Albert Benjamin Simpson's view of 'the baptism of the Holy Spirit' "a view distinct though not unique" : a study in historical theology /

Gilbertson, Richard Paul,

January 1988

Thesis (Th. M.)--Regent College, 1988. / Abstract. Vita. Catalogue of the published writings of A.B. Simpson: leaves [246]-258. Includes bibliographical references (leaves 268-282).

Cross-talk between marginal zone B cells and marginal zone macrophages

You, Yuying.

January 2010

Thesis (Ph.D.)--University of Alabama at Birmingham, 2010. / Title from PDF title page (viewed on July 8, 2010). Includes bibliographical references.

Studie over vertikale transmissie van hepatitis B-virus en de betekenis ervan voor de epidemiologie van hepatitus B-virusinfecties maternal-foetal transmission of hepatitis B-virus and its epidemiological significance /

Ypma, Tjipke Dirk,

January 1943

Thesis (doctoral)--Utrecht, 1979.

Pathology of hepatitis B-associated chronic liver disease and hepatocellular carcinoma in Hong Kong

Wu, Pui-chee.

January 1984

Thesis (M.D.)--University of Hong Kong, 1984. / Also available in print.

Site-directed in vitro immunization a model of sequential antigen-specific activation of human B cells /

Chin, Li-Te.

January 1994

Thesis (doctoral)--Lund University, 1994. / Added t.p. with thesis statement inserted.

IgE production regulation via CD23 stalk engagement and cell cycle stimulation /

Caven, Timothy Hays,

January 2006

Thesis (Ph. D.)--Virginia Commonwealth University, 2006. / Prepared for: Dept. of Microbiology and Immunology. Includes bibliographical references (p. 210-222). Also available online.

Albert Benjamin Simpson's view of 'the baptism of the Holy Spirit' "a view distinct though not unique" : a study in historical theology /

Gilbertson, Richard Paul,

January 1988

Thesis (Th. M.)--Regent College, 1988. / Abstract. Vita. Catalogue of the published writings of A.B. Simpson: leaves [246]-258. Includes bibliographical references (leaves 268-282).

The protein-protein interactions of the molecular chaperone, alphaB crystallin : an in-depth analysis of structure, function, and mechanism /

Ghosh, Joy Gispati.

January 2006

Thesis (Ph. D.)--University of Washington, 2006. / Vita. Includes bibliographical references (leaves 238-308).

Complexos de inclusão de anfotericina B com derivados de ciclodextrinas e sua incorporação em microemulsões lipídicas biocompatíveis /

Franzini, Cristina Maria.

January 2010

Orientador: Anselmo Gomes de Oliveira / Banca: Eryvaldo Sócrates Tabosa do Egito / Banca: Maria Vitória Lopes Badra Bentley / Banca: Marcos Antonio Corrêa / Banca: Marlus Chorilli / Resumo: O tratamento das infecções fúngicas sistêmicas impõe grandes dificuldades devido ao fato da terapia endovenosa requerer administração do fármaco solubilizado ou disperso em partículas de diminutas dimensões, além da necessidade de hospitalização. A anfotericina B (AmB) continua sendo um dos antibióticos mais efetivos para tais tratamentos, apesar de sua baixa solubilidade e graves efeitos colaterais. Considerando que microemulsões permitem contornar esses problemas e proporcionar administração oral do fármaco, essas formulações lipídicas contendo AmB estão sendo cada vez mais estudadas. Adicionalmente, a formação de complexos de inclusão com ciclodextrinas (CDs) também tem sido promissora no desenvolvimento de novas formas farmacêuticas. Neste trabalho os parâmetros de formação de microemulsões (MEs) contendo fosfatidilcolina de soja (FS), Tween-20 (Tw) e oleato de sódio (OS) como tensoativos e colesterol (CHO) como fase oleosa e a formação de complexos de inclusão com diferentes derivados de CD e sua incorporação nas MEs foi estudado. Um diagrama de fases pseudoternário foi elaborado objetivando caracterizar MEs. O comportamento reológico e a estruturação interna foram empregadas para avaliação e ainda caracterização por espalhamento dinâmico de luz. Foi avaliado o efeito da proporção de tensoativo e óleo na determinação do diâmetro da fase interna nos sistemas com ou sem AmB, além da avaliação da contribuição da fase oleosa e do tensoativo na incorporação do fármaco nas MEs. Um diagrama de solubilidade de AmB em CDs foi desenvolvido e suas constantes de estabilidade determinadas. O preparo de ME contendo CDs em sua fase aquosa, parâmetros de incorporação de AmB e estudos de liberação foram realizados seguidos de análise termogravimétrica, difração de raios x (DRX) e ressonância magnética nuclear (RMN)... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: The fungal infections treatment imposes many difficulties mainly because the intravenous therapy requires administration of solubilized or dispersed drug in particles of smaller dimension beyond the need for hospitalization. Despite its low solubility and serious adverse effects the amphotericin B (AmB) remains one of the most effective antibiotics to the treatment. Microemulsions allow circumvent these problems and provide oral administration. Therefore these lipid formulations containing AmB have been increasingly studied. Additionally, the formation of inclusion complexes with cyclodextrins (CDs) has also been promising in developing new dosage forms. In this work the formation parameters of microemulsions (MEs) containing soybean phosphatidylcholine (FS), Tween-20 (Tw) and sodium oleate (SO) as surfactant and cholesterol (CHO) as oil phase and the formation of inclusion complexes with different CDs derivatives and their incorporation into MEs were studied. The pseudo ternary phase diagram was built in order to characterize MEs. The rheological behavior and internal structure were evaluated and characterized by dynamic light scattering. The effect of the proportion of surfactant and oil phase in the diameter of the internal phase in systems with or without AmB was evaluated. Therefore the contribution of the oil phase and surfactant in the drug loading eficience was studied. The Solubility diagram of AmB in CDs was developed and its stability constants determined. The preparation of ME containing CDs in its aqueous phase, the incorporation AmB parameters and the release studies were performed followed by thermal analysis, x-ray (XRD) diffraction and nuclear magnetic resonance (NMR). The results reveal the MEs formation in regions containing up to 30% surfactant and about 11% of the oil phase. Under polarized light, the interest systems showed a dark background and lamellar structure... (Complete abstract click electronic access below) / Doutor

