Evaluation of Meibomian gland dysfunction using meibography in patients with xeroderma pigmentosum

Marcos, Allexya Affonso Antunes; Freitas, Denise; Hazarbassanov, Rossen Mihaylov; Fernandes, Arthur Gustavo; Castro, Ligia Pereira; Melo, Danilo Batista Vieira de; Menck, Carlos F. Martins; Morales, Melina Correia; Gomes, José Álvaro Pereira; Neto, Rubens Belfort; Singh, Arun D.

doi:10.5935/0004-2749.2022-0319

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Evaluation of Meibomian gland dysfunction using meibography in patients with xeroderma pigmentosum

Allexya Affonso Antunes Marcos^1,2; Denise Freitas¹; Rossen Mihaylov Hazarbassanov¹; Arthur Gustavo Fernandes¹; Ligia Pereira Castro³; Danilo Batista Vieira de Melo³; Carlos F. Martins Menck³; Melina Correia Morales¹; José Álvaro Pereira Gomes¹; Rubens Belfort Neto¹; Arun D. Singh⁴

DOI: 10.5935/0004-2749.2022-0319

ABSTRACT

To assess Meibomian gland dysfunction using meibography in patients with xeroderma pigmentosum and correlate with ocular surface changes. This cross-sectional study evaluated patients with xeroderma pigmentosum. All patients underwent a comprehensive and standardized interview. The best-corrected visual acuity of each eye was determined. Detailed ophthalmic examination was conducted, including biomicroscopy examination of the ocular surface, Schirmer test type I, and meibography, and fundus examination was also performed when possible. Meibomian gland dysfunction was assessed by non-contact meibography using Oculus Keratograph^® 5M (OCULUS Inc., Arlington, WA, USA). Saliva samples were collected using the Oragene DNA Self-collection kit (DNA Genotek Inc., Ottawa, Canada), and DNA was extracted as recommended by the manufacturer. Factors associated with abnormal meiboscores were assessed using generalized estimating equation models. A total of 42 participants were enrolled, and 27 patients underwent meibography. The meiboscore was abnormal in the upper eyelid in 8 (29.6%) patients and in the lower eyelid in 17 (62.9%). The likelihood of having abnormal meiboscores in the lower eyelid was 16.3 times greater than that in the upper eyelid.In the final multivariate model, age (p=0.001), mutation profile (p=0.006), and presence of ocular surface malignant tumor (OSMT) (p=0.014) remained significant for abnormal meiboscores. For a 1-year increase in age, the likelihood of abnormal meiboscores increased by 12%. Eyes with OSMT were 58.8 times more likely to have abnormal meiboscores than eyes without ocular surface malignant tumor.In the final model, age, xeroderma pigmentosum profile, previous cancer, and clinical alterations on the eyelid correlated with a meiboscore of ≥2.Meibomian gland dysfunction was common in patients with xeroderma pigmentosum, mainly in the lower eyelid. The severity of Meibomian gland dysfunction increases with age and is associated with severe eyelid changes.

Keywords: Meibomian glands/pathology; Meibomian glands/ diagnostic imaging; Photography; Xeroderma pigmentosum; Eyelid diseases/diagnostic imaging; Dry eye syndromes; DNA repair; Humans; Case report

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