HIV Infections Clinical Trial
Official title:
The Use of a Mobile Application to Support Physical Activity and Lifestyle Changes in Persons Living With HIV: the SMARTAPP Study.
Physical activity delays all-cause mortality in the general population and reduces the risk
of cardiovascular disease (CVD), stroke, type-2 diabetes and some types of cancer (Garber et
al., 2011). These diseases are associated with chronic inflammation, which is characterized
by activation of inflammatory signalling pathways with abnormal production of cytokines and
other mediators (Hotamisligil, 2006). Observational studies of large population cohorts have
consistently shown an association between physical inactivity and low-grade systemic
inflammation and interventional studies a reduction of inflammatory markers following
exercise (Beavers et al., 2010).
Chronic inflammation is also a predominant feature of treated human immunodeficiency virus
(HIV) infection (Lederman et al., 2013; Deeks et al., 2013). Compared to age-matched
HIV-negative subjects, persons with chronic HIV infection are at higher risk to develop
non-acquired immune deficiency syndrome (AIDS) related chronic diseases (Guaraldi et al.,
2011), and several studies have shown an association between chronic inflammation and higher
cardiovascular risk and overall mortality (Kuller et al., 2008, Duprez et al., 2012).
Recently, the investigators performed a pilot study of moderate physical activity that
enrolled sedentary HIV infected subjects treated with combination antiretroviral treatment
(cART), consisting of brisk walking, with or without strength exercise. Overall, after 12
weeks of training cholesterol profile and soluble and cell inflammatory markers improved
significantly. However, because of the considerable individual variability in exercise
responses, a program of physical activity needs be adjusted on an individual basis to be most
effective. During recent years, the use of mobile technologies has been implemented for
health monitoring interventions, including exercise. We hypothesized that the use of a mobile
application will favour engagement to exercise by providing motivational inputs, and
therefore adherence, and, as a consequence, an improvement of physical fitness.
The investigators hypothesized that the use of a mobile application will favour engagement to
exercise by providing motivational inputs, and therefore adherence, and, as a consequence, an
improvement of physical fitness. Therefore, the aim of this project is to improve health and
quality of life of patients living with HIV through self-empowerment by use of an innovative
mobile application, in order to assist and monitor individualized program of physical
activity and diet recommendation.
OBJECTIVES
Primary To compare the improvement of physical fitness between the EG and CG groups after 16
weeks of training.
Secondary
To compare the improvement of the following characteristics between the EG and CG groups
after 16 weeks of training:
1. anthropometry,
2. Blood lipids,
3. Inflammatory markers,
4. Quality of Life,
4. Mood State.
ENDPOINTS Primary The primary objective will be assessed by the proportion of subjects with
an improvement from baseline of 15% of maximal oxygen consumption (O2max) through 16 weeks of
training.
Secondary
The secondary endpoints will be assessed by the 16-week changes in the following measures:
1. BMI and %Fat Mass,
2. Blood Total-, LDL-, HDL-Cholesterol,
3. Blood IL-6, hs-PCR, d-Dimer, IL-18; myostatin; T-cell activation markers,
4. F12 questionnaire,
5. Profile of Mood State questionnaire.
STUDY DESIGN Multicentre, randomized, open-label, pilot study enrolling HIV-infected
subjects, of age ≥18 years, with or without cART, either sedentary or already practicing
mild/moderate physical activity.+
Subjects satisfying the inclusion and exclusion criteria will be randomized 1:1 to one of the
following arms:
i) experimental group (EG), where participants will be trained with an exercise program for
16 weeks with the use of a smartphone application; ii) control group (CG), where participants
will be trained with an exercise program for 16 weeks without smartphone application.
You will be screened for eligibility by an infectious diseases specialist and a sport
medicine specialist through collection of clinical and treatment history, physical
examination, routine blood screen, ECG at rest and during submaximal cycle ergometer test.
Eligible patients will sign a written informed consent and will be followed-up at screening,
baseline (start of the training program) and after 16 weeks of training, except for profile
of mood states that will be assessed weekly
Each study visit will include: the evaluation of CDC stage, anthropometric assessment
(height, weight), systolic and diastolic blood pressure, smoking status, assessment of the
antiretroviral and concomitant therapies and routine laboratory tests. Additional 30 mL of
peripheral blood will be withdrawn at baseline and at the end of the study (week 16) and
stored in a biobank for further investigations for patients recruited from San Raffaele
Hospital. The demographic, clinical, physical fitness, quality of life information will be
accurately recorded at the study visits in an electronic Case Report Form (eCRF).
