Transcript Cells Notes
Today’s Plan: 1/18/11 Bellwork: Go over Test (20 mins) Cell Microscopy Lab(40 mins) Cells Notes (25 mins) Today’s Plan: 1/19/11 Bellwork: Finish Microscopy (20 mins) Begin AP Lab 1 (40 mins) Cells Notes (the rest of class) Cells Notes Inside the “black box” Until the advent of the electron microscope, only the nucleus and membrane were known Chemical analysis and cell fractionation gave us some clue as to the chemical make up of cells, but that’s only part of the picture The human eye is unable to detect things smaller than .1mm Eukaryotic cells range from 10-100 micrometers Prokaryotic cells run from 1-10 micrometers, but the smallest are almost 100 nm Most cellular organelles are about the size of bacteria, however, a few, like the ribosome, are smaller still 2 Main Cell Types Prokaryotes No nucleus or membrane-bound organelles Has a region called the nucleoid for its genetic material Only Archaebacteria and Eubacteria are prokaryotic Eukaryotes Have a nucleus and an array of membranebound organelles Because of the membrane system, cell parts are compartmentalized and division of labor is more efficient Figure 7-1 Ribosomes Plasmids Cytoplasm Flagellum Chromosome Plasma membrane Cell wall Figure 7-6a Generalized animal cell Nuclear envelope Nucleus Nucleolus Chromosomes Centrioles Rough endoplasmic reticulum Ribosomes Peroxisome Structures that occur in animal cells but not plant cells Smooth endoplasmic reticulum Golgi apparatus Lysosome Mitochondrion Cytoskeletal element Plasma membrane Figure 7-6b Generalized plant cell Nuclear envelope Nucleolus Nucleus Chromosomes Structures that occur in plant cells but not animal cells Cell wall Chloroplast Rough endoplasmic reticulum Ribosomes Smooth endoplasmic reticulum Golgi apparatus Vacuole (lysosome) Peroxisome Mitochondrion Plasma membrane Cytoskeletal element On average, prokaryotes are about 10 times smaller than eukaryotic cells in diameter and about 1000 times smaller than eukaryotic cells in volume. Today’s Plan: 1/15/10 Bellwork: Set up Dialysis Tubes (25 mins) Continue with Cells notes/Finish Microscopy lab (40 mins) Finish Dialysis Tubes (20 mins) Nucleus Contains the genes responsible for cell function (chromatin-uncoiled, tangled, DNA mass) Contains Nucleolus which makes the ribosomes Nuclear pores in the nuclear envelope allow RNA and ribosomes to pass to the cytoplasm for making proteins Free ribosomes usually make proteins to be used within the cytoplasm Bound ribosomes usually make proteins that need packaging Nuclear envelope is lined with the nuclear lamina-a network of proteins that help the nucleus maintain its shape Figure 7-7 Nucleus Loosely packed sections of chromosomes Densely packed sections of chromosomes Nucleolus Nuclear envelope Figure 7-23 Outer surface of nuclear envelope Nuclear pores The Endomembrane System Endoplasmic Reticulum (ER) Vast network of membrane and sacs called cisternae Consists of approximately ½ of the totalmembrane of the cell Smooth=no bound ribosomes, synthesizes lipids, metabolizes glucose and detoxifies drugs/poisons Rough=bound ribosomes, which thread the emerging proteins that they make through the cisternal space into the ER Transitional=“budding” area where secretory proteins are sent in transport vesicles to the Golgi apparatus Figure 7-9 Rough endoplasmic reticulum Lumen of rough ER Ribosomes on outside of rough ER Free ribosomes in cytoplasm Golgi Apparatus Part of the endomembrane system that consists of flattened membranous sacs Wharehouses, sorts, modifies, packages, and ships the products of the ER “Polarity” exists because of the 1-way movement through the cisternae as ER products pass from the cis pole to the trans pole of the sac Figure 7-10 The cis face of the Golgi apparatus is oriented towards the rough ER The trans face of the Golgi apparatus is oriented towards the plasma membrane Golgi apparatus Vesicle cis face Lumen of Golgi apparatus Cisternae Vesicles trans face Figure 7-26 THE SECRETORY PATHWAY: A MODEL RNA Rough ER 1. Protein enters ER while being synthesized by ribosome. 