Targeting Oxidative Stress to Prevent Vascular and Skeletal Muscle Dysfunction During Disuse

NCT ID: NCT04351113

Last Updated: 2025-04-23

Basic Information

• Recruitment Status: RECRUITING
• Clinical Phase: NA
• Total Enrollment: 72 participants
• Study Classification: INTERVENTIONAL
• Study Start Date: 2019-09-01
• Study Completion Date: 2025-12-31

Brief Summary

Prolonged periods of reduced activity are associated with decreased vascular function and muscle atrophy. Physical inactivity due to acute hospitalization is also associated with impaired recovery, hospital readmission, and increased mortality. Older adults are a particularly vulnerable population as functional (vascular and skeletal muscle mitochondrial dysfunction) and structural deficits (loss in muscle mass leading to a reduction in strength) are a consequence of the aging process. The combination of inactivity and aging poses an added health threat to these individuals by accelerating the negative impact on vascular and skeletal muscle function and dysfunction. The underlying factors leading to vascular and skeletal muscle dysfunction are unknown, but have been linked to increases in oxidative stress. Additionally, there is a lack of understanding of how vascular function is impacted by inactivity in humans and how these changes are related to skeletal muscle function. It is our goal to investigate the mechanisms that contribute to disuse muscle atrophy and vascular dysfunction in order to diminish their negative impact, and preserve vascular and skeletal muscle function across all the lifespan.

Detailed Description

Disuse following injury or during acute hospitalization is associated with a host of negative outcomes including functional deficiencies, hospital readmission, disability, and increased mortality. Older adults are a particularly vulnerable population as functional (vascular and skeletal muscle dysfunction) and structural deficits (loss in muscle mass leading to a reduction in strength) are present as a consequence of the aging process. Any additional and accelerated insult caused by disuse poses a serious health threat to these older individuals by depleting their already diminished physiological and functional reserve and hastening the onset of disability. Current strategies aimed at preserving function during disuse have focused on preserving skeletal muscle mass and strength while the critical role of the vasculature has been largely ignored. Moreover, the underlying cause of dysfunction has not been adequately addressed in humans. This disintegrated and myopic approach likely contributes to the fact that interventions capable of preserving health during disuse do not exist. The vascular and skeletal muscle systems are inextricably linked to optimal mobility through oxygen and nutrient delivery, thus, vascular dysfunction likely contributes to and exacerbates skeletal muscle deficiencies that occur during disuse. To fully understand the impact of disuse on health and mobility and develop effective countermeasures it is our contention that both the vascular and musculoskeletal systems must be examined and the root cause of the problem must be addressed. While the underlying factors leading to these accelerated losses during disuse are unknown, they appear to be mechanistically linked to oxidative stress.

The long term goal is to minimize losses in vascular and skeletal muscle function that occur during disuse in order to maintain functional reserve and avoid serious adverse events. The objective here, which is the next step in pursuit of this goal, is to determine how oxidative stress contributes to disuse-induced vascular and skeletal muscle dysfunction. It is our central hypothesis that oxidative stress triggers the accelerated declines in vascular and skeletal muscle function during disuse. To test this hypothesis and provide compelling evidence that oxidative stress is the trigger of dysfunction the investigators will utilize two novel and fundamentally distinct strategies to improve redox balance during disuse. In Aim 1, the mitochondrial targeted antioxidant (MITO-AO) mitoquinone will be administered during disuse to improve free radical scavenging at the level of the mitochondria. In Aim 2, activation of Nuclear Factor Erythroid-2-like 2 (Nrf2) the "master regulator of antioxidant enzymes" will be accomplished with PB125 (a novel naturally occurring Nrf2 activator) to augment endogenous antioxidant defense systems. The impact of these interventions on measures of isolated and integrated vascular and skeletal muscle function before and after disuse will be examined. The central hypothesis is supported by preliminary data reporting substantial losses in vascular and skeletal muscle function and concomitant increases in oxidative stress following 5 days of bed rest. Importantly, MITO-AO prevents disuse-induced losses in muscle mass and restores age-related deficits in vascular function in aged animals and humans (preliminary data). Additionally, PB125 activates the Nrf2 pathway at multiple control points resulting in prolonged and amplified activation and subsequent gene expression of key antioxidant enzymes leading to a decrease in oxidative stress in humans (preliminary data).

