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Midterm Review Components of the Cytoskeleton • Three main types of fibers make up the cytoskeleton: – Microtubules are the thickest of the three components of the cytoskeleton – Microfilaments, also called actin filaments, are the thinnest components – Intermediate filaments are fibers with diameters in a middle range Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings 3 Types of Cytoskeleton Fibers: Microtubules • • • • Protein = tubulin Largest fibers Shape/support cell Track for organelle movement • Forms spindle for mitosis/meiosis • Component of cilia/flagella • Plant & animal cells Microfilaments • Protein = actin • Smallest fibers • Support cell on smaller scale • Cell movement • Eg. ameboid movement, cytoplasmic streaming, muscle cell contraction • Plant & animal cells Intermediate Filaments • Intermediate size • Permanent fixtures • Maintain shape of cell • Fix position of organelles • Only in some animal cells Water Potential • What is the water potential equation? Water Potential • What is the water potential equation? Water potential equation: ψ = ψS + ψP • Water potential (ψ) = free energy of water • Solute potential (ψS) = solute concentration (osmotic potential) • Pressure potential (ψP) = physical pressure on solution Water Potential • How do you calculate Solute Potential? Water Potential • How do you calculate Solute Potential? ψS = -iCRT • • • • i = ionization constant (# particles made in water) C = molar concentration R = pressure constant (0.0831 liter bars/mole-K) T = temperature in K (273 + °C) • The addition of solute to water lowers the solute potential (more negative) and therefore decreases the water potential. Water Potential Water Potential Water Potential What is the water potential of a cell with a solute potential of -0.67 kPa and a pressure potential of 0.43 kPa? Macromolecules • List the 4 macromolecules, their monomers, polymers, and types of bonds. Macromolecules • List the 4 macromolecules, their monomers, polymers, and types of bonds. – Carbs: monosaccharides, polysaccharides, glycosidic linkage – Lipids: fatty acids and glycerol, triglycerides, ester linkage – Proteins: amino acids, polypeptides, peptide bonds – Nucleic Acids: nucleotides, nucleic acids, phosphodiester bonds Macromolecules • Describe the basic structure of an amino acid. Amino Acid • R group = side chains • Properties: • hydrophobic • hydrophilic • ionic (acids & bases) • “amino” : -NH2 • “acid” : -COOH Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings Macromolecules • What are the 4 levels of protein structure and describe them. Four Levels of Protein Structure 1. Primary – Amino acid (AA) sequence – 20 different AA’s – peptide bonds link AA’s Four Levels of Protein Structure (continued) 2.Secondary – Gains 3-D shape (folds, coils) by H-bonding – Alpha (α) helix, Beta (β) pleated sheet Four Levels of Protein Structure (continued) 3.Tertiary – Bonding between side chains (R groups) of amino acids – H bonds, ionic bonds, disulfide bridges, van der Waals interactions Four Levels of Protein Structure (continued) 4.Quaternary – 2+ polypeptides bond together – R groups of polypeptide chains held together with H bonds, ionic bonds, disulfide bridges, van der Waals interactions Natural Killer (NK) cells perforate cells • All cells in the body (except red blood cells) have a class 1 MHC protein on their surface • Cancerous or infected cells no longer express this protein; NK attack these damaged cells – release perforin protein into membrane of target cell – forms pore allowing fluid to natural killer cell flow in & out of cell – cell ruptures (lysis) cell – granzymes also released to induce membrane perforin apoptosis cell membrane virus-infected cell Helper T Cells: A Response to Nearly All Antigens • CD4 binds the class II MHC molecule – keeps the helper T cell joined to the antigenpresenting cell while activation occurs • Activated helper T cells secrete cytokines that stimulate other lymphocytes Antigenpresenting cell Peptide antigen Bacterium Class II MHC molecule CD4 TCR (T cell receptor) Helper T cell Humoral immunity (secretion of antibodies by plasma cells) Cytokines + B cell + + + Cytotoxic T cell Cell-mediated immunity (attack on infected cells) Fig. 43-18-3 Released cytotoxic T cell Cytotoxic T cell Perforin Granzymes CD8 TCR Class I MHC molecule Target cell Dying target cell Pore Peptide