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Induction of retinopathy by fibrillar oxalate assemblies

Medicine and Health

Induction of retinopathy by fibrillar oxalate assemblies

D. Zaguri, S. Shaham-niv, et al.

This groundbreaking research by Dor Zaguri and colleagues uncovers a novel aspect of human metabolic disorders, revealing that oxalate can create ordered fibrils, leading to retinal cytotoxicity and dysfunction in animal models. The findings not only reflect patterns seen in hyperoxaluria patients but also introduce a new molecular insight into oxalate-associated diseases.... show more
Abstract
The formation of metabolite fibrillar assemblies represents a paradigm shift in the study of human metabolic disorders. Yet, direct clinical relevance has been attributed only to metabolite crystals. A notable example for metabolite crystallization is calcium oxalate crystals observed in various diseases, including primary hyperoxaluria. We unexpectedly observed retinal damage among young hyperoxaluria patients in the absence of crystals. Exploring the possible formation of alternative supramolecular organizations and their biological role, here we show that oxalate can form ordered fibrils with no associated calcium. These fibrils inflict intense retinal cytotoxicity in cultured cells. A rat model injected with oxalate fibrils recaptures patterns of retinal dysfunction observed in patients. Antibodies purified from hyperoxaluria patient sera recognize oxalate fibrils regardless of the presence of calcium. These findings highlight a new molecular basis for oxalate-associated disease, and to our knowledge provide the first direct clinical indication for the pathogenic role of metabolite fibrillar assemblies.
Publisher
Communications Chemistry
Published On
Jan 03, 2020
Authors
Dor Zaguri, Shira Shaham-Niv, Efrat Naaman, Michael Mimouni, Daniella Magen, Shirley Pollack, Topaz Kreiser, Rina Leibu, Sigal Rencus-Lazar, Lihi Adler-Abramovich, Ido Perlman, Ehud Gazit, Shiri Zayit-Soudry
Tags
oxalate
fibrils
retinal dysfunction
metabolic disorders
hyperoxaluria
cytotoxicity
molecular basis
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