Global ETD Search

111	Value of pharmaceutical innovation the access effects, diffusion process, and health effects of new drugs / Cong, Ze. January 2009 (has links) (PDF) Thesis (Ph.D.)--Pardee Rand Graduate School, 2009. / Title from PDF t.p. Includes bibliographical references.
112	Automated manipulation of zebrafish embryos for high-throughput toxicology screening of nanomaterials / Mandrell, David. January 1900 (has links) Thesis (M.S.)--Oregon State University, 2011. / Printout. Includes bibliographical references (leaves 58-59). Also available on the World Wide Web.
113	Síntese e avaliação farmacológica de novos derivados da pomalidomida para o tratamento da anemia falciforme / Melo, Thaís Regina Ferreira de. January 2018 (has links) Orientador: Jean Leandro dos Santos / Banca: Carolina Lanaro / Banca: Magnun Nueldo Nunes dos Santos / Banca: Rafael Victorio Carvalho Guido / Banca: Jeanine Giarolla Vargas / Resumo: A Anemia Falciforme (AF) é uma anemia hemolítica genética caracterizada por uma mutação no gene da globina beta. Além do quadro vaso-oclusivo, os pacientes com AF apresentam processo inflamatório crônico caracterizado pelo aumento de diversas citocinas pró-inflamatórias, a exemplo do Fator de Necrose Tumoral alfa (TNF-α). Atualmente, a hidroxiureia (HU) é o único fármaco disponível para o tratamento e seus efeitos benéficos estão associados ao óxido nítrico (NO), gerado após biotransformação. O NO desempenha efeitos benéficos na doença tais como: vasodilatação, inibição da agregação plaquetária e aumento na produção de hemoglobina fetal (HbF). Nesse contexto, foram sintetizados os compostos 3(a-b); 4(a-b) e 5(a-b) obtidos através da estratégia de hibridação molecular da subunidade inibidora de TNF-α presente na pomalidomida com o núcleo furoxânico (1,2,5-oxadiazol-2-N-óxido) com propriedades doadores de NO. Os compostos sintetizados foram obtidos em rendimentos que variaram entre 13 e 30%. As moléculas do estudo demonstraram capacidade de liberar NO em níveis que variaram entre 1 e 30%. Em cultura de células CD34+, o composto 4b (2,5 μM) foi capaz de induzir gobina γ, enquanto HU foi ativa apenas em concentrações 4 vezes superiores (10 μM). Estudos preliminares do possível mecanismo de ação mostraram que o composto 4b não interefe na expressão de fatores de transcrição a exemplo do BCL11A, IKAROS, LRF e nos níveis de acetilação de histona H3. O composto 4b foi capaz de induzi... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Sickle Cell Anemia is a genetic blood disease in which there is a mutation in the β-hemoglobin gene. This mutation promotes polymerization of hemoglobin molecules that change the structure of the erythrocyte cytoskeleton promoting sickling of the cell. Moreover, there is increased adhesion of blood cells in the vessel contributing to the increasement of the vaso-occlusive process, the main characteristic of the disease. It is further known that the chronic inflammation associated with the disease contributes to a number of complications and among the process responsible for this proinflammatory cytokine is TNF-α, which is an important target for therapeutic intervention. Hydroxyurea (HU) is the only available drug for treatment and its beneficial effects are associated with the same capacity biotransformation of nitric oxide. The NO plays beneficial effects such as vasodilation, inhibition of platelet aggregation and production of fetal hemoglobin (Hb F), latter has the function of decreasing polymerization of hemoglobin. In this context, continuing the research line that aims at planning, synthesis and pharmacological evaluation of new prototypes drug candidates for the treatment of sickle cell anemia complications, in this work have synthesized a series of four new hybrid compounds ( I- IV) containing the phtalimide (TNF-alfa inhibitory subunit) and furoxan subunits ( nitric oxide donors) according to structural design. The compounds were presented as NO donors. Compounds I-IV were shown to be inhibitors of TNF-α in the immunoassay of this cytokine assay and the compound IV is the most promising inhibiting between 65% in smaller concentrations than the other. In the assay of ADP-induced platelet aggregation, compounds III and IV were able to inhibit platelet aggregation sigficantily. In addition, the compound I after 72 hours was... (Complete abstract click electronic access below) / Doutor Hemoglobinopatia. Hemoglobina. Doadores de óxido nítrico. Sangue - Doenças. Medicamentos - Desenvolvimento. Drug development
