Lipidomic Analyses Reveal Specific Alterations of Phosphatidylcholine in Dystrophic Mdx Muscle.

William J Valentine,Suzumi M Tokuoka,Hideo Shindou,Takao Shimizu,Yoshitsugu Aoki,Norio Motohashi,Sherif A Mostafa,Natsuko F Inagaki,Joel Z Nordin,Fumie Hamano,Yoshihiro Kita

doi:10.3389/fphys.2021.698166

Abstract

In Duchenne muscular dystrophy (DMD), lack of dystrophin increases the permeability of myofiber plasma membranes to ions and larger macromolecules, disrupting calcium signaling and leading to progressive muscle wasting. Although the biological origin and meaning are unclear, alterations of phosphatidylcholine (PC) are reported in affected skeletal muscles of patients with DMD that may include higher levels of fatty acid (FA) 18:1 chains and lower levels of FA 18:2 chains, possibly reflected in relatively high levels of PC 34:1 (with 16:0_18:1 chain sets) and low levels of PC 34:2 (with 16:0_18:2 chain sets). Similar PC alterations have been reported to occur in the mdx mouse model of DMD. However, altered ratios of PC 34:1 to PC 34:2 have been variably reported, and we also observed that PC 34:2 levels were nearly equally elevated as PC 34:1 in the affected mdx muscles. We hypothesized that experimental factors that often varied between studies; including muscle types sampled, mouse ages, and mouse diets; may strongly impact the PC alterations detected in dystrophic muscle of mdx mice, especially the PC 34:1 to PC 34:2 ratios. In order to test our hypothesis, we performed comprehensive lipidomic analyses of PC and phosphatidylethanolamine (PE) in several muscles (extensor digitorum longus, gastrocnemius, and soleus) and determined the mdx-specific alterations. The alterations in PC 34:1 and PC 34:2 were closely monitored from the neonate period to the adult, and also in mice raised on several diets that varied in their fats. PC 34:1 was naturally high in neonate’s muscle and decreased until age ∼3-weeks (disease onset age), and thereafter remained low in WT muscles but was higher in regenerated mdx muscles. Among the muscle types, soleus showed a distinctive phospholipid pattern with early and diminished mdx alterations. Diet was a major factor to impact PC 34:1/PC 34:2 ratios because mdx-specific alterations of PC 34:2 but not PC 34:1 were strictly dependent on diet. Our study identifies high PC 34:1 as a consistent biochemical feature of regenerated mdx-muscle and indicates nutritional approaches are also effective to modify the phospholipid compositions.

Highlights

Phosphatidylcholine (PC) is a main component of the lipid bilayer in plasma cell membranes that surrounds muscle fibers
Other than loss of dystrophin, which may cause PC 34:1/PC 34:2 ratios in muscles to differ between studies, we first examined how phospholipid profiles vary in different muscles of healthy adults C57BL/6 mice
We previously reported that PPARδ and PGC1α agonists lead to enhanced levels of docosahexaenoic acid (DHA)-containing PC and PE in skeletal muscle cells through upregulation of

Summary

Introduction

Phosphatidylcholine (PC) is a main component of the lipid bilayer in plasma cell membranes that surrounds muscle fibers. This bilayer forms a hydrophobic barrier that functions to prevent the unregulated passage of ions and other charged molecules, which would otherwise lead to myofiber death and muscle wasting. The biological origin and meaning of the altered PC in DMD muscles has been unknown, considering the role of acyl chains of phospholipid in biomembrane integrity, the replacement of FA 18:2 chains with FA 18:1 chains is of considerable interest, especially because mono-unsaturated chains like FA 18:1 are more conformationally stable than polyunsaturated chains like FA 18:2 (Feller et al, 2002), and large alterations of the PC 34:1/PC 34:2 ratios may affect biophysical properties of the membranes that impact the disease course

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Conclusion