A review of methods used in assessing non-serious adverse drug events in observational studies among type 2 diabetes mellitus patients

Hakobyan, Liana; Haaijer‐Ruskamp, Flora; Zeeuw, Dick de; Dobre, Daniela; Denig, Petra

doi:10.1186/1477-7525-9-83

Cited by 25 publications

(29 citation statements)

References 89 publications

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“…The favourable safety profile of EPs 7630 is underlined by the fact that no SADRs were reported in this large patient population. AE rates under EPs 7630 were generally somewhat higher in randomised, controlled studies as compared to post-marketing surveillance and open outcomes studies, but this was to be expected which is in line with current literature surveys and reviews [41,42]. In the 19 double-blind, randomized, placebo-controlled trials covered by our review, AEs observed under EPs 7630 and placebo were similar with regard to type and incidence for the majority of system groups or symptoms.…”

Section: Discussionsupporting

confidence: 88%

Safety and Tolerability of EPs 7630 in Clinical Trials

Kamin¹

2013

Adv Pharmacoepidem Drug Safety

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Herbal medicines play an increasingly important role in the perception of physicians and patients looking for equally effective, albeit safer approaches to conventional management of certain diseases. The controversy surrounding effective management regimes for respiratory tract infections (RTI) has made many healthcare providers reconsider current therapeutic strategies.This review presenting the available evidence from clinical trials and non-interventional studies on the safety and tolerability profile of EPs 7630 is based on publications and study reports of 29 clinical trials and post-marketing surveillance studies completed by February 2010. It includes study data from 10,026 adults and children suffering from acute or chronic RTI such as acute tonsillopharyngitis, rhinopharyngitis, sinusitis, bronchitis, or COPD and from 31 healthy subjects.In 19 double-blind, placebo-controlled trials, the type and incidence rate of adverse events under EPs 7630 were similar to those in patients treated with placebo. For gastrointestinal complaints and epistaxis, event rate differences of 2.9% and of 0.6% against EPs 7630 were determined; hypersensitivity reactions and all other system groups showed rate differences <0.5%. For liver associated events, rate differences of 0.0% for all events and of 0.1% for potentially related events were observed. Patients treated with EPs 7630 did not exhibit increased liver enzyme or bilirubin values -neither in terms of a shift in the mean, nor according to individual deviations from the reference ranges. These findings were fully supported by the data from the post-marketing surveillance studies reviewed.EPs 7630 appears to be a well-tolerated herbal medicine in the management of RTI in adults and children alike. Evidence for hepatotoxic effects in humans during routine administration was neither provided in the literature, nor by our own analyses. its isolated constituents have demonstrated pharmacological activities including moderate direct antibacterial and antiviral action and notable immune-modulatory capabilities: immune-modulatory activities are mediated mainly by the release of tumour necrosis factor α and nitric oxides, the stimulation of interferon β, and an increase in natural killer cell activity [5][6][7][8]; further biological activities in vitro are improved phagocytosis, oxidative burst and intracellular killing by human peripheral blood phagocytes, and inhibition of interaction between group-A-streptococci and host epithelia [9,10]. Safety and Tolerability of EPs 7630 in Clinical TrialsSeveral open-label and randomised double-blind clinical studies have been published over the last years in the indications of tonsillopharyngitis, bronchitis and sinusitis [11][12][13][14][15][16][17][18][19][20][21][22][23][24][25][26][27][28][29][30]. While systematic reviews and meta-analyses of EPs 7630 for acute bronchitis and RTI [31,32] This review adds to these findings by providing the first overview of safety and tolerability of EPs 7630 based on publications and st...

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Section: Discussionsupporting

confidence: 88%

Safety and Tolerability of EPs 7630 in Clinical Trials

Kamin¹

2013

Adv Pharmacoepidem Drug Safety

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“…The probability of drug-related symptoms occurring can be derived from the frequencies for the side effects as given in the SPCs. However, the information in the SPC is based on clinical trials in specific patient populations with a short follow-up period, and thus may differ from frequencies in clinical practice [37, 38]. These differences may explain why muscle pain in statin users is more frequently reported in clinical practice than that in the SPCs.…”

Section: Discussionmentioning

confidence: 99%

Evaluation of Potentially Drug-Related Patient-Reported Common Symptoms Assessed During Clinical Medication Reviews: A Cross-Sectional Observational Study