antigen Fig. 43-19 Humoral Immunity Antigen-presenting cell Bacterium Peptide antigen B cell Class II MHC molecule TCR Clone of plasma cells + CD4 Cytokines Secreted antibody molecules Endoplasmic reticulum of plasma cell Helper T cell Activated helper T cell Clone of memory B cells 2 µm The Role of Antibodies in Immunity • Neutralization - pathogen can’t infect host because it’s bound to antibody • Opsonization - antibodies bound to antigens increase phagocytosis • Antibodies together with proteins of the complement system generate a membrane attack complex and cell lysis Viral neutralization Opsonization Activation of complement system and pore formation Bacterium Complement proteins Virus Formation of membrane attack complex Flow of water and ions Macrophage Pore Foreign cell Evolution • Allopatric and Sympatric Speciation Two main modes of speciation: Allopatric Speciation Sympatric Speciation “other” “homeland” “together” “homeland” Geographically isolated populations Overlapping populations within home range • Caused by geologic events or processes • Evolves by natural selection & genetic drift Gene flow between subpopulations blocked by: • polyploidy • sexual selection • habitat differentiation Eg. Squirrels on N/S rims of Grand Canyon Eg. polyploidy in crops (oats, cotton, potatoes, wheat) Fig. 24-14-4 • Incomplete reproductive barriers • Possible outcomes: reinforcement, fusion, stability Isolated population diverges Possible outcomes: Hybrid zone Reinforcement OR Fusion Gene flow Hybrid Population (five individuals are shown) OR Barrier to gene flow Stability Evolution – Hybrid Zones Evolution • Draw a phylogenetic tree to correspond to the following data. Species 1 2 3 4 5 1 - 2 1 - 3 8 8 - 4 19 20 19 - 5 7 9 2 18 - Evolution Species 1 2 3 4 5 1 - 2 1 - 3 8 8 - 4 19 20 19 - • Species 1 & 2 – only 1 difference • Species 3 & 5 – only 2 differences • Species 4 compared to 1, 2, 3, & 5 – most differences outgroup 5 7 9 2 18 - Evolution Species 1 2 3 4 5 1 - 2 1 - 3 8 8 - 4 19 20 19 - 5 7 9 2 18 - Membrane Transport • What is the difference between hypertonic, hypotonic, and isotonic? Membrane Transport • What is the difference between hypertonic, hypotonic, and isotonic? – Isotonic solution: Solute concentration is the same as that inside the cell; no net water movement across the plasma membrane – Hypertonic solution: Solute concentration is greater than that inside the cell; cell loses water – Hypotonic solution: Solute concentration is less than that inside the cell; cell gains water Fig. 7-13 Hypotonic solution H2O Isotonic solution H2O H2O Hypertonic solution H2O (a) Animal cell Lysed Normal Shriveled Hypotonic solution H2O Isotonic solution H2O H2O Hypertonic solution H2O (b) Plant cell Turgid (normal) Flaccid Plasmolyzed Fig. 7-UN3 “Cell” 0.03 M sucrose 0.02 M glucose Environment: 0.01 M sucrose 0.01 M glucose 0.01 M fructose Fig. 7-UN4 Membrane Transport • Side A in a U-tube has 5M sucrose and 3M glucose. Side B has 2M sucrose and 1M glucose. The membrane is permeable to glucose and water only. What happens to each side? Membrane Transport • Side A in a U-tube has 3M sucrose and 1M glucose. Side B has 1M sucrose and 3M glucose. The membrane is permeable to glucose and water only. What happens to each side? Photosynthesis • What are the 2 main steps of Photosynthesis? – Light Reactions – Calvin Cycle Fig. 10-5-4 CO2 H2O Light NADP+ ADP + P i Light Reactions Calvin Cycle ATP NADPH Chloroplast O2 [CH2O] (sugar) Fig. 10-13-5 4 Primary acceptor 2 H+ + 1/ O 2 2 H2O e– 2 Primary acceptor e– Pq Cytochrome complex e– e– 3 8 P700 5 Light ATP synthase 6 ATP Pigment molecules PS I NADP+ + H+ NADPH Pc e– P680 PS II Fd NADP+ reductase e– 1 Light 7 Fig. 10-17 STROMA (low H+ concentration) Cytochrome Photosystem I complex Light Photosystem II Light Fd NADP+ reductase 3 NADP+ + H+ 4 H+ NADPH Pq – H2O THYLAKOID SPACE (high H+ concentration) e– e 1 1/ Pc 2 2 O2 +2 H+ 4 H+ To Calvin Cycle Thylakoid membrane STROMA (low H+ concentration) ATP synthase ADP + P i ATP H+ Fig. 10-18-3 Input 3 (Entering one at a time) CO2 Phase 1: Carbon fixation Rubisco 3 P Short-lived intermediate P 6 P 3-Phosphoglycerate 3P P Ribulose bisphosphate (RuBP) 6 ATP 6 ADP 3 ADP 3 Calvin Cycle 6 P P 1,3-Bisphosphoglycerate ATP 6 NADPH Phase 3: Regeneration of the CO2 acceptor (RuBP) 6 NADP+ 6 Pi P 5 G3P 6 P Glyceraldehyde-3-phosphate (G3P) 1 Output P G3P (a sugar) Glucose and other organic