中国新纪录属——异粗额蚜属(半翅目,蚜科)

记述了中国蚜科Aphididae长管蚜亚科Macrosiphinae1新纪录属——异粗额蚜属Anaulacorthum Ghosh & Raychaudhuri,1972;重记述了张家界异粗额蚜Anaulacorthum zhangjiajiensis(Zhang,1992)的形态特征,提供了该种的地理分布与寄主植物信息,绘制了形态特征图。研究标本保存在中国科学院动物研究所国家动物博物馆。     

石斛小菇的药理活性研究

对分离自野生铁皮石斛中的一种新的内生真菌石斛小菇进行了初步的药理活性测定,发现石斛小菇的发酵液对小鼠中枢神经系统有兴奋作用,石斛小菇菌丝体和发酵液的粗提物具有与中药石斛相似的镇痛作用,并结合化学方法确定了石斛小菇粗提物中与其镇痛药效相对应的活性部位。     

银杏内酯对原代培养神经元缺氧诱导因子-1α基因表达的影响

目的研究银杏内酯(ginkgolides,Gin)对单纯缺氧和模拟缺血神经元的缺氧诱导因子1α(hypoxiainduciblefactor1α,HIF1α)表达的影响。方法用RTPCR法检测原代培养胚胎小鼠皮层神经元经缺氧或剥夺氧和葡萄糖两种损伤处理,以及给予Gin(终浓度为37.5μg/ml)预保护时,HIF1αmRNA表达的变化。结果在培养的皮层神经元中HIF1αmRNA有一定的基础表达,Gin处理24h可明显提高HIF1α的表达水平;经单纯缺氧1h后,HIF1αmRNA表达上调,而预先给予Gin其表达强度进一步提高;但经剥夺氧和葡萄糖处理的神经元,HIF1αmRNA表达较未缺氧对照组明显降低,而预加Gin则能减轻HIF1αmRNA表达的下降。结论Gin对缺氧/缺血损伤神经元的HIF1αmRNA表达有上调作用。     

ROCK is Involved in Vimentin Phosphorylation and Rearrangement Induced by Dengue Virus

Our previous study showed that dengue virus 2 (DENV2) infection induces rearrangement of vimentin into dense structures at the perinuclear area. However, the underlying mechanism of this phenomenon is poorly characterized. In the present work, we found that vimentin and Ser71 phosphorylated vimentin display similar distributions in DENV2-infected cells. DENV2 infection also induced ROCK activation and phosphorylation of vimentin at Ser71 as the DENV2 infection progressed. Furthermore, Ser71 phosphorylation and vimentin rearrangement induced by DENV2 infection were blocked by the ROCK inhibitor Y-27632. In addition, DENV2 led to endoplasmic reticulum (ER) redistribution in the perinuclear region of the host cells, which was partially blocked by pretreatment with Y-27632. Together, these data support indicate that ROCK may have a role in governing regulating vimentin and ER rearrangement during DENV2 infection. We hypothesize that DENV2 infection, via ROCK activation, induces both vimentin rearrangement and ER redistribution around the perinuclear region, which may play a structural role in anchoring DENV2 to replication sites.     

CYP2C19 Phenotype,Stent Thrombosis,Myocardial Infarction,and Mortality in Patients with Coronary Stent Placement in a Chinese Population

Background

Several studies have indicated that CYP2C19 loss-of-function polymorphisms have a higher risk of stent thrombosis (ST) after percutaneous coronary interventions (PCIs). However, this association has not been investigated thoroughly in a Chinese population. In this study, we aimed to determine the effect of CYP2C19*2 and CYP2C19*3 loss-of-function polymorphisms on the occurrence of ST and other adverse clinical events in a Chinese population.

Methods

We designed a cohort study among 1068 consecutive patients undergoing intracoronary stent implantation after preloading with 600 mg of clopidogrel. CYP2C19*2 and CYP2C19*3 were genotyped by using polymerase chain reaction-restriction fragment length polymorphism analysis. The adverse clinical events recorded were ST, death, myocardial infarction (MI), and bleeding events. The primary end point of the study was the incidence of cumulative ST within 1 year after PCI. The secondary end point was other adverse clinical outcomes 1 year after the procedure.