Conditions

Aging; Oxidative Stress; Vascular Endothelium; Skeletal Muscle; Antioxidants

Study Design

• Allocation Method: RANDOMIZED
• Intervention Model: PARALLEL
• Primary Study Purpose: DIAGNOSTIC
• Blinding Strategy: DOUBLE

Study Groups

MITO-AO

Healthy older adult subjects ages 65-75 will take the supplement MITO-AO during a 5 day bed rest and will be assessed for vascular function independent of metabolism with passive leg movement (PLM), skeletal muscle bioenergetics independent of vascular constraints (i.e. blood flow and O2 supply) with phosphorous magnetic resonance spectroscopy (31P-MRS), and skeletal muscle bioenergetics under normal blood flow and O2 supply.

Group Type: EXPERIMENTAL

MITO-AO

Intervention Type: DIETARY_SUPPLEMENT

Participants will receive 160 mg with breakfast on day 1 of bed rest and 40 mg with breakfast on days 2-5.

Passive Leg Movement (PLM)

Intervention Type: OTHER

Participants will be tested for passive leg movement on baseline day 1, bed rest day 1, and post bed rest.

Plantar flexion

Intervention Type: OTHER

Participants will undergo plantar flexion on baseline day 2, pre bed rest, and post bed rest.

Isometric knee extensor test

Intervention Type: OTHER

Participants will undergo isometric knee extension on baseline day 2, pre bed rest, and post bed rest.

Bed rest

Intervention Type: OTHER

Participants will undergo 5 days bed rest after 5 day baseline assessments

PB-125

Healthy older adult subjects ages 65-75 will take the supplement PB-125 during a 5 day bed rest and will be assessed for vascular function independent of metabolism with passive leg movement (PLM), skeletal muscle bioenergetics independent of vascular constraints (i.e. blood flow and O2 supply) with phosphorous magnetic resonance spectroscopy (P-MRS), and skeletal muscle bioenergetics under normal blood flow and O2 supply.

Group Type: EXPERIMENTAL

PB-125

Intervention Type: DIETARY_SUPPLEMENT

Participants will receive 100 mg on days 1-5 of bed rest.

Passive Leg Movement (PLM)

Intervention Type: OTHER

Participants will be tested for passive leg movement on baseline day 1, bed rest day 1, and post bed rest.

Plantar flexion

Intervention Type: OTHER

Participants will undergo plantar flexion on baseline day 2, pre bed rest, and post bed rest.

Isometric knee extensor test

Intervention Type: OTHER

Participants will undergo isometric knee extension on baseline day 2, pre bed rest, and post bed rest.

Bed rest

Intervention Type: OTHER

Participants will undergo 5 days bed rest after 5 day baseline assessments

Placebo

Healthy older adult subjects ages 65-75 will take placebo during a 5 day bed rest and will be assessed for vascular function independent of metabolism with passive leg movement (PLM), skeletal muscle bioenergetics independent of vascular constraints (i.e. blood flow and O2 supply) with phosphorous magnetic resonance spectroscopy (P-MRS), and skeletal muscle bioenergetics under normal blood flow and O2 supply.

Group Type: PLACEBO_COMPARATOR

Placebo

Intervention Type: OTHER

Participants will receive Placebo on days 1-5 of bed rest.

Passive Leg Movement (PLM)

Intervention Type: OTHER

Participants will be tested for passive leg movement on baseline day 1, bed rest day 1, and post bed rest.

Plantar flexion

Intervention Type: OTHER

Participants will undergo plantar flexion on baseline day 2, pre bed rest, and post bed rest.

Isometric knee extensor test

Intervention Type: OTHER

Participants will undergo isometric knee extension on baseline day 2, pre bed rest, and post bed rest.

Bed rest

Intervention Type: OTHER

Participants will undergo 5 days bed rest after 5 day baseline assessments

Interventions

MITO-AO

Participants will receive 160 mg with breakfast on day 1 of bed rest and 40 mg with breakfast on days 2-5.

Intervention Type: DIETARY_SUPPLEMENT

PB-125

Participants will receive 100 mg on days 1-5 of bed rest.

Intervention Type: DIETARY_SUPPLEMENT

Placebo

Participants will receive Placebo on days 1-5 of bed rest.

Intervention Type: OTHER

Passive Leg Movement (PLM)

Participants will be tested for passive leg movement on baseline day 1, bed rest day 1, and post bed rest.

Intervention Type: OTHER

Plantar flexion

Participants will undergo plantar flexion on baseline day 2, pre bed rest, and post bed rest.

Intervention Type: OTHER

Isometric knee extensor test

Participants will undergo isometric knee extension on baseline day 2, pre bed rest, and post bed rest.

