N1-methylnicotinamide is a signalling molecule produced in skeletal muscle coordinating energy metabolism

Kristoffer Ström; David Morales-Alamo; Filip Ottosson; Anna Edlund; Line Hjort; Sine W. Jörgensen; Peter Almgren; Yuedan Zhou; Marcos Martin-Rincon; Carl Ekman; Alberto Pérez-López; Ola Ekström; Ismael Perez-Suarez; Markus Mattiasson; Pedro De Pablos-Velasco; Nikolay Oskolkov; Emma Ahlqvist; Nils Wierup; Lena Eliasson; Allan Vaag; Leif Groop; Karin G. Stenkula; Céline Fernandez; Jose A.L. Calbet; Hans Christer Holmberg; Ola Hansson

doi:10.1038/s41598-018-21099-1

N¹-methylnicotinamide is a signalling molecule produced in skeletal muscle coordinating energy metabolism

Kristoffer Ström, David Morales-Alamo, Filip Ottosson, Anna Edlund, Line Hjort, Sine W. Jörgensen, Peter Almgren, Yuedan Zhou, Marcos Martin-Rincon, Carl Ekman, Alberto Pérez-López, Ola Ekström, Ismael Perez-Suarez, Markus Mattiasson, Pedro De Pablos-Velasco, Nikolay Oskolkov, Emma Ahlqvist, Nils Wierup, Lena Eliasson, Allan VaagLeif Groop, Karin G. Stenkula, Céline Fernandez, Jose A.L. Calbet, Hans Christer Holmberg, Ola Hansson

Forskningsoutput: Tidskriftsbidrag › Artikel i vetenskaplig tidskrift › Peer review

Sammanfattning

Obesity is a major health problem, and although caloric restriction and exercise are successful strategies to lose adipose tissue in obese individuals, a simultaneous decrease in skeletal muscle mass, negatively effects metabolism and muscle function. To deeper understand molecular events occurring in muscle during weight-loss, we measured the expressional change in human skeletal muscle following a combination of severe caloric restriction and exercise over 4 days in 15 Swedish men. Key metabolic genes were regulated after the intervention, indicating a shift from carbohydrate to fat metabolism. Nicotinamide N-methyltransferase (NNMT) was the most consistently upregulated gene following the energy-deficit exercise. Circulating levels of N¹-methylnicotinamide (MNA), the product of NNMT activity, were doubled after the intervention. The fasting-fed state was an important determinant of plasma MNA levels, peaking at ~18 h of fasting and being lowest ~3 h after a meal. In culture, MNA was secreted by isolated human myotubes and stimulated lipolysis directly, with no effect on glucagon or insulin secretion. We propose that MNA is a novel myokine that enhances the utilization of energy stores in response to low muscle energy availability. Future research should focus on applying MNA as a biomarker to identify individuals with metabolic disturbances at an early stage.

Originalspråk	engelska
Artikelnummer	3016
Tidskrift	Scientific Reports
Volym	8
Nummer	1
DOI	https://doi.org/10.1038/s41598-018-21099-1
Status	Published - 2018 dec. 1

Ämnesklassifikation (UKÄ)

Endokrinologi och diabetes

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10.1038/s41598-018-21099-1

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Ström, K., Morales-Alamo, D., Ottosson, F., Edlund, A., Hjort, L., Jörgensen, S. W., Almgren, P., Zhou, Y., Martin-Rincon, M., Ekman, C., Pérez-López, A., Ekström, O., Perez-Suarez, I., Mattiasson, M., De Pablos-Velasco, P., Oskolkov, N., Ahlqvist, E., Wierup, N., Eliasson, L., ... Hansson, O. (2018). N¹-methylnicotinamide is a signalling molecule produced in skeletal muscle coordinating energy metabolism. Scientific Reports, 8(1), [3016]. https://doi.org/10.1038/s41598-018-21099-1

@article{bde7ce36db9b4b2aa2e3fffdb3fbf67d,

title = "N1-methylnicotinamide is a signalling molecule produced in skeletal muscle coordinating energy metabolism",

abstract = "Obesity is a major health problem, and although caloric restriction and exercise are successful strategies to lose adipose tissue in obese individuals, a simultaneous decrease in skeletal muscle mass, negatively effects metabolism and muscle function. To deeper understand molecular events occurring in muscle during weight-loss, we measured the expressional change in human skeletal muscle following a combination of severe caloric restriction and exercise over 4 days in 15 Swedish men. Key metabolic genes were regulated after the intervention, indicating a shift from carbohydrate to fat metabolism. Nicotinamide N-methyltransferase (NNMT) was the most consistently upregulated gene following the energy-deficit exercise. Circulating levels of N1-methylnicotinamide (MNA), the product of NNMT activity, were doubled after the intervention. The fasting-fed state was an important determinant of plasma MNA levels, peaking at ~18 h of fasting and being lowest ~3 h after a meal. In culture, MNA was secreted by isolated human myotubes and stimulated lipolysis directly, with no effect on glucagon or insulin secretion. We propose that MNA is a novel myokine that enhances the utilization of energy stores in response to low muscle energy availability. Future research should focus on applying MNA as a biomarker to identify individuals with metabolic disturbances at an early stage.",

