After the Second World War, the so-called pharmacological explosion took place, leading to major advances in the treatment of diseases that were once inevitably fatal or disabling.

This pharmacological expansion contributed to the occurrence of catastrophic incidents, such as the phocomelia epidemic attributed to thalidomide. Since then, concerns about drug safety have contributed to the development and application of clinical and epidemiological methods to assess the benefits and potential risks of any type of therapeutic intervention, whether pharmacological or not.¹1 Laporte JR. Principios básicos de investigación clínica. 2nd ed. Barcelona: Astrazéneca; 2001.

Indisputably, the administration of a medication aims to obtain a beneficial effect for those who take it. Nonetheless, it is important that the assumptions arising from the analysis of scientific evidence are not forgotten: firstly, some drugs do not have the desired efficacy, and secondly, regardless of their beneficial effects, every medication may produce undesired effects.

When a drug is launched on the market, all the knowledge about it is based on pre-marketing studies: during the development of the molecule, experimental studies on its effects and toxicity are conducted in animals (pre-clinical studies). If no unacceptable toxic effects are observed, the first clinical trials in humans are conducted. These are termed phase I, II, and III studies, which investigate aspects of the pharmacokinetics, toxicity, and efficacy in humans.

In clinical trials, several factors may interfere with the results, such as inclusion and exclusion criteria, sample sizes, and even “apparently ethical” criteria, which, while fully justified in the early stages of the assessment of a new drug, preclude scientific study in certain populations. For a long time, with some exceptions, children have been excluded from clinical trials. Only in phase IV (post-marketing) are the drugs used in children, which may lead them to become the subjects of uncontrolled clinical practice.¹1 Laporte JR. Principios básicos de investigación clínica. 2nd ed. Barcelona: Astrazéneca; 2001.^,22 Meiners MMMA, Berqsten-Mendes G. Prescrição de medicamentos para crianças hospitalizadas como avaliar a qualidade? Rev Ass Med Bras. 2001;47:332-7.

This practice of pediatric prescription without clinical evidence, in situations that are different from those studied and advocated (indications, dosages, extemporaneous formulations, age group in which tested), is known as off-label use, which has been demonstrated to be associated with an increase in adverse effects³3 Manson J, Pirmohamed M, Nunn T. Off-label and unlicensed medicine use and adverse drug reactions in children: a narrative review of the literature. Eur J Pharmacol. 2012;68:21-8.^–55 Aagaard L, Hansen EH. Prescribing of medicines in the Danish pediatric population outwit the licensed age group: characteristics of adverse drug reactions. Br J Clin Pharmacol. 2011;71:751-7. and should be discouraged.

In this issue of the Revista Paulista de Pediatria, Gonçalves and Heineck conducted a cross-sectional study, with a simple methodology.⁶6 Gonçalves MG, Heineck I. Frequência de prescrições de medicamentos off label e não licenciados para pediatria na atenção primária à saúde em município do sul do Brasil. Rev Paul Pediatr. 2016;34:11-7. In their study, the authors demonstrated that, of the total, 232 (31.7%) prescriptions were off-label, and the following types and frequency were observed: off-label dose – 90 (38.8%); age – 73 (31.5%); and administration frequency – 68 (29.3%). The greatest concern was the finding of overdose of medications whose use in this situation may be fatal, such as salbutamol.

In Brazil, off-label prescription in pediatrics is a frequent practice. Is this practice necessary? What can be done to ensure the safety of children?

In order to protect the health of children and to ensure that medications are used in a more ethical way, in 2007 the European Union issued legislation for the development and authorization of pediatric drugs.⁷7 Noguera VF. Trabajo de Investigación: Análisis descriptivo de los planes de investigación em Pediatria resueltos por la Agencia Europea del Medicamento durante el período 2007-2009, Doctorado em Farmacologia, Universidade Autonoma de Barcelona. Available in: http://ddd.uab.cat/pub/trerecpro/2011/hdl_2072_116979/TR_FerrandoNoguera.pdf
http://ddd.uab.cat/pub/trerecpro/2011/hd... Since then, pharmaceutical companies have been required to develop their medicines both for the adult and pediatric populations, aiming to adapt the drug to the needs, dosage, dosage form, and administration route, among others, in order to ensure effectiveness and that safety is not affected by the risk of overdose. A Pediatric Committee was also created to evaluate the pediatric investigation plans (PIPs) presented by pharmaceutical companies. The committee consists of 12 representatives of the member states; among its functions, the elaboration of an inventory of specific pediatric needs is noteworthy.⁷7 Noguera VF. Trabajo de Investigación: Análisis descriptivo de los planes de investigación em Pediatria resueltos por la Agencia Europea del Medicamento durante el período 2007-2009, Doctorado em Farmacologia, Universidade Autonoma de Barcelona. Available in: http://ddd.uab.cat/pub/trerecpro/2011/hdl_2072_116979/TR_FerrandoNoguera.pdf
http://ddd.uab.cat/pub/trerecpro/2011/hd...

