Tratamiento psicofarmacológico de la esquizofrenia en la población infantojuvenil: estado del arte.

La esquizofrenia es una patología crónica y grave que se caracteriza por la presencia de delirios, alucinaciones, síntomas negativos, desorganización del pensamiento y del comportamiento. Si  bien su prevalencia en menores de 13 años es muy baja, aumenta sustancialmente durante la adolescencia. Cuando se desarrolla antes de los 18 años se denomina esquizofrenia de inicio precoz y representa del 12 al 33 % del total de los individuos con este trastorno. Existen fármacos como el haloperidol, risperidona, paliperidona, aripiprazol, olanzapina, quetiapina, brexpiprazol y lurasidona aprobados por la Food and Drug Administration (FDA) para el tratamiento de la esquizofrenia en adolescentes. Sin embargo, a excepción del haloperidol, todas las indicaciones farmacológicas que se realizan para tratar este trastorno en menores de 13 años resultan "off label" (fuera de las indicaciones de la ficha técnica). Si bien esta práctica no se encuentra prohibida, conlleva riesgos adicionales. En el siguiente trabajo se revisará la evidencia disponible acerca del uso de los antipsicóticos para el tratamiento de la esquizofrenia en la población infantojuvenil, con el objetivo de realizar una síntesis de la información con aplicabilidad clínica.

Off-label prescriptions in child and adolescent psychiatry. Why, when and how? / Prescripciones off-label en psiquiatría infanto-juvenil. ¿Por qué, cuándo y cómo?

In the paediatric population, paticulary in the field of child and adolescent psychiatry, off-label indications are the rule rather than the exception. This may occur when a drug is indicated for a pathology, age, route of administration or treatment length other than those described in the product label. Argentina, unlike other countries, has no explicit regulation on off-label prescribing. Therefore, the prescription of a medicine in a manner different from that approved by the National Administration of Medicines, Food and Medical Technology (ANMAT) does not have a regulatory framework regarding the conditions that must be met at the time of treatment. Although off-label use is not prohibited, it carries an additional risk. In order to encourage research in paediatrics, regulatory agencies such as the Food and Drug Administration (FDA) and the European Medicines Agency (EMA) have introduced legislative reform. The following paper will review the current framework of the regulatory agencies that are relevant to the paediatric population and will analyse criteria to guide physicians in the rational use of off-label pharmacotherapy.

En la población pediátrica y particularmente en el ámbito de la psiquiatría infanto-juvenil, las indicaciones off-label representan una regla más que una excepción. Esta práctica puede ocurrir cuando un fármaco se indica en una patología, rango terapéutico, edad, vía de administración o duración distinta a las que se describen en el prospecto. Argentina, a diferencia de otros países, no tiene una regulación expresa en relación a la prescripción off-label. Por lo tanto, la indicación de un medicamento de manera diferente a la aprobada por la Administración Nacional de Medicamentos, Alimentos y Tecnología Médica (ANMAT) no posee un marco normativo en lo referente a las condiciones que deben ser cumplidas al momento de ese acto médico. Si bien el uso off-label no se encuentra prohibido, conlleva un riesgo adicional. Con el objetivo de fomentar la investigación en pediatría, las agencias reguladoras como la Food and Drug Administration (FDA) y la European Medicines Agency (EMA) han introducido reformas legislativas. En el siguiente trabajo se revisarán las normativas vigentes de las agencias reguladores que competen a la población pediátrica y se analizarán criterios que orienten al médico al uso racional de la farmacoterapia off-label.

Risperidone inhibits contractions induced by serotonin and histamine and reduces K+ currents in smooth muscle of human umbilical artery.

Risperidone is an antipsychotic commonly used during pregnancy. Because it can cross the placental barrier, our objective was to evaluate its actions on the smooth muscle of the human umbilical artery (HUA). Risperidone preincubation (1-300 nmol/L for 20 minutes) produced a significant decrease in maximum force development induced by serotonin or histamine in HUA rings. When applied on top of stable contractions induced by these agonists risperidone produced quick relaxations (IC(50) = 1 nmol/L for serotonin and 72 nmol/L for histamine). Risperidone induced the contraction of vascular rings depolarized by 40 mmol/L extracellular K(+) but not in the case of 80 mmol/L K(+), suggesting inhibition of K(+) channels. The patch-clamp technique showed that risperidone (3 nmol/L) inhibited whole-cell K(+) currents in freshly isolated HUA smooth muscle cells. Our results are the first showing risperidone effects in human vascular smooth muscle and highlight that its use during pregnancy should be adequately monitored.

Effects of light ethanol consumption during pregnancy: increased frequency of minor anomalies in the newborn and altered contractility of umbilical cord artery.

This study explores the effects of light maternal ethanol consumption during pregnancy on the appearance of minor malformations in neonates as well as on the contractile properties of their umbilical cord arteries (UCAs). Clinical external findings of newborns of women declaring light ethanol consumption during any period of their pregnancies [ethanol-exposed group (E group), n=79] were compared with those of nonexposed mothers [nonexposed to ethanol group (NE group), n=100]. Women who smoked or had any associated pathology were excluded. E group mothers consumed, on average, 200-250 mL ethanol/trimester (upper limit 700 mL/trimester). Sixty-six percent of the neonates in the E group presented at least one minor malformation (retromicrognathia and minor anomalies of the auricular/preauricular area were the more common), whereas only 16% of the NE group did (p=0.0000). The percentage of children exhibiting Apgar scores <7 was significantly greater in the E group (11% versus 2%, p=0.0119). UCAs from the E group developed significantly less contractile force (p<0.05) than those of the NE group when exposed to 1 microM serotonin (5-HT) or to a high K+ depolarizing solution. This difference persisted after inhibition of endothelial release of nitric oxide (NO) and prostacyclin. In conclusion, even light drinking should be considered a risk during pregnancy.