This document summarizes key aspects of biology unit 2 on prokaryotes and eukaryotes, cell organelles, mitosis, meiosis, fertilization, and stem cells. It describes that prokaryotes lack organelles and a nucleus, while eukaryotes have membrane-bound organelles and a nucleus containing DNA. It outlines the structure and functions of major cell organelles like the endoplasmic reticulum, mitochondria, and lysosomes. It also provides an overview of the stages of mitosis and meiosis, including how genetic variation arises, and explains human and plant fertilization processes. Finally, it defines somatic stem cells, stem cell cloning, and totipotent cells.
This document summarizes key aspects of biology unit 2 on prokaryotes and eukaryotes, cell organelles, mitosis, meiosis, fertilization, and stem cells. It describes that prokaryotes lack organelles and a nucleus, while eukaryotes have membrane-bound organelles and a nucleus containing DNA. It outlines the structure and functions of major cell organelles like the endoplasmic reticulum, mitochondria, and lysosomes. It also provides an overview of the stages of mitosis and meiosis, including how genetic variation arises, and explains human and plant fertilization processes. Finally, it defines somatic stem cells, stem cell cloning, and totipotent cells.
This document summarizes key aspects of biology unit 2 on prokaryotes and eukaryotes, cell organelles, mitosis, meiosis, fertilization, and stem cells. It describes that prokaryotes lack organelles and a nucleus, while eukaryotes have membrane-bound organelles and a nucleus containing DNA. It outlines the structure and functions of major cell organelles like the endoplasmic reticulum, mitochondria, and lysosomes. It also provides an overview of the stages of mitosis and meiosis, including how genetic variation arises, and explains human and plant fertilization processes. Finally, it defines somatic stem cells, stem cell cloning, and totipotent cells.
This document summarizes key aspects of biology unit 2 on prokaryotes and eukaryotes, cell organelles, mitosis, meiosis, fertilization, and stem cells. It describes that prokaryotes lack organelles and a nucleus, while eukaryotes have membrane-bound organelles and a nucleus containing DNA. It outlines the structure and functions of major cell organelles like the endoplasmic reticulum, mitochondria, and lysosomes. It also provides an overview of the stages of mitosis and meiosis, including how genetic variation arises, and explains human and plant fertilization processes. Finally, it defines somatic stem cells, stem cell cloning, and totipotent cells.
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Biology Unit 2 Revision
Topic 3 Voice of the Genome
Prokaryotes: The cell in which the genetic material is not enclosed by a nuclear envelope. They also contain no membrane bound organelles. Most prokaryotes possess a cell wall. An example is bacteria which have a rigid protective cell wall made on peptidoglycan. Next there is a cell membrane that holds the cells content. Bacteria have a circular piece of DNA in a region of cytoplasm called a nucleoid and other smaller rings of DNA known as plasmids. Bacteria feed by extracellular digestion. Protein synthesis occurs on ribosomes and cell respiration occurs on mesosomes (inner extensions of the cell surface membrane). Some bacteria also have flagella.
Eukaryotes: Contains organelles that are membrane bound that separate the contents of the organelles from the cytoplasm of the cell. They are generally larger than prokaryotes and can carry out chemical reactions very efficiently. Animals, plants, fungi and protoctists are made up of eukaryotic cells.