2. Protein exits ER, travels to cis face of Golgi apparatus. cis face of Golgi apparatus Golgi apparatus 3. Protein enters Golgi apparatus and is processed as the cisternum moves toward the trans face. 4. Protein exits Golgi trans face of Golgi apparatus apparatus at trans face and moves to plasma membrane. Plasma membrane 5. Protein is secreted from cell. Today’s Plan: 1/19/10 Bellwork: Set up potatoes (20 mins) Do Lab Part E and finish Microscopy (40 mins) Plasma Membrane notes (25 mins) Lysosomes and Vacuoles Lysosomes are sacs for storage of hydrolytic enzymes These enzymes work best in an acidic environment, so H+ are pumped into the lysosome Can digest external elements that are brought into the cell or can digest old, worn-out cell components Pompe’s disease-occurs when a person’s lysosomes lack an enzyme for metabolizing glycogen, which builds up Tay-Sachs disease-occurs when lysosomes lack a lipid-digesting enzyme and causes brain impairment Vacuoles are membrane sacs for general storage Food vacuoles Contractile vacuoles (pump water out of the cell) Central vacuole (in plants) is surrounded by membrane called the tonoplast-part of the plants endomembrane system Figure 7-13 Lysosomes Material being digested within lysosomes Figure 7-16 Vacuole Vacuole Other membrane-bound organelles Mitochondria Chloroplasts (and other plastids) Generates ATP during the last 2 stages of aerobic cellular respiration Consists of 2 membranes. The inner membrane is folded into cristae, and inside is called the matrix 2 membranes form the intermembrane space Contains membranous discs called thylakoids that are stacked into grana-chlorophyll is embedded on the thylakoid membranes Contains fluid called stroma that surrounds the thylakoids Other plastids store pigments or starch (amyloplasts) Peroxisome Single membrane-bound organelle that contain enzymes which transfer hydrogen to oxygen, making Hydrogen peroxide Also contains enzymes that convert the peroxide to water since the peroxide is toxic to the cell Figure 7-17 Mitochondrion Outer and inner membranes Matrix Cristae Figure 7-18 Chloroplast Stroma Thylakoids Granum Outer and inner membranes Figure 7-12 Peroxisomes Peroxisome membrane Peroxisome lumen Cytoskeleton Supports and gives structure to the cell Also involved in movement (cilia and flagella) Can act as a “monorail” for the organelles to move around the cell Consists of proteins Microtubules (thickest)-hollow, walls made of tubulin molecules, grow from centrosome (near nucleus) to also form the centrioles for cell division Microfilaments (thinnest)-twisted actin molecules, in muscle cells are paired with myosin filaments for contraction Intermediate filaments-fibrous proteins supercoiled, make up nuclear lamella, and support long extensions of the cell Figure 7-30-Table 7-3 Figure 7-31 Actin filaments in mammalian cell Intermediate filaments in mammalian cell Microtubules in mammalian cell Cell Surfaces Cell Wall-Plant Cells only Made of cellulose Primary cell wall-thin, flexible, secreted in young plant cells (outermost cell surface) Middle Lamella-sticky layer between primary cell walls of adjacent plant cells (contains pectin) Secondary Cell wall-laid down by older plant cells between the p.m. and primary cell wall. This is much thicker, and usually consists of several layers Extracellular Matrix-Animal Cells only Network of glycoproteins (like collagen) and proteoglycans (another type of glycoprotein that’s thinner and contain more carbohydrate than the typical glycoprotein) which connect to fibronectins and integrins that connect directly to the cytoskeleton. This allows changes on the outside of the cell to be transmitted to the inside of the cell and vice-versa, which allows for regulation of the cell’s behavior Figure 7-19 Cell wall Plasma membrane of cell 1 Plasma membrane of cell 2 Cytoplasm Cell wall Cell wall of cell 1 of cell 2 of cell 1 Cytoplasm of cell 2 Figure 8-5 Gel-forming polysaccharides Collagen ECM Fibronectin Integrin Plasma membrane Cytoskeleton Actin filament Figure 8-4 Collagen molecules are made of three chains that wind around each other. 