Anfotericina B.

Ciclodextrinas.

Amphotericin B. eng

Cyclodextrins. eng

Interrogating novel functions of the I kappa B kinases via CRISPR-Cas9 gene editing and small molecule inhibition

Prescott, Jack

January 2018

The NF-kB signalling pathway is a critical mediator of the cellular responses to inflammatory cytokines. The IκB kinase (IKK) complex, which is composed of two catalytic subunits (IKKα and IKKβ) and one regulatory subunit (IKKγ/NEMO) acts as the master regulator of NF-κB transcription factor activity. Seminal genetic studies in knockout (KO) mouse embryonic fibroblasts (MEFs) have defined two pathways of NF-κB activation; a canonical pathway, activated in response to cytokines such as TNFα/IL-1β, that requires NEMO and predominantly IKKβ catalytic activity; and a non-canonical pathway, activated in response to a subset of TNF-family cytokines, which requires IKKα and NIK kinase. We have generated and validated CRISPR-Cas9 IKKα, IKKβ and IKKα/β DKO HCT116 colorectal cancer cell lines to interrogate novel functions of the I kappa B kinases in colorectal cancer, including the relative contributions of these kinases to the activation of NF-κB signalling pathways downstream of TNFα induction. Contrary to the seminal studies in KO MEFs, IKKα appeared to make a more significant contribution to canonical NF-κB induction in these cells than IKKβ. Western blot studies demonstrated that both IKKs contributed to the phosphorylation and degradation of IκB and the phosphorylation of the NF-κB subunit, p65 at Serine 536. However, high-content immunofluorescence studies demonstrated that IKKα KO cells were defective in TNFα-induced nuclear translocation of p65 compared to WT and IKKβ KO cells. Additionally, NF-κB-driven luciferase reporter assays showed that IKKα, but not IKKβ, KO cells exhibited significantly reduced NF-κB-dependent gene expression following TNFα stimulation. We also have evidence to suggest that the phosphorylation site at Serine 468 on p65, previously defined as an IKKβ-dependent site, is in-fact an IKKα-dependent site in these cells. Furthermore, IKKα knockout revealed a potentially important role for IKKα activity in preventing the stabilisation of NIK protein following prolonged TNFα stimulation. RNA sequencing analysis of wild-type, IKKα KO, IKKβ KO and IKKα/β DKO cells stimulated with TNFα was performed to identify genes whose expression were differentially deregulated by IKK KO. These analyses confirmed the importance of IKKα for canonical NF-κB gene expression. Furthermore, IKKβ knockout had unexpected effects on the expression of a broad range of genes involved in chromatin organisation, cytoskeletal organisation, mitotic cell cycle control and the DNA damage response. During the characterisation of IKK KO cells it was discovered that the expression of NEMO was downregulated at the protein, but not mRNA level by approximately 50% in IKKα KO cells and 90% in IKKα/β DKO cells. IKKβ KO cells, meanwhile, exhibited wild-type NEMO expression. Emetine-chase and radioactive pulse chase labelling experiments demonstrated that the half-life of NEMO in IKKα and IKKα/β DKO cells was significantly shortened due to enhanced proteasomal turnover. Bioinformatics analyses predicted significant regions of intrinsic structural disorder within NEMO, particularly at the N- and C-termini, the former of which overlapped with the IKK binding domain. On this basis, the susceptibility of NEMO to in vitro degradation by the 20S proteasome was examined, with NEMO proving be a highly effective substrate of the 20S proteasome. Importantly, IKKα and IKKβ were both shown to protect NEMO from proteasomal degradation, leading us to propose a model whereby interaction with IKK kinase subunits sequesters/masks intrinsically disordered regions in NEMO that would otherwise make NEMO a highly effective substrate for ubiquitin-dependent and/or ubiquitin-independent proteasomal degradation. BMS-345541 is a commercially available allosteric inhibitor of IKKβ that has been used extensively in numerous studies, including a report that proposed novel functions for IKKβ in mitotic cell cycle progression (Blazkova et al., 2007). Similar antiproliferative effects to those reported by Blazkova et al., were observed during the characterisation of a novel ATP-competitive inhibitor of IKKβ, AZD2230. In depth characterisation of the selectivity of AZD2230 and BMS-345541, however, revealed that the antiproliferative effects of AZD2230 and BMS-345541 are, in fact, due to off-target inhibition, potentially at the level of RNA Polymerase II C-terminal domain phosphorylation, and hence general transcription. Collectively, these studies reveal novel functions of the IKK kinases in NF-κB signalling and inform therapeutic strategies for targeting chronic canonical NF-κB activation in colorectal cancer.

NF-kappa B ; I kappa B kinase ; NEMO