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1、Biochemistry of Hormones12第一節(jié) 概 述 一、細胞間信息傳遞到類型:內(nèi)分泌(遠距分泌)神經(jīng)分泌神經(jīng)內(nèi)分泌自身分泌外分泌:外激素3Communication by extracellular signals usually involves the following steps: Synthesis and release of the signaling molecule by the signaling cell;Transport of the signal to the target cell; Binding of the signal by a speci
2、fic receptor protein leading to its activation; Initiation of one or more intracellular signal-transduction pathways by the activated receptor; Specific changes in cellular function, metabolism, or development; Removal of the signal, which often terminates the cellular response.4Signaling Molecules
3、in Animals Operateover Various Distances5Cellular communication by means of cellular secretions6Patterns of Signaling Endocrine Paracrine Autocrine7激素作用的特點信使作用相對特異性高效放大作用(nM、pM級)激素間相互作用:協(xié)同、拮抗、允許8含氮激素 1. 蛋白質(zhì)和肽類激素 2. 氨基酸衍生物類固醇激素脂肪酸衍生物二、激素的分類根據(jù)化學性質(zhì)9松果體激素丘腦下部激素垂體前葉激素垂體后葉激素性腺和胎盤激素局部激素外激素根據(jù)產(chǎn)生部位10三、激素的合成、分
4、泌、轉(zhuǎn)運行代謝激素的合成11激素的分泌1213激素的轉(zhuǎn)運游離型結(jié)合型細胞內(nèi)降解與葡萄糖醛酸或硫酸結(jié)合而排出激素的代謝14四、激素的作用及其機制促進生長和發(fā)育保證生殖控制細胞外液的穩(wěn)態(tài)調(diào)節(jié)代謝過程調(diào)節(jié)消化活動參與應激和免疫反應激素的作用15 含氮激素的作用機制 類固醇激素的作用機制 甲狀腺激素的作用機制激素的作用機制16Receptors17受體的特性Receptor飽和性高親和力(affinity)強特異性信息傳遞作用上調(diào)(upregulation)/下調(diào)(downregulation)18Maximal Cellular Response toa Signaling Molecule May
5、 Not Require Activation ofAll Receptors19FIGURE 13-3 The maximal physiological response to many external signals occurs when only a fraction of the receptor molecules are occupied by ligand. In this situation, plots of the extent of ligand binding and of physiological response at different ligand co
6、ncentrations differ. Here 50% of the maximal physiological response is induced at a ligand concentration at which only 18% of the receptors are occupied. Likewise, 80% of the maximal response is induced when the ligand concentration equals the Kd value, at which 50% of the receptors are occupied.20S
7、ensitivity of a Cell to External Signals Is Determined by the Number of Surface Receptors21Binding Assays Are Used to Detect Receptors and Determine Their Kd Values22Shown here are data for insulin-specific receptors on the surface of liver cells. A suspension of cells is incubated for 1h at 4 with
8、increasing concentrations of 125I-labeled insulin. The amount of radioactivity bound to cells is measured. The total binding curve A represents insulin specifically bound to high-affinity receptors as well as insulin nonspecifically bound with low affinity to other molecules on the cell surface. The
9、 contribution of nonspecific binding to total binding is determined by repeating the binding assay in the presence of a 100-fold excess of unlabeled insulin, which saturates all the specific high-affinity sites. In this case, all the labeled insulin binds to nonspecific sites, yielding curve C. The
10、specific binding curve B is calculated as the difference between curves A and C.FIGURE 13-4 Binding assays for cell-surface receptors can determine the Kd for high-affinity ligands and the number of receptors per cell.23The synthetic ligand alprenolol, which binds with high affinity to the epinephri
11、ne receptor on liver cells (Kd 310-9M), is used to detect the binding of two low-affinity ligands, the natural hormone epinephrine (EP) and a synthetic ligand called isoproterenol (IP). Assays are performed with a constant amount of 3Halprenolol to which increasing amounts of unlabeled epinephrine o
12、r isoproterenol are added. In a plot of the inhibition of 3Halprenolol binding versus epinephrine or isoproterenol concentration the concentration of the competitor that inhibits alprenolol binding by 50% approximates the Kd value for competitor binding. The Kd for binding of epinephrine to its rece
13、ptor on liver cells is only 510-5 M and would not be measurable by a direct binding assay with 3Hepinephrine. The Kd for binding of isoproterenol, which induces the normal cellular response, is more than tenfold lower.FIGURE 10-5 Binding of low-affinity ligands to cell-surface receptors can be detec
14、ted in competition assays.24FIGURE 10-6 Functional expression assay can identify a cDNA encoding a cell-surface receptor. Target cells lacking receptors for a particular ligand (X) are stably transfected with a cDNA expression vector encoding the receptor. The design of the expression vector permits
15、 selection of transformed cells from those that do not incorporate the vector into their genome. 25G蛋白Guanine nucleotide-binding regulatory protein(, , )26Diversity of G Protein-Coupled Receptor Signal Transduction Pathways 2728G ProteinCoupled Receptors That Activate or Inhibit Adenylyl Cyclase29第二
16、信使之一cAMP30FIGURE 13-7 Four common intracellular second messengers.The major direct effect or effects of each compound are indicated below its structural formula. Ca2+ and several membrane-bound phosphoinositides also act as second messengers.31Adenylyl Cyclase Is Stimulated and Inhibited by Differen
