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1.
研究中枢神经介素U(NMU)受体2(NMU2R)与黑皮质激素(MC)受体途径(MCR3/4)在调节摄食行为和能量平衡方面的相互作用关系.对禁食或不禁食大鼠脑室注射NMU2R内源性配体NMU和MCR3/4信号途径高亲和力拮抗剂SHU9119,通过测定不同时间点大鼠摄食量和体重变化,探讨中枢NMU2R和黑皮质素受体途径在调节动物摄食行为上的作用及其相互关系.脑室注射NMU对大鼠食欲有显著抑制作用;在同时注射NMU和SHU9119的情况下,NMU2R对大鼠的这种食欲抑制作用会部分受到MCR3/4信号途径变化的影响;同样,对SHU9119前处理大鼠脑内注射NMU,NMU2R抑制食欲的作用也会明显降低,其在摄食方面的作用被部分抑制.结果提示,NMU能够有效的调节摄食行为,而且这种在摄食行为上的调控作用可能部分受MC受体途径介导.  相似文献   

2.
Peppiatt CM  Howarth C  Mobbs P  Attwell D 《Nature》2006,443(7112):700-704
Neural activity increases local blood flow in the central nervous system (CNS), which is the basis of BOLD (blood oxygen level dependent) and PET (positron emission tomography) functional imaging techniques. Blood flow is assumed to be regulated by precapillary arterioles, because capillaries lack smooth muscle. However, most (65%) noradrenergic innervation of CNS blood vessels terminates near capillaries rather than arterioles, and in muscle and brain a dilatory signal propagates from vessels near metabolically active cells to precapillary arterioles, suggesting that blood flow control is initiated in capillaries. Pericytes, which are apposed to CNS capillaries and contain contractile proteins, could initiate such signalling. Here we show that pericytes can control capillary diameter in whole retina and cerebellar slices. Electrical stimulation of retinal pericytes evoked a localized capillary constriction, which propagated at approximately 2 microm s(-1) to constrict distant pericytes. Superfused ATP in retina or noradrenaline in cerebellum resulted in constriction of capillaries by pericytes, and glutamate reversed the constriction produced by noradrenaline. Electrical stimulation or puffing GABA (gamma-amino butyric acid) receptor blockers in the inner retina also evoked pericyte constriction. In simulated ischaemia, some pericytes constricted capillaries. Pericytes are probably modulators of blood flow in response to changes in neural activity, which may contribute to functional imaging signals and to CNS vascular disease.  相似文献   

3.
Calcium release from the endoplasmic reticulum controls a number of cellular processes, including proliferation and contraction of smooth muscle and other cells. Calcium release from inositol 1,4,5-trisphosphate (IP3)-sensitive stores is negatively regulated by binding of calmodulin to the IP3 receptor (IP3R) and the NO/cGMP/cGMP kinase I (cGKI) signalling pathway. Activation of cGKI decreases IP3-stimulated elevations in intracellular calcium, induces smooth muscle relaxation and contributes to the antiproliferative and pro-apoptotic effects of NO/cGMP. Here we show that, in microsomal smooth muscle membranes, cGKIbeta phosphorylated the IP3R and cGKIbeta, and a protein of relative molecular mass 125,000 which we now identify as the IP3R-associated cGMP kinase substrate (IRAG). These proteins were co-immunoprecipitated by antibodies directed against cGKI, IP3R or IRAG. IRAG was found in many tissues including aorta, trachea and uterus, and was localized perinuclearly after heterologous expression in COS-7 cells. Bradykinin-stimulated calcium release was not affected by the expression of either IRAG or cGKIbeta, which we tested in the absence and presence of cGMP. However, calcium release was inhibited after co-expression of IRAG and cGKIbeta in the presence of cGMP. These results identify IRAG as an essential NO/cGKI-dependent regulator of IP3-induced calcium release.  相似文献   

