Skeletal-Muscle Metabolic Reprogramming in ALS-SOD1G93A Mice Predates Disease Onset and Is A Promising Therapeutic Target

被引:63
作者
Scaricamazza, Silvia [1 ,2 ]
Salvatori, Illari [2 ]
Giacovazzo, Giacomo [2 ]
Loeffler, Jean Philippe [3 ,4 ]
Rene, Frederique [3 ,4 ]
Rosina, Marco [1 ]
Quessada, Cyril [3 ,4 ]
Proietti, Daisy [2 ]
Heil, Constantin [2 ]
Rossi, Simona [1 ,5 ]
Battistini, Stefania [6 ]
Giannini, Fabio [6 ]
Volpi, Nila [6 ]
Steyn, Frederik J. [7 ,8 ]
Ngo, Shyuan T. [8 ,9 ,10 ]
Ferraro, Elisabetta [11 ]
Madaro, Luca [2 ,12 ]
Coccurello, Roberto [2 ,13 ]
Valle, Cristiana [2 ,5 ]
Ferri, Alberto [2 ,5 ]
机构
[1] Univ Roma Tor Vergata, Dept Biol, Rome, Italy
[2] IRCCS Fdn Santa Lucia, Rome, Italy
[3] Univ Strasbourg, UMR S 1118, Strasbourg, France
[4] Cent & Peripheral Mechanisms Neurodegenerat, INSERM, U1118, Strasbourg, France
[5] CNR, Inst Translat Pharmacol IFT, Rome, Italy
[6] Univ Siena, Dept Med Surg & Neurol Sci, Siena, Italy
[7] Univ Queensland, Sch Biomed Sci, Brisbane, Qld, Australia
[8] Univ Queensland, Ctr Clin Res, Brisbane, Qld, Australia
[9] Univ Queensland, Australian Inst Bioengn & Nanotechnol, Brisbane, Qld, Australia
[10] Univ Queensland, Queensland Brain Inst, Brisbane, Qld, Australia
[11] Univ Pisa, Dept Biol, Pisa, Italy
[12] Sapienza Univ Rome, DAHFMO Unit Histol & Med Embryol, Rome, Italy
[13] CNR, Inst Complex Syst ISC, Rome, Italy
来源
ISCIENCE | 2020年 / 23卷 / 05期
基金
英国医学研究理事会;
关键词
FATTY-ACID OXIDATION; MOUSE MODEL; MITOCHONDRIAL BIOGENESIS; SARCOLIPIN; MECHANISMS; ACCUMULATION; HYPERMETABOLISM; EXPRESSION; INHIBITOR; REGULATOR;
D O I
10.1016/j.isci.2020.101087
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Patients with ALS show, in addition to the loss of motor neurons in the spinal cord, brainstem, and cerebral cortex, an abnormal depletion of energy stores alongside hypermetabolism. In this study, we show that bioenergetic defects and muscle remodeling occur in skeletal muscle of the SOD1(G93A) mouse model of ALS mice prior to disease onset and before the activation of muscle denervation markers, respectively. These changes in muscle physiology were followed by an increase in energy expenditure unrelated to physical activity. Finally, chronic treatment of SOD1(G93A) mice with Ranolazine, an FDA-approved inhibitor of fatty acid beta-oxidation, led to a decrease in energy expenditure in symptomatic SOD1(G93A) mice, and this occurred in parallel with a robust, albeit temporary, recovery of the pathological phenotype.
引用
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页数:36
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