Also in 2007, the World Health Organization (WHO) published the first list of Essential Medicines for Children, which is reviewed every 2 years, and launched the “make medicines child size” campaign, in order to raise awareness and promote a global action on the problem of lack of pediatric formulations.⁸8 Finney E. Children's medicine: a situation analysis [Internet]. WHO; 2011. Available in: http://www.who.int/childmedicines/progress/CM_analysis.pdf
http://www.who.int/childmedicines/progre...

In 2012, under the Investigational New Drug (IND) program, the Food and Drug Administration (FDA), the regulation agency of the United States, created the Safety and Innovation Act (FDASIA-2012), which established the Pediatric Study Plan. This plan is required for new molecules, new indications, new dosage forms, new dosages, and new administration routes.⁹9 https://www.fda.gov/regulatoryinformation/guidances/ucm126486.htm
https://www.fda.gov/regulatoryinformatio... ^,1010 http://www.fda.gov/RegulatoryInformation/Legislation/FederalFoodDrugandCosmeticActFDCAct/SignificantAmendmentstotheFDCAct/FDASIA/
http://www.fda.gov/RegulatoryInformation...

In Brazil, there are isolated initiatives by healthcare institutions that, by standardizing drugs and creating pharmacology committees, among other measures, are able to evaluate the off-label use of drugs. In the state of São Paulo, the Health Surveillance Center (Centro de Vigilância Sanitária [CVS]) acts in the pharmacovigilance area based on the reports of adverse events, publishing Therapeutic Alerts on Pharmacovigilance in the Official Journal. The CVS has recently published two alerts, “Methylphenidate: indications and adverse reactions” (July 2013) and “Risk of pancreatic cancer associated with incretin-based therapy” (February 2014). Both are focused on alerting, following adverse reactions from the off-label use of drugs. The first is widely used in children.¹¹11 São Paulo, Secretaria de Estado da Saúde, Centro de Vigilância Sanitária. Comunicado CVS - Alerta Terapêutico em Farmacovigilância - 01/2014: Risco de Pancreatite e Neoplasia Pancreática associado à terapia baseada nas Incretinas. Available in: http://www.cvs.saude.sp.gov.br/zip/ALERTA%2001_2014_Incretinas_sem_bandeirola.pdf
http://www.cvs.saude.sp.gov.br/zip/ALERT... ^,1212 São Paulo, Secretaria de Estado da Saúde, Centro de Vigilância Sanitária. Comunicado CVS – 45 – Divulgação do Alerta Terapêutico em Farmacovigilância 01/2013 – Metilfenidato – Indicações Terapêuticas e Reações Adversas. Available in: http://www.cvs.saude.sp.gov.br/zip/ALERTA%20TERAP%C3%8AUTICO%2010%20Metilfenidato_010813_final.pdf
http://www.cvs.saude.sp.gov.br/zip/ALERT... At the federal level, the Collegiate Board Resolution (Resolução da Diretoria Colegiada [RDC]) No. 9, of 20 February 2015, which aims to establish the procedures and requirements for the conduction of clinical drug trials, indicated that post-marketing clinical trials are subject only to the Notification of Clinical Trial.¹³13 Brasil, Ministério da Saúde, Agência Nacional de Vigilância Sanitária, Resolução da Diretoria Colegiada – RDC N° 9, de 20 de fevereiro de 2015, que tem por objetivo definir procedimentos e requisitos para realização de ensaios clínicos com medicamentos. Available in: http://portal.anvisa.gov.br/wps/wcm/connect/c3dc820047823081b0a7fbfe096a5d32/RDC+9-2015.pdf?MOD=AJPERES
hhttp://portal.anvisa.gov.br/wps/wcm/con...

Above all, to foster ethical off-label drug use, it is necessary that this exceptional use is clinically justified, even if it is accompanied by clarification and consent of the parents or guardians.¹⁴14 Brasil, Ministério da Saúde. CONITEC no SUS Secretaria de Ciência, Tecnologia e Insumos Humanos Estratégicos. Uso off label: erro ou necessidade? Rev Saúde Pública. 2012;46:398-9. This measure can be taken by healthcare facilities. The Brazilian National Health Surveillance Agency (Agência Nacional de Vigilância Sanitária [Anvisa]), following the example of the regulatory body of the European Union, should establish criteria and standards that stimulate comparative studies and demonstrate the efficacy and safety of medication use in children. When promising, therapies should be tested in controlled clinical trials and their package inserts should be reformulated.

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