ABSTRACT
Southern Brazil has the highest prevalence rate of AIDS in the country and is the only region in the Americas where HIV-1 subtype C prevails. OBJECTIVE: We evaluated the epidemiologic and clinical characteristics of pregnant women living with HIV/AIDS in the South region of Santa Catarina, Brazil. METHODS: All pregnant women with HIV infection attending the obstetric outpatient clinic of Criciúma, State of Santa Catarina, in 2007 (n = 46) were invited to participate. Data of 36 eligible participants were obtained through a standardized questionnaire. RESULTS: The great majority were young, with a steady partner, low family income, low education level and referring early first sexual intercourse. Many reported use of illicit non-injecting drugs (55.5 percent) and unprotected sex with partners that were HIV-positive (57.7 percent), injecting drug user (22.2 percent), male inmate (19.4 percent), truck driver (13.8 percent), with history of sexually transmitted disease (11.1 percent) or men who have sex with men (MSM) (2.8 percent). Most (66.7 percent) of the participants had their HIV diagnosis done during the pregnancy, 7 (19.4 percent) had a previous history of HIV mother-to-child transmission. Therapy based on highly active antiretroviral therapy (94 percent) was initiated at 19.3 weeks on average and 33 percent showed irregular antiretroviral adherence. CONCLUSION: These results confirm previous data on HIV epidemiology in Brazil and suggest that the women partners' sexual behavior and unprotected sexual intercourse are important aspects of HIV epidemic. Additional efforts in education, prophylaxis and medication adherence are needed.
Subject(s)
Adolescent , Adult , Female , Humans , Male , Pregnancy , Young Adult , HIV Infections/epidemiology , HIV-1 , Pregnancy Complications, Infectious/epidemiology , Brazil/epidemiology , Cross-Sectional Studies , HIV Infections/virology , Parity , Prevalence , Pregnancy Complications, Infectious/virology , Risk Factors , Sexual Behavior , Socioeconomic FactorsABSTRACT
Anti-obesity drugs such as mazindol and beta-phenylethylamine derivatives induce their therapeutic effects by inhibiting noradrenaline and dopamine reuptake. In the hypothalamus, noradrenaline and dopamine play an important role in the control of appetite. Sibutramine reduces food intake due to a mechanism of action discretely distinct from beta-phenylethylamine products. In fact, this drug also decreases serotonin reuptake, which is a neurotransmitter quite related to satiety. Rimonabant was considered anovelty on the treatment of obesity, mainly due to its quite new mechanism of action, which is based on the blockade of CB1 receptors. Thus, considering a recent increase in the consumption of such anti-obesity drugs, this study aimed to perform a systematic review about the safety of these drugs. Based on literature, this study concluded that beta-phenylethylaminic drugs and mazindol show many side effects, mainly due to the activation of the sympathetic system (i.e. cardiovascular and gastrointestinal effects, and also central side effects, such as anxiety, and insomnia). Despite sibutramine is well tolerated by patients, clinical studies show that this drugis able to evoke similar sympathetic central and peripheral effects. Regarding rimonabant, the clinical use of this drug was linked to an increase in the incidence of major depression. In conclusion, despite most of the side effects evoked by anti-obesity drugs are classified as of low to moderate intensity, physicians must be aware of such effects upon prescription. In addition, they have to pay attention to the contraindications of such anti-obesity drugs in order to avoid health complications.
