A Stable Upstream Stem-loop Structure Enhances Selection of the First 5''''-ORF-AUG as a Main Start Codon for Translation Initiation of Human ACAT1 mRNA

Acyl-coenzyme A:cholesterol acyltransferase (ACAT)is an integral membrane protein, which is mainly locatedin rough endoplasmic reticulum (ER), and is responsiblefor catalyzing the intracellular formation of cholesterylester from cholesterol and long-chain fatty acyl-coenzymeA [1,2]. Human ACAT1 cDNA K1 was firstly cloned andfunctionally expressed in 1993 [3]. Further studies withspecific anti-ACAT1 antibody (DM10) illustrated that onemajor 50 kD ACAT1 protein was expressed in various…     

Structure and function of interleukin-17 family cytokines

The recently identified interleukin-17 (IL-17) cytokines family, which comprises six members in mammals (IL-17A-F), plays essential roles in the host immunity against infectious diseases and chronic inflammatory diseases. The three-dimensional structures containing IL-17A or IL-17F have become available and revealed the unique structural features of IL-17s as well as their receptors. Molecular modeling in this review shows that IL-17s may adopt a “cysteine knot” fold commonly seen in nerve growth factor (NGF) and other neurotrophins. Further modeling analysis unmasks a signature interaction feature of the IL-17F/IL-17RA complex, where a small loop of IL-17RA slots into the deep groove of the interface of IL-17F homodimer. This is quite different from the interaction between the best known four-helix cytokines and their cognate receptors. On the other hand, structure of IL-17A and its monoclonal antibody (CAT-2200) shows that, albeit that the antigenic epitope of IL-17A resides outside of the IL-17A homodimer interface, its physical proximity to the receptor binding groove may explain that antibody blockage would be achieved by interfering with the ligand-receptor interaction. This review is to summarize the advance in understanding the structure and function of IL-17 family cytokines, focusing mainly on IL-17A, IL-17F and IL-17E, in the hope of gaining better knowledge of immunotherapeutic strategies against various inflammatory diseases.     

过氧化氢驱动的细胞色素P450酶研究进展

细胞色素P450酶在自然界中广泛存在,能催化多种类型的氧化反应,在有机合成和生物化工方面具有重要的应用潜力。尽管大多数P450酶通常需要辅酶和复杂的电子传递体系协助活化氧分子,一些P450酶也可以利用过氧化氢作为末端氧化剂,这极大地简化了催化循环,为P450酶的合成应用提供了一条新的简便途径。本文系统地介绍了几类过氧化氢驱动的P450酶催化体系,包括脂肪酸羟化酶P450SPα和P450BSβ、脂肪酸脱羧酶P450OleTJE、人工改造的羟化酶P450BM3和P450cam突变体、以及基于底物误识别策略的P450-H2O2体系。通过分析催化反应机制,本文探讨了P450-H2O2催化体系在目前存在的挑战和可能的解决途径,并对其进一步应用前景进行了展望。     

巴西人参化学成分和药理活性研究进展

巴西人参原产于南美洲,当地人把它当做具有壮阳、增强体质等作用的草药。巴西人参已在我国广西、浙江等地引种栽培成功,现代研究发现,其主要含有三萜和三萜皂苷类、甾体类等多种化学成分,具有抗肿瘤、抗炎、保护胃黏膜等药理活性。本文通过对近年来巴西人参的研究情况进行综述,阐明已有的化学物质基础和药理作用,为其进一步的深入研究和开发提供理论依据。     

The role of gut microbiota in the gut-brain axis: current challenges and perspectives

Brain and the gastrointestinal (GI) tract are intimately connected to form a bidirectional neurohumoral communication system. The communication between gut and brain, knows as the gut-brain axis, is so well established that the functional status of gut is always related to the condition of brain. The researches on the gut-brain axis were traditionally focused on the psychological status affecting the function of the GI tract. However, recent evidences showed that gut microbiota communicates with the brain via the gut-brain axis to modulate brain development and behavioral phenotypes. These recent fi ndings on the new role of gut microbiota in the gut-brain axis implicate that gut microbiota could associate with brain functions as well as neurological diseases via the gut-brain axis. To elucidate the role of gut microbiota in the gut-brain axis, precise identification of the composition of microbes constituting gut microbiota is an essential step. However, identifi cation of microbes constituting gut microbiota has been the main technological challenge currently due to massive amount of intestinal microbes and the diffi culties in culture of gut microbes. Current methods for identifi cation of microbes constituting gut microbiota are dependent on omics analysis methods by using advanced high tech equipment. Here, we review the association of gut microbiota with the gut-brain axis, including the pros and cons of the current high throughput methods for identifi cation of microbes constituting gut microbiota to elucidate the role of gut microbiota in the gut-brain axis.     