114	Falcipains as malarial drug targets Kanzi, Aquillah Mumo January 2013 (has links) Malaria is an infectious disease caused by parasites of the Plasmodium genus with mortality rates of more than a million annually, hence a major global public health concern. Plasmodium falciparum (P. falciparum) accounts for over 90% of malaria incidence. Increased resistance to antimalarial drugs by the Plasmodium parasite, coupled with the lack of an effective malaria vaccine necessitates the urgent need for new research avenues to develop novel and more potent antimalarial drugs. This study focused on falcipains, a group of P. falciparum cysteine proteases that belong to the clan CA and papain family C1, that have emerged as potential drug targets due to their involvement in a range of crucial functions in the P. falciparum life cycle. Recently, falcipain-2 has been validated as a drug target but little is known of its Plasmodium orthologs. Currently, there are several falcipain inhibitors that have been identified, most of which are peptide based but none has proceeded to drug development due to associated poor pharmacological profiles and susceptibility to degradation by host cysteine proteases. Non-peptides inhibitors have been shown to be more stable in vivo but limited information exists. In vivo studies on falcipain-2 and falcipain-3 inhibitors have also been complicated by varying outcomes, thus a good understanding of the structural variations of falcipain Plasmodium orthologs at the active site could go a long way to ease in vivo results interpretation and effective inhibitor design. In this study, we use bioinformatics approaches to perform comparative sequence and structural analysis and molecular docking to characterize protein-inhibitor interactions of falcipain homologs at the active site. Known FP-2 and FP-3 small molecule nonpeptide inhibitors were used to identify residue variations and their effect on inhibitor binding. This was done with the aim of screening a collection of selected non-peptide compounds of South African natural origin to identify possible new inhibitor leads. Natural compounds with high binding affinities across all Plasmodium orthologs were identified. These compounds were then used to search the ZINC database for similar compounds which could have better binding affinities across all selected falcipain homologs. Compounds with high binding affinities across all Plasmodium orthologs were found. Malaria Malaria -- Chemotherapy Plasmodium falciparum Antimalarials -- Development Cysteine proteinases Cysteine proteinases -- Inhibitors Papain Drug development Bioinformatics
115	Discovery and investigation of novel radiosensitising genes Tiwana, Gaganpreet Singh January 2015 (has links) Radiotherapy is second only to surgery in the curative management of patients with cancer, and yet the molecular mechanisms that determine the sensitivity of tumours to radiation remain largely unclear. A high-throughput radiosensitivity screening method based on clonogenicity was developed and a siRNA library against kinase targets was screened. The gold standard colony formation endpoint was chosen for determining reproductive cell death after radiation treatment, since effects on proliferation often do not reflect survival. Thiamine pyrophosphokinase-1 (TPK1), a key component of Vitamin B1/thiamine metabolism, was identified as a target for radiosensitisation. TPK1 knockdown caused significant radiosensitisation in cancer but not normal tissue cell lines. Other means of blocking this pathway such as knockdown of thiamine transporter-1 (THTR1) or treatment with the thiamine analogue pyrithiamine hydrobromide (PyrH) caused significant tumour specific radiosensitisation. There was persistent DNA damage in cells irradiated after TPK1 and THTR1 knockdown or PyrH treatment. Thus this screen allowed the identification of thiamine metabolism as a novel radiosensitisation target that affects DNA repair. Short-term modulation of thiamine metabolism could be a clinically exploitable strategy to achieve tumour specific radiosensitisation. Three additional genes, signal recognition particle-72 kDa (SRP72), glycogen synthase 3-beta (GSK3β) and MAP/Microtubule Affinity-Regulating Kinase 2 (MARK2) were also investigated. Knockdown of these genes radiosensitised both tumour and normal tissue cell lines and expression of two of them, GSK3β and SRP72 were found to be associated with poor recurrence-free survival in early breast cancer patients. 616.99
