Hypercholesterolemia Clinical Trial
Official title:
Pilot Study: Statin Therapy to Improve Medication Adherence
The purpose of this pilot study is to examine if using genetics can improve statin adherence in patients who should be taking statins but are not because of prior side effects with statins. This study will assist physicians in making a personalized health care plan for prevention of cardiovascular disease.
HMG Co-A reductase inhibitors ("statins") are commonly prescribed to lower low density
lipoprotein cholesterol (LDLc) and to prevent cardiovascular disease (CVD), a leading cause
of morbidity and mortality. Long-term adherence to statins in the primary care environment
is challenging; consequences of statin non-adherence include higher LDLc levels,
hospitalizations, costs, and death due to CVD.
Medication non-adherence is complex and multifactorial and can be associated with a number
of factors including medication cost, complexity of medication regimen, poor
provider-patient relationship / communication, and adverse side effects. For statins, side
effects such as muscle aches, cramping, and pain (referred to broadly as statin-related
myopathy) are a frequent cause of non-adherence. These symptoms are non-specific and are
frequent reasons for stopping statin therapy, due to patient or provider concern about the
possibility of statin-related myopathy. Many patients may be needlessly deprived of the
cardiovascular benefits of long-term statin use.
A genetic risk factor for statin myopathy and subsequent non-adherence has recently been
identified. In a genome-wide association study, a genetic variant (named SLCO1B1*5) was a
main contributor of statin myopathy. It was demonstrated that the SLCO1B1*5 variant is not
only a predictor of myopathy, but also of premature statin discontinuation. The risk with
the *5 allele is statin specific: greatest with simvastatin and atorvastatin use, the least
with pravastatin or rosuvastatin. Therefore, the SLCO1B1*5 variant is common, can predict
myopathy, subsequent non-adherence, and due to its statin-specific effects creates a novel
research paradigm for personalizing statins to an individual's genetic profile. Carriers of
the SLCO1B1*5 variant may do best on rosuvastatin, pravastatin, or fluvastatin whereas
non-carriers may be treated with any statin.
Specific Aims:
Aim 1: To measure the effect of genotype-guided statin prescription on patients' concerns
regarding the risks of statin therapy.
Aim 2: To measure and compare the effect of genotype-guided statin prescription to
non-guided therapy on statin adherence in patients who are currently not adherent to
statins.
The approach for this pilot study is to recruit 100 Duke University Health System (DUHS)
patients who receive care at Duke Primary Care at Pickett Road (DPC) or Center for Living
(CFL) clinics that have an indication for statin therapy to reduce cardiovascular risk, but
are not currently taking a statin. Consented patients will be genotyped for the SLCO1B1*5
allele at the Duke Molecular Diagnostics Laboratory. Test results will be returned first to
the provider along with genotype-specific strategies to revise and/or provide a new
prescription for statin therapy and next to the patient along with genotype-specific
information about their personal risk of side effects on certain statin therapies. The
primary outcome measures will be collected through the use of online surveys administered to
patients at two time points: 1) before genetic testing and 2) 4-months after testing.
Additional survey elements to address the patient's demographics, beliefs and concerns about
medications, history with prescription drugs (e.g., side effects and general compliance) and
overall experience with genetic testing during the study will be administered as well. It is
possible that subjects will re-experience symptoms of their prior statin-intolerance when
re-challenged with statins as part of this study. By avoiding certain types of statins (i.e.
simvastatin and atorvastatin) in carriers of the SLCO1B1*5 genetic variant and using those
statins (i.e. pravastatin and rosuvastatin) that in placebo controlled trials have no
increased risk of adverse events, this risk may be less likely.
Age-, sex-, diagnosis-, and provider-matched concurrent and historical controls will be
created in order to compare genetically-guided with non-genetically guided therapy
;
Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Prevention
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