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Design and synthesis of cationic amphiphilesFindlay, Brandon January 2012 (has links)
Cationic antimicrobial peptides (CAMPs) are produced by plants, animals and bacteria to protect their host against antagonistic microbes. The antitheses of selective antibiotics, these peptides are drawn by electrostatic and hydrophobic interactions to targets as diverse as the bacterial membrane, nucleic acids and serum proteins. This lack of specificity is their greatest strength, as mutations to single genes rarely lead to bacterial resistance. Resistance may be conferred by large scale alterations in cell envelope composition, which generally reduces bacterial fitness in the absence of peptide.
Clinical applications of natural CAMPs are limited, as the peptides are toxic to mammalian cells and rapidly inactivated in vivo by serum albumin and proteases. Faced with these challenges we have prepared a number of CAMP analogues, with the goal of creating lead compounds for further development of antibacterial therapeutics. Much of our work has focused on ultrashort lipopeptides and lipopeptoids, which have properties similar to natural CAMPs and extremely abbreviated sequences. The simple structure of these scaffolds allows rapid creation of CAMP analogues in a brief period of time, allowing us to rapidly explore the structural requirements for CAMP activity. The balance of this work focuses on imparting CAMP-like behaviour to known antibiotics, in order to expand their spectrum of susceptible bacteria and combat the development of drug-resistant bacteria. In particular, the aminoglycosides neomycin and tobramycin have been fused to phenolic disinfectants such as triclosan and biclotymol, in order to improve their diffusion across the bacterial envelope and activity against Gram-negative bacteria.
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Design and synthesis of cationic amphiphilesFindlay, Brandon January 2012 (has links)
Cationic antimicrobial peptides (CAMPs) are produced by plants, animals and bacteria to protect their host against antagonistic microbes. The antitheses of selective antibiotics, these peptides are drawn by electrostatic and hydrophobic interactions to targets as diverse as the bacterial membrane, nucleic acids and serum proteins. This lack of specificity is their greatest strength, as mutations to single genes rarely lead to bacterial resistance. Resistance may be conferred by large scale alterations in cell envelope composition, which generally reduces bacterial fitness in the absence of peptide.
Clinical applications of natural CAMPs are limited, as the peptides are toxic to mammalian cells and rapidly inactivated in vivo by serum albumin and proteases. Faced with these challenges we have prepared a number of CAMP analogues, with the goal of creating lead compounds for further development of antibacterial therapeutics. Much of our work has focused on ultrashort lipopeptides and lipopeptoids, which have properties similar to natural CAMPs and extremely abbreviated sequences. The simple structure of these scaffolds allows rapid creation of CAMP analogues in a brief period of time, allowing us to rapidly explore the structural requirements for CAMP activity. The balance of this work focuses on imparting CAMP-like behaviour to known antibiotics, in order to expand their spectrum of susceptible bacteria and combat the development of drug-resistant bacteria. In particular, the aminoglycosides neomycin and tobramycin have been fused to phenolic disinfectants such as triclosan and biclotymol, in order to improve their diffusion across the bacterial envelope and activity against Gram-negative bacteria.