4.
Cytokines are important in the regulation of haematopoiesis and immune responses, and can influence lymphocyte development. Here we have identified a class I cytokine receptor that is selectively expressed in lymphoid tissues and is capable of signal transduction. The full-length receptor was expressed in BaF3 cells, which created a functional assay for ligand detection and cloning. Conditioned media from activated human CD3+ T cells supported proliferation of the assay cell line. We constructed a complementary DNA expression library from activated human CD3+ T cells, and identified a cytokine with a four-helix-bundle structure using functional cloning. This cytokine is most closely related to IL2 and IL15, and has been designated IL21 with the receptor designated IL21 R. In vitro assays suggest that IL21 has a role in the proliferation and maturation of natural killer (NK) cell populations from bone marrow, in the proliferation of mature B-cell populations co-stimulated with anti-CD40, and in the proliferation of T cells co-stimulated with anti-CD3.  相似文献   

5.
The P2X 7 receptor (P2X7R) is an important member of the P2X family of ligand-gated ion channels that respond to ATP as the endogenous agonist. Studies suggest that P2X7R plays a potentially pivotal role in a variety of physiological functions, including peripheral and central neuronal transmission, smooth muscle contraction, and inflammation. Thus, P2X7R may be a potential target for drug development. Here, we used a FlexStation to examine the function of recombinant P2X7R stably expressed in human embryonic kidney 293 cells and to compare three high-throughput screening assays: a membrane potential assay, an ethidium bromide uptake assay, and a calcium influx assay. We found that all three assays were suitable for the analysis of P2X7R, but the calcium influx assay was the most robust and is the best choice as a first high-throughput screening assay when embarking on a P2X7R drug discovery project.  相似文献   

6.
甲状旁腺激素(PTH)与动物钙稳态调控和骨代谢平衡相关,其生理作用是通过甲状旁腺激素受体(PTHR)介导。甲状旁腺激素受体家族包括三个不同的亚型,其中甲状旁腺激素3型受体(PTH3R)在非哺乳类脊椎动物生长发育过程中起着重要作用,然而PTH3R在鸟类中的研究则相对较少。 本研究采用RT-PCR方法,首先克隆了珍珠鸟和家鸡的PTH3R基因全长cDNA序列。结果显示,家鸡PTH3R (cPTH3R) cDNA全长1632 bp,编码543个氨基酸,珍珠鸟PTH3R(zPTH3R-w) cDNA序列全长1563 bp,编码520个氨基酸,其蛋白均含有信号肽序列、七次跨膜区等特征性结构。此外,在珍珠鸟中还发现一个新剪接变体zPTH3R-v1,其cDNA序列全长1468 bp,编码488个氨基酸,其缺失了第3外显子进而导致第1跨膜结构域缺失。利用生物信息学方法,我们还对珍珠鸟和家鸡PTH3R蛋白序列进行三维建模。 采用RT-PCR方法,本研究也对珍珠鸟PTH3R基因进行组织表达分析。结果显示,zPTH3R及其剪切变体zPTH3R-v1在珍珠鸟脑及外周组织中广泛表达。珍珠鸟和家鸡PTH3R基因的成功克隆与结构解析,将为下一步开展PTH3R在鸟类中的功能研究奠定重要基础。  相似文献   

7.
Cloning and expression analysis of human reticulon 4c cDNA   总被引:2,自引:0,他引:2  
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8.
Characterization of the human cysteinyl leukotriene CysLT1 receptor.   总被引:29,自引:0,他引:29  
The cysteinyl leukotrienes-leukotriene C4(LTC4), leukotriene D4(LTD4) and leukotriene E4(LTE4)-are important mediators of human bronchial asthma. Pharmacological studies have determined that cysteinyl leukotrienes activate at least two receptors, designated CysLT1 and CysLT2. The CysLT1-selective antagonists, such as montelukast (Singulair), zafirlukast (Accolate) and pranlukast (Onon), are important in the treatment of asthma. Previous biochemical characterization of CysLT1 antagonists and the CysLT1 receptor has been in membrane preparations from tissues enriched for this receptor. Here we report the molecular and pharmacological characterization of the cloned human CysLT1 receptor. We describe the functional activation (calcium mobilization) of this receptor by LTD4 and LTC4, and competition for radiolabelled LTD4 binding to this receptor by the cysteinyl leukotrienes and three structurally distinct classes of CysLT1-receptor antagonists. We detected CysLT1-receptor messenger RNA in spleen, peripheral blood leukocytes and lung. In normal human lung, expression of the CysLT1-receptor mRNA was confined to smooth muscle cells and tissue macrophages. Finally, we mapped the human CysLT1-receptor gene to the X chromosome.  相似文献   

