Experimental Neurology, 200 Lothrop St., W1340 Biomedical Science Tower, Pittsburgh, PA 15260, USA.
Exp Neurol. 2011 Nov;232(1):90-9. doi: 10.1016/j.expneurol.2011.08.007. Epub 2011 Aug 16.
Nitro-oleic acid (9- and 10-nitro-octadeca-9-enoic acid, OA-NO(2)) is an electrophilic fatty acid nitroalkene derivative that modulates gene transcription and protein function via post-translational protein modification. Nitro-fatty acids are generated from unsaturated fatty acids by oxidative inflammatory reactions and acidic conditions in the presence of nitric oxide or nitrite. Nitroalkenes react with nucleophiles such as cysteine and histidine in a variety of susceptible proteins including transient receptor potential (TRP) channels in sensory neurons of the dorsal root and nodose ganglia. The present study revealed that OA-NO(2) activates TRP channels on afferent nerve terminals in the urinary bladder and thereby increases bladder activity. The TRPV1 agonist capsaicin (CAPS, 1 μM) and the TRPA1 agonist allyl isothiocyanate (AITC, 30 μM), elicited excitatory effects in bladder strips, increasing basal tone and amplitude of phasic bladder contractions (PBC). OA-NO(2) mimicked these effects in a concentration-dependent manner (1 μM-33 μM). The TRPA1 antagonist HC3-030031 (HC3, 30 μM) and the TRPV1 antagonist diaryl piperazine analog (DPA, 1 μM), reduced the effect of OA-NO(2) on phasic contraction amplitude and baseline tone. However, the non-selective TRP channel blocker, ruthenium red (30 μM) was a more effective inhibitor, reducing the effects of OA-NO(2) on basal tone by 75% and the effects on phasic amplitude by 85%. In bladder strips from CAPS-treated rats, the effect of OA-NO(2) on phasic contraction amplitude was reduced by 65% and the effect on basal tone was reduced by 60%. Pretreatment of bladder strips with a combination of neurokinin receptor antagonists (NK1 selective antagonist, CP 96345; NK2 selective antagonist, MEN 10,376; NK3 selective antagonist, SB 234,375, 1 μM each) reduced the effect of OA-NO(2) on basal tone, but not phasic contraction amplitude. These results indicate that nitroalkene fatty acid derivatives can activate TRP channels on CAPS-sensitive afferent nerve terminals, leading to increased bladder contractile activity. Nitrated fatty acids produced endogenously by the combination of fatty acids and oxides of nitrogen released from the urothelium and/or afferent nerves may play a role in modulating bladder activity.
硝酯油酸(9-和 10-硝基十八碳-9-烯酸,OA-NO(2))是一种亲电脂肪酸硝烯衍生物,通过翻译后蛋白质修饰调节基因转录和蛋白质功能。硝化脂肪酸是由不饱和脂肪酸在一氧化氮或亚硝酸盐存在下通过氧化炎症反应和酸性条件生成的。硝烯与半胱氨酸和组氨酸等各种敏感蛋白中的亲核试剂反应,包括背根和结状神经节感觉神经元中的瞬时受体电位(TRP)通道。本研究表明,OA-NO(2)激活膀胱传入神经末梢上的 TRP 通道,从而增加膀胱活动。辣椒素(CAPS,1 μM)和丙烯基异硫氰酸酯(AITC,30 μM)等 TRPV1 激动剂在膀胱条带中引起兴奋作用,增加基础张力和相位膀胱收缩(PBC)的幅度。OA-NO(2)以浓度依赖的方式模拟这些作用(1 μM-33 μM)。TRPA1 拮抗剂 HC3-030031(HC3,30 μM)和 TRPV1 拮抗剂二芳基哌嗪类似物(DPA,1 μM)降低了 OA-NO(2)对相位收缩幅度和基线张力的影响。然而,非选择性 TRP 通道阻滞剂钌红(30 μM)是一种更有效的抑制剂,使 OA-NO(2)对基础张力的影响降低 75%,对相位幅度的影响降低 85%。在 CAPS 处理的大鼠的膀胱条带中,OA-NO(2)对相位收缩幅度的作用降低了 65%,对基础张力的作用降低了 60%。膀胱条带预处理与神经激肽受体拮抗剂(NK1 选择性拮抗剂 CP 96345;NK2 选择性拮抗剂 MEN 10,376;NK3 选择性拮抗剂 SB 234,375,各 1 μM)联合使用,降低了 OA-NO(2)对基础张力的作用,但不降低相位收缩幅度。这些结果表明,硝烯脂肪酸衍生物可激活 CAPS 敏感传入神经末梢上的 TRP 通道,导致膀胱收缩活性增加。由尿路上皮和/或传入神经释放的脂肪酸和氮氧化物的组合产生的内源性硝化脂肪酸可能在调节膀胱活动中发挥作用。
