Brain temperature regulation in poor-grade subarachnoid hemorrhage patients – A multimodal neuromonitoring study

Elevated body temperature (T_core) is associated with poor outcome after subarachnoid hemorrhage (SAH). Brain temperature (T_brain) is usually higher than T_core. However, the implication of this difference (T_delta) remains unclear. We aimed to study factors associated with higher T_delta and its association with outcome. We included 46 SAH patients undergoing multimodal neuromonitoring, for a total of 7879 h of averaged data of T_core, T_brain, cerebral blood flow, cerebral perfusion pressure, intracranial pressure and cerebral metabolism (CMD). Three-months good functional outcome was defined as modified Rankin Scale ≤2. T_brain was tightly correlated with T_core (r = 0.948, p < 0.01), and was higher in 73.7% of neuromonitoring time (T_delta +0.18°C, IQR −0.01 – 0.37°C). A higher T_delta was associated with better metabolic state, indicated by lower CMD-glutamate (p = 0.003) and CMD-lactate (p < 0.001), and lower risk of mitochondrial dysfunction (MD) (OR = 0.2, p < 0.001). During MD, T_delta was significantly lower (0°C, IQR −0.2 – 0.1; p < 0.001). A higher T_delta was associated with improved outcome (OR = 7.7, p = 0.002). Our study suggests that T_brain is associated with brain metabolic activity and exceeds T_core when mitochondrial function is preserved. Further studies are needed to understand how T_delta may serve as a surrogate marker for brain function and predict clinical course and outcome after SAH.     

Assessment of neuroinflammation in the aging hippocampus using large-molecule microdialysis: Sex differences and role of purinergic receptors

Aging is associated with an enhanced neuroinflammatory response to acute immune challenge, often termed “inflammaging.” However, there are conflicting reports about whether baseline levels of inflammatory markers are elevated under ambient conditions in the aging brain, or whether such changes are observed predominantly in response to acute challenge. The present studies utilized two distinct approaches to assess inflammatory markers in young and aging Fischer 344 rats. Experiment 1 examined total tissue content of inflammatory markers from hippocampus of adult (3 month), middle-aged (12 month), and aging (18 month) male Fischer (F) 344 rats using multiplex analysis (23-plex). Though trends emerged for several cytokines, no significant differences in basal tissue content were observed across the 3 ages examined. Experiment 2 measured extracellular concentrations of inflammatory factors in the hippocampus from adult (3 month) and aging (18 month) males and females using large-molecule in vivo microdialysis. Although few significant aging-related changes were observed, robust sex differences were observed in extracellular concentrations of CCL3, CCL20, and IL-1α. Experiment 2 also evaluated the involvement of the P2X7 purinergic receptor in neuroinflammation using reverse dialysis of the selective agonist BzATP. BzATP produced an increase in IL-1α and IL-1β release and rapidly suppressed the release of CXCL1, CCL2, CCL3, CCL20, and IL-6. Other noteworthy sex by aging trends were observed in CCL3, IL-1β, and IL-6. Together, these findings provide important new insight into late-aging and sex differences in neuroinflammation, and their regulation by the P2X7 receptor.     