9.
T Sakurai  M Yanagisawa  Y Takuwa  H Miyazaki  S Kimura  K Goto  T Masaki 《Nature》1990,348(6303):732-735
Endothelin-1 was initially identified as a 21-residue potent vasoconstrictor peptide produced by vascular endothelial cells, but was subsequently found to have many effects on both vascular and non-vascular tissues. The discovery of three isopeptides of the endothelin family, ET-1, ET-2 and ET-3, each possessing a diverse set of pharmacological activities of different potency, suggested the existence of several different endothelin receptor subtypes. Endothelins may elicit biological responses by various signal-transduction mechanisms, including the G protein-coupled activation of phospholipase C and the activation of voltage-dependent Ca2+ channels. Thus, different subtypes of the endothelin receptor may use different signal-transduction mechanisms. Here we report the cloning of a complementary DNA encoding one subtype belonging to the superfamily of G protein-coupled receptors. COS-7 cells transfected with the cDNA express specific and high-affinity binding sites for endothelins, responding to binding by the production of inositol phosphates and a transient increase in the concentration of intracellular free Ca2+. The three endothelin isopeptides are roughly equipotent in displacing 125I-labelled ET-1 binding and causing Ca2+ mobilization. A messenger RNA corresponding to the cDNA is detected in many rat tissues including the brain, kidney and lung but not in vascular smooth muscle cells. These results indicate that this cDNA encodes a 'nonselective' subtype of the receptor which is different from the vascular smooth muscle receptor.  相似文献   

10.
同时分离和培养兔外周血平滑肌祖细胞(SPC)和内皮祖细胞(EPC),为组织工程膀胱的构建和血管化提供种子细胞.分离新西兰兔外周血中的单个核细胞,分别进行SPC和EPC的分离和培养;同时,培养兔膀胱平滑肌细胞(BSMC)作为对照.细胞爬片,观察细胞摄取Dil-AcLDL和结合FITC-UEA-1的能力;间接免疫荧光染色观察平滑肌肌动蛋白(SMA)、结蛋白(Desmin)、KDR、eNOS和vWF的表达情况;进行细胞增殖实验,观察PDGF-BB,VEGF对SPC和EPC的增殖作用.结果发现,培养1周后出现SPC克隆和EPC克隆,SPC呈梭形,长短不一;EPC形态均一,呈典型的鹅卵石形;培养的BSMC形态均一,为长梭形,呈峰谷样形态.利用克隆环分离SPC和EPC克隆,继续培养可得到高纯度的SPC和EPC.SPC不摄取Dil-AcLDL,不结合FITC-UEA-1;SPC表达SMA、Desmin和KDR,不表达eNOS和vWF.EPC同时摄取Dil-AcLDL和结合FITC-UEA-1;EPC表达eNOS、vWF和KDR,不表达SMA和Desmin.BSMC仅表达SMA和Desmin.PDGF-BB仅能促进SPC增殖...  相似文献   

11.
R T Jensen  S W Jones  K Folkers  J D Gardner 《Nature》1984,309(5963):61-63
The tetradecapeptide bombesin was originally isolated from frog skin. Bombesin-like peptides have since been detected in mammalian gastrointestinal tract, brain and lung. These peptides have potent pharmacological effects on the central nervous system; they cause contraction of intestinal, uterine and urinary tract smooth muscle; and stimulate the release of other peptides including gastrin, cholecystokinin, motilin, pancreatic polypeptide, neurotensin, insulin, enteroglucagon, prolactin and growth hormone. Specific plasma membrane receptors for bombesin have been demonstrated on pancreatic acinar cells, brain membranes and pituitary cells. Studies defining the physiological importance of bombesin have been impeded by the lack of a bombesin receptor antagonist. Here we describe experiments which demonstrate that a peptide originally described as a substance P receptor antagonist, [D-Arg, D-Pro, D-Trp, Leu ]substance P, is also a bombesin receptor antagonist. This peptide competitively inhibits the ability of bombesin to stimulate enzyme secretion from dispersed pancreatic acini, and also inhibits the action of other peptides that interact with the bombesin receptor.  相似文献   

