PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing

Domagoj Cikes; Kareem Elsayad; Erdinc Sezgin; Erika Koitai; Torma Ferenc; Michael Orthofer; Rebecca Yarwood; Leonhard X. Heinz; Vitaly Sedlyarov; Nasser Darwish Miranda; Adrian Taylor; Sophie Grapentine; Fathiya al-Murshedi; Anne Abot; Adelheid Weidinger; Candice Kutchukian; Colline Sanchez; Shane J.F. Cronin; Maria Novatchkova; Anoop Kavirayani; Thomas Schuetz; Bernhard Haubner; Lisa Haas; Astrid Hagelkruys; Suzanne Jackowski; Andrey Kozlov; Vincent Jacquemond; Claude Knauf; Giulio Superti-Furga; Eric Rullman; Thomas Gustafsson; John McDermot; Martin Lowe; Zsolt Radak; Jeffrey S. Chamberlain; Marica Bakovic; Siddharth Banka; Josef M. Penninger

doi:10.1038/s42255-023-00766-2

PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing

Domagoj Cikes^*, Kareem Elsayad^*, Erdinc Sezgin, Erika Koitai, Torma Ferenc, Michael Orthofer, Rebecca Yarwood, Leonhard X. Heinz, Vitaly Sedlyarov, Nasser Darwish Miranda, Adrian Taylor, Sophie Grapentine, Fathiya al-Murshedi, Anne Abot, Adelheid Weidinger, Candice Kutchukian, Colline Sanchez, Shane J.F. Cronin, Maria Novatchkova, Anoop KavirayaniThomas Schuetz, Bernhard Haubner, Lisa Haas, Astrid Hagelkruys, Suzanne Jackowski, Andrey Kozlov, Vincent Jacquemond, Claude Knauf, Giulio Superti-Furga, Eric Rullman, Thomas Gustafsson, John McDermot, Martin Lowe, Zsolt Radak, Jeffrey S. Chamberlain, Marica Bakovic, Siddharth Banka, Josef M. Penninger^*

^*المؤلف المقابل لهذا العمل

Genetics

نتاج البحث: المساهمة في مجلة › Article › مراجعة النظراء

5 اقتباسات (Scopus)

ملخص

Muscle degeneration is the most prevalent cause for frailty and dependency in inherited diseases and ageing. Elucidation of pathophysiological mechanisms, as well as effective treatments for muscle diseases, represents an important goal in improving human health. Here, we show that the lipid synthesis enzyme phosphatidylethanolamine cytidyltransferase (PCYT2/ECT) is critical to muscle health. Human deficiency in PCYT2 causes a severe disease with failure to thrive and progressive weakness. pcyt2-mutant zebrafish and muscle-specific Pcyt2-knockout mice recapitulate the participant phenotypes, with failure to thrive, progressive muscle weakness and accelerated ageing. Mechanistically, muscle Pcyt2 deficiency affects cellular bioenergetics and membrane lipid bilayer structure and stability. PCYT2 activity declines in ageing muscles of mice and humans, and adeno-associated virus-based delivery of PCYT2 ameliorates muscle weakness in Pcyt2-knockout and old mice, offering a therapy for individuals with a rare disease and muscle ageing. Thus, PCYT2 plays a fundamental and conserved role in vertebrate muscle health, linking PCYT2 and PCYT2-synthesized lipids to severe muscle dystrophy and ageing.

اللغة الأصلية	English
الصفحات (من إلى)	495-515
عدد الصفحات	21
دورية	Nature Metabolism
مستوى الصوت	5
رقم الإصدار	3
المعرِّفات الرقمية للأشياء	https://doi.org/10.1038/s42255-023-00766-2
حالة النشر	Published - مارس 20 2023

ASJC Scopus subject areas

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أهداف الأمم المتحدة للتنمية المستدامة

يساهم هذا المخرج في تحقيق أهداف الأمم المتحدة للتنمية المستدامة التالية (SDGs)

الوصول إلى المستند

10.1038/s42255-023-00766-2

الملفات والروابط الأخرى

قم بذكر هذا

Cikes, D., Elsayad, K., Sezgin, E., Koitai, E., Ferenc, T., Orthofer, M., Yarwood, R., Heinz, L. X., Sedlyarov, V., Miranda, N. D., Taylor, A., Grapentine, S., al-Murshedi, F., Abot, A., Weidinger, A., Kutchukian, C., Sanchez, C., Cronin, S. J. F., Novatchkova, M., ... Penninger, J. M. (2023). PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing. Nature Metabolism, 5(3), 495-515. https://doi.org/10.1038/s42255-023-00766-2

