採用的共聚物。IBP 納米粒子明顯優越的物理穩定性可歸功於粒子表面較高的PEG濃度。用聚山梨醇酯80包裹納米粒子對於提高IBP的大腦遞送有決定性作用。 / Objectives: The present thesis work was primarily aimed at assessing a relatively novel nanoparticle (NP) production technology termed flash nanoprecipitation (FNP) using two non-steroidal anti-inflammatory drugs, ibuprofen (IBP) and flurbiprofen (FBP), with different physiochemical properties and lipophilicity typical of most drugs (log P = 2-5). Both model drugs were proven to be of potential benefits to the treatment of Alzheimer’s disease, but exhibited poor brain delivery in vivo which could be ascribed to their extensive binding with plasma proteins in the blood. Therefore another aim of the present thesis was to determine whether FNP-produced NP formulations could enhance the delivery of these drugs into the brain. / Methods: Drugs were loaded into NPs of polyethylene glycol (PEG)-polylactic acid (PLA) copolymers of different molecular weights (MWs) by FNP using a four-stream multi-inlet vortex mixer (MIVM). The influence of several key processing variables on the physical properties and stability of the NPs was investigated. The NP preparations were characterized for particle size and size distribution by dynamic light scattering (DLS) sizing analysis; surface charges by zeta potential measurement; particle morphology by atomic force microscopy (AFM); surface composition by x-ray photoelectron spectroscopy (XPS); and drug loading (DL) and encapsulation efficiency (EE) by high performance liquid chromatography. Optimal IBP NP samples were assessed in vitro for cellular permeability using Caco-2 and MDCK cell lines and in vitro for brain uptake in normal mice. / Results: Both IBP and FBP NPs exhibited mean particle size in the range of 30-100nm and polydispersity below or around 0.2. The particles were nearly spherical in shape, as examined by AFM. Multiple linear regression analysis revealed that the relative impact of the processing variables on the particle size of IBP NPs followed the order: PLA-to-PEG MW ratio > supersaturation ratio > drug-to-copolymer ratio > Reynolds number. Similar statistical analysis for FBP NPs also indicated PLA-to-PEG MW ratio being the most significant determinant of particle size. The most stable IBP and FBP NPs in suspension form could last for over 1 month and 2 days respectively. NPs with DLs > 25% and EEs > 70% could be obtained by FNP. XPS in conjunction with AFM and zeta potential analysis revealed that PEG was located more on the surfaces of both IBP and FBP NPs than in the core, but the surface PEG density was higher for the IBP NPs. Coating of optimal IBP NPs with polysorbate 80 significantly improved the brain uptake of IBP in normal mice, compared to IBP solution. / Conclusion: Polymer-stabilized IBP and FBP NPs with particle size below 100 nm and narrow size distribution can be consistently generated by FNP using the MIVM. The copolymer used is the most important determinant of particle size. The superior physical stability of the IBP NPs can be ascribed to their relatively high surface PEG density. High DLs and EEs are achievable with the FNP process. Nanoparticle coating with polysorbate 80 is critical to enhancing the delivery of IBP to the brain in normal mice. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Zhang, Xinran. / Thesis (Ph.D.)--Chinese University of Hong Kong, 2013. / Includes bibliographical references (leaves 205-245). