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A Study Investigating the Effectiveness of a LifeSeasons NeuroQ Supplement With Lifestyle Changes to Improve Cognitive Function in Healthy Adults Who Have One or More Risk Factors for Cognitive Decline

Primary Purpose

Healthy

Status

Completed

Phase

Not Applicable

Locations

United States

Study Type

Interventional

Intervention

NeuroQ

About this trial

This is an interventional prevention trial for Healthy focused on measuring NeuroQ, Dr. Bredesen, PreCODE protocol, ReCODE method, cognitive decline, The End of Alzheimer's, cognitive support, cognitive health

Eligibility Criteria

45 Years - undefined (Adult, Older Adult)All SexesAccepts Healthy Volunteers

Inclusion Criteria:

Males and females 45 years of age or older with one or more of the following risk factors for cognitive decline:
- Self-reported genetic risk factor of Alzheimer's Disease or dementia as confirmed by Apolipoprotein 4 genetic testing
- Self-reported family history of Alzheimer's Disease or dementia in a first-degree relative
- Self-reported lifestyle risk factor: sedentary lifestyle; poor dietary habits (e.g. insufficient consumption of fruits and vegetables for necessary nutrients); poor social support network (e.g. majority of evenings and weekends are spent in isolation); poor stress management skills (e.g. binge eating habits or performing harmful activities during periods of stress); poor sleep habits; metabolic syndrome
- Exception: Individuals 60 years of age or older may be enrolled without any of the above risk factors.
BMI between 18.5 and 32.5 kg/m2
Female participants are not of child-bearing potential, defined as females who have undergone a sterilization procedure (e.g. hysterectomy, bilateral oophorectomy, bilateral tubal ligation, complete endometrial ablation) or have been post-menopausal (natural or surgically) for at least 1 year prior to screening

or,

Females of child-bearing potential must have a negative baseline urine pregnancy test and agree to use a medically approved method of birth control for the duration of the study. All hormonal birth control must have been in use for a minimum of three months. Acceptable methods of birth control include:

Hormonal contraceptives including oral contraceptives, hormone birth control patch (Ortho Evra), vaginal contraceptive ring (NuvaRing), injectable contraceptives (Depo-Provera, Lunelle), or hormone implant (Norplant System)
Double-barrier method
Intrauterine devices
Non-heterosexual lifestyle or agrees to use contraception if planning on changing to heterosexual partner(s)
Vasectomy of partner at least 6 months prior to screening 4. Self-reported as non-smoker or user of any nicotine-containing products 5. Absence of dementia or other significant cognitive impairment as assessed by Mini Mental State Exam-2 Standard Version (MMSE-2) score ≥24 6. Participants who test between the 24-75th percentile in the in one or more domains in the NCI 7. Low frequency of depressed mood as assessed by PHQ-9 score of 4 or less 8. Agree to avoid caffeine consumption 24 hours prior to in-clinic visits 9. Agree to avoid alcohol consumption 24 hours prior to in-clinic visits 10. Healthy as determined by medical history and laboratory results as assessed by QI

Exclusion Criteria:

Women who are pregnant, breast feeding, or planning to become pregnant during the trial
Allergy, sensitivity, or intolerance to the investigational product's (IP) active or inactive ingredients
Self-reported confirmation of neuropsychological condition and/or cognitive impairment that, in the QI's opinion, could interfere with study participation. For e.g.:
• Schizophrenia, bipolar disorder, post-traumatic stress disorder, brain injury, neurodegenerative disease, infections, insomnia
Participants with vitamin deficiencies affecting cognition:
- Magnesium
- Cobalamin (Vitamin B12)
- Folate below the normal clinical ranges, as assessed by the QI
Participants who test below the 24th percentile or above the 75th percentile in all domains in the NCI.
Current use of prescribed medications listed in Section 8.3.1.
Current use of over-the-counter medications, supplements, foods and/or drinks listed as concomitant medications.
Unstable metabolic disease or chronic diseases as assessed by the QI
Unstable hypertension. Treatment on a stable dose of medication for at least 3 months will be considered by the QI
Type II diabetes. Treatment on a stable dose of medication may be considered by the QI on a case by case basis
Significant cardiovascular event in the past 6 months. Participants with no significant cardiovascular event on stable medication may be included after assessment by the QI on a case by case basis
Major surgery in the past 3 months or individuals who have planned surgery during the course of the trial. Participants with minor surgery will be considered on a case-by-case basis by the QI
Cancer, except skin cancers completely excised with no chemotherapy or radiation with a follow up that is negative. Volunteers with cancer in full remission for more than five years after diagnosis are acceptable
Individuals who are immune-compromised
Verbal confirmation of a HIV-, Hepatitis B- and/or C-positive diagnosis
History of or current diagnosis with kidney and/or liver diseases as assessed by the QI on a case-by-case basis, with the exception of history of kidney stones symptom free for 6 months
Verbal confirmation of current or pre-existing thyroid condition. Treatment on a stable dose of medication for at least 3 months will be considered by the QI
Current or history of any significant diseases of the gastrointestinal tract
Verbal confirmation of blood/bleeding disorders
Self-reported chronic use of cannabinoid products or currently taking medical cannabinoid products containing >0.3% tetrahydrocannabinol
Alcohol or drug abuse within the last 12 months
High alcohol intake (>2 drinks per day or >10 standard drinks per week)
Blood donation 30 days prior to screening, during the study, or a planned donation within 30-days of the last study visit
Participation in other clinical research trials 30 days prior to screening
Individuals who are unable to give informed consent
Any other active or unstable medical condition, that, in the opinion of the QI, may adversely affect the participant's ability to complete the study or its measures or pose significant risk to the participant

Sites / Locations

Kapoor Medical Center
LifeSeasons Medical Center

Arms of the Study

Arm 1

Arm Type

Experimental

Arm Label

NeuroQ

Arm Description

Directions: take 2 capsules at the same time daily

Outcomes

Primary Outcome Measures

Change in cognition as assessed by change in Neurocognitive Index (NCI) score from CNS-Vital Signs (CNS-VS) panel from screening to end-of-study.

The Neurocognitive index is an average score derived from the domain scores or a general assessment of the overall neurocognitive status of the participant. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Secondary Outcome Measures

Change in Neurocognitive Index (NCI) individual domains from screening to end-of study in participants who are fully compliant with supplementation and lifestyle modification

Change in Neurocognitive Index (NCI) individual domains from screening to end-of-study in participants who are compliant with supplementation only

Change in Neurocognitive Index (NCI) individual domains from screening to end-of-study in participants who are compliant with lifestyle modification only

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - composite memory from screening to end-of-study

The composite memory domain measures how well subject can recognize, remember, and retrieve words and geometric figures. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - verbal memory from screening to end-of-study

The verbal memory domain measures how well subject can recognize, remember, and retrieve words. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - visual memory from screening to end-of-study

The visual memory domain measures how well subject can recognize, remember and retrieve geometric figures. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - psychomotor speed from screening to end-of-study

The psychomotor speed domain measures how well a subject perceives, attends, responds to visual-perceptual information, and performs motor speed and fine motor coordination. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - reaction time from screening to end-of-study

The reaction time domain measures how quickly the subject can react, in milliseconds, to a simple and increasingly complex direction set. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - complex attention from screening to end-of-study

The complex attention domain measures the ability to track and respond to a variety of stimuli over lengthy periods of time and/or perform mental tasks requiring vigilance quickly and accurately. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - cognitive flexibility from screening to end-of-study

The cognitive flexibility domain measures how well subject is able to adapt to rapidly changing and increasingly complex set of directions and/or to manipulate the information. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - processing speed from screening to end-of-study

The processing speed domain measures how well a subject recognizes and processes information i.e., perceiving, attending/responding to incoming information, motor speed, fine motor coordination, and visual-perceptual ability. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - executive function from screening to end-of-study

The executive function domain measures how well a subject recognizes rules, categories, and manages or navigates rapid decision making. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - simple attention from screening to end-of-study

The simple attention domain measures the participants ability to track and respond to a single defined stimulus over lengthy periods of time while performing vigilance and response inhibition quickly and accurately. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - motor speed from screening to end-of-study

The motor speed domain measures the participants ability to perform movements to produce and satisfy an intention towards a manual action and goal. The scores range from less than 70 (very low) to above 110 (above average). A higher score means higher neurocognitive function and higher capacity.

