RESUMO
Multiple drugs currently used in clinical practice have been approved by regulatory agencies based on studies that utilize composite endpoints. Composite endpoints are appealing because they reduce sample size requirements, follow-up periods, and costs. However, interpreting composite endpoints can be challenging, and their misuse is not uncommon. Incorrect interpretation of composite outcomes can lead to misleading conclusions that impact patient care. To correctly interpret composite outcomes, several important questions should be considered. Are the individual components of the composite outcome equally important to patients? Did the more and less important endpoints occur with similar frequency? Do the component endpoints exhibit similar relative risk reductions? If these questions receive affirmative answers, the use and interpretation of the composite endpoint would be appropriate. However, if any component of the composite endpoint fails to satisfy the aforementioned criteria, interpretation can become difficult, necessitating additional steps. Regulatory agencies acknowledge these challenges and have specific considerations when approving drugs based on studies employing composite endpoints. In conclusion, composite endpoints are valuable tools for evaluating the efficacy and net clinical benefit of interventions; however, cautious interpretation is advised.
RESUMO
Amid the coronavirus disease 2019 (COVID-19) pandemic, massive immunization campaigns became the most promising public health measure. During clinical trials, certain neurological adverse effects following immunization (AEFIs) were observed; however, acceptable safety profiles lead to emergency authorization for the distribution and use of the vaccines. To contribute to pharmacovigilance and lessen the potential negative impact that vaccine hesitancy would have on immunization programs, we conducted a review of the scientific literature concerning the epidemiological data, clinical presentation, and potential mechanisms of these neurological AEFIs. There is some epidemiological evidence linking COVID-19 vaccines to cerebral venous sinus thrombosis, arterial ischemic stroke, convulsive disorder, Guillain-Barré syndrome, facial nerve palsy, and other neurological conditions. Cerebral venous sinus thrombosis has been associated with a thrombotic thrombocytopenia induced by the vaccine, similar to that induced by heparin, which suggests similar pathogenic mechanisms (likely involving antibodies against platelet factor 4, a chemokine released from activated platelets). Arterial ischemic stroke is another thrombotic condition observed among some COVID-19 vaccine recipients. Vaccine-induced convulsive disorder might be the result of structural abnormalities potentially caused by the vaccine or autoimmune mechanisms. Guillain-Barré syndrome and facial nerve palsy may also be linked to the immunization event, possibly due to immune mechanisms such as uncontrolled cytokine release, autoantibody production, or bystander effect. However, these events are mostly uncommon and the evidence for the association with the vaccine is not conclusive. Furthermore, the potential pathophysiological mechanisms remain largely unknown. Nevertheless, neurological AEFIs can be serious, life-threatening or even fatal. In sum, COVID-19 vaccines are generally safe and the risk of neurological AEFIs does not outweigh the benefits of immunization. However, early diagnosis and treatment of neurological AEFIs are of utmost importance, and both health professionals and the public should be aware of these conditions.
A review of undesired effects involving the nervous system following the administration of COVID-19 vaccines Among the range of complications that can occur after a vaccine, some of them can affect the nervous system and its vasculature. This narrative review aims to evaluate some serious neurological conditions following COVID-19 vaccination. We searched biomedical journal databases where physicians around the globe reported different complications after the administration of different COVID-19 vaccines. Besides reports of cases in individual patients or small groups, we reviewed studies that included bigger groups of patients (e.g. vaccinated versus non-vaccinated) and compared the occurrence of these events between them. We found that after the administration of a certain type of vaccine (e.g. ChAdOx1-S/Oxford, AstraZeneca vaccine), serious neurological complications were rare, with abnormal clot formation involving cerebral blood vessels being one of the most important among them. Nonetheless, other conditions have been observed after the administration of the vaccines; however, it is not certain yet if the vaccines are the actual cause of these complications. There are some hypotheses that could explain why these adverse reactions take place after a vaccine. For instance, an abnormal immune response to the vaccine leads to the production of antibodies (i.e. proteins made by the immune system in response to the presence of a foreign substance). These antibodies trigger a response that could eventually result in clot formation. Besides, the immune response can also produce other adverse effects, including convulsive disorder, GuillainBarré syndrome, and facial nerve palsy. Scientific evidence suggests that vaccines are safe overall. While mild complications, such as pain at the site of injection or bruising might occur, more serious events remain rare. Furthermore, the complications derived from COVID-19 are far more likely in non-vaccinated individuals than the complications associated with the vaccine. Thus, vaccination continues to be the safest and most effective strategy to control the ongoing pandemic. However, both health professionals and the public should be aware of the possibility of serious neurological adverse reactions occurring after vaccination to allow early diagnosis and treatment.
