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407. Combining multiple healthcare databases for postmarketing drug and vaccine safety surveillance: why and how?

Author

Trifirò, G, Coloma, P M, Rijnbeek, P R, Romio, S, Mosseveld, B, Weibel, D, Bonhoeffer, J, Schuemie, M, van der Lei, J, and Sturkenboom, M

Abstract

A growing number of international initiatives (e.g. EU-ADR, Sentinel, OMOP, PROTECT and VAESCO) are based on the combined use of multiple healthcare databases for the conduct of active surveillance studies in the area of drug and vaccine safety. The motivation behind combining multiple healthcare databases is the earlier detection and validation, and hence earlier management, of potential safety issues. Overall, the combination of multiple healthcare databases increases statistical sample size and heterogeneity of exposure for postmarketing drug and vaccine safety surveillance, despite posing several technical challenges. Healthcare databases generally differ by underlying healthcare systems, type of information collected, drug/vaccine and medical event coding systems and language. Therefore, harmonization of medical data extraction through homogeneous coding algorithms across highly different databases is necessary. Although no standard procedure is currently available to achieve this, several approaches have been developed in recent projects. Another main challenge involves choosing the work models for data management and analyses whilst respecting country-specific regulations in terms of data privacy and anonymization. Dedicated software (e.g. Jerboa) has been produced to deal with privacy issues by sharing only anonymized and aggregated data using a common data model. Finally, storage and safe access to the data from different databases requires the development of a proper remote research environment. The aim of this review is to provide a summary of the potential, disadvantages, methodological issues and possible solutions concerning the conduct of postmarketing multidatabase drug and vaccine safety studies, as demonstrated by several international initiatives. [ABSTRACT FROM AUTHOR]

Published
2013
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408. Transplantation for acute liver failure in patients exposed to NSAIDs or paracetamol (acetaminophen): the multinational case-population SALT study.

Author

Gulmez SE, Larrey D, Pageaux GP, Lignot S, Lassalle R, Jové J, Gatta A, McCormick PA, Metselaar HJ, Monteiro E, Thorburn D, Bernal W, Zouboulis-Vafiadis I, de Vries C, Perez-Gutthann S, Sturkenboom M, Bénichou J, Montastruc JL, Horsmans Y, and Salvo F

Abstract

Background: Most NSAIDs are thought to be able to cause hepatic injury and acute liver failure (ALF), but the event rates of those leading to transplantation (ALFT) remain uncertain.Objectives: The aim of the study was to estimate population event rates for NSAID-associated ALFT METHODS: This was a case-population study of ALFT in 57 eligible liver transplant centres in seven countries (France, Greece, Ireland, Italy, The Netherlands, Portugal and the UK). Cases were all adults registered from 2005 to 2007 for a liver transplant following ALFT without identified clinical aetiology, exposed to an NSAID or paracetamol (acetaminophen) within 30 days before the onset of clinical symptoms. NSAID and paracetamol population exposures were assessed using national sales data from Intercontinental Marketing Services (IMS). Risk was estimated as the rate of ALFT per million treatment-years (MTY).Results: In the 52 participating centres, 9479 patients were registered for transplantation, with 600 for ALFT, 301 of whom, without clinical aetiology, had been exposed to a drug within 30 days. Of these 301 patients, 40 had been exposed to an NSAID and 192 to paracetamol (81 of whom were without overdose). Event rates per MTY were 1.59 (95 % CI 1.1-2.2) for all NSAIDs pooled, 2.3 (95 % CI 1.2-3.9) for ibuprofen, 1.9 (95 % CI 0.8-3.7) for nimesulide, 1.6 (95 % CI 0.6-3.4) for diclofenac and 1.6 (95 % CI 0.3-4.5) for ketoprofen. For paracetamol, the event rate was 3.3 per MTY (95 % CI 2.6-4.1) without overdoses and 7.8 (95 % CI 6.8-9.0) including overdoses.Conclusions: ALF leading to registration for transplantation after exposure to an NSAID was rare, with no major difference between NSAID. Non-overdose paracetamol-exposed liver failure was twice more common than NSAID-exposed liver failure. [ABSTRACT FROM AUTHOR]

Published
2013
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409. Assessing the risk of osteonecrosis of the jaw due to bisphosphonate therapy in the secondary prevention of osteoporotic fractures.

Author

Lapi, F., Cipriani, F., Caputi, A., Corrao, G., Vaccheri, A., Sturkenboom, M., Bari, M., Gregori, D., Carle, F., Staniscia, T., Vestri, A., Brandi, M., Fusco, V., Campisi, G., and Mazzaglia, G.

Subjects
OSTEONECROSIS, ACADEMIC medical centers, CHI-squared test, CONFIDENCE intervals, DIPHOSPHONATES, EPIDEMIOLOGY, BONE fractures, JAWS, OSTEOPOROSIS, QUESTIONNAIRES, RESEARCH funding, T-test (Statistics), LOGISTIC regression analysis, DATA analysis, CASE-control method, DATA analysis software, DESCRIPTIVE statistics, DISEASE complications, DISEASE risk factors
Abstract

Summary: There is evidence that the use oral bisphosphonates can lead to osteronecrosis of the jaws (ONJ). Although the occurrence of ONJ appears rare among oral bisphosphonates (BPs) users, it is important to know that it exists and can be opportunely minimized. Introduction: The purpose of this study is to evaluate the association between BPs prescribed for the secondary prevention of osteoporotic fractures and the occurrence of ONJ. Methods: An Italian record linkage claims database with a target population of around 18 million individuals (6 million over 55 years of age) constituted the data source. We conducted a nested case-control study within a cohort of individuals aged 55+ years old, who were discharged from hospitals with a primary diagnosis of incident osteoporotic fracture. The date related to the discharge diagnosis of ONJ was the index date. Conditional logistic regression for matched data was fitted to estimate the odds ratio (OR) along with 95 % confidence intervals (95 % CI) for the likely association between use of BPs and the risk of ONJ. Results: Any one of the 61 ascertained cases of ONJ (incidence rate, 36.6 per 100,000 person-years) was matched to 20 controls for a total of 1120 controls. When the exposure to BPs was modeled according to recency (i.e., exposure time window prior to the index date) of use, the adjusted OR (95 % CI) for current users was 2.8 (1.3-5.9) against never users. The cumulative use of BPs has shown to increase the incidence of ONJ among patients with primary osteoporotic fractures, although not statistically significant risk has been observed. Conclusions: Although the risk of BP-related ONJ appears low in non-oncological indications, it is important to be aware that it exists and to know how it may be predicted and possibly minimized. [ABSTRACT FROM AUTHOR]

Published
2013
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410. Individual NSAIDs and upper gastrointestinal complications: a systematic review and meta-analysis of observational studies (the SOS project).

Author

Castellsague J, Riera-Guardia N, Calingaert B, Varas-Lorenzo C, Fourrier-Reglat A, Nicotra F, Sturkenboom M, Perez-Gutthann S, Castellsague, Jordi, Riera-Guardia, Nuria, Calingaert, Brian, Varas-Lorenzo, Cristina, Fourrier-Reglat, Annie, Nicotra, Federica, Sturkenboom, Miriam, Perez-Gutthann, Susana, and Safety of Non-Steroidal Anti-Inflammatory Drugs (SOS) Project

Abstract

Background: The risk of upper gastrointestinal (GI) complications associated with the use of NSAIDs is a serious public health concern. The risk varies between individual NSAIDs; however, there is little information on the risk associated with some NSAIDs and on the impact of risk factors. These data are necessary to evaluate the benefit-risk of individual NSAIDs for clinical and health policy decision making. Within the European Community's Seventh Framework Programme, the Safety Of non-Steroidal anti-inflammatory drugs (NSAIDs) [SOS] project aims to develop decision models for regulatory and clinical use of individual NSAIDs according to their GI and cardiovascular safety.Objective: The aim of this study was to conduct a systematic review and meta-analysis of observational studies to provide summary relative risks (RR) of upper GI complications (UGIC) associated with the use of individual NSAIDs, including selective cyclooxygenase-2 inhibitors.Methods: We used the MEDLINE database to identify cohort and case-control studies published between 1 January 1980 and 31 May 2011, providing adjusted effect estimates for UGIC comparing individual NSAIDs with non-use of NSAIDs. We estimated pooled RR and 95% CIs of UGIC for individual NSAIDs overall and by dose using fixed- and random-effects methods. Subgroup analyses were conducted to evaluate methodological and clinical heterogeneity between studies.Results: A total of 2984 articles were identified and 59 were selected for data abstraction. After review of the abstracted information, 28 studies met the meta-analysis inclusion criteria. Pooled RR ranged from 1.43 (95% CI 0.65, 3.15) for aceclofenac to 18.45 (95% CI 10.99, 30.97) for azapropazone. RR was less than 2 for aceclofenac, celecoxib (RR 1.45; 95% CI 1.17, 1.81) and ibuprofen (RR 1.84; 95% CI 1.54, 2.20); 2 to less than 4 for rofecoxib (RR 2.32; 95% CI 1.89, 2.86), sulindac (RR 2.89; 95% CI 1.90, 4.42), diclofenac (RR 3.34; 95% CI 2.79, 3.99), meloxicam (RR 3.47; 95% CI 2.19, 5.50), nimesulide (RR 3.83; 95% CI 3.20, 4.60) and ketoprofen (RR 3.92; 95% CI 2.70, 5.69); 4-5 for tenoxicam (RR 4.10; 95% CI 2.16, 7.79), naproxen (RR 4.10; 95% CI 3.22, 5.23), indometacin (RR 4.14; 95% CI 2.91, 5.90) and diflunisal (RR 4.37; 95% CI 1.07, 17.81); and greater than 5 for piroxicam (RR 7.43; 95% CI 5.19, 10.63), ketorolac (RR 11.50; 95% CI 5.56, 23.78) and azapropazone. RRs for the use of high daily doses of NSAIDs versus non-use were 2-3 times higher than those associated with low daily doses.Conclusions: We confirmed variability in the risk of UGIC among individual NSAIDs as used in clinical practice. Factors influencing findings across studies (e.g. definition and validation of UGIC, exposure assessment, analysis of new vs prevalent users) and the scarce data on the effect of dose and duration of use of NSAIDs and on concurrent use of other medications need to be addressed in future studies, including SOS. [ABSTRACT FROM AUTHOR]

