Aromatase inhibitors are the most used endocrine therapy for hormone-positive breast cancer. Despite the evidence that aromatase inhibitor therapy is associated with increased risk of cardiovascular events, potentially related to the duration of use, no studies have been conducted to characterize the long-term effects of aromatase inhibitor therapy on the heart or vessel structure and function as underlying determinants of cardiovascular mortality. This study will characterize the long-term effects of aromatase inhibitor therapy on established and novel health indices for CVD in breast cancer patients, by examining cross-sectionally compare health indices 1-, 5- and 10-years post-diagnosis in breast cancer survivors to controls. Specifically, our objectives are as follows: 1. To examine the effects of aromatase inhibitor therapy on early risk indicators for cardiovascular disease in the peripheral vasculature and heart, including aortic stiffness (primary outcome) and secondary outcomes of peripheral and carotid artery stiffness, blood biomarkers (lipids), blood pressure, carotid intima media thickness, endothelial function, and left ventricular ejection fraction, global longitudinal strain, and left ventricular diastolic function, in breast cancer survivors compared to controls. 2. To examine the effects of aromatase inhibitor therapy on factors related to cerebrovascular health, autonomic regulation, and cognitive function, including BDNF, heart rate variability, cerebrovascular function in response to a supine-sit-stand maneuver and squatting challenge, and a core battery of cognitive function tests, in breast cancer survivors compared to controls. 3. To examine the effects of aromatase inhibitor therapy on body composition, bone mineral density, and protein metabolism, in breast cancer survivors compared to controls. 4. To examine the effects of aromatase inhibitor therapy on lifestyle factors (behavioural), including diet, physical activity (including cardiorespiratory fitness), sleep, stress, and quality of life, in breast cancer survivors compared to controls. The investigators hypothesize that biologic and behavioural cardiovascular health indices will be deteriorated relative to controls as early as 1 year post-diagnosis and that prolonged use will further accelerate aging-related impairments.
Study Type
OBSERVATIONAL
Enrollment
112
Breast cancer survivors will have received usual care aromatase inhibitors for up to 10 years post-diagnosis.
University of Toronto
Toronto, Ontario, Canada
RECRUITINGAortic Stiffness
Aortic stiffness, measured non-invasively by pulse wave velocity, will be assessed using applanation tonometry.
Time frame: Day 2 (In-Person Session)
Brachial Artery Endothelial Function
Endothelial function will be assessed using the gold standard method of flow mediated dilation (FMD) using non-invasive duplex ultrasound (GE Vivid IQ) and edge-tracking software.
Time frame: Day 2 (In-Person Session)
Carotid Artery Stiffness
Functional assessment of the carotid artery stiffness will be assessed using B-mode ultrasound and artery edge-tracking software
Time frame: Day 2 (In-Person Session)
Carotid Intima Media Thickness
Structural assessment of the carotid artery thickness will be assessed using B-mode ultrasound and artery edge-tracking software
Time frame: Day 2 (In-Person Session)
Arterial Stiffness
Measured by Pulse Wave Velocity (PWV) of the arm and leg
Time frame: Day 2 (In-Person Session)
Left Ventricular Ejection Fraction (LVEF)
Cardiac outcomes will be assessed via echocardiography (GE Vivid IQ) and analyzed using Echopac software, represented as a % using the following formula: stroke volume/end diastolic volume x 100%.
Time frame: Day 2 (In-Person Session)
Global Longitudinal Strain
Cardiac outcomes will be assessed via echocardiography (GE Vivid IQ) and analyzed using Echopac software, expressed as a percentage of the relative change in length of the left ventricle through a cardiac cycle.
Time frame: Day 2 (In-Person Session)
Left Ventricular Diastolic Function
Cardiac outcomes will be assessed via echocardiography (GE Vivid IQ) and analyzed using Echopac software, assessed by the ratio of peak early diastolic velocity to peak mitral valve velocity (E/A ratio).
Time frame: Day 2 (In-Person Session)
Cerebrovascular Response
Cerebral blood flow velocity response (delta change compared to rest) of the middle cerebral artery will be assessed using transcranial Doppler ultrasound (Neurovision Transcranial Doppler System Model 500M) in accordance with recent guidelines, in response to postural changes (sit-to-stand) and exercise (squatting).
Time frame: Day 2 (In-Person Session)
Brain derived neurotrophic factor
Brain derived neurotrophic factor will be assessed via fasted venipuncture using in-house assays.
Time frame: Day 2 (In-Person Session)
Lipid profile
HDL, LDL, total Cholesterol, Triglycerides analyzed from blood serum using a clinical assay at a core lab.
Time frame: Day 2 (In-Person Session)
Hemoglobin A1c
Analyzed from blood plasma using a clinical assay at a core lab.
Time frame: Day 2 (In-Person Session)
Insulin resistance
Calculated as Homeostatic Model Assessment for Insulin Resistance (HOMA-IR) from fasting blood measures of glucose and insulin, analyzed using a clinical assay at a core lab.
Time frame: Day 2 (In-Person Session)
Protein metabolism
Analyzed from breathing test and urine sample before and after the participant consume a test protein drink.
Time frame: Day 1 (At-Home Session)
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