Cikes, D, Elsayad, K, Sezgin, E, Koitai, E, Ferenc, T, Orthofer, M, Yarwood, R, Heinz, LX, Sedlyarov, V, Miranda, ND, Taylor, A, Grapentine, S, al-Murshedi, F, Abot, A, Weidinger, A, Kutchukian, C, Sanchez, C, Cronin, SJF, Novatchkova, M, Kavirayani, A, Schuetz, T, Haubner, B, Haas, L, Hagelkruys, A, Jackowski, S, Kozlov, A, Jacquemond, V, Knauf, C, Superti-Furga, G, Rullman, E, Gustafsson, T, McDermot, J, Lowe, M, Radak, Z, Chamberlain, JS, Bakovic, M, Banka, S & Penninger, JM 2023, 'PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing', Nature Metabolism, المجلد 5, رقم 3, الصفحات 495-515. https://doi.org/10.1038/s42255-023-00766-2

@article{e59959cfa237433b94015fa590bfa9ba,

title = "PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing",

abstract = "Muscle degeneration is the most prevalent cause for frailty and dependency in inherited diseases and ageing. Elucidation of pathophysiological mechanisms, as well as effective treatments for muscle diseases, represents an important goal in improving human health. Here, we show that the lipid synthesis enzyme phosphatidylethanolamine cytidyltransferase (PCYT2/ECT) is critical to muscle health. Human deficiency in PCYT2 causes a severe disease with failure to thrive and progressive weakness. pcyt2-mutant zebrafish and muscle-specific Pcyt2-knockout mice recapitulate the participant phenotypes, with failure to thrive, progressive muscle weakness and accelerated ageing. Mechanistically, muscle Pcyt2 deficiency affects cellular bioenergetics and membrane lipid bilayer structure and stability. PCYT2 activity declines in ageing muscles of mice and humans, and adeno-associated virus-based delivery of PCYT2 ameliorates muscle weakness in Pcyt2-knockout and old mice, offering a therapy for individuals with a rare disease and muscle ageing. Thus, PCYT2 plays a fundamental and conserved role in vertebrate muscle health, linking PCYT2 and PCYT2-synthesized lipids to severe muscle dystrophy and ageing.",

keywords = "Animals, Humans, Mice, Failure to Thrive, Mice, Knockout, Muscle Weakness/genetics, Muscles, RNA Nucleotidyltransferases/chemistry, Zebrafish",

author = "Domagoj Cikes and Kareem Elsayad and Erdinc Sezgin and Erika Koitai and Torma Ferenc and Michael Orthofer and Rebecca Yarwood and Heinz, {Leonhard X.} and Vitaly Sedlyarov and Miranda, {Nasser Darwish} and Adrian Taylor and Sophie Grapentine and Fathiya al-Murshedi and Anne Abot and Adelheid Weidinger and Candice Kutchukian and Colline Sanchez and Cronin, {Shane J.F.} and Maria Novatchkova and Anoop Kavirayani and Thomas Schuetz and Bernhard Haubner and Lisa Haas and Astrid Hagelkruys and Suzanne Jackowski and Andrey Kozlov and Vincent Jacquemond and Claude Knauf and Giulio Superti-Furga and Eric Rullman and Thomas Gustafsson and John McDermot and Martin Lowe and Zsolt Radak and Chamberlain, {Jeffrey S.} and Marica Bakovic and Siddharth Banka and Penninger, {Josef M.}",