The complete nucleotide sequence of the mitochondrial genome of the cabbage butterfly,Artogeia melete （Lepidoptera： Pieridae）

The complete mitochondrial genome （mitogenome） of Artogeia melete was determined as being composed of 15,140 bp, including 13 protein-coding genes （PCGs）, 2 rRNA genes, 22 tRNA genes, and one control region. The gene order of A. melete mitogenome is typical of Lepidoptera and differs from the insect ancestral type in the location of trnM. The A. melete mitogenome has a total of 119 bp of intergenic spacer sequences spread over 10 regions, ranging in sizes between 1 and 48 bp. The nucleotide composition of the A. melete mitogenome is also biased toward A ＋ T nucleotides （79.77%）, which is higher than that of Ochrogaster lunifer （77.84%）, but lower than nine other lepidopterans sequenced. The PCGs have typical mitochondrial start codons, except for coxl, which contains the unusual CGA. The coxl, cox2, nad2, and nad5 genes of the A. melete mitogenome have incomplete stop codons （T）. The A. melete A ＋ T-rich region contains some conserved structures that are similar to those found in other lepidopteran mitogenomes, including a structure combining the motif ‘ATAGA＇, a 19-bp poly（T） stretch, a microsatellite （AT）n element, and a 9-bp poly（A） upstream trnM. The A. melete mitogenome contains a duplicated 36-bp repeat element, which consists of a 26- bp core sequence flanked by 10-bp perfectly inverted repeats.     

两例事故受照者染色体畸变分析及生物剂量估算

应用外周血淋巴细胞染色体畸变和CB微核分析方法,对2000年河南许昌“3.06”60Co辐射事故1例受照者(A)和2000年河南开封“6.26”辐射事故一例过量放射性核素内污染致γ射线照射受照者(B)的生物剂量进行估算。结果表明,“A”和“B”两例受照者依据双+环率估算的剂量分别为1.44Gy和0.15Gy,CB微核率估算的剂量分别为1.43Gy和0.22Gy,与用物理方法估算的剂量比较接近,亦与放射损伤的临床诊断一致。泊松分布检验证实,“A”偏离泊松分布,受到不均匀照射。提示染色体畸变和CB微核分析是非常可靠的生物计量估算方法。 Abstract:Biological doses were estimated by using the yields of dicentrics plus rings(dic+r) and cytokinesis-block micronuclei (CBMN) for two victims of the accident radiation occurred on Mar 6,2000 in the City of Xuchang(victim A),and Jun 26,2000 in the City of Kaifeng(victim B),Henan Province,respectively.The results indicated that the equvalent whole body doses based on the standard dose-response curves established by the analyses of dic+r and CBMN were estimated to be 1.44Gy and 1.43Gy(victim A),and 0.15Gy and 0.22Gy(victim B).These doses were very consistent with the mean doses calculated from physical measurement and conformable to the clinical dianosis.The dic+r aberrations of victim A did not accord with Poisson distribution.The analyses of chromosomal aberrations and CBMN are an extremely reliable method in biological dosimetry.The radiation which victim A was exposed to was heterogeneous.     

TRPC1 protects dopaminergic SH-SY5Y cells from MPP＋, salsolinol,and N-methyl-（R）-salsolinol-induced cytotoxicity

Neurotoxins and alterations in Ca2＋ homeostasis have been associated with Parkinson＇s disease （PD）, but the role of store-operated Ca2＋ entry channels is not well understood. Previous studies have shown the neurotoxicity of salsolinol and 1-methyl-4-phenylpyridinium ion on SH-SY5Y cells and cytoprotection induced by transient receptor potential protein 1 （TRPC1）. In the present study, N-methyl-（R）-salsolinol was tested for its cellular toxicity and effects on TRPC1 expression. MTT （3-（4,5-dimethylthiazol-2-yl）-2,5-dipbenyl- tetrazolium bromide） assays, DAPI （4＇,6-diamidino-2-pheny- lindole）, fluorescein isothiocyanate-Annexin-V/propidium iodide, western blot analysis, and JC-1 labeling revealed that the three indicated drugs could induce caspase-dependent, mitochondrial-mediated apoptosis. Exposure of SH-SY5Y cells to the indicated drugs resulted in a significant decrease in thapsigargin-mediated Ca2＋ influx and TRPC1 expression. Immnnocytochemistry experiments revealed that neurotoxins treatment induced TRPC1 translocation to the cytoplasm. Taken together, our results indicate that treatment with neurotoxins may alter Ca2＋ homeostasis and induce mitochondrial-mediated caspase-dependent cytotoxicity, an important characteristic of PD.