(2R,3R,4aS,6S,7S,8aS)-4a-Fluoro-8a-hydroxyperhydronaphthalene-2,3,6,7-te trayl tetraacetate

The title compound, C18H25FO9, exhibits a similar unit cell and packing to the alpha polymorph of axial 4a,8a-dihydroxyperhydronaphthalene-2,3,6,7-tetrayl tetraacetate. The carbonyl O atoms of two of the four acetate groups in the molecule are disordered over two sites with occupancy ratios of 0.59 (4):0.41 (4) and 0.57 (6):0.43 (6). Crystal packing is effected via intermolecular O-H center dot center dot center dot O hydrogen bonds, which link the tetraacetate molecules into tapes along the c axis.

Synthesis and reactivity of chiral tellurium azomethines: Pseudopolymorphism of [o-((((1S,2R)-2-hydroxy-2-phenyl-1-methylethyl)amino)methinyl)phenyl] tellurium(IV) bromide

A range of novel chiral tellurium compounds having an azomethine functional group in the position ortho to tellurium has been synthesized by the reaction of the tellurium-containing aldehydes bis(o-formylphenyl) telluride (1) and o-(butyltelluro)benzaldehyde (4) with chiral amines (R)-(+)-(1-pheylethylamine) and (1R,2S)-(-)-norephedrine, respectively. The precursor aldehydes were prepared by using a reported procedure with slight but advantageous modifications. During the preparation of o-(butyltelluro)benzaldehyde, interesting side products, namely bis(o-formylphenyl) ditelluride ethylene acetal 5, bis(o-formylphenyl) tritelluride (6), and bis(o-formylphenyl) ditelluride (7) were isolated in moderate yields. The ditelluride 7 has been characterized by single-crystal X-ray diffraction studies. The liquid Schiff bases 10 and 11 were further characterized by derivatizing with liquid bromine. The title compound was obtained in excellent yield by reacting the Schiff base 11 with elemental bromine. Detailed NMR studies indicated the presence of a rigid environment for the hydroxyl group. Single-crystal X-ray determinations of the crystals obtained from the different batches indicated. the presence of the two pseudopolymorphic forms 13a and 13b, respectively. In the case of 13a there is one molecule of CH3CN as solvent of crystallization, whereas in 13b half a molecule of CH3CN per molecule of the title compound lies along the 2-fold axis. In 13a the hydroxyl hydrogen is hydrogen-bonded to the nitrogen of the solvent molecule, whereas in 13b it is hydrogen-bonded to the bromine of the neighboring molecule.

Glycodelin-A interferes with IL-2/IL-2R signalling to induce cell growth arrest, loss of effector functions and apoptosis in T-lymphocytes

The progesterone-regulated glycoprotein glycodelin-A (GdA), secreted by the decidualized endometrium at high concentrations in primates, inhibits the maternal immune response against fetal antigens and thereby contributes to the tolerance of the semi-allogenic fetus during a normal pregnancy. Our earlier studies demonstrated the ability of GdA to induce an intrinsic apoptotic cascade in CD4 T-lymphocytes and suppress the cytolytic effector function of CD8 T-lymphocytes. In this report, we investigated further into the mechanism of action of GdA controlling perforin and granzyme B expression in CD8 T-lymphocytes and the mechanism of action of GdA leading to lymphocyte death. Flow cytometry analysis was performed to check for the surface expression of interleukin-2 receptor (IL-2R) and intracellular eomesodermin (Eomes) in activated T-lymphocytes, whereas quantitative RTPCR analysis was used to find out their mRNA profile upon GdA treatment. Western analysis was carried out to confirm the protein level of Bax and Bcl-2. GdA reduces the surface expression of the high-affinity IL-2R complex by down-regulating the synthesis of IL-2R (CD25). This disturbs the optimal IL-2 signalling and decreases the Eomes expression, which along with IL-2 directly regulates perforin and granzymes expression. Consequently, the CD8 T-lymphocytes undergo growth arrest and are unable to mature into competent cytotoxic T-lymphocytes. In the CD4 T-lymphocytes, growth factor IL-2 deprivation leads to proliferation inhibition, decreased Bcl-2/enhanced Bax expression, culminating in mitochondrial stress and cell death. GdA spurs cell cycle arrest, loss of effector functions and apoptosis in different T-cell subsets by making T-lymphocytes unable to respond to IL-2.

