Enhancement of presynaptic glutamate release and persistent inflammatory pain by increasing neuronal cAMP in the anterior cingulate cortex

Background

Primary erythromelalgia is an autosomal dominant pain disorder characterized by burning pain and skin redness in the extremities, with onset of symptoms during the first decade in the families whose mutations have been physiologically studied to date. Several mutations of voltage-gated Na⁺ channel Na_V1.7 have been linked with primary erythromelalgia. Recently, a new substitution Na_V1.7/I136V has been reported in a Taiwanese family, in which pain appeared at later ages (9–22 years, with onset at 17 years of age or later in 5 of 7 family members), with relatively slow progression (8–10 years) to involvement of the hands. The proband reported onset of symptoms first in his feet at the age of 11, which then progressed to his hands at the age of 19. The new mutation is located in transmembrane segment 1 (S1) of domain I (DI) in contrast to all Na_V1.7 mutations reported to date, which have been localized in the voltage sensor S4, the linker joining segments S4 and S5 or pore-lining segments S5 and S6 in DI, II and III.

Results

In this study, we characterized the gating and kinetic properties of I136V mutant channels in HEK293 cells using whole-cell patch clamp. I136V shifts the voltage-dependence of activation by -5.7 mV, a smaller shift in activation than the other erythromelalgia mutations that have been characterized. I136V also decreases the deactivation rate, and generates larger ramp currents.

Conclusion

The I136V substitution in Na_V1.7 alters channel gating and kinetic properties. Each of these changes may contribute to increased excitability of nociceptive dorsal root ganglion neurons, which underlies pain in erythromelalgia. The smaller shift in voltage-dependence of activation of Na_V1.7, compared to the other reported cases of inherited erythromelalgia, may contribute to the later age of onset and slower progression of the symptoms reported in association with this mutation.     

Selective activation of microglia in spinal cord but not higher cortical regions following nerve injury in adult mouse

Neuronal plasticity along the pathway for sensory transmission including the spinal cord and cortex plays an important role in chronic pain, including inflammatory and neuropathic pain. While recent studies indicate that microglia in the spinal cord are involved in neuropathic pain, a systematic study has not been performed in other regions of the central nervous system (CNS). In the present study, we used heterozygous Cx3cr1 ^GFP/+mice to characterize the morphological phenotypes of microglia following common peroneal nerve (CPN) ligation. We found that microglia showed a uniform distribution throughout the CNS, and peripheral nerve injury selectively activated microglia in the spinal cord dorsal horn and related ventral horn. In contrast, microglia was not activated in supraspinal regions of the CNS, including the anterior cingulate cortex (ACC), prefrontal cortex (PFC), primary and secondary somatosensory cortex (S1 and S2), insular cortex (IC), amygdala, hippocampus, periaqueductal gray (PAG) and rostral ventromedial medulla (RVM). Our results provide strong evidence that nerve injury primarily activates microglia in the spinal cord of adult mice, and pain-related cortical plasticity is likely mediated by neurons.     

A new species of Viola L. (Violaceae) from South Anatolia

A new species of Viola L., Viola yildirimlii M. Dinç & Y. Bağcı sp. nov. from South Anatolia is described and illustrated. It is found on the rocky slopes of Aladağ National Park, in the county of Adana, south Turkey, at an elevation of 1800 m. It belongs to Viola , subsect. Viola , and is similar to the Turkish endemics Viola isaurica Contandr. & Quézel and V. kizildaghensis M. Dinç & Ş. Yıldırımlı. Diagnostic morphologic characters for a detailed discrimination from two similar taxa and other Turkish Eflagellatae species are discussed.  © 2003 The Linnean Society of London, Botanical Journal of the Linnean Society , 2003, 141 , 477–482.     

FMRP acts as a key messenger for dopamine modulation in the forebrain

The fragile X mental retardation protein (FMRP) is an RNA-binding protein that controls translational efficiency and regulates synaptic plasticity. Here, we report that FMRP is involved in dopamine (DA) modulation of synaptic potentiation. AMPA glutamate receptor subtype 1 (GluR1) surface expression and phosphorylation in response to D1 receptor stimulation were reduced in cultured Fmr1(-/-) prefrontal cortex (PFC) neurons. Furthermore, D1 receptor signaling was impaired, accompanied by D1 receptor hyperphosphorylation at serine sites and subcellular redistribution of G protein-coupled receptor kinase 2 (GRK2) in both PFC and striatum of Fmr1(-/-) mice. FMRP interacted with GRK2, and pharmacological inhibition of GRK2 rescued D1 receptor signaling in Fmr1(-/-) neurons. Finally, D1 receptor agonist partially rescued hyperactivity and enhanced the motor function of Fmr1(-/-) mice. Our study has identified FMRP as a key messenger for DA modulation in the forebrain and may provide insights into the cellular and molecular mechanisms underlying fragile X syndrome.     

