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Stability of Vancomycin Hydrochloride for Oral Solution Stored in Unit Doses at Room and Refrigerated TemperaturesArchibald, Timothy, Lewis, Paul, Brown, Stacy 01 December 2018 (has links)
No description available.
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Stability Evaluation of Unit-Dose Vancomycin Hcl Oral Solutions in Plastic Capped Oral Syringes and Plastic Sealed Dosing CupsBrown, Stacy D., Lewis, Paul 01 November 2018 (has links)
Purpose:
Oral vancomycin is a first-line treatment for Clostridium difficile-associated diarrhea. Preparation of oral vancomycin solutions historically has been facilitated by extemporaneous compounding, using various formulas or compounding kits, such as FIRST® - Vancomycin. More recently, FIRVANQ™ (vancomycin HCl) for oral solution was approved by the FDA, replacing the FIRST® compounding kits. Preparation and storage of unit-doses of oral solutions can expedite delivery of the medication to the patient and reduce opportunity for dosing errors. In this study, we evaluated the stored stability of two preparations of vancomycin HCl oral solution (FIRST® – Vancomycin and FIRVANQ™), stored in oral syringes and dosing cups at refrigerated and room temperatures.
Methods:
Triplicate batches of vancomycin HCl oral solution (50 mg/mL) were prepared using FIRST® - Vancomycin and FIRVANQ™, aliquoted into plastic oral syringes and sealed dosing cups, and stored at refrigerated and room temperatures for a total of six batches. Additionally, remaining samples from FIRVANQ™ batches were unit-dosed in clear Luer-Lok™ syringes and stored under refrigeration as a seventh batch. Samples were removed and analyzed for vancomycin recovery using a previously validated high-performance liquid chromatography with ultraviolet detection (HPLC-UV) method over a 30-day period. Recovery was quantitatively assessed by comparing to a freshly prepared United States Pharmacopoeia (USP) reference standard on each day of sampling.
Results:
Stability was defined as recovery of 90 - 110% of labeled amount. For all tested samples, the chemical potency remained within the therapeutically acceptable window for the entire study period of 30 days. At room temperature, the FIRST® syringes and cups both retained 95% potency after 30 days. Under refrigeration, this product retained 100% potency and 91% potency in syringes and cups, respectively. Similarly, the FIRVANQ™ room temperature syringes were at 99% recovery and the room temperature cups at 95% recovery after 30 days. Refrigerated FIRVANQ™ retained a potency of 102% potency in the dosing cups after 30 days, and the both syringes types (clear and amber) were 97% and 101%, respectively, recovery during the study period.
Conclusion:
The percent recovery of vancomycin in each test group remains within 90 – 110% of the labeled amount throughout duration of study (0 – 30 days). Based on this study, unit-dosing has been shown to have a 30-day chemical stability. In this case, unit-dosing not only may be used to improve workflow and reduce dosing errors, but may also have an impact of reducing drug waste due to avoidance of discarding appropriately potent drug product. Additionally, stability within the study period was independent of storage container and condition. Finally, this unit-dosing practice for FIRVANQ™ is equally acceptable in the classic luer-slip amber plastic syringes, and the newer Luer-Lok™ clear plastic syringes.
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High-Performance Liquid Chromatographic Method for a Compounded Vancomycin Oral Solution for Application Toward a Beyond-Use Date DeterminationKirk, Loren, Brown, Stacy D. 01 February 2014 (has links)
No description available.
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DESENVOLVIMENTO DE FORMULAÇÃO NA FORMA DE SOLUÇÃO ORAL DE SILDENAFIL PARA USO NA DISFUNÇÃO ERÉTILPaula, Daniel Jesus de 20 January 2010 (has links)
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Previous issue date: 2010-01-20 / The sprouting of sildenafil citrate (CSLD) was presented as an oral therapeutical form
effective for Erectile Dysfunction Treatment, however, sidenafil, in the tablet form,
has a period of latency of 30 to 40 minutes, being lengthened if administrated with
foods. Liquid formulations present advantages regarding latency period when
comparable to solid formulations, beyond being also a viable alternative for pediatric
use in Pulmonary hypertension, for being easier to be administrated and for allowing
dosage adjustment. The present work had developed pharmaceutical formulations
like oral form of solution and had submitted them to tests in not controlled conditions
and Accelerated Stability Test described in the Resolution RE no 1, July 29th of 2005.
