Chapter 12 The Cell Cycle and Mitosis. The Key Roles of Cell Division Cell division functions in...
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Transcript of Chapter 12 The Cell Cycle and Mitosis. The Key Roles of Cell Division Cell division functions in...
![Page 1: Chapter 12 The Cell Cycle and Mitosis. The Key Roles of Cell Division Cell division functions in reproduction, growth, and repair Unicellular organisms.](https://reader036.fdocuments.in/reader036/viewer/2022081503/56649e355503460f94b238c9/html5/thumbnails/1.jpg)
Chapter 12
The Cell Cycle and Mitosis
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The Key Roles of Cell Division
Cell division functions in reproduction, growth, and repair
Unicellular organisms (ex. Amoeba) will divide to reproduce entire organisms
Cell division also will allows a multicellular organism to develop from a single cell
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The Key Roles of Cell Division
DNA is passed from one generation of cells to the next without dilution. -cell duplicates it DNA- moves the 2 copies to opposite ends of the cell- and then splits into 2 daughter cells
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The Key Roles of Cell Division
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Concept 12.1
Cell Division distributes identical sets of chromosomes to daughter cells
A cell’s genetic material is called its genome- prokaryote = single long DNA strand- eukaryote = number of DNA molecules
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Concept 12.1
The replication and distribution of DNA is manageable because it is packaged into chromosomes- the nuclei in human somatic cells contain 46 chromosomes- the nuclei in human gametes contains 23 chromosomes
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Concept 12.1
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Concept 12.1
The DNA-protein complex is called the chromatin and is a long thin fiber.
After the chromatin is duplicated, it will prepare for division. It will condense and coil up to form chromosomes.
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Concept 12.1
Each duplicated chromosome has 2 sister chromatids.- each contains identical copies of the chromosome’s DNA molecule- they are connected together at the centromere
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Concept 12.10.5 µm Chromosomes
Chromosomeduplication(including DNAsynthesis)
Chromo-some arm
Centromere
Sisterchromatids
DNA molecules
Separation ofsister chromatids
Centromere
Sister chromatids
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Concept 12.2
The mitotic phase alternates with interphase in the cell cycle
The mitotic (M) phase (mitosis and cytokenesis) is the shortest part of the cell cycle.
Interphase accounts for about 90% of the cell cycle.
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Concept 12.2
Interphase can be divided into subphases- G1 (first gap), S (synthesis), and G2 (second gap)- during subphases, cell grows by producing proteins and organelles- chromosomes are only duplicated during the S phase
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Concept 12.2
S(DNA synthesis)
MITOTIC(M) PHASE
Mito
sis
Cytokinesis
G1
G2
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Concept 12.2
Mitosis is broken down into 4 subphases- prophase, metaphase, anaphase, and telophase
Prophase- chromatin coil into chromosomes- nucleoli disappears- spindles begin to appear as centrosomes move to the poles of the cell
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Concept 12.2
The cell moves into prometaphase- nuclear envelope fragments- kinetochore attaches to forming spindles- cell prepares for metaphase
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Concept 12.2
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Concept 12.2
Metaphase- centrosomes area at opposite poles- chromosomes are on equator of cell, the metaphase plate
Anaphase- begins when the centromeres of the chromosomes separate
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Concept 12.2
- sister chromatids begin moving toward opposite poles- by the end, the poles have equal sets of chromosomes
Telophase- daughter nuclei form at the poles- nuclear envelope begins to reform
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Concept 12.2
- chromosomes become less tightly coiled
-Cytokenesis, the division of the cytoplasm, follows immediately
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Concept 12.2
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Concept 12.2
The mitotic spindle distributes chromosomes to the daughter cells-during interphase, the single centrosome replicates to form 2 centrosomes; during the early stage of mitosis, they separate and move toward opposite poles helping the spindle fibers
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Concept 12.2
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Concept 12.2
Cytokenesis divides the cytoplasm- in animals, cytokenesis occurs by the formation of a cleavage furrow- in plants the cleavage cannot occur because of the cell wall; vesicles will move to the center of the cell to form the cell plate.
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Concept 12.2
Cleavage furrow100 µm
Contractile ring ofmicrofilaments
Daughter cells
(a) Cleavage of an animal cell (SEM) (b) Cell plate formation in a plant cell (TEM)
Vesiclesformingcell plate
Wall ofparent cell
Cell plate
Daughter cells
New cell wall
1 µm
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Concept 12.2
The origins of mitosis are believed to be from bacterial organisms of cell reproduction- prokaryotes reproduce by binary fission (“dividing in half”)- prokaryotes do not have mitotic spindles; instead, once the DNA replicates, the copies of the region move apart rapidly
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Concept 12.2Origin ofreplication
Two copiesof origin
E. coli cell Bacterialchromosome
Plasmamembrane
Cell wall
Origin Origin
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Concept 12.3
The cell cycle is driven by specific chemical signals present in the cytoplasm
Sequential events of the cell cycle are directed by a distinct cell cycle control system- driven by a built in clock- the cell cycle is regulated at certain checkpoints by internal and external controls
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Concept 12.3
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The checkpoint is a control point where stop and go-ahead signals can regulate the cycle- kinases, a type of regulatory protein that activate or inactivate other proteins, give the signals for G1 and G2 checkpoints
Concept 12.3
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Concept 12.3
To be active the kinase must be attached to a cyclin (kinases become cyclin-dependent kinases or Cdks)- the activity of Cdks rises and falls with changes in the [cyclin]- first called MPF = “maturation promoting factor” or “M-phase-promoting factor”
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Concept 12.3
- when cyclins accumulate during G2, MPF initiates mitosis
Internal and external cues help regulate the cell cycle- for cells to divide a growth factor, a specific protein, is released to stimulate cell division
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Concept 12.3
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Concept 12.3
The discovery of growth factors has led us to understand density-dependent inhibition of cell division- when a cell population reaches a certain density, the amount of growth factors and nutrients needed for division becomes insufficient for increased growth
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Concept 12.3
Most animal cells also exhibit anchorage dependence- to divide, the cell must be attached to a substratum (ex. inside of a culture jar or extracellular matrix of a tissue)
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Concept 12.3
Anchorage dependence
Density-dependent inhibition
Density-dependent inhibition
(a) Normal mammalian cells (b) Cancer cells25 µm25 µm
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Concept 12.3
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Concept 12.3
Cancer cells have escaped from cell cycle controls- they do not respond to the control mechanisms- they do not stop dividing when growth factors are depleted; don’t respond to density dependant inhibition
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Concept 12.3
- if cancer cells stop dividing, it is at random points and not at the checkpoints
Caner begins when a single cell tissue undergoes a transformation- if the cell evades destruction by the immune system it may form a tumor
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Concept 12.3
- if the abnormal cell remain at the original site, it is called a benign tumor- a malignant tumor becomes invasive enough to impair the functions of organs- the spread of cancer cells from the original site is called metastasis
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Concept 12.3
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Concept 12.3