辽宁省丹东地区吸血蠓类(双翅目:蠓科)生态调查

吸血蠓类对人畜危害较大,不仅是多种疾病的传播媒介,而且刺叮吸血骚扰性很大。1988年我们在辽宁省丹东地区东沟和风城二县郊区进行了采集和生态习性的调查,现将结果报道如下。材料和方法器材由军事医学科学院微生物流行病研究所提供的诱蠓帐、捕虫网和吸虫器。调查方法     

痛泻要方对“肝气乘脾”泄泻小鼠肠黏膜及肠内容物消化酶活性的影响

目的探讨痛泻要方对"肝气乘脾"泄泻小鼠肠道酶活性的影响。方法采用"番泻叶-离心管束缚夹尾法"进行"肝气乘脾"泄泻造模,造模成功后以痛泻要方治疗,造模和治疗后分别分析小鼠肠道酶活性。结果造模后,模型组小鼠肠道内容物的淀粉酶活性显著降低(t=4.007,P=0.015),纤维素酶、蛋白酶、蔗糖酶活性下降不显著。模型组小鼠肠黏膜蛋白酶、淀粉酶、蔗糖酶活性显著下降(t_蛋=5.652,P=0.005;Z_淀=-1.964,P=0.050;t_蔗=4.737,P=0.009)。痛泻要方治疗后,中药干预组小鼠肠道内容物蛋白酶、纤维素酶、乳糖酶和蔗糖酶活性变化不显著;自然恢复组的淀粉酶活性显著高于正常组(t=-7.497,P=0.002)。中药干预组小鼠肠道前段黏膜蛋白酶、乳糖酶、淀粉酶、蔗糖酶活性恢复不显著;中药干预组小鼠肠道黏膜中段乳糖酶、蔗糖酶活性显著低于自然恢复组(t_乳=4.074,P=0.013;t_蔗=8.072,P0.001),而蛋白酶、淀粉酶及纤维素酶活性均高于自然恢复组;中药干预组小鼠肠道后段黏膜乳糖酶、蔗糖酶及淀粉酶活性显著高于正常组(t_乳=-7.962,P0.001;t_蔗=-15.921,P0.001;Z_淀=6.489,P=0.034),蛋白酶与纤维素酶活性均有所升高。结论 "肝气乘脾"泄泻肠道内容物及黏膜淀粉酶活性显著降低,痛泻要方对"肝气乘脾"泄泻小鼠肠黏膜乳糖酶、蔗糖酶及淀粉酶活性作用显著。     

不同胃癌前病变中医证型PG、G-17、CEA和叶酸水平变化及相关性研究

目的:对不同胃癌前病变中医证型和血清胃蛋白酶原(pepsinogen,PG)、胃泌素-17(gastrin-17,G-17)、癌胚抗原(carcinoembryonic antigen,CEA)和叶酸水平变化的关系进行探讨,为胃癌前病变的诊断提供一定的依据。方法:以80例胃癌前病变(precancerous lesion of gastric cancer,PLGC)患者研究组,80例健康者为对照组,对研究组患者进行中医临床辨证分型,对两组研究对象的血清PG、G-17、CEA和叶酸进行测定比较。结果:研究组PLGC患者中医证型分布不均匀,差异显著(P<0.05),由多到少依次为湿热蕴胃并/兼脾胃虚寒证>胃络瘀阻并/兼气阴两虚证>痰湿中阻并/兼脾胃气虚证>肝胃气滞并/兼气阴两虚证>肝胃气滞并/兼脾胃虚寒证>湿热蕴胃并/兼胃阴不足证。PLGC不同中医证型患者血清PG I和PG II水平差异显著(P<0.05);与对照组比较,各证型PG I水平均显著降低,PG II水平均显著升高(P<0.05)。且湿热蕴胃并/兼脾胃虚寒证和胃络瘀阻并/兼气阴两虚证的PG I水平显著低于其他证候,血清PG II水平显著高于其他(P<0.05)。与对照组比较,研究组不同证候的G-17、CEA水平显著升高,叶酸水平显著降低(P<0.05);观察组中湿热蕴胃并/兼脾胃虚寒证和胃络瘀阻并/兼气阴两虚证G-17、CEA显著高于其他证候,叶酸水平显著低于其他证候(P<0.05)。结论:胃癌前病变不同中医证型血清PG、G-17、CEA和叶酸存在明显差异。     

