ABSTRACT
Abstract Introduction Otomycosis is a common diseases that can be associated with many complications including involvement of the inner ear and mortality in rare cases. Management of otomycosis can be challenging, and requires a close follow-up. Treatment options for otomycosis include local debridement, local and systemic antifungal agents and utilization of topical antiseptics. Objective This study was designed to compare the recovery rate of otomycosis using two therapeutic methods; topical betadine (Povidone-iodine) and clotrimazole. Methods In this single-blind clinical trial, 204 patients with otomycosis were selected using a non-probability convenient sampling method and were randomly assigned to two treatment groups of topical betadine and clotrimazole (102 patients in each group). Response to treatment was assessed at 4, 10 and 20 days after treatment. Data were analyzed using the independent t-test, Chi-Square and Fisher exact test in SPSS v.18 software, at a significance level of p < 0.05. Results The results showed that out of 204 patients with otomycosis, fungi type isolated included Aspergillus in 151 cases (74%), and Candida albicans in 53 patients (26%). On the fourth day after treatment, 13 patients (13.1%) in the group treated with betadine and 10 patients (9.8%) in the group treated with clotrimazole showed a good clinical response to treatment (p = 0.75). A good response to treatment was reported for 44 (43.1%) and 47 patients (46.1%) on the tenth day after the treatment (p = 0.85); and 70 (68.6%) and 68 patients (67.6%) on the twentieth day after treatment (p = 0.46) in the groups treated with betadine and clotrimazole, respectively. The response to treatment was thus not significantly different in the two groups. Conclusion In the present study the efficacy of betadine and clotrimazole was the same for the treatment of otomycosis. The result of this study supports the use of betadine as an effective antifungal in otomycosis treatment, helping to avoid the emergence of resistant organisms.
Resumo Introdução A otomicose é uma das doenças comuns associadas a muitas complicações, como envolvimento da orelha interna e mortalidade em casos raros. O tratamento da otomicose pode ser realmente desafiador e requer um acompanhamento rigoroso. As opções de tratamento para otomicose podem incluir desbridamento local, agentes antifúngicos locais e sistêmicos e uso de antissépticos tópicos, os medicamentos tópicos recomendados para o tratamento da otomicose. Objetivo Comparar a taxa de recuperação de otomicose utilizando dois métodos terapêuticos de betadina tópica (povidona-iodo) e clotrimazol. Método Neste ensaio clínico simples cego, 204 pacientes com otomicose foram selecionados utilizando-se método de amostragem de não probabilidade conveniente e randomizados para dois grupos de tratamento, com betadina tópica e com clotrimazol (102 pacientes em cada grupo). A resposta ao tratamento foi avaliada aos 4, 10 e 20 dias após o tratamento. Os dados foram analisados utilizando o teste t independente, qui-quadrado e teste de Fisher no software SPSS v.18, com nível de significância de p < 0,05. Resultados Os resultados mostraram que dos 204 pacientes com otomicose, os tipos de fungos isolados incluíram Aspergillus em 151 casos (74%) e Candida albicans em 53 pacientes (26%). No quarto dia após o tratamento, 13 pacientes (13,1%) no grupo tratado com betadina e 10 pacientes (9,8%) no grupo tratado com clotrimazol apresentaram boa resposta ao tratamento (p = 0,75). Uma boa resposta ao tratamento foi relatada para 44 (43,1%) e 47 pacientes (46,1%) no décimo dia após o tratamento (p = 0,85); e 70 (68,6%) e 68 pacientes (67,6%) no vigésimo dia após o tratamento (p = 0,46) no grupo tratado com betadina e clotrimazol, respectivamente. Assim, a resposta ao tratamento não foi significativamente diferente nos dois grupos. Conclusão No presente estudo, a eficácia da betadina e do clotrimazol foi a mesma no tratamento da otomicose. O resultado deste estudo apoia o uso de betadina como um antifúngico eficaz no tratamento da otomicose que pode ajudar a evitar o surgimento de organismos resistentes.