3 chains Collagen molecule Collagen fibrils in the extracellular matrix Cell in connective tissue Collagen fibrils running lengthwise Collagen fibrils in cross section Each collagen fibril is composed of many collagen molecules Today’s Plan:1/20/10 Bellwork: Finish Lab 1 (20 mins) Begin Lab 3 (30 mins) Continue Notes (30 mins) Cell Junctions In plants, the cell walls have plasmodesmata to allow for cytoplasmic exchange between cells. Animal cells have 3 main junctions Tight junction-membranes are fused, forms a seal (useful in intestines) Desmosomes-intermediate fillaments transect neighboring membranes, acting like bolts to hold cells together Gap Junction-Proteinaceous pores between membranes allowing for cytoplasmic exchange Why different junctions? There are situations where strength is integral, however there are other situations where cells must chemically communicate, requiring flow between membranes Figure 8-14 Plasmodesmata create gaps that connect plant cells. Cell walls Tubule of endoplasmic reticulum passing through plasmodesmata Smooth endoplasmic reticulum Cell wall Cell wall of cell 1 of cell 2 Membrane of cell 1 Membrane of cell 2 Gap junctions create gaps that connect animal cells. Gap junctions Membrane proteins from adjacent cells line up to form a channel Figure 8-10 Electron micrograph of a tight junction Three-dimensional view of a tight junction A tight junction forms a watertight seal between epithelial cells Plasma membranes of adjacent cells Tight junction Membrane proteins that form a tight junction Figure 8-11 Micrograph of desmosome 3-D view of desmosome Plasma membranes of adjacent cells Desmosome Anchoring proteins inside cell Membrane proteins that link cells Intermediate filaments Plasma Membrane Structure Recall that phospholipids are the basic membrane molecules They contain a phosphate (hydrophilic) and 2 fatty acid tails (hydrophobic)-amphipathic They form bilayers so that the lipid tails are always isolated from water. Chemical analysis reveals that proteins are present as well. It was originally believed that the proteins coated the inner and outer surfaces of the P.M. However our current understanding is that proteins of the plasma membrane also have hydrophobic and hydrophilic regions, and therefore transect the P.M Figure 6-4b Phospholipid Polar head (hydrophilic) Nonpolar tail (hydrophobic) Figure 6-5 Lipid micelles Lipid bilayers Water No water Hydrophilic heads interact with water Hydrophobic tails interact with each other Hydrophilic heads interact with water The Fluid Mosaic Model of the P.M. Phospholipids within the P.M. aren’t static, they shift laterally past one another because the interactions of these molecules are weaker than covalent bonds-Fluid Proteins appear to be directed by the cytoskeleton below the PM Besides phospholipids and proteins, cholesterol is embedded in the membraneMosaic This lends stability to the membrane by reducing the fluid nature of the membrane at high temps and keeps the phospholipids from compacting at low temperatures and solidifying-this would reduce its permeability Figure 6-10 Lipid bilayer with no unsaturated fatty acids Lower permeability Lipid bilayer with many unsaturated fatty acids Higher permeability Figure 6-13 Phospholipids are in constant lateral motion, but rarely flip to the other side of the bilayer Membrane Proteins Integral proteins (embedded) Transect the membrane (either entirely or partially) Peripheral proteins Bound loosely to the surface of the PM (or embedded proteins) On inner surface, can be bound to cytoskeleton On outer surface, can be bound to the ECM Figure 6-20 Outside cell Peripheral membrane protein Integral membrane protein Inside cell Peripheral membrane protein Today’s Plan: 1/21/10 Finish Membrane Notes (20 mins) Finish Part I of Lab 3(30 mins) Finish notes on cell cycle(30 mins) Membrane Functions Transport-to maintain homeostasis Enzymatic activity-enzymes embedded in membranes that do metabolic processes (ATP synthase) Signal transduction-a