Nucleus: Contains the cells DNA. Surrounded by a nuclear envelope (a double membrane structured by a phospholipid by layer with a gap called perinuclear space). On the surface of the nuclear envelope there are nuclear pores in which diffusion occurs. The nucleus contains chromatin (DNA & protein) and a nucleolus (site of ribosome assembly). Ribosomes: Small dense organelles usually round on the surface of RER but can also be found independently. They consist of 65% rRNA and 35% protein. They are the site of translation in protein synthesis. Endoplasmic Reticulum: Connected to the nucleus. ER has a membrane that is continuous with the outer membrane of the nuclear envelope. ER often has attachment sites of ribosomes creating RER (rough endoplasmic reticulum). RER is folded over itself several times forming flattened stacks called cisternae. Its function is to keep together and transport the proteins made on the ribosomes. Newly made proteins are threaded through pores in the membrane and accumulate in the RER lumen where they are free to fold into the 3-d shape. RER is also a storage unit for enzymes and other proteins. Small vesicles contain newly synthesised proteins bud off the end of ER and either fuse with the Golgi complex or pass directly on to the cell surface membrane. SER are not continuous with the nuclear envelope and is the site of steroid production. It also contains enzymes that detoxify or make harmless a wide variety of organic molecules and it acts as a storage site for calcium in skeletal muscle cells. Mitochondria: Large, individual organelles, usually spherical or elongated that occur in large numbers in most cells. The function is to create ATP via aerobic respiration. Mitochondria have a double membrane. The outer membrane is smooth whereas the inner membrane is folded. This gives a large internal surface area on which complex reactions of AR take place. The inner folds are called cristae and also contain a matrix fluid. Centrioles: Short bundles of micro-filaments, at right angles to each other, which are found in the clear area of cytoplasm. Centrioles are the centre of cytoskeleton formation. For this reason they are known as microtubule organising centres. Lysosomes: Small vesicles that contain a mixture of powerful lytic enzymes. They are needed to destroy old or surplus organelles, digest material taken into the cell e.g. bacteria that have just been ingested by white blood cells are destroyed by lysosomes (Phagocytosis). They also destroy whole tissues or cells as part of the cell cycle. Golgi body: tightly packed group of flattened cavities or vesicles. The whole organelle is a shifting, flexible structure; vesicles are constantly being added and lost. Vesicles or proteins from RER join the Golgi body and are then altered and then bud off to undergo exocytosis. Mitosis (PMAT): Prophase: The DNA has already replicated during Interphase and the chromosomes now condense, each chromosome is a double structure made from two genetically identical pairs. Metaphase: The nuclear membrane has gone and the chromosomes arrange themselves on the equator of the spindle. Anaphase: The chromatids are pulled apart by spindle fibres and move to opposite poles. Telophase: Cytokinesis is beginning. The chromosomes become no longer individually visible. Meiosis Prophase 1: Early P1 starts when the chromosomes condense and the nucleolus disappears. Mid P1, the homologous chromosomes, one from each parent pairs up. Each pair forms a bivalent. In Late P1, recombination (cross over) takes place. One or both of the chromatids of the two homologous chromosomes breaks off at certain points and fuses with the chromatid of the other chromosome in the bivalent forming joints called chiasmata. Prophase 1 ends with the chromatids of each bivalent entwined and joined by chiasmata. Metaphase 1: Nuclear membrane disappears and spindle is fully developed. The bivalents move to the equator of the spindle in the same way as mitosis. Anaphase 1: The chromatid pairs of a bivalent are pulled apart by spindle fibres. At the end of A1, the chromatid pair from one of the original homologous chromosomes is positioned at one pole of the cell and the chromatid pair from the other homologous chromosome is at the other end of the pole. Telophase 1: Spindles disappear and the nuclear envelope re-forms around the two sets of chromosomes. At the same time cytokinesis separates the cytoplasm, forming two daughter cells preparing for the second meiotic division. Prophase 2: For each chromosome, the chromatid pair attaches itself to the new spindle, which forms at right angles to the first. Metaphase 2: Each chromatid pair lines up on the equator of the spindle. Anaphase 2: The chromatids are pulled apart and move to opposite poles. Telophase 2: The spindle disappears, the nuclear membrane re-forms, chromosomes expand and cytokinesis forms 2 separate cells forming 4 haploid cells known as a tetrad. Genetic variation is achieved by: The