116	Estabilidade, polimorfismo, dissolução e correlação in vivo-in vitro de Darunavir comprimidos Corrêa, Josilene Chaves Ruela [UNESP] 23 April 2014 (has links) (PDF) Made available in DSpace on 2014-08-13T14:50:59Z (GMT). No. of bitstreams: 0 Previous issue date: 2014-04-23Bitstream added on 2014-08-13T17:59:47Z : No. of bitstreams: 1 000773667_20170423.pdf: 241128 bytes, checksum: 2eb6497bc7ab87727dcefc224bee3822 (MD5) Bitstreams deleted on 2017-04-24T11:16:39Z: 000773667_20170423.pdf,. Added 1 bitstream(s) on 2017-04-24T11:17:26Z : No. of bitstreams: 1 000773667.pdf: 2224116 bytes, checksum: e342a365c65436e77801c3e655df11ec (MD5) / Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP) / Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq) / O darunavir, antirretroviral inibidor de protease, compõe a terapia considerada altamente eficaz no tratamento da síndrome da imunodeficiência humana adquirida, e é um dos fármacos disponibilizados gratuitamente pelo Sistema Único de Saúde (SUS). Os produtos genéricos têm contribuído para a manutenção e abrangência desta política de distribuição gratuita de medicamentos, ao reduzir os custos desses produtos. Neste propósito, este estudo busca fornecer informações sobre o comportamento físicoquímico e estabilidade do fármaco e da formulação, diante de diferentes condições climáticas, bem como, sobre sua solubilidade e liberação a partir da formulação. Além disso, pretende apresentar ferramentas in vitro e in silico que contribuam, no futuro próximo, para a produção de novos produtos contendo darunavir que apresentem alta qualidade, especialmente, genéricos do medicamento referência. Para tanto, a solubilidade do fármaco foi investigada em diferentes meios. A baixa solubilidade aquosa do fármaco foi verificada, e os meios adequados aos testes de dissolução foram escolhidos. O perfil de dissolução in vitro do darunavir e de absorção in vivo a partir papel dos comprimidos de Prezista® contendo 300 mg de fármaco foram investigados. Obtevese um perfil de dissolução discriminativo para o produto e um método de quantificação por espectrofotometria derivada foi desenvolvido e validade. Uma correlação entre os dados de fração dissolvida in vitro e fração absorvida in vivo do darunavir foi alcançada (r2= 0,95). Este é um método preditivo para avaliar o desempenho in vivo do darunavir a partir de comprimidos de liberação imediata, com base em dados in vitro, e é importante para minimizar o uso de animais e seres humanos em experimentos durante o desenvolvimento novos produtos farmacêuticos contendo darunavir. Além disso, uma ferramenta in silico foi desenvolvida e validada para a previsão da ... / Darunavir, a protease inhibitor, constitute the highly active antiretroviral therapy against the acquired immunodeficiency syndrome. It is one of agents given free by the Brazilian Health System (SUS). Generic products have contributed to the maintenance and the policy of free distribution of medicines by the decreasing of costs of these products. In this way, this study seeks to provide information on the physical and chemical behavior and stability of the drug and formulation, facing different weather conditions, as well as provide information on their solubility and release from the formulation. It also aims to provide in vitro and in silico tools to contribute in the near future, for the production of new products containing darunavir, especially generic medicines. Therefore, the solubility of the drug was investigated in different media. The low aqueous solubility of the drug was observed, and suitable media for dissolution testing were chosen. The in vitro dissolution profile of darunavir and the in vivo absorption from Prezista® (tablets containing 300 mg of drug) were investigated. It was obtained a discriminating dissolution profile of the product and a method of quantification by spectrophotometry derivative was developed and validated. A correlation between the data of in vitro dissolved fraction and in vivo absorbed fraction of darunavir was achieved (r2 = 0.95). This is a predictive method to evaluate the in vivo performance of darunavir from immediate-release tablets, based on in vitro data, and it is important to minimize the use of animals and humans in experiments during the development of new medicines containing darunavir. In addition, an in silico tool was developed and validated for predicting the oral bioavailability of darunavir formulations, from their dissolution profile. For this, physiologically based pharmacokinetic modeling was applied through Simcyp® software. These, in vitro and in silico tools, assist in ... / FAPESP: 11/05836-4 Polimorfismo (Cristalografia) Soropositividade para HIV AIDS (Doença) Fármacos Medicamentos - Desenvolvimento Drug development
