Clinical Trial Details
— Status: Enrolling by invitation
Administrative data
| NCT number |
NCT05622006 |
| Other study ID # |
GENSED |
| Secondary ID |
|
| Status |
Enrolling by invitation |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
August 22, 2022 |
| Est. completion date |
August 30, 2023 |
Study information
| Verified date |
May 2023 |
| Source |
Norwegian School of Sport Sciences |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
The knowledge gap on sedentary behavior and sedentary breaks includes whether detrimental
effects of sedentary behavior can be fully attenuated by 1.) sedentary breaks 2.) physical
activity or 3.) both combined. Specifically, when breaking sedentary time which physical
activity pattern- and intensity modifies the negative effects of sedentary behavior on
glucose- and lipid metabolism? This lack of quantitative evidence calls for prospective
experimental studies investigating the physiological and biological impacts of sedentary
behavior, as well as the effectiveness of different strategies to reduce sedentary time.
Thus, quantifying effects of the intensity, frequency, volume and investigating the patterns
of sedentary breaks and/or physical activity on predefined outcomes is of importance.
Aims:
Our primary aims are to investigate the effects of breaking up sedentary time on glucose- and
lipid metabolism and thus examine whether pattern for sedentary bouts and breaks and physical
activity intensity during sedentary breaks matter. Specifically, the aims of the PhD-project
are to provide knowledge on the following questions:
• How does different patterns of accumulation of sedentary bouts and breaks acutely influence
glucose- and lipid metabolism under iso-caloric conditions?
Description:
The participants will undergo 4 different trial conditions of which all are iso-caloric, but
with different intervals of sitting and executing moderate physical activity by treadmill
walking corresponding to 45-55% of their individual VO2max/peak values, estimated from the
individual's pre-test. The total duration of sedentary- and physical activity time will be
identical in each trial condition. This study has a is randomized cross-over design. If found
eligible from step 1 and 2 in the inclusion process, participants will be invited to a final
screening day in our lab. Eligible participants then consenting to joining the study will
continue on to 4 trial days. Due to possible acute rise in insulin for up to 48 hours, a 5-14
day washout period between trials will be used to avoid carryover effects. In the washout
periods between experimental conditions the participants will resume their habitual life
activities and behaviours, i.e., diet and physical activity patterns. However, from visit 2,
during washout the participants will wear accelerometers (ActiGraph GTX3+, Pensacola, FL)
during waking hours to objectively measure sedentary time and physical activity. Average
sedentary time (hour/day) and time spent in , light-, moderate- and vigorous physical
activity intensity (min/day) will be derived. During the main trial days, the participants
may read or work on a personal computer during the sedentary time in the respective trial
conditions. The sample size calculations with glucose as the primary outcome, are based on
the study by Dunstan et al. (2012). They estimated that 19 paired observations were needed to
secure a power of 0.90 in order to detect the smallest expected effect size between the
interventions, when using a two-tailed test with a significance level of 5%. To account for
the possibility of dropouts the sample size in the present project is set to recruit 30
participants, with 25 participants completing the trials, and thus planning for 80% power
