Université Claude Bernard Lyon 1, Faculté de Médecine, EA 4170 and Plateau NeuroChem, Lyon, France.
PLoS One. 2011 Mar 9;6(3):e16891. doi: 10.1371/journal.pone.0016891.
Involvement of nitric oxide (NO) in the pathophysiology of human African trypanosomiasis (HAT) was analyzed in a HAT animal model (rat infected with Trypanosoma brucei brucei). With this model, it was previously reported that trypanosomes were capable of limiting trypanocidal properties carried by NO by decreasing its blood concentration. It was also observed that brain NO concentration, contrary to blood, increases throughout the infection process. The present approach analyses the brain impairments occurring in the regulations exerted by arginase and N(G), N(G)-dimethylarginine dimethylaminohydrolase (DDAH) on NO Synthases (NOS). In this respect: (i) cerebral enzymatic activities, mRNA and protein expression of arginase and DDAH were determined; (ii) immunohistochemical distribution and morphometric parameters of cells expressing DDAH-1 and DDAH-2 isoforms were examined within the diencephalon; (iii) amino acid profiles relating to NOS/arginase/DDAH pathways were established.
METHODOLOGY/PRINCIPAL FINDINGS: Arginase and DDAH activities together with mRNA (RT-PCR) and protein (western-blot) expressions were determined in diencephalic brain structures of healthy or infected rats at various days post-infection (D5, D10, D16, D22). While arginase activity remained constant, that of DDAH increased at D10 (+65%) and D16 (+51%) in agreement with western-blot and amino acids data (liquid chromatography tandem-mass spectrometry). Only DDAH-2 isoform appeared to be up-regulated at the transcriptional level throughout the infection process. Immunohistochemical staining further revealed that DDAH-1 and DDAH-2 are contained within interneurons and neurons, respectively.
CONCLUSION/SIGNIFICANCE: In the brain of infected animals, the lack of change observed in arginase activity indicates that polyamine production is not enhanced. Increases in DDAH-2 isoform may contribute to the overproduction of NO. These changes are at variance with those reported in the periphery. As a whole, the above processes may ensure additive protection against trypanosome entry into the brain, i.e., maintenance of NO trypanocidal pressure and limitation of polyamine production, necessary for trypanosome growth.
一氧化氮(NO)在人类非洲锥虫病(HAT)的病理生理学中的作用在 HAT 动物模型(感染布氏锥虫布鲁斯氏菌的大鼠)中进行了分析。使用该模型,先前的报道表明,锥虫能够通过降低其血液浓度来限制由 NO 携带的杀锥虫特性。还观察到,与血液相反,整个感染过程中大脑 NO 浓度增加。本研究分析了精氨酸酶和 N(G)、N(G)-二甲基精氨酸二甲氨基水解酶(DDAH)对一氧化氮合酶(NOS)的调节中发生的脑损伤。在这方面:(i)测定了大脑的酶活性、精氨酸酶和 DDAH 的 mRNA 和蛋白表达;(ii)检查了间脑内表达 DDAH-1 和 DDAH-2 同工型的细胞的免疫组织化学分布和形态计量学参数;(iii)建立了与 NOS/精氨酸酶/DDAH 途径相关的氨基酸谱。
方法/主要发现:在感染后不同天数(D5、D10、D16、D22)的健康或感染大鼠的间脑结构中,测定了精氨酸酶和 DDAH 的活性(RT-PCR)以及 mRNA(western-blot)和蛋白(western-blot)表达。虽然精氨酸酶活性保持不变,但 DDAH 在 D10(+65%)和 D16(+51%)时的活性增加,与 western-blot 和氨基酸数据(液相色谱串联质谱法)一致。只有 DDAH-2 同工型在整个感染过程中在转录水平上似乎被上调。免疫组织化学染色进一步表明,DDAH-1 和 DDAH-2 分别存在于中间神经元和神经元中。
结论/意义:在感染动物的大脑中,观察到精氨酸酶活性没有变化表明多胺的产生没有增加。DDAH-2 同工型的增加可能有助于 NO 的过度产生。这些变化与外周报道的变化不同。总的来说,上述过程可能为防止锥虫进入大脑提供额外的保护,即维持对锥虫的杀伤压力和限制多胺的产生,这对锥虫的生长是必要的。
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