Los fármacos antiobesidad tales como el mazindoly los derivados de la beta-feniletilamina actúan inhibiendo la recaptación de la noradrenalinay de la dopamina, neurotransmisores que en el hipotálamo desenvuelven papel importante en el control del apetito. La sibutramina presenta mecanismo de acción discretamente diferente porque disminuye también la recaptación deserotonina, lo cual es positivo porque la activación del sistema serotoninérgico provoca saciedad. El rimonabanto surgió como una novedad para el tratamiento de la obesidad debido a su mecanismo de acción por medio del bloqueo de receptores cannabinoides CB1. Así, considerando el uso creciente y indiscriminado de moduladores del apetito este estudio tiene como principal objetivo realizar una revisión sistemática de la literatura sobre los efectos adversos de estos fármacos. De acuerdo con la literatura, este estudio concluyó que los fármacos beta-feniletilamínicos y el mazindol provocan varios efectos adversos derivados dela activación del sistema simpático, como sonlos efectos gastrointestinales y cardiovasculares, además de algunos efectos secundarios centrales, tales como ansiedad e insomnio. A pesar de la sibutramina ser mejor tolerada por los pacientes, los estudios clínicos muestran que este fármaco es responsable de varios efectos centrales y periféricos simpáticos. Con relación al rimonabanto, a pesar de la expectativa en relación a su mecanismo de acción innovador, su uso clínico demostró efectos adversos graves, como una depresión mayor. Enconclusión, aun cuando la mayor parte de los efectos secundarios provocados por los fármacos anti-obesidad fueron clasificados como de bajao moderada intensidad, los médicos deben estar conscientes de tales efectos secundarios en el momento de la prescripción de un fármaco anorexígeno. Además, deben estar atentos a las contra indicaciones de los tratamientos para la obesidad, a fin de evitar complicaciones mayores.
Fármacos anorexígenos como o mazindole os derivados da beta-feniletilamina ageminibindo a recaptação de noradrenalina edopamina, cujos neuro transmissores estão envolvidos em nível hipotalâmico no controle do apetite. A sibutramina possui mecanismo de ação ligeiramente diverso, pois também inibe a recaptação de serotonina, sendo um ponto positivo, visto que a ativação do sistema serotoninérgico promove a saciedade. O rimonabanto despontou como uma novidade no tratamento da obesidade, graças ao seu mecanismo de ação baseado no bloqueio de receptores canabinoides CB1. Considerando o uso crescente e indiscriminado de moduladores do apetite, o presente estudo visa fazer uma revisão sistemática da literatura sobre os efeitos adversos e as contraindicações do uso desses fármacos. Com base na literatura, este estudo concluiu que os fármacos beta-feniletilamínicos e o mazindol apresentam muitos efeitos adversos decorrentes da ativação do sistema simpático, como distúrbios gastrintestinais e cardiovasculares, além de alguns efeitos centrais, como ansiedade e insônia. Apesar de a sibutramina ser mais bem tolerada, os estudos clínicos mostram que este fármaco é também responsável por sintomas relacionados à ativação simpática periférica e a estimulação do sistema nervoso central. O rimonabanto, apesar das expectativas com relação ao seu mecanismo de ação inovador, mostrou efeitos adversos graves, como depressão maior. Em conclusão, muito embora os efeitos adversos fossem considerados de intensidade leve ou moderada, o médico precisa ter em mente tais situações no momento da prescrição de um fármaco anorexígeno. Além disso, deve estaratento às contraindicações dos tratamentos para obesidade, a fim de evitar maiores complicações.
Subject(s)
Appetite Depressants/analysis , Appetite Depressants/adverse effects , Appetite Depressants/pharmacology , Amphetamines/adverse effects , Anti-Obesity Agents/adverse effects , Anti-Obesity Agents/pharmacology , Obesity , Synaptic TransmissionABSTRACT
Melissa officinalis (L.) (Lamiaceae), a plant known as the lemon balm, is native to the east Mediterranean region and west Asia. Also found in tropical countries, such as Brazil, where it is popularly known as "erva-cidreira" or "melissa", it is widely used in aqueous- or alcoholic-extract form in the treatment of various disorders. The aim was to investigate in vivo its antigenotoxicity and antimutagenicity, as well as its genotoxic/mutagenic potential through comet and micronucleus assaying. CF-1 male mice were treated with ethanolic (Mo-EE) (250 or 500 mg/kg) or aqueous (Mo-AE) (100 mg/kg) solutions of an M. officinalis extract for 2 weeks, prior to treatment with saline or Methyl methanesulfonate (MMS) doses by intraperitoneal injection. Irrespective of the doses, no genotoxic or mutagenic effects were observed in blood and bone-marrow samples. Although Mo-EE exerted an antigenotoxic effect on the blood cells of mice treated with the alkylating agent (MMS) in all the doses, this was not so with Mo-AE. Micronucleus testing revealed the protector effect of Mo-EE, but only when administered at the highest dose. The implication that an ethanolic extract of M. officinalis has antigenotoxic/antimutagenic properties is an indication of its medicinal relevance.