note = "Funding Information: The authors thank the participants and their families for participating in the study. We thank all members of our laboratories for helpful discussions. We are grateful to Vienna BioCenter Core Facilities: Mouse Phenotyping Unit, Histopathology Unit, Bioinformatics Unit, BioOptics Unit, Electron Microscopy Unit and Comparative Medicine Unit. We are grateful to the Lipidomics Facility, and K. Klavins and T. Hannich at the CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences for assistance with lipidomics analysis. We also thank T. Huan and A. Hui (UBC Vancouver) for mouse tissue and mitochondria lipidomics analysis. We thank A. Klymchenko (Laboratoire de Bioimagerie et Pathologies Universit{\'e} de Strasbourg, Strasbourg, France) for providing the NR12S probe. We are thankful to the Sen. Paul D. Wellstone Muscular Dystrophy Cooperative Specialized Research Center Viral Vector Core Facility for AAV6 production. We also thank K. P. Campbell and M. E. Anderson (University of Iowa, Carver College of Medicine) for advice on muscle tissue handling. We thank A. Al-Qassabi from the Sultan Qaboos University for the clinical assessment of the participants. D.C. and J.M.P. are supported by the Austrian Federal Ministry of Education, Science and Research, the Austrian Academy of Sciences, and the City of Vienna, and grants from the Austrian Science Fund (FWF) Wittgenstein award (Z 271-B19), the T. von Zastrow Foundation, and a Canada 150 Research Chairs Program (F18-01336). J.S.C. is supported by grants RO1AR44533 and P50AR065139 from the US National Institutes of Health. C.K. is supported by a grant from the Agence Nationale de la Recherche (ANR-18-CE14-0007-01). A.V.K. is supported by European Union{\textquoteright}s Horizon 2020 research and innovation programme under the Marie Sk{\l}odowska-Curie grant agreement no. 67544, and an Austrian Science Fund (FWF; no P-33799). A.W. is supported by Austrian Research Promotion Agency (FFG) project no 867674. E.S. is supported by a SciLifeLab fellowship and Karolinska Institutet Foundation Grants. Work in the laboratory of G.S.-F. is supported by the Austrian Academy of Sciences, the European Research Council (ERC AdG 695214 GameofGates) and the Innovative Medicines Initiative 2 Joint Undertaking (grant agreement no. 777372, ReSOLUTE). S.B., M.L. and R.Y. acknowledge the support of the Spastic Paraplegia Foundation. Funding Information: The authors thank the participants and their families for participating in the study. We thank all members of our laboratories for helpful discussions. We are grateful to Vienna BioCenter Core Facilities: Mouse Phenotyping Unit, Histopathology Unit, Bioinformatics Unit, BioOptics Unit, Electron Microscopy Unit and Comparative Medicine Unit. We are grateful to the Lipidomics Facility, and K. Klavins and T. Hannich at the CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences for assistance with lipidomics analysis. We also thank T. Huan and A. Hui (UBC Vancouver) for mouse tissue and mitochondria lipidomics analysis. We thank A. Klymchenko (Laboratoire de Bioimagerie et Pathologies Universit{\'e} de Strasbourg, Strasbourg, France) for providing the NR12S probe. We are thankful to the Sen. Paul D. Wellstone Muscular Dystrophy Cooperative Specialized Research Center Viral Vector Core Facility for AAV6 production. We also thank K. P. Campbell and M. E. Anderson (University of Iowa, Carver College of Medicine) for advice on muscle tissue handling. We thank A. Al-Qassabi from the Sultan Qaboos University for the clinical assessment of the participants. D.C. and J.M.P. are supported by the Austrian Federal Ministry of Education, Science and Research, the Austrian Academy of Sciences, and the City of Vienna, and grants from the Austrian Science Fund (FWF) Wittgenstein award (Z 271-B19), the T. von Zastrow Foundation, and a Canada 150 Research Chairs Program (F18-01336). J.S.C. is supported by grants RO1AR44533 and P50AR065139 from the US National Institutes of Health. C.K. is supported by a grant from the Agence Nationale de la Recherche (ANR-18-CE14-0007-01). A.V.K. is supported by European Union{\textquoteright}s Horizon 2020 research and innovation programme under the Marie Sk{\l}odowska-Curie grant agreement no. 67544, and an Austrian Science Fund (FWF; no P-33799). A.W. is supported by Austrian Research Promotion Agency (FFG) project no 867674. E.S. is supported by a SciLifeLab fellowship and Karolinska Institutet Foundation Grants. Work in the laboratory of G.S.-F. is supported by the Austrian Academy of Sciences, the European Research Council (ERC AdG 695214 GameofGates) and the Innovative Medicines Initiative 2 Joint Undertaking (grant agreement no. 777372, ReSOLUTE). S.B., M.L. and R.Y. acknowledge the support of the Spastic Paraplegia Foundation. Publisher Copyright: {\textcopyright} 2023, The Author(s), under exclusive licence to Springer Nature Limited. {\textcopyright} 2023. The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2023",

month = mar,

day = "20",

doi = "10.1038/s42255-023-00766-2",

language = "English",

volume = "5",

pages = "495--515",

journal = "Nature Metabolism",

issn = "2522-5812",

publisher = "Springer Berlin",

number = "3",

}

TY - JOUR

T1 - PCYT2-regulated lipid biosynthesis is critical to muscle health and ageing

AU - Cikes, Domagoj

AU - Elsayad, Kareem

AU - Sezgin, Erdinc

AU - Koitai, Erika

AU - Ferenc, Torma

AU - Orthofer, Michael

AU - Yarwood, Rebecca

AU - Heinz, Leonhard X.