Published
2012
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411. Abstracts of papers and posters Meeting on Pharmaceutical Sciences

Author

Coile, Russell C., primary, Wiedhaup, K., additional, Bommel, Ilva, additional, Mol, Miriam, additional, Vries, Michiel, additional, Massey, E. W., additional, Biller, J., additional, Davis, J. N., additional, Adams, H. P., additional, Marler, J. R., additional, Magnani, H. N., additional, Schotte, A., additional, Janssen, P. F. M., additional, Leysen, J. E., additional, Skrabanja, A. T. P., additional, Flendrig, L., additional, Iren, F., additional, Schrijnemakers, E. W. M., additional, Reinhoud, P. J., additional, Kijne, J. W., additional, Knevelman, A., additional, Wit, H. J. C., additional, Vries, J. D., additional, Bult, A., additional, Beijnen, J. H., additional, Winden, E. C. A., additional, Talsma, H., additional, Crommelin, D. J. A., additional, Storm, G., additional, Oussoren, C., additional, Zuidema, J., additional, Vingerhoeds, M. H., additional, Smit, R. H. P., additional, Dinther, F. v., additional, Hultermans, T., additional, Beumer, T., additional, Fransz, A. N., additional, Vromans, H., additional, Bloemhof, D. A., additional, Mansvelt, F. J. W., additional, Brouwers, J. R. B. J., additional, Raemaekers, J., additional, Boskma, R. J., additional, Bloemhof, H., additional, Graaf, S. S. N., additional, Uges, D. R. A., additional, Kosterink, J. G. W., additional, Jonge, M. W. A., additional, Smit, E. F., additional, Kengen, R. A. M., additional, Leij, L., additional, Piers, D. A., additional, Shochat, D., additional, The, T. H., additional, Luurtsema, Gert, additional, Franssen, Eric, additional, Visser, Geb, additional, Jeronimus-Stratingh, Margot, additional, Bruins, Andries, additional, Vaalburg, Wim, additional, Luurtsema, G., additional, Medema, J., additional, Elsinga, P. H., additional, Franssen, E. J. F., additional, Visser, G. M., additional, Vaalburg, W., additional, Jmker, Jan I., additional, Uges, Donald R. A., additional, Paauw, Hugo, additional, Maas, Max, additional, Vos, Henk, additional, Hettelaar, Jenny, additional, Slolk, L. M. L., additional, Brand, W., additional, Smit, B. J., additional, Franssen, R. M. E., additional, Vinks, A. A. T. M. M., additional, Touw, D. J., additional, Heijerman, H. G. M., additional, Danhof, M., additional, Bakker, W., additional, Hermans, J., additional, Driessen, G. J., additional, Wolters, R., additional, Go, I. H., additional, Fennis, J., additional, Gribnau, F. W. J., additional, Heerdink, Eibert R., additional, Leufkens, Hubert G., additional, Bakker, Albert, additional, Heerdink, E. R., additional, Lau, H. S., additional, Bakker, A., additional, Porsius, A. J., additional, Beuning, K. S., additional, Postma-Lim, E., additional, Boer, A., additional, Nagtegaal, J. E., additional, Stecher, N., additional, Sturkenboom, M. C. J. M., additional, Jong-van den Berg, L. T. W., additional, Cornel, M. C., additional, Stricker, B. H. Ch., additional, Wesseling, H., additional, Bemt, P. M. L. A., additional, Kil, P. J. M., additional, Meyboom, R. H. B., additional, Koning, G. H. P., additional, Herings, Ron M. C., additional, Stricker, Bruno H. Ch., additional, Leufkens, Hubert G. M., additional, Urquhart, John, additional, Boer, Anthonius, additional, Sturmans, Ferd, additional, Middeibeek, Alma, additional, Sturkenboom, Miriam C. J. M., additional, Jong-van den Berg, Lolkje T. W., additional, Lammers, M. W., additional, Hekster, Y. A., additional, Keyser, A., additional, Meinardi, H., additional, Renier, W. O., additional, Lier, H., additional, Veehof, L., additional, Stewart, R., additional, Mevboom-de Jong, B., additional, Haaijer-Ruskamp, F. M., additional, Visser, L. E., additional, Velden, J., additional, Paes, A. H. P., additional, Mil, J. W. F., additional, Tromp, Th. F. J., additional, Casparie, M. K., additional, Kuijpers, A., additional, Stuvt, P. M. J., additional, Dijkers, F. W., additional, Ree, C. M., additional, Ruben, B. A., additional, Mokkink, H. G. A., additional, Post, D., additional, Gubbels, J. W., additional, Stokx, L. J., additional, Foets, M., additional, Florax, C., additional, Dijk, A., additional, Peters, E. T. J., additional, Werf, G. T., additional, Denig, P., additional, Boerkamp, Ellis J. C., additional, Haaijer-Ruskamp, Flora M., additional, Reuyl, Jan C., additional, Versluis, Albert, additional, Trigtv, Anke M., additional, Jong- vd Berg, Lolkie T. W., additional, Willems, Jaap, additional, Kaldeway, Hans, additional, Wieringa, Nicolien, additional, Herxheimer, Andrew, additional, Vos, Rein, additional, Heijman, Jennifer, additional, Rikken, Floor, additional, Omta, S. W. F., additional, Bouter, L. M., additional, Engelen, J. M. L., additional, Leufkens, H. G. M., additional, Steffens, B., additional, Thijssen, J. J. H., additional, Boer, D., additional, Tissot van Patot, H. A., additional, Leusink, J. A., additional, Jongh, B. M., additional, Reuvers, Inge H., additional, Galiën, Trea A., additional, Tromp, Dick F. J., additional, Hendrikx, N. E. H. W., additional, Werf, G. Th., additional, Vos, R., additional, Swart, J. A. A., additional, Haisma, H. J., additional, Borchert, J. C. H., additional, Versantvoort, M. W., additional, Steenbergen, M. J., additional, Hennink, W. E., additional, Wolthuis, W. N. E., additional, Hooff, R. J. M., additional, Wientjes, K. J. C., additional, Schmidt, F. J., additional, Schoonen, A. J. M., additional, Wierik, G. H. P., additional, Eissens, A. C., additional, Lerk, C. F., additional, Haas, M., additional, Iwema Bakker, W. I., additional, Reinhoudt, D. N., additional, Mijer, D. K. F., additional, Zeeuw, D., additional, Proost, J. H., additional, Wierda, J. M. K. H., additional, Meijer, D. K. F., additional, Kuipers, M., additional, Swart, P. J., additional, Hendriks, M. M. W. B., additional, Kamps, J. A. A. M., additional, Struska, B., additional, Thomas, C., additional, Nijenhuis, A. M., additional, Scherphof, G. L., additional, Swaan, Peter W., additional, Stehouwer, Marco C., additional, Blok, Eric J. C., additional, Tukker, Josef J., additional, Dijk, J., additional, Gorissen, H. R. M., additional, Groot-Padberg, Y. M., additional, Olling, M., additional, Gelderen, C. E. M., additional, Salomons, P., additional, Barends, D. M., additional, Meulenbelt, J., additional, Rauws, A. G., additional, Craane-van Hinsberg, W. H. M., additional, Verhoef, J. C., additional, Junginger, H., additional, and Boddé, H. E., additional

Published
1993
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413. Acitretin (Neotigason®)

Author

Bouvy, M. L., primary, Sturkenboom, M. C. J. M., additional, Cornel, M. C., additional, De Jong-Van den Berg, L. T. W., additional, Stricker, B. H. C., additional, and Wesseling, H., additional

Published
1992
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415. Incidence of Multiple Sclerosis in the General Population in the Netherlands, 1996-2008.

