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N/A N=26 Randomized Triple-blind Treatment

Mechanisms of Light-based Therapies for Dry Eye Disease

Dry Eye Syndromes · Meibomian Gland Dysfunction

Bottom Line

View on ClinicalTrials.gov: NCT06004895 ↗
Enrolled (actual)
26
Serious AEs
0.0%
Results posted
Jul 2025
Primary outcome: Primary: Change From Baseline in Non-invasive Tear Break Up Time to the Final Follow-up 3 Months After Final Treatment Session — -2.61; -0.85 seconds

Study Design & Population

Study type
Interventional
Phase
N/A
Interventions
Actual IPL (Device); Sham IPL (Device); LLLT (Device)
Age
Adult, Older Adult · 18+ yrs
Sex
All
Sponsor
Aston University
Primary completion
Nov 2024

Outcome Measures

OutcomeResultp-value
PRIMARY
Change From Baseline in Non-invasive Tear Break Up Time to the Final Follow-up 3 Months After Final Treatment Session		 -2.61; -0.85
SECONDARY
Change From Baseline in Ocular Surface Disease Index Scores to the Final Follow-up 3 Months After Final Treatment Session		 -11.34; -11.34
SECONDARY
Change From Baseline in 5-Item Dry Eye Questionnaire Scores to the Final Follow-up 3 Months After Final Treatment Session		 -3.29; -3.29
SECONDARY
Change From Baseline in Tear Meniscus Height to the Final Follow-up 3 Months After Final Treatment Session		 0.03; 0.05
SECONDARY
Change From Baseline in Lipid Layer Pattern Grading to the Final Follow-up 3 Months After Final Treatment Session		 0.54; 0.38
SECONDARY
Change From Baseline in Bulbar Conjunctival Hyperaemia to the Final Follow-up 3 Months After Final Treatment Session		 0.05; -0.12
SECONDARY
Change From Baseline in Total Blinks to the Final Follow-up 3 Months After Final Treatment Session		 -0.96; -0.96
SECONDARY
Change From Baseline in Visual Acuity to the Final Follow-up 3 Months After Final Treatment Session		 -0.02; 0.002
SECONDARY
Change From Baseline in Fluorescein Corneal Staining to the Final Follow-up 3 Months After Final Treatment Session		 -0.46; -0.29
SECONDARY
Change From Baseline in Lissamine Green Bulbar Conjunctival Staining to the Final Follow-up 3 Months After Final Treatment Session		 -0.42; -0.29
SECONDARY
Change From Baseline in Lissamine Green Lid Wiper Epitheliopathy to the Final Follow-up 3 Months After Final Treatment Session		 0.31; 0.15
SECONDARY
Change From Baseline in Lower Lid Meibography Meiboscore to the Final Follow-up 3 Months After Final Treatment Session		 -0.08; 0.08
SECONDARY
Change From Baseline in Demodex Presence to the Final Follow-up 3 Months After Final Treatment Session		 -0.04; -0.17
SECONDARY
Change From Baseline in Number of Blocked or Capped Meibomian Glands to the Final Follow-up 3 Months After Final Treatment Session		 0; 0
SECONDARY
Change From Baseline in Lid Margin Telangiectasia Grading to the Final Follow-up 3 Months After Final Treatment Session		 -0.33; -0.29
SECONDARY
Change From Baseline in Meibum Expressibility to the Final Follow-up 3 Months After Final Treatment Session		 -0.35; -0.50
SECONDARY
Change From Baseline in Meibum Quality to the Final Follow-up 3 Months After Final Treatment Session		 -0.07; 0.08
SECONDARY
Change From Baseline in Total Central Corneal Nerve Length to the Final Follow-up 3 Months After Final Treatment Session		 -0.76; 0.18
SECONDARY
Change From Baseline in Total Inferior Whorl Nerve Length to the Final Follow-up 3 Months After Final Treatment Session		 -2.15; -0.15
SECONDARY
Change From Baseline in Putative Tissue-Resident Memory T-Cell Density to the Final Follow-up 3 Months After Final Treatment Session		 -0.65; -4.95
SECONDARY
Change From Baseline in Adapted Symptom Assessment Questionnaire in Dry Eye Frequency Scores to the Final Follow-up 3 Months After Final Treatment Session		 -21.63; -20.54
SECONDARY
Change From Baseline in Adapted Symptom Assessment Questionnaire in Dry Eye Severity Scores to the Final Follow-up 3 Months After Final Treatment Session		 -18.54; -16.75
SECONDARY
Change From Baseline in Partial Blinks to the Final Follow-up 3 Months After Final Treatment Session		 -2.04; -2.04
SECONDARY
Change From Baseline in Upper Lid Meibography Meiboscore to the Final Follow-up 3 Months After Final Treatment Session		 0; 0
SECONDARY
Change From Baseline in Putative Dendritic Cell Density to the Final Follow-up 3 Months After Final Treatment Session		 1.24; 0.98