AU - Sedlyarov, Vitaly

AU - Miranda, Nasser Darwish

AU - Taylor, Adrian

AU - Grapentine, Sophie

AU - al-Murshedi, Fathiya

AU - Abot, Anne

AU - Weidinger, Adelheid

AU - Kutchukian, Candice

AU - Sanchez, Colline

AU - Cronin, Shane J.F.

AU - Novatchkova, Maria

AU - Kavirayani, Anoop

AU - Schuetz, Thomas

AU - Haubner, Bernhard

AU - Haas, Lisa

AU - Hagelkruys, Astrid

AU - Jackowski, Suzanne

AU - Kozlov, Andrey

AU - Jacquemond, Vincent

AU - Knauf, Claude

AU - Superti-Furga, Giulio

AU - Rullman, Eric

AU - Gustafsson, Thomas

AU - McDermot, John

AU - Lowe, Martin

AU - Radak, Zsolt

AU - Chamberlain, Jeffrey S.

AU - Bakovic, Marica

AU - Banka, Siddharth

AU - Penninger, Josef M.

N1 - Funding Information: The authors thank the participants and their families for participating in the study. We thank all members of our laboratories for helpful discussions. We are grateful to Vienna BioCenter Core Facilities: Mouse Phenotyping Unit, Histopathology Unit, Bioinformatics Unit, BioOptics Unit, Electron Microscopy Unit and Comparative Medicine Unit. We are grateful to the Lipidomics Facility, and K. Klavins and T. Hannich at the CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences for assistance with lipidomics analysis. We also thank T. Huan and A. Hui (UBC Vancouver) for mouse tissue and mitochondria lipidomics analysis. We thank A. Klymchenko (Laboratoire de Bioimagerie et Pathologies Université de Strasbourg, Strasbourg, France) for providing the NR12S probe. We are thankful to the Sen. Paul D. Wellstone Muscular Dystrophy Cooperative Specialized Research Center Viral Vector Core Facility for AAV6 production. We also thank K. P. Campbell and M. E. Anderson (University of Iowa, Carver College of Medicine) for advice on muscle tissue handling. We thank A. Al-Qassabi from the Sultan Qaboos University for the clinical assessment of the participants. D.C. and J.M.P. are supported by the Austrian Federal Ministry of Education, Science and Research, the Austrian Academy of Sciences, and the City of Vienna, and grants from the Austrian Science Fund (FWF) Wittgenstein award (Z 271-B19), the T. von Zastrow Foundation, and a Canada 150 Research Chairs Program (F18-01336). J.S.C. is supported by grants RO1AR44533 and P50AR065139 from the US National Institutes of Health. C.K. is supported by a grant from the Agence Nationale de la Recherche (ANR-18-CE14-0007-01). A.V.K. is supported by European Union’s Horizon 2020 research and innovation programme under the Marie Skłodowska-Curie grant agreement no. 67544, and an Austrian Science Fund (FWF; no P-33799). A.W. is supported by Austrian Research Promotion Agency (FFG) project no 867674. E.S. is supported by a SciLifeLab fellowship and Karolinska Institutet Foundation Grants. Work in the laboratory of G.S.-F. is supported by the Austrian Academy of Sciences, the European Research Council (ERC AdG 695214 GameofGates) and the Innovative Medicines Initiative 2 Joint Undertaking (grant agreement no. 777372, ReSOLUTE). S.B., M.L. and R.Y. acknowledge the support of the Spastic Paraplegia Foundation. Funding Information: The authors thank the participants and their families for participating in the study. We thank all members of our laboratories for helpful discussions. We are grateful to Vienna BioCenter Core Facilities: Mouse Phenotyping Unit, Histopathology Unit, Bioinformatics Unit, BioOptics Unit, Electron Microscopy Unit and Comparative Medicine Unit. We are grateful to the Lipidomics Facility, and K. Klavins and T. Hannich at the CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences for assistance with lipidomics analysis. We also thank T. Huan and A. Hui (UBC Vancouver) for mouse tissue and mitochondria lipidomics analysis. We thank A. Klymchenko (Laboratoire de Bioimagerie et Pathologies Université de Strasbourg, Strasbourg, France) for providing the NR12S probe. We are thankful to the Sen. Paul D. Wellstone Muscular Dystrophy Cooperative Specialized Research Center Viral Vector Core Facility for AAV6 production. We also thank K. P. Campbell and M. E. Anderson (University of Iowa, Carver College of Medicine) for advice on muscle tissue handling. We thank A. Al-Qassabi from the Sultan Qaboos University for the clinical assessment of the participants. D.C. and J.M.P. are supported by the Austrian Federal Ministry of Education, Science and Research, the Austrian Academy of Sciences, and the City of Vienna, and grants from the Austrian Science Fund (FWF) Wittgenstein award (Z 271-B19), the T. von Zastrow Foundation, and a Canada 150 Research Chairs Program (F18-01336). J.S.C. is supported by grants RO1AR44533 and P50AR065139 from the US National Institutes of Health. C.K. is supported by a grant from the Agence Nationale de la Recherche (ANR-18-CE14-0007-01). A.V.K. is supported by European Union’s Horizon 2020 research and innovation programme under the Marie Skłodowska-Curie grant agreement no. 67544, and an Austrian Science Fund (FWF; no P-33799). A.W. is supported by Austrian Research Promotion Agency (FFG) project no 867674. E.S. is supported by a SciLifeLab fellowship and Karolinska Institutet Foundation Grants. Work in the laboratory of G.S.-F. is supported by the Austrian Academy of Sciences, the European Research Council (ERC AdG 695214 GameofGates) and the Innovative Medicines Initiative 2 Joint Undertaking (grant agreement no. 777372, ReSOLUTE). S.B., M.L. and R.Y. acknowledge the support of the Spastic Paraplegia Foundation. Publisher Copyright: © 2023, The Author(s), under exclusive licence to Springer Nature Limited. © 2023. The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2023/3/20

