key term - Cell Cycle Checkpoints

5 Must Know Facts For Your Next Test

1. There are three main checkpoints in the cell cycle: G1 checkpoint, G2 checkpoint, and M checkpoint, each serving specific functions in monitoring the cell's readiness to proceed.
2. The G1 checkpoint checks for DNA damage, nutrient availability, and growth signals, ensuring conditions are favorable for DNA replication.
3. The G2 checkpoint verifies that DNA has been accurately replicated and checks for DNA damage before allowing the cell to enter mitosis.
4. The M checkpoint, also known as the spindle checkpoint, ensures that all chromosomes are properly attached to the spindle apparatus before the cell divides.
5. If a cell does not meet the necessary criteria at a checkpoint, it may enter a resting state (G0 phase) or undergo apoptosis to prevent potential malignancies.

Review Questions

• How do cell cycle checkpoints contribute to preventing cancer?
  • Cell cycle checkpoints act as critical regulatory mechanisms that monitor key processes during the cell cycle. By assessing DNA integrity and ensuring proper chromosome alignment before division, these checkpoints help prevent the proliferation of cells with genetic abnormalities. If a checkpoint detects issues like DNA damage, it can halt the cycle or trigger apoptosis, thereby reducing the risk of cancerous growths.
• Discuss the roles of cyclins and cyclin-dependent kinases (CDKs) in relation to cell cycle checkpoints.
  • Cyclins are proteins that bind to and activate cyclin-dependent kinases (CDKs), which are essential for driving progression through various phases of the cell cycle. Each checkpoint is associated with specific cyclin-CDK complexes that need to be activated for the cell to proceed. For instance, if DNA damage is detected at the G1 checkpoint, specific cyclins will not activate their CDKs, preventing further progress until repairs are made.
• Evaluate how failures in cell cycle checkpoints can lead to cancer development and discuss potential therapeutic strategies targeting these failures.
  • Failures in cell cycle checkpoints can allow cells with damaged DNA or improper chromosome segregation to continue dividing unchecked, which can lead to tumorigenesis. Mutations in tumor suppressor genes that regulate these checkpoints often result in a loss of function, eliminating the control over cell division. Therapeutic strategies targeting these failures may include developing drugs that restore checkpoint function or induce apoptosis in aberrant cells. Additionally, gene therapy could be utilized to correct mutations in tumor suppressor genes, enhancing cellular surveillance against cancer.