ABSTRACT
The objective of this study was to identify drugs that received dose adjustments (DA) and pharmaceutical alternatives (PA) that avoid DA, and calculate the economic percentage of this replacement. A descriptive, observational and cross-sectional study was performed in a second level hospital. The pharmacy and nursing services was accompanied to identify the drugs that received DA and the compounding techniques. After identifying all the drugs that received DA, was identified in the Brazilian market the corresponding pharmaceutical alternative, with the Drugs Price List of Brazilian Health Regulatory Agency. For those drugs that was not available any PA, was performed a research of studies that describe compounding techniques in international scientific databases. Was identify 88 drugs that received DA, and these, 50 do not have any PA. Were identified compounding techniques to 40 drugs. Although any drug has your own particularity of compounding, the compounding techniques can be grouped in five categories. The standardization of 29 drugs can reduce in 28% the DA procedure and cost saving of 34,85%/month. We can conclude that every three drugs prescribed, one received DA and every three DA, one can be avoided by the selection of 29 PA, saving cost as well. The use and standardization of five techniques would attend the pharmaceutics recommendations for better dissolution, bioavailability and patient safety.
Uniterms:
Pharmaceutical preparations/hospitals; Patient safety; Pharmacoeconomics; Drugs/descritive study/ Off-Label Use.
INTRODUCTION
Dose adjustment (DA) is performed to supply a patient's therapeutic needs when non-standard dosages are needed (Brasil, 2007; FDA, 2013). The lack of liquid pharmaceutical forms for oral use on the market has become a problem for the pharmacotherapy of patients that primarily uses liquid formulations, such as pediatric patients, the elderly, patients receiving drugs via probe, patients with dysphagia, and patients with dementias, Parkinson's, or Alzheimer's disease (Haywood, Glass, 2013HAYWOOD, A.; GLASS, B.D. Liquid Dosage Forms Extemporaneously Prepared from Commercially Available Products - Considering New Evidence on Stability. J. Pharm. Pharm. Sci., v.16, n.3, p. 441-55, 2013. ; Thombre, Berchielli, Rogers, 2014THOMBRE, A.G.; BERCHIELLI, A; ROGERS, J. F. Extemporaneously prepared controlled release formulations for accelerating the early phase development of drug candidates. Drug Discov. Today, v.19, n.5, p.694-700, 2014. ). Patients with these problems require extemporaneous oral preparations in order to ensure the patient's therapy. DA is common in health systems; however, there are no guarantees regarding the quality, effectiveness, and safety of drugs after DA and DA can expose the patient to adverse events (Glass, Haywood, 2006).
With the aim of ensuring the pharmacotherapy of the patient, contributing to the culture of patient safety, and objectively identifying drugs that underwent DA and pharmaceutical alternatives (PAs) that could avoid DA, we compared DA to the compounding techniques described in the literature and calculated the economy of PAs.
METHODS
Study design
This was a pharmaco-epidemiological, descriptive, and observational cross-sectional study based on the guideline Strengthening the Reporting of Observational studies in Epidemiology (STROBE) (Von Elm et al., 2008).
Study site
This study was conducted at the State Hospital Américo Brasiliense (HEAB) in Américo Brasiliense, São Paulo state. The hospital assists patients from 24 cities in the region.
Study period
Patient prescriptions were monitored in July 2013.
Data collect
Patient prescriptions were monitored daily. The nursing staff's work was monitored to check the drug manipulation techniques, administration, and storage after DA. The PAs and the costs were identified in the Brazilian market with the Drugs Price List of ANVISA (ANVISA, 2015). The DAs were classified into derivation or subdivision of the pharmaceutical form, according to the current legislation (Brasil, 2007). For those drugs without available PAs, studies that describe compounding techniques were studied, using the descriptors: "Drug name" - for each drug; "Drug Compounding"; "Drug Stability"; and "Pharmaceutical Preparations" in the databases LILACS, SciELO, and PubMed.
Ethical considerations
The study was approved by the ethics committee of the Institute Lauro de Souza Lima as the project "Proposta de implantação de um serviço de farmacovigilância no Hospital Estadual de Américo Brasiliense" under protocol E-015/10; it was also approved by the hospital board.