心衰患者动脉血气波浪式变化及其幅度降低的初步实验证据*

目的: 心力衰竭患者呼吸调控异常的机制众说纷纭,特别是动脉血气周期性波浪式变化信号的改变及其与心功能的关系尚缺乏直接的试验证据。本文依据心力衰竭患者动脉血气周期性波浪式变化信号的降低幅度,探讨心力衰竭导致呼吸调控异常的机制。方法: 选择5名心力衰竭患者,连续桡动脉逐搏取血,测定PaO₂,PaCO₂,pHa和SaO₂。选取2个典型呼吸周期,用于分析动脉血气的波浪式变化。比较患者相邻最高和最低值,以验证是否存在周期性波浪式信号变化。此外,将心力衰竭患者与心功能正常患者动脉血气周期性波浪式信号的变化幅度进行统计学t检验分析,比较有无差异。结果: 心力衰竭患者包括2例外科手术和3例ICU住院监护患者,4男1女,年龄(69±7)岁,身高(169±10)cm,体质量(75±19)kg,左心射血分数(LVEF)=(38±3)%。动脉血液充满肝素化细长塑化管需要17±2次心跳,即取血需要17±2次心跳,覆盖超过2个呼吸周期。心力衰竭患者PaO₂,PaCO₂,[H⁺]a和SaO₂均呈现明显的波浪式变化(P<0.05),幅度分别是(7.94±2.02)mmHg,(1.18±0.56)mmHg,(0.54±0.17)nmol/L和(0.21±0.07)%,分别是各自均值的(6.1±1.5)%,(3.2±1.5)%,(1.5±0.5)%和(0.2±0.1)%。与心功能正常患者比较,动脉血气波浪式变化幅度呈现明显降低趋势,但仅PaO₂和[H⁺]a有明显统计学差异(P<0.05)。结论: 采用连续逐搏动脉取血血气分析法证实,心力衰竭患者自主呼吸时动脉血气也有周期性波浪式变化信号,但其变化幅度较心功能正常患者明显降低。     

代谢、血液碱化和纯氧影响呼吸调控的人体实验研究II： 血液碱化后运动试验*

目的: 在完成吸入室内空气状态下症状限制性最大极限心肺运动试验(CPET)和动脉血气指标动态变化规律的基础上,进一步探讨体液酸碱度和CO₂含量对呼吸调控的影响。方法: 选正常志愿者5名,给予5%NaHCO₃(总量0.3 g/kg)分次口服,每5 min口服75 ml(3.75g )。总量服完1 h后,重复CPET。于静息、热身、运动及恢复期,连续测定肺通气指标及每分钟动脉取样的血气指标变化,并与本人在非碱化血液条件下对照数据进行配对t检验比较。结果: 碱化血液之后,CPET期间随着运动功率逐步递增,气体交换和血气指标的反应模式与非碱化血液对照相似（P>0.05）;即与静息状态比较,每分通气量、潮气量、呼吸频率、VO₂、VCO₂均呈现近于线性渐进性递增(P<0.05~0.001)。与碱化血液前吸入室内空气的对照比较：在碱化血液条件下,所有时间点血红蛋白浓度,PaCO₂与pH均显著提高(P<0.05);除无氧阈PaCO₂减低外,只有热身状态呈增高态势,统计学有显著差异(P<0.05);而PaO₂无差异(P>0.05),各状态均较对照状态减低,除恢复期外均有统计学差异(P<0.05)。与非碱化血液对照比较,除静息每分通气量低于对照(P<0.05）外,所有通气指标均无统计学差异(P>0.05)。结论: 碱化血液条件下, 尽管有更高的CaCO₂, PaCO₂ 和 pHa平均水平及更低的Hba和[H⁺]a平均水平,机体对CPET的呼吸反应模式基本相似。     

基于样带的唐古特白刺灌丛沙包空间格局尺度研究

黄河河岸与库布齐沙漠之间生态过渡带上的唐古特白刺(Nitraria Tangutorum)灌丛沙包由于遭受到不同程度的破坏而表现出一定程度的退化,空间格局尺度从一定程度上表征了其破碎化程度。我们分别应用样方方差法,小波分析,分维,谱分析以及空隙度分析等方法对鄂尔多斯高原北缘唐古特白刺灌丛沙包的空间格局尺度进行了比较研究,旨在选出适合分析干旱半干旱区白刺灌丛沙包空间格局尺度的方法,并确定研究区内唐古特白刺灌丛沙包的空间格局尺度,为保护唐古特白刺灌丛沙包提供科学依据。结果表明:(1)TTLQV法得到的格局尺度过大,而小波分析得到的格局尺度过小,分维分析得到的格局尺度除了相对较小之外,趋势也不明显,因此都不适合分析干旱半干旱区白刺灌丛沙包的空间格局尺度;(2)而3TLQV,tQV,谱分析和空隙度分析所得到的结果则相对容易接受,其大小顺序是:3TLQV>tQV>空隙度分析>谱分析;(3)独贵塔拉、呼和木独和巴拉贡唐古特白刺灌丛沙包的空间格局尺度分别为16.7～27.1m,10.2～25.0m和8.8～17.0m,这一结果将有助于在今后的研究中合理地确定研究范围和尺度。