Standardized Educational Plan for Epilepsy Patients With Comorbidities

Epilepsy Clinical Trial

— EDU-COM  

Official title:

Comprehensive Information Imparted to Patients With Epilepsy and Comorbidity and Decreased Prevalence of Adverse Treatment Effects. The EDU-COM Study.

Clinical Trial Details — Status: Completed

Administrative data

• NCT number: NCT01804322
• Other study ID #: FARM77RW2S
• Status: Completed
• Phase: Phase 4
• First received: March 1, 2013
• Last updated: March 5, 2013
• Start date: February 2009
• Est. completion date: September 2012

Study information

• Verified date: March 2013
• Source: San Gerardo Hospital
• Contact: n/a
• Is FDA regulated: No
• Health authority: Italy: The Italian Medicines Agency
• Study type: Interventional

Clinical Trial Summary

Epilepsy requires long-term drug treatment and is frequently associated with other clinical conditions. Combinations of antiepileptic drugs and other compounds are fairly common and increase with age. Adverse drug reactions and drug interactions are expected and may affect compliance, particularly in patients not receiving adequate information. Primary objective of the study is to verify if a comprehensive and standardized educational plan is followed by a significant reduction of the number of adult patients with epilepsy and comorbidity presenting clinically relevant adverse treatment effects. Secondary objectives include effects on number of adverse treatment events, health-related quality of life (HRQOL), direct medical costs, and patient's compliance. The study is a randomized, controlled, open-label, pragmatic trial. Included are consecutive adult outpatients with 1+ concurrent clinical conditions on chronic treatment and at least one clinically relevant treatment-related adverse event and/or clinically relevant drug interaction. Eligible patients will be randomized to receive a comprehensive and standardized educational plan (experimental arm) or to usual care, ie management of adverse event/drug interaction as done in clinical practice (control arm). The experimental plan consists in discussing with patient and caregiver the cause and nature of adverse event/drug interaction, the tolerability profile of each drug, the clinical manifestations associated with current drug interaction(s), contraindications of potentially interfering over-the-counter drugs, indications and benefits of suggested treatment changes, and withdrawal of potentially interfering, contraindicated or ineffective drugs. All patients will be seen at one, three and six months after admission.

Expected results: The number of patients free from clinically relevant adverse treatment events and/or drug interactions in each treatment arm at end of study is expected to be higher in patients assigned to comprehensive and standardized educational plan compared to usual care (primary outcome). Patients on the experimental plan are also expected to be more commonly free from relevant adverse events and/or drug interactions at each intermediate visit, to present a lower number of adverse treatment events, to imply lower costs for medical contacts, hospital admissions, and drugs, to present better HRQOL scores, and to present less weekly treatment omissions.

Description:

OBJECTIVES OF THE STUDY The primary objective of the study is to verify whether or not a comprehensive and standardized educational plan is followed by a significant reduction of the number of adult patients with epilepsy and comorbidity presenting clinically relevant adverse treatment effects.

Secondary objectives include the effects of the following comprehensive and standardized educational plan:

• Reduction of the total number of adverse treatment events

• Reduction of the number of medical contacts

• Improvement of the health-related quality of the patient's life (HRQOL)

• Reduction of the direct costs of the health care assistance

• Improvement of the patient's compliance

The hypothesis to be tested is that a comprehensive and standardized educational plan is superior to the present modalities adopted to manage treatment safety in clinical practice for the following reasons:

• It raises the level of attention towards the putative adverse effects of the drugs currently taken and the possible drug interactions

• It helps identifying any clinically relevant event at onset to prevent the occurrence of symptoms or signs leading to medical contact and hospital admission

• It educates the patient to live with the treatment schedule representing the best compromise in terms of safety

METHODS Study design. This is a randomized, controlled, open-label, pragmatic trial. Study population. Patients eligible for inclusion are identified among those consecutively seen in the outpatient services of the participating units.

Intervention. Patients fulfilling the inclusion/exclusion criteria will be randomized to receive a comprehensive and standardized educational plan (experimental arm) or to usual care, ie the management of the adverse event/drug interaction as usually done in clinical practice and in keeping with each unit's modalities (control arm).

The comprehensive and standardized educational plan consists in the discussion with the patient and, if available, the caregiver of each of the following points (of which a written summary will be made available:

• The cause and nature of the adverse event and/or drug interaction

• The tolerability profile of each drug present in the schedule, illustrated as a simple list including the commonest adverse events presented in decreasing order of frequency

• The clinical manifestations (if any) associated with the current drug interaction(s)

• Any contraindication to the use of over-the-counter drugs potentially interfering with the current treatment schedule

• The reasons for and the potential benefits of the suggested treatment change

• An encouragement to withdraw any potentially interfering or contraindicated drug or compounds not unequivocally found to be efficacious for that specific case

Study conduction. After signing the informed consent form, eligible patients will be immediately randomized to receive the comprehensive and standardized educational plan or to usual care. Patients assigned to the experimental arm will be given an appointment for a one-hour private meeting to discuss all the items included in the comprehensive educational plan. The patients assigned to the control arm will be managed as done in the context of usual care in that same ambulatory visit. All patients will be seen at one, three and six months after admission and whenever indicated for the management of the individual case.

Outcomes. These include one primary and a number of secondary outcomes. The primary outcome is defined by the number of patients free from clinically relevant adverse treatment events and/or the number of drug interactions in each treatment arm at end of study.

Secondary outcomes include the following:

• The number of patients free from clinically relevant adverse treatment events and/or drug interactions in each treatment arm at each intermediate visit

• The mean and median number of adverse treatment events in each treatment arm, at each intermediate visit and at end of study

• The monetary costs of medical contacts, hospital admissions, and drugs; the one-hour meetings with patients assigned to the experimental arm will be included in the costs. Costs will be calculated by the healthcare economy service of Mario Negri Institute according to current national values.

