Mizuta Kentaro, Xu Dingbang, Pan Yaping, Comas George, Sonett Joshua R, Zhang Yi, Panettieri Reynold A, Yang Jay, Emala Charles W
Deptartment of Anesthesiology, College of Physicians and Surgeons of Columbia University, 630 W. 168th St., P&S Box 46, New York, New York 10032, USA.
Am J Physiol Lung Cell Mol Physiol. 2008 Jun;294(6):L1206-16. doi: 10.1152/ajplung.00287.2007. Epub 2008 Apr 11.
Gamma-aminobutyric acid (GABA) is the major inhibitory neurotransmitter in the mammalian central nervous system and exerts its actions via both ionotropic (GABA(A)) channels and metabotropic (GABA(B)) receptors. GABA(A) channels are ubiquitously expressed in neuronal tissues, and in mature neurons modulate an inward chloride current resulting in neuronal inhibition due to membrane hyperpolarization. In airway smooth muscle (ASM) cells, membrane hyperpolarization favors smooth muscle relaxation. Although GABA(A) channels and GABA(B) receptors have been functionally identified on peripheral nerves in the lung, GABA(A) channels have never been identified on ASM itself. We detected the mRNA encoding of the GABA(A) alpha(4)-, alpha(5)-, beta(3)-, delta-, gamma(1-3)-, pi-, and theta-subunits in total RNA isolated from native human and guinea pig ASM and from cultured human ASM cells. Selected immunoblots identified the GABA(A) alpha(4)-, alpha(5)-, beta(3)-, and gamma(2)-subunit proteins in native human and guinea pig ASM and cultured human ASM cells. The GABA(A) beta(3)-subunit protein was immunohistochemically localized to ASM in guinea pig tracheal rings. While muscimol, a specific GABA(A) channel agonist, did not affect the magnitude or the time to peak contractile effect of substance P, it directly concentration dependently relaxed a tachykinin-induced contraction in guinea pig tracheal rings, which was inhibited by the GABA(A)-selective antagonist gabazine. Muscimol also relaxed a contraction induced by an alternative contractile agonist histamine. These results demonstrate that functional GABA(A) channels are expressed on ASM and suggest a novel therapeutic target for the relaxation of ASM in diseases such as asthma and chronic obstructive lung disease.
γ-氨基丁酸(GABA)是哺乳动物中枢神经系统中的主要抑制性神经递质,通过离子型(GABA(A))通道和代谢型(GABA(B))受体发挥作用。GABA(A)通道在神经组织中广泛表达,在成熟神经元中调节内向氯化物电流,由于膜超极化导致神经元抑制。在气道平滑肌(ASM)细胞中,膜超极化有利于平滑肌松弛。虽然GABA(A)通道和GABA(B)受体已在肺外周神经上被功能性鉴定,但ASM本身从未鉴定出GABA(A)通道。我们在从天然人及豚鼠ASM以及培养的人ASM细胞中分离的总RNA中检测到了编码GABA(A)α(4)-、α(5)-、β(3)-、δ-、γ(1-3)-、π-和θ-亚基的mRNA。选定的免疫印迹法在天然人及豚鼠ASM以及培养的人ASM细胞中鉴定出了GABA(A)α(4)-、α(5)-、β(3)-和γ(2)-亚基蛋白。GABA(A)β(3)-亚基蛋白通过免疫组织化学定位在豚鼠气管环的ASM中。虽然特异性GABA(A)通道激动剂蝇蕈醇不影响P物质收缩效应的幅度或达到峰值的时间,但它直接以浓度依赖的方式松弛了豚鼠气管环中速激肽诱导的收缩,该收缩被GABA(A)选择性拮抗剂荷包牡丹碱抑制。蝇蕈醇还松弛了由另一种收缩激动剂组胺诱导的收缩。这些结果表明功能性GABA(A)通道在ASM上表达,并提示在哮喘和慢性阻塞性肺疾病等疾病中,ASM松弛存在一个新的治疗靶点。