少数民族中医体质类型研究现状

中医体质学以人为研究对象,为了研究不同体质构成特点、演变规律、影响因素、分类标准,从而指导疾病的预防、诊治、康复与养生。目前关于生理和病理状态下的中医体质研究日益受到关注,因为对其研究符合中医”治未病”的理念,而关于少数民族的中医体质类型研究开展较少,但对少数民族之间和汉族之间中医体质的比较研究及与生活习惯,生活环境的联系将能更好地说明先天因素和后天环境对中医体质形成的影响。本文就这一领域的研究现状进行总结,对少数民族中医体质的研究一方面可为少数民族人群的疾病防治提供依据,另一方面有助于中医体质形成机理的阐明。     

黄腻舌苔和薄白舌苔微生物种群差异

【背景】舌苔是指舌头上覆盖的由食物残渣、微生物、舌苔上皮角质细胞组成的物质。根据舌苔的厚度、颜色等苔质情况来鉴别病人的健康与疾病状况,是“望”诊的重要内容之一,是中医临床辨证施治的主要依据之一。但是舌苔苔质的形成和微生物菌群的关系还有待深入研究。【目的】探索黄腻舌苔和薄白舌苔菌群群落组成的差异及与舌苔苔质形成的关系。【方法】以薄白舌苔和黄腻舌苔为研究对象,用刮舌板刮取青年学生人群的舌苔表面,获得舌苔样品进行总DNA提取,PCR扩增微生物16S rRNA基因,通过高通量测序获得16S rRNA基因序列,然后通过交互序列分析软件分析样品中细菌菌群种类及差异。【结果】黄腻和薄白舌苔原核微生物群落组成具有明显差异。其中,在门水平上,Patescibacteria和蓝细菌门细菌在黄腻舌苔上明显比薄白舌苔多,具有极显著差异(P<0.01);在属和种水平上,放线菌(Actinomyces)的组成具有显著差异(P<0.05),黄腻舌苔中放线菌含量明显高于薄白舌苔;而薄白舌苔中的卟啉单胞菌属(Porphyromonas)和莫拉氏菌属(Moraxella)的含量明显高于黄腻舌苔,差异显著(P<0.05)。【结论】黄腻舌苔苔厚、色黄、有异味,有可能是放线菌含量过高导致。而且,有些放线菌可以导致侵袭性细菌性疾病,称作放线菌病。因此,健康人出现黄腻苔,可在一定程度上提示体内潜在的炎性预警。薄白舌苔正常菌群莫拉氏菌属(Moraxella)和卟啉单胞菌属(Porphyromonas)显著比黄腻舌苔上的多,说明这两种正常菌群可能在维护正常口气和舌苔功能方面具有重要的作用。     

Honokiol: A non-adipogenic PPARγ agonist from nature

Background

Peroxisome proliferator-activated receptor gamma (PPARγ) agonists are clinically used to counteract hyperglycemia. However, so far experienced unwanted side effects, such as weight gain, promote the search for new PPARγ activators.

Methods

We used a combination of in silico, in vitro, cell-based and in vivo models to identify and validate natural products as promising leads for partial novel PPARγ agonists.

Results

The natural product honokiol from the traditional Chinese herbal drug Magnolia bark was in silico predicted to bind into the PPARγ ligand binding pocket as dimer. Honokiol indeed directly bound to purified PPARγ ligand-binding domain (LBD) and acted as partial agonist in a PPARγ-mediated luciferase reporter assay. Honokiol was then directly compared to the clinically used full agonist pioglitazone with regard to stimulation of glucose uptake in adipocytes as well as adipogenic differentiation in 3T3-L1 pre-adipocytes and mouse embryonic fibroblasts. While honokiol stimulated basal glucose uptake to a similar extent as pioglitazone, it did not induce adipogenesis in contrast to pioglitazone. In diabetic KKAy mice oral application of honokiol prevented hyperglycemia and suppressed weight gain.