homologous chromosome pairs originate in different organisms, one maternal and one paternal and hence are genetically different. Blocks of genes are swapped between the chromatids of homologous chromosomes as the chiasmata form during prophase 1. Each daughter cell can receive a copy of either chromosome from a pair, and each copy may have undergone cross-over and have different genes from the other three. This is called independent assortment. Sperm cell: Have a head composed of an acrosome (special type of lysosome) and a nucleus. The acrosome contains digestive enzymes that digest through the zona pellucida in the egg cell. The sperm has a middle piece that holds large amounts of mitochondria to provide energy for the sperm to move. The rest of the cell is a flagellum made of microtubules. Egg cell:
The sperm travel through the cervix and the uterus and into one of the oviducts. When the sperm are in the oviduct, fertilisation may occur. The sperm swim towards the ovum in the oviduct. Once the sperm cell comes into contact with the granulosa cells of the egg cell, an acrosome reaction occurs. The enzymes digest the zona pellucida so that the sperm can move towards the plasma membrane of the egg cell. The sperm head fuses with the cell membrane of the cell. This triggers a cortical reaction. The egg cell releases the contents of the vesicles called cortical granules in the space between the cell membrane and zona pellucida. This makes the zona pellucida thicken and hence making it impermeable to other sperm. This ensures the fertilisation of only one of each gamete. Only the sperm nucleus enters the egg cell (the tail is discarded). The 2 nuclei fuse. This creates a zygote. Plant fertilisation: A pollen grain land on the stigma of a flower where the pollen grain absorbs water and splits open. A pollen tube grows out of the grain down into the style. 3 nuclei are found the pollen tube (one tube nucleus and 2 male gamete nuclei behind it). The tube nucleus produces enzymes that digest surrounding cells and hence making a way through for the pollen tube. When the tube reaches the ovary, it grows through the micropyle (a tiny hole in the ovule wall) and into the embryo sac within the ovule. In the embryo sac, the tube nucleus disintegrates and the tip of the pollen tube bursts, releasing the 2 male nuclei. One male nuclei fuses with the egg nucleus to make a zygote and then divides by mitosis to become the embryo of the seed. The 2 nd male nucleus fuses with 2 other nuclei called polar nuclei at the centre of the embryo sac. This produces a cell with a large nucleus which divides to become a food store (endosperm) for the seed. This process is called a double fertilisation. Stem cell: An undifferentiated cell whose daughter may differentiate into many other cell types. Somatic stem cells exist in small numbers in grown adults. They are hard to extract and differentiate into a very limited number of cells hence being multipotent (less variation than pluripotent). They can be found in bone marrow and are hard to culture outside of the body. Stem cell cloning: adult stem cell is removed from the body and the nucleus is placed inside an empty ovum creating a new pre-embryo cell containing patient DNA. A mild electric shock is administered to stimulate mitosis and create a collection of embryonic stem cells with the patient DNA. Stem cells are then cultured into desired organ etc. The advantages are: reduced need for donors, reduced rejection, and cure diseases. Disadvantages are: we currently are not sure how to properly perform the procedure, concerns that the treatment causes late onset cancer. Immunosuppressant. Totipotent cell: Totipotent cells have the ability to keep differentiating into an entire organism. For a cell to be totipotent it must have the capacity, present in the cells of an embryo, to develop into any type of cell with none of its genes switched of permanently. Plant cells are totipotent during their entire lifetime. Embryonic stem cells are usually totipotent until the blastocyst state, when the embryo would implant in its mothers uterus, where the inner cells become pluripotent. Pluripotent cell: Refers to a stem cell that has the potential to differentiate into any of the three germ layers: endoderm (interior stomach lining, gastrointestinal tract, the lungs), mesoderm (muscle, bone, blood, urogenital), or ectoderm (epidermal tissues and nervous system. Pluripotent stem cells can give rise to any foetal or adult cell type. However, alone they cannot develop into a foetal or adult animal as they lack the potential to give rise to extra embryonic tissue, such as the placenta. These can usually be found in adult stem cells, which are located in the bone marrow. The blood that drains from the placenta and umbilical cord after birth is a rich source of pluripotent stem cells. If this blood is frozen and stored it can later be used for the treatment of the child - or their family - should they need them