Author

Kramer, M. A., van Der Maas, N. A. T., van Soest, E. M., Kemmeren, J. M., de Melker, H. E., and Sturkenboom, M. C. J. M.

Abstract

Background: We estimated the multiple sclerosis (MS) incidence in the Netherlands for better active monitoring of potential vaccine safety signals. Methods: A retrospective cohort study (1996-2008) was conducted using a population-based general practice research database containing electronic medical records. Additional information was collected to validate incident probable cases. Results: In the source population (648,656 persons), 146 incident probable MS cases were identified. Overall incidence rate was 6.3/100,000 person years (py; 95% Cl, 5.2-7.2). In the subgroup in which MS could be fully validated, the incidence increased from 4/100,000 py (95% CI, 3-5) in 1996-2004 to 9/100,000 py in 2007/8 (95% Cl, 6-16). This increase was highest among women, but not statistically significantly different by gender. The median lag time between first recorded symptoms and MS diagnosis decreased from 32 months (<1998) to 2 months (>2005). Conclusions: MS is rare in the Netherlands. In recent years, there was a slight increase in the incidence especially among women during the fertile age. This increase coincided with a decrease in lag time between symptoms and diagnosis, both for men and women. This trend should be taken into account in the interpretation of MS cases occurring in a population where new vaccinations will be introduced shortly. [ABSTRACT FROM AUTHOR]

Published
2012
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416. Risk of recurrent myocardial infarction with the concomitant use of clopidogrel and proton pump inhibitors.

Author

Valkhoff, V. E., 't Jong, G. W., Van Soest, E. M., Kuipers, E. J., and Sturkenboom, M. C. J. M.

Subjects
CLOPIDOGREL, CARDIOVASCULAR diseases, MYOCARDIAL infarction, PROTON pump inhibitors, ADENOSINE diphosphate
Abstract

Background The association between myocardial infarction (MI) and co-administration of proton pump inhibitors (PPIs) and clopidogrel remains controversial. Aim To quantify the association between concomitant use of PPIs and clopidogrel and occurrence of recurrent MI. Methods We conducted a case-control study within a cohort of acute MI patients in PHARMO Record Linkage System (1999-2008). The cases were patients readmitted for MI. PPI exposure was categorized as current (3-1 days before MI), past (30-3 days before MI), or no use (>30 days before MI). We used conditional logistic regression analyses. Results Among 23 655 patients hospitalized following MI, we identified 1247 patients readmitted for MI. Among clopidogrel users, current PPI use was associated with an increased risk of recurrent MI (OR: 1.62, 95% CI: 1.15- 2.27) when compared with no PPI use, but not when compared with past PPI use (OR: 0.95, 95% CI: 0.38-2.41). Among clopidogrel non-users, current PPI use was associated with an increased risk of recurrent MI (OR: 1.38, 95% CI: 1.18-1.61) when compared with no PPI use. Conclusions The apparent association between recurrent MI and use of PPIs with clopidogrel depends on the design, and is affected by confounding by indication. The association is not present when (un)measured confounding is addressed by design. [ABSTRACT FROM AUTHOR]

Published
2011
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418. A novel programme to evaluate and communicate 10-year risk of CHD reduces predicted risk and improves patients’ modifiable risk factor profile.

Author

Benner, J. S., Erhardt, L., Flammer, M., Moller, R. A., Rajicic, N., Changela, K., Yunis, C., Cherry, S. B., Gaciong, Z., Johnson, E. S., Sturkenboom, M. C. J. M., García-Puig, J., and Girerd, X.

Abstract

Aims: We assessed whether a novel programme to evaluate/communicate predicted coronary heart disease (CHD) risk could lower patients’ predicted Framingham CHD risk vs. usual care. Methods: The Risk Evaluation and Communication Health Outcomes and Utilization Trial was a prospective, controlled, cluster-randomised trial in nine European countries, among patients at moderate cardiovascular risk. Following baseline assessments, physicians in the intervention group calculated patients’ predicted CHD risk and were instructed to advise patients according to a risk evaluation/communication programme. Usual care physicians did not calculate patients’ risk and provided usual care only. The primary end-point was Framingham 10-year CHD risk at 6 months with intervention vs. usual care. Results: Of 1103 patients across 100 sites, 524 patients receiving intervention, and 461 receiving usual care, were analysed for efficacy. After 6 months, mean predicted risks were 12.5% with intervention, and 13.7% with usual care [odds ratio = 0.896; p = 0.001, adjusted for risk at baseline (17.2% intervention; 16.9% usual care) and other covariates]. The proportion of patients achieving both blood pressure and low-density lipoprotein cholesterol targets was significantly higher with intervention (25.4%) than usual care (14.1%; p < 0.001), and 29.3% of smokers in the intervention group quit smoking vs. 21.4% of those receiving usual care (p = 0.04). Conclusions: A physician-implemented CHD risk evaluation/communication programme improved patients’ modifiable risk factor profile, and lowered predicted CHD risk compared with usual care. By combining this strategy with more intensive treatment to reduce residual modifiable risk, we believe that substantial improvements in cardiovascular disease prevention could be achieved in clinical practice. [ABSTRACT FROM AUTHOR]

Published
2008
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419. The diagnostic value of 124I-PET in patients with differentiated thyroid cancer.

Author

Phan, Ha T. T., Jager, Pieter L., Paans, Anne M. J., Plukker, John T. M., Sturkenboom, M. G. G., Sluiter, W. J., Wolffenbuttel, Bruce H. R., Dierckx, Rudi A. J. O., and Links, Thera P.

Subjects
CLINICAL trials, THYROID disease diagnosis, DIAGNOSTIC imaging, RADIONUCLIDE imaging, POSITRON emission tomography, POSITRON emission
Abstract

The purpose of this prospective study was to evaluate the clinical diagnostic value of iodine-124 (124I)-positron emission tomography (PET) in patients with advanced differentiated thyroid carcinoma (DTC) and to compare the 124I-PET imaging results with the 131I whole-body scan (WBS). Twenty patients with histologically proven advanced DTC (including T4, extra-nodal tumour growth, or distant metastases) underwent diagnostic 131I-WBS, 124I-PET scan, and post-treatment 131I-WBS 4 months after ablation. The findings on the 124I-PET were compared with the findings on the diagnostic and post-therapeutic 131I-WBS and were also correlated with radiologic and/or cytological investigations. 124 I-PET vs diagnostic 131 I-WBS. Eleven patients showed uptake on the 124I-PET. Only 3 of these 11 patients also showed uptake on the diagnostic 131I scan, but the uptake was more clearly visible and the abnormalities were more extensive on the 124I-PET. 124 I-PET vs post-treatment 131 I-WBS. Eleven patients showed uptake on the 124I-PET, which was also visible on the post-treatment scan in nine patients; in the other two patients, no uptake was observed on the post-treatment scan and no anatomical localisation could be confirmed. Two patients showed only uptake on the post-treatment scan without uptake on the 124I-PET: in one, the uptake was confirmed by MRI, and in the other, no anatomical localisation was found. In seven patients, no uptake was observed on both the scans. 124I-PET proved to be a superior diagnostic tool as compared to low-dose diagnostic 131I scans and adequately predicted findings on subsequent high-dose post-treatment 131I scans. [ABSTRACT FROM AUTHOR]

Published
2008
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420. Increasing incidence of Barrett's oesophagus in the general population.

Author

van Soest, E. M., Kuipers, E. J., Siersema, P. D., Dieleman, J. P., and Sturkenboom, M. C. J. M.