author = "Kristoffer Str{\"o}m and David Morales-Alamo and Filip Ottosson and Anna Edlund and Line Hjort and J{\"o}rgensen, {Sine W.} and Peter Almgren and Yuedan Zhou and Marcos Martin-Rincon and Carl Ekman and Alberto P{\'e}rez-L{\'o}pez and Ola Ekstr{\"o}m and Ismael Perez-Suarez and Markus Mattiasson and {De Pablos-Velasco}, Pedro and Nikolay Oskolkov and Emma Ahlqvist and Nils Wierup and Lena Eliasson and Allan Vaag and Leif Groop and Stenkula, {Karin G.} and C{\'e}line Fernandez and Calbet, {Jose A.L.} and Holmberg, {Hans Christer} and Ola Hansson",

year = "2018",

month = dec,

day = "1",

doi = "10.1038/s41598-018-21099-1",

language = "English",

volume = "8",

journal = "Scientific Reports",

issn = "2045-2322",

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Ström, K, Morales-Alamo, D, Ottosson, F , Edlund, A, Hjort, L, Jörgensen, SW, Almgren, P, Zhou, Y, Martin-Rincon, M, Ekman, C, Pérez-López, A, Ekström, O, Perez-Suarez, I, Mattiasson, M, De Pablos-Velasco, P, Oskolkov, N, Ahlqvist, E , Wierup, N , Eliasson, L , Vaag, A, Groop, L, Stenkula, KG , Fernandez, C, Calbet, JAL, Holmberg, HC & Hansson, O 2018, 'N¹-methylnicotinamide is a signalling molecule produced in skeletal muscle coordinating energy metabolism', Scientific Reports, vol. 8, nr. 1, 3016. https://doi.org/10.1038/s41598-018-21099-1

TY - JOUR

T1 - N1-methylnicotinamide is a signalling molecule produced in skeletal muscle coordinating energy metabolism

AU - Ström, Kristoffer

AU - Morales-Alamo, David

AU - Ottosson, Filip

AU - Edlund, Anna

AU - Hjort, Line

AU - Jörgensen, Sine W.

AU - Almgren, Peter

AU - Zhou, Yuedan

AU - Martin-Rincon, Marcos

AU - Ekman, Carl

AU - Pérez-López, Alberto

AU - Ekström, Ola

AU - Perez-Suarez, Ismael

AU - Mattiasson, Markus

AU - De Pablos-Velasco, Pedro

AU - Oskolkov, Nikolay

AU - Ahlqvist, Emma

AU - Wierup, Nils

AU - Eliasson, Lena

AU - Vaag, Allan

AU - Groop, Leif

AU - Stenkula, Karin G.

AU - Fernandez, Céline

AU - Calbet, Jose A.L.

AU - Holmberg, Hans Christer

AU - Hansson, Ola

PY - 2018/12/1

Y1 - 2018/12/1

N2 - Obesity is a major health problem, and although caloric restriction and exercise are successful strategies to lose adipose tissue in obese individuals, a simultaneous decrease in skeletal muscle mass, negatively effects metabolism and muscle function. To deeper understand molecular events occurring in muscle during weight-loss, we measured the expressional change in human skeletal muscle following a combination of severe caloric restriction and exercise over 4 days in 15 Swedish men. Key metabolic genes were regulated after the intervention, indicating a shift from carbohydrate to fat metabolism. Nicotinamide N-methyltransferase (NNMT) was the most consistently upregulated gene following the energy-deficit exercise. Circulating levels of N1-methylnicotinamide (MNA), the product of NNMT activity, were doubled after the intervention. The fasting-fed state was an important determinant of plasma MNA levels, peaking at ~18 h of fasting and being lowest ~3 h after a meal. In culture, MNA was secreted by isolated human myotubes and stimulated lipolysis directly, with no effect on glucagon or insulin secretion. We propose that MNA is a novel myokine that enhances the utilization of energy stores in response to low muscle energy availability. Future research should focus on applying MNA as a biomarker to identify individuals with metabolic disturbances at an early stage.

AB - Obesity is a major health problem, and although caloric restriction and exercise are successful strategies to lose adipose tissue in obese individuals, a simultaneous decrease in skeletal muscle mass, negatively effects metabolism and muscle function. To deeper understand molecular events occurring in muscle during weight-loss, we measured the expressional change in human skeletal muscle following a combination of severe caloric restriction and exercise over 4 days in 15 Swedish men. Key metabolic genes were regulated after the intervention, indicating a shift from carbohydrate to fat metabolism. Nicotinamide N-methyltransferase (NNMT) was the most consistently upregulated gene following the energy-deficit exercise. Circulating levels of N1-methylnicotinamide (MNA), the product of NNMT activity, were doubled after the intervention. The fasting-fed state was an important determinant of plasma MNA levels, peaking at ~18 h of fasting and being lowest ~3 h after a meal. In culture, MNA was secreted by isolated human myotubes and stimulated lipolysis directly, with no effect on glucagon or insulin secretion. We propose that MNA is a novel myokine that enhances the utilization of energy stores in response to low muscle energy availability. Future research should focus on applying MNA as a biomarker to identify individuals with metabolic disturbances at an early stage.

U2 - 10.1038/s41598-018-21099-1

DO - 10.1038/s41598-018-21099-1

M3 - Article

C2 - 29445118

AN - SCOPUS:85042133592

VL - 8

JO - Scientific Reports

JF - Scientific Reports

SN - 2045-2322

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