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Abstracts also in Chinese. / Table of Contents --- p.I / Acknowledgements --- p.VI / Abstract --- p.VIII / 摘要 --- p.X / List of Figures --- p.XII / List of Tables --- p.XVII / List of Abbreviations --- p.XIX / Chapter Chapter One --- Introduction / Chapter 1.1 --- Rationale of the study --- p.1 / Chapter 1.2 --- General review of nanoparticulate drug carrier systems --- p.4 / Chapter 1.2.1 --- Background of nanoscience --- p.4 / Chapter 1.2.2 --- Applications of nanoparticulate drug delivery systems --- p.4 / Chapter 1.2.2.1 --- Improved delivery of poorly water soluble drugs --- p.5 / Chapter 1.2.2.2 --- Targeted drug delivery --- p.6 / Chapter 1.2.2.3 --- Drug delivery across the blood brain barrier --- p.8 / Chapter 1.2.2.4 --- Other drug delivery applications --- p.10 / Chapter 1.2.3 --- Types of nanoparticulate drug delivery systems --- p.10 / Chapter 1.2.3.1 --- Nanocrystals --- p.10 / Chapter 1.2.3.2 --- Solid lipid nanoparticles --- p.11 / Chapter 1.2.3.2.1 --- Preparation methods --- p.12 / Chapter 1.2.3.2.2 --- Drug delivery --- p.12 / Chapter 1.2.3.3 --- Polymeric nanoparticles --- p.14 / Chapter 1.2.3.3.1 --- Preparation methods --- p.15 / Chapter 1.2.3.3.2 --- Drug delivery --- p.17 / Chapter 1.2.4 --- Characterization of nanoparticulate drug delivery systems --- p.20 / Chapter 1.2.4.1 --- Particle size and size distribution --- p.21 / Chapter 1.2.4.2 --- Morphology --- p.21 / Chapter 1.2.4.3 --- Zeta potential --- p.23 / Chapter 1.2.4.4 --- Surface chemical composition --- p.23 / Chapter 1.2.4.5 --- Crystallinity --- p.24 / Chapter 1.3 --- Flash Nanoprecipitation technique --- p.25 / Chapter 1.3.1 --- Mechanism and evolution --- p.25 / Chapter 1.3.2 --- Applications --- p.30 / Chapter 1.4 --- Ibuprofen and flurbiprofen --- p.32 / Chapter 1.4.1 --- General characteristics --- p.32 / Chapter 1.4.2 --- Physicochemical properties --- p.33 / Chapter 1.4.3 --- New therapeutic indications --- p.34 / Chapter 1.5 --- Scope of the thesis --- p.36 / Chapter Chapter Two --- Influence of Processing Variables on the Physical Properties and Stability of Ibuprofen and Flurbiprofen Nanosuspensions / Chapter 2.1 --- Introduction --- p.38 / Chapter 2.2 --- Materials and Methods --- p.39 / Chapter 2.2.1 --- Materials --- p.39 / Chapter 2.2.2 --- Solubility of ibuprofen and flurbiprofen in water and acetone mixtures --- p.39 / Chapter 2.2.3 --- Nanoparticle formulation preparation --- p.40 / Chapter 2.2.3.1 --- Determination of the minimum Reynolds number (Re) for homogenous mixing --- p.40 / Chapter 2.2.3.2 --- Effects of processing parameters on particle size and size distribution of ADCP-protected IBP and FBP nanoparticles. --- p.41 / Chapter 2.2.4 --- Particle size and size distribution measurement --- p.42 / Chapter 2.2.5 --- Statistics --- p.42 / Chapter 2.2.6 --- Assessment of nanosuspension stability --- p.42 / Chapter 2.3 --- Results and discussion --- p.43 / Chapter 2.3.1 --- Solubilities of ibuprofen and flurbiprofen in water and acetone mixtures --- p.43 / Chapter 2.3.2 --- Determination of the minimum Re for homogenous mixing --- p.44 / Chapter 2.3.3 --- Effects of processing parameters on particle size and size distribution of the ADCP-protected IBP and FBP nanoparticles. --- p.47 / Chapter 2.3.3.1 --- Effect of solvent type --- p.47 / Chapter 2.3.3.2 --- Effect of PLA-to-PEG MW ratio --- p.64 / Chapter 2.3.3.3 --- Effect of supersaturation --- p.64 / Chapter 2.3.3.4 --- Effect of Re --- p.70 / Chapter 2.3.3.5 --- Effect of drug-to-ADCP ratio --- p.71 / Chapter 2.3.4 --- Effects of processing parameters on the stability of ADCP-stabilized IBP and FBP nanoparticles --- p.72 / Chapter 2.3.4.1 --- Three-day stability --- p.72 / Chapter 2.3.4.2 --- Long-term stability --- p.83 / Chapter 2.4 --- Summary --- p.85 / Chapter Chapter Three --- Drying of Ibuprofen Nanoparticle Suspensions / Chapter 3.1 --- Introduction --- p.86 / Chapter 3.2 --- Materials and Methods --- p.88 / Chapter 3.2.1 --- Materials --- p.88 / Chapter 3.2.2 --- Preparation of IBP nanoparticle formulations with hydrophilic stabilizers or at refrigerated temperature --- p.89 / Chapter 3.2.3 --- Dialysis of nanoparticle formulations --- p.89 / Chapter 3.2.4 --- Freeze-thawing of selected nanoparticle preparations --- p.89 / Chapter 3.2.5 --- Freeze-drying of nanoparticle formulations --- p.90 / Chapter 3.2.6 --- Reconstitution --- p.90 / Chapter 3.2.7 --- Hydrogen bonding coacervate precipitation --- p.91 / Chapter 3.3 --- Results and discussion --- p.91 / Chapter 3.3.1 --- Preparation and dialysis of IBP nanoparticle formulations with hydrophilic stabilizers --- p.92 / Chapter 3.3.2 --- Freeze-drying using cryoprotectants and lyoprotectants --- p.94 / Chapter 3.3.3 --- Freeze-drying with different concentrations of glucose, sucrose and PVA --- p.101 / Chapter 3.3.4 --- Freeze-drying of nanoparticles prepared under other processing conditions --- p.105 / Chapter 3.3.5 --- Hydrogen bonding coacervate precipitation --- p.108 / Chapter 3.4 --- Summary --- p.110 / Chapter Chapter Four --- Physicochemical Characterization of Ibuprofen and Flurbiprofen Nanoparticles / Chapter 4.1 --- Introduction --- p.111 / Chapter 4.2 --- Materials and Methods --- p.112 / Chapter 4.2.1 --- Materials --- p.112 / Chapter 4.2.2 --- Encapsulation efficiency (EE) and drug loading (DL) of IBP nanoparticles --- p.112 / Chapter 4.2.3 --- HPLC analysis of IBP and FBP --- p.113 / Chapter 4.2.4 --- Nanoparticle morphology --- p.114 / Chapter 4.2.4.1 --- SEM --- p.114 / Chapter 4.2.4.2 --- AFM --- p.114 / Chapter 4.2.5 --- Zeta potential measurement --- p.115 / Chapter 4.2.6 --- Surface composition analysis --- p.115 / Chapter 4.3 --- Results and discussion --- p.116 / Chapter 4.3.1 --- Encapsulation efficiency (EE) and drug loading (DL) of IBP nanoparticles --- p.116 / Chapter 4.3.2 --- Nanoparticle morphology --- p.121 / Chapter 4.3.3 --- Surface charges of the nanoparticles --- p.126 / Chapter 4.3.4 --- Surface composition of nanoparticles --- p.128 / Chapter 4.4 --- Summary --- p.145 / Chapter Chapter Five --- Cellular Permeability and In Vivo Brain Uptake of Ibuprofen Nanoparticles / Chapter 5.1 --- Introduction --- p.146 / Chapter 5.2 --- Materials and methods --- p.148 / Chapter 5.2.1 --- Materials --- p.148 / Chapter 5.2.2 --- Methods --- p.148 / Chapter 5.2.2.1 --- Cellular permeability study --- p.148 / Chapter 5.2.2.1.1 --- Cell culture --- p.148 / Chapter 5.2.2.1.2 --- Cell viability study --- p.149 / Chapter 5.2.2.1.3 --- MDCK and Caco-2 cell monolayer permeability assay --- p.150 / Chapter 5.2.2.2 --- In vivo brain uptake study --- p.151 / Chapter 5.2.2.2.1 --- HPLC-UV analysis --- p.151 / Chapter 5.2.2.2.2 --- Preparation of calibration samples --- p.151 / Chapter 5.2.2.2.3 --- Sample preparation --- p.152 / Chapter 5.2.2.2.4 --- Validation of assay methods --- p.153 / Chapter 5.2.2.2.5 --- Animal experiments --- p.154 / Chapter 5.2.2.2.6 --- Data Analysis --- p.155 / Chapter 5.3 --- Results and discussion --- p.155 / Chapter 5.3.1 --- Cellular permeability study --- p.155 / Chapter 5.3.1.1 --- Cell viability study --- p.155 / Chapter 5.3.1.2 --- MDCK and Caco-2 cell monolayer permeability assay --- p.157 / Chapter 5.3.2 --- In vivo brain uptake study --- p.158 / Chapter 5.3.2.1 --- Method validation --- p.158 / Chapter 5.3.2.2 --- Brain uptake of IBP nanoparticles --- p.159 / Chapter 5.4 --- Summary --- p.166 / Chapter Chapter Six --- Conclusions and Future Studies / Chapter 6.1. --- Conclusions --- p.167 / Chapter 6.2. --- Future studies --- p.172 / Appendices --- p.174 / References --- p.205