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Partículas e filmes híbridos de polímeros e compostos de amônio quaternário com atividade antimicrobiana / Particles and films hybrid of polymers and quaternary ammonium compounds with antimicrobial activityMelo, Letícia Dias de 02 February 2011 (has links)
Partículas e filmes híbridos de polímeros e compostos de amônio quaternário (CAQ) foram caracterizados quanto a propriedades físicas e atividade contra cepas de Pseudomonas aeruginosa ATCC 27853 e Staphylococcus aureus ATCC 25923. Partículas híbridas foram obtidas a partir de fragmentos de bicamada (BF) de brometo de dioctadecildimetilamônio (DODAB), adicionados consecutivamente de soluções de carboximetilcelulose (CMC) e cloreto de poli (dialildimetilamônio) (PDDA) e, a seguir, caracterizadas por espalhamento de luz dinâmico para determinação de distribuições de tamanho, diâmetro médio (Dz) e potencial-zeta (ζ). Filmes híbridos foram obtidos por revestimento rotacional de lamínulas de vidro a partir de uma solução clorofórmica de poli (metil metacrilato) (PMMA) e CAQ onde [PMMA] = 10 mg/mL e [CAQs] = 0,03 4 mM de DODAB, brometo de cetiltrimetilamônio (CTAB) ou brometo de tetrapropilamônio (TPAB). Molhabilidade dos filmes e difusibilidade dos CAQs nos filmes imersos em água foram avaliadas por determinação de ângulo de contato e de tensão superficial na interface ar-água, respectivamente. Atividade antimicrobiana foi avaliada por plaqueamento e contagem de viáveis, tanto para os filmes quanto para as partículas. Para os filmes, também foram determinados halos de inibição. Partículas de DODAB BF/ CMC/ PDDA exibiram Dz e ζ dependentes da concentração dos componentes. A 0,1 mM de DODAB, 0,1 mg/mL de CMC e 0,1 mg/mL de PDDA, foram obtidas partículas pequenas (Dz = 100 nm; ζ = 30 mV). Com 0,5 mM de DODAB, 0,5 mg/mL de CMC e 0,5 mg/mL de PDDA foram obtidas partículas grandes (Dz = 470 nm; ζ = 50 mV). Contra 107 UFC/mL, 1 - 2 µg/mL de PDDA, sozinho em solução ou em forma de partículas, matou 99 % das células de P. aeruginosa. O mesmo ocorreu contra S. aureus (107 UFC/mL) em 10 µg/mL de PDDA. A ação antimicrobiana mostrou-se dependente da quantidade de cargas positivas nas partículas e independente do tamanho da partícula. Filmes de PMMA/ CAQ apresentaram maior molhabilidade do que aqueles de PMMA puro. Filmes de PMMA/ DODAB e PMMA/ TPAB submersos em água não causaram alterações de tensão superficial na interface ar-água, indicando baixa difusibilidade destes CAQs a partir dos filmes. Filmes de PMMA/ CTAB submersos em água reduziram a tensão superficial até aproximadamente 60 mN/m, mostrando a difusibilidade do CTAB no filme e sua organização na interface ar-água. O efeito antimicrobiano dos filmes PMMA/ DODAB e PMMA/ CTAB foi dependente da concentração do CAQ utilizada no preparo do filme. Viabilidade celular de 0% contra 107 UFC/mL de ambas as bactérias ocorreu com 4 mM de DODAB ou, com 2 ou 0,2 mM de CTAB contra P. aeruginosa ou S. aureus, respectivamente. Filmes de PMMA/ TPAB não apresentaram atividade antimicrobiana. Com a emergência de micro-organismos resistentes aos antibióticos, os novos nanomateriais antimicrobianos híbridos de polímeros e compostos de amônio quaternário podem representar uma alternativa de fácil obtenção e baixo custo. / Hybrid particles and films from polymers and quaternary ammonium compounds (QAC) were characterized regarding its physical properties and antimicrobial activity against strains of Pseudomonas aeruginosa ATCC 27853 or Staphylococcus aureus ATCC 25923. Hybrid particles were obtained from dioctadecyldimethylammonium bromide (DODAB) bilayer fragments (BF), consecutively added of carboximethylcellulose (CMC) and poly (diallyldimethylammonium) chloride (PDDA) solutions, and then, characterized by dynamic light-scattering for determination of size distributions, z-average diameter (Dz) and zeta-potential (ζ). Hybrid films were obtained by spin-coating of a chloroformic solution of poly (methylmethacrylate) (PMMA) and QAC on glass coverslips at [PMMA] = 10 mg/mL and [QACs] = 0.03 -4 mM where QACs were DODAB, cetyltrimethylammonium