117	Sistemas precursores de cristais líquidos mucoadesivos para administração bucal de peptídeo antigelatinolítico associados à terapia fotodinâmica no tratamento do câncer bucal / Calixto, Giovana Maria Fioramonti. January 2017 (has links) Orientador: Marlus Chorilli / Banca: Maria Vitória Lopes Badra Bentley / Banca: Renata Fonseca Vianna Lopez / Banca: Carlota de Oliveira Rangel Yagui / Banca: Raquel Mantuanelli Scarel Caminaga / Resumo: O câncer bucal é uma doença altamente incidente na população mundial, podendo provocar invalidez, deformidades faciais e morte. O tratamento de escolha é a quimioterapia e radioterapia, que causam vários efeitos adversos como xerostomia, mucosite, perda de cabelo, náusea, dores e vômitos. A administração de moléculas bioativas, como o peptídeo antitumoral CTT1, demonstrou ser um tratamento inovador e eficaz para o câncer bucal. No entanto, peptídeos apresentam baixa biodisponibilidade oral, o que diminui o desempenho clínico do tratamento. Portanto, a sua administração pela via bucal incorporado em sistemas nanoestruturados mucoadesivos precursores de cristais líquidos (SPCL) constituídos por álcool cetílico etoxilado 20 e propoxilado 5, ácido oleico e fase aquosa contendo água (FA), dispersão polimérica de quitosana (FQ), dispersão polimérica de polietilenoimina (FP) ou dispersão de quitosana associada a polietilenoimina (FPQ) surge como uma valiosa estratégia, visto que a mucosa bucal apresenta alta permeabilidade e alta irrigação sanguínea, o que pode aumentar a absorção do CTT1. Ademais, o SPCL possibilita a incorporação concomitante do CTT1 com o fotossensibilizante azul de metileno (AM), permitindo a associação da terapia fotodinâmica (TFD) à terapia peptídica antitumoral, o que pode potencializar o tratamento do câncer bucal. O objetivo do trabalho foi avaliar o potencial de SPCL mucoadesivos para administração bucal do peptídeo CTT1 associados à TFD no tratamento do c... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: Oral cancer is a highly incident disease in the world population, and can cause disability, facial deformities and death. The treatment of choice is chemotherapy and radiotherapy, which cause various adverse effects like xerostomia, mucositis, hair loss, nausea, aches and vomiting. The administration of bioactive molecules, such as the antitumor peptide CTT1, has proven to be an innovative and effective treatment for oral cancer. However, peptides have low oral bioavailability, which decreases the clinical performance of the treatment. Therefore, its administration by the oral route incorporated in liquid crystal precursor (SPCL) mucoadhesive nanostructured systems consisting of ethoxylated ethoxylated 20 and propoxylated cetyl alcohol 5, oleic acid and aqueous phase containing water (FA), polymer dispersion of chitosan (CF), dispersion (FP) or polyethyleneimine-associated chitosan dispersion (FPQ) arises as a valuable strategy, since the buccal mucosa has high permeability and high blood supply, which may increase the uptake of CTT1. In addition, SPCL allows the simultaneous incorporation of CTT1 with the methylene blue photosensitizer (MA), allowing the association of photodynamic therapy (PDT) with antitumor peptide therapy, which may potentiate oral cancer treatment. The objective of this study was to evaluate the potential of mucoadhesive SPCL for buccal administration of the CTT1 peptide, as well as to evaluate the use of PDT using AM as a photosensitizer in oral cancer therapy. SPCL were characterized by polarized light microscopy (MLP), low-angle X-ray scattering (SAXS), in vitro mucoadhesion rheology and texture profile tests, which showed that all formulations acted as SPCL because (FPQ-P) and AM (FPQ-AM) were added to the liquid crystals after the addition of artificial saliva, and FPQ formed a more mucoadhesive and structured liquid crystal... (Complete abstract click electronic access below) / Doutor Medicamentos - Desenvolvimento. Nanotecnologia. Cristais líquidos. Microscopia de polarização. Peptídeos. Neoplasias bucais. Fotoquimioterapia. Drug development.