RESULTS
DA was identified in 88 (34.7%) different drugs of the 253 standardized drugs in the hospital pharmacy (Figure 1). The technique of derivation was standardized and described in the standard operating procedure as crushing the solid dosage form with the aid of a pestle, followed by immediate administration. The subdivision of the pharmaceutical form occurred in the hospital pharmacy and was performed by the pharmacy team. The subdivision technique used specialized equipment for this purpose, followed by packing and labeling with product information, including the active ingredient, expiry date, and batch number. Subdivisions of liquid dosage forms occurred in the ward in drug handling rooms by the nursing team. Only a portion of the ampoule contents were administered, corresponding to the desired concentration. No DA exceeded the shelf life of 48 hours.
Flowchart analysis of prescriptions of hospitalized patients, identification of dose adjustments, and pharmaceutical alternatives in the Brazilian market and the compounding techniques available in the literature.
In the Brazilian market, 29 PAs were identified for the 88 drugs that received DA, possibly decreasing DAs by 28.5% (856 / 2,998) (Table I).
For the 50 drugs that lacked PAs, 40 had known compounding techniques (Table II); the following ten drugs (or drug combinations) had no published compounding techniques: bisacodyl; citalopram; a combined dose of rifampicin, isoniazid, pyrazinamide, and ethambutol; doxazosin; finasteride; isosorbide; ivermectin; paracetamol and codeine combined; quetiapine; and sertraline.
Regarding the microbiological quality, studies show the necessity of adding parabens, such as methylparaben and propylparaben, in the extemporaneous formulations and refrigerated storage to avoid microbiological growth (OPAS, 1997; Haywood, Glass, 2013HAYWOOD, A.; GLASS, B.D. Liquid Dosage Forms Extemporaneously Prepared from Commercially Available Products - Considering New Evidence on Stability. J. Pharm. Pharm. Sci., v.16, n.3, p. 441-55, 2013. ; Alemón-Medina et al.,, 2014).
Furthermore, the hospital spent US$ 3,458.39 on performing DA. The economic analysis was calculated through the difference between the sum of DA (considering the frequency and cost for dosage form unity for each drug - for solid drugs, it was considered one tablet or capsule, and for liquid drugs, one milliliter) and the sum of the corresponding PA dosage (Table 1).
Through economic analysis, standardizing PAs could generate a cost savings of US$ 1,205.59. Only one drug (piperacilin + tazobactam powder for injection 4 g + 0.5 g) is responsible for US$ 1,190.41 of this cost savings.
DISCUSSION
DA is an indispensable practice in hospitals because many patients often have specific needs that require the administration of drugs in various dosage forms (Haywood, Glass, 2013HAYWOOD, A.; GLASS, B.D. Liquid Dosage Forms Extemporaneously Prepared from Commercially Available Products - Considering New Evidence on Stability. J. Pharm. Pharm. Sci., v.16, n.3, p. 441-55, 2013. ; Thombre, Berchielli, Rogers, 2014THOMBRE, A.G.; BERCHIELLI, A; ROGERS, J. F. Extemporaneously prepared controlled release formulations for accelerating the early phase development of drug candidates. Drug Discov. Today, v.19, n.5, p.694-700, 2014. ).
Generally, these patients are those who make use of catheters, have dysphagia, and/or require different doses of commercialized drugs. Therefore, of every four hospitalized patients, three patients require at least one PA to one or more prescribed drugs; however, the standardization of 29 PAs may reduce DA practices by one-third.
Nevertheless, the Pan American Health Organization/World Health Organization recommends preparing reduced therapeutic forms in order to facilitate the logistics (acquisition, storage, and distribution) of drugs, promoting the drug's rational use, avoiding duplication and saving money by avoiding waste (OPAS, 1997).
On the other hand, ensuring the safety, efficacy, and quality of pharmaceutical forms is given by the pre-registration of drugs through stability studies (short and long), pharmaceutical equivalence studies, such as dissolution profiles and other pharmacopoeia analysis, and in vitro studies of bioequivalence aspects (Mastroianni, Lucchetta, 2011MASTROIANNI, P.C.; LUCCHETTA, R.C. Regulamentação sanitária de medicamentos. Rev. Ciênc. Farm. Bás. Aplic., v.32, n.1, p.127-132, 2011. ). These issues are no longer guaranteed after DA.
