Sequence variants contributing to dysregulated inflammatory responses across keratoconic cone surface in adolescent patients with keratoconus

Katarzyna Jaskiewicz; Magdalena Maleszka-Kurpiel; Michał Kabza; Justyna A Karolak; Marzena Gajecka

doi:10.3389/fimmu.2023.1197054

Sequence variants contributing to dysregulated inflammatory responses across keratoconic cone surface in adolescent patients with keratoconus

Front Immunol. 2023 Jul 6:14:1197054. doi: 10.3389/fimmu.2023.1197054. eCollection 2023.

Authors

Katarzyna Jaskiewicz¹, Magdalena Maleszka-Kurpiel^{2

3}, Michał Kabza⁴, Justyna A Karolak⁴, Marzena Gajecka^{1

4}

Affiliations

¹ Institute of Human Genetics, Polish Academy of Sciences, Poznan, Poland.
² Optegra Eye Health Care Clinic in Poznan, Poznan, Poland.
³ Chair of Ophthalmology and Optometry, Poznan University of Medical Sciences, Poznan, Poland.
⁴ Chair and Department of Genetics and Pharmaceutical Microbiology, Poznan University of Medical Sciences, Poznan, Poland.

Abstract

Background: Keratoconus (KTCN) is the most common corneal ectasia resulting in a conical shape of the cornea. Here, genomic variation in the corneal epithelium (CE) across the keratoconic cone surface in patients with KTCN and its relevance in the functioning of the immune system were assessed.

Methods: Samples from four unrelated adolescent patients with KTCN and two control individuals were obtained during the CXL and PRK procedures, respectively. Three topographic regions, central, middle, and peripheral, were separated towards the whole-genome sequencing (WGS) study embracing a total of 18 experimental samples. The coding and non-coding sequence variation, including structural variation, was assessed and then evaluated together with the previously reported transcriptomic outcomes for the same CE samples and full-thickness corneas.

Results: First, pathway enrichment analysis of genes with identified coding variants pointed to "Antigen presentation" and "Interferon alpha/beta signaling" as the most overrepresented pathways, indicating the involvement of inflammatory responses in KTCN. Both coding and non-coding sequence variants were found in genes (or in their close proximity) linked to the previously revealed KTCN-specific cellular components, namely, "Actin cytoskeleton", "Extracellular matrix", "Collagen-containing extracellular matrix", "Focal adhesion", "Hippo signaling pathway", and "Wnt signaling" pathways. No genomic heterogeneity across the corneal surface was found comparing the assessed topographic regions. Thirty-five chromosomal regions enriched in both coding and non-coding KTCN-specific sequence variants were revealed, with a most representative 5q locus previously recognized as involved in KTCN.

Conclusion: The identified genomic features indicate the involvement of innate and adaptive immune system responses in KTCN pathogenesis.

Keywords: WGS; cornea; corneal epithelium; inflammation; keratoconus; non-coding sequence variation; whole genome.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Collagen / genetics
Cornea / pathology
Gene Expression Profiling
Humans
Keratoconus* / genetics
Keratoconus* / pathology
Transcriptome

Substances

Collagen

Grants and funding

This work was supported by National Science Centre in Poland (grant number: 2018/31/B/NZ5/03280 and 2021/41/B/NZ5/02245).