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CELL COMMUNICATION & SIGNAL TRANSDUCTION. Angelica D Francisco, MD, MSc. FUNCTIONAL INTEGRATION OF ORGAN SYSTEMS. CARDIOVASCULAR SYSTEM RESPIRATORY SYSTEM RENAL SYSTEM GASTROINTESTINAL SYSTEM BLOOD & IMMUNE SYSTEM NERVOUS SYSTEM ENDOCRINE SYSTEM MUSCULAR SYSTEM REPRODUCTIVE SYSTEM.
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CELL COMMUNICATION & SIGNAL TRANSDUCTION Angelica D Francisco, MD, MSc
FUNCTIONAL INTEGRATION OF ORGAN SYSTEMS • CARDIOVASCULAR SYSTEM • RESPIRATORY SYSTEM • RENAL SYSTEM • GASTROINTESTINAL SYSTEM • BLOOD & IMMUNE SYSTEM • NERVOUS SYSTEM • ENDOCRINE SYSTEM • MUSCULAR SYSTEM • REPRODUCTIVE SYSTEM
OBJECTIVES • EXPLAIN THE IMPORTANCE OF INTERCELLULAR COMMUNICATION HOMEOSTASIS. • ENUMERATE & DESCRIBE THE TYPES OF INTERCELLULAR COMMUNICATION. • DESCRIBE THE TYPES OF RECEPTORS AND THE THEIR EFFECTS ON THE CELL IN RESPONSE TO CHEMICAL SIGNALS.
OBJECTIVES • DESCRIBE THE DIFFERENT SIGNAL TRANSDUCTION MECHANISMS IN THE CELL. • DESCRIBE THE EVENTS IN RESPONSE TO STMULATION OF G-PROTEIN COUPLED RECEPTORS. • EXPLAIN THE FUNCTION OF SECOND MESSENGERS IN THE TRANSDUCTION OF CHEMICAL SIGNALS IN THE CELL.
CELL COMMUNICATION • THE MECHANISM FOR THE CONTROL AND COORDINATION OF CELL RESPONSE
CHEMICAL MEDIATORS & RECEPTORS CHEMICAL MESSENGERS • HORMONES • NEUROTRANSMITTERS • OTHERS: AMINES, AMINO ACIDS, POLYPEPTIDES, NUCLEOTIDES
CHEMICAL MEDIATORS & RECEPTORS RECEPTORS • PROTEIN MOLECULES TO WHICH A CHEMICAL MESSENGER CAN BIND IN ORDER TO STIMULATE A CELL RESPONSE • FOUND IN CELL MEMBRANE, CYTOPLASM, NUCLEUS
TYPES OF INTERCELLULAR COMMUNICATION • NEURAL COMMUNICATION via NEURONS • ENDOCRINE COMMUNICATION via BLOOD/LYMPH • PARACRINE/AUTOCRINE via ECF
GAP JUNCTIONS INTERCELLULAR CONNECTION THAT ALLOWS FOR SUBSTANCES TO PASS FREELY BETWEEN CELLS WITHOUT ENTERING THE ECF FUNCTION: • RAPID PROPAGATION OF ELECTRICAL ACTIVITY FROM CELL TO CELL FOUND IN: • CARDIAC MUSCLE • SMOOTH MUSCLE
NEURAL COMMUNICATION • RELEASE OF NEUROTRANSMITTER AT SYNAPSE • RAPID COMMUNICATION, msec • LONG DISTANCES • DISCRETE
ENDOCRINE COMMUNICATION • RELEASE OF HORMONE INTO BLOOD/LYMPH, AFFECTING DISTANT TARGET CELL • EFFECT SLOW (sec to hrs) • EFFECTS PROLONGED • DISCRETE (eg. ANTIDIURETIC HORMONE) OR DIFFUSE (eg. INSULIN, THYROID HORMONE)
PARACRINE COMMUNICATION PARACRINE • SECRETION OF CHEMICAL INTO IF, ACTS ON NEARBY CELLS
AUTOCRINE COMMUNICATION AUTOCRINE • SECRETION OF CHEMICAL INTO INTERSTITIAL FLUID, AFFECTING SAME CELL
RECOGNITION TRANSMITTER-RECEPTOR BINDING • TRANSDUCTION SECOND MESSENGER eg. cAMP • TRANSMISSION SECOND MESSENGER SIGNAL TO EFFECTOR • RESPONSE
RECOGNITION RECEPTOR:LIGAND BINDING
RECEPTORS FOR CHEMICAL MESSENGERS REGULATION OF RECEPTORS • UP-REGULATION: INCREASE IN NUMBER WHEN CHEMICAL MESSERNGER IS DEFICIENT
RECEPTORS FOR CHEMICAL MESSENGERS REGULATION OF RECEPTORS • DOWN-REGULATION: DECREASE IN NUMBER/ACTIVITY WHEN CHEMICAL MESSENGER IS IN EXCESS INTERNALIZATION (DECLINE IN NUMBER) DESENSITIZATION (LESS RESPONSIVE)
