The main aim of the current study is to investigate whether consuming grapes rich in flavonoids just before mental stress can protect cerebrovascular and peripheral vascular function, mood and cognition, from the negative effects of mental stress in young healthy adults. A second, exploratory aim, will further address whether quality of habitual diet, microbiome health (composition; metabolites production e.g. Short-chain fatty acids) and levels of cardiorespiratory fitness play a role on the beneficial effects of grapes during mental stress. All participants will receive a high-flavonoid grape intervention (60 g freeze-dried grape powder, equivalent to 300 g fresh grapes) and a low-flavonoid grape intervention (60 g powdere isocaloric-matched control). It is hypothesized that the high-flavonoid grape intervention will improve cortical oxygenation and cognitive function in the context of mental stress, and prevent the stress-induced decline in peripheral endothelial function following stress. Furthermore, it is hypothesized that individuals with poorer diets, cardiorespiratory fitness and a poorer gut microbiome will benefit more from the grape intervention in the context of mental stress.
Psychological stress is widespread in our societies, and has been extensively shown to have negative consequences for human health. Specifically, psychological stress induces significant declines in human vascular function, as measured by brachial Flow-mediated Dilatation (FMD). We have demonstrated that flavonoid interventions can prevent the harmful effects of stress on the vascular system. Indeed, flavonoid-rich interventions have also been extensively shown to improve peripheral and cerebrovascular function in the absence of stress. However, the effect of flavonoids on cerebrovascular function and cognition in the context of mental stress is unknown. In the proposed project, our key objectives are to investigate whether grape intake prior to a mental stress task results in better brain oxygenation and vascular function, which leads to improved cognitive performance and mood in young healthy adults. These data will establish whether grapes can be effective as a 'stress snack' to optimize cognitive and brain function in the context of psychological stress. Furthermore, we will explore whether there are certain participant characteristics that mediate the impact of grape flavonoids on cerebrovascular function and cognition in the context of mental stress. Such as, physical fitness (assessed by a VO2 max test), composition of gut microbiome (assessed by faecal sample), habitual diet (assessed by 3-day food diary and the food frequency questionnaire), and eating behaviour and chronic stress (assessed by the eating behaviour questionnaire and perceived stress scale). This work will be important to guide future dietary recommendations around stress and might ultimately result in increased intake of flavonoid-rich grapes and other flavonoid-rich fruits/vegetables overall.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
TRIPLE
Enrollment
44
High-flavonoid grape powder: 60 g, equivalent to 300 g fresh grapes. Total polyphenols: 437 mg/100g).
60 g powder isocaloric-matched control (Total polyphenols: \< 60 mg)
School of Sport, Exercise & Rehabilitation Sciences
Birmingham, West Midlands, United Kingdom
RECRUITINGPre-frontal cortical Tissue Oxygenation Index (NIRS) - TOI
Pre-frontal levels of Tissue Oxygenation Index (% TOI) will be assessed by functional Near-Infrared Spectroscopy (fNIRS). The NIRS device measures changes in chromophore concentrations of oxyhaemoglobin (O2Hb) and deoxyhaemoglobin (HHb), providing depth-resolved measures of total tissue oxygen saturation.
Time frame: Change from pre-intervention baseline to 1 hour post-intervention (during mental stress) and 1 hour 15 minutes post-intervention (during cognitive tasks, 10 minutes post-stress)
Pre-frontal cortical Tissue Oxygenation Index (NIRS) - O2Hb
Pre-frontal levels of oxygenated (O2Hb) haemoglobin concentration (μmol) will be assessed by functional Near-Infrared Spectroscopy (fNIRS).
Time frame: Change from pre-intervention baseline to 1 hour post-intervention (during mental stress) and 1 hour 15 minutes post-intervention (during cognitive tasks, 10 minutes post-stress).
Pre-frontal cortical Tissue Oxygenation Index (NIRS) - HHb
Pre-frontal levels of deoxygenated (HHb) haemoglobin concentration (μmol) will be assessed by functional Near-Infrared Spectroscopy (fNIRS).
