A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome

We report on the unexpected finding that click modification of iduronyl azides results in a conformational flip of the pyranose ring, which led to the development of a new strategy for the design of superior enzyme substrates for the diagnostic assaying of iduronate-2-sulfatase (I2S), a lysosomal en...

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Autores principales: Schwarz, Markus, Skrinjar, Philipp, Fink, Michael J., Kronister, Stefan, Mechtler, Thomas, Koukos, Panagiotis I., Bonvin, Alexandre M. J. J., Kasper, David C., Mikula, Hannes
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2020
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8163285/
https://www.ncbi.nlm.nih.gov/pubmed/34094461
http://dx.doi.org/10.1039/d0sc04696e
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author Schwarz, Markus
Skrinjar, Philipp
Fink, Michael J.
Kronister, Stefan
Mechtler, Thomas
Koukos, Panagiotis I.
Bonvin, Alexandre M. J. J.
Kasper, David C.
Mikula, Hannes
author_facet Schwarz, Markus
Skrinjar, Philipp
Fink, Michael J.
Kronister, Stefan
Mechtler, Thomas
Koukos, Panagiotis I.
Bonvin, Alexandre M. J. J.
Kasper, David C.
Mikula, Hannes
author_sort Schwarz, Markus
collection PubMed
description We report on the unexpected finding that click modification of iduronyl azides results in a conformational flip of the pyranose ring, which led to the development of a new strategy for the design of superior enzyme substrates for the diagnostic assaying of iduronate-2-sulfatase (I2S), a lysosomal enzyme related to Hunter syndrome. Synthetic substrates are essential in testing newborns for metabolic disorders to enable early initiation of therapy. Our click-flipped iduronyl triazole showed a remarkably better performance with I2S than commonly used O-iduronates. We found that both O- and triazole-linked substrates are accepted by the enzyme, irrespective of their different conformations, but only the O-linked product inhibits the activity of I2S. Thus, in the long reaction times required for clinical assays, the triazole substrate substantially outperforms the O-iduronate. Applying our click-flipped substrate to assay I2S in dried blood spots sampled from affected patients and random newborns significantly increased the confidence in discriminating between these groups, clearly indicating the potential of the click-flip strategy to control the biomolecular function of carbohydrates.
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spelling pubmed-81632852021-06-04 A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome Schwarz, Markus Skrinjar, Philipp Fink, Michael J. Kronister, Stefan Mechtler, Thomas Koukos, Panagiotis I. Bonvin, Alexandre M. J. J. Kasper, David C. Mikula, Hannes Chem Sci Chemistry We report on the unexpected finding that click modification of iduronyl azides results in a conformational flip of the pyranose ring, which led to the development of a new strategy for the design of superior enzyme substrates for the diagnostic assaying of iduronate-2-sulfatase (I2S), a lysosomal enzyme related to Hunter syndrome. Synthetic substrates are essential in testing newborns for metabolic disorders to enable early initiation of therapy. Our click-flipped iduronyl triazole showed a remarkably better performance with I2S than commonly used O-iduronates. We found that both O- and triazole-linked substrates are accepted by the enzyme, irrespective of their different conformations, but only the O-linked product inhibits the activity of I2S. Thus, in the long reaction times required for clinical assays, the triazole substrate substantially outperforms the O-iduronate. Applying our click-flipped substrate to assay I2S in dried blood spots sampled from affected patients and random newborns significantly increased the confidence in discriminating between these groups, clearly indicating the potential of the click-flip strategy to control the biomolecular function of carbohydrates. The Royal Society of Chemistry 2020-10-23 /pmc/articles/PMC8163285/ /pubmed/34094461 http://dx.doi.org/10.1039/d0sc04696e Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by-nc/3.0/
spellingShingle Chemistry
Schwarz, Markus
Skrinjar, Philipp
Fink, Michael J.
Kronister, Stefan
Mechtler, Thomas
Koukos, Panagiotis I.
Bonvin, Alexandre M. J. J.
Kasper, David C.
Mikula, Hannes
A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome
title A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome
title_full A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome
title_fullStr A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome
title_full_unstemmed A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome
title_short A click-flipped enzyme substrate boosts the performance of the diagnostic screening for Hunter syndrome
title_sort click-flipped enzyme substrate boosts the performance of the diagnostic screening for hunter syndrome
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8163285/
https://www.ncbi.nlm.nih.gov/pubmed/34094461
http://dx.doi.org/10.1039/d0sc04696e
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