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Piezo1 在小鼠 TRPV1 阳性伤害感受器中介导机械信号。

Piezo1 mediates mechanical signals in TRPV1-positive nociceptors in mice.

机构信息

Brain Science Institute, Korea Institute of Science and Technology (KIST), Seoul, Republic of Korea.

Department of Life Sciences, Korea University, Seoul, Republic of Korea.

出版信息

Acta Physiol (Oxf). 2024 Nov;240(11):e14236. doi: 10.1111/apha.14236. Epub 2024 Sep 26.

Abstract

AIM

This investigation addresses Piezo1's expression and mechanistic role in dorsal root ganglion (DRG) neurons and delineates its participation in mechanical and inflammatory pain modulation.

METHODS

We analyzed Piezo1's expression patterns in DRG neurons and utilized Piezo1-specific shRNA to modulate its activity. Electrophysiological assessments of mechanically activated (MA) currents in DRG neurons and behavioral analyses in mouse models of inflammatory pain were conducted to elucidate Piezo1's functional implications. Additionally, we investigated the excitability of TRPV1-expressing DRG neurons, particularly under inflammatory conditions.

RESULTS

Piezo1 was preferentially expressed in DRG neurons co-expressing the TRPV1 nociceptor marker. Knockdown of Piezo1 attenuated intermediately adapting MA currents and lessened tactile pain hypersensitivity in models of inflammatory pain. Additionally, silencing Piezo1 modified the excitability of TRPV1-expressing neurons under inflammatory stress.

CONCLUSION

Piezo1 emerges as a key mediator in the transmission of mechanical and inflammatory pain, indicating its potential as a novel target for pain management therapies. Our finding not only advances the understanding of nociceptive signaling but also emphasizes the therapeutic potential of modulating Piezo1 in the treatment of pain.

摘要

目的

本研究旨在探讨 Piezo1 在背根神经节(DRG)神经元中的表达模式和作用机制,并阐明其在机械和炎症性疼痛调节中的作用。

方法

我们分析了 Piezo1 在 DRG 神经元中的表达模式,并利用 Piezo1 特异性 shRNA 来调节其活性。我们还进行了 DRG 神经元机械激活(MA)电流的电生理评估和炎症性疼痛小鼠模型中的行为分析,以阐明 Piezo1 的功能意义。此外,我们研究了 TRPV1 表达的 DRG 神经元的兴奋性,特别是在炎症条件下。

结果

Piezo1 优先表达于共同表达 TRPV1 伤害感受器标记物的 DRG 神经元中。Piezo1 的敲低减弱了中间适应性 MA 电流,并减轻了炎症性疼痛模型中的触觉痛觉过敏。此外,沉默 Piezo1 改变了炎症应激下 TRPV1 表达神经元的兴奋性。

结论

Piezo1 作为机械和炎症性疼痛传递的关键介质出现,表明其作为疼痛管理治疗新靶点的潜力。我们的发现不仅推进了伤害性信号转导的理解,还强调了调节 Piezo1 在疼痛治疗中的治疗潜力。

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