compounds Phase 2: Reduction Cotransport: membrane protein enables “downhill” diffusion of one solute to drive “uphill” transport of other Eg. sucrose-H+ cotransporter (sugar-loading in plants) Point Mutations • A point mutation is a change in one base in a gene • Effects can vary: – Mutations in noncoding regions often harmless – Mutations in gene might not affect protein production b/c of redundancy in genetic code – Mutations that result in change in protein production are often harmful, but can sometimes increase the fit between organism and environment Evolution • Orthologous and Paralogous genes Fig. 26-18 Ancestral gene Ancestral species Speciation with divergence of gene Species A Orthologous genes Species B (a) Orthologous genes Species A Gene duplication and divergence Paralogous genes Species A after many generations (b) Paralogous genes Thermodynamics • What is the Gibb’s Free Energy equation? Thermodynamics • What is the Gibb’s Free Energy equation? – ∆G = ∆H – T∆S – ∆G = change in free energy – ∆H = change in total energy – ∆S = change in entropy – T = temperature in Kelvin Thermodynamics • What is the Gibb’s Free Energy equation? – ∆G = ∆H – T∆S – In a reaction that occurs at 25°C, the enthalpy is 52.78 kJ and the entropy is 0.21 kJ/K. Calculate the ∆G. Thermodynamics • What is the Gibb’s Free Energy equation? – ∆G = ∆H – T∆S – In a reaction that occurs at 25°C, the enthalpy is 52.78 kJ and the entropy is 0.21 kJ/K. Calculate the ∆G. – ∆G = (52.78) – (25 + 273)(0.21) – ∆G = (52.78) – (298)(0.21) – ∆G = (52.78) – (62.58) – ∆G = -9.8 kJ Evolution • What is the difference between the Founder Effect and the Bottleneck Effect? Evolution Evolution • What are the 4 observations and 2 inferences that Darwin developed? Evolution • What are the 4 observations and 2 inferences that Darwin developed? – Members of a population vary greatly in their traits – Traits are inherited from parents to offspring – All species are capable of producing more offspring than the environment can support – Many offspring doe not survive – Individuals whose inherited traits give them a higher probability of surviving and reproducing in a given environment tend to leave more offspring than other individuals – This unequal ability of individuals to survive and reproduce will lead to the accumulation of favorable traits in the population over generations Fig. 26-11 Evolution Tuna Leopard TAXA Vertebral column (backbone) 0 1 1 1 1 1 Hinged jaws 0 0 1 1 1 1 Four walking legs 0 0 0 1 1 1 Amniotic (shelled) egg 0 0 0 0 1 1 Hair 0 0 0 0 0 1 (a) Character table From this data, create a phylogenetic tree Fig. 26-11 Evolution Lancelet (outgroup) Lamprey Tuna Vertebral column Salamander Hinged jaws Turtle Four walking legs Amniotic egg Leopard Hair (b) Phylogenetic tree Evolution • What are the 2 Hardy-Weinberg equations? And what does each symbol represent? Evolution • What are the 2 Hardy-Weinberg equations? And what does each symbol represent? – – – – – p2 + 2pq + q2 = 1 p+q=1 p = frequency of the dominant allele q = frequency of the recessive allele p2 = frequency of the homozygous dominant genotype – q2 = frequency of the homozygous recessive genotype – 2pq = frequency of the heterozygous genotype Evolution • What are the five conditions necessary for a population to be in Hardy-Weinberg equilibrium? Evolution • What are the five conditions necessary for a population to be in Hardy-Weinberg equilibrium? – No mutations – Random mating – No natural selection – Extremely large population size – No gene flow Evolution • What are the differences between directional selection, disruptive selection, and stabilizing selection? Fig. 23-13 Original population Original Evolved population population (a) Directional selection Phenotypes (fur color) (b) Disruptive selection (c) Stabilizing selection Evolution • What are the steps to producing the first cells on earth? Evolution • What are the steps to producing the first cells on earth? – Abiotic synthesis of small organic molecules – Joining of those small molecules into macromolecules – Packaging molecules into “protobionts” – Formation of self-replication molecules Cells • What are the functions of the following cell parts? – Nucleus – Ribosomes – Smooth ER – Rough ER – Golgi Cells • What are the functions of the following cell parts? – Nucleus: contains cell DNA – Ribosomes: make proteins – Smooth ER: makes lipids, stores calcium, detoxification, breaks