Conclusion

We identified honokiol as a partial non-adipogenic PPARγ agonist in vitro which prevented hyperglycemia and weight gain in vivo.

General significance

This observed activity profile suggests honokiol as promising new pharmaceutical lead or dietary supplement to combat metabolic disease, and provides a molecular explanation for the use of Magnolia in traditional medicine.     

Han ethnicity-specific type 2 diabetic treatment from traditional Chinese medicine?

Insulin-degrading enzyme (IDE) gene is one of the type 2 diabetes mellitus susceptibility genes specific to the Han Chinese population. IDE, a zinc-metalloendopeptidase, is a potential target for controlling insulin degradation. Potential lead compounds for IDE inhibition were identified from traditional Chinese medicine (TCM) through virtual screening and evaluation of their pharmacokinetic properties of absorption, distribution, metabolism, excretion, and toxicity. Molecular dynamics (MD) simulation was performed to validate the stability of complexes from docking simulation. The top three TCM compounds, dihydrocaffeic acid, isopraeroside IV, and scopolin, formed stable H–bond interactions with key residue Asn139, and were linked to active pocket residues His108, His112, and Glu189 through zinc. Torsion angle trajectories also indicated some stable interactions for each ligand with IDE. Molecular level analysis revealed that the TCM candidates might affect IDE through competitive binding to the active site and steric hindrance. Structural feature analysis reveals that high amounts of hydroxyl groups and carboxylic moieties contribute to anchor the ligand within the complex. Hence, we suggest the top three TCM compounds as potential inhibitor leads against IDE protein to control insulin degradation for type 2 diabetes mellitus.

An animated interactive 3D complement (I3DC) is available in Proteopedia at http://proteopedia.org/w/Journal:JBSD:29     

A possible strategy against head and neck cancer: in silico investigation of three-in-one inhibitors

Overexpression of epidermal growth factor receptor (EGFR), Her2, and uroporphyrinogen decarboxylase (UROD) occurs in a variety of malignant tumor tissues. UROD has potential to modulate tumor response of radiotherapy for head and neck cancer, and EGFR and Her2 are common drug targets for the treatment of head and neck cancer. This study attempts to find a possible lead compound backbone from TCM Database@Taiwan (http://tcm.cmu.edu.tw/) for EGFR, Her2, and UROD proteins against head and neck cancer using computational techniques. Possible traditional Chinese medicine (TCM) lead compounds had potential binding affinities with EGFR, Her2, and UROD proteins. The candidates formed stable interactions with residues Arg803, Thr854 in EGFR, residues Thr862, Asp863 in Her2 protein, and residues Arg37, Arg41 in UROD protein, which are key residues in the binding or catalytic domain of EGFR, Her2, and UROD proteins. Thus, the TCM candidates indicated a possible molecule backbone for evolving potential inhibitors for three drug target proteins against head and neck cancer.

An animated interactive 3D complement (I3DC) is available in Proteopedia at http://proteopedia.org/w/Journal:JBSD:35     

金双歧联合通腑合剂治疗急性胰腺炎的临床研究

【摘 要】 目的 观察金双歧联合通腑合剂治疗急性胰腺炎的临床效果。方法 120例胰腺炎患者,随机分为常规治疗组、通腑合剂组和联合治疗组,每组40例。采取不同治疗方法,分别观察3组患者的临床治疗效果、实验室指标改善情况以及住院时间等。结果 联合治疗组治疗效果明显优于常规治疗组及通腑合剂组（P<0.05）,未出现恶化病例,其腹痛、腹胀缓解时间及血淀粉酶（AMY）和C反应蛋白（CRP）恢复时间明显短于常规治疗组和通腑治疗组,差异均有统计学意义（P<0.05）。联合治疗组和通腑合剂组在血白细胞（WBC）和血脂肪酶（LPS）恢复上差异无统计学意义（P>0.05）,但均优于常规治疗组,差异有统计学意义（P<0.05）。结论 金双歧联合通腑合剂治疗急性胰腺炎有较好的临床效果,并能缩短住院时间。