Summary

Dry eye disease is a common condition affecting millions worldwide and costing millions in healthcare due to reduced work productivity and quality of life. The disruption of oil glands in our eyelids known as Meibomian glands, which produce the oily layer of our tears to protect it from evaporating, is one of the most common contributors of dry eye disease. Much effort has been put into developing effective treatments for this condition as new treatments are constantly being introduced to the market. The purpose of this clinical trial is to investigate how proven light-based therapies work in treating dry eye disease and oil gland disruption. These therapies include intense-pulsed light therapy (IPL) which uses a series of light flashes on the facial skin surface, and low-level light therapy (LLLT) which uses a mask with a series of light-emitting diodes (LEDs) to warm the body cells. The main questions it aims to answer are: 1. What are the short- and long-term changes associated with these treatments on the eyelids and surface of the eyes? 2. Does LLLT alone work better than IPL+LLLT in treating dry eye disease and oil gland disruption? Participants with dry eye disease and oil gland disruption will receive four treatments with these light-based therapies each separated by two to three weeks apart, and followed up two to three weeks and three months after the final treatment session. One eye of the participant will receive intense pulsed light together with low-level light therapy, while the other eye will receive only low-level light therapy with a sham intense pulsed light treatment so that the researchers can compare if clinical signs and symptoms improve in one eye more than the other.

Eligibility Criteria

Inclusion Criteria

  • Individuals with dry eye disease symptoms (Ocular Surface Disease Index questionnaire (OSDI) score ≥ 13 or Dry Eye Questionnaire (DEQ5) score > 6) and signs (tear film instability measured with non-invasive tear break-up time 5 corneal spots, > 9 conjunctival spots or lid margin staining ≥ 2mm in length and ≥ 25% in width) (Wolffsohn et al., 2017)
  • Individuals need to also have Meibomian gland dysfunction. The diagnosis of Meibomian gland dysfunction depends on how many of 5 glands in the central lower eyelid can express oil, and the quality of the oil. A diagnosis is made if there is decreased expressibility (grade 1-3 on the Pflugfelder scale) and reduced quality of oil (grade 1-3 on Bron scale). Any presence of gland blockage and/or loss of oil glands grade 2 to grade 4 of either eyelid [Pult and Reide-Pult, 2013]) will also justify a diagnosis of Meibomian gland dysfunction
  • Age ≥ 18 years, male or female
  • Able to provide written consent in English
  • Able to attend multiple visits (4 treatment visits) and followed up for 2 weeks and 3 months after final treatment

Exclusion Criteria

  • Pregnancy
  • Contraindications to IPL treatment (Individuals with darker skin types - Fitzpatrick skin type V or VI, photosensitive epilepsy, tattoos, implants, electrical or acoustic prosthetics, semi-permanent make-up, pigmented lesions or skin cancer in the treatment area, pacemakers, use of photosensitising medication the past 3 months or during treatment period)
  • Facial or ocular IPL or LLLT treatment within the past 6 months or during study period in addition to those provided in the study
  • Use of topical medical eyedrops in the past 3 months or during study period
  • Contact lens wear in the past 2 weeks or during study period
  • Systemic conditions that can cause dry eye disease or corneal nerve loss including diabetes and Sjögren's syndrome
  • Other active ocular surface diseases or history of ocular surgery or corneal infections
  • Individuals with 1 eye
View full record on ClinicalTrials.gov →

Data sourced from ClinicalTrials.gov (NCT06004895). Outcome figures and adverse-event rates are extracted automatically from the registry's posted results and are provided for clinician reference, not as a substitute for the primary publication.

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