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The Cell Cycle Chapter 12
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Overview: The Key Roles of Cell Division
The ability of organisms to reproduce best distinguishes living things from nonliving matter The continuity of life is based on the reproduction of cells, or cell division
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Multicellular organisms depend on cell division for:
In unicellular organisms, division of one cell reproduces the entire organism Multicellular organisms depend on cell division for: Development from a fertilized cell Growth Repair Cell division is an integral part of the cell cycle, the life of a cell from formation to its own division
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(a) Reproduction (b) Growth and development (c) Tissue renewal 100 µm
Fig. 12-2 100 µm 200 µm 20 µm (a) Reproduction (b) Growth and development (c) Tissue renewal Figure 12.2 The functions of cell division
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12.1: Cell division produces genetically identical daughter cells
Most cell division results in daughter cells with identical genetic information, DNA A special type of division produces nonidentical daughter cells (gametes, or sperm and egg cells)
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Organization of the Genetic Material
All the DNA in a cell constitutes the cell’s genome A genome can consist of a single DNA molecule (common in prokaryotic cells) or a number of DNA molecules (common in eukaryotic cells) DNA molecules in a cell are packaged into chromosomes
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Fig. 12-3 Figure 12.3 Eukaryotic chromosomes 20 µm
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Every eukaryotic species has a characteristic number of chromosomes in each cell nucleus
Somatic cells (nonreproductive cells) have two sets of chromosomes Gametes (reproductive cells: sperm and eggs) have half as many chromosomes as somatic cells Eukaryotic chromosomes consist of chromatin, a complex of DNA and protein that condenses during cell division
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Distribution of Chromosomes During Eukaryotic Cell Division
In preparation for cell division, DNA is replicated and the chromosomes condense Each duplicated chromosome has two sister chromatids, which separate during cell division The centromere is the narrow “waist” of the duplicated chromosome, where the two chromatids are most closely attached
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0.5 µm Chromosomes DNA molecules Chromo- some arm Chromosome
Fig. 12-4 0.5 µm Chromosomes DNA molecules Chromo- some arm Chromosome duplication (including DNA synthesis) Centromere Sister chromatids Figure 12.4 Chromosome duplication and distribution during cell division Separation of sister chromatids Centromere Sister chromatids
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Eukaryotic cell division consists of:
Mitosis – division of the nuclear DNA Cytokinesis, the division of the cytoplasm Gametes are produced by a variation of cell division called meiosis Meiosis yields nonidentical daughter cells that have only one set of chromosomes, half as many as the parent cell
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12.2: The mitotic phase alternates with interphase in the cell cycle
Phases of the Cell Cycle The cell cycle consists of Mitotic (M) phase (mitosis and cytokinesis) Interphase (cell growth and copying of chromosomes in preparation for cell division)
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Interphase (about 90% of the cell cycle) is divided into three subphases:
G1 phase (“first gap”) S phase (“synthesis”) G2 phase (“second gap”) The cell grows during all three phases, but chromosomes are duplicated only during the S phase
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S (DNA synthesis) G1 Cytokinesis G2 Mitosis
Fig. 12-5 INTERPHASE S (DNA synthesis) G1 Cytokinesis G2 Mitosis Figure 12.5 The cell cycle MITOTIC (M) PHASE
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Mitosis is conventionally divided into five phases:
Prophase Prometaphase Metaphase Anaphase Telophase Cytokinesis occurs during late telophase For the Cell Biology Video Myosin and Cytokinesis, go to Animation and Video Files.
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Chromosome, consisting of two sister chromatids
Fig. 12-6b G2 of Interphase Prophase Prometaphase Centrosomes (with centriole pairs) Chromatin (duplicated) Early mitotic spindle Aster Centromere Fragments of nuclear envelope Nonkinetochore microtubules Figure 12.6 The mitotic division of an animal cell Nucleolus Nuclear envelope Plasma membrane Chromosome, consisting of two sister chromatids Kinetochore Kinetochore microtubule
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Telophase and Cytokinesis
Fig. 12-6d Metaphase Anaphase Telophase and Cytokinesis Metaphase plate Cleavage furrow Nucleolus forming Figure 12.6 The mitotic division of an animal cell Daughter chromosomes Nuclear envelope forming Spindle Centrosome at one spindle pole
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The Mitotic Spindle The mitotic spindle is composed of microtubules which controls chromosome movement during mitosis During prophase, assembly of spindle microtubules begins in the centrosome, the microtubule organizing center The centrosome replicates, forming two centrosomes that migrate to opposite ends of the cell, as spindle microtubules grow out from them For the Cell Biology Video Spindle Formation During Mitosis, go to Animation and Video Files.