down carbs – Rough ER: secretes glycoproteins, distributes vesicles – Golgi: makes macromolecules, modifies proteins, packages proteins Cells • Which organelles are part of the endomembrane system and how do they work together? Cells • Which organelles are part of the endomembrane system and how do they work together? – Nuclear envelope – Endoplasmic reticulum – Golgi apparatus – Lysosomes – Vacuoles – Plasma membrane Fig. 6-16-3 Nucleus Rough ER Smooth ER cis Golgi trans Golgi Plasma membrane Membrane Transport • Label the parts of the plasma membrane Fig. 7-7 Fibers of extracellular matrix (ECM) Glycoprotein Carbohydrate Glycolipid EXTRACELLULAR SIDE OF MEMBRANE Cholesterol Microfilaments of cytoskeleton Peripheral proteins Integral protein CYTOPLASMIC SIDE OF MEMBRANE Cell Respiration • What are the 3-4 main steps of Cellular Respiration? Cell Respiration • What are the 3-4 main steps of Cellular Respiration? – Glycolysis – Intermediate Step/Link Reaction – Krebs Cycle/Citric Acid Cycle – Oxidative Phosphorylation Fig. 9-6-3 Electrons carried via NADH and FADH2 Electrons carried via NADH Citric acid cycle Glycolysis Pyruvate Glucose Oxidative phosphorylation: electron transport and chemiosmosis Mitochondrion Cytosol ATP ATP ATP Substrate-level phosphorylation Substrate-level phosphorylation Oxidative phosphorylation Fig. 9-8 Energy investment phase Glucose 2 ADP + 2 P 2 ATP used 4 ATP formed Energy payoff phase 4 ADP + 4 P 2 NAD+ + 4 e– + 4 H+ 2 NADH + 2 H+ 2 Pyruvate + 2 H2O Net Glucose 4 ATP formed – 2 ATP used 2 NAD+ + 4 e– + 4 H+ 2 Pyruvate + 2 H2O 2 ATP 2 NADH + 2 H+ CYTOSOL MITOCHONDRION NAD+ Transport protein 1 Pyruvate NADH + H+ 2 3 CO2 Coenzyme A Acetyl CoA Fig. 9-11 Pyruvate CO2 NAD+ CoA NADH + H+ Acetyl CoA CoA CoA Citric acid cycle FADH2 2 CO2 3 NAD+ 3 NADH FAD + 3 H+ ADP + P i ATP NADH 50 2 e– NAD+ FADH2 2 e– 40 FMN FAD Multiprotein complexes FAD Fe•S Fe•S Q Cyt b 30 Fe•S Cyt c1 IV Cyt c Cyt a Cyt a3 20 10 2 e– (from NADH or FADH2) 0 2 H+ + 1/2 O2 H 2O Cell Respiration • What are the 2 types of anaerobic respiration? – Alcoholic fermentation – Lactic Acid fermentation • In alcohol fermentation, pyruvate is converted to ethanol in two steps, with the first releasing CO2 • Alcohol fermentation by yeast is used in brewing, winemaking, and baking Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings • In lactic acid fermentation, pyruvate is reduced by NADH, forming lactate as an end product, with no release of CO2 • Lactic acid fermentation by some fungi and bacteria is used to make cheese and yogurt • Human muscle cells use lactic acid fermentation to generate ATP when O2 is scarce Copyright © 2008 Pearson Education, Inc., publishing as Pearson Benjamin Cummings Photosynthesis • What are the 2 main steps of Photosynthesis? Thermodynamics • What are the 2 laws of thermodynamics? Thermodynamics • What are the 2 laws of thermodynamics? – First law of thermodynamics: the energy of the universe is constant: – Energy can be transferred and transformed, but it cannot be created or destroyed – Second law of thermodynamics: – Every energy transfer or transformation increases the entropy (disorder/randomness) of the universe Enzymes • What is the difference between a competitive and noncompetitive inhibitor? Enzymes • What is the difference between a competitive and noncompetitive inhibitor? – Competitive inhibitors bind to the active site of an enzyme, competing with the substrate – Noncompetitive inhibitors bind to another part of an enzyme, causing the enzyme to change shape and making the active site less effective Fig. 8-19 Substrate Active site Competitive inhibitor Enzyme Noncompetitive inhibitor (a) Normal binding (b) Competitive inhibition (c) Noncompetitive inhibition Enzymes • What is end product inhibition? Enzymes • What is end product inhibition? – the end product of a metabolic pathway shuts down the pathway – Feedback inhibition (negative feedback) prevents a cell from wasting chemical resources by synthesizing more product than is needed Fig. 8-22 Initial substrate (threonine) Active site available Isoleucine used up by cell Threonine in active site Enzyme 1 (threonine deaminase) Intermediate A Feedback inhibition Isoleucine binds to allosteric site Enzyme 2 Active site of enzyme 1 no longer binds Intermediate B threonine; pathway is Enzyme 3 switched off. Intermediate C Enzyme 4 Intermediate D Enzyme 5 End product (isoleucine)