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Transcript
Regulation Regulation A central theme that runs through many regulatory mechanisms is the role that low molecular substances, made by cells or present in environment, have in mediating control. These low molecular weight molecules, called effector molecules or ligands, interact with specific proteins called allosteric proteins, in a non-covalent fashion, and alter the properties of these proteins. Regulation of Gene Expression new σ new RNA pol Use of regulatory proteins Allosteric protein Positive regulatory proteins Activator proteins Regulatory RNA Negative regulatory proteins Repressor proteins Regulation 5 General Classes of Enzymes An Inducible Enzyme System Regulation is specific Constitutive enzymes (house keeping genes) Inducible enzymes Repressible enzyme systems Operon: a collection of genes that are functionally related and are transcribed as a single unit (polycistronic or polygenic message), which is under the control of a single operator/promoter region or regulatory region. Lactose Operon: Jacob and Monod (J. Mol. Biol 3:318-356, 1961) Fig. 8.11 Regulation Lactose metabolism lactose (glucose-galactose) Diauxic Growth Glucose and lactose glucose + galactose β-galactosidase (β-gal) Glucose effect Catabolite repression lacZ gene Fig. 8.18 Gratuitous Inducers β-gal permease (lacY gene) Transacetylase (lacA gene) (allolactose) The lac Operon Regulation Regulation of the lac Operon by the lac Repressor How explain catabolite repression? Lactose operon is also under positive control Activator protein- catabolite activator protein (CAP) CAP + cAMP -------> CAP/cAMP (active) Catabolite Repression Catabolite Activator Protein (CAP) ATP ---------> c-AMP ----------> AMP Adenylcyclase phosphodiesterase • also called cyclic AMP receptor protein (CRP) • brings about the coordinate regulation of catabolite operons • exists two forms – active form when 3’,5’-cyclic adenosine monophosphate (cAMP) is bound – inactive form when it is free of cAMP Fig. 8.19 Regulation Regulation of the lac Operon by the lac Repressor and CAP Phosphotransferase System Maltose Operon (Regulon) Sequential Enzyme Induction Galactose Metabolism Lactose (glucose-galactose) glucose + galactose Expression controlled by an activator protein not a repressor protein β-galactosidase Inducer galactose operon glucose Negative and positive control Fig. 8.15 No CAP/cAMP involved Positive Control of Enzyme Induction Regulation Fig. 8.17 Tryptophan Operon and Biosynthetic Pathway Feedback, end-product, inhibition Repression Attenuation Tryptophan Biosynthetic Pathway Erythrose-4-phosphate + 7 enzymes 3 enzymes Chorismic acid L-tryptophan PEP L-phenylalanine L-tyrosine Regulation Enzyme Inhibition by an Allosteric Effector Feedback (end-product) Inhibition ~1000 Anthranilate synthetase Chorismic acid + or - Anthranilic acid L- trp More than one effector Reduce flow of carbon through trp biosynthetic pathway Fig. 8.3 Tryptophan Operon Tryptophan Operon A repressible enzyme system Leader region consists of 162 bp Trp biosynthetic genes Trp repressor gene Trp P 0 L E D C B A encodes a 14 aa’s peptide have ribosome binding site have a start/stop codon repressed Inactive repressor + trp De-repressed Active repressor Operon controlled by attenuation (lessen in amount) have regions of homolgy Regulation sufficiency 9/10 transcription is terminated in leader region Fig. 8.25a Tryptophan Operon Trp limitation 10/10 times transcription is initiated RNA pol reads into trp genes Trp limitation Anti-terminator loop Fig. 8.25b Regulation Regulation of Branched Pathways by Feedback Inhibition Fig. 8.24 Isozymes: catalyze same reaction but are subject to different effector molecules Isofunctional Enzyme Inhibition 3-deoxy-Darabinoheptulosonate7-phosphate Fig. 8.5 Regulation Need all effectors associated with enzyme to have inhibition Assimilation of Inorganic Nitrogen Concerted feedback inhibition Each effector binding inhibits enzyme by a certain percent Two Mechanisms: 1. Glutamic dehydrogenase α-ketoglutarate + NH3 -----> glutamic acid 2. Second mechanism uses a 2 enzyme system: L-glutamine synthetase and glutamate synthetase or GOGAT enzyme. GS Glutamic acid + NH3 + ATP -------> glutamine GOGAT Glutamine + α -ketoglutarate --------> 2 glutamic acids AMP-adenyl transferase Glutamine Synthetase Cumulative Feedback Inhibition Covalent modification • Enzyme composed of 12 identical protein subunits. • Each subunit has 8 distinct allosteric sites (96 allosteric sites). • As each effector molecule binds get a % inhibition in enzyme activity. •Enzyme is also regulated by covalent modification. To have cumulative feedback inhibition each of the 12 subunits must first be covalently modified. less active More sensitive to FB inhibition PII + UTP -------> PII-UMP low Glutamine/α-ketoglutarate Fig. 8.6 Regulation Flagella Phase Variation Salmonella typhimurium Site specific recombination Riboswitches: Found in few bacteria, plants, and fungi Regulation by RNA’s sRNA’s: 40-400 nt in lenght