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An aster (a radial array of short microtubules) extends from each centrosome
The spindle includes the centrosomes, the spindle microtubules, and the asters
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During prometaphase, some spindle microtubules attach to the centromere kinetochores of the chromosomes and begin to move the chromosomes At metaphase, the chromosomes are all lined up at the metaphase plate, the midway point between the spindle’s two poles
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Microtubules Chromosomes
Fig. 12-7 Aster Centrosome Sister chromatids Microtubules Chromosomes Metaphase plate Kineto- chores Centrosome 1 µm Figure 12.7 The mitotic spindle at metaphase Overlapping nonkinetochore microtubules Kinetochore microtubules 0.5 µm
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The microtubules shorten by depolymerizing at their kinetochore ends
In anaphase, sister chromatids separate and move along the kinetochore microtubules toward opposite ends of the cell The microtubules shorten by depolymerizing at their kinetochore ends For the Cell Biology Video Microtubules in Anaphase, go to Animation and Video Files.
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EXPERIMENT RESULTS CONCLUSION Kinetochore Spindle pole Mark Chromosome
Fig. 12-8 EXPERIMENT Kinetochore Spindle pole Mark RESULTS Figure 12.8 At which end do kinetochore microtubules shorten during anaphase? CONCLUSION Chromosome movement Kinetochore Motor protein Tubulin subunits Microtubule Chromosome
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Chromosome movement Kinetochore Tubulin Motor Subunits Microtubule
Fig. 12-8b CONCLUSION Chromosome movement Kinetochore Tubulin Subunits Motor protein Microtubule Figure 12.8 At which end do kinetochore microtubules shorten during anaphase? Chromosome
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Nonkinetochore microtubules from opposite poles overlap and push against each other, elongating the cell In telophase, the nuclear envelope reforms around genetically identical daughter nuclei at opposite ends of the cell For the Cell Biology Video Microtubules in Cell Division, go to Animation and Video Files.
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Cytokinesis In animal cells, cytokinesis occurs by a process known as cleavage, forming a cleavage furrow In plant cells, a cell plate forms during cytokinesis
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10 µm Fig. 12-10 Nucleus Chromatin condensing Nucleolus Chromosomes
Cell plate Figure Mitosis in a plant cell 1 Prophase 2 Prometaphase 3 Metaphase 4 Anaphase 5 Telophase
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Nucleus 1 Prophase Chromatin condensing Nucleolus Fig. 12-10a
Figure Mitosis in a plant cell 1 Prophase
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Chromosomes 2 Prometaphase Fig. 12-10b
Figure Mitosis in a plant cell 2 Prometaphase
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Fig c Figure Mitosis in a plant cell 3 Metaphase
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Fig d Figure Mitosis in a plant cell 4 Anaphase
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10 µm Cell plate 5 Telophase Fig. 12-10e
Figure Mitosis in a plant cell 5 Telophase
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Binary Fission Prokaryotes (bacteria and archaea) reproduce by a type of cell division called binary fission In binary fission, the chromosome replicates (beginning at the origin of replication), and the two daughter chromosomes actively move apart
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Cell wall Origin of replication Plasma membrane E. coli cell Bacterial
Fig Cell wall Origin of replication Plasma membrane E. coli cell Bacterial chromosome Two copies of origin Figure Bacterial cell division by binary fission
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Cell wall Origin of replication Plasma membrane E. coli cell Bacterial
Fig Cell wall Origin of replication Plasma membrane E. coli cell Bacterial chromosome Two copies of origin Origin Origin Figure Bacterial cell division by binary fission
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Cell wall Origin of replication Plasma membrane E. coli cell Bacterial
Fig Cell wall Origin of replication Plasma membrane E. coli cell Bacterial chromosome Two copies of origin Origin Origin Figure Bacterial cell division by binary fission
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Cell wall Origin of replication Plasma membrane E. coli cell Bacterial
Fig Cell wall Origin of replication Plasma membrane E. coli cell Bacterial chromosome Two copies of origin Origin Origin Figure Bacterial cell division by binary fission
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The Evolution of Mitosis
Since prokaryotes evolved before eukaryotes, mitosis probably evolved from binary fission Certain protists exhibit types of cell division that appears to be an intermediate between binary fission and mitosis
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12.3: Control of the Cell Cycle
The frequency of cell division varies depending on the type of cell These differences result from regulation of the cell cycle at the molecular level
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The Cell Cycle Control System
The sequential events of the cell cycle are directed by a distinct cell cycle control system, which is similar to a clock The cell cycle control system is regulated by both internal and external controls The clock has specific checkpoints where the cell cycle stops until a go-ahead signal is received
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G1 checkpoint Control system S G1 G2 M M checkpoint G2 checkpoint
Fig G1 checkpoint Control system S G1 G2 M Figure Mechanical analogy for the cell cycle control system M checkpoint G2 checkpoint
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For many cells, the G1 checkpoint seems to be the most important one