118	Catequina e epicatequina minimizam a toxicidade induzida pela amiodarona em fibroblasto de pulmão humano (MRC-5) Santos, Luciana Fernandes Silva 20 November 2015 (has links) A amiodarona é um dos fármacos mais usados para o tratamento de arritmias cardíacas, tanto ventriculares como supraventriculares. Apesar de sua eficácia, o uso da amiodarona está associado a vários efeitos adversos, incluindo a toxicidade pulmonar. O mecanismo pelo qual a amiodarona causa lesão nas células pulmonares humanas não é inteiramente conhecido, mas estudos em cultura de células hepáticas humanas e pulmonares de ratos têm sugerido que a disfunção mitocondrial e o estresse oxidativo têm um papel importante na citotoxicidade da amiodarona. Os compostos fenólicos, incluindo catequina e epicatequina são amplamente distribuídos na natureza e conhecidos por sua capacidade de reduzir o estresse oxidativo. Além disso, alguns compostos fenólicos são capazes de modular a atividade mitocondrial. Em vista disso, o objetivo deste trabalho foi avaliar a capacidade dos compostos fenólicos catequina e epicatequina em a disfunção mitocondrial e os danos oxidativos causados pela amiodarona em células de fibroblasto de pulmão humano (MRC-5). Para atingir os objetivos as células MRC-5 foram tratadas com diferentes concentrações de catequina e epicatequina e após foram expostas a amiodarona 100 μM. A disfunção mitocondrial foi determinada através da atividade do complexo I da cadeia de transporte de elétrons e a biossíntese de ATP usando kits específicos. A viabilidade celular foi avaliada através do ensaio de 3-[4,5- dimetiltiazol 2-il]-2,5 difenil brometo de tetrazolina. A atividade das enzimas superóxido dismutase e catalase foram determinadas espectrofotometricamente. Os danos oxidativos a lipídeos e proteínas foram verificados através dos ensaios de substâncias reativas ao acido tiobarbitúrico e a proteínas carboniladas, respectivamente, e os níveis de óxido nítrico foram avaliados usando o método de Griess. Os resultados mostraram que a amiodarona inibiu a atividade do complexo I da cadeia de transporte de elétrons em 53% e a biossíntese de ATP em 9,5% e tanto a catequina como a epicatequina foram capazes de evitar estes efeitos em todas as concentrações (5, 10, 20 μM) testadas. Verificou-se que a amiodarona reduziu a atividade das enzimas superóxido dismutase e catalase (indicando produção de superóxido e peróxido de hidrogênio) e aumentou os danos oxidativos a lipídeos e proteínas. Os compostos fenólicos catequina e epicatequina foram capazes de minimizar as alterações no metabolismo redox induzidos pela amiodarona e aumentar a viabilidade nas células MRC-5. Catequina e epicatequina reduziram a depleção de óxido nítrico causada pela amiodarona. Este trabalho mostrou, pela primeira vez, que o mecanismo de toxicidade da amiodarona em células MRC-5 está associado à disfunção mitocondrial, principal causa de geração de dano oxidativo celular e que estes efeitos tóxicos são em parte reduzidos pela catequina e epicatequina. Embora outros estudos sejam necessários, estes dados abrem novas perspectivas para estudos visando o desenvolvimento de medicamentos que minimizem os efeitos tóxicos da amiodarona. / Submitted by Ana Guimarães Pereira (agpereir@ucs.br) on 2015-12-09T15:32:21Z No. of bitstreams: 1 Dissertacao Luciana Fernandes Silva Santos.pdf: 1790981 bytes, checksum: 4f3e8dbb7bc255b525503174b7e1a3d2 (MD5) / Made available in DSpace on 2015-12-09T15:32:21Z (GMT). No. of bitstreams: 1 Dissertacao Luciana Fernandes Silva Santos.pdf: 1790981 bytes, checksum: 4f3e8dbb7bc255b525503174b7e1a3d2 (MD5) / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior, CAPES. / Amiodarone is among the most widely used drugs for the treatment of ventricular and supraventricular cardiac arrhythmias. However, the use of amiodarone is associated with several side effects including pulmonary toxicity. The mechanism of amiodarone toxicity is not well known, but studies in human liver cells and rats lung cells have been suggested that mitochondrial dysfunction and oxidative stress play important role in the amiodarone cytotoxicity. Phenolic compounds, including catechin and epicatechin are widespread in nature and known for their ability to reduce oxidative stress. In addition, some phenolic compounds are able to modulate mitochondrial activity. Therefore, the objective of this study was to evaluate the ability of phenolic compounds catechin and epicatechin