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表达 Rax 的前体细胞衍生的成体产黑素细胞皮质素原神经元减轻先天性下丘脑产黑素细胞皮质素原缺乏的代谢效应。

Adult-born proopiomelanocortin neurons derived from Rax-expressing precursors mitigate the metabolic effects of congenital hypothalamic proopiomelanocortin deficiency.

机构信息

Department of Molecular & Integrative Physiology, University of Michigan Medical School, 2800 Plymouth Rd, Ann Arbor, MI, 48109, USA.

Department of Medicine, Division of Endocrinology, Diabetes and Metabolism, Tufts Medical Center, 800 Washington St, Boston, MA, 02111, USA.

出版信息

Mol Metab. 2021 Nov;53:101312. doi: 10.1016/j.molmet.2021.101312. Epub 2021 Jul 28.

Abstract

OBJECTIVE

Proopiomelanocortin (POMC) neurons of the hypothalamic arcuate nucleus are essential regulators of energy balance. Selective loss of POMC production in these cells results in extreme obesity and metabolic comorbidities. Neurogenesis occurs in the adult hypothalamus, but it remains uncertain whether functional POMC neurons emerge in physiologically significant numbers during adulthood. Here, we tested whether Rax-expressing precursors generate POMC neurons in adult mice and rescue the metabolic phenotype caused by congenital hypothalamic POMC deficiency.

METHODS

Initially, we identified hypothalamic Rax-expressing cell types using wild-type and Rax-CreERT2:Ai34D mice. Then we generated compound Rax-CreERT2:ArcPomc mice in which endogenous hypothalamic Pomc expression is silenced, but can be restored by tamoxifen administration selectively in neurons derived from Rax progenitors. The number of POMC neurons generated by Rax progenitors in adult mice and their axonal projections was determined. The metabolic effects of these neurons were assessed by measuring food intake, bodyweight, and body composition, along with glucose and insulin levels.

RESULTS

We found that Rax is expressed by tanycytes and a previously unrecognized cell type in the hypothalamic parenchyma of adult mice. Rax progenitors generated ~10% of the normal adult hypothalamic POMC neuron population within two weeks of tamoxifen treatment. The same rate and steady state of POMC neurogenesis persisted from young adult to aged mice. These new POMC neurons established terminal projections to brain regions that were involved in energy homeostasis. Mice with Rax progenitor-derived POMC neurons had reduced body fat mass, improved glucose tolerance, increased insulin sensitivity, and decreased bodyweight in proportion to the number of new POMC neurons.

CONCLUSIONS

These data demonstrate that Rax progenitors generate POMC neurons in sufficient numbers during adulthood to mitigate the metabolic abnormalities of hypothalamic POMC-deficient mice. The findings suggest that adult hypothalamic neurogenesis is a robust phenomenon in mice that can significantly impact energy homeostasis.

摘要

目的

下丘脑弓状核的前阿黑皮素原(POMC)神经元是能量平衡的重要调节者。这些细胞中 POMC 产物的选择性缺失会导致极度肥胖和代谢合并症。成人下丘脑会发生神经发生,但尚不确定在成年期是否会以生理上有意义的数量产生功能性 POMC 神经元。在这里,我们测试了 Rax 表达前体是否会在成年小鼠中产生 POMC 神经元,并挽救由先天性下丘脑 POMC 缺乏引起的代谢表型。

方法

最初,我们使用野生型和 Rax-CreERT2:Ai34D 小鼠鉴定了下丘脑 Rax 表达的细胞类型。然后,我们在复合 Rax-CreERT2:ArcPomc 小鼠中生成了内源性下丘脑 Pomc 表达被沉默,但可以通过 tamoxifen 处理选择性地在源自 Rax 祖细胞的神经元中恢复的小鼠。通过测量食物摄入、体重和身体成分以及葡萄糖和胰岛素水平,确定成年小鼠中 Rax 祖细胞产生的 POMC 神经元的数量及其轴突投射。通过测量食物摄入、体重和身体成分以及葡萄糖和胰岛素水平,评估这些神经元的代谢效应。

结果

我们发现,Rax 在成年小鼠下丘脑实质中的 tanycytes 和以前未被识别的细胞类型中表达。在 tamoxifen 处理后的两周内,Rax 祖细胞产生了正常成年下丘脑 POMC 神经元群体的~10%。从年轻成年到老年小鼠,相同的速率和 POMC 神经发生的稳定状态持续存在。这些新的 POMC 神经元建立了到参与能量稳态的脑区的终末投射。具有 Rax 祖细胞衍生的 POMC 神经元的小鼠体脂减少、葡萄糖耐量提高、胰岛素敏感性增加,体重减轻与新 POMC 神经元的数量成正比。

结论

这些数据表明,Rax 祖细胞在成年期以足够的数量产生 POMC 神经元,以减轻下丘脑 POMC 缺乏小鼠的代谢异常。这些发现表明,成年下丘脑神经发生是小鼠中一种强大的现象,可以显著影响能量稳态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/38b7/8383116/262003623eee/gr1.jpg

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