Schoenmakers¹,

Teichert

Wensing

et al. 2017

Drug Saf

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IntroductionHealthcare professionals tend to consider common non-alarming drug-related symptoms to be of little clinical relevance. However, such symptoms can have a substantial impact on the individual patient. Insight into patient-reported symptoms could aid pharmacists to identify improvements in medication treatment, for instance in the patient interview at the start of a clinical medication review (CMR).ObjectiveThe objectives of this study were to describe the numbers and types of patient-reported symptoms assessed during a CMR and to elucidate their potential association with the drugs in use.MethodsThis observational study was performed using data from a clinical trial on patient-reported outcomes of CMRs. Patients taking at least five drugs and who were eligible for a CMR were selected by 15 community pharmacies. Patients were asked to fill in a structured instrument, the Patient Reported Outcome Measure, Inquiry into Side Effects (PROMISE). Among other domains, this instrument offers a list of 22 symptom categories to report symptoms and their relationship with the drugs in use. The results of the PROMISE instrument together with information on patients’ actual drug use were available for analysis. Besides descriptive analysis, associations with side effects as listed in the summary of product characteristics (SPC) of the drugs in use were assessed with logistic regression analysis.ResultsOf the 180 patients included, 168 patients (93.3%) reported at least one symptom via the PROMISE instrument, which could be discussed with the pharmacist during the patient interview. In total, the patients reported 1102 symptoms in 22 symptom categories. Of these patients, 101 (56.1%) assumed that at one or more of the symptoms experienced were related to the drugs in use and 107 (59.4%) reported at least one symptom that corresponded to a ‘very common’ side effect listed in the SPC of a drug in use. Each additional drug in use with a specific symptom listed as a ‘very common’ side effect in its SPC statistically significantly increased the probability of a patient reporting the symptoms of ‘dry mouth/thirst, mouth complaints’, ‘constipation’, ‘diarrhoea’ and ‘sweating’.ConclusionMany patient-reported symptoms and symptoms potentially related to drugs in use were identified by administering the PROMISE instrument to users of at least five drugs being taking long-term. This information can be used in CMRs to improve patients’ drug therapy.Electronic supplementary materialThe online version of this article (doi:10.1007/s40264-017-0504-7) contains supplementary material, which is available to authorized users.

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“…Patient self-reports of adverse drug events (ADEs) are an important additional source of information on the safety of drugs because they differ from healthcare professional reports [2][3][4][5][6][7]. Healthcare professionals often underestimate symptomatic ADEs experienced by patients [7,8]. The added value of patient reports is acknowledged by the Food and Drug Administration (FDA) as well as the European Medicines Agency [9,10].…”

Section: Introductionmentioning

confidence: 99%

Development and Initial Validation of a Patient-Reported Adverse Drug Event Questionnaire

et al. 2013

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Background Direct patient reporting of adverse drug events (ADEs) is relevant for the evaluation of drug safety. To collect such data in clinical trials and postmarketing studies, a valid questionnaire is needed that can measure all possible ADEs experienced by patients. Objective Our aim was to develop and test a generic questionnaire to identify ADEs and quantify their nature and causality as reported by patients. Methods We created a draft list of common ADEs in layterms, which were classified in body categories and mapped to the Medical Dictionary for Regulatory Activities (MedDRA Ò ) terminology. Questions about the nature and causality were derived from existing questionnaires and causality scales. Content validity was tested through cognitive debriefing, revising the questionnaire in an iterative process. Feasibility and reliability were assessed using a Web-based version of the questionnaire. Patients received the questionnaire twice. Feasibility was assessed by the reported time needed for completion and ease of use. Reliability was calculated using Cohen's kappa and proportion of positive agreement (PPA) on: (1) any ADE at patient level; (2) similar ADEs at MedDRA Ò System Organ Class level; and (3) the same ADE at ADE-specific level.Results In the development phase, 28 patients with type 2 diabetes or asthma/chronic obstructive pulmonary disease (COPD) participated. Questions and answer options were rephrased, layout was improved, and changes were made in the classification of ADEs. The final questionnaire consisted of 252 ADEs organized in 16 body categories, and included 14 questions per reported ADE. A total of 135 patients using a median of five different drugs completed the Web-based questionnaire twice. The median completion time was 15 min for patients not reporting any ADE, and 30 min for patients reporting at least one ADE. Three quarters of the patients found the questionnaire easy to use. Test-retest reliability was acceptable at patient level (j = 0.50, PPA 0.64) and at MedDRA Ò System Organ Class level (j = 0.52, PPA 0.54), but was low at ADEspecific level (j = 0.38, PPA 0.38). Conclusion We developed a generic patient-reported ADE questionnaire and confirmed its content validity. The questionnaire was feasible and reliable for reporting any ADE and similar ADEs at MedDRA Ò System Organ Class level. Additional work is, however, needed to reliably quantify specific ADEs reported by patients.

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A review of methods used in assessing non-serious adverse drug events in observational studies among type 2 diabetes mellitus patients

Cited by 25 publications

References 89 publications

Safety and Tolerability of EPs 7630 in Clinical Trials

Safety and Tolerability of EPs 7630 in Clinical Trials

Evaluation of Potentially Drug-Related Patient-Reported Common Symptoms Assessed During Clinical Medication Reviews: A Cross-Sectional Observational Study

Development and Initial Validation of a Patient-Reported Adverse Drug Event Questionnaire

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