PMID- 27579830
OWN - NLM
STAT- MEDLINE
DCOM- 20170428
LR  - 20230805
IS  - 2376-1032 (Electronic)
IS  - 2376-0540 (Print)
IS  - 2376-0540 (Linking)
VI  - 22
IP  - 9
DP  - 2016 Sep
TI  - Estimated Budget Impact of Increased Use of Mirabegron, A Novel Treatment for 
      Overactive Bladder.
PG  - 1072-84
LID - 10.18553/jmcp.2016.22.9.1072 [doi]
AB  - BACKGROUND: Oral pharmacological treatment for overactive bladder (OAB) consists 
      of antimuscarinics and the beta-3 adrenergic agonist mirabegron. Antimuscarinic 
      adverse events (AEs) such as dry mouth, constipation, and blurry vision can 
      result in frequent treatment discontinuation rates, leaving part of the OAB 
      population untreated. Antimuscarinics also contribute to a patient's 
      anticholinergic cognitive burden (ACB), so the Beers Criteria recommends cautious 
      use of antimuscarinics in elderly patients who take multiple anticholinergic 
      medications or have cognitive impairment. Since mirabegron does not affect the 
      cholinergic pathways, it is unlikely to contribute to a patient's ACB. OBJECTIVE: 
      To estimate the health care costs associated with the pharmacological treatment 
      of OAB with mirabegron and antimuscarinics from U.S. commercial payer and 
      Medicare Advantage perspectives, using a budget impact model. METHODS: For this 
      budget impact model, 2 analyses were performed. The primary analysis estimated 
      the budgetary impact of increasing the use of mirabegron in a closed patient 
      cohort treated with oral pharmacological treatments. The secondary analysis 
      modeled the economic impact in an open cohort by allowing untreated patients to 
      begin treatment with mirabegron after potential contraindication, intolerance, or 
      lack of effectiveness of antimuscarinics. The analyses were performed over a 
      3-year time horizon. The economic impact of increased mirabegron use was 
      quantified using direct medical costs, including prescription costs and health 
      resource utilization (HRU) costs. Costs of comorbidities included pharmacy and 
      medical costs of treating OAB-related urinary tract infections (UTI), skin 
      rashes, and depression. An analysis of a large single-site integrated health 
      network database was commissioned to quantify ACB-related HRU in terms of the 
      increases in yearly outpatient and emergency department visits. Based on this 
      analysis, the model associated each unit increase in ACB score with increased HRU 
      and probability of mild cognitive impairment. Clinical outcomes of increased use 
      of mirabegron were presented as the number of AEs and comorbidity episodes that 
      could be avoided. One-way sensitivity analyses were performed to quantify the 
      expected budget impact over the range of uncertainty for the key input variables. 
      RESULTS: Primary analysis calculated the impact of increasing the use of 
      mirabegron from 4.5% to 5.3%, 7.1%, and 9.4% in years 1, 2, and 3, respectively, 
      among oral pharmacological OAB treatments that included generic and branded 
      antimuscarinics: oxybutynin, tolterodine, trospium, darifenacin, fesoterodine, 
      and solifenacin. For a 1 million-member U.S. commercial payer plan, the total 
      prescription costs increased, and the total medical costs decreased during the 
      3-year time horizon, yielding increases of $0.005, $0.016, and $0.031 from 
      current per member per month (PMPM) costs and $0.90, $2.92, and $5.53 from 
      current per treated member per month (PTMPM) costs, an average of less than 2% of 
      current OAB treatment costs. For the Medicare Advantage plan, the resulting 
      incremental PMPM costs were $0.010, $0.034, and $0.065, and the incremental PTMPM 
      costs were $0.93, $3.04, and $5.76; all were less than 4% of the current cost. 
      The secondary analysis estimated the budgetary effects of reducing the untreated 
      population by 1% annually by initiating treatment with mirabegron. For a 
      commercial payer, this resulted in PMPM cost increases of $0.156, $0.311, and 
      $0.467 from the current value, while the incremental PTMPM cost increased by 
      $6.17, $11.67, and $16.61. For the Medicare Advantage plan, the incremental 
      increases in PMPM costs were $0.277, $0.553, and $0.830, and in PTMPM costs were 
      $6.42, $12.15, and $17.29. Clinically, treating more OAB patients resulted in 
      fewer OAB-related comorbidities from both health plan perspectives, since most 
      events associated with nontreatment could be avoided. In the Medicare Advantage 
      population of the secondary analysis, the total numbers of avoided events were 
      predicted as 452 UTIs, 2,598 depression diagnoses, and 3,020 skin rashes during 
      the time horizon of the model. CONCLUSIONS: Mirabegron addresses an unmet need 
      for therapy for certain OAB patients, for whom antimuscarinics are not 
      recommended because of a risk of cognitive impairment and who are intolerant to 
      the anticholinergic AEs. Using mirabegron involves moderate additional economic 
      cost to a commercial or Medicare Advantage health plan for which medical cost 
      savings can offset a substantial part of increased pharmacy costs. DISCLOSURES: 
      Funding for this study was provided by Astellas. Perk, Wielage, T. Klein, and R. 