In addition, it is recommended that therapeutic forms be updated every two years, not just for the inclusion or exclusion of drugs, but also to review the submissions to ensure the best posology for the patient profile (OPAS, 1997). Once the drugs were available to patients in the most appropriate pharmaceutical form and without manipulation (Catalán et al., 2001CATALÁN, E.; PADILLA, F.; HERVÁS, F.; PÉREZ, M.A.; RUIZ, F. Fármacos orales que no deben ser triturados. Enferm. Intens., v.12, n.3, p.146-150, 2001.; Habib et al., 2014HABIB, W.A.; ALANIZI, A.S.; ABDELHAMID, M.M.; ALANIZI, F.K. Accuracy of tablet splitting: Comparison study between hand splitting and tablet cutter. Saudi Pharm.. J., v.22, n.5, p.454-459, 2014. ), patients would not be exposed to the inherent risks of DA (Paparella, 2010PAPARELLA, S. Identified safety risks with splitting and crushing oral drugs. J. Emerg. Nurs., v.36, n.2, p.156-158, 2010. ); this would also decrease costs.
Therefore, the data from this study highlight the importance of continuous expansion and revision of therapeutic forms, considering not only the managerial and administrative aspects of hospital pharmacy (selection, acquisition, and distribution of drugs), but also the management of patient safety at the institution.
For those drugs that do not have available commercial alternatives, DA is often inevitable. Every DA is considered off-label use, because it is a manipulation and formulation of extemporaneous doses from the marketed drugs (Kairuz et al., 2007KAIRUZ, T.E.; GARGIULO, D.; BUNT, C.; GARG, S. Quality, Safety and Efficacy in the "Off-Label" use of medicines. Curr. Drug Saf., v.2, n.1, p.89-95, 2007.. ; ANVISA, 2010; EMA, 2014MA, C.; DECARIE, D.; ENSOM, M.H. Stability of clonidine suspension in oral plastic syringes. Am. J. Health-Syst. Pharm., v.71, n.15, p.657-661, 2014. ; Carvalho, 2016CARVALHO, M.L. Challenges on off label medicine use. Rev. Paulista Ped., v.34, n.1, p.1-2, 2016. ); therefore, DA should be discussed by the health team and be provided in the clinical protocols of the service.
Additionally, it was observed that derivation is standardized in the hospital and was based on the tablet dispersion technique, respecting the period of lateness (48 hours) set by ANVISA (Brasil, 2007), showing conformity (Glass, Haywood, 2006GLASS, B.D.; HAYWOOD, A. Stability considerations in liquid dosage forms extemporaneously prepared from commercially available products. J. Pharm. Pharmac. Sci., v.9, n.3, p.398-426, 2006. ). However, studies (Allen, 2012ALLEN, L.V. Losartan Potassium 2.5 mg/mL Oral Suspension. U.S. Pharm., v.37, n.9, p.46-47, 2012.; Alemón-Medina et al., 2014; Shoosanglertwijit et al., 2015) demonstrate that the validity of the PA is often greater than seven days, under certain criteria for manipulation and storage.
Glass and Haywood (Glass, Haywood, 2006GLASS, B.D.; HAYWOOD, A. Stability considerations in liquid dosage forms extemporaneously prepared from commercially available products. J. Pharm. Pharmac. Sci., v.9, n.3, p.398-426, 2006. ) suggest a decision-flow for choosing the DA procedure. If there is need for an extemporaneous preparation of liquid, one must seek a commercially available alternative to avoid the DA. If none are available, the second option would be to search for a therapeutic equivalent. If there is no therapeutic equivalent with the same efficacy and safety, the third option would be the preparation of an extemporaneous solution, according to the pharmacopoeia. When lacking the monograph of preparation, it is recommended to research a validated formulation. Without this, the literature should be used to find DA techniques specific to the drug. In a final decision, the standardized tablet dispersion technique should be used.