Number of participants motivated to make lasting changes to their lifestyle at end-of-study.

Change in Mini Mental State Exam Version 2 (MMSE-2) score from screening to end-of study.

The Mini Mental State Exam Version 2 is an assessment of the level of consciousness. It is a series of 30 questions scored either 0 (incorrect) or 1 (correct). The range of scores is 0 to 30. A higher value means the participant answered more questions correctly.

Full Information

NCT ID

NCT04149639

First Posted

October 30, 2019

Last Updated

March 1, 2021

Sponsor

LifeSeasons Inc.

Collaborators

KGK Science Inc.

1. Study Identification

Unique Protocol Identification Number

NCT04149639

Brief Title

A Study Investigating the Effectiveness of a LifeSeasons NeuroQ Supplement With Lifestyle Changes to Improve Cognitive Function in Healthy Adults Who Have One or More Risk Factors for Cognitive Decline

Official Title

An Open-label Study to Investigate the Effectiveness of a LifeSeasons NeuroQ Supplement in Addition to Four Bredesen Recommended Lifestyle Changes to Improve Cognitive Function in Healthy Adults Who Have One or More Risk Factors for Cognitive Decline

Study Type

Interventional

2. Study Status

Record Verification Date

November 2019

Overall Recruitment Status

Completed

Study Start Date

November 8, 2019 (Actual)

Primary Completion Date

July 7, 2020 (Actual)

Study Completion Date

July 7, 2020 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

LifeSeasons Inc.

Collaborators

KGK Science Inc.

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

5. Study Description

Brief Summary

The objective of this study is to evaluate the efficacy of a NeuroQ supplement designed by Dr. Bredesen to complement his Lifestyle modification protocol. Eligible participants will be expected to consume the NeuroQ supplement and are recommended to make lifestyle changes based on Dr. Bredesen's protocol. Forty participants are expected to enroll into the study, completing study assessments at check in visits days 30 and 60, and at the end of study visit on day 90. A brief follow up phone call will be conducted approximately 30 days after study completion to ask participants if they have continued using the lifestyle changes and if they have purchased and continued to consume the NeuroQ supplement.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Healthy

Keywords

NeuroQ, Dr. Bredesen, PreCODE protocol, ReCODE method, cognitive decline, The End of Alzheimer's, cognitive support, cognitive health

7. Study Design

Primary Purpose

Prevention

Study Phase

Not Applicable

Interventional Study Model

Single Group Assignment

Model Description

Open-label design

Masking

None (Open Label)

Allocation

N/A

Enrollment

40 (Actual)

8. Arms, Groups, and Interventions

Arm Title

NeuroQ

Arm Type

Experimental

Arm Description

Directions: take 2 capsules at the same time daily

Intervention Type

Dietary Supplement

Intervention Name(s)

NeuroQ

Intervention Description

Supplement includes phosphatidylserine, coffee fruit, curcumin, ginkgo, gotu kola, and propolis active ingredients inside a veggie capsule.

Primary Outcome Measure Information:

Title

Change in cognition as assessed by change in Neurocognitive Index (NCI) score from CNS-Vital Signs (CNS-VS) panel from screening to end-of-study.

Description

Time Frame

90-135 days

Secondary Outcome Measure Information:

Title

Change in Neurocognitive Index (NCI) individual domains from screening to end-of study in participants who are fully compliant with supplementation and lifestyle modification

Description

Time Frame

90-135 days

Title

Change in Neurocognitive Index (NCI) individual domains from screening to end-of-study in participants who are compliant with supplementation only

Description

Time Frame

90-135 days

Title

Change in Neurocognitive Index (NCI) individual domains from screening to end-of-study in participants who are compliant with lifestyle modification only

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - composite memory from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - verbal memory from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - visual memory from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - psychomotor speed from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - reaction time from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - complex attention from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - cognitive flexibility from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - processing speed from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - executive function from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - simple attention from screening to end-of-study

Description

Time Frame

90-135 days

Title

Change in individual Central Nervous System-Vital Signs (CNS-VS) domain - motor speed from screening to end-of-study

Description

Time Frame

90-135 days

Title

Number of participants motivated to make lasting changes to their lifestyle at end-of-study.

Time Frame

90-120 days

Title

Change in Mini Mental State Exam Version 2 (MMSE-2) score from screening to end-of study.

