从噬菌体展示随机12肽库中筛选与IRS-1PH结构域相结合的多肽模体

将胰岛素受体底物-1(IRS-1)的PH结构域(pleckstrin homology domain)编码序列克隆到融合表达载体pRSETA中,阳性克隆经IPTG诱导,表达出氨基端带6个连续组氨酸残基的融合蛋白。经检测,表达的目的蛋白一部分以可溶形式存在。利用Ni-NTA金属螯合亲和层析法在非变性条件下对表达的目的蛋白进行纯化,纯度大于98％。将纯化的目的蛋白包被于聚苯乙烯平皿上作为靶蛋白,经过4轮淘筛,得到能够与IRS-1的PH结构域相结合的重组噬菌体克隆;从中随机挑选出50个克隆进行DNA序列测定,对获得的短肽序列进行了分析。并通过ELISA检测了这些克隆与IRS-1的PH结构域的结合活性。     

Mitogenomic phylogeny of the Percichthyidae and Centrarchiformes (Percomorphaceae): comparison with recent nuclear gene-based studies and simultaneous analysis

Delineation of the fish family Percichthyidae (Percomorphaceae) has a long and convoluted history, with recent morphological-based studies restricting species members to South American and Australian freshwater and catadromous temperate perches. Four recent nuclear gene-based phylogenetic studies, however, found that the Percichthyidae was not monophyletic and was nested within a newly discovered inter-familial clade of Percomorphaceae, the Centrarchiformes, which comprises the Centrarchidae and 12 other families. Here, we reexamined the systematics of the Percichthyidae and Centrarchiformes based on new mitogenomic information. Our mitogenomic results are globally congruent with the recent nuclear gene-based studies although the overall amount of phylogenetic signal of the mitogenome is lower. They do not support the monophyly of the Percichthyidae, because the catadromous genus Percalates is not exclusively related to the freshwater percichthyids. The Percichthyidae (minus Percalates) and Percalates belong to a larger clade, equivalent to the Centrarchiformes, but their respective sister groups are unresolved. Because all recent analyses recover a monophyletic Centrarchiformes but with substantially different intra-relationships, we performed a simultaneous analysis for a character set combining the mitogenome and 19 nuclear genes previously published, for 22 centrarchiform taxa. This analysis furthermore indicates that the Centrarchiformes are divided into three lineages and the superfamily Cirrhitoidea is monophyletic as well as the temperate and freshwater centrarchiform perch-like fishes. It also clarifies some of the relationships within the freshwater Percichthyidae.     

卵泡刺激素受体FSHR234纳米抗体的分离纯化及多克隆抗体的制备

【背景】卵泡刺激素受体(Follicle-stimulating hormone receptor,FSHR)在人体成熟破骨细胞及单核细胞表面表达,成为阻断卵泡刺激素(FSH)作用的潜在靶点,制备亲和力较高的FSHR抗体已成为靶向治疗FSH相关疾病的切入点。【目的】构建FSHR重组载体获得表达量较高的可溶性蛋白,进一步制备骆驼多克隆抗体及其纳米抗体。【方法】利用XhoⅠ和Bam HⅠ双酶切重组质粒p ET30a-FSHR234,将目的基因fshr构建于p GEX-4T-1载体并进行原核表达,利用Western blot及ELISA检测目的蛋白的配体结合能力。免疫新疆双峰驼制备骆驼多克隆抗体,并利用噬菌体展示技术筛选获得FSHR纳米抗体。细胞免疫化学法检测FSHR抗体在coav-3的表达情况。【结果】构建了pGEX-4T-1-FSHR234重组质粒,获得了表达量较高的FSHR234可溶性蛋白;并构建了5株FSHR纳米抗体,鉴定出一株结合能力较强的纳米抗体,命名为VHH-3F9。【结论】制备的骆驼FSHR多克隆抗体效价达1:128 000,筛选获得的VHH-3F9纳米抗体能与FSHR234具有较高的结合性,且两者均能表达于coav-3细胞表面。     