Subjects
ESOPHAGEAL cancer, ENDOSCOPY, DATABASES, ADENOCARCINOMA, MEDICAL records, COMPUTER files
Abstract

Background: Barrett's oesophagus (BO) predisposes to oesophageal adenocarcinoma. Epidemiological data suggest that the incidence of BO is rising but it is unclear whether this reflects a true rise in incidence of BO or an increase in detection secondary to more upper gastrointestinal endoscopies performed. This study aimed to examine the changes in BO incidence relative to the number of upper gastrointestinal endoscopies performed in the general population. Methods: We conducted a cohort study using the integrated Primary Care Information database. This general practice research database contains the complete and longitudinal electronic medical records of more than 500 000 persons. Results: In total, 260 incident cases of BO were identified during the study period. The incidence of BO increased from 14.3/100 000 person years in 1997 (95% confidence interval (CI) 8.6-22.4) to 23.1 / 100 000 person years (95% CI 17.2-30.6) in 2002 (r² = 0.87). The number of upper gastrointestinal endoscopies decreased from 7.2/1000 person years (95% CI 6.7-7.7) to 5.7/1000 person years (95% CI 5.4-6.1) over the same time period. This resulted in an overall increase in detected BO per 1000 endoscopies from 19.8 (95% CI 12.0-31.0) in 1997 to 40.5(95% CI 30.0-53.5) in 2002 (r²=0.93). The incidence of adenocarcinoma increased from 1.7/100 000 person years (95% CI 0.3-5.4) in 1997 to 6.0/100000 person years (95% CI 3.3-10.2) in 2002 (r²=0.87). Conclusion: The incidence of diagnosed BO is increasing, independent of the number of upper gastrointestinal endoscopies that are being performed. This increase in BO incidence will likely result in a further increase in the incidence of oesophageal adenocarcinomas in the near future. [ABSTRACT FROM AUTHOR]

Published
2005
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421. Annual Revaccination Against Influenza and Mortality Risk in Community-Dwelling Elderly Persons.

Author

Voordouw, A. C. G., Sturkenboom, M. C. J. M., Dieleman, J. P., Stijnen, Th., Smith, D. J., van der Lei, J., and Stricker, Bruno H. Ch.

Subjects
*INFLUENZA vaccines, *PREVENTION of communicable diseases, *IMMUNIZATION of older people, *VACCINATION, *MORTALITY, *GROUP homes, *RESPIRATORY infections, *COMORBIDITY, *CLINICAL trials, *HEALTH outcome assessment
Abstract

Context Although large-scale observational studies have demonstrated the effectiveness of influenza vaccination, no large studies have systematically addressed the clinical benefit of annual revaccinations. Objective To investigate the effect of annual influenza revaccination on mortality in community-dwelling elderly persons. Design, Setting, and Participants A population-based cohort study using the computerized Integrated Primary Care Information (IPCI) database in the Netherlands including community-dwelling individuals aged 65 years or older from 1996 through 2002. For each year, we computed the individual cumulative exposure to influenza vaccination since study start. Main Outcome Measure Association between the number of consecutive influenza vaccinations and all-cause mortality vs no vaccination after adjusting for age, sex, chronic respiratory and cardiovascular disease, hypertension, diabetes mellitus, renal failure, and cancer. Results The study population included 26 071 individuals, of whom 3485 died during follow-up. Overall, a first vaccination was associated with a nonsignificant annual reduction of mortality risk of 10% (hazard ratio [HR], 0.90; 95% confidence interval [CI], 0.78-1.03) while revaccination was associated with a reduced mortality risk of 24% (HR, 0.76; 95% CI, 0.70-0.83). Compared with a first vaccination, revaccination was associated with a reduced annual mortality risk of 15% (HR, 0.85; 95% CI, 0.75-0.96). During the epidemic periods this reduction was 28% (HR, 0.72; 95% CI, 0.53-0.96). Similar estimates were obtained for persons with and without chronic comorbidity and those aged 70 years or older at baseline. Overall, influenza vaccination is estimated to prevent 1 death for every 302 vaccinees at a vaccination coverage that varied between 64% and 74%. Conclusion Annual influenza vaccination is associated with a reduction in all-cause mortality risk in a population of community-dwelling elderly persons, particularly in older in... [ABSTRACT FROM AUTHOR]

Published
2004
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422. Adherence to proton pump inhibitors or H 2-receptor antagonists during the use of non-steroidal anti-inflammatory drugs.

Author

Sturkenboom, M. C. J. M., Burke, T. A., Tangelder, M. J. D., Dieleman, J. P., Walton, S., and Goldstein, J. L.

Subjects
*PROTON pump inhibitors, *NONSTEROIDAL anti-inflammatory agents, *GASTROINTESTINAL diseases, *ENZYME inhibitors
Abstract

: The efficacy of proton pump inhibitors (PPIs) or histamine-2 receptor antagonists (H2RAs) prescribed as prophylaxis for NSAID-related upper gastrointestinal (UGI) toxicity is dependent upon patient adherence. : To describe patient adherence to prophylactically prescribed PPIs and H2RAs in the clinical setting. : We conducted a retrospective observational cohort study using the Integrated Primary Care Information Project database. The study population consisted of incident non-specific NSAID users prescribed a PPI or H2RA specifically as prophylaxis for NSAID-related UGI toxicity. Patients were classified as non-adherent if < 75% of days of NSAID use were covered by one of these agents, and as continuing users after discontinuation of NSAID use if they had a renewed prescription for these agents after their last NSAID prescription. : The study cohort comprised 784 patients: 374 with H2RAs, 405 with PPIs, and 5 with both PPI and H2RA. Eighty-five percent of H2RA users and 7% of PPI users were prescribed these drugs at doses below the minimum recommended/effective dose for NSAID-associated gastroduodenal ulcer prophylaxis. Thirty-seven percent of patients were non-adherent. The lowest rate of non-adherence was associated with the first NSAID prescription (9%), increasing to 61% for patients with ⩾ 3 prescriptions. In a cohort of subjects who stopped their NSAID and were followed for up to 2 years ( n = 711), there was significant persistent use of acid suppressive agents; 40% of patients had at least one additional prescription for the acid suppressive agent after stopping NSAIDs, and> 30% received enough drug to cover a period longer than 2 months after stopping their NSAID. : The pattern of PPI and H2RA prescriptions, when prescribed as prophylactic strategy, does not correspond with the pattern of NSAID use. Physicians should consider the medical impact of non-adherence with dual therapies and the impact of prolonged use of GPAs on treatment cost. [ABSTRACT FROM AUTHOR]

Published
2003
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423. Clinical Renal Pharmacology and Therapeutics.

Author

Trimarchi, Hernan, Schiel, A., Freixas, E., Dieleman, J. P., Sturkenboom, M. C. J. M., Jambroes, M., Knoll, Greg A., Sahgal, A., Nair, R. C., Butler, J. V., McAvoy, H., McEnroy, D., Hu, Y., Carpenter, J. P., Cheung, A. T., Kincaid-Smith, Priscilla, Fairley, K., Packham, D., and Elian, K. M.

Subjects
PHARMACOLOGY, THERAPEUTICS, CHEMICAL inhibitors, HEMODIALYSIS, HOMEOSTASIS
Abstract

Presents several studies on clinical renal pharmacology and therapeutics. Risk factors for the urological symptoms in a cohort of users of the HIV protease inhibitor indinavir sulfate; Risk of hyperkalemia in hemodialysis patients taking angiotensin-converting enzyme inhibitors or angiotensin receptor blockers; Effects of spironolactone on potassium homeostasis in elderly patients with congestive heart failure.

Published
2003

424. Neuropsychiatric events during prophylactic use of mefloquine before travelling.

Author

van Riemsdijk, M. M., Ditters, J. M., Sturkenboom, M. C. J. M., Tulen, J. H. M., Ligthelm, R. J., Overbosch, D., and Stricker, B. H. Ch.

Subjects
MEFLOQUINE, ANTIMALARIALS, ANTIPARASITIC agents, DRUG therapy for malaria, CLINICAL psychology, NEUROPSYCHIATRY
Abstract

Introduction. It has been suggested that neuropsychiatric events during use of mefloquine are more common in females than in males and are partly explained by the psychological stress of travelling. Therefore, we investigated neuropsychiatric events in females and males on mefloquine in the 3-week prophylactic period that precedes travelling. Furthermore, we investigated whether first-time users had a higher risk of neuropsychiatric adverse events than subjects with a history of mefloquine use. Methods. We enrolled all patients who visited a Travel Clinic for mefloquine prophylaxis during the period 1 May 1999 to 7 March 2000. Each patient was followed from baseline (prior to starting mefloquine) up to 3 weeks after the start of mefloquine but before travelling. We asked patients to register any adverse event in a diary and measured the intra-individual change in scores on the Dutch Shortened Profile Of Mood States (POMS) at baseline and at the end of follow-up. Results. The final cohort consisted of 179 subjects with a mean age of 3 years. Females reported adverse events more frequently than males (P=0.005). Overall, we observed a small but significant increase in the score on the domain fatigue [0.74 points, 95% confidence interval (CI) 0.18, 1.30]. The effect was exclusively present in females and not in males. First-time users of mefloquine increased 2.81 points (95% CI 0.70, 4.92) on the total score of the POMS, and among those, women showed the largest increase of 4.58 points (95% CI 0.74, 8.43). Conclusion. The use of mefloquine was associated with neuropsychiatric adverse effects. Females encountered neuropsychiatric effects more frequently than males, which could be confirmed by validated psychological tests. Neuropsychiatric effects were more common in first-time users than in individuals who had used mefloquine before. [ABSTRACT FROM AUTHOR]

Published
2002
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426. Incidence and Mortality of Acute Pancreatitis between 1985 and 1995.