to minimize the mitochondrial dysfunction and oxidative damage induced by amiodarone in human lung fibroblast cells (MRC-5). To achieve the objectives, MRC-5 cells were treated with different concentrations of catechin and epicatechin and then amiodarone 100 μM. Mitochondrial dysfunction was determined by the activity of complex I of the electron transport chain and ATP biosynthesis using specific kits. Cell viability was assessed by 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay. The activity of the enzymes superoxide dismutase and catalase were determined spectrophotometrically. The oxidative damage to lipids and proteins have been verified through the test substances reactive to the thiobarbituric acid and carbonyl protein, respectively, and nitric oxide levels were evaluated using the Griess method. The results showed that amiodarone inhibit 53% of the activity of complex I of the electron transport chain and 9.5% of ATP biosynthesis and both catechin and epicatechin were able to avoid these effects in all concentrations (5 10, 20 mM) tested. It was found that amiodarone reduced the superoxide dismutase and catalase activities (indicating the production of radicals superoxide and hydrogen peroxide) and increased oxidative damage to lipids and proteins. Phenolic compounds catechin and epicatechin were able to minimize alterations in the redox metabolism and increase in viability of MRC-5 cells. Furthermore, catechin and epicatechin reduced nitric oxide depletion caused by amiodarone. This study showed, for the first time, that toxicity of amiodarone in human lung cultured cells is associated, at least, in part, with mitochondrial dysfunction which was avoided by catechin and epicatechin. Although further studies are needed, these data open new perspectives for studies aiming the development of drugs that minimize the toxic effects of amiodarone. Biotecnologia farmacêutica Medicamentos - Desenvolvimento Arritmia - Tratamento Fenóis Pharmaceutical biotechnology Drug development Arrhythmia - Treatment Phenols
119	Pesquisa e desenvolvimento de fármacos no Brasil: estratégias de fomento / Drug research and development in Brazil: fomentation strategies Silvio Barberato Filho 10 July 2006 (has links) Pode-se afirmar que no século XX originou-se uma indústria farmacêutica multinacional com extraordinária capacidade de pesquisa e desenvolvimento para produzir novos fármacos. Porém, contradizendo este potencial inovador, o número de fármacos introduzidos no mercado vem declinando desde 1960 e as oportunidades abertas com os avanços da biologia molecular, da genômica, da bioinformática e da química ainda não trouxeram os resultados esperados. No Brasil, a pesquisa científica tem obtido resultados de grande relevância, mas encontra muitas dificuldades para levar novos produtos ao mercado. O objetivo principal deste trabalho é discutir estratégias de fomento para a pesquisa e desenvolvimento de fármacos no país, procurando conciliar os requisitos técnicos e econômicos deste processo com as competências preexistentes. O referencial metodológico adotado enfatiza o papel determinante das relações econômicas na pesquisa e desenvolvimento de fármacos e procura encontrar caminhos compatíveis com a realidade nacional. Para tanto, discute as características técnicas e econômicas desta atividade, bem como a estratégia das empresas inovadoras e algumas experiências brasileiras nesta área do conhecimento. Fundamentado na análise de 766 novos fármacos introduzidos no mercado mundial entre 1984-2003, nos pilares econômicos do processo de inovação e no contexto político-institucional da pesquisa e desenvolvimento de fármacos, propõe alternativas para aprimorar o desenvolvimento científico e tecnológico do setor farmacêutico brasileiro. Muitas atividades relacionadas com a pesquisa e desenvolvimento de fármacos são realizadas no país, mas encontram-se dispersas nas principais universidades, centros e institutos de pesquisa. O mapeamento destas competências representa o ponto de partida para a criação de uma rede de inovação no setor farmacêutico. Um dos gargalos identificados neste trabalho é a fragilidade do suporte institucional para negociações de alta tecnologia, do qual fazem parte as patentes, os acordos de cooperação e a transferência de tecnologia. Para viabilizar, no Brasil, a incorporação de ferramentas de alta tecnologia empregadas no desenvolvimento de fármacos foi proposta a criação do Laboratório