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Cell Signaling AP Chapter 11 Evolution of cell signaling • Similarities in pathways in bacteria, protists, fungi, plants, and animals suggest an early evolution of signaling pathways • Multicellular better due to coordination and control of pathways http://www.youtube.com/watch?v=FsGwgiIv_NU Boseman video Bacteria communication “bacteria talking to each other” • Quorum sensingconcentration of signaling molecules allows bacteria to sense their local density • Ex- Vibrio – glowing bacteria (luciferase enzyme) give off auto inducers into their environment autoinducers Quorum sensing can lead to the formation of biofilms Slime molds – chemical signaling • Slime molds live as solitary amoebae. • When slime mold cells begin to starve or dehydrate, they release a pheromone-like chemical called cyclic AMP. This messenger molecule alerts other slime mold amoebae. They detect the cAMP and follow the scent to join forces with the troubled amoebae forming a large mass of cells. Other slime mold amoebae detect the cAMP and follow the scent to join forces with the troubled amoebae. cAMP is an important chemical word in the language of cells and seems to be understood and made by all cells, even our own. Fruiting body formation in fungi chemical signaling Local and long-distance signaling Direct cytoplasmic connections: - gap junctions or plasmodesmata in plant cells - contact of surface molecules (cell-tocell recognition via receptors Plasmodesmata in plant cells Gap junctions in animal cells Immune cells – direct contact Local regulators – nearby cells • paracrine signaling – only includes cells of a particular organ • synaptic signaling – between neurons • Long distance • endocrine signaling • nerve transmission 3 stages of cell signaling 1. Reception 2. Transduction 3. Response http://www.youtube.com/watch?v=qOVkedxDqQo Boseman video on cell signaling pathways Fig. 11-6-1 EXTRACELLULAR FLUID 1 Reception Receptor Signaling molecule CYTOPLASM Plasma membrane Fig. 11-6-2 CYTOPLASM EXTRACELLULAR FLUID Plasma membrane 1 Reception 2 Transduction Receptor Relay molecules in a signal transduction pathway Signaling molecule Fig. 11-6-3 CYTOPLASM EXTRACELLULAR FLUID Plasma membrane 1 Reception 2 Transduction 3 Response Receptor Activation of cellular response Relay molecules in a signal transduction pathway Signaling molecule Reception • Ligand – the signal molecule, fits like a lock and key to receptor • Most ligands bind to cell surface receptors; some bind to intracellular receptors • Usually induces a shape change in receptor protein’s shape Types of receptors Bind with water-soluble molecules on membrane: • G-Protein-linked Receptor • Tyrosine Kinase Receptor • Ligand-gated Ion Channel Bind with hydrophobic receptors: • Intracellular Receptors G- Protein-Linked Receptors • 7 protein helices that span the membrane • Binding of the ligand to the G-protein receptor, activates a specific G protein located on the cytoplasm side. How GDP becomes GTP. • The activated G-protein activates a membrane-bound enzyme which continues on its pathway. • The GTP goes back to GDP. Animation: Membrane-Bound Receptors that Activate G Proteins Fig. 11-7a Signaling-molecule binding site Segment that interacts with G proteins G protein-coupled receptor Fig. 11-7b Plasma membrane G protein-coupled receptor Activated receptor Signaling molecule GDP CYTOPLASM GDP Enzyme G protein (inactive) GTP 2 1 Activated enzyme GTP GDP Pi Cellular response 3 4 Inactive enzyme How important is the G-protein system? • Used by hormones, neurotransmitters, sensory reception, development…. • Many bacteria produce toxins that interfere with with G-protein systems • Up to 60% of medicines influence Gprotein pathways Tyrosine kinase receptors • Receptor tyrosine kinases are membrane receptors that attach phosphates from ATP to tyrosines (Remember kinase…ATP.) • Once the receptors are activated, relay proteins bind