Clinical Trial Details
— Status: Terminated
Administrative data
| NCT number |
NCT02720211 |
| Other study ID # |
IRB #86498 |
| Secondary ID |
|
| Status |
Terminated |
| Phase |
N/A
|
| First received |
|
| Last updated |
|
| Start date |
August 2016 |
| Est. completion date |
November 6, 2018 |
Study information
| Verified date |
November 2022 |
| Source |
University of Utah |
| Contact |
n/a |
| Is FDA regulated |
No |
| Health authority |
|
| Study type |
Interventional
|
Clinical Trial Summary
Nearly all migraine sufferers report sensitivity to light during a headache and a significant
proportion of sufferers report light sensitivity between attacks. Light is also a common
trigger for migraine headaches. Spectacle lenses that have been treated with tints and
spectacle lenses that have been treated with thin-films have both been shown to reduce light
sensitivity and headache in patients with migraine. At this time, it is not clear which
spectacle lens treatment is superior. The purpose of this trial is to determine if there's a
significant, therapeutic advantage to either spectacle lens treatment. Both treatments could
be a novel, non-invasive adjuvant in the treatment of migraine.
Description:
Approximately 6% of men and 18% of women are afflicted with migraines. (Stovner et al., 2006)
Over 90% of patients with migraines report a sensitivity to light (photophobia) during
headaches. (Evans et al., 2008) Some migraine sufferers report that light can trigger a
migraine and some have a chronic sensitivity to light (Main et al., 1997). Migraineurs are
especially sensitive to non-incandescent lighting sources such as fluorescent lights,
computer monitors, and gas-vapor lamps (Katz and Digre, 2016).
The pathway that mediates photophobia appears to involve intrinsically photosensitive retinal
ganglion cells ("IPRGCs"; Hattar et al., 2002) and trigeminal afferents (Noseda et al., 2010;
Digre and Brennan, 2012). These retinal cells do not require input from photoreceptors to be
activated by light, and they have been shown to be responsible for circadian rhythm
entrainment and the pupillary light reflex. As such, these cells constitute a pathway
separate from that of the visual pathway (Güler et al., 2008). IPRGCs contain the chromophore
melanopsin. In these cells, 480 nm light (in the blue-green portion of the visible spectrum)
isomerizes melanopsin and triggers the phototransduction cascade. However, IPRGCs can also be
stimulated by rods and cones. Thus, IPRGCs can be stimulated directly by 480-nm light or
indirectly by any light in the visible spectrum.
In the present study, the investigators will use a neutral gray tint to decrease stimulation
of the eye by all wavelengths in the visible spectrum. The investigators will compare this
intervention to a thin-film spectacle coating designed to specifically block 480-nm light.
The gray tint will decrease both direct and indirect stimulation of the IPRGCs by blocking
all wavelengths of the visible spectrum. The 480-nm thin-film will specifically target direct
stimulation of the IPRGC.
All tints and thin films will be calibrated such that the optical density, that is the
overall "darkness" of all study lenses, will be the same. All study lenses will appear to
have the same overall light blocking effect to study subjects. The lenses are intended to be
a preventative or prophylactic treatment for chronic migraine.
