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短暂性棕色脂肪样细胞来源于周围神经祖细胞对骨形态发生蛋白 2 的反应。

Transient brown adipocyte-like cells derive from peripheral nerve progenitors in response to bone morphogenetic protein 2.

机构信息

Center for Cell and Gene Therapy, Baylor College of Medicine, Houston, TX, USA.

出版信息

Stem Cells Transl Med. 2012 Dec;1(12):874-85. doi: 10.5966/sctm.2012-0090. Epub 2012 Nov 26.

Abstract

Perineurial-associated brown adipocyte-like cells were rapidly generated during bone morphogenetic protein 2 (BMP2)-induced sciatic nerve remodeling in the mouse. Two days after intramuscular injection of transduced mouse fibroblast cells expressing BMP2 into wild-type mice, there was replication of beta-3 adrenergic receptor(+) (ADRB3(+)) cells within the sciatic nerve perineurium. Fluorescence-activated cell sorting and analysis of cells isolated from these nerves confirmed ADRB3(+) cell expansion and their expression of the neural migration marker HNK1. Similar analysis performed 4 days after BMP2 delivery revealed a significant decrease in ADRB3(+) cells from isolated sciatic nerves, with their concurrent appearance within the adjacent soft tissue, suggesting migration away from the nerve. These soft tissue-derived cells also expressed the brown adipose marker uncoupling protein 1 (UCP1). Quantification of ADRB3-specific RNA in total hind limb tissue revealed a 3-fold increase 2 days after delivery of BMP2, followed by a 70-fold increase in UCP1-specific RNA after 3 days. Expression levels then rapidly returned to baseline by 4 days. Interestingly, these ADRB3(+) UCP1(+) cells also expressed the neural guidance factor reelin. Reelin(+) cells demonstrated distinct patterns within the injected muscle, concentrated toward the area of BMP2 release. Blocking mast cell degranulation-induced nerve remodeling resulted in the complete abrogation of UCP1-specific RNA and protein expression within the hind limbs following BMP2 injection. The data collectively suggest that local BMP2 administration initiates a cascade of events leading to the expansion, migration, and differentiation of progenitors from the peripheral nerve perineurium to brown adipose-like cells in the mouse, a necessary prerequisite for associated nerve remodeling.

摘要

骨形态发生蛋白 2(BMP2)诱导的小鼠坐骨神经重塑过程中,快速产生了与神经膜细胞相关的棕色脂肪细胞样细胞。在将表达 BMP2 的转导小鼠成纤维细胞注射到野生型小鼠的肌肉中两天后,β-3 肾上腺素能受体(ADRB3(+))细胞在坐骨神经神经膜内复制。对这些神经中分离的细胞进行荧光激活细胞分选和分析证实了 ADRB3(+)细胞的扩增及其对神经迁移标记物 HNK1 的表达。在 BMP2 给药后 4 天进行的类似分析显示,从分离的坐骨神经中分离的 ADRB3(+)细胞显著减少,同时出现在相邻的软组织中,提示其从神经迁移。这些软组织来源的细胞也表达棕色脂肪标记物解偶联蛋白 1(UCP1)。在 BMP2 给药后 2 天,总后肢组织中 ADRB3 特异性 RNA 的定量分析显示其增加了 3 倍,3 天后 UCP1 特异性 RNA 增加了 70 倍。表达水平随后在 4 天迅速恢复到基线。有趣的是,这些 ADRB3(+)UCP1(+)细胞也表达了神经导向因子 reelin。Reelin(+)细胞在注射的肌肉中表现出不同的模式,集中在 BMP2 释放区域。阻断肥大细胞脱颗粒诱导的神经重塑导致 BMP2 注射后后肢中 UCP1 特异性 RNA 和蛋白表达完全被阻断。这些数据表明,局部 BMP2 给药启动了一系列事件,导致来自外周神经神经膜的祖细胞的扩增、迁移和分化为小鼠中的棕色脂肪样细胞,这是相关神经重塑的必要前提。

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