Randomization Randomization list will be computer-generated (block sizes of ten) and will be
incorporated within the electronic clinical report form (eCRF) of the study. Study
participants, study nurses and study physicians will be aware of the allocation group but
allocation will be concealed from laboratory staff.
Discontinuation from the study You may withdraw consent at any time for any reason or be
dropped from the study at discretion of the investigator if he/she violates the study plan or
for administrative or other reasons.
You will be discontinued from the study if you will:
- withdraw consent or
- miss the exercise sessions for ≥ 2 consecutive weeks (corresponding to 6 sessions).
Any female patient who becomes pregnant during the course of the study will be also
immediately withdrawn from the study.
Exercise program The exercise prescription will be scheduled according to the American
College of Sport Medicine guidelines (Garber et al., 2011). You will perform 3 outdoor
training sessions a week for 16 weeks, consisting of brisk walking or running for one hour.
In both groups, participants will be assigned the same volume and intensity of exercise.
After baseline O2max examination, participants will receive and individual training program
written by exercise scientists (MB, GP, ALT), which will be designed according to the
performance at O2max examination. The exercise program will be divided into two periods. In
the first period (weeks 1-4) subjects will train at 60-70% of maximal heart rate to improve
the aerobic metabolism capacity. Moreover, participants will be familiarized to both physical
activity (both EG and CG) and the use of mobile application (the EG only) through direct
coach supervision. In the second period (weeks 5-16), participants will train without direct
coach supervision, but following the individualized program on a designed timeline. The EG
participants will receive automatic real-time feedback though the application and both EG and
CG participants weekly feed-back from trainers. During this period exercise intensity, will
be increased to 70-80% of maximal heart rate.
Training adherence Adherence to the program will be defined as the proportion of sessions
attended during the 16-week training period and it will be calculated only among the
participants who will complete the study.
Anthropometric Assessment The anthropometric assessment will be performed before and at the
end of the program by the same operator following the standardized techniques described by
Lohman (1981). Anthropometric variables will include body mass, stature, and skinfold
thickness on the dominant side. Stature and body mass will be measured with a portable
stadiometer and scaled to the nearest 0.5 cm and 0.1 kg, respectively. Skinfolds will be
taken three times in each anatomic site using a calliper (Holtain Ltd, Crymych Uk) to the
nearest 0.2 mm. The average value obtained among the three measures will be computed. Body
density (d) will be calculated using the Jackson & Pollock equation (1985) from three
skinfolds (Female: triceps, suprailiac and thigh; Male: pectoral, abdominal and thigh). The
percentage of fat mass will be finally derived as: fat mass (%) = 495/ d - 450 (Siri et al.,
1961).
Physical Fitness Evaluation You will be instructed to arrive at the laboratory in a rested
and fully hydrated state and to avoid strenuous exercise in the 24 h preceding the testing
session. In addition, they will avoid alcohol intake in the 48 h before the exercise test.
All tests will be carried out in a well-ventilated laboratory at a temperature of 20-22°C on
an electromagnetically-braked cycle ergometer (Monarc, Ergometric 893, Finland). The protocol
will begin with subjects cycling at 50 W for 6 minutes; then the load will increase by 15 W
each minute until volitional exhaustion. The peak values of the main cardiovascular,
respiratory, and metabolic parameters will be taken as the highest 30-s mean value attained
before the subject's volitional exhaustion. Oxygen consumption (), carbon dioxide production
(), respiratory exchange ratio (RER) and pulmonary ventilation () will be measured on a
breath-by-breath basis by telemetric metabolimeter (Quarkb2, Cosmed, Rome, Italy). O2max will
be assessed according to the criterion described by Taylor et al. Heart rate (HR) will be
recorded during the whole test by a HR monitor (Polar S810, © Polar Electro 2011, Kempele,
Finland). The VT will be assessed according to the gas exchange method (V-Slope).24 Briefly,
the break point in the vs relationship will be detected and considered as the VT. Then the VT
will be expressed in percentage of the max.
Rating of Perceived Exertion The Borg 6-20 scale is selected to rate the perceived intensity
of exertion (Borg, 1982). A verbal-anchored scale will be shown to participants before,
immediately and after 30-min completing the training session. Each subject will be
familiarized on the use of Borg 6-20 scale, including anchoring procedures.
Total Quality Recovery scale (TQR) Psychophysiological recovery process status will be
checked using the Total Quality Recovery scale (TQR) (Kenttä et al., 1998). Participants will
provide a rating of perceived quality of recovery using a scaling from 6 (worst) to 20
(best). A verbal-anchored scale will be shown to the subjects, the morning after the training
session. Each subject will be familiarized on the use TQR scale, including anchoring
procedures.