Author

Eland, I. A., Sturkenboom, M. J. C. M., Wilson, J. H. P., and Stricker, B. H. Ch.

Subjects
*PANCREATITIS, *REPORTING of diseases, *HEALTH status indicators
Abstract

Background: The incidence of acute pancreatitis seems to have increased in Western countries. It has been suggested that this increase can be explained by improved diagnostic procedures. We performed a nationwide study to assess the annual sex- and age-specific incidence and mortality rates of acute pancreatitis in the Netherlands between 1985 and 1995, a period in which diagnostic procedures did not change considerably. Methods: We conducted a population-based retrospective follow-up study in which we used automated hospital discharge data accumulated by Prismant Health Care Information. All patients admitted with acute pancreatitis (ICD-9CM, 577.0) in the Netherlands were identified. We accounted for referrals to other hospitals to avoid double counting and for miscoding of chronic pancreatitis as acute pancreatitis. The annual population size was retrieved from the Netherlands Central Statistics Office. Results: The observed incidence of acute pancreatitis increased from 12.4/100,000 person-years (95% confidence interval (CI), 11.8-12.9) in 1985 to 15.9/100,000 person-years (95% CI, 15.3-16.5) in 1995. The annual mortality rate of acute pancreatitis remained fairly stable at 1.5/100,000 person-years. The incidence and mortality rate of acute pancreatitis increased considerably with age. The case-fatality proportion of first admissions for acute pancreatitis decreased from 14.3% to 10.7%. The case-fatality for relapses remained stable at 3.2%. Conclusions: In this retrospective study the observed incidence of acute pancreatitis increased by 28% between 1985 and 1995. Due to a decrease in the case-fatality proportion, the mortality remained stable during this period. [ABSTRACT FROM AUTHOR]

Published
2000
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427. Metallothionein in mice reduces intestinal zinc loss during acute endotoxin inflammation, but not during starvation or dietary zinc restriction.

Author

Philcox, Jeffrey C., Sturkenboom, Marieke, Philcox, J C, Sturkenboom, M, Coyle, P, and Rofe, A M

Subjects
METALLOTHIONEIN, ZINC in the body, MICE, STARVATION, ENDOTOXINS, SCIENTIFIC experimentation, PHYSIOLOGY, ZINC metabolism, ANIMALS, BODY composition, ENTERITIS, FECES, INTESTINES, LIVER, METALLOPROTEINS, MOTIVATION (Psychology), WATER-electrolyte balance (Physiology), WEIGHT loss, ZINC, LIPOPOLYSACCHARIDES
Abstract

Normal metallothionein [(MT)+/+] and MT-null (MT-/-) mice were used to examine the influence of MT on Zn retention and the metabolic consequences of 2 d food deprivation, with and without inflammation induced by intraperitoneal injection of bacterial endotoxin lipopolysaccharide (LPS). LPS reduced fecal Zn concentration in MT+/+ mice from 5.9 +/- 0.2 micromol/g on d 1 to 2.2 +/- 0.2 micromol/g on d 2, but not in MT-/- mice, 5.9 +/- 0.2 and 5.7 +/- 0. 5 micromol/g, respectively. MT+/+ mice fed an 8 mg Zn/kg diet and injected with LPS excreted 40% less Zn over 2 d than their MT-/- counterparts. Starvation for 2 d did not lower fecal Zn concentration in either genotype, although in MT+/+ mice, urinary Zn excretion was reduced from 12.7 +/- 1.3 nmol on d 1 to 5.9 +/- 1.8 nmol on d 2 and plasma Zn concentration was lowered to 9.8 +/- 0.4 micromol/L. Zn was not reduced in urine or plasma of MT-/- mice, with respective values of 10.8 +/- 2.0 nmol on d 1, 9.3 +/- 2.9 nmol on d 2 and 13.0 +/- 1.0 micromol/L. LPS injection resulted in much higher total liver Zn (677 +/- 27 nmol) and MT (106 +/- 2 nmol Cd bound/g) than starvation (Zn = 405 +/- 21, MT = 9 +/- 3) in MT+/+ mice after 2 d, but did not further reduce urinary Zn. LPS-injected MT-/- mice had no rise in liver Zn or fall in plasma and urine Zn. MT-/- mice fed a Zn-deficient (0.8 mg Zn/kg) diet lost 10% of body weight over 25 d compared with no loss in MT+/+ mice. Despite this, MT-/- mice excreted no more Zn via the gut than did MT+/+ mice. In summary, MT inhibits intestinal Zn loss when highly expressed. When uninduced, typically during Zn deficiency, MT appears to conserve Zn and body mass by reducing only urinary and other nonintestinal Zn losses. [ABSTRACT FROM AUTHOR]

Published
2000
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429. Communicating a drug alert.

Author

Sturkenboom, M., Jong-van den Berg, L., Cornel, M., Stricker, B., and Wesseling, H.

Abstract

In October 1990, a recall procedure was initiated for the teratogenic drug acitretin, and the recommended post-therapy contraception period after acitretin therapy was extended from 2 months to 2 years due to the possibility of its conversion to the lipophilic compound etretinate. The aim of the present study was to evaluate the communication procedures and their effects as a drug alert from the health authorities, the pharmaceutical company and professional associations of health professionals to the population at risk. A model was used to evaluate communication between three hierarchical levels. Data were obtained via semi-structured interviews and structured questionnaires. Communication procedures were evaluated according to channel characteristics and by analysis of their contents. The effect was measured as whether the drug dispensers identified acitretin users, contacted physicians, and whether physicians communicated in person with the population at risk. The penetration of direct mail from the health authorities and from the pharmaceutical company ranged from 97-98% and 65-94% at Level 2 (health professionals). The population at risk was informed via personal communication with health professionals, and/or the mass media. Of the women at risk, 19% were contacted by a dermatologist, 30% by their GP, and 39% by the pharmacist. 35% was never informed by any health professional. The Dutch health care system is adequately equipped for effective communication between health authorities, pharmaceutical industry and health professionals. Due to problems with identification in terms of past exposure, subsequent personal communication between health professionals and the population at risk was inadequate. Therefore, the role in personal communication of health professionals should be increased, as they can rapidly identify persons at risk as a result of previous exposure. In The Netherlands drug dispensers should have an important role. [ABSTRACT FROM AUTHOR]

Published
1994
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430. Tolerability and pharmacokinetic evaluation of inhaled dry powder hydroxychloroquine in healthy volunteers.

Author

de Reus, Y. A., Hagedoorn, P., Sturkenboom, M. G. G., Grasmeijer, F., Bolhuis, M. S., Sibum, I., Kerstjens, H. A. M., Frijlink, H. W., and Akkerman, O. W.

Subjects
*INHALERS, *HYDROXYCHLOROQUINE, *POWDERS, *PULMONARY function tests, *PHARMACOKINETICS, *BITTERNESS (Taste)
Abstract

Rationale: Inhaled antimicrobials enable high local concentrations where needed and, compared to orally administration, greatly reduce the potential for systemic side effects. In SARS-CoV-2 infections, hydroxychloroquine sulphate (HCQ) administered as dry powder via inhalation could be safer than oral HCQ allowing higher and therefore more effective pulmonary concentrations without dose limiting toxic effects. Objectives: To assess the local tolerability, safety and pharmacokinetic parameters of HCQ inhalations in single ascending doses of 5, 10 and 20 mg using the Cyclops dry powder inhaler. Methods: Twelve healthy volunteers were included in the study. Local tolerability and safety were assessed by pulmonary function tests, electrocardiogram and recording adverse events. To estimate systemic exposure, serum samples were collected before and 0.5, 2 and 3.5 h after inhalation. Results and discussion: Dry powder HCQ inhalations were well tolerated by the participants, except for transient bitter taste in all participants and minor coughing irritation. There was no significant change in QTc-interval or drop in FEV1 post inhalation. The serum HCQ concentration remained below 10 μg/L in all samples. Conclusion: Single doses of inhaled dry powder HCQ up to 20 mg are safe and well tolerated. Our data support that further studies with inhaled HCQ dry powder to evaluate pulmonary pharmacokinetics and efficacy are warranted. [ABSTRACT FROM AUTHOR]

Published
2022
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433. Correction to: Impact of risk minimisation measures on the use of strontium ranelate in Europe: a multi-national cohort study in 5 EU countries by the EU-ADR Alliance.

Author

Berencsi, K., Sami, A., Ali, M. S., Marinier, K., Deltour, N., Perez-Gutthann, S., Pedersen, L., Rijnbeek, P., Van der Lei, J., Lapi, F., Simonetti, M., Reyes, C., Sturkenboom, M. C. J. M., and Prieto-Alhambra, D.