Time frame: Change from pre-intervention baseline to 1 hour post-intervention (during mental stress) and 1 hour 15 minutes post-intervention (during cognitive tasks, 10 minutes post-stress).
Pre-frontal cortical Tissue Oxygenation Index (NIRS) - nTHI
Pre-frontal levels of normalised haemoglobin index (relative value of total haemoglobin normalised to the initial value, nTHI) content (a.u.) will be assessed by functional Near-Infrared Spectroscopy (fNIRS).
Time frame: Change from pre-intervention baseline to 1 hour post-intervention (during mental stress) and 1 hour 15 minutes post-intervention (during cognitive tasks, 10 minutes post-stress).
Flow-mediated dilatation (FMD) of the brachial artery
FMD of the brachial artery. Expressed as % FMD: change in brachial diameter from baseline to peak dilation following 5 minutes of arterial occlusion. Brachial artery diameter and blood flow will be measured using Doppler ultrasonography (uSmart 3300, Terason).
Time frame: Change from pre-intervention baseline to 2 hours and 2 hours 45 minutes post-intervention (45-90 minutes post-stress).
Common Carotid Artery (CCA) - Blood flow
Common Carotid Artery (CCA) blood flow velocity (ml min-1) will be measured using Doppler ultrasonography (uSmart 3300, Terason) interfaced with the Quipu analysis software. CCA blood flow is calculated using CCA blood velocity and diameter across 2 minutes of recording.
Time frame: Change from pre-intervention baseline to 2 hours and 2 hours 45 minutes post-intervention (45-90 minutes post-stress).
Common Carotid Artery (CCA) - Shear rate
Common Carotid Artery (CCA) shear rate (s-1) will be measured using Doppler ultrasonography (uSmart 3300, Terason) interfaced with the Quipu analysis software.
Time frame: Change from pre-intervention baseline to 2 hours and 2 hours 45 minutes post-intervention (45-90 minutes post-stress).
Executive Function (MANT) - Accuracy
Executive function accuracy will be measured using the Modified Attention Network Task (MANT) which measures response to cognitive load
Time frame: Change from pre-intervention baseline to 1 hour 15 minutes post-intervention (10 minutes post-stress).
Executive Function (Switch) - Accuracy
Executive function accuracy will be measured using the Switch Task which considers cognitive flexibility.
Time frame: Change from pre-intervention baseline to 1 hour 15 minutes post-intervention (10 minutes post-stress).
Executive Function (MANT) - Reaction time
Executive function reaction time will be measured using Modified Attention Network Task (MANT) which measures response to cognitive load.
Time frame: Change from pre-intervention baseline to 1 hour 15 minutes post-intervention (10 minutes post-stress).
Executive Function (Switch) - Reaction time
Executive function reaction time will be measured using the Switch Task which considers cognitive flexibility.
Time frame: Change from pre-intervention baseline to 1 hour 15 minutes post-intervention (10 minutes post-stress).
Executive Function (MANT) - Inverse Efficiency Score
Executive function inverse efficiency will be measured using the Modified Attention Network Task (MANT), calculated by dividing task reaction time by task accuracy.
Time frame: Change from pre-intervention baseline to 1 hour 15 minutes post-intervention (10 minutes post-stress).
Executive Function (Switch) - Inverse Efficiency Score
Executive function inverse efficiency will be measured using the Switch Task, calculated by dividing task reaction time by task accuracy.
Time frame: Change from pre-intervention baseline to 1 hour 15 minutes post-intervention (10 minutes post-stress).
Mood (POMS)
Mood (total mood disturbance, TMD) will be assessed by the questionnaire Profile-of-Mood-States (POMS).
Time frame: Change from pre-intervention baseline to 1 hour post-intervention (immediately following stress), 2 hours and 2 hours 45 minutes post-intervention (45-90 minutes post-stress).
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