17、t Receptor-Ligand Complexes32FIGURE 13-15 Hormone-induced activation and inhibition of AC in adipose cells. Ligand binding to Gs-coupled receptors causes activation of AC, whereas ligand binding to Gi-coupled receptors causes inhibition of the enzyme. The G subunit in both Gs and Gi proteins is iden
18、tical; the G subunits and their corresponding receptors differ. Ligand-stimulated formation of active GGTP complexes occurs by the same mechanism in both Gs and Gi proteins. However, GsGTP and GiGTP interact differently with AC, so that one stimulates and the other inhibits its catalytic activity. 3
19、3cAMP-Activated Protein Kinase A Mediates Various Responses in Different Cells34Cyclic Nucleotide Metabolism - cAMP 35激素通過第二信使刺激肝糖原水解36其它第二信使cGMP三磷酸肌醇(IP3)二酰甘油(DG)Ca 2+37Cyclic Nucleotide Metabolism - cGMP 38FIGURE 13-28 Synthesis of DAG and IP3 from membrane-bound phosphatidylinositol (PI). Each PI
20、 kinase places a phosphate (yellow circles) on a specific hydroxyl group on the inositol ring, producing the phosphoinositides PIP and PIP2. Cleavage of PIP2 by PLC yields DAG and IP3. 39Inositol 1,4,5-Trisphosphate (IP3) Triggers Release of Ca2+ from the Endoplasmic Reticulum40Signaling by Inositol
21、 Phospholipids 41Diacylglycerol (DAG) Activates PKC, Which Regulates Many Other Proteins42Cyclic nucleotide metabolism-cGMP4344NO is synthesized in endothelial cells in response to Ach and the subsequent elevation in cytosolic Ca2+. NO diffuses locally through tissues and activates an intracellular
22、NO receptor with GC activity in nearby smooth muscle cells. The resulting rise in cGMP leads to activation of PKG, relaxation of the muscle, and thus vasodilation. The cell-surface receptor for atrial natriuretic factor (ANF) also has intrinsic GC activity; stimulation of this receptor on smooth mus
23、cle cells also leads to increased cGMP and subsequent muscle relaxation. FIGURE 13-30 Regulation of contractility of arterial smooth muscle by NO and cGMP.454647類固醇激素的作用機理484950Signal transduction pathways involved in prolactin regulation51Glucocorticoid receptor signaling52T3的作用機理5354細胞信號轉(zhuǎn)導Physical
24、 signal transduction: light, sound, radiation, gravity, temperature, moisture,magnetic field.Chemical signal transduction Direct: physical, intercellular channels Indirect: local mediator, hormones, neurotrnasmitters55胞內(nèi)信號轉(zhuǎn)導機制 cAMP-PKA pathway cGMA-PKG pathway PI-PKC pathway Ca 2+ -calmodulin pathwa
25、y56信號轉(zhuǎn)導的基本規(guī)律 放大作用 信號的通用性和特異性 信號轉(zhuǎn)導的激活和失活 信號系統(tǒng)間存在交互作用 細胞對信號的反應可快可慢57FIGURE 13-18 Amplification of an external signal downstream from a cell-surface receptor. Binding of a single epinephrine molecule to one Gs proteincoupled receptor molecule induces synthesis of a large number of cAMP molecules. Four
26、cAMP activate two molecules of PKA, but each activated PKA phosphorylates and activates multiple product molecules. This second level of amplification may involve several sequential reactions in which the product of one reaction activates the enzyme catalyzing the next reaction. 58The Mitogen-activa
27、ted Protein Kinase (MAPK) Cascades 5960NPY Inhibition of Catecholamine Release 6162Cytokines, Growth Factors and Hormones 63Cytokines, Growth Factors and HormonesCytokines, growth factors (GF), and hormones are all chemical messengers that mediate intercellular communication. The regulation of cellu
28、lar and nuclear functions by cytokines, growth factors, and peptide or protein hormones is initiated through the activation of cell surface receptors (Rc). All receptors have two main components: 1) a ligand-binding domain that ensures ligand specificity and 2) an effector domain that initiates the
29、generation of the biological response upon ligand binding. The activated receptor may then interact with other cellular components to complete the signal transduction process. Many growth factors bind to receptors that are linked through G-proteins to membrane-bound phospholipase C (PLC). Activation
30、 of PLC cleaves phosphatidylinositol 4,5-bisphosphate (PIP2) to form diacylglycerols (DAG) and D-myo-inositol-1, 4, 5-trisphosphate (IP3). IP3 regulates intracellular Ca2+ by binding to the IP3 receptor on the endoplasmic reticulum (ER) and stimulating Ca2+ release from the ER. Free intracellular Ca
31、2+ can bind to calmodulin, and this Ca2+-calmodulin complex, in the presence of cyclic-AMP (cAMP), activates protein kinase A (PKA) by binding to the regulatory subunit of the enzyme. DAG binds to and activates protein kinase C (PKC). Other hormone receptors may be linked through G-proteins to adeny
32、l cyclase (AC) instead of PLC. Activation of AC increases the cellular levels of cAMP and, in the presence of the Ca2+-calmodulin complex, will activate PKA. Additionally, some growth factor and cytokine receptors are protein tyrosine kinases (PTK) that are directly activated by ligand-receptor inte
33、raction. Activation of any of the protein kinases, PKA, PKC, or PTK, catalyzes the phosphorylation of other proteins within the cell. Enzymes that are activated or inhibited by phosphorylation may mediate functional processes within the cell, while others may be one step in a protein kinase cascade that regulates nuclear events.Steroid hormones (i.e. estrogen, glucocor
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