Drug delivery systems

Anti-inflammatory agents

Nanoparticles

Nanostructured materials

Drug Delivery Systems

Nanostructures

Inflammation

Anti-Inflammatory Agents

Immunological studies of the anti-inflammatory protein, Sj16, of Schistosoma japonicum. / CUHK electronic theses & dissertations collection

January 2009

Schistosome is the causative agent of schistosomiasis which is one of the world's most prevalent tropical diseases. In the skin of infected host, significant inflammatory response to the parasite is not observed. Previous studies from Schistosoma mansoni showed that this subdued inflammatory response was due to a 16-KDa protein, Sm16, which is present abundantly in the secretions of schistosomulae. Provided that Schistosoma japonicum shares the same infective pathway as S. mansoni by penetrating the skin, it seems logical that S. japonicum has a protein with a similar role to Sm16 to down-regulate host immune responses. According to the cDNA sequence of Sm16, a corresponding gene (designated Sj16) of Sm16 has previously been amplified and cloned from the cercarial cDNA of S. japonicum. Sequence analysis showed that Sj16 shares 99% identity with Sm16 in its nucleotide sequence, and 100% identity in its protein sequence. While previous studiers reported their failure in obtaining the soluble recombinant protein of Sm16, we expressed and purified the recombinant Sj16 (rSj16) from E. coli in the present study. Western blot and ELISA analysis showed that S. japonicum-infected rabbit sera could not recognize rSj16, indicating that native Sj16 might fail to induce circulating antibodies during S. japonicum infection. In the in vivo study, rSj16 dramatically suppressed not only the recruitment of leukocytes to the peritoneal cavity of BALB/c mice injected with thioglycollate, but also the maturation of thioglycollate-induced peritoneal macrophages. The suppression effect was accompanied by a marked up-regulation of IL-10 and IL-1RA transcripts, and down-regulation of IL-12p35, IL-1beta and MIP-2 transcripts in peritoneal cells. Further analysis revealed that rSj16 also inhibited both humoral and cellular immune responses to heterologous antigens. In addition, rSj16 was found to induce macrophage differentiation of the murine myeloid leukemia WEHI-3B (JCS) cells, and regulate the differentiation of mouse hematopoietic cells towards the macrophage lineage. Although previous studies indicated the involvement of endogenous IL-1alpha, IL-1beta and TNF-alpha in the macrophage differentiation of JCS cells, the results from this study suggested that rSj16-induced JCS cell differentiation do not rely on the endogenous production of these three cytokines. This is the first study to successfully express and purify sufficient soluble rSj16, and demonstrate the anti-inflammatory and immunomodulatory effects of the rSj16. / Hu, Shaomin. / Adviser: Ming Chiu Fung. / Source: Dissertation Abstracts International, Volume: 71-01, Section: B, page: 0210. / Thesis (Ph.D.)--Chinese University of Hong Kong, 2009. / Includes bibliographical references (leaves 139-154). / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Electronic reproduction. Ann Arbor, MI : ProQuest Information and Learning Company, [200-] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Abstracts in English and Chinese.

Anti-inflammatory agents

Schistosoma japonicum--Immunology

Schistosomiasis--Immunological aspects

Anti-Inflammatory Agents

Helminth Proteins

Schistosoma japonicum--immunology

Schistosomiasis--immunology

Molecular basis for the anti-inflammatory properties of chlomethiazole /

Simi, Anastasia,

January 2003

Diss. (sammanfattning) Stockholm : Karol. inst., 2003. / Härtill 5 uppsatser.

The effect of prophylactic use of oral ketorolac and ibuprofen in the control of endodontic post treatment pain a thesis submitted in partial fulfillment ... for the degree of Master of Science in Endodontics ... /

Olazabal-Bello, Angelita C.

January 1993

Thesis (M.S.)--University of Michigan, 1993.

The relative effectiveness of non-steroidal anti-inflammatory drugs (Ibuprofen®) and a taping method (Kinesio Taping® Method) in the treatment of episodic tension-type headaches

Henry, Justin Michael

January 2009

Dissertation submitted in partial compliance with the requirements for a Masters Degree in Technology: Chiropractic, Durban University of Technology, 2009. / Headaches are one of the most common clinical conditions in medicine, and 80% of these are tension-type headaches (TTH). TTH has a greater socioeconomic impact than any other type of headache due to its prevalence. Within the TTH category, episodic TTH are more prevalent than chronic TTH. The mainstay in the treatment of TTH are simple analgesics and NSAIDs. Unless contraindicated, NSAIDs are often the most effective treatment for ETTH. However patients suffering with TTH tend to relate their headaches to increased muscle stiffness in the neck and shoulders and thus the non-pharmacological treatment of ETTH could be directed at the associated musculoskeletal components of ETTH. It is therefore proposed that the Kinesio Taping® Method may have an effect in the treatment of the muscular component of ETTH. Method: This study was a prospective randomised clinical trial with two intervention groups (n=16) aimed at determining the relative effectiveness of a NSAID and the Kinesio Taping® Method in the treatment of ETTHs. The patients were treated at 5 consultations over a 3 week period. Feedback was obtained using the: NRS – 101, the CMCC Neck Disability Index and a Headache Diary. Results: The Headache Diary showed a reduction in the presence and number, mean duration and pain intensity of ETTH in both groups. These treatment effects were sustained after the cessation of treatment with the exception of mean pain intensity in the Kinesio Taping® Method group. The mean NRS score decreased in both groups but at a slightly faster rate in the Kinesio Taping® Method group. The CMCC showed an improvement in the functional ability of the patients in both groups. Conclusion: There seems to be no significant difference in the relative effectiveness of the treatment modalities. We can thus state that the overall short-term reduction in symptomatology supports the use of NSAIDs or Kinesio Taping® Method in the treatment of ETTH.

Clinical trial

Tension-type headache

Taping

Anti-inflammatory agents

Non-steroidal

Chiropractic

Tension headache--Chiropractic treatment

Ibuprofen

Bandages and bandaging

Applied kinesiology

Pain--Measurement

Nonsteroidal anti-inflammatory agents