植物转录抑制子的结构特征及其作用机理

转录因子依转录调控能力可分为激活子和抑制子。植物转录抑制蛋白的分类依据很多,从作用方式上可分为主动抑制子和被动抑制子两大类：根据与DNA结合的方式则可分为锌指类、MYB类、AP2／EREBP类、bHLH类和bZlP类等。植物主动抑制子通过其含有的抑制域对转录直接起抑制作用。抑制域又可分很多类,但多数为含有类似EAR基序的保守性基序,其上具有几个保守性亮氨酸残基。植物转录抑制子主要通过对激活子或基本转录复合物产生作用及改变染色体结构3种方式来抑制目标基因的转录。有关植物转录抑制子的研究虽很欠缺,但以拟南芥SUPERMAN等抑制子的EAR基序为代表的研究表明,抑制域是阐明植物转录抑制子功能和下游基因表达调控机理的核心对象,而融合抑制子沉默技术（CRES-T）也为人为调控基因沉默带来了新的技术手段。     

siRNA介导的NFBD1表达沉默对HeLa细胞增殖与凋亡的影响

NFBD1,也称MDC1,是1个参与细胞内DNA损伤后细胞应答反应的重要分子．为探讨NFBD1在细胞增殖和凋亡中的作用及其作为分子靶点用于肿瘤治疗的潜在价值,本研究采用siRNA技术抑制NFBD1的表达,并观察了其对人宫颈癌细胞HeLa细胞增殖和细胞凋亡的影响．半定量RT-PCR和蛋白质印迹分析结果表明,筛选到的短链NFBD1 siRNA能有效抑制内源NFBD1的表达,抑制程度约100％．细胞生长曲线分析结果表明,siRNA介导的NFBD1表达沉默导致HeLa细胞生长增殖的显著抑制．FACS分析结果表明,NFBD1表达抑制导致sub-G₁峰的出现,同时蛋白质印迹分析观察到了caspase 3和PARP（poly-ADP-ribose polymerase）的剪接激活,表明NFBD1表达抑制诱发了细胞凋亡．在该凋亡过程中,P-53及其下游靶分子Bax和Puma的表达水平均没有发生明显变化,但Noxa的表达在mRNA和蛋白质水平上均显著上调,强烈提示该凋亡过程很可能是1个不依赖P53的凋亡途径,且Noxa的转录激活在该凋亡过程中可能起着重要作用．这些结果表明,NFBD1参与细胞生长增殖和凋亡的调节,是一个潜在的肿瘤治疗新靶点．     

颗粒裂解肽G13结构域的重组表达及蛋白质结构预测

基因工程构建表达是获得抗菌肽的一种成本较低的方法,本实验人工合成G13结构域编码DNA序列,PCR扩增后,用T-A克隆法与pBAD/TOPO ThioFusion表达载体连接,通过PCR鉴定筛选出正确重组质粒,在大肠杆菌Top10中对目的蛋白进行表达,大肠杆菌工程菌经阿拉伯糖诱导后取样,用SDS-PAGE检测表达情况,采用生物信息学方法对表达蛋白的结构特征进行模拟分析。结果显示：目的蛋白在原核系统中实现了高效表达,表达量高达67%以上,主要以包涵体形式表达。蛋白结构预测结果显示,目的蛋白原有的α螺旋活性结构无改变,从而为抗菌肽高效生产提供了有效可靠的研究途径。     

Lipid droplet proteins and metabolic diseases

Lipid droplets (LDs) are ubiquitous cellular organelles for lipid storage which are composed of a neutral lipid core bounded by a protein decorated phospholipid monolayer. Although lipid storage is their most obvious function, LDs are far from inert as they participate in maintaining lipid homeostasis through lipid synthesis, metabolism, and transportation. Furthermore, they are involved in cell signaling and other molecular events closely associated with human disease such as dyslipidemia, obesity, lipodystrophy, diabetes, fatty liver, atherosclerosis, and others. The last decade has seen a great increase in the attention paid to LD biology. Regardless, many fundamental features of LD biology remain obscure. In this review, we will discuss key aspects of LD biology including their biogenesis, growth and regression. We will also summarize the current knowledge about the role LDs play in human disease, especially from the perspective of the dynamics of the associated proteins. This article is part of a Special issue entitled Cardiac adaptations to obesity, diabetes and insulin resistance, edited by Professors Jan F.C. Glatz, Jason R.B. Dyck and Christine Des Rosiers.