Results

The cumulative 1-year incidence of ST was 0.88% in patients with extensive metabolizers (EMs) (CYP2C19*1/*1 genotype), 4.67% in patients with intermediate metabolizers (IMs) (CYP2C19*1/*2 or *1/*3 genotype), and 10.0% in patients with poor metabolizers (PMs) (CYP2C19*2/*2, *2/*3, or *3/*3 genotype) (P<0.001). The one-year event-free survival was 97.8% in patients with EMs, 96.5% in patients with IMs, and 92.0% in patients with PMs (P = 0.014). Multivariate analysis confirmed the independent association of CYP2C19 loss-of-function allele carriage with ST (P = 0.009) and total mortality (P<0.05).

Conclusion

PM patients had an increased risk of ST, death, and MI after coronary stent placement in a Chinese population.     

Sex and dosing-time dependencies in irinotecan-induced circadian disruption

Circadian disruption accelerates malignant growth; thus, it should be avoided in anticancer therapy. The circadian disruptive effects of irinotecan, a topoisomerase I inhibitor, was investigated according to dosing time and sex. In previous work, irinotecan achieved best tolerability following dosing at zeitgeber time (ZT) 11 in male and ZT15 in female mice, whereas worst toxicity corresponded to treatment at ZT23 and ZT3 in male and female mice, respectively. Here, irinotecan (50 mg/kg intravenous [i.v.]) was delivered at the sex-specific optimal or worst circadian timing in male and female B6D2F1 mice. Circadian disruption was assessed with rest-activity, body temperature, plasma corticosterone, and liver mRNA expressions of clock genes Rev-erbα, Per2, and Bmal1. Baseline circadian rhythms in rest-activity, body temperature, and plasma corticosterone were more prominent in females as compared to males. Severe circadian disruption was documented for all physiology and molecular clock endpoints in female mice treated at the ZT of worst tolerability. Conversely, irinotecan administration at the ZT of best tolerability induced slight alteration of circadian physiology and clock-gene expression patterns in female mice. In male mice, irinotecan produced moderate alterations of circadian physiology and clock-gene expression patterns, irrespective of treatment ZT. However, the average expression of Rev-erbα, Per2, and Bmal1 were down-regulated 2- to 10-fold with irinotecan at the worst ZT, while being minimally or unaffected at the best ZT, irrespective of sex. Corticosterone secretion increased acutely within 2?h with a sex-specific response pattern, resulting in a ZT-dependent phase-advance or -delay in both sex. The mRNA expressions of irinotecan clock-controlled metabolism genes Ce2, Ugt1a1, and Top1 were unchanged or down-regulated according to irinotecan timing and sex. This study shows that the circadian timing system represents an important toxicity target of irinotecan in female mice, where circadian disruption persists after wrongly timed treatment. As a result, the mechanisms underling cancer chronotherapeutics are expectedly more susceptible to disruption in females as compared to males. Thus, the optimal circadian timing of chemotherapy requires precise determination according to sex, and should involve the noninvasive monitoring of circadian biomarkers.     

Isolation of a buprofezin co-metabolizing strain of <Emphasis Type="Italic">Pseudomonas</Emphasis> sp. DFS35-4 and identification of the buprofezin transformation pathway

Buprofezin is a widely used insecticide that has caused environmental pollution in many areas. However, biodegradation of buprofezin by pure cultures has not been extensively studied, and the transformation pathway of buprofezin remains unclear. In this paper, a buprofezin co-metabolizing strain of DFS35-4 was isolated from a buprofezin-polluted soil in China. Strain DFS35-4 was preliminarily identified as Pseudomonas sp. based on its morphological, physiological, and biochemical properties, as well as 16S rRNA gene analysis. In the presence of 2.0 g l⁻¹ sodium citrate, strain DFS35-4 degraded over 70% of 50 mg l⁻¹ buprofezin in 3 days. Strain DFS35-4 efficiently degraded buprofezin in the pH range of 5.0–10.0 and at temperatures between 20 and 30°C. Three metabolites, 2-imino-5-phenyl-3-(propan-2-yl)-1,3,5-thiadiazinan-4-one, 2-imino-5-phenyl-1,3,5-thiadiazinan-4-one, and methyl(phenyl) carbamic acid, were identified during the degradation of buprofezin using gas chromatography–mass spectrometry (GC–MS) and tandem mass spectrometry (MS/MS). A partial transformation pathway of buprofezin in Pseudomonas sp. DFS35-4 was proposed based on these metabolites.     