It was used as methodology of analysis for dosing of the active ingredient High
pressure liquid chromatography (HPLC). The methodology was submitted to
validation, obeying resolution RE no 899, May 29th of 2005.The solutions were tested
initially in three concentrations (7,5, 5,0 and3.33%). The development of CSLD
solutions was made in the 3,33%concentration, since in the other concentrations (5
and 7.5%), the active ingredient precipitated due to solubility problems in ambient
temperature. The analytical methodology passed in the described tests of validation
in the RE no 899 of May 29th of 2003 and showed a safe and efficient method to
dosing CSLD in solution. The solutions with higher concentration of Soluphuor
solutions kept throughout the time the characteristics of physical, chemical and
microbiological stability, simulating the conditions of use in ambient temperature and
through Accelerated Stability Test lead as Resolution RE no 1, July 29th of 2005 as
well as in not controlled conditions (in use). While the solution with lower
concentration of solvent demonstrated unstable regarding to the solubility due the
lesser ratio of Soluphuor in the formulation, being therefore considered inadequate.
Solutions when propagated in different liquids (water, beer, soda, whiskey)didn't have
significant alterations regarding its organoleptics characteristics and nor had
intervened with the physico-chemical stability concerning to the concentration of
active ingredient. Concluding, the two solutions in the concentration of 3,33%
formulated with bigger concentration of Soluphuor had presented good physical,
chemical and microbiological stability and they possibly have easy industrial and
commercial application therefore they can have lower time of latency in the Erectile
Dysfunction. / O surgimento do citrato de sildenafil (CSLD) apresentou-se como uma
terapêutica oral efetiva para o tratamento da Disfunção Erétil (DE), no entanto o
sildenafil, na forma de comprimidos, tem um período de latência de 30 a 40 minutos,
podendo se prolongar mais se for tomado com alimentos. As formulações líquidas
apresentam vantagens quanto ao período de latência em relação às formulações
sólidas, alem de ser uma alternativa viável para o uso pediátrico na Hipertensão
Pulmonar, por ser mais fácil de ser administrado e por permitir o ajuste da posologia.
O presente trabalho desenvolveu formulações farmacêuticas na forma de solução
oral e as submeteram a testes em condições não controladas (de prateleiras) e
Estabilidade Acelerada descritos na Resolução RE nº 1 de 29 de julho de 2005.
Usou-se como metodologia de análise para doseamento do princípio ativo, a
Cromatografia Líquida de Alta Eficiência (CLAE). A metodologia foi submetida à
validação, obedecendo a resolução RE nº 899 de 29 de maio de 2003. Foram
desenvolvidas inicialmente soluções em três concentrações (7,5, 5,0 e 3,33%) e com
diferentes proporções de solvente Soluphuor®. As soluções de CSLD na
concentração de 3,33% foram submetidas aos testes de estabilidade uma vez que
as nas outras concentrações (5 e 7,5 %) houve precipitação do principio ativo por
problemas na solubilidade a temperatura ambiente. A metodologia analítica foi
aprovada nos testes de validação descritos na RE nº 899 de 29 de maio de 2003 e
se mostrou um método seguro e eficaz para dosear CSLD em solução. As soluções
com maior concentração de Solufuor mantiveram ao longo do tempo as
características de estabilidade física, química e microbiológica, simulando as
condições de uso em temperatura ambiente e através de estudo de estabilidade
acelerado conduzido conforme Resolução RE nº 1 de 29 de julho de 2005 bem como
em condições não controladas. Enquanto a solução com menor concentração do
solvente se demonstrou instável quanto a solubilidade devido a menor proporção de
Soluphuor ® na fórmula, sendo portanto, considerada inadequada. As soluções de
CSLD na concentração 3,33% quando veiculadas em diferentes líquidos (água,
cerveja, uísque e refrigerante) não tiveram alterações significantes quanto as suas
características organolépticas e nem interferiram na estabilidade fisicoquímica
quanto ao teor de principio ativo. Concluindo, as duas soluções na concentração de
3,33% formuladas com maior concentração de 2-pirrolidona apresentaram boa
estabilidade física, química e microbiológica e possivelmente tenham fácil aplicação
industrial e comercial pois podem ter o tempo de latência na Disfunção Erétil
diminuído.
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