Subject(s)
Humans , Male , Female , Adult , Middle Aged , Young Adult , Povidone-Iodine/administration & dosage , Clotrimazole/administration & dosage , Otomycosis/drug therapy , Anti-Infective Agents, Local/administration & dosage , Antifungal Agents/administration & dosage , Aspergillus/isolation & purification , Time Factors , Administration, Cutaneous , Candida albicans/isolation & purification , Single-Blind Method , Reproducibility of Results , Treatment OutcomeABSTRACT
La aspergilosis nasal es una de las principales causas de afección crónica de las fosas nasales en el canino. La sinología clínica es típica en toda enfermedad nasal crónica. Se presenta sobre todo epistaxis y ocasionalmente dolor. La evaluación rinoscópica de la zona permite encontrar hallazgos asociados con la patología y tomar muestras para citología y cultivo. La terapéutica sistémica con antifúngicos orales ha sido de utilidad variable, pero actualmente se ha remplazado con la medicación tópica directa en el área afectada. Este artículo describe el caso clínico de un canino, macho de cuatro años de edad, que fue presentado a consulta por secreción nasal mucosanguinolenta unilateral con una semana de evolución. El paciente se venía tratando en otro centro veterinario con ciclonamina y vitamina K por un posible trastorno en la coagulación. Después de una serie de exámenes que incluyeron rinoscopia y cultivo para hongos, se diagnosticó aspergilosis nasal. Se realizaron dos aplicaciones de clotrimazol intranasal que permitieron la resolución de los signos clínicos.
Nasal aspergillosis is a major chronic disease affecting the nostrils in dogs. Clinical sinology is typical in every chronic nasal disease. Epistaxis and occasional pain occurs. Rhinoscopic assessment of the area evidences findings associated with the pathology and allows collecting samples for cytology and culture. Systemic therapy with oral antifungals has had variable utility, but now it has been replaced by direct topical medication to the affected area. This article describes the case of a 4-years-old male dog, submitted to consultation by unilateral muco-bloody nasal discharge with a week of evolution. The patient was treated by another vet center with cyclonamine and vitamin K for a possible clotting disorder. After a series of tests that included rhinoscopy and fungal culture, nasal aspergillosis was diagnosed. Intranasal clotrimazole was applied twice and it allowed the resolution of the clinical signs.
A aspergilose nasal é uma das principais causas de afecção crônica das fossas nasais no canino. A sinologia clínica é típica em toda doença nasal crônica. Apresenta-se sobre tudo epistaxe e ocasionalmente dor. O exame rinoscópico da zona permite encontrar achados associados com a patologia e tomar amostras para citologia e cultivo. A terapêutica sistêmica com antifúngicos orais tem sido de utilidade variável, mas atualmente substituiu-se com a medicação tópica direta na área afetada. Este artigo descreve o caso clínico de um canino, macho de 4 anos de idade, que foi apresentado à consulta por secreção nasal muco sanguinolento unilateral com uma semana de evolução. O paciente estava sendo tratado em outro centro veterinário com ciclonamina e vitamina K por um possível transtorno na coagulação. Depois de uma série de exames que incluíram rinoscopia e cultivo para fungos, se diagnosticou aspergilose nasal. Realizaram-se duas aplicações de clotrimazol intranasal que permitiram a resolução dos sinais clínicos.
ABSTRACT
La candidiasis orofaríngea (COF) permanece como una de las principales infecciones oportunistas en pacientes infectados con el virus de la inmunodeficiencia humana (VIH) y con el síndrome de inmunodeficiencia adquirida (sida), y aunque su incidencia ha disminuido con la introducción de la terapia antirretroviral de alta eficacia, continúa siendo una afección característica en estos pacientes. En el presente trabajo se realizó un estudio de susceptibilidad in vitro mediante la metodología del CLSI, frente a itraconazol, ketoconazol y clotrimazol de 144 aislamientos clínicos de Candida, aisladas de la cavidad oral de pacientes infectados con el VIH/sida con cuadros clínicos de COF. La identificación de los aislamientos demostró que más del 90% pertenecían a Candida albicans. Al determinar el patrón general de susceptibilidad frente a los azoles estudiados mediante el método de microdilución en caldo del documento M27-A2 del Clinical and Laboratory Standard Institute, C. albicans exhibió valores de concentración mínima inhibitoria (CMI) en un rango de 0,01 a 8µg/mL para el itraconazol y el ketoconazol y de 0,01 a 2 g/mL para el clotrimazol. Sólo el 2,1 % de los aislamientos mostró franca resistencia frente al itraconazol, en tanto que el 3,5 % quedó clasificado dentro de la categoría susceptible dosis-dependiente para este triazol. La mayoría de los aislamientos de C. albicans mostraron valores de CMI frente al ketoconazol y al clotrimazol menores a 0.06 g/mL, siendo de un 96,9% (129 aislamientos) y de un 97,7% (129 aislamientos), respectivamente. El clotrimazol tuvo una mejor actividadin vitro comparado con los restantes azoles frente a los aislamientos estudiados. Candida spp. Mostró una elevada sensibilidad in vitro a los azoles estudiados. Se hace necesario continuar realizando estudios epidemiológicos para determinar los patrones de susceptibilidad y tasas de resistencias frente a los agentes...
