9 results on '"Bertrand Guignard"'
Search Results
2. Development and retrospective evaluation of a clinical decision support system for the efficient detection of drug-related problems by clinical pharmacists
- Author
-
Christian Skalafouris, Anne-Laure Blanc, Olivier Grosgurin, Christophe Marti, Caroline Samer, Christian Lovis, Pascal Bonnabry, and Bertrand Guignard
- Subjects
Pharmacology ,Pharmaceutical Science ,Pharmacology (medical) ,Pharmacy ,Toxicology - Abstract
Background Clinical decision support systems (CDSS) can help identify drug-related problems (DRPs). However, the alert specificity remains variable. Defining more relevant alerts for detecting DRPs would improve CDSS. Aim Develop electronic queries that assist pharmacists in conducting medication reviews and an assessment of the performance of this model to detect DRPs. Method Electronic queries were set up in CDSS using “triggers” from electronic health records: drug prescriptions, laboratory values, medical problems, vital signs, demographics. They were based on a previous study where 315 patients admitted in internal medicine benefited from a multidisciplinary medication review (gold-standard) to highlight potential DRPs. Electronic queries were retrospectively tested to assess performance in detecting DRPs revealed with gold-standard. For each electronic query, sensitivity, specificity, positive and negative predictive value were computed. Results Of 909 DRPs, 700 (77.8%) were used to create 366 electronic queries. Electronic queries correctly detected 77.1% of DRPs, median sensitivity and specificity reached 100.0% (IQRs, 100.0%–100.0%) and 99.7% (IQRs, 97.0%–100.0%); median positive predictive value and negative predictive value reached 50.0% (IQRs, 12.5%–100.0%) and 100.0% (IQRs, 100.0%–100.0%). Performances varied according to “triggers” (p Conclusion Electronic queries based on electronic heath records had high sensitivity and negative predictive value and acceptable specificity and positive predictive value and may contribute to facilitate medication review. Implementing some of these electronic queries (the most effective and clinically relevant) in current practice will allow a better assessment of their impact on the efficiency of the clinical pharmacist.
- Published
- 2022
- Full Text
- View/download PDF
3. Patients’ perceptions of conflicting information on chronic medications: a prospective survey in Switzerland
- Author
-
Beatriz Santos, Katherine S Blondon, Elisabeth Van Gessel, Bernard Cerutti, Claudine Backes, Sophie Locher, Bertrand Guignard, Pascal Bonnabry, Delesha Carpenter, and Marie P Schneider
- Subjects
Adult ,Cross-Sectional Studies ,Surveys and Questionnaires ,Humans ,Prospective Studies ,General Medicine ,Pharmacists ,Switzerland ,Medication Adherence - Abstract
ObjectiveThe number of patients with chronic diseases and subsequent visits to various healthcare professionals has been rising over the past decades, exposing patients to potential risks of receiving conflicting medication information. This study aims to investigate the prevalence of conflicting information on medications perceived by chronic patients in Switzerland and to understand its impact on patients’ medication self-management and navigation in the healthcare system.ParticipantsThis cross-sectional study included adult patients taking at least one prescribed medication for at least 6 months, who had visited at least two physicians in the past 3 months.Main outcome measuresData on patients’ perceptions of conflicting information were collected in person through a 17-item questionnaire available on paper and electronically with four domains: (1) whether the patient had perceived any conflicting information, (2) categories of conflicting information, (3) impact and (4) sources involved in the conflicting information.ResultsOf the 405 included patients, 47% perceived conflicting information related to one or more medication topics including indication, schedule, dosage, risk, severity or duration of side effects. Patients who perceived conflicting information were prescribed more drugs than those perceiving no conflicting information (pConclusionNearly half the patients in our study perceived conflicting information in the outpatient healthcare system, which can decrease medication effectiveness and pose safety issues. This issue is widely overlooked and unaddressed. Consistency of information among healthcare providers in partnership with patients should be reinforced through guidelines and new models of interprofessional care.