binding site on a receptor protein may chemically change when bound, transmitting the signal to the inside of the cell Intercellular joining-proteins link together cells (desmosomes) Recognition-glycoproteins on cell surfaces may bind to sites on adjacent membrane proteins so that the cells may recognize one another Attachment to the cytoskeleton and ECM-can allow for coordination between the two Transport across membranes Hydrophobic core Barrier for most polar substances (except very small ones like water and ethanol) Does not inhibit hydrophobic molecules like oxygen gas, carbon dioxide, and hydrocarbons Whatever can’t get in through the membrane, must somehow use a protein to get in (either by pump or channel with a hydrophilic tube in the center) Concentration and transport Rules Concentration gradient= Diffusion rule= particles move from ____ to ____ concentration until they reach __________ ______________ (movement with a concentration gradient) Osmosis= Passive= Active= Water always moves to the _______ _______ because _______________. Figure 6-15 OSMOSIS 1. Start with more solute 2. Water undergoes a net on one side of the lipid bilayer than the other, using molecules that cannot cross the selectively permeable membrane. movement from the region of low concentration of solute to the region of high concentration. Concentration descriptors Hypertonic solutions= Hypotonic solutions= Isotonic solutions= Remember, Hypotonic and hypertonic work in pairs! If the cell’s environment is hypotonic to the cell, than the cell is hypertonic to the environment (and vice-versa) Figure 6-16 Hypertonic solution Hypotonic solution Net flow of water out of cell; cell shrinks Net flow of water into cell; cell swells or even bursts Isotonic solution No change Osmoregulation Cells have to constantly regulate water uptake and loss or there are consequences (particularly animal cells) Lysis occurs if too much water flows in (some cells have contractile vacuoles to cope with this) Shrivelling and dehydration occur if too much water is lost from the cell (plasmolysis in plant cells occurs when this happens and the PM pulls away from the cell wall) Protein-Facilitated Diffusion Some proteins can change shape (enzyme-style) when molecules that need transport bind to specific sites This is done with a concentration gradient and therefore requires no energy Figure 6-25b Potassium channels allow only potassium ions to pass Potassium ions can enter the through. channel, but cannot pass into the cell Outside cell Inside cell Closed When a change in electrical charge occurs outside the membrane, the protein changes shape and allows the ions to pass through Open Active Transport Goes against a concentration gradient Therefore requires energy Ex: Sodium/Potassium Pump Figure 6-28-1 HOW THE SODIUM-POTASSIUM PUMP (Na+/K+- ATPase) WORKS Outside cell Inside cell Phosphate group 1. Three binding sites within 2. Three sodium ions from the protein have a high affinity for sodium ions. the inside of the cell bind to these sites. 3. A phosphate group from ATP binds to the protein. In response, the protein changes shape. 4. The sodium ions leave the protein and diffuse to the exterior of the cell. Figure 6-28-2 HOW THE SODIUM-POTASSIUM PUMP (Na+/K+- ATPase) WORKS 5. In this conformation, the 6. Two potassium ions bind 7. The phosphate group drops 8. The potassium ions leave protein has binding sites with a high affinity for potassium ions. to the pump. off the protein. In response, the protein changes back to its original shape. the protein and diffuse to the interior of the cell. These 8 steps repeat. Figure 6-29 Diffusion Facilitated diffusion Active transport Outside cell Inside cell Passive movement of small, uncharged molecules along an electrochemical gradient, through a membrane Passive movement of … Active movement of … Cell Communication Is believed to have evolved in prokaryotes and singlecelled eukaryotes In single-celled organisms, the primary purpose of signaling is to induce conjugation This has become a useful process for multicellular