在体皮肤微透析分析制川乌-白芍配伍对芍药苷局部药代动力学的影响

目的:考察制川乌对白芍中芍药苷经皮转运的影响,从经皮转运角度研究制川乌-白芍配伍协同增效作用机制。方法:以昆明种清洁级小鼠为实验对象,分别经皮给予白芍凝胶、制川乌-白芍凝胶和白芍-氮酮凝胶,采用皮肤微透析取样技术,建立HPLC测定透析液中芍药苷的浓度,流动相乙腈-0.1%磷酸水溶液(14∶86),检测波长230 nm;利用DAS 2.0软件计算局部药动学参数,采用扫描电镜考察药物对小鼠皮肤角质层的影响。结果:白芍凝胶组的药时曲线下面积(AUC_(0-t)),平均滞留时间(MRT_(0-t)),半衰期(t_(1/2)),达峰时间(T_(max))和药峰浓度(C_(max))分别为(3.28±1.01)mg·L~(-1)·h,(3.95±0.32)h,(0.92±0.44)h,(2.00±0)h和(0.72±0.24)mg·L~(-1);白芍-制川乌凝胶组MRT_(0-t),AUC_(0-t),t_(1/2),T_(max)和C_(max)分别为(3.35±0.08)h,(10.64±1.24)mg·L~(-1)·h,(1.32±0.67)h,(1.00±0)h和(3.06±0.38)mg·L~(-1),白芍-氮酮凝胶组AUC_(0-t),MRT_(0-t),t_(1/2),T_(max),C_(max)分别为(59.82±13.51)mg·L~(-1)·h,(3.67±0.08)h,(0.89±0.16)h,(2.67±0.29)h和(13.24±4.14)mg·L~(-1)。与白芍凝胶组比较,制川乌-白芍凝胶组AUC_(0-t)和C_(max)均显著增大,T_(max)明显缩短。扫描电镜观察结果表明制川乌作用皮肤后,角质层细胞间隙明显增加,且与氮酮对皮肤的作用类似。结论:制川乌-白芍配伍能显著提高芍药苷的透皮吸收,达到配伍"增效"的目的,这可能与制川乌降低角质层的屏障作用有关。     

Intraabdominal microdialysis – methodological challenges

Microdialysis is used for in vivo sampling of extracellular molecules. The technique provides a continuous and dynamic view of concentrations of both endogenous released and exogenous administered substances. Microdialysis carries a low risk of complications and has proven to be a safe procedure in humans. The technique has been applied in several clinical areas, including gastrointestinal surgery. Microdialysis may be used for studies of tissue metabolism, and the technique is also a promising tool for pharmacological studies of drug penetration into abdominal organ tissue and the peritoneal cavity. The clinical significance of intraabdominal microdialysis in postoperative monitoring of surgical patients has yet to be proven. In this review, we introduce the microdialysis technique, and we present an overview of theoretical and practical considerations that should be taken into account when using microdialysis in intraabdominal clinical research.     

Serotonin‐2C receptor agonists decrease potassium‐stimulated GABA release in the nucleus accumbens

The serotonin 5‐HT_2C receptor has shown promise in vivo as a pharmacotherapeutic target for alcoholism. For example, recently, a novel 4‐phenyl‐2‐N,N‐dimethylaminotetralin (PAT) drug candidate, that demonstrates 5‐HT_2C receptor agonist activity together with 5‐HT_2A/2B receptor inverse agonist activity, was shown to reduce operant responding for ethanol after peripheral administration to rats. Previous studies have shown that the 5‐HT_2C receptor is found throughout the mesoaccumbens pathway and that 5‐HT_2C receptor agonism causes activation of ventral tegmental area (VTA) GABA neurons. It is unknown what effect 5‐HT_2C receptor modulation has on GABA release in the nucleus accumbens core (NAcc). To this end, microdialysis coupled to capillary electrophoresis with laser‐induced fluorescence was used to quantify extracellular neurotransmitter concentrations in the NAcc under basal and after potassium stimulation conditions, in response to PAT analogs and other 5‐HT_2C receptor modulators administered by reverse dialysis to rats. 5‐HT_2C receptor agonists specifically attenuated stimulated GABA release in the NAcc while 5‐HT_2C antagonists or inverse agonists had no effect. Agents with activity at 5‐HT_2A receptors had no effect on GABA release. Thus, in contrast to results reported for the VTA, current results suggest 5‐HT_2C receptor agonists decrease stimulated GABA release in the NAcc, and provide a possible mechanism of action for 5HT_2C‐mediated negative modulation of ethanol self‐administration. Synapse 69:78–85, 2015. © 2014 Wiley Periodicals, Inc.     

Chronic social isolation during adolescence augments catecholamine response to acute ethanol in the basolateral amygdala