Subjects
BONE growth, DRUGS, OSTEOPOROSIS
Abstract

The original version of this article, published on 26 November 2019 contained a mistake. [ABSTRACT FROM AUTHOR]

Published
2020
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434. Abstracts of papers

Author

Tognoni, G., Medawar, Charles, Romero, M., Venturini, F., Di Pasquale, R., Font, M., Boissel, J. -P., Liberati, Alessandro, Rampazzo, R., Scroccaro, G., Torri, Valter, Fossati, R., Liberati, A., Marsoni, S., Altimiras, J., Di Pasquale, R., Cattaruzzi, C., Aqostinis, L., Maggini, M., Garcia Rodriguez, L. A., Raschetti, R., Simon, G., Troncon, M. G., Herxheimer, Andrew, Mignot, G., Bardelay, D., Nasi, G. F., Bonati, M., Messori, A., Li, Wan Po A., Rampaszo, R., van Hooreweghe, M., Robays, H., Rømsing, J., Møller-Sonnergaard, J., Hertel, S., Rasmussen, M., Todd, Sybil, Nuessle, Sally, Carlen, I., Tanner, M., Reinke, C., Marty, S., Saponaro, S., Luzzi, R., Claesson, C. B., Cornelius, C., Thorslund, M., Winblad, B., Leufkens, Hubert G., Heerdink, Eibert R., Bakker, Albert, Sturkenboom, M. C. J. M., Middelbeek, A., de Jong van den Berg, L. T. W., van den Berg, PB, Stricker, BHCh, Garattini, Silvio, Conti, G., Hazebroucq, G., Raza, A., Labbrozzi, D., Nicolucci, A., Ingela, Wiklund, Lucioni, Carlo, Salek, M. S., Griffith, A. R., Spiller, C., Luscombe, D. K., and Bayer, A. J.

Published
1994
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435. Can the EU-ADR Database Network Detect Drug Safety Signals Faster than Spontaneous Reporting System?

Author

Trifiro, G., Patadia, V., Schuemie, M., Coloma, P., Rosa Gini, Herings, R., Mazzaglia, G., Picelli, G., Scotti, L., Pedersen, L., Lei, J., Sturkenboom, M., Trifiro, G, Patadia, V, Schuemie, M, Coloma, P, Gini, R, Herings, R, Mazzaglia, G, Picelli, G, Scotti, L, Pedersen, L, Van der Lei, J, and Sturkenboom, M

Subjects
Spontaneuous reporting, Electronic Healthcare Database, Adverse Drug Reaction, Signal detection
Abstract

Background: Several ongoing initiatives are exploring if mining electronic health records (EHRs) may fasten the process of drug safety signal detection. We investigated if the signal concerning rofecoxib and acute myocardial infarction could have been identified in EU-ADR database network faster than spontaneous reporting system (SRS), and earlier than rofecoxib withdrawal (30th September 2004). Methods: EU-ADR distributed network comprises of seven EHR databases covering approximately a population of almost 30 million persons from four European Countries during the years 1996–2010. Harmonized data extraction and analysis has been conducted in all databases through custom-built software Jerboa, which allows for data aggregation and elaboration while databases remained locally. A signal was defined as statistically significant (p-value

436. HARMONISING DEFINITIONS OF ADVERSE EVENTS AMONG 8 EUROPEAN HEALTHCARE DATABASES PARTICIPATING IN THE EU-ADR PROJECT

Author

Gini, R., Avillach, P., Coloma, P. M., Mougin, F., Dufour, J-C, Thiessard, F., Joubert, M., Mazzaglia, G., Giaquinto, C., Fornari, C., Herings, R., Julia Hippisley-Cox, Molokhia, M., Pedersen, L., Fourrier-Reglat, A., Fieschi, M., Sturkenboom, M., Lei, J., Pariente, A., Trifiro, G., Gini, R, Avillach, P, Coloma, P, Mougin, F, Dufour, J, Thiessard, F, Joubert, M, Mazzaglia, G, Giaquinto, C, Fornari, C, Herings, R, Hippisley-Cox, J, Molokhia, M, Pedersen, L, Fourrier-Réglat, A, Fieschi, M, Sturkenboom, M, Van Der Lei, J, Pariente, A, and Trifirò, G

Subjects
Semantic Interoperability
Abstract

INTRODUCTION Detection of clinical events from diverse electronic sources of information such as hospital discharge claims (HOSP), death registries (DEATH), laboratory values (LAB), and general practice databases (GP) may be useful for various epidemiological purposes. In particular, the EU-ADR project aims to detect adverse events deemed to be important in pharmacovigilance. Eight databases (DBs) from four countries, combining different sources of information, participate in the project. A common conceptual framework was lacking to describe harmoniously the algorithm by which each DB detected each event. OBJECTIVES Describe the algorithms that 8 different DBs used to identify 6 events: Acute myocardial infarction (AMI), Acute Renal Failure (ARF), Anaphylactic Shock (AS), Bullous Eruption (BE), Rhabdomyolysis (RHABD), Upper Gastrointestinal Bleeding (UGIB). Benchmark corresponding incidence rates (IRs). METHODS A list of medical concepts corresponding to each event of interest was provided and projected to the DSs different coding systems (ICD9, ICD10, READ, ICPC) and natural languages through the Unified Medical Language System (UMLS). Specific sources of information contained in each DB were classified in a common framework and DBs with similar structures were asked to search for concepts within the same sources. RESULTS Concepts were mainly searched for in GP diagnoses and primary diagnoses of HOSP, but for some events DEATH (AMI, ARF, AS) and LAB (RHABD) were independently used by DBs having them. Resulting age-adjusted IRs vary as follows across DBs: 1-2/1,000PY (AMI), 3-7/10,000PY (UGIB), 2-12/100,000PY (AS), 2-17/100,000PY (BE), 1-8/100,000PY (RHABD), 3-49/100,000PY (ARF). CONCLUSIONS It is possible to describe event extractions from heterogeneous DBs in a common conceptual framework. Residual differences in IRs may be due either to differences in the underlying populations or to differences in the characteristics (structure, coding system) of the DBs.

437. Triage and Evaluation of Potential Safety Signals Identified from Electronic Healthcare Record Databases

Author

Coloma, P. M., Schuemie, M. J., Trifiro, G., Furlong, L., Mulligen, E., Bauer-Mehren, A., Avillach, P., Kors, J., Sanz, F., Mestres, J., Oliveira, J. L., Boyer, S., Helgee, E. A., Molokhia, M., Matthews, J., Prieto-Merino, D., Rosa Gini, Herings, R. M. C., Mazzaglia, G., Picelli, G., Scotti, L., Pedetsen, L., Lei, J., Sturkenboom, M. C. J. M., Coloma, P, Schuemie, M, Trifiro, G, Furlong, L, Van Mulligen, E, Bauer-Mehren, A, Avillach, P, Kors, J, Sanz, F, Mestres, J, Oliveira, J, Boyer, S, Helgee, E, Molokhia, M, Matthews, J, Prieto-Merino, D, Gini, R, Herings, R, Mazzaglia, G, Picelli, G, Scotti, L, Pedetsen, L, Van der Lei, J, and Sturkenboom, M

Subjects
Spontaneuous reporting, Validation studies, Electronic Healthcare Database, Adverse Drug Reaction, Signal detection
Abstract

Background: There is huge potential for mining electronic healthcare records (EHR) databases to augment current systems in pharmacovigilance.[1-3] Like any signal detection system, there is a need to establish ‘rules’ how to trigger an alert, when to consider a signal likely enough to be true to warrant follow-up or even to require immediate health policy intervention.[4,5] Objectives: To describe the process of prioritisation of drug-adverse event associations derived from signal detection using EHR databases in the EU-ADR Project. Methods: Association measures between drug use and acute myocardial infarction (AMI) were generated by first applying various statistical methods on healthcare data from seven databases of the EUADR network.[6] Association estimates were ranked based on the best performing method (Longitudinal Gamma Poisson Shrinker). Matched case-control and self-controlled case series methods were additionallyconducted to deal with temporality and confounding effect, while the LEOPARD method was applied to specifically detect protopathic bias. Consistency of the association among drugs of the same class and the number of excess cases attributable to the drug exposure were further assessed to prioritize the list of potential signals. Finally, signal filtering and signal substantiation were done using different bioinformatics workflows to determine the novelty and plausibility of the identified signals. Results: Demographic, clinical and prescription/dispensing data in three European Countries were obtained from 21 171 291 individuals with 154 474 063 person-years of follow-up within the period 1995–2011. Overall, 163 potential signals forAMI were identified based on statistical association. Of these, 72 signals were flagged by LEOPARDas likely due to protopathic bias. Further signal refinement to reduce possible confounding decreased the number of signals to 39. Nine signals remained after applying the criteria for novelty and plausibility. Conclusion: We propose a prioritisation strategy for drug safety signal detection using EHR by taking into account, in addition to statistical association, also public health relevance, novelty, and plausibility. This strategy needs to be further tested using other EHR data sources and other adverse events.