- Published
- 2022
- Full Text
- View/download PDF
4. Development and assessment of PharmaCheck: an electronic screening tool for the prevention of twenty major adverse drug events
- Author
-
Jérôme Stirnemann, Pascal Bonnabry, François Eggimann, Christian Skalafouris, Jean-Luc Reny, Olivier Grosgurin, Megane Jermini, Damien Grauser, Daniel Teixeira, Bertrand Guignard, and Christel Bruggmann
- Subjects
Drug ,medicine.medical_specialty ,Drug-Related Side Effects and Adverse Reactions ,business.industry ,Health Policy ,media_common.quotation_subject ,Health Informatics ,Decision Support Systems, Clinical ,Medical Order Entry Systems ,Computer Science Applications ,medicine ,Humans ,Screening tool ,Electronics ,Intensive care medicine ,business ,Fatigue ,media_common - Abstract
Background Adverse drug events (ADEs) can be prevented by deploying clinical decision support systems (CDSS) that directly assist physicians, via computerized order entry systems, and clinical pharmacists performing medication reviews as part of medical rounds. However, physicians using CDSS are known to be exposed to the alert-fatigue phenomenon. Our study aimed to assess the performance of PharmaCheck—a CDSS to help clinical pharmacists detect high-risk situations with the potential to lead to ADEs—and its impact on clinical pharmacists’ activities. Methods Twenty clinical rules, divided into four risk classes, were set for the daily screening of high-risk situations in the electronic health records of patients admitted to our General Internal Medicine Department. Alerts to clinical pharmacists encouraged them to telephone prescribers and suggest any necessary treatment adjustments. PharmaCheck’s performance was assessed using the intervention’s positive predictive value (PPV), which characterizes the proportion of interventions for each alert triggered. PharmaCheck’s impact was assessed by considering clinical pharmacists as a filter for ruling out futile alerts and by comparing the final clinical PPV with a pharmacist (the proportion of interventions that led to a change in the medical regimen) to the final clinical PPV without a pharmacist. Results Over 132 days, 447 alerts were triggered for 383 patients, leading to 90 interventions (overall intervention PPV = 20.1%). By risk class, intervention PPVs made up 26.9% (n = 65/242) of abnormal laboratory value alerts, 3.1% (4/127) of alerts for contraindicated medications or medications to be used with caution, 28.2% (20/71) of drug–drug interaction alerts, and 14.3% (1/7) of inadequate mode of administration alerts. Clinical PPVs reached 71.0% (64/90) when pharmacists filtered alerts and 14% (64/242) if they were not doing it. Conclusion PharmaCheck enabled clinical pharmacists to improve their traditional processes and broaden their coverage by focusing on 20 high-risk situations. Alert management by pharmacists seemed to be a more effective way of preventing risky situations and alert-fatigue than a model addressing alerts to physicians exclusively. Some fine-tuning could enhance PharmaCheck's performance by considering the information quality of triggers, the variability of clinical settings, and the fact that some prescription processes are already highly secured.