12.
A major impediment in the treatment of neurological diseases is the presence of the blood-brain barrier, which precludes the entry of therapeutic molecules from blood to brain. Here we show that a short peptide derived from rabies virus glycoprotein (RVG) enables the transvascular delivery of small interfering RNA (siRNA) to the brain. This 29-amino-acid peptide specifically binds to the acetylcholine receptor expressed by neuronal cells. To enable siRNA binding, a chimaeric peptide was synthesized by adding nonamer arginine residues at the carboxy terminus of RVG. This RVG-9R peptide was able to bind and transduce siRNA to neuronal cells in vitro, resulting in efficient gene silencing. After intravenous injection into mice, RVG-9R delivered siRNA to the neuronal cells, resulting in specific gene silencing within the brain. Furthermore, intravenous treatment with RVG-9R-bound antiviral siRNA afforded robust protection against fatal viral encephalitis in mice. Repeated administration of RVG-9R-bound siRNA did not induce inflammatory cytokines or anti-peptide antibodies. Thus, RVG-9R provides a safe and noninvasive approach for the delivery of siRNA and potentially other therapeutic molecules across the blood-brain barrier.  相似文献   

13.
Presence of Ti (WT31) negative T lymphocytes in normal blood and thymus   总被引:43,自引:0,他引:43  
L L Lanier  A Weiss 《Nature》1986,324(6094):268-270
The antigen receptor expressed on most T lymphocytes is a disulphide-linked heterodimer (Ti) that is composed of alpha-chain and beta-chain subunits. On the surface of human T lymphocytes, Ti is non-covalently associated with three invariant proteins, designated CD3-gamma, -delta, and -epsilon. It has been suggested that Ti is obligatory for CD3 expression. But a T leukaemia cell line, IL-2 (interleukin 2) dependent T-cell clones established from fetal blood and IL-2 dependent cell lines established from immunodeficiency patients with bare lymphocyte syndrome and ectodermal dysplasia syndrome have recently been shown to express CD3, but not Ti (detected due to monoclonal antibody WT31). These lymphocytes may express the product of the T-cell antigen receptor gamma (TCR-gamma) gene, rather than the alpha/beta heterodimer, in association with CD3. Preliminary studies suggested that T cells expressing CD3 but lacking Ti are present in low frequency in normal lymphoid tissues. Here we show that in normal blood and thymus CD3+, WT31-T cells express neither CD4 nor CD8. The low frequency (less than 0.2-0.9% of total thymocytes) of CD3+, WT31- cells in the thymus suggests that this population does not represent a major stage of thymic development and may be a distinct lineage of T cells.  相似文献   

14.
Met-enkephalin circulates in human plasma   总被引:7,自引:0,他引:7  
V Clement-Jones  P J Lowry  L H Rees  G M Besser 《Nature》1980,283(5744):295-297
The physiological roles of Met-enkephalin and Leu-enkephalin are still unknown. They may act as neurotransmitters in the central and peripheral nervous systems. Met-enkephalin has been detected in several species in a variety of tissues including brain, spinal cord and gut using bioassays, opiate receptor assays and radioimmunoassays (RIA). It has also been detected in human gut immunocytochemically and in human brain and cerebrospinal fluid by opiate receptor assay and RIA. However, all reported assays show some degree of cross-reaction with Leu-enkephalin and unequivocal differentiation between the two enkephalins and the larger endorphins has not always been possible. Thus the existence of Met-enkephalin in human tissues and fluids remains in doubt. Using a highly specific RIA, we have now obtained evidence that Met-enkephalin-like material circulates in the plasma of normal subjects and may be secreted by the adrenal gland. Chromatographically the material exists in plasma mainly as the intact pentapeptide and not as the biologically inactive degradation product Gly-Gly-Phe-Met as would be expected from metabolic studies.  相似文献   

