Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial

Markus Messerli; Eva Blozik; Noortje Vriends; Kurt E Hersberger

doi:10.1186/s12913-016-1384-8

Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial

Standard

Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial. / Messerli, Markus; Blozik, Eva; Vriends, Noortje; Hersberger, Kurt E.

in: BMC HEALTH SERV RES, Jahrgang 16, 23.04.2016, S. 145.

Publikationen: SCORING: Beitrag in Fachzeitschrift/Zeitung › SCORING: Zeitschriftenaufsatz › Forschung › Begutachtung

Harvard

Messerli, M, Blozik, E, Vriends, N & Hersberger, KE 2016, 'Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial', BMC HEALTH SERV RES, Jg. 16, S. 145. https://doi.org/10.1186/s12913-016-1384-8

APA

Messerli, M., Blozik, E., Vriends, N., & Hersberger, K. E. (2016). Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial. BMC HEALTH SERV RES, 16, 145. https://doi.org/10.1186/s12913-016-1384-8

Vancouver

Messerli M, Blozik E, Vriends N, Hersberger KE. Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial. BMC HEALTH SERV RES. 2016 Apr 23;16:145. https://doi.org/10.1186/s12913-016-1384-8

Bibtex

@article{0661e0ce38b94655acc811f2315ee6ce,

title = "Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial",

abstract = "BACKGROUND: In 2010 the 'Polymedication Check' (PMC), a pharmacist-led medication review, was newly introduced to be delivered independently from the prescriber and reimbursed by the Swiss health insurances. This study aimed at evaluating the impact of this new cognitive service focusing on medicines use and patients' adherence in everyday life.METHODS: This randomised controlled trial was conducted in 54 Swiss community pharmacies. Eligible patients used ≥4 prescribed medicines over >3 months. The intervention group received a PMC at study start (T-0) and after 28 weeks (T-28) while the control group received only a PMC at T-28. Primary outcome measure was change in patients' objective adherence, calculated as Medication Possession Ratio (MPR) and Daily Polypharmacy Possession Ratio (DPPR), using refill data from the pharmacies and patient information of dosing. Subjective adherence was assessed as secondary outcome by self-report questionnaires (at T-0 and T-28) and telephone interviews (at T-2 and T-16), where participants estimated their overall adherence on a scale from 0-100%.RESULTS AND DISCUSSION: A total of 450 patients were randomly allocated to intervention (N = 218, 48.4%) and control group (N = 232, 51.6%). Dropout rate was fairly low and comparable for both groups (N Int = 37 (17.0%), NCont = 41 (17.7%), p = 0.845). Main addressed drug-related problem (DRP) during PMC at T-0 was insufficient adherence to at least one medicine (N = 69, 26.7%). At T-28, 1020 chronic therapies fulfilled inclusion criteria for MPR calculation, representing 293 of 372 patients (78.8%). Mean MPR and adherence to polypharmacy (DPPR) for both groups were equally high (MPRInt = 88.3, SD = 19.03; MPRCont = 87.5, SD = 20.75 (p = 0.811) and DPPRInt = 88.0, SD = 13.31; DPPRCont = 87.5, SD = 20.75 (p = 0.906), respectively). Mean absolute change of subjective adherence between T-0 and T-2 was +1.03% in the intervention and -0.41% in the control group (p = 0.058). The number of patients reporting a change of their adherence of more than ±5 points on a scale 0-100% between T-0 and T-2 was significantly higher in the intervention group (NImprovement = 30; NWorsening = 14) than in the control group (NImprovement = 20; NWorsening = 24; p = 0.028).CONCLUSION: Through the PMC pharmacist were able to identify a significant number of DRPs. Participants showed high baseline objective adherence of 87.5%, providing little potential for improvement. Hence, no significant increase of objective adherence was observed. However, regarding changes in subjective adherence of more than ±5% the PMC showed a positive effect.TRIAL REGISTRATION: Clinical trial registry database, NCT01739816; first entry on November 27, 2012.",

keywords = "Adolescent, Adult, Aged, Counseling, Databases, Factual, Drug Utilization Review, Female, General Practice, Hospitalization, Humans, Male, Medication Adherence, Middle Aged, Patient Acceptance of Health Care, Patient Dropouts, Pharmacies, Pharmacists, Polypharmacy, Prospective Studies, Self Report, Switzerland, Young Adult, Journal Article, Multicenter Study, Randomized Controlled Trial, Research Support, Non-U.S. Gov't",

author = "Markus Messerli and Eva Blozik and Noortje Vriends and Hersberger, {Kurt E}",

year = "2016",

month = apr,

day = "23",

doi = "10.1186/s12913-016-1384-8",

language = "English",

volume = "16",

pages = "145",

journal = "BMC HEALTH SERV RES",

issn = "1472-6963",

publisher = "BioMed Central Ltd.",

}

RIS

TY - JOUR

T1 - Impact of a community pharmacist-led medication review on medicines use in patients on polypharmacy--a prospective randomised controlled trial