438. Drug Use and Acute Liver Injury in Children: Signal Detection Using Multiple Healthcare Databases

Author

Ferrajolo, C., Trifiro, G., Coloma, P. M., Schuemie, M. J., Rosa Gini, Herings, R., Cox, J. Hippisley, Mazzaglia, G., Picelli, G., Scotti, L., Pedersen, L., Lei, J., Sturkenboom, M., Ferrajolo, C, Trifiro, G, Coloma, P, Schuemie, M, Gini, R, Herings, R, Cox, J, Mazzaglia, G, Picelli, G, Scotti, L, Pedersen, L, Van der Lei, J, and Sturkenboom, M

Subjects
Epidemiology, Electronic Health Record, Child, Adverse Drug Reaction, Liver Failure
Abstract

Background: Drug-induced acute liver injury (ALI) is one of the leading causes of drug withdrawal from the market. There is, however, lack of data on ALI in the pediatric population. Combining multi-country electronic healthcare databases offers the opportunity to explore the risk of ALI in children and adolescents and facilitate detection of potential drug safety signals. Objectives: To identify drugs potentially associated with ALI in the pediatric population using the EU-ADR database network and to estimate the power of such a network for signal detection concerning ALI as a function of actual drug use, minimal detectable relative risk (RR) and Background incidence rate (IR) of ALI in children and adolescents. Methods: We extracted data on all potential cases of ALI and data concerning prescribed/dispensed drugs among individuals 0–15 years registered within eight European, population-based, electronicmedical record and claims databases of the EU-ADR network during the period 1995–2010. We estimated the Background IR of ALI in the pediatric population and assessed drug use according to number of person-years (PYs) of exposure by Anatomical Therapeutic and Chemical (ATC) classification, 5th level. Based on IR of ALI derived within EU-ADR, power = 80% and alpha = 5%, we estimated how much drug exposure would be necessary to allow for detection of a signal concerning ALI. Finally, among drugs with enough exposure, all potential signals were identified by measuring age- and sex-adjusted relative risks of ALI, with all other drugs as comparator. Results: Children 0–15 years of age contributed 20 088 726 PYs of follow-up to the EU-ADR database network. The incidence rate for ALI was estimated to be 4.3 per 100 000 PYs in this pediatric population. The total amount of drug exposure that would be required to detect a ‘weak’ association (RR= 2) with ALI, if present, was 186 490 PYs and 28 554 PYs to detect a ‘moderate’ association (RR = 4). The following drugs were identified to be potentially associated with ALI: amoxicillin (RR 4.3, 95% CI 2.6, 7.0); clarithromycin (3.7, 1.8, 7.5); cetirizine (3.1, 1.5, 6.5); flunisolide (2.5, 1.0, 6.8); budesonide (2.5, 1.1, 5.5); and amoxicillin plus clavulanic acid (2.3, 1.3, 4.1). Conclusions: Combining multiple electronic healthcare databases may facilitate identification of potentially drug-related cases of ALI and increase the power for drug safety signal detection in the pediatric population. Except for the anti-asthmatic medications, the signals detected are already known in adults.

439. Comparison of Signal Detection Using Healthcare Database Network versus Spontaneous Reporting System Database: the EU-ADR Experience

Author

Trifiro, G., Patadia, V., Coloma, P. M., Schuemie, M. J., Rosa Gini, Herings, R., Cox, J. Hippisley, Mazzaglia, G., Picelli, G., Scotti, L., Pedersen, L., Avillach, P., Lel, J., Sturkenboom, M., Trifiro, G, Patadia, V, Coloma, P, Schuemie, M, Gini, R, Herings, R, Cox, J, Mazzaglia, G, Picelli, G, Scotti, L, Pedersen, L, Avillach, P, van der Lel, J, and Sturkenboom, M

Subjects
safety, validation, adverse drug-reaction, project, experience, pharmacovigilance, event, design, database, performance
Abstract

Background: The EU-ADR project aims to exploit different European electronic healthcare records (EHR) databases for drug safety signal detection. Currently, it is unknown what could be the additional value of using EHR databases for signal detection, with respect to traditional pharmacovigilance system. Objectives: To describe the preliminary results of the comparison of signal detection, as conducted in EU-ADR database network versus US Food and Drug Administration and World Health Organization spontaneous reporting databases. Methods: EU-ADR data sources consist of eight databases in four countries (Denmark, Italy, Netherlands, and United Kingdom) that are combined through distributed data network.[1] A custom-built software (Jerboaª) elaborates harmonized input data that are produced locally and generates aggregated data which are then stored in a central repository. These data are subsequently analyzed using a variety of signal detection methods adapted to longitudinal data (e.g., Longitudinal Gamma Poisson Shrinker). As potential signals, all drugs that are associated with ten events of interest (bullous eruptions - BE, acute renal failure - ARF, acute myocardial infarction - AMI, anaphylactic shock - AS, rhabdomyolysis - RHABD, upper gastrointestinal bleeding – UGIB, neutropenia – NEUTROP, pancytopenia – PANCYT, acute liver injury – ALI, and cardiac valve fibrosis) have been detected via different data mining techniques in the two systems. The number of drugs that could be investigated and the potential signals detected for each event of interest were then compared between spontaneous reporting systems (SRS) and EU-ADR network. Results: SRSs could explore, as potential signals, a larger number of drugs for the ten events, in comparison to EU-ADR, particularly for rare events generally thought to be highly drug attributable (i.e. BE: 3393 vs 228). The highest proportion of signals detected in SRSs was found for BE, ARF and AS, while for AMI, ARF, and UGIB in EUADR. When restricted to the same set of drugs, overall EU-ADR could identify a larger number of signals than SRSs, while some signals were detected in both systems. Conclusions: EU-ADR database network may complement traditional pharmacovigilance system, especially for the detection of signals regarding adverse events that are frequent in the general population and are not highly drug attributable.

440. Demographic risk factors and lymphocyte populations in patients with tuberculosis and their healthy contacts

Author

Antonio PONTICIELLO, Perna, F., Sturkenboom, M. C. J. M., Marchetiello, I., Bocchino, M., Sanduzzi, A., Epidemiology, Ponticiello, Antonio, Perna, Francesco, Sturkenboom, M. C. J., Marchetiello, Ilaria, Bocchino, Marialuisa, Sanduzzi Zamparelli, Alessandro, Sturkenboom, Mc, Marchetiello, I, and SANDUZZI ZAMPARELLI, Alessandro

Subjects
Adult, Male, TRANSMISSION, SUBSETS, PULMONARY TUBERCULOSIS, Cohort Studies, Sex Factors, SDG 3 - Good Health and Well-being, Risk Factors, INFECTION, Prevalence, IMMUNE-RESPONSE, Humans, Lymphocytes, Prospective Studies, Tuberculosis, Pulmonary, Aged, Age Factors, CYTOTOXIC T-CELLS, Middle Aged, Lymphocyte Subsets, Italy, Socioeconomic Factors, GAMMA-INTERFERON, Female, MYCOBACTERIUM-TUBERCULOSIS, Contact Tracing, CD8(+), ALPHA-BETA
Abstract

SETTING: Campania, a southern region of Italy, and the Institute of Respiratory Diseases, Monaldi Hospital, University 'Federico II', Naples. OBJECTIVE: To evaluate clinical and socio-demographic risk factors for tuberculosis (TB) infection and/ or disease. Peripheral blood lymphocytes from a subcohort of 19 patients and 53 contacts were studied by flow cytometry. DESIGN: A prospective study among patients with newly diagnosed pulmonary tuberculosis and their close contacts. RESULTS: A total of 90 patients and 277 contacts were enrolled. The prevalence of infection was 45% (95%CI 39-51%) among contacts. Age, sex, delay in diagnosis and treatment, cavitation on chest radiograph, cough, unwillingness to cover the mouth, and volume of air shared by close contacts and patients were investigated as potential risk factors for infection. Only delay in diagnosis of cases remained independently associated with an increased risk of infection (P < 0.0002), and hemoptysis was the only factor capable of reducing the delay significantly. The CD8(+)CD28(+) cytotoxic subset was significantly diminished in the patients (P < 0.001), whereas the CD8(+)CD28(-) and CD8(+)CD57(+) (suppressor and NK-like subsets) were elevated (P < 0.001 and P = 0.04). CONCLUSIONS: These data show that delay in diagnosis of cases is a crucial factor for tuberculosis and that cytotoxic CD8(+) cells play a primary role in immune response to tuberculosis.