15.
Interleukin-2 (IL-2) has a key role in the antigen-specific clonal growth of T lymphocytes, by virtue of its interaction with a specific cell-surface receptor (IL-2R). The growth signal seems to be delivered by IL-2 bound to the high-affinity, but not the low-affinity, receptor. Genes encoding IL-2 and its receptor (that is, Tac-antigen) have been cloned and analysed in detail. We have now achieved cell-type-specific reconstitution of the high-affinity human IL-2R by expressing the complementary DNA cloned from normal lymphocytes. A mouse T-lymphocytic line, EL-4, expressed human IL-2R with high (dissociation constant (Kd) = 160-220 pM) and low (Kd = 2.1-2.2 nM) affinity for recombinant human IL-2, while mouse L929 cells expressed only a single class of the IL-2R with lower affinity (Kd = 34.5 nM) for the ligand. We also show that the human IL-2R expressed in EL-4 cells responds to IL-2 and mediates reversed signal transduction: growth of the EL-4 cells harbouring the IL-2R is inhibited specifically by human recombinant IL-2. The approach described here may provide a general experimental framework for elucidating the molecular basis of signal transduction mediated by specific receptor-ligand interaction.  相似文献   

16.
F L Kidd  J T Isaac 《Nature》1999,400(6744):569-573
Most of the fast excitatory synaptic transmission in the mammalian brain is mediated by ionotrophic glutamate receptors, of which there are three subtypes: AMPA (alpha-amino-3-hydroxyl-5-methyl-4-isoxazolepropionate), NMDA (N-methyl-D-aspartate) and kainate. Although kainate-receptor subunits (GluR5-7, KA1 and 2) are widely expressed in the mammalian central nervous system, little is known about their function. The development of pharmacological agents that distinguish between AMPA and kainate receptors has now allowed the functions of kainate receptors to be investigated. The modulation of synaptic transmission by kainate receptors and their synaptic activation in a variety of brain regions have been reported. The expression of kainate receptor subunits is developmentally regulated but their role in plasticity and development is unknown. Here we show that developing thalamocortical synapses express postsynaptic kainate receptors as well as AMPA receptors; however, the two receptor subtypes do not colocalize. During the critical period for experience-dependent plasticity, the kainate-receptor contribution to transmission decreases; a similar decrease occurs when long-term potentiation is induced in vitro. This indicates that during development there is activity-dependent regulation of the expression of kainate receptors at thalamocortical synapses.  相似文献   

17.
18.
芦丁镉金属配合物经耳脉静脉注射家兔,观察其血压变化;制备离体主动脉平滑肌条,将其固定在灌流肌槽中,记录离体主动脉平滑肌条张力的变化。观察芦丁镉对家兔动脉血压的影响以及对去甲肾上腺素(NA)诱发的离体主动脉肌条收缩的影响。结果表明,静脉注射芦丁镉可引起动脉血压的降低(P<0.05);而在灌流槽中单独加入芦丁镉时不能观察到离体血管紧张性的改变,但是在NA作用的基础上再加入芦丁镉后,便可使离体血管收缩效应减弱(P<0.05)。因此,芦丁合镉金属配合物具有降低血压和抑制NA引起的血管的收缩效应。  相似文献   

19.
Expression of functional sodium channels from cloned cDNA   总被引:7,自引:0,他引:7  
M Noda  T Ikeda  H Suzuki  H Takeshima  T Takahashi  M Kuno  S Numa 《Nature》1986,322(6082):826-828
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20.
披针叶黄华生物碱及其生物活性   总被引:11,自引:3,他引:8  
披针叶黄华含有双稠哌喧类生物碱,从其总生物碱中提取分离出10种双稠哌啶类生物碱,它们分别属于三种结构类型:(1)臭豆碱类型;(2)鹰爪豆碱类型;(3)羽扇豆碱类型,其中五种生物碱已进行过生物活性测试,它们对细菌、昆虫、线虫以及哺乳类动物有多种生理和药理活性,其总碱对试验动物产生肌肉松弛、降低血压、以及减慢心律等作用。  相似文献   

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