Daniela Rezende Garcia Junqueira
University of Sydney
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Revista Da Associacao Medica Brasileira | 2013
Daniela Rezende Garcia Junqueira; Maria das Graças Carvalho; Edson Perini
Heparin is a natural agent with antithrombotic action, commercially available for therapeutic use as unfractionated heparin and low molecular weight heparin. Heparin-induced thrombocytopenia (HIT) is a serious adverse reaction to heparin that promotes antibody-mediated platelet activation. HIT is defined as a relative reduction in platelet count of 50% (even when the platelet count at its lowest level is above>150 x 10(9)/L) occurring within five to 14 days after initiation of the therapy. Thrombocytopenia is the main feature that directs the clinical suspicion of the reaction and the increased risk of thromboembolic complications is the most important and paradoxical consequence. The diagnosis is a delicate issue, and requires a combination of clinical probability and laboratory tests for the detection of platelet activation induced by HIT antibodies. The absolute risk of HIT has been estimated between 1% and 5% under treatment with unfractionated heparin, and less than 1% with low molecular weight heparin. However, high-quality evidence about the risk of HIT from randomized clinical trials is scarce. In addition, information on the frequency of HIT in developing countries is not widely available. This review aims to provide a better understanding of the key features of this reaction and updated information on its frequency to health professionals and other interested parties. Knowledge, familiarity, and access to therapeutic options for the treatment of this adverse reaction are mandatory to minimize the associated risks, improving patient safety.
European Journal of Pain | 2014
Daniela Rezende Garcia Junqueira; Manuela L. Ferreira; Kathryn M. Refshauge; Christopher G. Maher; John L. Hopper; Mark J. Hancock; M.G. Carvalho; Paulo H. Ferreira
Heritability and population‐specific lifestyle factors are considered to significantly contribute to chronic low back pain (LBP), but traditional population studies fail to (1) adjust for genetics; and (2) use standard and validated definitions for LBP and for lifestyle factors.
Revista De Saude Publica | 2014
Edson Perini; Daniela Rezende Garcia Junqueira; Lorena Gomes Cunha Lana; Tatiana Chama Borges Luz
OBJECTIVE To analyze the patterns and legal requirements of methylphenidate consumption. METHODS We conducted a cross-sectional study of the data from prescription notification forms and balance lists of drugs sales – psychoactive and others – subject to special control in the fifth largest city of Brazil, in 2006. We determined the defined and prescribed daily doses, the average prescription and dispensation periods, and the regional sales distribution in the municipality. In addition, we estimated the costs of drug acquisition and analyzed the individual drug consumption profile using the Lorenz curve. RESULTS The balance lists data covered all notified sales of the drug while data from prescription notification forms covered 50.6% of the pharmacies that sold it, including those with the highest sales volumes. Total methylphenidate consumption was 0.37 DDD/1,000 inhabitants/day. Sales were concentrated in more developed areas, and regular-release tablets were the most commonly prescribed pharmaceutical formulation. In some regions of the city, approximately 20.0% of the prescriptions and dispensation exceeded 30 mg/day and 30 days of treatment. CONCLUSIONS Methylphenidate was widely consumed in the municipality and mainly in the most developed areas. Of note, the consumption of formulations with the higher abuse risk was the most predominant. Both its prescription and dispensation contrasted with current pharmacotherapeutic recommendations and legal requirements. Therefore, the commercialization of methylphenidate should be monitored more closely, and its use in the treatment of behavioral changes of psychological disorders needs to be discussed in detail, in line with the concepts of the quality use of medicines.
BMJ Open | 2014
Lorena Gomes Cunha Lana; Daniela Rezende Garcia Junqueira; Edson Perini; Cristiane Menezes de Pádua
Introduction Lipodystrophy is a frequent and disfiguring adverse effect of antiretroviral therapy (ART) in patients with HIV. It affects the quality of life of the patient and adherence to treatment, and generates new needs for comprehensive healthcare services. The aim of this study will be to conduct a systematic review of the literature from observational studies and describe lipodystrophy among patients with HIV infection during current or previous use of ART. Methods and analysis A systematic review of observational studies published in MEDLINE, CINAHL, LILACS, EMBASE and International Pharmaceutical Abstracts will be carried out. Citations of included studies will be checked to identify additional studies not identified in the electronic searches. It will include any observational study that considered lipodystrophy as the primary or secondary outcome and that had enrolled adolescent and adult patients with HIV infection who were on current or previous ART for at least 6 months. Data extraction and analysis will be performed independently by two reviewers. The extracted data will be discussed, decisions documented and, where necessary, the authors of the studies will be contacted for clarification. Measures of frequency, prevalence and incidence of lipodystrophy will be stratified according to definition, method of diagnosis and risk factors of the outcome. Ethics and dissemination Ethics is not required given this is a protocol for a systematic review. The findings of this study will be widely disseminated through peer-reviewed publications and conference presentations. Updates of the review will be conducted to inform and guide healthcare practice. Protocol registration PROSPERO—42013005450.
Cochrane Database of Systematic Reviews | 2017
Daniela Rezende Garcia Junqueira; Liliane Zorzela; Edson Perini
European Spine Journal | 2014
Markus Hübscher; Manuela L. Ferreira; Daniela Rezende Garcia Junqueira; Kathryn M. Refshauge; Christopher G. Maher; John L. Hopper; Paulo H. Ferreira
Twin Research and Human Genetics | 2016
Paulo H. Ferreira; Vinicius C. Oliveira; Daniela Rezende Garcia Junqueira; Lígia C. Cisneros; Lucas C. Ferreira; Kate T. Murphy; Juan R. Ordoñana; John L. Hopper; Luci Fuscaldi Teixeira-Salmela
Archive | 2017
Túlio Pinho Navarro; Alan Dardik; Daniela Rezende Garcia Junqueira; Ligia de Loiola Cisneros
Archive | 2017
Túlio Pinho Navarro; Alan Dardik; Daniela Rezende Garcia Junqueira; Ligia de Loiola Cisneros
XIII International Back Pain Forum | 2014
Daniela Rezende Garcia Junqueira; Manuela L Ferreira; K. M. Refshauge; C. G. Maher; John L. Hopper; Mark J. Hancock; Paulo H. Ferreira