444. I-MOVE: a European network to measure the effectiveness of influenza vaccines

Author

Valenciano, M., Ciancio, Bc, I-Move, Study Team, Ciancio, B. C., Kramarz, P., Nicoll, A., Kissling, E., Moren, A., Savulescu, C., Seyler, T., Mazick, A., Widgren, K., Bui, T., Cohen, J. M., Daviaud, I., Mosnier, A., Oroszi, B., Caini, S., Csohan, A., Horvath, J. K., Rozsa, M., Barret, A. S., Domegan, L., O Donnell, J., Declich, S., Puzelli, S., Rizzo, C., Rota, M. C., Dieleman, J., Sturkenboom, M., Wijnans, L., Voordouw, B., Gluchowska, M., Paradowska-Stankiewicz, I., Stefanoff, P., Batista, I., Barreto, M., Conde, P., Falcao, J. M., Goncalves, P., Guiomar, R., Machado, A., Nunes, B., Pechirra, P., Helena Rebelo-de-Andrade, Santos, L., Falcao, I., Alexandrescu, V., Ivanciuc, A., Lupulescu, E., Pitigoi, D., Durnall, H., Fleming, D., Andrews, N., Hardelid, P., Kafatos, G., Pebody, R., Watson, J., Zambon, M., Kavanagh, K., Robertson, C., Mcmenamin, J., Reynolds, A., Larrauri, A., Jimenez-Jorge, S., Mateo, S., Pozo, F., Barricarte, A., Castilla, J., Garcia Cenoz, M., Martinez-Baz, I., and Guevara, M.

447. Fluoroquinolones and risk of Achilles tendon disorders: case-control study.

Author

van der Linden, P D, Sturkenboom, M C J M, Herings, R M C, Leufkens, H G M, and Stricker, B H Ch

Subjects
*TENDONS, *ACHILLES tendon injuries, *MEDICAL care for older people, *DRUG prescribing, *DRUGS
Abstract

Presents a nested case-control study among users of fluoroquinolones in a large general practice database in Great Britain, to study the association with Achilles tendon disorders. Participants, methods, and results; Conclusion that exposure to fluoroquinolones increases the risk of Achilles tendon disorders, although this adverse effect is relatively rare; Statement that prescibers should be aware of the risk, especially in elderly people taking corticosteroids.

Published
2002
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448. Chronic disease prevalence from Italian administrative databases in the VALORE project: a validation through comparison of population estimates with general practice databases and national survey

Author

Gini Rosa, Francesconi Paolo, Mazzaglia Giampiero, Cricelli Iacopo, Pasqua Alessandro, Gallina Pietro, Brugaletta Salvatore, Donato Daniele, Donatini Andrea, Marini Alessandro, Zocchetti Carlo, Cricelli Claudio, Damiani Gianfranco, Bellentani Mariadonata, Sturkenboom Miriam CJM, and Schuemie Martijn J

Subjects
Prevalence, Chronic disease, Validation studies, Data reuse, Public aspects of medicine, RA1-1270
Abstract

Abstract Background Administrative databases are widely available and have been extensively used to provide estimates of chronic disease prevalence for the purpose of surveillance of both geographical and temporal trends. There are, however, other sources of data available, such as medical records from primary care and national surveys. In this paper we compare disease prevalence estimates obtained from these three different data sources. Methods Data from general practitioners (GP) and administrative transactions for health services were collected from five Italian regions (Veneto, Emilia Romagna, Tuscany, Marche and Sicily) belonging to all the three macroareas of the country (North, Center, South). Crude prevalence estimates were calculated by data source and region for diabetes, ischaemic heart disease, heart failure and chronic obstructive pulmonary disease (COPD). For diabetes and COPD, prevalence estimates were also obtained from a national health survey. When necessary, estimates were adjusted for completeness of data ascertainment. Results Crude prevalence estimates of diabetes in administrative databases (range: from 4.8% to 7.1%) were lower than corresponding GP (6.2%-8.5%) and survey-based estimates (5.1%-7.5%). Geographical trends were similar in the three sources and estimates based on treatment were the same, while estimates adjusted for completeness of ascertainment (6.1%-8.8%) were slightly higher. For ischaemic heart disease administrative and GP data sources were fairly consistent, with prevalence ranging from 3.7% to 4.7% and from 3.3% to 4.9%, respectively. In the case of heart failure administrative estimates were consistently higher than GPs’ estimates in all five regions, the highest difference being 1.4% vs 1.1%. For COPD the estimates from administrative data, ranging from 3.1% to 5.2%, fell into the confidence interval of the Survey estimates in four regions, but failed to detect the higher prevalence in the most Southern region (4.0% in administrative data vs 6.8% in survey data). The prevalence estimates for COPD from GP data were consistently higher than the corresponding estimates from the other two sources. Conclusion This study supports the use of data from Italian administrative databases to estimate geographic differences in population prevalence of ischaemic heart disease, treated diabetes, diabetes mellitus and heart failure. The algorithm for COPD used in this study requires further refinement.

Published
2013
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449. Burden of acute otitis media in primary care pediatrics in Italy: a secondary data analysis from the Pedianet database

Author

Marchisio Paola, Cantarutti Luigi, Sturkenboom Miriam, Girotto Silvia, Picelli Gino, Dona Daniele, Scamarcia Antonio, Villa Marco, and Giaquinto Carlo

Subjects
Acute otitis media, Incidence, Primary care pediatrics, Pediatrics, RJ1-570
Abstract

Abstract Background The incidence of acute otitis media (AOM) vary from country to country. Geographical variations together with differences in study designs, reporting and settings play a role. We assessed the incidence of AOM in Italian children seen by primary care paediatricians (PCPs), and described the methods used to diagnose the disease. Methods This secondary data analysis from the Pedianet database considered children aged 0 – 6 years between 01/2003 and 12/2007. The AOM episodes were identified and validated by means of patient diaries. Incidence rates/100 person-years (PY) were calculated for total AOM and for single or recurrent AOM. Results The 92,373 children (52.1% males) were followed up for a total of 227,361 PY: 23,039 (24.9%) presented 38,241 episodes of AOM (94.6% single episodes and 5.4% recurrent episodes). The total incidence rate of AOM in the 5-year period was 16.8 episodes per 100 PY (95% CI: 16.7-16.9), including single AOM (15.9 episodes per 100 PY; 95% CI: 15.7-16.1) and recurrent AOM (0.9 episodes per 100 PY; 95% CI: 0.9-0.9). There was a slight and continuously negative trend decrease over time (annual percent change −4.6%; 95%CI: -5.3, -3.9%). The AOM incidence rate varied with age, peaking in children aged 3 to 4 years (22.2 episodes per 100 PY; 95% CI 21.8-22.7). The vast majority of the AOM episodes (36,842/38,241, 96.3%) were diagnosed using a static otoscope; a pneumatic otoscope was used in only 3.7%. Conclusions Our data fill a gap in our knowledge of the incidence of AOM in Italy, and indicate that AOM represents a considerable burden for the Italian PCP system. Educational programmes concerning the diagnosis of AOM are needed, as are further studies to monitor the incidence in relation to the introduction of wider pneumococcal conjugate vaccines.

Published
2012
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450. Effectiveness of a MF-59™-adjuvanted pandemic influenza vaccine to prevent 2009 A/H1N1 influenza-related hospitalisation; a matched case-control study

Author

van der Sande Marianne AB, Sturkenboom Miriam CJM, Dieleman Jeanne P, Wijnans Eleonora G, Steens Anneke, and van der Hoek Wim

Subjects
Infectious and parasitic diseases, RC109-216
Abstract

Abstract Background During the 2009 influenza A/H1N1 pandemic, adjuvanted influenza vaccines were used for the first time on a large scale. Results on the effectiveness of the vaccines in preventing 2009 influenza A/H1N1-related hospitalisation are scanty and varying. Methods We conducted a matched case-control study in individuals with an indication for vaccination due to underlying medical conditions and/or age ≥ 60 years in the Netherlands. Cases were patients hospitalised with laboratory-confirmed 2009 A/H1N1 influenza infection between November 16, 2009 and January 15, 2010. Controls were matched to cases on age, sex and type of underlying medical condition(s) and drawn from an extensive general practitioner network. Conditional logistic regression was used to estimate the vaccine effectiveness (VE = 1 - OR). Different sensitivity analyses were used to assess confounding by severity of underlying medical condition(s) and the effect of different assumptions for missing dates of vaccination. Results 149 cases and 28,238 matched controls were included. It was estimated that 22% of the cases and 28% of the controls received vaccination more than 7 days before the date of onset of symptoms in cases. A significant number of breakthrough infections were observed. The VE was estimated at 19% (95%CI -28-49). After restricting the analysis to cases with controls suffering from severe underlying medical conditions, the VE was 49% (95%CI 16-69). Conclusions The number of breakthrough infections, resulting in modest VE estimates, suggests that the MF-59™ adjuvanted vaccine may have had only a limited impact on preventing 2009 influenza A/H1N1-related hospitalisation in this setting. As the main aim of influenza vaccination programmes is to reduce severe influenza-related morbidity and mortality from influenza in persons at high risk of complications, a more effective vaccine, or additional preventive measures, are needed.

Published
2011
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