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Oxidative stress is one of the primary instigators of the onset of various human ailments, including cancers, cardiovascular diseases, and dementia. Particularly, oxidative stress severely affects low-density lipid & protein (LDL) oxidation, leading to several detrimental health effects. Therefore, in this study, the effect of beeswax alcohol (BWA) was evaluated in the prevention of LDL oxidation, enhancement of paraoxonase 1 (PON-1) activity of high-density lipid & protein (HDL), and zebrafish embryo survivability. Furthermore, the implication of BWA consumption on the oxidative plasma variables was assessed by a preliminary clinical study on middle-aged and older human subjects (n = 50). Results support BWA augmentation of PON-1 activity in a dose-dependent manner (10-30 µM), which was significantly better than the effect exerted by coenzyme Q10 (CoQ10). Moreover, BWA significantly curtails LDL/apo-B oxidation evoked by CuSO4 (final 0.5 µM) and a causes a marked reduction in lipid peroxidation in LDL. The transmission electron microscopy (TEM) analysis revealed a healing effect of BWA towards the restoration of LDL morphology and size impaired by the exposure of Cu2+ ions (final 0.5 µM). Additionally, BWA counters the toxicity induced by carboxymethyllysine (CML, 500 ng) and rescues zebrafish embryos from development deformities and apoptotic cell death. A completely randomized, double-blinded, placebo-controlled preliminary clinical study on middle- and older-aged human subjects (n = 50) showed that 12 weeks of BWA (100 mg/day) supplementation efficiently diminished serum malondialdehyde (MDA) and total hydroperoxides and enhanced total antioxidant status by 25%, 27%, and 22%, respectively, compared to the placebo-control and baseline values. Furthermore, the consumption of BWA did not exhibit any noteworthy changes in physical variables, lipid profile, glucose levels, and biomarkers pertinent to kidney and liver function, thus confirming the safety of BWA for consumption. Conclusively, in vitro, BWA prevents LDL oxidation, enhances PON-1 activity in HDL, and positively influences oxidative variables in human subjects.
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BACKGROUND: Non-alcoholic fatty liver disease (NAFLD) encompasses a spectrum of diseases ranging from steatosis to steatohepatitis and cirrhosis. Given the increasing incidence of NAFLD and the long-term consequences of this disease, it is important to identify the risk factors and therapeutic measures. Abexol is a mixture of beeswax alcohols with antioxidant, gastro-protective and anti-inflammatory effects. The aim was to conduct a pooled analysis of clinical trials data of the effects of Abexol treatment in patients with NAFLD. METHODS: The present analysis includes the data of all patients with NAFLD obtained from medium-term randomized, double-blinded, placebo controlled clinical studies with Abexol. One hundred patients with NAFLD received Abexol (100 mg/day) or placebo for 6 months. Significant changes in the ultrasound analysis of the liver were considered a primary efficacy variable. Secondary endpoints were decreased homeostasis model assessment (HOMA) index and insulin levels, and improved clinical symptoms. Statistical analysis of all data was according to the intention-to-treat method. RESULTS: Both groups were statistically homogeneous at baseline conditions. At 6 months of treatment, the number of Abexol-treated patients exhibiting a normal liver echo pattern on ultrasonography was greater than that of the placebo patients (P < 0.05). Abexol significantly reduced (P < 0.05) insulin levels and HOMA index. The proportion of Abexol patients showing symptom improvement was higher (P < 0.01) than that of the placebo group. Treatments were safe and well tolerated. CONCLUSIONS: Treatment of Abexol during 6 months significantly ameliorates liver fat accumulation and insulin resistances, meanwhile improving clinical evolution in patients with NAFLD. The treatment was safe and well tolerated in these patients.
