白细胞型12/15-脂氧合酶对于骨骼肌损伤后及时的炎症消退和有效的组织再生至关重要。

Leukocyte-type 12/15-lipoxygenase is essential for timely inflammation-resolution and effective tissue regeneration following skeletal muscle injury.

作者信息

Sharma Binayok, Lu Xinyue, Rehman Hamood, Figueiredo Vandré C, Davis Carol, Van Remmen Holly, Kuang Shihuan, Brooks Susan V, Maddipati Krishna Rao, Markworth James F

机构信息

Department of Animal Sciences, College of Agriculture, Purdue University, West Lafayette, IN, USA.

Department of Animal Sciences, College of Agriculture, Purdue University, West Lafayette, IN, USA; Interdepartmental Nutrition Program (INP), Purdue University, West Lafayette, IN, USA; Center for Aging and the Life Course (CALC), Purdue University, West Lafayette, IN, USA.

出版信息

Mol Metab. 2025 Aug 5;100:102224. doi: 10.1016/j.molmet.2025.102224.

DOI:10.1016/j.molmet.2025.102224

PMID:40769490

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12391815/

Abstract

OBJECTIVES

Unlike traditional anti-inflammatory therapies which may interfere with musculoskeletal tissue repair, pharmacological administration of specialized pro-resolving lipid mediators (SPMs) promotes timely resolution of inflammation while stimulating skeletal muscle regeneration. Despite this, the potential role of endogenous inflammation-resolution circuits in skeletal muscle injury and repair remains unknown.

METHODS

We investigated the effect of whole-body knockout of leukocyte-type 12/15-lipoxygenase (12/15-LOX) on acute inflammation and regeneration in vivo following skeletal muscle injury in mice. We further tested the impact of 12/15-LOX deficiency on polarization of bone marrow-derived macrophages and differentiation of myogenic progenitor cells in vitro.

RESULTS

Alox15 mice displayed lower intramuscular concentrations of 12/15-LOX-derived lipid mediators than wild type (WT) mice, and this was associated with chronic low-grade muscle inflammation. Alox15-/- mice mounted an exaggerated acute immune response to sterile skeletal muscle injury which was associated with a local imbalance of pro-inflammatory vs. pro-resolving lipid mediators. Alox15 mice also displayed defects in myogenic gene expression, myofiber size, and myonuclear accretion. Mechanistically, bone marrow-derived macrophages (MФ) obtained from Alox15 mice produced less 12/15-LOX-derived lipid mediators and this was associated with impaired M2 polarization. Isolated myogenic progenitor cells also produced many LOX metabolites in response to long chain polyunsaturated fatty acid (LC-PUFA) supplementation, including bioactive SPMs. Alox15 myoblasts were both impaired in their ability to produce SPMs and were insensitive to the stimulatory effect of LC-PUFAs on in vitro myogenesis.

CONCLUSIONS

12/15-LOX is essential for timely resolution of acute inflammation and direct determination of myogenic progenitor cell fate following skeletal muscle injury.

摘要

目的

与可能干扰肌肉骨骼组织修复的传统抗炎疗法不同，专门的促消退脂质介质（SPM）的药物给药可促进炎症的及时消退，同时刺激骨骼肌再生。尽管如此，内源性炎症消退回路在骨骼肌损伤和修复中的潜在作用仍不清楚。

方法

我们研究了白细胞型12/15-脂氧合酶（12/15-LOX）全身敲除对小鼠骨骼肌损伤后体内急性炎症和再生的影响。我们进一步测试了12/15-LOX缺乏对体外骨髓来源巨噬细胞极化和成肌祖细胞分化的影响。

结果

Alox15小鼠肌肉内12/15-LOX衍生脂质介质的浓度低于野生型（WT）小鼠，这与慢性低度肌肉炎症有关。Alox15-/-小鼠对无菌骨骼肌损伤产生过度的急性免疫反应，这与促炎与促消退脂质介质的局部失衡有关。Alox15小鼠在成肌基因表达、肌纤维大小和肌核增加方面也存在缺陷。从机制上讲，从Alox15小鼠获得的骨髓来源巨噬细胞（MФ）产生的12/15-LOX衍生脂质介质较少，这与M2极化受损有关。分离的成肌祖细胞在补充长链多不饱和脂肪酸（LC-PUFA）后也产生许多LOX代谢产物，包括生物活性SPM。Alox15成肌细胞产生SPM的能力受损，并且对LC-PUFAs对体外成肌的刺激作用不敏感。