• Total HRQOL summary score changes (comparing last follow-up to admission visit)

• Number of patients with at least weekly omissions of the assigned treatment schedules

Randomization. A centralized randomization procedure will be adopted. Randomization will be performed by accessing to a user-friendly, protected centralized database, which will proceed to the assignment to the experimental or control arm after verification of the appropriateness of the inclusion/exclusion criteria. To control for center-related confounding, a separate randomization list will be made available for each center.

Blinding (masking). For the purposes of the study, treating and evaluating physicians will be represented by different persons. Given the diversity between the two management policies, neither the patients nor the caring physicians involved in administering interventions will be blind to the assigned arm. An attempt will be made to blind physicians assessing outcomes.

Statistical analysis. The data will be analyzed using the SPSS-13 package for PC. The statistical analysis plan will include descriptive statistics to compare the baseline characteristics of the two populations and the distribution of the treatment schedules, the number and type of adverse events (present at baseline or occurring during follow-up), and the proposed changes, along with the cost items (medical contacts, hospitalizations, drug costs) and the HRQOL scores. For descriptive statistics, the chi-square test, the Student's t test, the analysis of variance (ANOVA) or equivalent non parametric tests will be used as appropriate. The chi-square test will be also used to test the number of patients free from relevant adverse events at end of study (primary end-point) and at each intermediate visit. The analysis of the primary end-point is based on the intention-to-treat analysis and includes all randomized patients. Repeated measures ANOVA will be used to compare the difference between the two treatment arms in the mean change in the number of adverse events, the number of omitted drug doses, the total monetary costs, and the total HRQOL scores at each follow-up visit (where applicable) and at study end.

Timing. The duration of the entire study is 24 months with the following distribution:

• Months 1-3: Protocol approval by the local units' ethics committees and preparation of the electronic database

• Months 4-15: Patients' enrolment

• Months 16-21: Completion of follow-up

• Months 22-24: Data analysis and scientific report An interim assessment of the recruitment rate will be performed at the end of month 12 to decide whether or not the enrolment can be completed as expected. If needed, a request will be made to postpone patients' enrolment to the end of month 21 and the study completion of the end of month 30.

Ethical aspects. Each eligible patient will be properly informed about the study aims, the use of the diaries, and the requirements to be met at each visit. A summary sheet outlining the study objectives and conduct will be given to the patient and will be part of the written informed consent form. The patient will be also instructed about the possibility to withdraw from the study for any plausible reason without any interference with the management of his/her disease as done in clinical practice. The confidentiality of the data collected for the study purposes will be granted by giving access (through nominal username and password) only to persons officially involved in the study conduction. The data will be managed without disclosing the patients' identity.

Recruitment information / eligibility

• Status: Completed
• Enrollment: 187
• Est. completion date: September 2012
• Est. primary completion date: December 2011
• Accepts healthy volunteers: No
• Gender: Both
• Age group: 18 Years and older

Eligibility

Inclusion Criteria:

• Age 18 years or older

• Presence of one or more concurrent clinical conditions requiring chronic treatment (ie, daily treatment lasting one month or longer)

• At least one clinically relevant adverse event attributable to the present treatment(s) and/or a clinically relevant drug interaction; for the purposes of this study, a clinically relevant adverse event is any symptom and/or clinical and/or laboratory sign requiring treatment change; a clinically relevant drug interaction is an interaction requiring active monitoring and/or treatment change

• The treatment schedule can be modified to eliminate adverse event(s) and/or risky drug interactions; the decision to modify the treatment is left to the caring physician's judgment

Exclusion Criteria:

• Age younger than 18 years

• Absence of concurrent chronic treatments

• Presence of polytherapy with AEDs unassociated to treatments for concurrent (non-epileptic) disorders

• The treatment schedule cannot be changed even at the presence of clinically relevant adverse events

• Patient is unable to understand or comply with an educational plan; the application of this exclusion criterion is left to the caring physician's judgment

• Patient or caregiver is unwilling to release a written informed consent

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Single Blind (Outcomes Assessor), Primary Purpose: Treatment

Related Conditions & MeSH terms

• Epilepsy

Intervention

Other:
• Standardized educational plan
The comprehensive and standardized educational plan consists in the discussion with the patient each of the following points: The cause and nature of the adverse event and/or drug interaction The tolerability profile of each drug present in the schedule The clinical manifestations associated with the current drug interactions Any contraindication to the use of over-the-counter drugs potentially interfering with the current treatment schedule The reasons for and the potential benefits of the suggested treatment change An encouragement to withdraw any potentially interfering or contraindicated drug
• usual care
usual care according to the participating Epilepsy Centers

Locations

Country	Name	City	State
Italy	Azienda Ospedaliera San Gerardo, Central Contact (9 recruting centers)	Monza	MB

Sponsors (2)

Lead Sponsor	Collaborator
San Gerardo Hospital	Agenzia Italiana del Farmaco

Country where clinical trial is conducted

Italy, 

Outcome

Type	Measure	Description	Time frame	Safety issue
Other	The monetary costs of medical contacts, hospital admissions, and drugs; the one-hour meetings with patients assigned to the experimental arm will be included in the costs		6 months	No
Primary	The primary outcome is defined by the number of patients free from clinically relevant adverse treatment events and/or drug interactions in each treatment arm at end of study.		6 months	Yes
Secondary	The mean and median number of adverse treatment events in each treatment arm, at each intermediate visit and at end of study		6 months	Yes
Secondary	Total HRQOL summary score changes (comparing last follow-up to admission visit		6 months	No
Secondary	The mean and median number of drug interactions in each treatment arm, at each intermediate visit and at end of study		6 months	Yes