Y1 - 2023/3/20

N2 - Muscle degeneration is the most prevalent cause for frailty and dependency in inherited diseases and ageing. Elucidation of pathophysiological mechanisms, as well as effective treatments for muscle diseases, represents an important goal in improving human health. Here, we show that the lipid synthesis enzyme phosphatidylethanolamine cytidyltransferase (PCYT2/ECT) is critical to muscle health. Human deficiency in PCYT2 causes a severe disease with failure to thrive and progressive weakness. pcyt2-mutant zebrafish and muscle-specific Pcyt2-knockout mice recapitulate the participant phenotypes, with failure to thrive, progressive muscle weakness and accelerated ageing. Mechanistically, muscle Pcyt2 deficiency affects cellular bioenergetics and membrane lipid bilayer structure and stability. PCYT2 activity declines in ageing muscles of mice and humans, and adeno-associated virus-based delivery of PCYT2 ameliorates muscle weakness in Pcyt2-knockout and old mice, offering a therapy for individuals with a rare disease and muscle ageing. Thus, PCYT2 plays a fundamental and conserved role in vertebrate muscle health, linking PCYT2 and PCYT2-synthesized lipids to severe muscle dystrophy and ageing.

AB - Muscle degeneration is the most prevalent cause for frailty and dependency in inherited diseases and ageing. Elucidation of pathophysiological mechanisms, as well as effective treatments for muscle diseases, represents an important goal in improving human health. Here, we show that the lipid synthesis enzyme phosphatidylethanolamine cytidyltransferase (PCYT2/ECT) is critical to muscle health. Human deficiency in PCYT2 causes a severe disease with failure to thrive and progressive weakness. pcyt2-mutant zebrafish and muscle-specific Pcyt2-knockout mice recapitulate the participant phenotypes, with failure to thrive, progressive muscle weakness and accelerated ageing. Mechanistically, muscle Pcyt2 deficiency affects cellular bioenergetics and membrane lipid bilayer structure and stability. PCYT2 activity declines in ageing muscles of mice and humans, and adeno-associated virus-based delivery of PCYT2 ameliorates muscle weakness in Pcyt2-knockout and old mice, offering a therapy for individuals with a rare disease and muscle ageing. Thus, PCYT2 plays a fundamental and conserved role in vertebrate muscle health, linking PCYT2 and PCYT2-synthesized lipids to severe muscle dystrophy and ageing.

KW - Animals

KW - Humans

KW - Mice

KW - Failure to Thrive

KW - Mice, Knockout

KW - Muscle Weakness/genetics

KW - Muscles

KW - RNA Nucleotidyltransferases/chemistry

KW - Zebrafish

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UR - http://www.scopus.com/inward/citedby.url?scp=85150446406&partnerID=8YFLogxK

UR - https://www.mendeley.com/catalogue/6148385e-0073-304e-a86b-595b091ba168/

U2 - 10.1038/s42255-023-00766-2

DO - 10.1038/s42255-023-00766-2

M3 - Article

C2 - 36941451

AN - SCOPUS:85150446406

SN - 2522-5812

VL - 5

SP - 495

EP - 515

JO - Nature Metabolism

JF - Nature Metabolism

IS - 3

ER -