The advantage of technique standardization, as found in the literature review, is that it increases the stability of extemporaneous solutions and improves the dissolution of the drugs, thereby ensuring greater bioavailability and absorption, ensuring therapeutic effectiveness, and preventing adverse drug events. Moreover, changes in drug dosage forms can lead to changes in the polymorphic and morphological behaviors of drugs, which may cause therapeutic ineffectiveness, because while medicines are produced and stored, they tend to seek the most stable form, which is not always the more active and safe form (Glass, Haywood, 2006GLASS, B.D.; HAYWOOD, A. Stability considerations in liquid dosage forms extemporaneously prepared from commercially available products. J. Pharm. Pharmac. Sci., v.9, n.3, p.398-426, 2006. ; Capucho, Mastroianni, Cuffini, 2008CAPUCHO, H.C.; MASTROIANNI, P.C.; CUFFINI, S. Farmacovigilância no Brasil: a relação entre polimorfismo de fármaco, efetividade e segurança dos medicamentos. Rev. Ciênc. Farm. Bás. Aplic., v.29, n.3, p.277-283, 2008.; Paparella, 2010PAPARELLA, S. Identified safety risks with splitting and crushing oral drugs. J. Emerg. Nurs., v.36, n.2, p.156-158, 2010. ; Glass, Haywood, 2013).
The techniques found for the production of extemporaneous solutions are generally characterized by choosing the most appropriate vehicle (water or simple syrup) and the addition of pharmaceutical adjuvants, such as those used for suspending, thickening, binding, and acidifying. Other commercial alternatives, such as galenical bases, could be used to prepare extemporaneous solutions. This option for the preparation of DA, in order to ensure the quality of freshly-prepared solution and promote increased patient safety, will require periodic review.
A limitation of the study was the data collection time, a month, which can be a limitation for DA frequency analysis; however, the analysis period was not qualitatively limiting to identify the drugs that received DA, and other studies showed similar numbers of patients and prescriptions analyzed (Joosub et al., 2015JOOSUB, I.; GRAY, A.; CRISOSTOMO, A.; SALAM, A. Cost-minimization analysis of imipenem/cilastatin versus meropenem in moderate to severe infections at a tertiary care hospital in Saudi Arabia. Saudi Pharm. J., v.23, n.6, p.626-632, 2015. ; Mahmood et al., 2016MAHMOOD, A.; ELNOUR, A.A.; ALI, A.A.A.; HASSAN, N.A.G.M.; SHEHAB A.; BHAGAVATHULA, A.S. Evaluation of rational use of medicines (RUM) in four government hospital in UAE. Saudi Pharmac. J., v.24, n.2, p.189-196, 2016. ). We believed that many of the 88 different drugs undergo DA in other hospitals, and the 40 techniques described in the literature may contribute to the stability, safety, and quality of such preparations.
Thus, data from this study suggest the need to change the selection process and standardization of drugs and the need for cost-effectiveness and cost-benefit studies to evaluate the effectiveness and safety of DA.
These data close a gap in the literature, contributing to our understanding of the inherent risks of DA and identifying potential cost savings.
For every three dispensed drugs, one received DA, and three of every four patients needed at least one of their drugs to undergo DA in their drug therapy, highlighting the importance and relevance of this practice in hospitals. Furthermore, for every three DA, one could be avoided with the selection of a PA. Each drug has its peculiarities for ensuring dissolution, bioavailability, and absorption of the drugs, consequently promoting safe and effective pharmacotherapy.
Therefore, data from this study corroborate the need for cost-benefit studies to evaluate the effectiveness, safety, and economy generated by the DA process.
ACKNOWLEDGMENTS
We thank the State Hospital of Américo Brasiliense for supporting this study.
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FINANCIAL SUPPORT
This study was supported by the Program of Support for Scientific Development at the Faculty of Pharmaceutical Sciences at the Universidade Estadual Paulista "Júlio de Mesquita Filho" (PADC).
Publication Dates
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Publication in this collection
Sept 2016
History
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Received
06 Oct 2015 -
Accepted
25 Aug 2016