AI Article Synopsis

  • Diabetic retinopathy (DR) is a serious eye condition linked to type 2 diabetes mellitus (T2DM), and this study investigates the role of myelomonocytic proangiogenic cells (PAC) in its development.
  • The researchers compared PAC from healthy individuals to those from T2DM patients, both with and without DR, examining their characteristics and abilities to support blood vessel formation.
  • Results showed that T2DM PAC have altered properties and functions, which could contribute to poor vascular support in the eye and potentially lead to harmful new blood vessel growth in DR.

Article Abstract

Purpose: Diabetic retinopathy (DR) is a major microvascular complication of type 2 diabetes mellitus (T2DM). Myelomonocytic proangiogenic cells (PAC) have been implicated in DR pathogenesis, but their functional and developmental abnormalities are unclear. In this study we assessed PAC characteristics from healthy controls, T2DM patients with DR (DR) and without (NoDR) in order to determine the consequence of the diabetic condition on PAC phenotype and function, and whether these differ between DR and NoDR patients.

Methods: PAC were generated by culturing PBMC on fibronectin coating and then immunophenotyped using flow cytometry. Furthermore, cells were sorted based on CD14, CD105, and CD133 expression and added to an 3-D endothelial tubule formation assay, containing GFP-expressing human retinal endothelial cells (REC), pericytes, and pro-angiogenic growth factors. Tubule formation was quantified by fluorescence microscopy and image analysis. Moreover, sorted populations were analyzed for angiogenic mediator production using a multiplex assay.

Results: The expression of CD16, CD105 and CD31, but not CD133, was lower in PAC from T2DM patients with or without DR. Myeloid and non-myeloid T2DM-derived sorted populations increased REC angiogenesis as compared to control cultures. They also showed increased S100A8 secretion, decreased VEGF-A secretion, and similar levels of IL-8, HGF, and IL-3 as compared to healthy control (HC)-derived cell populations.

Conclusion: T2DM PAC are phenotypically and functionally altered compared to PAC from HC. Differences between DR and NoDR PAC are limited. We propose that impaired T2DM PAC provide inadequate vascular support and promote compensatory, albeit pathological, retinal neovascularization.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11182312PMC
http://dx.doi.org/10.3389/fopht.2023.1119050DOI Listing

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