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Long QT syndromes can be either acquired or congenital. Drugs are one of the many etiologies that may induce acquired long QT syndrome. In fact, many drugs frequently used in the clinical setting are a known risk factor for a prolonged QT interval, thus increasing the chances of developing torsade de pointes. The molecular mechanisms involved in the prolongation of the QT interval are common to most medications. However, there is considerable inter-individual variability in drug response, thus making the application of personalized medicine a relevant aspect in long QT syndrome, in order to evaluate the risk of every individual from a pharmacogenetic standpoint.
Assuntos
Efeitos Colaterais e Reações Adversas Relacionados a Medicamentos , Síndrome do QT Longo/induzido quimicamente , Torsades de Pointes/induzido quimicamente , Humanos , Preparações Farmacêuticas , Fatores de RiscoRESUMO
La warfarina es el anticoagulante más empleado en el mundo por su conveniencia y bajo costo. Sin embargo, su efectividad y seguridad están determinadas por el monitoreo paraclínico del INR, el control de la ingesta de vitamina K, las interacciones medicamentosas y el perfil farmacogenético entre otros factores, que podrían condicionar la ocurrencia de complicaciones trombóticas o hemorrágicas. Se presenta el caso de una paciente con hemorragia en el muslo secundaria a warfarina, en quien la falta de adherencia al esquema posológico prescrito, la falta de seguimiento y una posible interacción con el omeprazol fueron identificados por el servicio de Farmacia Clínica del hospital como factores determinantes de la reacción adversa a medicamento. La intervención farmacéutica consistió en sugerir la sustitución de warfarina por apixabán, medicamento de una costo-efectividad similar, que no requiere monitoreo paraclínico y carece de interacciones medicamentosas en la paciente
Warfarin is the most widely used anticoagulant in the world due to its convenience and low cost. However, its effectiveness and safety are determined by monitoring INR, control of vitamin K intake, drug interactions and the pharmacogenetic profile among other factors, which could condition the occurrence of thrombotic or hemorrhagic complications. We present the case of a patient with a haemorrhage in the thigh (that is) secondary to warfarin, in whom the lack of adherence to the prescribed dosage regimen, the lack of follow-up and a possible interaction with omeprazole were identified by the hospital's Clinical Pharmacy service as determinant factors for the adverse drug reaction. The pharmaceutical intervention consisted of suggesting the substitution of warfarin for apixaban, a similar cost-effective drug that does not require paraclinical monitoring and lacks drug interactions in patients
Assuntos
Humanos , Feminino , Idoso de 80 Anos ou mais , Erros de Medicação/efeitos adversos , Varfarina/efeitos adversos , Hemorragia/complicações , Adesão à Medicação , Substituição de Medicamentos/métodos , Erros de Medicação/prevenção & controle , Farmacovigilância , Anticoagulantes/efeitos adversos , Acenocumarol/efeitos adversos , Tromboembolia/prevenção & controleRESUMO
Forty-one year old female admitted to the hospital because of symptoms and signs suggestive of pulmonary thromboembolism which was confirmed by CT angiography. There was no history of prior thromboembolic events, smoking, venous stasis or vascular lesion (negative lupus anticoagulant and anticardiolipins). The only documented hypercoagulability factor was the use of an oral contraceptive containing drospirenone and ethinylestradiol for the last year. The patient was treated with anticoagulants such as enoxaparin and she recovered without sequelae; she is currently under treatment with warfarin as an outpatient. It is known that the use of combined oral contraceptives in patients over 35 years old requires caution, largely due to higher risk of thromboembolic events associated with increased hepatic synthesis of several coagulation factors. Therefore, this case represents a potentially fatal and preventable severe adverse reaction(AU)
