Hallmarks of Cancer I (Jahn) PDF
Document Details
University of Florida
Stephan C. Jahn, Ph.D.
Tags
Summary
These lecture notes cover the hallmarks of cancer, exploring the mechanisms that drive uncontrolled cell growth. The document delves into concepts such as cell signaling, mutations, and tumor suppressor proteins like p53 and Rb, providing insights into the intricacies of cancer development. The presentation is well-structured, allowing for a clear understanding of the key processes in the progression of cancer.
Full Transcript
The Hallmarks of Cancer Stephan C. Jahn, Ph.D. So… What IS cancer? Cancer is essentially a cell gone rogue. What makes a cell go rogue? Cells normally only grow when told to Gas pedal Cells normally stop when they need to Brakes DNA mutations make incorrect proteins...
The Hallmarks of Cancer Stephan C. Jahn, Ph.D. So… What IS cancer? Cancer is essentially a cell gone rogue. What makes a cell go rogue? Cells normally only grow when told to Gas pedal Cells normally stop when they need to Brakes DNA mutations make incorrect proteins Gas pedal gets stuck Brakes don’t work The Hallmarks of Cancer Hanahan, D. and Weinberg, R. The Hallmarks of Cancer, Cell (2000) 100, p. 57-70 Hanahan, D. and Weinberg, R. Hallmarks of Cancer: The Next Generation, Cell (2011) 144, p. 646-674 Hallmark #1: Self-Sufficiency in Growth Signals Cell growth is normally tightly regulated, requiring a pro-growth signal. Cancer cells bypass this requirement in a number of ways George Weller [CC BY-SA 3.0 (https://creativecommons.org/licenses/by-sa/3.0)], from Wikimedia Commons An Introduction to Cell Signaling Pro-growth molecule (ligand) binds to extracellular domain Intracellular domain becomes active Signaling cascade proceeds Pro-growth proteins are transcribed Mechanisms to Become Self Sufficient Abnormal ligand production, autocrine (self) signaling Induced paracrine (external) signaling Upregulated receptor levels Mutation-induced constitutive signaling Yuji Miyamoto, Koichi Suyama and Hideo Baba [CC BY-SA 4.0 (https://creativecommons.org/licenses/by-sa/4.0)], via Wikimedia Commons Ras Signaling Yuji Miyamoto, Koichi Suyama and Hideo Baba [CC BY-SA 4.0 (https://creativecommons.org/licenses/by-sa/4.0)], via Wikimedia Commons Mutations in Ras Mutations in Ras are found in 20-30% of all cancers Point mutations in Ras are the most common abnormality in proto-oncogenes G12V mutation blocks GAP binding, locking Ras in it’s active state Q61K mutation raises the activation energy of GTP hydrolysis, blocking it Hallmark #2: Insensitivity to Anti- Growth Signals Normal cells need to overcome anti- growth signals in order to divide Anti-growth signals can be both normal and/or induced Anti-growth signals can originate either internally or externally The Tumor Suppressor p53 Transcription Mechanisms of p53 Inactivation >50% of tumors contain a mutation or deletion of p53 R72P mutation blocks DNA binding The Tumor Suppressor Rb George Weller [CC BY-SA 3.0 (https://creativecommons.org/licenses/by-sa/3.0)], from Wikimedia Commons The Tumor Suppressor Rb CNX OpenStax [CC BY 4.0 (https://creativecommons.org/licenses/by/4.0)], via Wikimedia Commons Mechanisms for Disregulation of Rb Mutant Rb Protein is present, but unable to bind E2F Downregulated Rb Protein is underexpressed, leaving unbound E2F Overactive Cdks Wild-type protein is normally expressed, but is constitutively hyperphosphorylated, inactivating it Contact Inhibition Takai et al., Nature Reviews Molecular Cell Biology. 9.8 (Aug. 2008):