定量分析丝氨酸/甘氨酸转换影响胃癌细胞增殖的动力学机制

目的 胃癌（GC）严重影响人类的健康生活,研究表明其与丝氨酸/甘氨酸代谢密切相关。丝氨酸/甘氨酸代谢对于肿瘤细胞的增殖能力具有重要影响。本文的研究目的是探究丝氨酸/甘氨酸代谢能够影响胃癌细胞增殖能力的分子机制。方法 本文通过一种基于随机和非梯度系统的势能景观所建立的大型代谢网络动力学建模方法,构建了一个稳定的胃癌细胞代谢动力学模型。基于对模型的调控,定量分析丝氨酸/甘氨酸代谢影响胃癌细胞增殖的动力学机制。对一般代谢网络动力学方程添加随机噪声,通过随机动力学分解得到代谢网络参数空间的李雅普诺夫（Lyapunov）函数。进一步减少与随机波动相关的Lyapunov函数变化,从而得到稳定的代谢网络。结果 在动力学参数不足的情况下,成功构建了胃癌细胞代谢网络的动力学模型。当胞外丝氨酸可用时,模型优先消耗丝氨酸;当甘氨酸生成丝氨酸的速率增加时,模型显著上调生成S-腺苷甲硫氨酸（SAM）和S-腺苷同型半胱氨酸（SAH）的稳态通量。结论 本文证明了胃癌细胞对于丝氨酸的优先摄取以及丝氨酸/甘氨酸转化速率对SAM生成的重要作用,其可能通过调节细胞甲基化进程影响胃癌细胞的增殖能力,为靶向丝氨酸/甘氨酸代谢的癌症治疗提供了新的思路和方向。     

槐树长珠蚧的生物学特性

槐树长珠蚧Neogreenia sophorica Wu是2004年发现于北京东城区的一种新害虫,危害槐树。在北京1年发生1代,有3个龄期,以2龄若虫过冬。营孤雌生殖。每头雌蚧平均产卵105粒,平均孵化率47.53%。1龄若虫期有扩散能力,固定后分布在树干基部1m以上,直径大于5cm的枝条的树皮下。防治的最佳时机应在1龄若虫涌散期。     

Analysis of the compliance and the related influence factors in the follow-up process of surveillance for Creutzfeldt-Jakob disease in China

Creutzfeldt-Jakob disease (CJD) is a kind of rare, rapidly progressive fatal central nervous system disorders. In China, the surveillance for CJD has started since 2006. As one of the major issues in CJD surveillance, the follow-up process via telephone plays important role in CJD diagnosis and surveillance. Although the follow-up process was conducted by the experiential staffs from CJD surveillance center in China CDC, it is frequently encountered that some interviewed family members do not cooperate well during follow-up. To screen the possible factors influence on the compliances of the interviewees during CJD follow-up, 11 independent variables from patient aspect and 4 variables from interviewee aspect were selected and a questionnaire was prepared. Based on 199 suspected sporadic CJD cases reported to CJD surveillance center in 2013, a telephone-inquiring was conducted and the degree of compliances of the interviewees were given as good, fair or poor. After screened with univariate analysis and evaluated ordinal logistic regression analysis, several indictors, such as the patient gender, CJD diagnosis, numbers of clinical symptoms, continual medical treatment after diagnosis, medical treatment mode, as well as the relationship with the patient and CJD knowledge of the interviewees, showed influence on the compliance in CJD follow-up process significantly. The data here provide for the first time the factors related with the compliances of the interviewed family members of the suspected CJD patients during follow-up process, which supplies useful clue for us to improve CJD follow-up process and increase the capacity of CJD surveillance.