for any specific reason. However there are several problems, firstly it would take a lot of storage space to do this for everyone which means huge financial funding. Secondly there is evidence that suggests that the precursor cells of conditions such as leukaemia are already present in the blood at birth, therefore because the benefits are as yet largely unproven, the only way parents can do this in the UK is to pay around 500 pounds to do it privately. Parkinson's Disease - A brain disorder that stops nerve cells from working as they don't produce dopamine neurones, scientists hope that stem cell treatment will allow them to replace the lost brain cells and restore dopamine production, letting people return to a normal life. Diabetes - Type 1 diabetes usually develops when people are young; the insulin secreting cells in the pancreas are destroyed or stop making insulin, so the blood glucose concentration is uncontrolled. Although insulin injections work well enough, people affected by diabetes have to monitor their food intake. Stem cell therapy could give them working pancreas cells again, restoring insulin production and blood glucose control. Cellular differentiation: the process by which a less specialized cell becomes a more specialized cell type. Differentiation occurs numerous times during the development of a multicellular organism as the organism changes from a simple zygote to a complex system of tissues and cell types. Differentiation is a common process in adults as well; adult stem cells divide and create fully-differentiated daughter cells during tissue repair and during normal cell replacement. Differentiation dramatically changes a cell's size, shape, membrane potential, metabolic activity, and responsiveness to signals. These changes are largely due to highly-controlled modifications in gene expression, as selected mRNA produces certain proteins, which changes the cells complexion - therefore differentiating it. With a few exceptions, cellular differentiation almost never involves a change in the DNA sequence itself. Thus, different cells can have very different physical characteristics despite having the same genome. A cell that is able to differentiate into all cell types of the adult organism is known as pluripotent. Such cells are called embryonic stem cells in animals and meristematic cells in higher plants. A cell that is able to differentiate into all cell types, including the placental tissue, is known as totipotent. In mammals, only the zygote and subsequent blastomeres are totipotent, while in plants many differentiated cells can become totipotent with simple laboratory techniques. In cytopathology, the level of cellular differentiation is used as a measure of cancer progression. Genetic Terms: Allele- this is a different version of a gene. Most plants, all humans and animals have two copies of each gene, one from each parent - this is called diploid. The two copies can be the same or different. When they are the same the organism is called a homozygote and when they are different it is called a heterozygote. Different alleles have different base sequences, which code for different versions of the same characteristics. Phenotype- the characteristics the alleles produce. Genotype- the alleles a person has. Variation in phenotype- The variation in phenotype is largely influenced by the genotypes. A variation in genotype results in a variation in phenotype. There are some characteristics that are only controlled by one gene. These are called monogenic characteristics. However, most characteristics are controlled by a number of genes; they are stated to be polygenic. The Environment- There are some characteristics that are only influenced by genotype, e.g. blood group; however the majority of characteristics are influence by both the genotype and the environment.
1. Height- this is polygenic and affected by environmental factors. It is mostly determined by a persons genotype, for example tall parents usually have tall children. However, malnourishment can cause children to not reach their maximum height because protein is required for growth. 2. Monoamine Oxidase A(MAOA)-this is an enzyme used to hydrolyse monoamines in humans. The production of this enzyme is caused by a single gene, but environmental factors such as smoking tobacco can reduce the amount produced, causing low levels of MAOA. Low levels of MAOA are linked with mental health problems. 3. Cancer- this is when cells dont stop dividing leading to tumours (lumps of cells) forming. The risk of developing cancer is affected by both genes and environmental factors such as diet. 4. Animal hair colour- this is polygenic. However, the environment affects the hair colour for some animals. For example, some arctic animals have adapted to have dark hair in summer and white hair in winter. This is triggered by environmental factors such as temperature change; however, this is not possible if the animal does not have the genes for it.