Nacional de Pesquisa e Desenvolvimento de Fármacos. Além de garantir sofisticação técnica, este Laboratório Nacional atuaria como instituição aberta, multidisciplinar, assumindo o papel de um centro de articulação das iniciativas voltadas para o desenvolvimento de fármacos, podendo gerar recursos para financiar a pesquisa e contribuir para o desenvolvimento científico e tecnológico. Acordos de cooperação com empresas inovadoras e organismos internacionais fazem parte das estratégias para captação de recursos. Linhas de pesquisa alinhadas com as necessidades do Sistema Único de Saúde e com outras políticas do setor público também devem nortear a pesquisa e desenvolvimento de fármacos no país. A exploração de novos alvos moleculares, articulada com projetos genômicos, inovações incrementais, doenças negligenciadas e produtos naturais são apontados como áreas estratégicas. A afirmação de que o Brasil reúne as condições necessárias para participar do processo de desenvolvimento de fármacos - hipótese primária deste trabalho - encontra sustentação nos argumentos apresentados e revela que as condições para a inovação tecnológica nunca foram tão favoráveis quanto agora. Estimular o debate acerca de estratégias que possam fomentar o desenvolvimento científico e tecnológico da pesquisa e desenvolvimento de fármacos no país representa a contribuição almejada por este trabalho. / It can be asserted that in the twentieth century a multinational pharmaceutical industry with extraordinary research and development capacity to produce new drugs arose. However, contradicting this innovative potential, the number of new chemical entities introduced in the market is declining since 1960 and the opportunities open with the progresses of molecular biology, genomics, bioinformatics and chemistry haven\'t brought the expected results yet. In Brazil, the scientific research has been obtaining results of great relevance, but a lot of difficulty is found to introduce new products into the market. The main purpose of this work is to discuss fomentation strategies for the drug research and development in the country, trying to reconcile technical and economic requirements of this process with the pre-existent competences. The adopted methodological referential emphasizes the decisive role of economic relationships in drug research and development and tries to find out compatible ways with the national reality. For that, it discusses the technical and economic characteristics of this activity, as well as the strategy of innovative companies and some Brazilian experiences in this knowledge area. Based on the analysis of 766 new chemical entities introduced in world market among 1984 to 2003, in economic pillars of the innovation process and in political-institutional context of drug research and development, alternatives are proposed to straighten out the scientific and technological development of Brazilian pharmaceutical sector. Many activities related to the drug research and development are accomplished in the country, but they are scattered in the main universities, research centers and institutes. The charting of these competences represents the start up to create an innovation net in the pharmaceutical section. One of the bottlenecks identified in this work is the fragility of institutional support for high technology negotiations, of which patents, cooperation agreements and technology transference make part. To make it possible, in Brazil, incorporation of high technology tools used in drug development, creation of National Laboratory of Drug Research and Development was proposed. Besides guaranteeing technical sophistication, this National Laboratory would act as an open institution, multidisciplinary, shouldering the role of an articulation center of initiatives aiming drug development, being able to generate resources to finance research and to contribute to scientific and technological development. Cooperation agreements with innovative companies and international organisms are part of strategies to raise funds research fields aligned with the needs of the Brazilian Unique Health System (SUS) and with other policies of Public Sector also must direct the drug research and development in the country. New molecular targets evaluation articulated in genomic process, incremental innovations, neglected diseases and natural products are pointed out as strategic areas. The statement that Brazil has conditions of participating in the process of drug development - primary hypothesis of this work - finds back-up in reported arguments and reveals that conditions for technological innovation have never been as favorable as now. To stimulate the debate concerning strategies that can foment scientific and technological development of drug research and development in the country represents the contribution aimed for this work. Desenvolvimento de fármacos Gestão tecnológica Indústria farmacêutica Pesquisa de fármacos Drug development Drug research Pharmaceutical industry Technology management