to them and become activated themselves. • A receptor tyrosine kinase can trigger multiple signal transduction pathways at once Fig. 11-7c Ligand-binding site Signaling molecule (ligand) Signaling molecule Helix Tyrosines Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Tyr Receptor tyrosine kinase proteins CYTOPLASM Dimer 1 2 Activated relay proteins Tyr Tyr Tyr Tyr P Tyr P Tyr Tyr Tyr P 6 ATP Activated tyrosine kinase regions 6 ADP Tyr Tyr P Tyr Tyr P Tyr P Tyr P Tyr Tyr P P P P Tyr P Tyr Fully activated receptor tyrosine kinase Inactive relay proteins 3 4 Cellular response 1 Cellular response 2 Tyrosine Kinase Receptors • Binding of the signal molecules causes the two polypeptides to join. They are activated and act as enzymes to phosphorylate the tyrosines in the tails. The receptor protein is now recognized by relay proteins, triggering different effects. Ligand-gated ion channel • A ligand-gated ion channel receptor acts as a gate • When a signal molecule binds as a ligand to the receptor, the gate allows specific ions, such as Na+ or Ca2+, through a channel in the receptor • Ex- in neurotransmitters and nervous signal transmission Fig. 11-7d 1 Signaling molecule (ligand) Gate closed Ligand-gated ion channel receptor 2 Ions Plasma membrane Gate open Cellular response 3 Gate closed Ligand-Gated Ion Channels http://msjensen.cehd.umn.edu/1135/Links/Animations/Flash/0003-swf_receptors_link.swf Intracellular Receptors • Some receptor proteins are intracellular, found in the cytosol or nucleus of target cells • Small or hydrophobic chemical messengers can readily cross the membrane and activate receptors • Examples of hydrophobic messengers are the steroid and thyroid hormones of animals • An activated hormone-receptor complex can act as a transcription factor, turning on specific genes Fig. 11-8-5 Hormone (testosterone) EXTRACELLULAR FLUID Plasma membrane Receptor protein Hormonereceptor complex DNA mRNA NUCLEUS CYTOPLASM New protein Intracellular Receptors http://highered.mcgraw-hill.com/olc/dl/120109/bio46.swf Signal Transduction • Allow for amplification of signals • Signal coordination and regulation • Involves 1) second messengers (cAMP and Ca+2) 2) relay proteins such as protein kinases How does epinephrine work?...an example of cAMP messenging • Epinephrine acts via cyclic AMP (cAMP) as a second messenger. • An activated G protein activates the enzyme adenylyl cyclase (THINK CYCLING!) which turns ATP to cAMP. • Then cAMP can activate other inactive molecules to reach the desired product. action of epinephrine Video | DnaTube.com - Scientific Video Site Fig. 11-10 Adenylyl cyclase Phosphodiesterase Pyrophosphate P ATP Pi cAMP AMP Fig. 11-11 First messenger Adenylyl cyclase G protein G protein-coupled receptor GTP ATP cAMP Second messenger Protein kinase A Cellular responses cAMP second messenger systems Membrane Structure • Calcium ions also act as second messengers. One example is activating an enzyme phospholipase C to produce two more messengers which will open Ca channels. The signal receptor may be a G protein or a tyrosine kinase receptor. Fig. 11-13-3 EXTRACELLULAR FLUID Signaling molecule (first messenger) G protein DAG GTP G protein-coupled receptor PIP2 Phospholipase C IP3 (second messenger) IP3-gated calcium channel Endoplasmic reticulum (ER) CYTOSOL Various proteins activated Ca2+ Ca2+ (second messenger ) Cellular responses RELAY PROTEINS • Enzymes called protein kinases are also important links in transduction. • A protein kinase catalyzes the transfer of PHOSPHATE GROUPS from ATP to another protein to activate it. • Amplification is possible in these type of pathways. Fig. 11-9 Signaling molecule Receptor Activated relay molecule Inactive protein kinase 1 Active protein kinase 1 Inactive protein kinase 2 ATP ADP Pi P Active protein kinase 2 PP Inactive protein kinase 3 Pi ATP ADP Active protein kinase 3 PP Inactive protein P ATP P ADP Pi PP Active protein Cellular response This can