Description

Time Frame

90-135 days

Other Pre-specified Outcome Measures:

Title

Incidence of pre-emergent and post-emergent adverse events following 30-day, supplementation.

Time Frame

30 days

Title

Incidence of pre-emergent and post-emergent adverse events following 60-day, supplementation.

Time Frame

60 days

Title

Incidence of pre-emergent and post-emergent adverse events following 90-day, supplementation.

Time Frame

90 days

Title

Change in systolic blood pressure following 30-day supplementation

Time Frame

30 days

Title

Change in systolic blood pressure following 60-day supplementation

Time Frame

60 days

Title

Change in systolic blood pressure following 90-day supplementation

Time Frame

90 days

Title

Change in diastolic blood pressure following 30-day supplementation

Time Frame

30 days

Title

Change in diastolic blood pressure following 60-day supplementation

Time Frame

60 days

Title

Change in diastolic blood pressure following 90-day supplementation

Time Frame

90 days

Title

Change in heart rate following 30-day supplementation

Time Frame

30 days

Title

Change in heart rate following 60-day supplementation

Time Frame

60 days

Title

Change in heart rate following 90-day supplementation

Time Frame

90 days

Title

Change in CMP following 90-day supplementation

Time Frame

90 days

Title

Change in complete blood count following 90-day supplementation

Time Frame

90 days

Title

Change in neutrophil levels in the blood following 90-day supplementation

Description

Units: XE9/L

Time Frame

90 days

Title

Change in lymphocyte blood levels following 90-day supplementation

Description

Units: XE9/L

Time Frame

90 days

Title

Change in monocyte blood levels following 90-day supplementation

Description

Units: XE9/L

Time Frame

90 days

Title

Change in eosinophil blood levels following 90-day supplementation

Description

Units: XE9/L

Time Frame

90 days

Title

Change in basophil blood levels following 90-day supplementation

Description

Units: XE9/L

Time Frame

90 days

Title

Change in red blood cell (RBC) count following 90-day supplementation

Time Frame

90 days

Title

Change in hemoglobin levels in the blood following 90-day supplementation

Description

Units: g/L

Time Frame

90 days

Title

Change in hematocrit levels in the blood following 90-day supplementation

Description

Units: L/L

Time Frame

90 days

Title

Change in platelet count following 90-day supplementation

Time Frame

90 days

Title

Change in mean corpuscular volume (MCV) following 90-day supplementation

Time Frame

90 days

Title

Change in mean corpuscular hemoglobin (MCH) following 90-day supplementation

Description

Units: pg

Time Frame

90 days

Title

Change in mean corpuscular hemoglobin concentration (MCHC) following 90-day supplementation

Time Frame

90 days

Title

Change in red cell distribution width (RDW) following 90-day supplementation

Time Frame

90 days

Title

Difference in brain activity as measured by quantitative electroencephalography (qEEG) from baseline to end-of-study in 10 participants.

Description

Alpha, Beta, Delta, and Theta bandwidths will be analyzed using the eVox system.

