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CD44 signaling in Müller cells impacts photoreceptor function and survival in healthy and diseased retinas

Monika Ayten, Tobias Straub, Lew Kaplan, Stefanie M. Hauck, Antje Grosche, Susanne Koch

2024Journal of Neuroinflammation26 citationsDOIOpen Access PDF

Abstract

Abstract Retinitis pigmentosa (RP), an inherited retinal disease, affects 1,5 million people worldwide. The initial mutation-driven photoreceptor degeneration leads to chronic inflammation, characterized by Müller cell activation and upregulation of CD44. CD44 is a cell surface transmembrane glycoprotein and the primary receptor for hyaluronic acid. It is involved in many pathological processes, but little is known about CD44’s retinal functions. CD44 expression is also increased in Müller cells from our Pde6b STOP/STOP RP mouse model. To gain a more detailed understanding of CD44’s role in healthy and diseased retinas, we analyzed Cd44 −/− and Cd44 −/− Pde6b STOP/STOP mice, respectively. The loss of CD44 led to enhanced photoreceptor degeneration, reduced retinal function, and increased inflammatory response. To understand the underlying mechanism, we performed proteomic analysis on isolated Müller cells from Cd44 −/− and Cd44 −/− Pde6b STOP/STOP retinas and identified a significant downregulation of glutamate transporter 1 (SLC1A2). This downregulation was accompanied by higher glutamate levels, suggesting impaired glutamate homeostasis. These novel findings indicate that CD44 stimulates glutamate uptake via SLC1A2 in Müller cells, which in turn, supports photoreceptor survival and function.

Topics & Concepts

Retinitis pigmentosaDownregulation and upregulationCD44Retinal regenerationCell biologyRetinal degenerationBiologyNeuroscienceRetinaCellRegeneration (biology)BiochemistryGeneRetinal Development and DisordersRetinal Diseases and TreatmentsConnexins and lens biology