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内耳血管周围驻留的巨噬细胞样黑素细胞对于内淋巴液-血液屏障的完整性至关重要。

Perivascular-resident macrophage-like melanocytes in the inner ear are essential for the integrity of the intrastrial fluid-blood barrier.

机构信息

Oregon Hearing Research Center, NRC04, Department of Otolaryngology/Head and Neck Surgery, Oregon Health and Science University, Portland, OR 97239, USA.

出版信息

Proc Natl Acad Sci U S A. 2012 Jun 26;109(26):10388-93. doi: 10.1073/pnas.1205210109. Epub 2012 Jun 11.

Abstract

The microenvironment of the cochlea is maintained by the barrier between the systemic circulation and the fluids inside the stria vascularis. However, the mechanisms that control the permeability of the intrastrial fluid-blood barrier remain largely unknown. The barrier comprises endothelial cells connected to each other by tight junctions and an underlying basement membrane. In a recent study, we found that the intrastrial fluid-blood barrier also includes a large number of perivascular cells with both macrophage and melanocyte characteristics. The perivascular-resident macrophage-like melanocytes (PVM/Ms) are in close contact with vessels through cytoplasmic processes. Here we demonstrate that PVM/Ms have an important role in maintaining the integrity of the intrastrial fluid-blood barrier and hearing function. Using a cell culture-based in vitro model and a genetically induced PVM/M-depleted animal model, we show that absence of PVM/Ms increases the permeability of the intrastrial fluid-blood barrier to both low- and high-molecular-weight tracers. The increased permeability is caused by decreased expression of pigment epithelial-derived factor, which regulates expression of several tight junction-associated proteins instrumental to barrier integrity. When tested for endocochlear potential and auditory brainstem response, PVM/M-depleted animals show substantial drop in endocochlear potential with accompanying hearing loss. Our results demonstrate a critical role for PVM/Ms in regulating the permeability of the intrastrial fluid-blood barrier for establishing a normal endocochlear potential hearing threshold.

摘要

耳蜗的微环境由位于血管纹内的液体与全身循环之间的屏障来维持。然而,控制内淋巴-血屏障通透性的机制在很大程度上仍然未知。该屏障由通过紧密连接相互连接的内皮细胞和基底膜组成。在最近的一项研究中,我们发现内淋巴-血屏障还包括大量具有巨噬细胞和黑色素细胞特征的血管周细胞。血管周细胞驻留的巨噬样黑色素细胞(PVM/Ms)通过细胞质突起与血管紧密接触。在这里,我们证明 PVM/Ms 在维持内淋巴-血屏障和听力功能的完整性方面起着重要作用。使用基于细胞培养的体外模型和基因诱导的 PVM/M 耗竭动物模型,我们表明 PVM/Ms 的缺失会增加内淋巴-血屏障对低分子量和高分子量示踪剂的通透性。这种通透性的增加是由于色素上皮衍生因子的表达减少所致,该因子调节几个紧密连接相关蛋白的表达,这些蛋白对屏障的完整性至关重要。当对内耳电位和听觉脑干反应进行测试时,PVM/M 耗竭动物的内淋巴电位显著下降,同时伴有听力损失。我们的结果表明 PVM/Ms 在调节内淋巴-血屏障的通透性以建立正常的内耳电位听力阈值方面起着关键作用。

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