bromide (CTAB) or tetrapropylammonium bromide (TPAB). Films wettability and QACs diffusibility in the films immersed in water were evaluated by determinations of contact angle and surface tension at air-water interface, respectively. Antimicrobial activity was evaluated by plating and CFU counting both for particles and films. For the hybrid films, width of inhibition zone was also determined. DODAB BF/ CMC/ PDDA particles exhibited Dz and ζ dependent on the concentrations of the components. At 0.1 mM DODAB, 0.1 mg/mL CMC, and 0.1 mg/mL PDDA, small cationic particles were obtained (Dz = 100 nm; ζ = 30 mV). At 0.5 mM DODAB, 0.5 mg/mL CMC and 0.5 mg/mL PDDA, large cationic particles were obtained (Dz = 470 nm; ζ = 50 mV). At 107 CFU/mL, cell viability of 1 % for P. aeruginosa was obtained for PDDA in solution or covering particles at 1 or 2 µg/mL PDDA, respectively. Against S. aureus (107 CFU/mL) at 10 µg/mL PDDA, a similar result was obtained. The antimicrobial effect was dependent on the amount of positive charge on particles and independent on particle size. The hybrid films of PMMA/ QAC showed higher wettability than those of pure PMMA. PMMA/ DODAB and PMMA/ TPAB hybrid films, submerged in water, did not cause changes in surface tension at the air-water interface, indicating low diffusibility for both DODAB and TPAB in hybrid films. Films of PMMA/ CTAB, submerged in water, reduced the surface tension to about 60 mN/m, showing that CTAB could diffuse from the film to the air-water interface and change its surface tension. The antimicrobial effect of PMMA/ DODAB and PMMA/ CTAB hybrid films was clearly dependent on the QAC concentration used to prepare the films. Cell viability of 0% for P. aeruginosa and S. aureus (107 CFU/mL) occurred at 4 mM DODAB, or 2 and 0.2 mM CTAB, respectively. Films of PMMA/ TPAB showed no antimicrobial activity. With the emergence of microorganisms resistant to antibiotics, the novel hybrid antimicrobial nanomaterials may become important since they are inexpensive and easy to obtain.
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Partículas e filmes híbridos de polímeros e compostos de amônio quaternário com atividade antimicrobiana / Particles and films hybrid of polymers and quaternary ammonium compounds with antimicrobial activityLetícia Dias de Melo 02 February 2011 (has links)
Partículas e filmes híbridos de polímeros e compostos de amônio quaternário (CAQ) foram caracterizados quanto a propriedades físicas e atividade contra cepas de Pseudomonas aeruginosa ATCC 27853 e Staphylococcus aureus ATCC 25923. Partículas híbridas foram obtidas a partir de fragmentos de bicamada (BF) de brometo de dioctadecildimetilamônio (DODAB), adicionados consecutivamente de soluções de carboximetilcelulose (CMC) e cloreto de poli (dialildimetilamônio) (PDDA) e, a seguir, caracterizadas por espalhamento de luz dinâmico para determinação de distribuições de tamanho, diâmetro médio (Dz) e potencial-zeta (ζ). Filmes híbridos foram obtidos por revestimento rotacional de lamínulas de vidro a partir de uma solução clorofórmica de poli (metil metacrilato) (PMMA) e CAQ onde [PMMA] = 10 mg/mL e [CAQs] = 0,03 4 mM de DODAB, brometo de cetiltrimetilamônio (CTAB) ou brometo de tetrapropilamônio (TPAB). Molhabilidade dos filmes e difusibilidade dos CAQs nos filmes imersos em água foram avaliadas por determinação de ângulo de contato e de tensão superficial na interface ar-água, respectivamente. Atividade antimicrobiana foi avaliada por plaqueamento e contagem de viáveis, tanto para os filmes quanto para as partículas. Para os filmes, também foram determinados halos de inibição. Partículas de DODAB BF/ CMC/ PDDA exibiram Dz e ζ dependentes da concentração dos componentes. A 0,1 mM de DODAB, 0,1 mg/mL de CMC e 0,1 mg/mL de PDDA, foram obtidas partículas pequenas (Dz = 100 nm; ζ = 30 mV). Com 0,5 mM de DODAB, 0,5 mg/mL de CMC e 0,5 mg/mL de PDDA foram obtidas partículas grandes (Dz = 470 nm; ζ = 50 mV). Contra 107 UFC/mL, 1 - 2 µg/mL de PDDA, sozinho em solução ou em forma de partículas, matou 99 % das células de P. aeruginosa. O mesmo ocorreu contra S. aureus (107 