冠心病患者血清中可溶性白介素2受体(SIL-2R)水平的观察

本工作用酶联免疫吸附试验双夹心法测定了26名冠心病人血清中可溶性白介素2受体（SIL－2R）的水平，同时用24名正常人及21名无动脉硬化的其他病人作对照。结果表明，冠心病人组的SIL－2R水平高于正常人组（P＜0．05），而无动脉硬化的其他病人组与正常人组之间则无差异。鉴于SIL－2R是T细胞被抗原激活后的产物，此结果说明病人体内有免疫应答增高的现象存在。提示这可能是冠心病发病机理中免疫损伤的部分内容，并提示临床防治冠心病时，除应纠正脂质代谢异常外，也要考虑对病人免疫状态的调正。

Efeito do extrato de Euterpe oleracea Mart.(Açaí) sobre a disfunção endotelial, estresse oxidativo e alterações vasculares e renais associados à hipertensão renovascular dois rins, 1 clip (2R,1C)

Estudos recentes mostram que o açaí é rico em polifenóis e uma dieta rica em polifenóis pode estar envolvida na proteção contra o risco cardiovascular. O objetivo deste estudo foi avaliar o efeito do tratamento crônico de animais hipertensos 2R,1C com extrato hidroalcoólico do caroço do açaí (ASE) sobre o desenvolvimento da hipertensão e disfunção endotelial; estresse oxidativo e sobre as alterações vasculares e renais. Ratos Wistar machos foram utilizados para obtenção da hipertensão renovascular 2R,1C e ratos controles 2R (sham) foram somente submetidos à laparotomia e receberam tratamento diário com veículo ou ASE (200 mg/Kg/dia) durante 40 dias. A pressão arterial sistólica (PAS) foi aferida por pletismografia de cauda e os efeitos vasodilatadores da acetilcolina (ACh) e nitroglicerina (NG) foram estudados em leito arterial mesentérico (LAM) perfundido e pré-contraído com norepinefrina. A atividade das enzimas SOD, CAT, GPx, os níveis de MDA, a carbonilação de proteínas e os níveis de nitrito foram avaliados por espectrofotometria. As expressões de enzimas pró e antioxidantes foram avaliadas por western blot. A atividade de MMP-2 foi avaliada por zimografia. Os níveis séricos de creatinina foram avaliados através de kit, por espectrofotometria. As alterações vasculares e renais foram avaliadas por microscopia de luz. A PAS foi maior nos animais 2R,1C, e o tratamento com ASE preveniu o desenvolvimento da hipertensão. O efeito vasodilatador reduzido da ACh em animais 2R,1C foi recuperado pelo ASE. O efeito vasodilatador da NG não foi diferente entre os grupos. O dano oxidativo avaliado pela peroxidação lipídica e carbonilação de proteínas foi maior nos animais 2R,1C, e reduzido pelo tratamento com ASE. As atividades da SOD, CAT e GPx foram menores em amostras de mesentério, plasma, rim e coração de animais 2R,1C e o tratamento com ASE aumentou estas atividades. A produção de NO foi menor no plasma, mesentério e rim dos animais 2R,1C, e o tratamento com ASE aumentou a produção de NO somente no rim e mesentério destes animais. A expressão de SOD-1, 2, eNOS e TIMP-1 foram menores nos animais 2R,1C e o tratamento com ASE aumentou a expressão destas enzimas. A expressão de NOX-4 e MMP-2 e a atividade de MMP-2 foram maiores nos animais 2R,1C e o tratamento com ASE reduziu a expressão destas enzimas e a atividade de MMP-2. Os animais 2R,1C apresentaram um aumento na espessura da camada média da aorta e artéria mesentérica e um aumento na relação média/lúmen da aorta, e estas alterações foram prevenidas pelo ASE. Os níveis séricos aumentados de creatinina nos animais 2R,1C foram reduzidos por ASE. As alterações morfológicas renais nos animais 2R,1C foram prevenidas pelo ASE. Portanto, o tratamento com ASE previne o desenvolvimento da hipertensão, melhora a disfunção endotelial e previne as alterações vasculares e renais em ratos 2R,1C. A redução da atividade antioxidante e o aumento na peroxidação lipídica e carbonilação de proteínas sugerem o envolvimento de um mecanismo deficiente da defesa antioxidante e de um dano oxidativo aumentado, os quais foram revertidos pelo ASE.