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Introducción. Los resultados de los estudios clínicos muestran que el tratamiento con policosanol (20 mg/día) + aspirina produce beneficios frente a placebo + aspirina en pacientes con ictus isquémico no cardioembólico reciente. Objetivo. Analizar los efectos del tratamiento con policosanol en pacientes hipertensos incluidos en dos ensayos de recuperación de ictus isquémico no cardioembólico. Pacientes y métodos. Pacientes hipertensos que sufrieron un ictus en los 30 días previos y que, con una puntuación de 2 a 4 en la escala de Rankin modificada (mRS), se distribuyeron aleatoriamente en dos grupos y recibieron policosanol + aspirina o placebo + aspirina durante seis meses. La variable primaria de eficacia fue la reducción de la puntuación en la mRS. Resultados. Se incluyó a un total de 142 pacientes hipertensos (edad media: 66 años) en el análisis. El policosanol + aspirina disminuyó significativamente la puntuación de la mRS desde el primer chequeo intermedio. El efecto del tratamiento con policosanol no desapareció, sino que incluso mejoró después de seis meses de tratamiento. El número de pacientes que alcanzaron valores de la mRS <= 1 fue mayor en el grupo de policosanol + aspirina (80,3%) que en el de placebo + aspirina (8,5%). Dos pacientes causaron baja del estudio y cuatro (dos de cada grupo) refirieron efectos adversos leves. Conclusiones. El tratamiento durante seis meses con policosanol + aspirina a pacientes hipertensos que habían sufrido un ictus isquémico no cardioembólico demostró ser más efectivo que el tratamiento con placebo + aspirina en su recuperación funcional
Introduction. Clinical studies results show that policosanol (20 mg/day) + aspirin therapy had benefits versus placebo + aspirin to patients with recent non-cardioembolic ischemic stroke. Aim. To analyze the policosanol treatment effects in the hypertensive patients included in two non-cardioembolic ischemic stroke recovery trials. Patients and methods. Hypertensive patients with a modified Rankin Scale (mRS) score 2 to 4 were randomized, within 30 days of onset, to policosanol + aspirin or placebo + aspirin, for six months. The primary outcome was mRS score reduction. Results. One hundred forty two hypertensive patients (mean age: 66 years) were included in the analysis. Policosanol + aspirin decreased significantly the mRS score mean from the first interim check-up. The policosanol treatment effect did not wear off, on the contrary, even improved after six months therapy. More over, policosanol + aspirin (80.3%) treatment achieved significant results (mRS ≤ 1), whereas the placebo + aspirin did not (8.5%). Two patients discontinued and four (two from each group) referred mild adverse events. Conclusions. The treatment for six months with policosanol + aspirin in hypertensive patients who had suffered a noncardioembolic ischemic stroke proved to be more effective than the placebo + aspirin treatment in the functional recovery of these patients
Assuntos
Humanos , Masculino , Feminino , Pessoa de Meia-Idade , Idoso , Acidente Vascular Cerebral/tratamento farmacológico , Hipertensão/tratamento farmacológico , Álcoois Graxos/uso terapêutico , Aspirina/uso terapêutico , Resultado do Tratamento , Reabilitação do Acidente Vascular Cerebral , Metabolismo dos LipídeosRESUMO
Introduction: the gastric mucosa is susceptible to the effects of aggressive factors, which are counterbalanced by mucosal defensive factors. Acid peptic diseases result from the imbalance between these aggressive and defensive factors. Aspirin-induced ulcer is a model of NSAIDs-induced damage in which neutrophil infiltration plays a key role. Objective: this paper investigates the protective effect of D-002 against aspirin-induced ulcers and associated neutrophil infiltration in the gastric mucosa. Methods: rats were randomized into six groups of 8 rats each. A negative vehicle control, and five aspirin (300 mg/kg)-treated groups: a positive control, orally treated with the vehicle, three with D-002 (25, 50 and 100 mg/kg, respectively) and other with 10 mg/kg Omeprazole. Five hours after induced damage the rats were sacrificed. The stomachs were removed and opened, and lesions examined macroscopically