120	The Emergence of Crowdsourcing and Open-Source Models in Drug Development / The Emergence of Crowdsourcing and Open-Source Models in Drug Development Evaldsson, Johan, Ljungdahl, Thomas, Suter, Fredrik January 2012 (has links) Contemporary cases of crowdsourcing (CS) and open source development (OS) related to drug development have been selected and studied. Contemporary examples of CS/OS from within and outside of the pharmaceutical industries have been presented to give a background and suggest possible benefits and problems. The main criteria for selection have been that the case must seek to advance drug development and must use crowdsourcing or open source as a mechanism. The cases found in our search show a large diversity in terms of application, usage, and possible implications for the pharmaceutical industry. We found that crowdsourcing within a scientific problem context produced good results, but that open source initiatives were either poorly financed and not successful or focused on neglected diseases made possible through strong backing by non-profit organizations. An analysis of which the pharmaceutical companies where that showed activity on the platforms identified R&D-intensive and biotech companies as the most active. Contract research organizations (CROs) and generics manufacturers (GMs) showed almost complete absence. We argue that GMs are not likely to be interested in this kind of R&D, but CROs are an untapped resource. Finally we propose a hypothetical model that takes into account all the findings from our study and the literature. This model is based on a limited type of open source with a limited number of partners making use of the untapped CRO resource through crowdsourcing. / Ett antal pågående fall av samverkans-modellen crowdsourcing (CS) samt fenomenet av ”öppen-innovation”, open-innovation (OI) har studerats i kontexten läkemedelsutveckling. I denna fall-studien presenteras ett antal fall där CS och OI används både inom och utom läkemedelsindustrin. Detta har gjorts för att skapa en bättre förståelse för fenomenen samt att tydliggöra problem och att belysa fördela med öppen-innovation och olika typer av samverkans-modeller. Huvudkriteriet för utvalen av fall har varit ett avancerat stadium i läkemedelsutvecklingen samt att något av de två verktygen OI eller CS används aktivt i utvecklingsarbetet. Fall-studien klargör en tydlig differens mellan olika applikations-typer och hur man i verkligheten implementerar dessa verktyg i forskningsarbete. Vår fall-studie indikerar goda resultat då man använder samverkans-modellen CS inom forskningsarbete, men att ”öppen-innovation” OI inte gav samma goda resultat då immateriella mekanismer bromsar öppenheten i läkemedelsindustrin. Inom läkemedels-utvecklingen för Negleted Diseases fann vi däremot en större aktivitet vilken grundar sig på icke-vinst-drivande aktörers intressen. Genom en analys av aktörer inom läkemedelsindustrin har vi kunna framtyda att forsknings-och utveckligns-företag samt Biotech som de som mest ser och utnyttjar potentiallen i CS och OI. Contract research organizations (CROs) och Generics Manufacturers (GMs) är nästan uteslutande frånvarande i resultaten från vår analys. Våra resultat visar att GM-företagen inte har mycket intresse av varken CS eller OI, men att för CRO-företagen finns det vinning i att utnyttja dessa resurser. Slutligen förespråkar vi en fortsatt forskning i ämnet baserat på fall-studien för att kunna ta fram en hypotetisk-CS modell, vilken skulle baseras på ett begränsat antal av samarbetspartners vars potentiella vinning skulle visas genom utnyttjandet av samverkans-modellen CS. / Johan Evaldsson +733-706822 open innovation crowdsourcing open source drug development Nursing Omvårdnad Business Administration Företagsekonomi Computer Sciences Datavetenskap (datalogi)

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