AU - Messerli, Markus

AU - Blozik, Eva

AU - Vriends, Noortje

AU - Hersberger, Kurt E

PY - 2016/4/23

Y1 - 2016/4/23

N2 - BACKGROUND: In 2010 the 'Polymedication Check' (PMC), a pharmacist-led medication review, was newly introduced to be delivered independently from the prescriber and reimbursed by the Swiss health insurances. This study aimed at evaluating the impact of this new cognitive service focusing on medicines use and patients' adherence in everyday life.METHODS: This randomised controlled trial was conducted in 54 Swiss community pharmacies. Eligible patients used ≥4 prescribed medicines over >3 months. The intervention group received a PMC at study start (T-0) and after 28 weeks (T-28) while the control group received only a PMC at T-28. Primary outcome measure was change in patients' objective adherence, calculated as Medication Possession Ratio (MPR) and Daily Polypharmacy Possession Ratio (DPPR), using refill data from the pharmacies and patient information of dosing. Subjective adherence was assessed as secondary outcome by self-report questionnaires (at T-0 and T-28) and telephone interviews (at T-2 and T-16), where participants estimated their overall adherence on a scale from 0-100%.RESULTS AND DISCUSSION: A total of 450 patients were randomly allocated to intervention (N = 218, 48.4%) and control group (N = 232, 51.6%). Dropout rate was fairly low and comparable for both groups (N Int = 37 (17.0%), NCont = 41 (17.7%), p = 0.845). Main addressed drug-related problem (DRP) during PMC at T-0 was insufficient adherence to at least one medicine (N = 69, 26.7%). At T-28, 1020 chronic therapies fulfilled inclusion criteria for MPR calculation, representing 293 of 372 patients (78.8%). Mean MPR and adherence to polypharmacy (DPPR) for both groups were equally high (MPRInt = 88.3, SD = 19.03; MPRCont = 87.5, SD = 20.75 (p = 0.811) and DPPRInt = 88.0, SD = 13.31; DPPRCont = 87.5, SD = 20.75 (p = 0.906), respectively). Mean absolute change of subjective adherence between T-0 and T-2 was +1.03% in the intervention and -0.41% in the control group (p = 0.058). The number of patients reporting a change of their adherence of more than ±5 points on a scale 0-100% between T-0 and T-2 was significantly higher in the intervention group (NImprovement = 30; NWorsening = 14) than in the control group (NImprovement = 20; NWorsening = 24; p = 0.028).CONCLUSION: Through the PMC pharmacist were able to identify a significant number of DRPs. Participants showed high baseline objective adherence of 87.5%, providing little potential for improvement. Hence, no significant increase of objective adherence was observed. However, regarding changes in subjective adherence of more than ±5% the PMC showed a positive effect.TRIAL REGISTRATION: Clinical trial registry database, NCT01739816; first entry on November 27, 2012.

AB - BACKGROUND: In 2010 the 'Polymedication Check' (PMC), a pharmacist-led medication review, was newly introduced to be delivered independently from the prescriber and reimbursed by the Swiss health insurances. This study aimed at evaluating the impact of this new cognitive service focusing on medicines use and patients' adherence in everyday life.METHODS: This randomised controlled trial was conducted in 54 Swiss community pharmacies. Eligible patients used ≥4 prescribed medicines over >3 months. The intervention group received a PMC at study start (T-0) and after 28 weeks (T-28) while the control group received only a PMC at T-28. Primary outcome measure was change in patients' objective adherence, calculated as Medication Possession Ratio (MPR) and Daily Polypharmacy Possession Ratio (DPPR), using refill data from the pharmacies and patient information of dosing. Subjective adherence was assessed as secondary outcome by self-report questionnaires (at T-0 and T-28) and telephone interviews (at T-2 and T-16), where participants estimated their overall adherence on a scale from 0-100%.RESULTS AND DISCUSSION: A total of 450 patients were randomly allocated to intervention (N = 218, 48.4%) and control group (N = 232, 51.6%). Dropout rate was fairly low and comparable for both groups (N Int = 37 (17.0%), NCont = 41 (17.7%), p = 0.845). Main addressed drug-related problem (DRP) during PMC at T-0 was insufficient adherence to at least one medicine (N = 69, 26.7%). At T-28, 1020 chronic therapies fulfilled inclusion criteria for MPR calculation, representing 293 of 372 patients (78.8%). Mean MPR and adherence to polypharmacy (DPPR) for both groups were equally high (MPRInt = 88.3, SD = 19.03; MPRCont = 87.5, SD = 20.75 (p = 0.811) and DPPRInt = 88.0, SD = 13.31; DPPRCont = 87.5, SD = 20.75 (p = 0.906), respectively). Mean absolute change of subjective adherence between T-0 and T-2 was +1.03% in the intervention and -0.41% in the control group (p = 0.058). The number of patients reporting a change of their adherence of more than ±5 points on a scale 0-100% between T-0 and T-2 was significantly higher in the intervention group (NImprovement = 30; NWorsening = 14) than in the control group (NImprovement = 20; NWorsening = 24; p = 0.028).CONCLUSION: Through the PMC pharmacist were able to identify a significant number of DRPs. Participants showed high baseline objective adherence of 87.5%, providing little potential for improvement. Hence, no significant increase of objective adherence was observed. However, regarding changes in subjective adherence of more than ±5% the PMC showed a positive effect.TRIAL REGISTRATION: Clinical trial registry database, NCT01739816; first entry on November 27, 2012.

KW - Adolescent

KW - Adult

KW - Aged

KW - Counseling

KW - Databases, Factual

KW - Drug Utilization Review

KW - Female

KW - General Practice

KW - Hospitalization

KW - Humans

KW - Male

KW - Medication Adherence

KW - Middle Aged

KW - Patient Acceptance of Health Care

KW - Patient Dropouts

KW - Pharmacies

KW - Pharmacists

KW - Polypharmacy

KW - Prospective Studies

KW - Self Report

KW - Switzerland

KW - Young Adult

KW - Journal Article

KW - Multicenter Study

KW - Randomized Controlled Trial

KW - Research Support, Non-U.S. Gov't

U2 - 10.1186/s12913-016-1384-8

DO - 10.1186/s12913-016-1384-8

M3 - SCORING: Journal article

C2 - 27108410

VL - 16

SP - 145

JO - BMC HEALTH SERV RES

JF - BMC HEALTH SERV RES

SN - 1472-6963

ER -