Adolescent social isolation (SI) results in numerous behavioral alterations associated with increased risk of alcoholism. Notably, many of these changes involve the basolateral amygdala (BLA), including increased alcohol seeking. The BLA sends a strong glutamatergic projection to the nucleus accumbens and activation of this pathway potentiates reward‐seeking behavior. Dopamine (DA) and norepinephrine (NE) exert powerful excitatory and inhibitory effects on BLA activity and chronic stress can disrupt the excitation‐inhibition balance maintained by these catecholamines. Notably, the impact of SI on BLA DA and NE neurotransmission is unknown. Thus the aim of this study was to characterize SI‐mediated catecholamine alterations in the BLA. Male Long Evans rats were housed in groups of four (GH) or in SI for 6 weeks during adolescence. DA and NE transporter levels were then measured using Western blot hybridization and baseline and ethanol‐stimulated DA and NE levels were quantified using microdialysis. DA transporter levels were increased and baseline DA levels were decreased in SI compared to GH rats. SI also increased DA responses to an acute ethanol (2 g kg^?1) challenge. While no group differences were noted in NE transporter or baseline NE levels, acute ethanol (2 g kg^?1) only significantly increased NE levels in SI animals. Collectively, these SI‐dependent changes in BLA catecholamine signaling may lead to an increase in BLA excitability and a strengthening of the glutamatergic projection between the BLA and NAc. Such changes may promote the elevated ethanol drinking behavior observed in rats subjected to chronic adolescent stress. Synapse 69:385–395, 2015 . © 2015 Wiley Periodicals, Inc.     

A novel Na+‐Independent alanine‐serine‐cysteine transporter 1 inhibitor inhibits both influx and efflux of D‐Serine

NMDA receptor dysfunctions are hypothesized to underlie the pathophysiology of schizophrenia, and treatment with D‐serine (D‐Ser), an NMDA receptor coagonist, may improve the clinical symptoms of schizophrenia. Thus, upregulating the synaptic D‐Ser level is a novel strategy for schizophrenia treatment. Na⁺‐independent alanine‐serine‐cysteine transporter 1 (asc‐1) is a transporter responsible for regulating the extracellular D‐Ser levels in the brain. In this study, we discovered a novel asc‐1 inhibitor, (+)‐amino(1‐(3,5‐dichlorophenyl)‐3,5‐dimethyl‐1H‐pyrazol‐4‐yl)acetic acid (ACPP), and assessed its pharmacological profile. ACPP inhibited the D‐[³H]Ser uptake in human asc‐1‐expressing CHO cells and rat primary neurons with IC₅₀ values of 0.72 ± 0.13 and 0.89 ± 0.30 μM, respectively. In accordance with the lower asc‐1 expression levels in astrocytes, ACPP did not inhibit D‐Ser uptake in rat primary astrocytes. In a microdialysis study, ACPP dose dependently decreased the extracellular D‐Ser levels in the rat hippocampus under the same conditions in which the asc‐1 inhibitor S‐methyl‐L‐cysteine (SMLC) increased it. To obtain insights into this difference, we conducted a D‐[³H]Ser efflux assay using asc‐1‐expressing CHO cells. ACPP inhibited D‐[³H]Ser efflux, whereas SMLC increased it. These results suggest that ACPP is a novel inhibitor of asc‐1. © 2016 Wiley Periodicals, Inc.     

Changes in extracellular striatal acetylcholine and brain seizure activity following acute exposure to nerve agents in freely moving guinea pigs

Organophosphorus nerve agents irreversibly inhibit acetylcholinesterase (AChE) in the peripheral and central nervous systems, causing an increase in the concentration of acetylcholine (ACh) in the synapse or neuromuscular junction and subsequent adverse effects. In this study, in vivo microdialysis was utilized to collect samples from the striatum for monitoring changes in extracellular ACh levels along with cortical electroencephalographic (EEG) recordings for identifying seizure activity after acute subcutaneous (s.c.) exposure to 1.0?×?LD₅₀ of the nerve agents sarin, soman, or one of two V-type agents (VX, or a Russian V-agent, designated VR) in unanesthetized freely moving guinea pigs. Based on EEG recordings, these animals were subsequently divided into groups that developed seizures (S) and those that did not develop seizures (NS). Maximum ACh levels in the striatum were observed at 60–70?min for sarin and soman S groups and 105?min for VX and VR S groups. In all NS groups the greatest increase in extracellular ACh occurred within 30?min after exposure, although in the sarin NS group a few sporadic increases of ACh from control occurred. Animals that developed seizures, regardless of the nerve agent, had significantly higher extracellular striatal ACh levels compared to the controls or those animals that did not develop seizures, yet both S and NS groups displayed similar levels of blood AChE inhibition. Regardless of the agent, all animals in the non-seizure groups survived 24?h, while lethality (25–42%) was observed only in animals that experienced seizure activity.