get pretty complicated! Cell Responses • Alteration of metabolism • Rearrangement of cytoskeleton • Modulation of gene activity Fig. 11-14 Growth factor Reception Receptor Phosphorylatio n cascade Modulating Gene Activity Transduction CYTOPLASM Inactive transcription factor Active transcription factor P Response DNA Gene NUCLEUS mRNA Fig. 11-15 Reception Binding of epinephrine to G protein-coupled receptor (1 molecule) Transduction Inactive G protein Active G protein (102 molecules) Alteration of Metabolism Inactive adenylyl cyclase Active adenylyl cyclase (102) ATP Cyclic AMP (104) Inactive protein kinase A Active protein kinase A (104) Inactive phosphorylase kinase Active phosphorylase kinase (105) Inactive glycogen phosphorylase Active glycogen phosphorylase (106) Response Glycogen Glucose-1-phosphate (108 molecules) Fig. 11-16 RESULTS Rearrangement Wild-type (shmoos) Of cytoskeleton ∆Fus3 ∆formin CONCLUSION 1 Mating factor G protein-coupled receptor Shmoo projection forming Formin P Fus3 GTP GDP Phosphorylation cascade 2 Actin subunit P Formin Formin P 4 Fus3 Fus3 P Microfilament 5 3 Fine-Tuning of the Response • Multistep pathways have two important benefits: – Amplifying the signal (and thus the response) – Contributing to the specificity of the response Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings The Specificity of Cell Signaling and Coordination of the Response • Different kinds of cells have different collections of proteins which allow cells to detect and respond to different signals. • Even the same signal can have different effects in cells with different proteins and pathways Fig. 11-17 Signaling molecule Same signal - different effects in cells with different proteins and pathways Pathway branching and “cross-talk” further help the cell coordinate incoming signals Receptor Relay molecules Response 1 Cell A. Pathway leads to a single response. Response 2 Response 3 Cell B. Pathway branches, leading to two responses. Activation or inhibition Response 4 Cell C. Cross-talk occurs between two pathways. Response 5 Cell D. Different receptor leads to a different response. Signaling Efficiency: Scaffolding Proteins and Signaling Complexes • Scaffolding proteins are large relay proteins to which other relay proteins are attached • Scaffolding proteins can increase the signal transduction efficiency by grouping together different proteins involved in the same pathway Fig. 11-18 Signaling molecule Plasma membrane Receptor Three different protein kinases Scaffolding protein Disruptions in cell signaling pathways • Bacterial infections (cholera, anthrax, pertussis) • Animal toxins • Hormone imbalances (diabetes) • Cancer • Plant diseases Boseman video on disruptions Apoptosis (programmed cell death) integrates multiple cell-signaling pathways • Apoptosis is programmed or controlled cell suicide • A cell is chopped and packaged into vesicles that are digested by scavenger cells • Apoptosis prevents enzymes from leaking out of a dying cell and damaging neighboring cells • Apoptosis is important in shaping an organism during embryonic development Fig. 11-20b Ced-9 (inactive) Cell forms blebs Deathsignaling molecule Active Active Ced-4 Ced-3 Activation cascade (b) Death signal Other proteases Nucleases Apoptotic Pathways and the Signals That Trigger Them • Caspases are the main proteases (enzymes that cut up proteins) that carry out apoptosis • Apoptosis can be triggered by: – An extracellular death-signaling ligand – DNA damage in the nucleus – Protein misfolding in the endoplasmic reticulum Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings • Apoptosis evolved early in animal evolution and is essential for the development and maintenance of all animals • Apoptosis may be involved in some diseases (for example, Parkinson’s and Alzheimer’s); interference with apoptosis may contribute to some cancers Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings Fig. 11-21 Interdigital tissue 1 mm