If a cell receives a go-ahead signal at the G1 checkpoint, it will usually complete the S, G2, and M phases and divide If the cell does not receive the go-ahead signal, it will exit the cycle, switching into a nondividing state called the G0 phase
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G0 G1 G1 G1 checkpoint (b) Cell does not receive a go-ahead signal
Fig G0 G1 checkpoint Figure The G1 checkpoint G1 G1 Cell receives a go-ahead signal (b) Cell does not receive a go-ahead signal
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Cyclins and Cyclin-Dependent Kinases
Two types of regulatory proteins are involved in cell cycle control: cyclins and cyclin-dependent kinases (Cdks) The activity of cyclins and Cdks fluctuates during the cell cycle MPF (maturation-promoting factor) is a cyclin-Cdk complex that triggers a cell’s passage past the G2 checkpoint into the M phase
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M G1 S G2 M G1 S G2 M G1 Fig. 12-17 MPF activity Cyclin concentration
Time (a) Fluctuation of MPF activity and cyclin concentration during the cell cycle G1 S Cdk Figure Molecular control of the cell cycle at the G2 checkpoint Cyclin accumulation M Degraded cyclin G2 G2 Cdk Cyclin is degraded checkpoint Cyclin MPF (b) Molecular mechanisms that help regulate the cell cycle
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(b) Molecular mechanisms that help regulate the cell cycle
Fig b G1 S Cdk Cyclin accumulation M Degraded cyclin G2 G2 checkpoint Cdk Figure Molecular control of the cell cycle at the G2 checkpoint Cyclin is degraded Cyclin MPF (b) Molecular mechanisms that help regulate the cell cycle
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Stop and Go Signs: Internal and External Signals at the Checkpoints
An example of an internal signal is that kinetochores not attached to spindle microtubules send a molecular signal that delays anaphase Some external signals are growth factors, proteins released by certain cells that stimulate other cells to divide For example, platelet-derived growth factor (PDGF) stimulates the division of human fibroblast cells in culture
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Scalpels Petri plate Without PDGF cells fail to divide With PDGF
Fig Scalpels Petri plate Without PDGF cells fail to divide Figure The effect of a growth factor on cell division With PDGF cells prolifer- ate Cultured fibroblasts 10 µm
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Another example of external signals is density-dependent inhibition, in which crowded cells stop dividing Most animal cells also exhibit anchorage dependence, in which they must be attached to a substratum in order to divide
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Density-dependent inhibition
Fig Anchorage dependence Density-dependent inhibition Density-dependent inhibition Figure Density-dependent inhibition and anchorage dependence of cell division 25 µm 25 µm (a) Normal mammalian cells (b) Cancer cells
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Cancer cells exhibit neither density-dependent inhibition nor anchorage dependence
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Cancer: Is the Loss of Control of the Cell Cycle
Cancer cells do not respond to the body’s control mechanisms Cancer cells may not need growth factors to grow and divide: They may make their own growth factor They may relay a growth factor’s signal without the presence of the growth factor They may have an abnormal cell cycle control system
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A normal cell is converted to a cancerous cell by a process called transformation
Cancer cells form tumors, masses of abnormal cells within otherwise normal tissue If abnormal cells remain at the original site, the lump is called a benign tumor Malignant tumors invade surrounding tissues and can metastasize, exporting cancer cells to other parts of the body, where they may form secondary tumors
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Lymph vessel Tumor Blood vessel Cancer cell Glandular tissue
Fig Lymph vessel Tumor Blood vessel Cancer cell Glandular tissue Metastatic tumor 1 A tumor grows from a single cancer cell. 2 Cancer cells invade neigh- boring tissue. 3 Cancer cells spread to other parts of the body. 4 Cancer cells may survive and establish a new tumor in another part of the body. Figure The growth and metastasis of a malignant breast tumor
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REVIEW
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G1 S Cytokinesis Mitosis G2 MITOTIC (M) PHASE Prophase Telophase and
Fig. 12-UN1 INTERPHASE G1 S Cytokinesis Mitosis G2 MITOTIC (M) PHASE Prophase Telophase and Cytokinesis Prometaphase Anaphase Metaphase
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Fig. 12-UN2
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Fig. 12-UN3
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Fig. 12-UN4
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Fig. 12-UN5
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Fig. 12-UN6
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You should now be able to:
Describe the structural organization of the prokaryotic genome and the eukaryotic genome List the phases of the cell cycle; describe the sequence of events during each phase List the phases of mitosis and describe the events characteristic of each phase Draw or describe the mitotic spindle, including centrosomes, kinetochore microtubules, nonkinetochore microtubules, and asters
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Compare cytokinesis in animals and plants
Describe the process of binary fission in bacteria and explain how eukaryotic mitosis may have evolved from binary fission Explain how the abnormal cell division of cancerous cells escapes normal cell cycle controls Distinguish between benign, malignant, and metastatic tumors
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