Profile of Mood State (POMS) The POMS questionnaire contains 32 items reflecting an
individual's mood on five primary dimensions (i.e. depression, fatigue, vigour, tension and
anger). Subjects will complete POMS individually once a week. The POMS data will be analysed
for each specific dimension and "energy index" was calculated as "vigour-fatigue" and used to
monitor changes in energy balance.
Quality of life The SF-12 questionnaire is derived from Short-Form Health Survey (36-item).
It is a patient-reported survey of patient health (Brazier et al., 1992). This questionnaire
was used to evaluate the participant's perception of QOL in the domains of physical
functioning, role limitations due to physical health, emotional well-being, social
functioning and general health with higher scores indicating greater QOL.
Nutrition The use of a daily food diary will be adopted to assess the nutritional habits of
participants; the diary will be fulfilled at least 3 days a week (during 2 working days and 1
day during week-end) and the patient will be requested to indicate the name, the amount and
the cooking method of consumed foods and seasonings; beverages will also be included in the
report. Diet quality and diet variety indexes will be evaluated starting from the food diary
provided by the patients.
Concomitant medications The use of concomitant medications/therapies (already ongoing or that
might need to be prescribed during the study) are allowed and recorded. No specific
restrictions are foreseen during the course of the study with regard to concomitant therapy
or vaccination.
Laboratory analysis Blood examination will include complete blood count; standard biochemical
exams with fasting total, high-density lipoprotein (HDL) and low-density lipoprotein (LDL)
cholesterol, triglycerides, glucose, insulin, glycated haemoglobin (HbA1c); cluster of
differentiation 4 (CD4+) and cluster of differentiation 8 (CD8+) T-cell counts, HIV-1-RNA
plasma level (Abbott RealTime HIV-1 assay). The Homeostatic Model Assessment (HOMA)-I and the
Veterans Aging Cohort Study Risk (VACS) indexes will also be calculated [15].
Inflammatory markers Soluble biomarkers will be measured in cryopreserved plasma samples,
drawn at BL and at the end of the program, by commercially available enzyme-linked
immunosorbent assays according to manufacturers' recommendation. These will include
high-sensitivity C-reactive protein (hsCRP, Catalog Number DCRP00), interleukin-6 (IL-6,
Catalog Number D6050), D-dimer (Asserachrom, Diagnostica Stago, Asnieres-Sur-Seine, France),
interleukin-18 (IL-18) (Medical and Biological Laboratories, Nagoya, Japan), myostatin
(Cusabio, China).
Flow cytometry for cell-activation markers will be measured on cryopreserved peripheral blood
mononuclear cells isolated by Ficoll-Paque gradient from EDTA-anticoagulated whole blood.
After thawing and PBS-washing, 3 x 105 cells will be stained using phycoerythrin
(PE)-conjugated anti-HLA-DR, PE-cyanin red 5.1-conjugated anti-CD38, Alexa Fluor
647-conjugated anti-CD3, fluorescein isothiocyanate-conjugated anti-CD4 or anti-CD8
(BD-Biosciences, San Diego, CA). CD38+ and HLA-DR+ cells will be gated from the CD3+/CD4+ or
CD3+/CD8+ cells on a 2-dimensional dot plot. Analyses will be performed by FACSCalibur with
CellQuest software (BD-Biosciences) and results reported as percentages of CD3+/CD4+ and
CD3+/CD8+ T-cells expressing both HLA-DR and CD38.
For both soluble and inflammatory markers, samples will be analysed in batch at the end of
the study and blindly with respect to group assignment.
Sample size We estimated that a sample size of 48 patients per group, or a total of 96
subjects would be required in order to detect a 30% increase in the proportion of subjects
with an improvement of VO2max through 16 weeks of training, from 40% (hypothesized for the
control arm, i.e. no use of the smartphone application) to 70% (hypothesized for the
experimental arm, i.e. use of the smartphone application arm), with 80% power at an α of
0.05.
As the improvement of VO2max is directly correlated to the adherence to training sessions, we
expect that the proportion in the experimental arm (using the smartphone application as
supervision) might be similar to that observed in a previous paper (Bonato et al., 2016),
reporting that the adherence to exercise program with the supervision of professional coaches
was found to be 67%. On the contrary, in absence of training supervision (control group) we
expect a lower adherence, i.e. 40%. As the accrual of such a number of subjects is not
feasible, we plan to enrol 60 patients.
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