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Regulation of Cell Division

Regulation of Cell Division. Frequency of cell division. Varies with cell type Skin cells Divide frequently throughout life Liver cells Retain ability to divide Mature nerve cells & muscle cells Do not divide after maturity. Cell Cycle control. Two irreversible points in cell cycle

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Regulation of Cell Division

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  1. Regulation of Cell Division

  2. Frequency of cell division • Varies with cell type • Skin cells • Divide frequently throughout life • Liver cells • Retain ability to divide • Mature nerve cells & muscle cells • Do not divide after maturity

  3. Cell Cycle control • Two irreversible points in cell cycle • Replication of genetic material • Separation of sister chromatids • Cell can be put on hold at specificcheckpoints

  4. Checkpoint control system • Cell cycle controlled by STOP and GO chemical signals at critical points • Signals indicate if key cellular processes have been completed correctly • 3 major checkpoints

  5. Checkpoint Control System • G1 • Can DNA synthesis begin? • G2 • Has DNA synthesis been completed correctly? • Commitment to mitosis • M phases • Spindle checkpoint • Can sister chromatids separate correctly?

  6. G1 Checkpoint • G1 checkpoint is most critical • Primary decision point • “restriction point” • If cell receives “go” signal, it divides • If cell does not receive “go” signal, cell exits cycle & switches to Go phase • Non-dividing state

  7. G0 Phase • Non-dividing, differentiated state • Most human cells in Go phase • Liver cells • In G0, but can be “called back” to cell • Nerve & muscle cells • Highly specialized; arrested in G0 & can never divide

  8. Control of Cell Cycle

  9. Activation of Cell Division • How do cells know when to divide? • Cell communication = signals • Chemical signals in cytoplasm give cue • Signals usually mean proteins • Activators • inhibitors

  10. “Go-ahead” signals • Signals that promote cell growth & division • Proteins • Internal signals • “promoting factors” • External signals • “growth factors” • Primary mechanism of control • Phosphorylation • Kinase enzymes

  11. Protein signals – Promoting Factors • Cyclins • Regulatory proteins • Levels cycle in the cell • Cdks • Cyclin-dependentkinases • Enzyme activates cellular proteins • MPF • Maturation (mitosis) promoting factor • APC • Anaphase promoting complex

  12. Cyclins & Cdks (1970s-80s) • Interaction of Cdks & different cyclins triggers the stages of the cell cycle Leland H. Hartwell: checkpoints Sir Paul Nurse: cyclins Tim Hunt: Cdks

  13. Cyclin & cyclin dependent kinases • CDKs & cyclin drive cell from one phase to the next in the cell cycle • Genes for these regulatory proteins have been highly conserved through evolution • Proper regulation of cell cycle is key to life • These genes are basically the same in yeast, insects, plants, & animals

  14. External signals • Growth factors • Protein signals released by body cells that stimulate other cells to divide • Density-dependent inhibition • Crowded cells stop dividing • Mass of cells use up growth factors • Not enough left to trigger cell division • Anchorage dependence • To divide cells must be attached to a substrate

  15. Growth Factor Signals

  16. Example of a Growth Factor: Platelet Derived Growth Factor • Made by platelets • Binding of PDGF to cell receptors stimulates fibroblast cell division • Helps heal wounds

  17. Growth Factors and Cancer • Proto-oncogenes • Normal genes that become oncogenes (cancer-causing) when mutated • Stimulates cell growth • If switched on cancause cancer • Ex.: RAS (activates cyclins) • Tumor-suppressor genes • Inhibit cell division • If switched off can cause cancer • Ex.: p53 – The cell cycle enforcer – discovered at Stony Brook by Dr. Arnold Levine

  18. Cancer & Cell Growth • Cancer is essentially a failure of cell division control • Unrestrained, uncontrolled cell growth • What control is lost? • Checkpoint stops • Gene p53 plays a key role in G1 checkpoint • p53 protein halts cell division if it detects damaged DNA • Stimulates repair enzymes to fix DNA • Forces cell into G0 resting stage • Keeps cell in G1 arrest • Causes apoptosis of damaged cell • All cancers have to shut down p53 activity

  19. Development of Cancer • Cancer develops only after a cell experiences ~ 6 key mutations (“hits”) • Unlimited growth • Turn ongrowth promoter genes • Ignore checkpoints • Turn off tumor suppressor genes • Escape apoptosis • Turn off suicide genes • Immortality = unlimited divisions • Turn on chromosome maintenance genes • Promotes blood vessel growth • Turn on blood vessel growth genes • Overcome anchor & density dependence • Turn off censor gene

  20. UV radiation Chemical exposure Radiation exposure Heat Cigarette smoke Pollution Age Genetics “Hits” can be triggered by…

  21. Tumors – mass of abnormal cells • Benign tumor • Abnormal cells remain at original sit as a lump • P53 has halted cell division • Most do not cause serious problems & can be removed by surgery • Malignant tumor • Cells leave original site • Lose attachment to nearby cells • Carried by blood & lymph system to other tissues • Start more tumors = metastasis • Impair functions of organs throughout body

  22. Traditional treatments for cancer • Treatments target rapidly dividing cells • High energy radiation & chemotherapy with toxic drugs

  23. New “Miracle Drugs” • Drugs targeting proteins (enzymes) found only in tumor cells • Gleevec • Treatment for adult leukemia & stomach cancer • 1st successful targeted drug

  24. Cancers = cell cycle genes • Cancer results from genetic changes that affect the cell cycle • Proto-oncogenes • Normal cellular genes code for proteins that stimulate normal cell growth & division • Oncogenes • Mutations that alter proto-oncogenes cause them to become cancer-causing genes

  25. Proto-oncogenes & oncogenes • Genetic change that can turn proto-oncogenes into oncogenes • Removing repression of genes

  26. Cancers = failures of regulation • Cancer cells have escaped cell cycle controls • Do not respond normally to the body’s control mechanisms • Divide excessively & invade other tissues • If unchecked, they can kill the organism

  27. Effects of signal pathways

  28. Multi-step model for cancer • Multiple mutations underlie the development of cancer • Several changes must occur at DNA level for cell to become fully cancerous • Including at least 1 active oncogene & mutation or loss of several tumor-suppressor genes • Telomerase is often activated

  29. p53 gene • “Guardian of the Genome” • The “anti-cancer gene” • After DNA damage is detected, p53 initiates: • DNA repair • Growth arrest • apoptosis • Almost all cancers have mutations in p53

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