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Chapter 4 Vocabulary: Cell Theory Prokaryote Eukaryote Organelle Plasma membrane Nucleus Ribosome Endoplasmic reticulum Golgi apparatus Lysosome Mitochondria Chloroplast Cytoskeleton Endosymbiosis Outline 4.1 Cell Theory Cell Theory: 1. All living things are composed of cells 2. Cells are the basic functional unit of life 3. All cells come from pre-existing cells Cell size is limited by surface area : volume ratio Flow of nutrients in and waste out is not fast enough to keep up with the metabolic activity of the cell. Cell signaling impaired. Membrane vastly important Basic Requirements to be a cell: 1. Genetic material (DNA) 2. Cytoplasm (chemical reactions) 3. Plasma membrane 4.2 Prokaryotic Cells Smaller, simpler Metabolically diverse Bacterial domains: Archaebacteria and Eubacteria Before the nucleus Nucleoid region (one circular chromosome) Some bacteria carry plasmids (small circles of DNA with non-essential genes like antibiotic resistance) We use plasmids to manipulate cells. No membrane bound organelles Have ribosomes for protein synthesis No internal membrane (all metabolic activity occurs in the cytoplasm and at the cell membrane) No true cytoskeleton Use flagella for movement Use pili for attachment and to exchange genetic information Cell walls made of peptidoglycan (specific to bacteria) antibiotics stop formation of peptidoglycan. When you get sick you probably have about 1million cells infecting your body. Some of these cells double every 20min. Antibiotics don’t allow for the formation of peptidoglycan so the old ones die off and the new ones can’t make it. Without it they are not viable cells. Antibiotics reduce bacteria by decimals not kill all at once. If you don’t finish antibiotics cells can make peptidoglycan again and re-infect. Gram positive bacteria have lots of peptidoglycan. These infections can be treated with penicillin because it stops the formation of peptidoglycan. Without an adequate cell wall the bacteria don’t survive. Gram negative bacteria don’t have a large layer of peptidoglycan so penicillin isn’t as effective against them. Instead they are treated with mycin which stops bacterial ribosomes (which are slightly different from eukaryotic ribosomes). Without ribosomes the bacteria can’t make necessary proteins and they don’t survive. 4.3 Eukaryotic cells Larger (10X) Fungi, protists, plants, animals True nucleus – DNA is housed in a membrane-bound nucleus Membrane bound organelles (Compartmentalization of function) Nucleus: Houses DNA Like a fortress with double bi-layers and envelopes and guard proteins (pores) Site of transcription (DNA mRNA) Components of ribosomes are made in the nucleolus Ribosomes: rRNA and protein complex that translates proteins Free ribosomes synthesize cytoplasmic, nuclear, mitochondrial and other organelle proteins. Membrane-associated ribosomes synthesize proteins for the membrane and endomembrane system and proteins for export from the cell 4.4 Endomembrane System Rough ER: studded with ribosomes synthesize proteins for the membrane and endomembrane system and proteins for export from the cell modify proteins with addition of glycoproteins Smooth ER: no ribosomes, contains embedded enzymes Synthesis of carbohydrates, lipids, steroid hormones and membrane lipids Stores calcium ions for signaling Neutralizes toxins Golgi apparatus: collects, packages, modifies and distributes molecules Lysosomes: breakdown proteins, lipids, carbs and nucleic acids Recycle organelles, enzymes, etc Digest pathogens Microbodies Peroxisomes: oxidize fatty acids Vacuole: help cells maintain tonicity Specialized for different functions in different cells 4.5 Mitochondria and Chloroplast Mitochondria: produces ATP from macromolecules by oxidative metabolism Chloroplast: produces food for cells via photosynthesis Endosymbiant Theory: Theory proposed by Lynn Margulis in 1967 that explains how we go from prokaryotic cells with no organelles to eukaryotic cells with all these organelles. Early Earth had little or no free O2 Evolution of photosynthetic organisms changed the composition of the Earth’s atmosphere Cells evolved in response to the new O2 and took advantage of it by producing more energy using it (because it has a better redox potential) Aerobic respiration Predatory cells could have engulfed these cells that were capable of performing aerobic respiration. If cells were not digested eventually the host might gain some benefit from the ATP produced. Likewise, the prey would benefit from being sheltered and fed. Prey became mitochondria Which today has its own single circular genome and ribosomes Mitochondria also replicate independently of the host and have a few DNA “words” that are unique to them. Can use mitochondrial DNA to determine eukaryotic relatedness based on similarity (because only passed on by the mother) Possible that the bacteria they originally were is Rickettsia prowazekii which causes typhus (fever, chills, pain, rash from rat’s flea bites or body lice – rare in US) Chloroplasts have a similar story only they allowed hosts to photosynthesize. Different chloroplasts in different organisms just like diff bacteria – possible this engulfment happened more than once!?! Proof of Endosymbiant Theory: Same size as bacteria Double membranes Circular DNA Prokaryotic ribosomes A few “words” in DNA is different from near universal code. First amino acid added is formyl-methionine; not methionine. Replicate independently No histones associated with DNA There are still bacteria so NOT all organisms ingested others. Some parasitic eukaryotes have lost certain organelles (specifically mitochondria) because they don’t need to make energy; they just sap it from the host. Protists with no mitochondria include Microsporidia, Entamoeba histolytica, Giardia intestinalis. All are found in contaminated drinking water and lead to diarrhea, upset stomach, cramps and dehydration. 4.6 Cytoskeleton Functions: Reinforce Organize Move things around Actin filaments (Microfilaments) – thinnest Cellular movement Microtubules – keeps organelles and other structures in place and also facilitates their movement Can be built up or broken down at will – not permanently stable Use motor proteins Intermediate filaments – the most stable cytoskeleton components Used to strengthen and maintain cell shape Motor proteins are fueled by ATP Use kinesin and dynein Important for contraction of muscle Important for plants so chloroplasts can be at the best absorbing point. 4.7 Extracellular Structures and Cell Movement Flagella: 9+2 structure attached by a basal body used to propel organisms forward. Cilia: 9+2 structure of numerous hair-like projections that beat in synchrony. Cell Walls: Plants and protists use cellulose Fungi use chitin Animals do not possess. Instead they crease an extracellular matrix of glycoproteins 4.8 Cell-To-Cell Interactions Surface markers identify cells Tight junctions connect plasma membranes of cells forming a sheet (These are water tight) Adhering junctions occur in places exposed to continual stretching (heart and skin). (Anchored to ECM) Gap junctions connect cells directly to increase speed of flow between them like in the heart. (Open channels) Plasmodesmata are gap junctions in plants This chapter is pretty basic cell anatomy. Make sure you cover surface area : volume constraints. You can skip microscopes. I have included some additional notes on prokaryotes. When I cover prokaryotes I generally put a picture on the overhead and draw all over it as I discuss the anatomy. Don’t worry too much about difference between archea and Eubacteria. As far as Eukaryotic organelles students should get a feel for how a cell is interconnected; how the organelles work together like departments in a company. Mitochondria and chloroplast are important to introduce since we will see these organelles again in respiration and photosynthesis. I also included some extra information on the Endosymbiant Theory which links prokaryotes to eukaryotes. Table 4.2 lists all relevant eukaryotic organelles. In 4.6 talk about the 3 components of the cytoskeleton and what they do, but don’t worry about how they do it. 4.7 you can talk about structures and types of movement, but in a by the way sort of way. I do not have time to cover 4.8 other than to mention the surface markers and the junctions.