and microscopically. Ulcer indexes and neutrophil infiltration per ulcer areas were measured. Results: all positive, none negative, controls exhibited aspirin-induced ulcers. Oral treatment with D-002 (25-100 mg/kg) dose-dependently and significantly reduced aspirin-induced gastric lesions (37 to 75 ), the mean number of microscopic ulcers (40 to 72 por ciento) and neutrophil infiltration (41.7 to 83.1 por ciento) in the rat gastric mucosa. Conclusion: Oral treatment with D-002 (25-100 mg/kg) effectively protects against aspirin-induced ulcers and decreases the neutrophil infiltration in the gastric mucosa induced by aspirin ulceration(AU)
Introducción: la integridad de la mucosa gástrica depende del balance entre los factores agresivos y defensivos. La úlcera inducida por aspirina es un modelo de daño por antiinflamatorios no esteroidales en el cual el infiltrado de neutrófilos desempeña una función fundamental. Objetivo: evaluar el efecto protector del D-002 sobre la úlcera inducida por aspirina asociada al infiltrado de neutrófilos en la mucosa gástrica. Métodos: las ratas fueron aleatorizadas en seis grupos de ocho animales cada uno. Un control negativo con vehículo y cinco grupos tratados con aspirina (300 mg/kg): un control positivo, tratado por vía oral con vehículo, tres grupos con D-002 (25, 50 and 100 mg/kg respectivamente) y otro con omeprazol 10 mg/kg. Cinco horas después de inducido el daño las ratas fueron sacrificadas y se extrajeron sus estómagos para su análisis morfológico. Se determinó el índice de úlcera, el número de úlceras microscópicas y el número de neutrófilos por área ulcerada. Resultados: todos los controles positivos y ninguno negativo mostraron lesiones en la mucosa. El tratamiento por vía oral con D-002 (25-100 mg/kg) redujo de modo significativo y dependiente de la dosis el índice de úlceras gástricas (37-75 percent), el promedio de úlceras microscópicas (40- 72 percent) y la infiltración de neutrófilos (41,7-83,1 percent) en la mucosa de las ratas. Conclusiones: el tratamiento por vía oral con D-002 (25-100 mg/kg) protege la mucosa gástrica de las ratas del daño inducido por aspirina, lo que disminuye el índice de úlcera y el infiltrado de neutrófilos(AU)
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Animais , Ratos , Aspirina/efeitos adversos , Úlcera Gástrica/etiologia , Infiltração de NeutrófilosRESUMO
Introduction: the gastric mucosa is susceptible to the effects of aggressive factors, which are counterbalanced by mucosal defensive factors. Acid peptic diseases result from the imbalance between these aggressive and defensive factors. Aspirin-induced ulcer is a model of NSAIDs-induced damage in which neutrophil infiltration plays a key role. Objective: this paper investigates the protective effect of D-002 against aspirin-induced ulcers and associated neutrophil infiltration in the gastric mucosa. Methods: rats were randomized into six groups of 8 rats each. A negative vehicle control, and five aspirin (300 mg/kg)-treated groups: a positive control, orally treated with the vehicle, three with D-002 (25, 50 and 100 mg/kg, respectively) and other with 10 mg/kg Omeprazole. Five hours after induced damage the rats were sacrificed. The stomachs were removed and opened, and lesions examined macroscopically and microscopically. Ulcer indexes and neutrophil infiltration per ulcer areas were measured. Results: all positive, none negative, controls exhibited aspirin-induced ulcers. Oral treatment with D-002 (25-100 mg/kg) dose-dependently and significantly reduced aspirin-induced gastric lesions (37 to 75 ), the mean number of microscopic ulcers (40 to 72 por ciento) and neutrophil infiltration (41.7 to 83.1 por ciento) in the rat gastric mucosa. Conclusion: Oral treatment with D-002 (25-100 mg/kg) effectively protects against aspirin-induced ulcers and decreases the neutrophil infiltration in the gastric mucosa induced by aspirin ulceration