- Published
- 2021
5. Pratique de la pharmacie clinique en Suisse romande
- Author
-
Olivier Bugnon, Johnny Beney, Chantal Csajka, Pascal Bonnabry, and Bertrand Guignard
- Published
- 2018
- Full Text
- View/download PDF
6. Detection of Live and Antibiotic-Killed Bacteria by Quantitative Real-Time PCR of Specific Fragments of rRNA
- Author
-
Philippe Moreillon, Steve Aellen, Marisa Haenni, Bertrand Guignard, and Yok-Ai Que
- Subjects
DNA, Bacterial ,Genetic Markers ,Ofloxacin ,Colony Count, Microbial ,Levofloxacin ,Microbial Sensitivity Tests ,Penicillins ,Biology ,Polymerase Chain Reaction ,Bacterial genetics ,Microbiology ,RNA, Ribosomal, 16S ,medicine ,Pharmacology (medical) ,Antibacterial agent ,Pharmacology ,Analytical Procedures ,Streptococcus gordonii ,Streptococcus ,Amplicon ,Ribosomal RNA ,16S ribosomal RNA ,biology.organism_classification ,Molecular biology ,Anti-Bacterial Agents ,Penicillin ,Kinetics ,RNA, Bacterial ,Infectious Diseases ,Genes, Bacterial ,RNA, Ribosomal ,Mutation ,Bacteria ,medicine.drug - Abstract
Assessing bacterial viability by molecular markers might help accelerate the measurement of antibiotic-induced killing. This study investigated whether rRNA could be suitable for this purpose. Cultures of penicillin-susceptible and penicillin-tolerant (Tol1 mutant) Streptococcus gordonii were exposed to mechanistically different penicillin and levofloxacin. Bacterial survival was assessed by viable counts and compared to quantitative real-time PCR amplification of either the 16S rRNA genes or the 16S rRNA, following reverse transcription. Penicillin-susceptible S. gordonii lost ≥4 log 10 CFU/ml of viability over 48 h of penicillin treatment. In comparison, the Tol1 mutant lost ≤1 log 10 CFU/ml. Amplification of a 427-bp fragment of 16S rRNA genes yielded amplicons that increased proportionally to viable counts during bacterial growth but did not decrease during drug-induced killing. In contrast, the same 427-bp fragment amplified from 16S rRNA paralleled both bacterial growth and drug-induced killing. It also differentiated between penicillin-induced killing of the parent and the Tol1 mutant (≥4 log 10 CFU/ml and ≤1 log 10 CFU/ml, respectively) and detected killing by mechanistically unrelated levofloxacin. Since large fragments of polynucleotides might be degraded faster than smaller fragments, the experiments were repeated by amplifying a 119-bp region internal to the original 427-bp fragment. The amount of 119-bp amplicons increased proportionally to viability during growth but remained stable during drug treatment. Thus, 16S rRNA was a marker of antibiotic-induced killing, but the size of the amplified fragment was critical for differentiation between live and dead bacteria.
- Published
- 2006
- Full Text
- View/download PDF
7. β-lactams against methicillin-resistant
- Author
-
Philippe Moreillon, José M. Entenza, and Bertrand Guignard
- Subjects
Pharmacology ,Cephem ,Carbapenem ,medicine.drug_class ,Cephalosporin ,Antibiotics ,biochemical phenomena, metabolism, and nutrition ,Biology ,medicine.disease_cause ,Methicillin-resistant Staphylococcus aureus ,Microbiology ,Penicillin ,Staphylococcus aureus ,Ampicillin ,Drug Discovery ,polycyclic compounds ,medicine ,medicine.drug - Abstract
Methicillin-resistant Staphylococcus aureus (MRSA) have developed resistance to virtually all non-experimental antibiotics. They are intrinsically resistant to beta-lactams by virtue of newly acquired low-affinity penicillin-binding protein 2A (PBP2A). Because PBP2A can build the wall when other PBPs are blocked by beta-lactams, designing beta-lactams capable of blocking this additional target should help solve the issue. Older molecules including penicillin G, amoxicillin and ampicillin had relatively good PBP2A affinities, and successfully treated experimental endocarditis caused by MRSA, provided that the bacterial penicillinase could be inhibited. Newer anti-PBP2A beta-lactams with over 10-fold greater PBP2A affinities and low minimal inhibitory concentrations were developed, primarily in the cephem and carbapenem classes. They are also very resistant to penicillinase. Most have demonstrated anti-MRSA activity in animal models of infection, and two--the carbapenem CS-023 and the cephalosporin ceftopibrole medocaril--have proceeded to Phase II and Phase III clinical evaluation. Thus, clinically useful anti-MRSA beta-lactams are imminent.