Time Frame

90 days

10. Eligibility

Sex

All

Minimum Age & Unit of Time

45 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: Males and females 45 years of age or older with one or more of the following risk factors for cognitive decline: Self-reported genetic risk factor of Alzheimer's Disease or dementia as confirmed by Apolipoprotein 4 genetic testing Self-reported family history of Alzheimer's Disease or dementia in a first-degree relative Self-reported lifestyle risk factor: sedentary lifestyle; poor dietary habits (e.g. insufficient consumption of fruits and vegetables for necessary nutrients); poor social support network (e.g. majority of evenings and weekends are spent in isolation); poor stress management skills (e.g. binge eating habits or performing harmful activities during periods of stress); poor sleep habits; metabolic syndrome Exception: Individuals 60 years of age or older may be enrolled without any of the above risk factors. BMI between 18.5 and 32.5 kg/m2 Female participants are not of child-bearing potential, defined as females who have undergone a sterilization procedure (e.g. hysterectomy, bilateral oophorectomy, bilateral tubal ligation, complete endometrial ablation) or have been post-menopausal (natural or surgically) for at least 1 year prior to screening or, Females of child-bearing potential must have a negative baseline urine pregnancy test and agree to use a medically approved method of birth control for the duration of the study. All hormonal birth control must have been in use for a minimum of three months. Acceptable methods of birth control include: Hormonal contraceptives including oral contraceptives, hormone birth control patch (Ortho Evra), vaginal contraceptive ring (NuvaRing), injectable contraceptives (Depo-Provera, Lunelle), or hormone implant (Norplant System) Double-barrier method Intrauterine devices Non-heterosexual lifestyle or agrees to use contraception if planning on changing to heterosexual partner(s) Vasectomy of partner at least 6 months prior to screening 4. Self-reported as non-smoker or user of any nicotine-containing products 5. Absence of dementia or other significant cognitive impairment as assessed by Mini Mental State Exam-2 Standard Version (MMSE-2) score ≥24 6. Participants who test between the 24-75th percentile in the in one or more domains in the NCI 7. Low frequency of depressed mood as assessed by PHQ-9 score of 4 or less 8. Agree to avoid caffeine consumption 24 hours prior to in-clinic visits 9. Agree to avoid alcohol consumption 24 hours prior to in-clinic visits 10. Healthy as determined by medical history and laboratory results as assessed by QI Exclusion Criteria: Women who are pregnant, breast feeding, or planning to become pregnant during the trial Allergy, sensitivity, or intolerance to the investigational product's (IP) active or inactive ingredients Self-reported confirmation of neuropsychological condition and/or cognitive impairment that, in the QI's opinion, could interfere with study participation. For e.g.: • Schizophrenia, bipolar disorder, post-traumatic stress disorder, brain injury, neurodegenerative disease, infections, insomnia Participants with vitamin deficiencies affecting cognition: Magnesium Cobalamin (Vitamin B12) Folate below the normal clinical ranges, as assessed by the QI Participants who test below the 24th percentile or above the 75th percentile in all domains in the NCI. Current use of prescribed medications listed in Section 8.3.1. Current use of over-the-counter medications, supplements, foods and/or drinks listed as concomitant medications. Unstable metabolic disease or chronic diseases as assessed by the QI Unstable hypertension. Treatment on a stable dose of medication for at least 3 months will be considered by the QI Type II diabetes. Treatment on a stable dose of medication may be considered by the QI on a case by case basis Significant cardiovascular event in the past 6 months. Participants with no significant cardiovascular event on stable medication may be included after assessment by the QI on a case by case basis Major surgery in the past 3 months or individuals who have planned surgery during the course of the trial. Participants with minor surgery will be considered on a case-by-case basis by the QI Cancer, except skin cancers completely excised with no chemotherapy or radiation with a follow up that is negative. Volunteers with cancer in full remission for more than five years after diagnosis are acceptable Individuals who are immune-compromised Verbal confirmation of a HIV-, Hepatitis B- and/or C-positive diagnosis History of or current diagnosis with kidney and/or liver diseases as assessed by the QI on a case-by-case basis, with the exception of history of kidney stones symptom free for 6 months Verbal confirmation of current or pre-existing thyroid condition. Treatment on a stable dose of medication for at least 3 months will be considered by the QI Current or history of any significant diseases of the gastrointestinal tract Verbal confirmation of blood/bleeding disorders Self-reported chronic use of cannabinoid products or currently taking medical cannabinoid products containing >0.3% tetrahydrocannabinol Alcohol or drug abuse within the last 12 months High alcohol intake (>2 drinks per day or >10 standard drinks per week) Blood donation 30 days prior to screening, during the study, or a planned donation within 30-days of the last study visit Participation in other clinical research trials 30 days prior to screening Individuals who are unable to give informed consent Any other active or unstable medical condition, that, in the opinion of the QI, may adversely affect the participant's ability to complete the study or its measures or pose significant risk to the participant

Overall Study Officials:

First Name & Middle Initial & Last Name & Degree

Jamie Langston

Organizational Affiliation

LifeSeasons Inc.

Official's Role

Study Director

Facility Information:

Facility Name

Kapoor Medical Center

City

Studio City

State/Province

California

ZIP/Postal Code

91604

Country

United States

Facility Name

LifeSeasons Medical Center

City

Flower Mound

State/Province

Texas

ZIP/Postal Code

75077

Country

United States

12. IPD Sharing Statement

Plan to Share IPD

Learn more about this trial

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