树鼩IL-2Rα(CD25)基因的分离、鉴定及表达分析

3%～66.4%.RT-PCR检测发现,tsCD25 mRNA分布于树鼩的外周血、脾脏和肺,并受PMA 和 ionomycin 刺激的调节.我们的结果为下一步制备tsCD25单克隆抗体,抑制CD4+CD25+Tregs功能以及开展有关的研究工作奠定了基础.

Stereoselective coordination chemistry of the tetradentate chelating ligand (2R,3R)-bis(2,2 '-dipyridyl-5-methoxyl) butane

The enantiomerically pure ligand L-3RR (2R, 3R)-bis(2,2'-dipyridyl-5-methoxyl) butane has been synthesised by linking two 2,2'-bipyridine units with (2R, 3R)-butandiol. The reaction of L-3RR with Zn(II) afforded a mononuclear species and the H-1 NMR spectroscopy points to a C-1 symmetry, expected for a distorted trigonal bipyramidal coordination environment. These observations were confirmed by MM2 calculations and electrospray mass spectrometry. The reaction of L-3RR with iron(II) indicated the formation of a dinuclear species by mass spectrometry. Solution state CD spectroscopy indicates that both complexes adopt a Lambda-configuration, implying a single stranded dinuclear iron(II) complex is present rather than the anticipated triple helical architecture.

CD69, CD25, and HLA-DR activation antigen expression on CD3+ lymphocytes and relationship to serum TNF-alpha, IFN-gamma, and sIL-2R levels in aging

Aging is associated with changes in lymphocyte subsets and unexplained HLA-DR upregulation on T-lymphocytes. We further investigated this activation, by measuring early (CD69), middle (CD25), and late (HLA-DR) T-lymphocyte activation markers on CD3+ lymphocytes, across subjects (20-100 years) together with serum tumor necrosis factor (TNF-alpha), interferon-gamma (IFN-gamma), and soluble interleukin-2 receptor (sIL-2R). HLA-DR was present as a CD3+ HLA-DR+ subset that constituted 8% of total lymphocytes, increased twofold with age and included CD4+, CD8+, and CD45RA+ phenotypes. HLA-DR was also expressed on a CD8+ CD57+ subset. The CD3+ CD25+ subset constituted 13% of lymphocytes, fell with age but was weakly associated with the CD3+ HLA-DR+ subset especially in older subjects. A small 3-5% CD3+ CD69+ subsets showed no age effect. Serum sIL-2R, TNF-alpha, but not IFN-gamma, were associated with CD3+ HLA-DR+ lymphocytes, TNF-alpha with CD8+ CD57+ count and sIL-2R and IFN-gamma with the CD3+ CD25+/CD3+ CD4+ ratio. The study confirms age-related upregulation of HLA-DR on CD3+ lymphocytes, shows some evidence for associated upregulation of CD25 on CD3+ cells in older subjects, and links serum TNF-alpha, IFN-gamma, and sIL2-R to T-lymphocyte activation.

Three rounds (1R/2R/3R) of genome duplications and the evolution of the glycolytic pathway in vertebrates

Affiliation: Henner Brinkmann : Département de biochimie, Faculté de médecine, Université de Montreal