Mujer de 41 años que ingresa al hospital por cuadro clínico sugestivo de tromboembolismo pulmonar, el cual fue confirmado por AngioTAC. No había antecedentes de eventos tromboembólicos previos, tabaquismo, estasis venosa ni de lesión vascular (anticoagulante lúpico y anticardiolipinas negativo). Como único factor de hipercoagulabilidad que se documenta es el consumo de un anticonceptivo oral que contenía drospirenona y etinilestradiol desde un año atrás. La paciente fue anticoagulada con enoxaparina y se recuperó sin secuelas y actualmente se encuentra en manejo ambulatorio con warfarina. El uso de anticonceptivos orales en combinación se debe realizar con precaución en pacientes mayores de 35 años, en buena medida por el aumento del riesgo de eventos tromboembólicos asociado al incremento en la síntesis hepática de algunos factores de coagulación. Por lo tanto, éste representa un caso de reacción adversa severa, potencialmente fatal y prevenible(AU)
Assuntos
Humanos , Feminino , Embolia Pulmonar/tratamento farmacológico , Varfarina/uso terapêutico , Anticoncepcionais Orais Combinados/efeitos adversosRESUMO
A case of a 76 year old Colombian patient who developed an episode of postural hypotension, after using 4mg of doxazosin for treatment of benign prostatic hypertrophy (BPH) is presented. Because of his age and severity of symptoms (asthenia, weakness, adynamia), the patient was hospitalized. Changing doxazosin by tamsulosin allowed control of symptoms of BPH with no further episodes of orthostatic hypotension.
Se presenta el caso de un paciente colombiano de 76 años quien sufrió un episodio de hipotensión postural, después de tomar doxazosina de 4 mg para el manejo de la hiperplasia prostática benigna (HPB). Debido a la severidad de los síntomas (astenia, debilidad y adinamia), el paciente fue hospitalizado. El cambio de doxazosina por tamsulosina permitió el control de los síntomas de la HPB sin episodios ulteriores de hipotensión ortostática.
RESUMO
Este es el reporte de un caso clínico de una paciente con diagnóstico de Síndrome de Stevens-Johnson inducido por fenitoína, quien ingresó a un hospital universitario de tercer nivel en la ciudad de Bogotá, Colombia. Trece días después del inicio del medicamento mencionado por un diagnóstico de síndrome convulsivo focal, la paciente consulta por la aparición de lesiones máculo papulares en cabeza y tronco acompañadas de úlceras orales y genitales. La presentación y distribución de las lesiones, el compromiso sistémico y la asociación temporal con el consumo de fenitoína, apoyaron el diagnóstico de Síndrome de Stevens-Johnson, el cual fue confirmado por el Servicio de Dermatología. La paciente respondió adecuadamente al tratamiento instaurado siendo dada de alta 10 días después de su ingreso sin complicaciones.
This is a case report of a female patient with a diagnosis of Stevens-Johnson Syndrome induced by Phenytoin. The patient was admitted to a third level hospital. Thirteen days after she started phenytoin use (prescribed for her focal seizure disorder), she presented some maculo-papular lesions in head and thorax, associated with oral and genital ulcers. Distribution and presentation of lesions, the systemic compromise, associated with the temporary use of Phenytoin, supported the diagnosis of SJS. The diagnosis was confirmed by Dermatology. The patient was treated successfully and she was discharged without complications ten days after her admission.