organisms, which have evolved the ability to do longdistance signaling Local regulators-travel short distances from the cell Synaptic signaling-between nerve cells Hormonal signaling Cell junction signaling and cell recognition (as discussed before) The 3 Stages of Cell Signaling Reception Signal is detected when it binds to a receptor protein on the cell’s surface Transduction The surface binding causes a change in the integral protein which initiates transduction inside the cell (can be 1-step, but more often involves multiple steps in a biochemical pathway) Response The signal triggers a cell’s response Ex:Lactose present in the body needs lactase to break it down Figure 8-17 OVERVIEW OF SIGNAL TRANSDUCTION PATHWAY Intercellular signal Outside of cell Receptor protein in membrane 1. Signal is received. Inside of cell 2. Signal is transduced. Intracellular signal 3. Signal is amplified. Cell activity changes For example, specific genes or proteins are activated or deactivated. 4. Cell responds. Receptors Just as with enzymes, the signaling molecule and receptor shape must be complimentary Ligand=molecule that specifically binds to another molecule This ligand binding generally causes a change in the shape of the protein receptor, enabling it to react with other cellular molecules Some receptors are found within the cell, so the signal molecule has to pass through the membrane to dock with the receptor (ex: testosterone) Figure 8-18 HOW DO G PROTEINS WORK? Enzyme Signal Receptor Enzyme GTP GDP Substrate Second messenger GTP G protein in “off” conformation G protein in “on” conformation Triggers response 1. G protein binds GDP. Signal 2. Signal-receptor complex changes 3. In response to binding of activated arrives and binds to receptor. conformation. G protein binds GTP and splits into two parts. G protein, enzyme catalyzes a reaction that produces a second messenger. Figure 8-16 STEROID HORMONES BIND TO SIGNAL RECEPTORS INSIDE THE CELL. Steroid hormone Plasma membrane Receptor in cytosol 1. Steroid hormone diffuses across plasma membrane into cell. 2. Hormone binds to receptor, inducing conformational change. Nucleus 3. Hormone-receptor complex binds to DNA, inducing change in gene activity. Target gene DNA Signal Transduction Pathways Protein Phosphorylation and Dephosphorylation Protein kinase transfers phosphate groups from ATP to a protein (usually another proteing kinase), wich activates the protein, causing the next step in the pathway until the correct protein is activated This is turned off by special enzymes which later remove the phosphates from the protein, called protein phosphatases Second Messengers Small molecules or ions that are not proteins and can be triggered inside the cell once reception occurs Ex: cAMP (in the liver cells for the breakup of glycogen), Ca 2+ (muscle cell contrations, secretion, cell division) Figure 8-19 HOW DO ENZYME-LINKED RECEPTORS WORK? GTP P ATP ADP Inactive protein 1 Inactive protein 2 Signal GDP GDP Ras protein P Active protein 1 P ATP ADP P Active protein 2 ATP ADP Inactive protein 3 Triggers response Ras protein Receptor tyrosine kinase (RTK) P GTP ATP ADP Bridging proteins 1. Signal arrives and binds to 2. Signal-receptor complex 3. Proteins form a bridge to Ras. 4. Ras catalyzes the receptor. changes conformation and is phosphorylated. Ras exchanges its GDP for a GTP. phosphorylation of an intracellular protein, activating it. 5. Phosphorylation cascade results, each protein phosphorylating another until a response is triggered in the cell. Cellular Responses Responses are triggered either in the nucleus (triggering transcription) or cytoplasm (regulating the proteins’ activities) Fine-tuning the response Amplification-cascades where each step produces a greater concentration of activated products Specificity of proteins-ex: epi has one effect on the heart and another on the liver because each cell type has different proteins that respond to epi Today’s Plan: 8/13/09 Finish AP Lab 3 (1st ½ of class) Finish notes (Last ½ of class) The Cell Cycle Interphase Mitosis (M