Comparison Between Continuous and Pulsed Oral Doxycycline Treatment Protocols for Refractory Meibomian Gland Dysfunction

Comparison Between Continuous and Pulsed Oral Doxycycline Treatment Protocols for Refractory Meibomian Gland Dysfunction - 9 Months Follow-up Prospective Study

Status

Completed

Phases

Unknown

Study type

Observational

Source

ClinicalTrials.gov

Registry ID

NCT06520007

Enrollment

Registered

2024-07-25

Start date

2023-03-01

Completion date

2024-05-01

Last updated

2024-07-25

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Meibomian Gland Dysfunction, Blepharitis, Doxycycline Adverse Reaction

Keywords

Meibomian gland dysfunction, Ocular surface disease, Doxycycline, Blepharitis

Brief summary

The goal of this observational study (spontaneous, non-randomised, prospective cohort, phase IV) is to compare the efficacy and safety of two different oral doxycycline treatment protocols (LCP - Low dose continuous protocol & FPP - Full dose pulsed protocol) for meibomian gland dysfunction (MGD) in patients with refractory MGD (OSDI \> 13 after at least 2 months treatment with warm compresses and lacrimal substitutes - first-line therapy). Systemic doxycycline doesn't have a standardized treatment protocol and this is why those patients are treated as in normal clinical practice. The main questions it aims to answer are: Which treatment protocol has a greater impact on patient symptoms during the follow-up (OSDI score reduction)? Which treatment protocol has a greater impact on patient signs during the follow-up (TBUT and corneal staining variations)? Which treatment protocol is safer (in terms of adverse events rate)? Participants will be visited every 3 months (V0-V1-V2-V3) with signs and symptoms assessment (TBUT, corneal staining, OSDI score) after being treated for 3 months with the assigned doxycycline treatment protocol (LCP or FPP).

Detailed description

This spontaneous, prospective, non-randomized, parallel-group, phase IV study was conducted in compliance with the tenets of the Declaration of Helsinki. All study participants were fully consented, and written informed consent was obtained. This study included patients with refractory MGD. Refractory MGD is defined as symptomatic MGC (OSDI \> 13 points) despite 2 months of first-line treatment with lacrimal substitutes 3 times per day and meibomian gland expression with warm compresses twice per day. The study will consist of 3 visits: Baseline (day 0), Visit 2 (day 90 ± 5 - 3rd month), Visit 3 (day 180 ± 5 - 6 month). At each visit, patients will receive an OSDI questionnaire, NIBUT, type I Schirmer test and AS assessment, including TBUT, corneal staining (Oxford scale) At baseline, eligible patients will be enrolled and treated with the assigned protocol. The investigators will assign the protocol (non-randomized) in a 1:1 ratio. At Visit 2, NIBUT, TBUT, Oxford scale and OSDI improvement will be evaluated compared with Visit 1. Patients will be carefully asked about their compliance with the treatment. Patients who interrupted the treatment for adverse events or low compliance (\<75% of the protocol adherence) will exit the study and be excluded from the analysis. At Visit 3, the study population will be evaluated as done in Visit 2 The protocols in the study are the following: LCD (low-dose continuous protocol) - 50 mg of doxycycline for three months FPP ( Full-dose pulsed protocol) - 100 mg of doxycycline for the first 15 days of the month for three months. The enrollment period will last about 6 months. Therefore, the study will end about 6 months after the last patient enrols.

Interventions

DRUGDoxycyclin

The drug has been prescribed, as in normal clinical practice, with the National Healthcare System. Patients have been fully informed about interactions, toxicity and posology schedule.

Study design

Observational model

COHORT

Time perspective

PROSPECTIVE

Eligibility

Sex/Gender

ALL

Age

18 Years to 100 Years

Healthy volunteers

Inclusion criteria

* 18 years or older * Provided written informed consent * OSDI score of 13 or more at the baseline visit after at least two months of first-line therapy (artificial tears and warm compresses) * Clinical diagnosis of MGD * Type 1 Schirmer test \> 10 mm * No previous history of allergy or sensitivity to doxycycline, * No use of additional topical or systemic antibiotics for the prior 2 months * No use of topical anti-inflammatory agents (ex: corticosteroids or cyclosporine) for the prior 3 months.

Exclusion criteria

* Active ocular inflammation in either eye, * Demodex blepharitis, * Ocular surgery within the past 3 months of baseline examination, * Structural ocular surface and eyelid abnormalities. * Sjögren's syndrome * Rheumatoid arthritis * Other systemic diseases resulting in dry eye * Known autoimmune disease * Doxycycline allergy or sensitivity * History of antibiotic therapy at any time within 2 months of the commencement of study * Use of significant calcium supplementation or other medications that could interfere with doxycycline absorption (es: Iron supplementation)

Design outcomes

Primary

Measure	Time frame	Description
OSDI score	Baseline - 3 months (90 days ± 5 days) - 6 months (180 days ± 5 days)	Ocular Surface Disease Index

Secondary

Measure	Time frame	Description
TBUT	Baseline - 3 months (90 days ± 5 days) - 6 months (180 days ± 5 days)	Tear break-up time
Corneal staining	Baseline - 3 months (90 days ± 5 days) - 6 months (180 days ± 5 days)	Oxford scale has been use to assess corneal staining
Adverse events	From baseline up to the 3rd month	Number of dropouts due to drug toxicity

Countries

Italy

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026