Introducción: la integridad de la mucosa gástrica depende del balance entre los factores agresivos y defensivos. La úlcera inducida por aspirina es un modelo de daño por antiinflamatorios no esteroidales en el cual el infiltrado de neutrófilos desempeña una función fundamental. Objetivo: evaluar el efecto protector del D-002 sobre la úlcera inducida por aspirina asociada al infiltrado de neutrófilos en la mucosa gástrica. Métodos: las ratas fueron aleatorizadas en seis grupos de ocho animales cada uno. Un control negativo con vehículo y cinco grupos tratados con aspirina (300 mg/kg): un control positivo, tratado por vía oral con vehículo, tres grupos con D-002 (25, 50 and 100 mg/kg respectivamente) y otro con omeprazol 10 mg/kg. Cinco horas después de inducido el daño las ratas fueron sacrificadas y se extrajeron sus estómagos para su análisis morfológico. Se determinó el índice de úlcera, el número de úlceras microscópicas y el número de neutrófilos por área ulcerada. Resultados: todos los controles positivos y ninguno negativo mostraron lesiones en la mucosa. El tratamiento por vía oral con D-002 (25-100 mg/kg) redujo de modo significativo y dependiente de la dosis el índice de úlceras gástricas (37-75 percent), el promedio de úlceras microscópicas (40- 72 percent) y la infiltración de neutrófilos (41,7-83,1 percent) en la mucosa de las ratas. Conclusiones: el tratamiento por vía oral con D-002 (25-100 mg/kg) protege la mucosa gástrica de las ratas del daño inducido por aspirina, lo que disminuye el índice de úlcera y el infiltrado de neutrófilos
Assuntos
Ratos , Aspirina/efeitos adversos , Infiltração de Neutrófilos , Úlcera Gástrica/etiologiaRESUMO
La artritis reumatoide, poliartritis inflamatoria más común del adulto, que afecta cerca del 1 % de la población mundial, predomina más en mujeres que en hombres, se presenta con mayor frecuencia entre los 30 y 50 años de edad, y conlleva a una gran discapacidad del paciente. Se caracteriza por una sinovitis erosiva simétrica, en la cual el tejido conjuntivo prolifera (pannus), invade y erosiona el cartílago y el hueso de las articulaciones y, a veces, por una afectación multisistémica. En la mayoría de los pacientes la enfermedad sigue una evolución crónica fluctuante que, si no se trata, ocasiona una progresiva destrucción, deformidad e incapacidad de las articulaciones afectadas. La enfermedad evoluciona con cifras elevadas de factor reumatoideo y /o anticuerpos anti-citrulinas. Constituyen aspectos esenciales del tratamiento óptimo de la enfermedad: el diagnóstico diferencial precoz; el tratamiento inicial con antiinflamatorios no esteroideos; el uso de fármacos modificadores del curso de la enfermedad; el uso posible de glucocorticoides, a dosis bajas por vía oral, o en inyección intraarticular; la evaluación periódica de la adecuación del tratamiento (monitorización radiológica, sérica y funcional de la progresión de la enfermedad y de la toxicidad asociada al tratamiento), y las intervenciones de educación y rehabilitación del paciente. Para evaluar nuevas terapias para el tratamiento de la artritis reumatoide, los modelos más usados son: el de la artritis inducida por adyuvante en ratas y artritis inducida por colágeno en ratas y ratones. Otros modelos recientes muestran datos limitados. La eficacia de varios compuestos revela que su efecto terapéutico es más predictivo de eficacia clínica en humano cuando se estudian los modelos de artritis por adyuvante y por colágeno, que los datos de un solo modelo(AU)
The rheumatoid arthritis, is the inflammatory polyarthritis commonest in adults affecting about the 1 % of world population, more predominant in women than men and more frequent in those aged 30 and 50 and entails a high level of inability of patient. It is characterized by a symmetrical erosive synovitis with proliferation of conjunctival tissue (pannus), invading and eroding the cartilage and joint bones, and sometimes, by a multisystem affection. In most patients the disease follows a fluctuating chronic course, which it is not treated, provoke a progressive destruction, deformity and inability of involved joints. The disease evolves with high figures of rheumatoid factor and/or anti- citrulline antibodies. These are essential features of an optimal treatment of this entity include: early differential diagnosis, initial treatment with non-steroidal anti-inflammatory drugs (NSAIDs), the use of disease course modifying drugs, the potential use of oral low-dose glucocorticoid agents or intra-articular injections, and a periodical assessment of treatment fitting (radiological serum and functional monitoring of disease progression and of treatment-associated toxicity) and the educational and rehabilitations interventions of patient. To assess the new therapies for treatment of rheumatoid arthritis, the more uses models are: that of the arthritis induced by adjuvant drugs in rats and the arthritis induced by collagen in rats and mice. Other new models show limited data. Effectiveness of several compounds reveals that its therapeutic effect is more predictive of the clinical effect in the human being when models of arthritis due to adjuvant drugs and collagen than data from an only one model(AU)