Phase) G1 Phase-cell growth (2n l-shaped) S Phase-copying chromosomes in prep. For Mitosis (2n xshaped) G2 Phase-More cell growth and prep for mitosis Prophase-mitotic spindles form (centrioles in animal cells only) and attach to spindle at kinetochore (centromere and corresponding DNA Segment) Metaphase-chromosomes migrate to middle of cell (metaphase plate) Anaphase-kinetochore microtubules shorten, pulling chromosomes Telophase-accompanies cytokinesis (2 daughter nuclei, each is 2n l-shaped) Cytokinesis-clevage furrow forms as actin and myosin contract in a ring around the elongated cell in animal cells. In plants, a cell plate forms between the daughter cells, dividing them (results in 2 cells Figure 11-3 Unreplicated chromosome The unreplicated chromosome consists of a single, long strand of DNA wrapped around proteins (proteins not shown). Gene 1 Gene 2 The DNA replicates, resulting in two copies of the same chromosome.. Replicated chromosome Gene 1 Gene 2 Copies of same chromosome Gene 1 Gene 2 The DNA condenses around its associated proteins, resulting in a compact chromosome that is 10,000 times shorter than its original length. Condensed replicated chromosome Copies of same chromosome, condensed Centromere Figure 11-5 Mitosis M DIVISION G2 G1 S INTERPHASE Figure 11-7a-1 PRIOR TO MITOSIS Chromosomes replicate. Centrosomes Chromosomes Centrioles 1. Interphase: After chromosome replication, each chromosome is composed of two sister chromatids. Centrosomes have replicated. Figure 11-7a-2 MITOSIS Sister chromatids separate; one chromosome copy goes to each daughter nucleus. Early mitotic spindle Kinetochore Spindle fibers 2. Prophase: Chromosomes 3. Prometaphase: Nuclear condense, and mitotic spindle begins to form. envelope breaks down. Spindle fibers contact chromosomes at kinetochore. 4. Metaphase: Chromosomes complete migration to middle of cell. Figure 11-7b CYTOKINESIS Cytoplasm is divided. 5. Anaphase: Sister chromatids 6. Telophase: The nuclear separate. Chromosomes are envelope re-forms, and the pulled to opposite poles of the cell. spindle apparatus disintegrates. 7. Cell division begins: Actin- 8. Cell division is myosin ring causes the plasma complete: Two membrane to begin pinching in. daughter cells form. Figure 11-7b-1 5. Anaphase: Sister chromatids 6. Telophase: The nuclear separate. Chromosomes are envelope re-forms, and the pulled to opposite poles of the cell. spindle apparatus disintegrates. Binary Fission Bacterial Cell Division In stead of centrioles, chromosome is attached to and remains attached to the plasma membrane The bacterial cell elongates, separating the chromosome and its copy When the growth and separation are complete, cytokinesis occurs Figure 11-8 STEPS IN BACTERIAL CELL DIVISION 1. Chromosome 2. Chromosome 3. Chromosomes 4. FtsZ ring 5. Fission is located midcell. replicates. pull apart; ring of FtsZ protein forms. complete. constricts. Membrane and cell wall infold. Controlling the cell cycle Cell cycle Control System Molecule cycling system for regulation Checkpoints-points in the cycle where the cell is halted until the go ahead chemical signal is given (ex: G1 in animal cells is most critical) Cell Cycle clock-Cyclin-dependent kinases (Cdks) are protein kinases that need cyclin to be active (regulating the levels of cyclin and Cdks regulates the cell cycle) Ex: MPF (maturation promoting factor)-cyclins accumulate during the G2, making Cdks activate which initiate Mitosis. This is turned off during the M phase when proteolytic enzymes break down the cyclin, allowing the cell to proceed through anaphase Figure 11-14 MPF component concentration Cyclin concentration regulates MPF concentration. G1 S G2 M phase G1 MPF activated by dephosphorylation of MPF Cdk P S G2 M phase G1 S MPF activated by dephosphorylation of MPF Cdk P MPF Cdk Time Activated MPF has an array of effects. Phosphorylate chromosomal proteins; initiate M phase Activated MPF P Cyclin Cdk Phosphorylate nuclear lamins; initiate nuclear envelope breakdown Phosphorylate microtubuleassociated proteins. Activate mitotic