The oropharyngeal candidiasis (OFC) remains as one of the principal opportunistic infections in patients infected with the human immunodeficiency virus (HIV) and with the acquired immunodeficiency syndrome (aids), and although his incidence has declined with the introduction of the highly active anti-retroviral therapy (HAART), remains as a typical complaint in these patients. A study of antifungal in vitro susceptibility testing, following the CLSI methodology, was realized against itraconazole, ketoconazole and clotrimazole of 144 clinical isolations of Candida, isolated from the oral cavity of patients infected with HIV/aids, with clinical pictures of OFC. The isolations identification, demonstrated that more than 90% belonged to Candida albicans. The determination of the general pattern of susceptibility, following the document M27-A2 of the Clinical and Laboratory Standard Institute, against to the studied azoles by means of the method of microdilution in liquid medium, show that the majority of C. albicans isolates showed values of MIC against ketoconazole and clotrimazole lower than 0.06 g/mL, representing a 96,9% (129 isolations) and a 97,7% (129 isolations), respectively. C. albicans exhibited the widest range of minimal inhibitory concentration (MIC). Only 2.1% of the isolations showed resistance against to itraconazole, while 3.5 % remained classified in the category sensible dose - dependent for this triazole. The majority of the strains showed values of MIC against ketoconazole and clotrimazole below 0.06 g/mL. The clotrimazole had a better in vitro activity compared with the remaining azoles opposite to the isolations. Candida spp. showed a high in vitro sensibility to the azoles studied. It becomes necessary the maintenance of epidemiologic studies for the determination of susceptibility patterns and of resistances rates against to the antifungal agents
Subject(s)
Female , Acquired Immunodeficiency Syndrome , Candida , Candida , Ketoconazole/therapeutic use , Clotrimazole/therapeutic use , HIV , Itraconazole/therapeutic use , AIDS-Related Opportunistic Infections/pathology , AIDS-Related Opportunistic Infections/drug therapyABSTRACT
Antimycotic clotrimazole (CTZ) has demonstrated remarkable activity against Plasmodium falciparum in vitro and in vivo. Hemoglobin degradation by Plasmodium parasites makes amino acids available for protein synthesis, inducing oxidative stress in infected cells and producing free heme. These events represent biochemical targets for potential antimalarials. In this study, we have tested the ability of CTZ to modify the oxidative status in Plasmodium berghei-infected erythrocytes. After hemolysis, activities of superoxide dismutase (SOD), catalase (CAT), glutathione cycle and NADPH+H+-producing dehydrogenases were investigated using UV-visible spectrophotometry. Thiobarbituric acid reactive substances (TBARS) were evaluated as a marker of lipid damage. Results showed that CTZ significantly decreased the overall activity of 6-phosphagluconate dehydrogenase (6PGD) compared to infected and non-treated cells; consequently, the glutathione cycle was inhibited, leaving the parasite vulnerable to the oxidative stress originating from hemoglobin degradation. As a compensatory response, CTZ prevented some loss of SOD and CAT activities in infected cells. The infection triggered lipid peroxidation in erythrocytes, which was decreased by CTZ. These results suggest the presence of a redox unbalance in cells treated with CTZ, discussing a possible effect of this compound disturbing the oxidative status in a Plasmodium berghei-infection.
O antifúngico clotrimazol (CTZ) tem demonstrado notável atividade contra Plasmodium falciparum. A degradação da hemoglobina por Plasmodium para a obtenção dos aminoácidos necessários à síntese protéica induz estresse oxidativo em eritrócitos devido à liberação de hemos oxidantes. Estes eventos representam alvos bioquímicos para a produção de antimaláricos potenciais. Neste estudo, testamos a capacidade do CTZ para modificar o estado oxidativo em eritrócitos infectados com Plasmodium berghei. Depois da hemólise, as atividades da superóxido dismutase (SOD), catalase (CAT), desidrogenases produtoras de NADPH+H+ e do ciclo de glutationa (GSH) foram investigados. A produção das espécies reativas ao ácido tiobarbitúrico (TBARS) foi avaliada como marcador de dano lipídico. Os resultados mostraram que o CTZ diminuiu a atividade da 6-fosfogliconato desidrogenase (6PGD), em comparação com eritrócitos infectados e não tratados. Consequentemente, o ciclo da GSH foi inibido, tornando os parasitas vulneráveis ao estresse oxidativo resultante da degradação da hemoglobina. Como resposta compensatória, CTZ impediu a perda de atividade da SOD e CAT nas células infectadas. A infecção induz peroxidação lipídica nos eritrócitos, sendo esta diminuída pelo CTZ. Estes resultados sugerem a existência de desequilíbrio redox nas células tratadas com CTZ, interferindo, assim, com o estado oxidativo verificado durante a infecção malárica.
