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首页> 外文期刊>Biochemical and Biophysical Research Communications >Insufficient liver maturation affects murine early postnatal hair cycle
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Insufficient liver maturation affects murine early postnatal hair cycle

机译:肝脏成熟不足会影响鼠早期后毛发循环

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Abnormal hair loss results from a variety of factors, such as metabolic dysfunctions, immunodeficiency, and environmental stressors. Here, we report that mutant mice having defects in liver function, develop alopecia. We have shown previously that in mice lacking a Cnot3 gene, which encodes an essential component of the CCR4-NOT deadenylase complex in liver (Cnot3-LKO mice), the liver does not mature properly, resulting in various pathologies such as hepatitis, hepatic necrosis, and anemia. Unexpectedly, Cnot3-LKO mice start to lose hair around postnatal day 17 (P17). The region of hair loss expands all across their backs and symptoms persist until around P28-30. Afterward, hair re-grows, and Cnot3-LKO mice show complete hair recovery by P40. The phenotype is dependent on mouse genotype, indicating that hair follicle morphogenesis and cycling are influenced by abnormal liver development. By performing histological, quantitative PCR, and immunoblot analyses, we detected sebaceous gland (SG) hypertrophy accompanied by an increase of peroxisome proliferator-activated receptor gamma (PPAR gamma). Collectively, these findings suggest that paracrine signaling related to liver function influences hair growth, at least in part, by altering lipid metabolism. (C) 2019 The Authors. Published by Elsevier Inc.
机译:异常脱发结果由各种因素,如代谢功能障碍,免疫缺陷和环境压力源。在这里,我们报告说患有肝功能缺陷的突变小鼠,发展脱发。我们先前表明,在缺乏CNOT3基因的小鼠中,它们在肝脏(CNOT3-LKO小鼠)中编码CCR4-not硬脑酶络合物的基本组分,肝脏不会适当成熟,导致各种病例如肝炎,肝脏坏死和贫血。意外地,CNOT3-LKO小鼠开始在第17天(P17)周围失去毛发。脱发地区遍布其背面,症状持续到P28-30周围。之后,头发重新生长,CNOT3-LKO小鼠通过P40显示完整的头发回收。表型取决于小鼠基因型,表明毛发卵泡形态发生和循环受异常肝脏发育的影响。通过进行组织学,定量PCR和免疫印迹分析,我们检测到皮脂腺(SG)肥大伴有过氧化物体增殖物激活的受体γ(PPARγ)的增加。总的来说,这些研究结果表明,与肝功能相关的旁静脉信号传导至少部分地通过改变脂质代谢来影响毛发生生长。 (c)2019年作者。 elsevier公司发布

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