Assuntos
Artrite Reumatoide/fisiopatologia , Artrite Reumatoide/terapiaRESUMO
La artritis reumatoide, poliartritis inflamatoria más común del adulto, que afecta cerca del 1 % de la población mundial, predomina más en mujeres que en hombres, se presenta con mayor frecuencia entre los 30 y 50 años de edad, y conlleva a una gran discapacidad del paciente. Se caracteriza por una sinovitis erosiva simétrica, en la cual el tejido conjuntivo prolifera (pannus), invade y erosiona el cartílago y el hueso de las articulaciones y, a veces, por una afectación multisistémica. En la mayoría de los pacientes la enfermedad sigue una evolución crónica fluctuante que, si no se trata, ocasiona una progresiva destrucción, deformidad e incapacidad de las articulaciones afectadas. La enfermedad evoluciona con cifras elevadas de factor reumatoideo y /o anticuerpos anti-citrulinas. Constituyen aspectos esenciales del tratamiento óptimo de la enfermedad: el diagnóstico diferencial precoz; el tratamiento inicial con antiinflamatorios no esteroideos; el uso de fármacos modificadores del curso de la enfermedad; el uso posible de glucocorticoides, a dosis bajas por vía oral, o en inyección intraarticular; la evaluación periódica de la adecuación del tratamiento (monitorización radiológica, sérica y funcional de la progresión de la enfermedad y de la toxicidad asociada al tratamiento), y las intervenciones de educación y rehabilitación del paciente. Para evaluar nuevas terapias para el tratamiento de la artritis reumatoide, los modelos más usados son: el de la artritis inducida por adyuvante en ratas y artritis inducida por colágeno en ratas y ratones. Otros modelos recientes muestran datos limitados. La eficacia de varios compuestos revela que su efecto terapéutico es más predictivo de eficacia clínica en humano cuando se estudian los modelos de artritis por adyuvante y por colágeno, que los datos de un solo modelo
The rheumatoid arthritis, is the inflammatory polyarthritis commonest in adults affecting about the 1 % of world population, more predominant in women than men and more frequent in those aged 30 and 50 and entails a high level of inability of patient. It is characterized by a symmetrical erosive synovitis with proliferation of conjunctival tissue (pannus), invading and eroding the cartilage and joint bones, and sometimes, by a multisystem affection. In most patients the disease follows a fluctuating chronic course, which it is not treated, provoke a progressive destruction, deformity and inability of involved joints. The disease evolves with high figures of rheumatoid factor and/or anti- citrulline antibodies. These are essential features of an optimal treatment of this entity include: early differential diagnosis, initial treatment with non-steroidal anti-inflammatory drugs (NSAIDs), the use of disease course modifying drugs, the potential use of oral low-dose glucocorticoid agents or intra-articular injections, and a periodical assessment of treatment fitting (radiological serum and functional monitoring of disease progression and of treatment-associated toxicity) and the educational and rehabilitations interventions of patient. To assess the new therapies for treatment of rheumatoid arthritis, the more uses models are: that of the arthritis induced by adjuvant drugs in rats and the arthritis induced by collagen in rats and mice. Other new models show limited data. Effectiveness of several compounds reveals that its therapeutic effect is more predictive of the clinical effect in the human being when models of arthritis due to adjuvant drugs and collagen than data from an only one model