SIGNAL TRANSDUCTION mechanisms types • ION CHANNEL ACTIVATION • G-PROTEIN ACTIVATION • ACTIVATION OF ENZYME ACTIVITY IN THE CELL • DIRECT ACTIVATION OF PROTEIN TRANSCRIPTION
SIGNAL TRANSDUCTION • FIRST MESSENGER: EXTRACELLULAR LIGANDS • SECOND MESSENGER: INTRACELLULAR MEDIATORS AMPLIFIES RESPONSE
TYPES OF RECEPTORS Cell membrane receptors • ION CHANNEL-LINKED RECEPTORS • G-PROTEIN COUPLED RECEPTORS • ENZYME-LINKED/CATALYTIC RECEPTORS Intracellular receptors • NUCLEAR RECEPTORS
ION CHANNEL-LINKED RECEPTORS • Action: CHANGE IN ION PERMEABLILITY OF the MEMBRANE
LIGAND-GATED ION CHANNEL • Action: INCREASED MEMBRANE PERMEABILITY TO Na+ ACETYLCHOLINE GATED Na+ CHANNEL
G-PROTEIN COUPLED RECEPTORS RECEPTORS ARE INTEGRAL PROTEINS WHOSE ACTIVITY IS THROUGH AN INTERMEDIARY G-PROTEIN
G-PROTEIN COUPLED RECEPTORS acTION: ACTIVATE/INACTIVATE MEMBRANE ASSOCIATED ENZYMES OR CHANNELS
G-PROTEIN COUPLED RECEPTOR SEVEN-HELIX RECEPTORS “SERPENTINE RECEPTORS”
G-PROTEIN COUPLED RECEPTOR • 3 SUBUNUITS • -SUBUNIT: BOUND TO GDP (INACTIVE) • β-SUBUNIT • γ-SUBUNIT • α AND γ-SUBUNITS ARE ATTACHED TO MEMBRANE GDP, GUANOSINE DIPHOSPHATE
GPCR SIGNALING GEF, GUANINE EXCHANGE FACTORS
GPCR SIGNALING GRS, REGULATOR OF G-PROTEIN SIGNALING
GPCR SIGNALING • ACTIVATION BY RECEPTOR-LIGAND BINDING • RECEPTOR INTERACTS WITH G-PROTEIN: GDP GTP • G-PROTEIN DISSOCIATES FROM RECEPTOR
GPCR SIGNALING • α-GTP AND βγ SUBUNITS DISSOCIATE • BOTH α-GTP AND βγ SUBUNITS INTERACT WITH THEIR EFFECTORS • HYDROLYSIS OF GTP TO GDP INACTIVATES α-SUBUNIT REASSEMBLY OF TRIMER
GPCR TRANSDUCTION PATHWAY • ACTIVATION/INIBITION OF ADENYLYL CYCLASE: ATP cAMP (Gs/Gi)
GCPR SECOND MESSENGER: cAMP aCTION: ACTIVATION OF PROTEIN KINASE A, PKA • CATALYZE PHOSPHORYLATION OF PROTEINS (i.e.,STIMULATION/INHIBITION OF ENZYMES) • PHOSPHORYLATES CREB IN NUCLEUS (i.e., REGULATE TRANSCRIPTION OF GENES) CREB, cAMP RESPONSIVE ELEMENT BINDING PROTEIN
GPCR TRANSDUCTION PATHWAY • Action: ACTIVATION OF PHOSPHODIESTERASE: cGMP GMP
GCPR SECOND MESSENGER: cGMP aCTIONs • CLOSURE OF cGMP-REGULATED ION CHANNELS(i.e., ALTERS MEMBRANE PERMEABILITY TO IONS) • ACTIVATES cGMP-DEPENDENT KINASE (i.e., STIMULATION/INHIBITION OF ENZYMES)
GPCR TRANSDUCTION PATHWAY Action: activateS PHOSPHOLIPASE C, PLC PIP2 (Phosphatidyl Inositol biPO4) PLC DAG + InsP3
GPCR TRANSDUCTION PATHWAY Action: activATES PHOSPHOLIPASE A2 MEMBRANE LIPIDS PLA2 ARACHIDONIC ACID
GCPR SECOND MESSENGER: InsP3/DAG actions: • InsP3, INOSITOL TRIPHOSPHATE • MOBILIZATION OF INTRACELLULAR Ca++ • DAG, DIACYLGLYCEROL • ACTIVATES PROTEIN KINASE C, PKC
ENZYME-LINKED/CATALYTIC RECEPTORS Ex. Insulin receptor: tyrosine kinase
NUCLEAR LINKED-RECEPTORS LIGANDS: LIPID SOLUBLE • CYTOPLASMIC RECEPTORS Ex. GLUCOCORTICOIDS & MINERALOCORTICOIDS • NUCLEAR RECEPTORS Ex. ESTROGEN, PROGESTERONE, THYROID HORMONES
CLINICAL APPLICATION ASPIRIN, NON-STEROIDAL ANTI-INFLAMMATORY DRUG • INHIBITS CYCLO-OXYGENASE IN ARACHIDONIC ACID PATHWAY • ANTI-CLOTTING: INHIBITS PLATELET FUNCTION