- Published
- 2005
- Full Text
- View/download PDF
8. Practical evaluation of the drug-related problem management process in Swiss community pharmacies
- Author
-
Olivier Bugnon, Bertrand Guignard, Bertha Kremer, and Jean-Marc Krähenbühl
- Subjects
medicine.medical_specialty ,Drug-Related Side Effects and Adverse Reactions ,Psychological intervention ,Pharmaceutical Science ,Collaborative Care ,Pharmacy ,Community Pharmacy Services ,Toxicology ,Pharmacists ,Professional Role ,Nursing ,Intervention (counseling) ,medicine ,Adverse Drug Reaction Reporting Systems ,Humans ,Pharmacology (medical) ,Drug Interactions ,Medical prescription ,Management process ,Quality of Health Care ,Pharmacology ,Dose-Response Relationship, Drug ,business.industry ,General Medicine ,Problem management ,Pharmaceutical care ,Pharmaceutical Preparations ,Family medicine ,business ,Software ,Switzerland - Abstract
Objective To develop and evaluate a coding system integrated into pharmaceutical software to routinely report and assess the process of community pharmacists’ interventions related to medical prescriptions. Setting A convenient sample of 20 Swiss community pharmacies. Method Pharmacists documented their interventions concerning all drug-related problems (DRPs) related to medical prescriptions during four consecutive weeks in 2005. The coding system assesses each step of the DRP management process; that is, the type of problem, possible negative outcomes, pharmaceutical decisions, and individuals involved. In order to be comprehensive, the management process of technical problems related to prescriptions and clinical DRPs was analysed separately. Main outcome measure DRP intervention rate and characterization of each step of the process. Results Of 38,663 prescriptions, 287 clinical DRPs required interventions. This corresponds to a mean intervention rate of 0.77% per pharmacy (SD = 0.61%). There was a large variability among pharmacies (0–2.6%). Most of the clinical DRPs were associated with dosage problems (n = 91) and drug–drug interactions (n = 45). The most frequent potential negative outcomes reported were quantitative inefficacy (n = 101) and quantitative safety (n = 94). Two-thirds of clinical DRPs required a prescription modification (n = 186), the most frequent being a change in dosage or drug regimen. In 110 interventions (38%), physicians were immediately contacted to take part in the decision. In 122 interventions (43%), pharmacists managed the interventions alone. However, in 55 interventions (19%), pharmacists managed the DRPs with the patient. From these 287 clinical interventions, 134 different codes were reported. Seven hundred and thirty-six technical problems related to prescriptions required intervention, which corresponded to a mean intervention rate of 1.90% per pharmacy. The main type of problem was a discrepancy with the medication record (n = 208). There were 494 instances that required a prescription modification. Pharmacists resolved 45% of all technical problems by themselves. Conclusion The developed coding system could describe the management process for DRPs. The observed intervention rate and the frequency of steps involved were comparable to those previously observed for pharmacists’ interventions. Data regarding the entire process used to manage drug-related problems can be useful in improving medication safety, education, and collaborative care.
- Published
- 2007
9. Beta-lactams against methicillin-resistant Staphylococcus aureus
- Author
-
Bertrand, Guignard, José M, Entenza, and Philippe, Moreillon
- Subjects
Clinical Trials as Topic ,Staphylococcus aureus ,Animals ,Humans ,Penicillin-Binding Proteins ,Methicillin Resistance ,beta-Lactams - Abstract
Methicillin-resistant Staphylococcus aureus (MRSA) have developed resistance to virtually all non-experimental antibiotics. They are intrinsically resistant to beta-lactams by virtue of newly acquired low-affinity penicillin-binding protein 2A (PBP2A). Because PBP2A can build the wall when other PBPs are blocked by beta-lactams, designing beta-lactams capable of blocking this additional target should help solve the issue. Older molecules including penicillin G, amoxicillin and ampicillin had relatively good PBP2A affinities, and successfully treated experimental endocarditis caused by MRSA, provided that the bacterial penicillinase could be inhibited. Newer anti-PBP2A beta-lactams with over 10-fold greater PBP2A affinities and low minimal inhibitory concentrations were developed, primarily in the cephem and carbapenem classes. They are also very resistant to penicillinase. Most have demonstrated anti-MRSA activity in animal models of infection, and two--the carbapenem CS-023 and the cephalosporin ceftopibrole medocaril--have proceeded to Phase II and Phase III clinical evaluation. Thus, clinically useful anti-MRSA beta-lactams are imminent.
- Published
- 2005
Catalog
Discovery Service for Jio Institute Digital Library
For full access to our library's resources, please sign in.