      Klein are employed by Medical Decision Modeling, a contract research company that 
      was paid to perform the described outcomes research and build the model contained 
      in this study. Campbell and Perkins are employed by the Regenstrief Institute, 
      which conducted a database analysis for this research. Campbell reports 
      consultancy fees from Astellas, as well as pending grants from Merck, Sharpe, and 
      Dohme Corp. Posta, Yuran, and Ng are employed by Astellas Pharma Global 
      Development, the developer of mirabegron. Study concept and design were 
      contributed by Perk, Wielage, R. Klein, and Ng. Campbell, T. Klein, and Perkins 
      took the lead in data collection, assisted by Perk, Wielage, and Ng. Data 
      interpretation was performed by Posta and Yuran, along with Perk, Wielage, R. 
      Klein, Ng, Campbell, and Perkins. The manuscript was written by Perk and R. 
      Klein, along with Wielage, T. Klein, Posta, Yuran, and Ng, and revised by all the 
      authors.
FAU - Perk, Sinem
AU  - Perk S
AD  - 1 Medical Decision Modeling, Indianapolis, Indiana.
FAU - Wielage, Ronald C
AU  - Wielage RC
AD  - 1 Medical Decision Modeling, Indianapolis, Indiana.
FAU - Campbell, Noll L
AU  - Campbell NL
AD  - 2 Center for Aging Research, Regenstrief Institute, Indianapolis, Indiana, and 
      Purdue University College of Pharmacy, West Lafayette, Indiana.
FAU - Klein, Timothy M
AU  - Klein TM
AD  - 1 Medical Decision Modeling, Indianapolis, Indiana.
FAU - Perkins, Anthony
AU  - Perkins A
AD  - 3 Center for Aging Research, Regenstrief Institute, Indianapolis, Indiana.
FAU - Posta, Linda M
AU  - Posta LM
AD  - 4 Medical Affairs, Americas, Astellas Pharmaceutical Global Development, 
      Northbrook, Illinois.
FAU - Yuran, Thomas
AU  - Yuran T
AD  - 4 Medical Affairs, Americas, Astellas Pharmaceutical Global Development, 
      Northbrook, Illinois.
FAU - Klein, Robert W
AU  - Klein RW
AD  - 1 Medical Decision Modeling, Indianapolis, Indiana.
FAU - Ng, Daniel B
AU  - Ng DB
AD  - 4 Medical Affairs, Americas, Astellas Pharmaceutical Global Development, 
      Northbrook, Illinois.
LA  - eng
PT  - Journal Article
PL  - United States
TA  - J Manag Care Spec Pharm
JT  - Journal of managed care & specialty pharmacy
JID - 101644425
RN  - 0 (Acetanilides)
RN  - 0 (Muscarinic Antagonists)
RN  - 0 (Thiazoles)
RN  - 0 (Urological Agents)
RN  - MVR3JL3B2V (mirabegron)
SB  - IM
MH  - Acetanilides/*economics/therapeutic use
MH  - Adult
MH  - Aged
MH  - Aged, 80 and over
MH  - *Budgets/trends
MH  - *Health Care Costs/trends
MH  - Humans
MH  - Insurance, Health/economics/trends
MH  - Medicare Part C/economics/trends
MH  - Middle Aged
MH  - Muscarinic Antagonists/economics/therapeutic use
MH  - Thiazoles/*economics/therapeutic use
MH  - Treatment Outcome
MH  - United States/epidemiology
MH  - Urinary Bladder, Overactive/drug therapy/*economics/epidemiology
MH  - Urological Agents/*economics/therapeutic use
PMC - PMC10397927
COIS- Funding for this study was provided by Astellas. Perk, Wielage, T. Klein, and R. 
      Klein are employed by Medical Decision Modeling, a contract research company that 
      was paid to perform the described outcomes research and build the model contained 
      in this study. Campbell and Perkins are employed by the Regenstrief Institute, 
      which conducted a database analysis for this research. Campbell reports 
      consultancy fees from Astellas, as well as pending grants from Merck, Sharpe, and 
      Dohme Corp. Posta, Yuran, and Ng are employed by Astellas Pharma Global 
      Development, the developer of mirabegron. Study concept and design were 
      contributed by Perk, Wielage, R. Klein, and Ng. Campbell, T. Klein, and Perkins 
      took the lead in data collection, assisted by Perk, Wielage, and Ng. Data 
      interpretation was performed by Posta and Yuran, along with Perk, Wielage, R. 
      Klein, Ng, Campbell, and Perkins. The manuscript was written by Perk and R. 
      Klein, along with Wielage, T. Klein, Posta, Yuran, and Ng, and revised by all the 
      authors.
EDAT- 2016/09/01 06:00
MHDA- 2017/04/30 06:00
PMCR- 2016/09/01
CRDT- 2016/09/01 06:00
PHST- 2016/09/01 06:00 [entrez]
PHST- 2016/09/01 06:00 [pubmed]
PHST- 2017/04/30 06:00 [medline]
PHST- 2016/09/01 00:00 [pmc-release]
AID - 10.18553/jmcp.2016.22.9.1072 [doi]
PST - ppublish
SO  - J Manag Care Spec Pharm. 2016 Sep;22(9):1072-84. doi: 
      10.18553/jmcp.2016.22.9.1072.