spindle? Cyclin + Cdk with P dephosphorylated, cyclin-dependent kinase subunit Phosphorylate an enzyme that degrades cyclin; cyclin concentrations decline Internal and External Regulating Cues Internal Cues Ex: M-phase checkpoint which occurs at Metaphase and ensures that all chromosomes are attached to spindles Kinetochores that aren’t attached to spindles send signals halting anaphase until they’re attached External Cues Growth factors released from other body cells Density-dependent inhibition-in Biology, we called this contact inhibition (when cells are lost, the Growth factor level increases so cells grow and divide) Figure 11-18 THE G1 CHECKPOINT IS SUBJECT TO SOCIAL CONTROL 1. Growth factors 2. Growth factors 3. Cyclin binds to 4. Cdk is activated arrive from other cells. cause increase in cyclin and E2F concentration. Cdk; Cdk is phosphorylated. Rb inactivates E2F by binding to it. by dephosphorylation. It catalyzes phosphorylation of Rb. 5. Rb releases E2F. 6. E2F enters nucleus and triggers production of S-phase proteins. Cancer Cells that are cancerous don’t respond to the cell’s normal controls of the cell cycle Some cancerous cells divide continuously and spread easily, while others stop completely at one of the various checkpoints Cancers can transform adjacent cells to form tumors Benign=cells remain unchanged within the tumor Malignant=tumor becomes invasive and impairs the organ’s function If cells break away from the tumor and spread through the blood stream, we say they metastasize Figure 11-17 Benign tumor Normal cells Benign tumor cells may continue to divide, but are not invasive (they do not spread from tumor) Malignant tumor Malignant tumor cells divide and spread to adjacent tissues and to distant tissues through lymphatic vessels and blood vessels Lymph vessel Blood vessel New tumor that has formed in distant tissue by metastasis Meiosis Forms the precursors of gametes (Cell goes from 2nn (x-shaped, 2 cells)n (l-shaped, 4 cells) Occurs in 2 divisions: Meiosis I (homologs line up during prophase I and crossing over occurs) and Meiosis II (looks the most like mitosis) Figure 12-4l PRIOR TO MEIOSIS MEIOSIS I Chromosomes replicate, forming sister chromatids. Homologous chromosomes separate. Tetrad (4 chromatids from homologous chromosomes) Nuclear Chromatin envelope Non-sister chromatids Spindle apparatus Chiasma 1. Interphase: 2. Early Prophase I: 3. Late Prophase I: 4. Metaphase I: 5. Anaphase I: Chromosomes replicate in parent cell, in uncondensed state. Chromosomes condense, nuclear envelope breaks up, spindle apparatus forms. Synapsis of homologous chromosomes. Crossing over of non-sister chromatids (often multiple crossovers between the same chromatids). Tetrads migrate to metaphase plate. Homologs separate and begin moving to opposite sides of cell. 6. Telophase I and Cytokinesis: Chromosomes move to opposite sides of cell, then cell divides. Figure 12-4r MEIOSIS II Sister chromatids separate. 7. Prophase II: 8. Metaphase II: 9. Anaphase II: Spindle apparatus forms. Chromosomes line up at middle of cell (metaphase plate). Sister chromatids separate, begin moving to opposite sides of cell. 10. Telophase II and Cytokinesis: Chromosomes move to opposite sides of cell, then cell divides. Genetic Variation Crossing over Synapsis of homologs during prophase I causes tetrads with chiasmata (crossing-over of chromatids from neighboring chromosomes), which mixes up sections of the chromosome between homologs Used to make linkage-maps Independent assortment Inheritance of one chromosome doesn’t affect the inheritance of another (non-linkage) Random fertilization You never know which resultant sperm will fertilize which resultant egg Figure 12-7-2 A CLOSER LOOK AT THREE KEY EVENTS IN MEIOSIS Centromere Non-sister chromatids 3. Crossing over, during prophase I. Complex of proteins forms where crossing over will occur. Chromosome segments are swapped between non-sister chromatids. Protein complex Crossing over usually occurs at least once in each non-sister chromatid, but is only shown on 1 pair here