Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration

Renza Spelat; Federico Ferro; Paolo Contessotto; Amal Aljaabary; Sergio Martin-Saldaña; Chunsheng Jin; Niclas G. Karlsson; Maura Grealy; Markus M. Hilscher; Fulvio Magni; Clizia Chinello; Michelle Kilcoyne; Abhay Pandit

doi:10.1038/s42003-022-04328-2

Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration

Renza Spelat, Federico Ferro, Paolo Contessotto, Amal Aljaabary, Sergio Martin-Saldaña, Chunsheng Jin, Niclas G. Karlsson, Maura Grealy, Markus M. Hilscher, Fulvio Magni, Clizia Chinello, Michelle Kilcoyne, Abhay Pandit

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Abstract

The ability of the zebrafish heart to regenerate following injury makes it a valuable model to deduce why this capability in mammals is limited to early neonatal stages. Although metabolic reprogramming and glycosylation remodeling have emerged as key aspects in many biological processes, how they may trigger a cardiac regenerative response in zebrafish is still a crucial question. Here, by using an up-to-date panel of transcriptomic, proteomic and glycomic approaches, we identify a metabolic switch from mitochondrial oxidative phosphorylation to glycolysis associated with membrane glycosylation remodeling during heart regeneration. Importantly, we establish the N- and O-linked glycan structural repertoire of the regenerating zebrafish heart, and link alterations in both sialylation and high mannose structures across the phases of regeneration. Our results show that metabolic reprogramming and glycan structural remodeling are potential drivers of tissue regeneration after cardiac injury, providing the biological rationale to develop novel therapeutics to elicit heart regeneration in mammals.

Original language	English
Article number	1365
Journal	Communications Biology
Volume	5
Issue number	1
DOIs	https://doi.org/10.1038/s42003-022-04328-2
Publication status	Published - Dec 2022

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Spelat, R., Ferro, F., Contessotto, P., Aljaabary, A., Martin-Saldaña, S., Jin, C., Karlsson, N. G., Grealy, M., Hilscher, M. M., Magni, F., Chinello, C., Kilcoyne, M., & Pandit, A. (2022). Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration. Communications Biology, 5(1), Article 1365. https://doi.org/10.1038/s42003-022-04328-2

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abstract = "The ability of the zebrafish heart to regenerate following injury makes it a valuable model to deduce why this capability in mammals is limited to early neonatal stages. Although metabolic reprogramming and glycosylation remodeling have emerged as key aspects in many biological processes, how they may trigger a cardiac regenerative response in zebrafish is still a crucial question. Here, by using an up-to-date panel of transcriptomic, proteomic and glycomic approaches, we identify a metabolic switch from mitochondrial oxidative phosphorylation to glycolysis associated with membrane glycosylation remodeling during heart regeneration. Importantly, we establish the N- and O-linked glycan structural repertoire of the regenerating zebrafish heart, and link alterations in both sialylation and high mannose structures across the phases of regeneration. Our results show that metabolic reprogramming and glycan structural remodeling are potential drivers of tissue regeneration after cardiac injury, providing the biological rationale to develop novel therapeutics to elicit heart regeneration in mammals.",

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doi = "10.1038/s42003-022-04328-2",

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T1 - Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration

AU - Spelat, Renza

AU - Ferro, Federico

AU - Contessotto, Paolo

AU - Aljaabary, Amal

AU - Martin-Saldaña, Sergio

AU - Jin, Chunsheng

AU - Karlsson, Niclas G.

AU - Grealy, Maura

AU - Hilscher, Markus M.

AU - Magni, Fulvio

AU - Chinello, Clizia

AU - Kilcoyne, Michelle

AU - Pandit, Abhay

PY - 2022/12

Y1 - 2022/12

N2 - The ability of the zebrafish heart to regenerate following injury makes it a valuable model to deduce why this capability in mammals is limited to early neonatal stages. Although metabolic reprogramming and glycosylation remodeling have emerged as key aspects in many biological processes, how they may trigger a cardiac regenerative response in zebrafish is still a crucial question. Here, by using an up-to-date panel of transcriptomic, proteomic and glycomic approaches, we identify a metabolic switch from mitochondrial oxidative phosphorylation to glycolysis associated with membrane glycosylation remodeling during heart regeneration. Importantly, we establish the N- and O-linked glycan structural repertoire of the regenerating zebrafish heart, and link alterations in both sialylation and high mannose structures across the phases of regeneration. Our results show that metabolic reprogramming and glycan structural remodeling are potential drivers of tissue regeneration after cardiac injury, providing the biological rationale to develop novel therapeutics to elicit heart regeneration in mammals.

AB - The ability of the zebrafish heart to regenerate following injury makes it a valuable model to deduce why this capability in mammals is limited to early neonatal stages. Although metabolic reprogramming and glycosylation remodeling have emerged as key aspects in many biological processes, how they may trigger a cardiac regenerative response in zebrafish is still a crucial question. Here, by using an up-to-date panel of transcriptomic, proteomic and glycomic approaches, we identify a metabolic switch from mitochondrial oxidative phosphorylation to glycolysis associated with membrane glycosylation remodeling during heart regeneration. Importantly, we establish the N- and O-linked glycan structural repertoire of the regenerating zebrafish heart, and link alterations in both sialylation and high mannose structures across the phases of regeneration. Our results show that metabolic reprogramming and glycan structural remodeling are potential drivers of tissue regeneration after cardiac injury, providing the biological rationale to develop novel therapeutics to elicit heart regeneration in mammals.

UR - https://www.scopus.com/pages/publications/85143993234

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DO - 10.1038/s42003-022-04328-2

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SN - 2399-3642

VL - 5

JO - Communications Biology

JF - Communications Biology

IS - 1

M1 - 1365

ER -

Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration

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