Subject(s)
Plasmodium berghei/physiology , Clotrimazole/analysis , Oxidative Stress/physiology , Erythrocytes/classification , Hemin/classificationABSTRACT
The intermediate conductance Ca2+-activated K+ channels (SK4, IKCa1) are present in lymphocytes, and their membrane expression is upregulated by various immunological stimuli. In this study, the activity of SK4 was compared between Bal-17 and WEHI-231 cell lines which represent mature and immature stages of murine B lymphocytes, respectively. The whole-cell patch clamp with high-Ca2+ (0.8microM) KCl pipette solution revealed a voltage-independent K+ current that was blocked by clotrimazole (1 mM), an SK4 blocker. The expression of mRNAs for SK4 was confirmed in both Bal-17 and WEHI-231 cells. The density of clotrimazole-sensitive SK4 current was significantly larger in Bal-17 than WEHI-231 cells (-11.4+/-3.1 Vs. -5.7+/-1.15 pA/pF). Also, the chronic stimulation of B cell receptors (BCR) by BCR-ligation (anti-IgM Ab, 3microgram/ml, 8~12 h) significantly upregulated the amplitude of clotrimazole-sensitive current from -11.4+/-3.1 to -53.1+/-8.6 pA/pF in Bal-17 cells. In WEHI-231 cells, the effect of BCR-ligation was significantly small (-5.7+/-1.15 to -9.0+/-1.00 pA/pF). The differential expression and regulation by BCR-ligation might reflect functional changes in the maturation of B lymphocytes.
Subject(s)
B-Lymphocytes , Cell Line , Clotrimazole , Lymphocytes , Membranes , Potassium Channels , Potassium Channels, Calcium-Activated , RNA, MessengerABSTRACT
Se determinó la susceptibilidad in vitro frente a clotrimazol y nistatina de 123 aislamientos de Candida, obtenidos mediante exudados vaginales de 404 mujeres que asistieron al Hospital Ginecoobstétrico "Ramón González Coro" de Ciudad de La Habana. De acuerdo con el número de colonias obtenidas en el aislamiento primario, las cepas fueron separadas en 2 categorías: colonización e infección. Para cada cepa se determinó la concentración mínima inhibitoria (CMI) de cada antifúngico, mediante un método de microdilución en caldo casitona. Las medias geométricas de los valores de CMI fueron mayores frente a nistatina (1,08 mg/mL) que frente a clotrimazol (0,22 mg/mL), aunque los rangos fueron similares (£ 0,125-16 mg/mL). Para Candida albicans, que fue la especie aislada con mayor frecuencia (54,5 %); las medias geométricas de los valores de la CMI fueron de 0,17 y 0,16 mg/mL para clotrimazol y de 0,71 y 0,92 mg/mL para nistatina, en ambas categorías. C. glabrata mostró el valor de CMI más elevado (16 mg/mL) frente a ambos antifúngicos. Solo los aislamientos de C. lusitaniae mostraron diferencia significativa (p < 0,01) entre los valores de CMI de nistatina de acuerdo con el número de colonias en el aislamiento primario. En aislamientos procedentes de mujeres tratadas con clotrimazol y/o nistatina en episodios anteriores de candidiasis, se observaron valores más elevados de las medias de CMI frente a nistatina que frente a clotrimazol; aunque esta diferencia no fue estadísticamente significativa.
The susceptibility in vitro of 123 isolates of Candida against clotrimazole and nystatin was determined. The isolates were obtained by vaginal smears from 404 women that attended "Ramón Gonzalez Coro" Gynecoobstetric Hospital, in Havana City According to the number of colonies obtained in the primary isolation, the strains were separated into 2 categories: colonization and infection. The inhibitory minimum concentration was determined for each antigunfal by a method of microdilution in casitone broth. The geometrical means of the IMC values were higher against nystatin (1.08 mg/mL) than against clotrimazole (0.22 mg/mL), eventhough the features were similar ( £ 0.125 -16 mg/mL) For Candida albicans, that was the most frequently isolated species (54.5 %), the geometrical means of the IMC values were 0.17 and 0.16 mg/mL for clotrimazole and 0.71 and 0.92 for nystatin, in both categories. C. glabrata showed the highest IMC values (16 mg/mL) against antifungals. Only the isolates of C. lusitaniae showed a significant difference (p < 0.001) between the IMC values of nystatin according to the number of colonies in the primary isolation. In isolates from women treated with clotrimazole and/or nystatin in previous episodes of candidiasis, there were observed more elevated values of the means of IMC against nystatin than against clotrimazole, although this difference was not statistically remarkable.