Intervention Type: OTHER

Bed rest

Participants will undergo 5 days bed rest after 5 day baseline assessments

Intervention Type: OTHER

Eligibility Criteria

Inclusion Criteria

• Age between 65-85 yrs
• Ability to sign informed consent
• Montreal cognitive assessment (MOCA) exam score greater-than or equal to 26 4. Free-living, prior to admission

Exclusion Criteria

• Cardiac abnormalities considered exclusionary by the study physician (e.g., congestive heart failure (CHF), coronary artery disease (CAD), right-to-left shunt)
• Uncontrolled endocrine or metabolic disease (e.g., hypo/hyperthyroidism, diabetes)
• Glomerular filtration rate (GFR) less-than 30 mL/min/1.73m2 or evidence of kidney disease or failure
• Vascular disease or risk factors of peripheral atherosclerosis. (e.g., uncontrolled hypertension, obesity, diabetes, hypercholesterolemia greater-than 250 mg/dl, claudication or evidence of venous or arterial insufficiency upon palpitation of femoral, popliteal and pedal arteries)
• Risk of deep vein thrombosis (DVT) including family history of thrombophilia, DVT, pulmonary emboli, myeloproliferative diseases including polycythemia (Hb greater-than 18 g/dL) or thrombocytosis (platelets greater-than 400x103/mL), and connective tissue diseases (positive lupus anticoagulant), hyperhomocysteinemia, deficiencies of factor V Leiden, proteins S and C, and antithrombin III
• Use of anticoagulant therapy (e.g., Coumadin, heparin)
• Elevated systolic pressure greater-than 150 or a diastolic blood pressure greater-than 100 (treated or untreated)
• Implanted electronic devices (e.g., pacemakers, electronic infusion pumps, stimulators)
• Cancer or history of successfully treated cancer (less than 1 year) other than basal cell carcinoma
• Currently on a weight-loss diet or body mass index greater-than 35 kg/m2 (a BMI of 35 kg/m2, which includes individuals that fall into to the Class I obesity category, has been selected to improve inclusion and generalizability to a greater percentage of the general population).
• Inability to abstain from smoking for duration of study
• A history of greater-than 20 pack per year smoking
• HIV or hepatitis B or C*
• Recent anabolic or corticosteroids use (within 3 months)
• Subjects with hemoglobin or hematocrit lower than accepted lab values
• Agitation/aggression disorder (by psychiatric history and exam)
• History of stroke with motor disability
• A recent history (less-than 12 months) of GI bleed
• Depression [greater-than 5 on the 15 items Geriatric Depression Scale (GDS)]
• Alcohol abuse (greater-than 2 drinks per day) or drug abuse (inappropriate use of prescription medications or use of any illicit/illegal drugs for recreational use)
• Exercise training (greater-than 1 session of moderate to high intensity aerobic or resistance exercise/week)
• Liver disease (aspartate aminotransferase/alanine aminotransferase 2 times above the normal limit, hyperbilirubinemia)
• Respiratory disease (acute upper respiratory infection, history of chronic lung disease with resting oxygen saturation less-than 97% on room air)
• Currently taking a mitochondrial targeted antioxidant or similarly acting nutraceutical
• Unwilling to cease dietary supplements 4 weeks prior to initiation of bed rest
• Participated in similar bed rest study during last 12 months
• Any other condition or event considered exclusionary by the PI and faculty physician

• Minimum Eligible Age: 65 Years
• Maximum Eligible Age: 85 Years
• Eligible Sex: ALL
• Accepts Healthy Volunteers: Yes

Sponsors

National Heart, Lung, and Blood Institute (NHLBI)

NIH

Sponsor Role: collaborator

Joel Trinity

OTHER

Sponsor Role: lead

Responsible Party

Joel Trinity

Research Assistant Professor

Responsibility Role: SPONSOR_INVESTIGATOR

Locations

VA Medical Center

Salt Lake City, Utah, United States

Site Status: RECRUITING

Countries

United States

Central Contacts

Joel D Trinity, PhD

Role: CONTACT

joel.trinity@hsc.utah.edu

801-584-2522

Facility Contacts

Joel Trinity, PhD.

Role: primary

joel.trinity@hsc.utah.edu

512-689-2187

J. David Symons, PhD.

Role: backup

j.david.symons@hsc.utah.edu

801-581-4769

Other Identifiers

1R01HL142603-01A1

Identifier Type: NIH

Identifier Source: secondary_id

View Link

IRB_00111321

Identifier Type: -

Identifier Source: org_study_id