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Otimiza??o e valida??o de m?todos anal?ticos para a determina??o simult?nea de tuberculost?ticos (4-FDC) por CLAE/DAD e CLUE/ DADPaiva, Marcelo Vitor de 21 March 2013 (has links)
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Previous issue date: 2013-03-21 / Tuberculosis is a serious disease, but curable in practically 100% of new cases,
since complied the principles of modern chemotherapy. Isoniazid (ISN), Rifampicin
(RIF), Pyrazinamide (PYR) and Chloride Ethambutol (ETA) are considered first line
drugs in the treatment of tuberculosis, by combining the highest level of efficiency
with acceptable degree of toxicity. Concerning USP 33 - NF28 (2010) the
chromatography analysis to 3 of 4 drugs (ISN, PYR and RIF) last in average 15
minutes and 10 minutes more to obtain the 4th drug (ETA) using a column and
mobile phase mixture different, becoming its industrial application unfavorable. Thus,
many studies have being carried out to minimize this problem. An alternative would
use the UFLC, which is based with the same principles of HPLC, however it uses
stationary phases with particles smaller than 2 ?m. Therefore, this study goals to
develop and validate new analytical methods to determine simultaneously the drugs
by HPLC/DAD and UFLC/DAD. For this, a analytical screening was carried out,
which verified that is necessary a gradient of mobile phase system A (acetate
buffer:methanol 94:6 v/v) and B (acetate buffer:acetonitrile 55:45 v/v). Furthermore,
to the development and optimization of the method in HPLC and UFLC, with
achievement of the values of system suitability into the criteria limits required for both
techniques, the validations have began. Standard solutions and tablets test solutions
were prepared and injected into HPLC and UFLC, containing 0.008 mg/mL ISN,
0.043 mg/mL PYR, 0.030 mg.mL-1 ETA and 0.016 mg/mL RIF. The validation of
analytical methods for HPLC and UFLC was carried out with the determination of
specificity/selectivity, analytical curve, linearity, precision, limits of detection and
quantification, accuracy and robustness. The methods were adequate for
determination of 4 drugs separately without interfered with the others. Precise, due to
the fact of the methods demonstrated since with the days variation, besides the
repeatability, the values were into the level required by the regular agency. Linear
(R> 0,99), once the methods were capable to demonstrate results directly
proportional to the concentration of the analyte sample, within of specified range.
Accurate, once the methods were capable to present values of variation coefficient
and recovery percentage into the required limits (98 to 102%). The methods showed
LOD and LOQ very low showing the high sensitivity of the methods for the four drugs.
The robustness of the methods were evaluate, facing the temperature and flow changes, where they showed robustness just with the preview conditions established
of temperature and flow, abrupt changes may influence with the results of methods / A tuberculose ? uma doen?a grave, por?m cur?vel em praticamente 100% dos casos
novos, desde que obedecidos os princ?pios da moderna quimioterapia. S?o
considerados f?rmacos de 1? linha no tratamento ? tuberculose: isoniazida,
pirazinamida, etambutol e rifampicina. De acordo com USP 33 - NF28 (2010) as
an?lises cromatogr?ficas para 3 dos 4 f?rmacos (isoniazida, pirazinamida e
rifampicina) duram em m?dia 15 minutos e mais 10 minutos para a obten??o do 4?
f?rmaco (etambutol) utilizando outra coluna, com outra mistura de fase m?vel,
tornando esta aplica??o na pr?tica industrial desfavor?vel. Uma das alternativas ?
utilizar o CLUE, o qual baseia-se nos mesmos princ?pios da CLAE, por?m utiliza
fases estacion?rias com part?culas menores que 2 ?m. Dessa forma pretende-se
com o presente estudo desenvolver e validar novos m?todos anal?ticos para
determina??o simult?nea de tuberculost?ticos por CLAE/DAD e CLUE/DAD. Para
isto, foi realizado um screening anal?tico, o qual verificou que ? necess?rio um
gradiente de sistema de fase m?vel A (tamp?o acetato:metanol 94:6 v/v) e B
(tamp?o acetato:acetonitrila 55:45 v/v). Posteriormente, ao desenvolvimento e
otimiza??o do m?todo em CLAE e CLUE com a obten??o dos valores de
adequabilidade do sistema dentro dos limites de aceita??es vigente para ambos as
t?cnicas, as valida??es deram-se in?cio. Solu??es padr?es e solu??es testes dos
comprimidos foram preparadas e injetadas no CLAE e CLUE, contendo isoniazida,
pirazinamida, etambutol e rifampicina nas concentra??es de 0,008, 0,043, 0,030 e
0,016 mg.mL-1, respectivamente. A valida??o dos m?todos anal?ticos foram
realizadas para: especificidade / seletividade, intervalos da curva anal?tica,
linearidade, limite de detec??o, limite de quantifica??o, exatid?o, precis?o
(repetibilidade, precis?o intermedi?ria) e robustez. Os m?todos foram adequados
para determina??o dos 4 f?rmacos separadamente sem interfer?ncia nos demais.
Precisos, devido ao fato de que os m?todos demonstraram que mesmo com
varia??o de dias, al?m da repetibilidade, os valores ficaram dentro da faixa
preconizada na legisla??o vigente. Lineares (R > 0,99), ou seja, os m?todos foram
capazes de demonstrar que os resultados obtidos eram diretamente proporcionais ?
concentra??o do analito na amostra, dentro de um intervalo especificado. Exatos,
uma vez que os m?todos foram capazes de apresentar valores de coeficiente de varia??o e porcentagem de recupera??o dentro dos limites exigidos (98 a 102%). Os
m?todos mostraram LD e LQ com n?veis baixos demonstrando que os m?todos
possuem elevada sensibilidade aos quarto f?rmacos. A robustez foi avaliada frente
?s altera??es de temperatura e fluxo, onde os m?todos demonstraram-se robustos
apenas nas condi??es previamente estabelecidas de temperatura e fluxo, altera??es
bruscas podem acarretar influ?ncia nos resultados dos m?todos
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