Gangula Pandu, Ravella Kalpana, Chukkapalli Sasanka, Rivera Mercedes, Srinivasan Shanthi, Hale Ashley, Channon Keith, Southerland Janet, Kesavalu Lakshmyya
Department of Physiology, Meharry Medical College, Nashville, TN, United States of America; School of Dentistry, Meharry Medical College, Nashville, TN, United States of America.
Department of Physiology, Meharry Medical College, Nashville, TN, United States of America.
PLoS One. 2015 Jun 25;10(6):e0129885. doi: 10.1371/journal.pone.0129885. eCollection 2015.
Periodontal disease is a highly prevalent chronic inflammatory disease and is associated with complex microbial infection in the subgingival cavity. Recently, American Heart Association supported a century old association between periodontal disease and atherosclerotic vascular disease. We have recently shown that polybacterial periodontal infection led to aortic atherosclerosis and modulation of lipid profiles; however the underlying mechanism(s) has not been yet demonstrated. Altered nitric oxide (NO) synthesis and tetrahydrobiopterin (BH4), a cofactor for nitric oxide synthases (NOS) has long been shown to be associated with vascular dysfunction and gastrointestinal motility disorders. We sought to examine the mechanism of periodontal infection leading to altered vascular and gastrointestinal smooth muscle relaxation, focusing on the BH4/nNOS pathways. In addition, we also have investigated how the antioxidant system (NRF2-Phase II enzyme expression) in vascular and GI specimens is altered by oral infection. Eight week old male ApoEnull mice were either sham-infected or infected orally for 16 weeks with a mixture of major periodontal bacteria Porphyromonas gingivalis, Treponema denticola and Tannerella forsythia to induce experimental periodontitis. Serum, vascular (mesenteric), stomach, and colon specimens were collected at the end of periodontal pathogen infection. Bacterial infection induced significant (p<0.05) reductions in the levels of BH4,in ratio of BH4:BH2+B and also in nitric oxide levels compared to sham-infected controls. In addition, we identified a significant (p<0.05) reduction in eNOS dimerization, nNOS dimerization and protein expression of BH4 biosynthesis enzymes; GCH-1, DHFR and NRF2 & Phase II enzymes in infected mice versus controls in both mesenteric artery and colon tissues. However, we found no differences in nNOS/BH4 protein expression in stomach tissues of infected and sham-infected mice. This suggests that a polybacterial infection can cause significant changes in the vascular and colonic BH4/nNOS/NRF2 pathways which might lead to impaired vascular relaxation and colonic motility.
牙周病是一种高度流行的慢性炎症性疾病,与龈下腔的复杂微生物感染有关。最近,美国心脏协会支持了一个存在百年之久的牙周病与动脉粥样硬化性血管疾病之间的关联。我们最近发现,多菌性牙周感染会导致主动脉粥样硬化并调节血脂水平;然而,其潜在机制尚未得到证实。一氧化氮(NO)合成的改变以及四氢生物蝶呤(BH4),一种一氧化氮合酶(NOS)的辅助因子,长期以来一直被证明与血管功能障碍和胃肠动力障碍有关。我们试图研究牙周感染导致血管和胃肠平滑肌舒张改变的机制,重点关注BH4/nNOS途径。此外,我们还研究了口腔感染如何改变血管和胃肠道标本中的抗氧化系统(NRF2-Ⅱ相酶表达)。8周龄雄性ApoE基因敲除小鼠要么接受假感染,要么用主要牙周细菌牙龈卟啉单胞菌、齿垢密螺旋体和福赛坦纳菌的混合物进行16周的口腔感染,以诱导实验性牙周炎。在牙周病原体感染结束时收集血清、血管(肠系膜)、胃和结肠标本。与假感染对照组相比,细菌感染导致BH4水平、BH4:BH2+B比值以及一氧化氮水平显著降低(p<0.05)。此外,我们发现感染小鼠与对照组相比,肠系膜动脉和结肠组织中内皮型一氧化氮合酶(eNOS)二聚化、神经元型一氧化氮合酶(nNOS)二聚化以及BH4生物合成酶;GCH-1、二氢叶酸还原酶(DHFR)以及NRF2和Ⅱ相酶的蛋白表达均显著降低(p<0.05)。然而,我们发现感染小鼠和假感染小鼠胃组织中nNOS/BH4蛋白表达没有差异。这表明多菌性感染可导致血管和结肠中BH4/nNOS/NRF2途径发生显著变化,这可能导致血管舒张受损和结肠动力障碍。
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