UFC/mL) em 10 µg/mL de PDDA. A ação antimicrobiana mostrou-se dependente da quantidade de cargas positivas nas partículas e independente do tamanho da partícula. Filmes de PMMA/ CAQ apresentaram maior molhabilidade do que aqueles de PMMA puro. Filmes de PMMA/ DODAB e PMMA/ TPAB submersos em água não causaram alterações de tensão superficial na interface ar-água, indicando baixa difusibilidade destes CAQs a partir dos filmes. Filmes de PMMA/ CTAB submersos em água reduziram a tensão superficial até aproximadamente 60 mN/m, mostrando a difusibilidade do CTAB no filme e sua organização na interface ar-água. O efeito antimicrobiano dos filmes PMMA/ DODAB e PMMA/ CTAB foi dependente da concentração do CAQ utilizada no preparo do filme. Viabilidade celular de 0% contra 107 UFC/mL de ambas as bactérias ocorreu com 4 mM de DODAB ou, com 2 ou 0,2 mM de CTAB contra P. aeruginosa ou S. aureus, respectivamente. Filmes de PMMA/ TPAB não apresentaram atividade antimicrobiana. Com a emergência de micro-organismos resistentes aos antibióticos, os novos nanomateriais antimicrobianos híbridos de polímeros e compostos de amônio quaternário podem representar uma alternativa de fácil obtenção e baixo custo. / Hybrid particles and films from polymers and quaternary ammonium compounds (QAC) were characterized regarding its physical properties and antimicrobial activity against strains of Pseudomonas aeruginosa ATCC 27853 or Staphylococcus aureus ATCC 25923. Hybrid particles were obtained from dioctadecyldimethylammonium bromide (DODAB) bilayer fragments (BF), consecutively added of carboximethylcellulose (CMC) and poly (diallyldimethylammonium) chloride (PDDA) solutions, and then, characterized by dynamic light-scattering for determination of size distributions, z-average diameter (Dz) and zeta-potential (ζ). Hybrid films were obtained by spin-coating of a chloroformic solution of poly (methylmethacrylate) (PMMA) and QAC on glass coverslips at [PMMA] = 10 mg/mL and [QACs] = 0.03 -4 mM where QACs were DODAB, cetyltrimethylammonium bromide (CTAB) or tetrapropylammonium bromide (TPAB). Films wettability and QACs diffusibility in the films immersed in water were evaluated by determinations of contact angle and surface tension at air-water interface, respectively. Antimicrobial activity was evaluated by plating and CFU counting both for particles and films. For the hybrid films, width of inhibition zone was also determined. DODAB BF/ CMC/ PDDA particles exhibited Dz and ζ dependent on the concentrations of the components. At 0.1 mM DODAB, 0.1 mg/mL CMC, and 0.1 mg/mL PDDA, small cationic particles were obtained (Dz = 100 nm; ζ = 30 mV). At 0.5 mM DODAB, 0.5 mg/mL CMC and 0.5 mg/mL PDDA, large cationic particles were obtained (Dz = 470 nm; ζ = 50 mV). At 107 CFU/mL, cell viability of 1 % for P. aeruginosa was obtained for PDDA in solution or covering particles at 1 or 2 µg/mL PDDA, respectively. Against S. aureus (107 CFU/mL) at 10 µg/mL PDDA, a similar result was obtained. The antimicrobial effect was dependent on the amount of positive charge on particles and independent on particle size. The hybrid films of PMMA/ QAC showed higher wettability than those of pure PMMA. PMMA/ DODAB and PMMA/ TPAB hybrid films, submerged in water, did not cause changes in surface tension at the air-water interface, indicating low diffusibility for both DODAB and TPAB in hybrid films. Films of PMMA/ CTAB, submerged in water, reduced the surface tension to about 60 mN/m, showing that CTAB could diffuse from the film to the air-water interface and change its surface tension. The antimicrobial effect of PMMA/ DODAB and PMMA/ CTAB hybrid films was clearly dependent on the QAC concentration used to prepare the films. Cell viability of 0% for P. aeruginosa and S. aureus (107 CFU/mL) occurred at 4 mM DODAB, or 2 and 0.2 mM CTAB, respectively. Films of PMMA/ TPAB showed no antimicrobial activity. With the emergence of microorganisms resistant to antibiotics, the novel hybrid antimicrobial nanomaterials may become important since they are inexpensive and easy to obtain.
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