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CANCER POINT MUTATIONS DNA AMPLIFICATION EPIGENETIC MUTATIONS CHROMOSOMAL REARRANGEMENT MUTATIONS CAUSE ACTIVATION OF ONCOGENES INACTIVATION OF TUMOUR SUPRESSOR GENES
RAS Growth factor receptor Activated P P P Transcription factor activated P Cyclin , CDK RAS GENE’S GENERAL WORKING
RAS PROTEINS  RAS is a group of proteins that include – KRAS, KRASB, HRAS, NRAS.  These proteins are GTPases that remove gamma phosphate of GTP to give GDP.  About 89% of human cancers are caused by KRAS G12C mutations.  G12C = A single point mutation with a glycine-to-cysteine substitution at codon 12.  G12C mutations makes KRAS lose its GTPase activity .  This locks KRAS in the GTP bound state and it remains active.  The mutant cysteine KRAS G12C creates a narrow pocket that is susceptible to targeting.  It is hypothesized that an adjacent histidine 95 (H95) residue may provide a site to stabilize drug-protein interactions.  Sotorasib and Adagrasib bind covalently to cysteine.  These inhibitors lock KRAS G12C in inactive state thereby blocking the oncogenic signalling. Sotorasib Adagrasib
mTOR • mTOR: Mammalian target of rapamycin • Regulates: Cell proliferation, autophagy, gene transcription, protein, lipid, nucleotide synthesis, immune cell differentiation. • Associates: Cancer, tumor metabolism, insulin resistance other diseases. • “Rapamycin can affect translation by inhibiting the activity of mTOR, a protein kinase that plays a crucial role in regulating protein synthesis”. I Want to enter in mTOR pathway R
mTORC1 mTOR mTORC2 Raptor GβL Deptor Rictor GβL Deptor PRR5 SIN1 • The mTOR complexes affect translation by phosphorylation of multiple translation factors, including eIF4G. • The mTOR gene itself mutated in cancer.
• mTORC1 is the complex that is primarily inhibited by rapamycin, and it is involved in regulating protein synthesis, autophagy, and lipid metabolism. • mTORC2, involved in regulating cell survival, proliferation, and metabolism. • mTOR is involved in a variety of signaling pathways that regulate cellular metabolism, growth, and survival. mTOR PI3K/Akt- pathways mTOR C1 Increase protein synthesis and cell growth P mTOR AMPK pathways mTOR C1 decrease protein synthesis mTOR mTOR TGF β pathways Insulin pathways mTOR C1 Increases protein synthesis mTOR C1 Increased protein synthesis and lipid synthesis
CONCLUSIONS • Targeting these central cellular processes has advantage to be more directed to cancer cells than non-specific chemotherapeutics agents. • On the side disadvantages, targeting transcription and translation may affect multiple pathways. • Probability of killing healthy cells is lower with targeted therapies than with the general chemotherapeutics. • The role of CDK inhibitor are not limited to cancer diseases but also other diseases such as in HIV. • The large number of proteins involved will continue to provide drug development possibilities far into the future so that specific and effective treatment can be achieved.
References: • https://pubmed.ncbi.nlm.nih.gov// • https://youtu.be/1mo80kTZgW4 • https://cellandbioscience.biomedcentral.com/articles/10.1186/s13578- 020-00396-1 • https://www.medchemexpress.com/cx-5461.html THANK YOU

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BIOLOGY 2024.pdf

  • 1. CANCER POINT MUTATIONS DNA AMPLIFICATION EPIGENETIC MUTATIONS CHROMOSOMAL REARRANGEMENT MUTATIONS CAUSE ACTIVATION OF ONCOGENES INACTIVATION OF TUMOUR SUPRESSOR GENES
  • 2. RAS Growth factor receptor Activated P P P Transcription factor activated P Cyclin , CDK RAS GENE’S GENERAL WORKING
  • 3. RAS PROTEINS  RAS is a group of proteins that include – KRAS, KRASB, HRAS, NRAS.  These proteins are GTPases that remove gamma phosphate of GTP to give GDP.  About 89% of human cancers are caused by KRAS G12C mutations.  G12C = A single point mutation with a glycine-to-cysteine substitution at codon 12.  G12C mutations makes KRAS lose its GTPase activity .  This locks KRAS in the GTP bound state and it remains active.  The mutant cysteine KRAS G12C creates a narrow pocket that is susceptible to targeting.  It is hypothesized that an adjacent histidine 95 (H95) residue may provide a site to stabilize drug-protein interactions.  Sotorasib and Adagrasib bind covalently to cysteine.  These inhibitors lock KRAS G12C in inactive state thereby blocking the oncogenic signalling. Sotorasib Adagrasib
  • 4. mTOR • mTOR: Mammalian target of rapamycin • Regulates: Cell proliferation, autophagy, gene transcription, protein, lipid, nucleotide synthesis, immune cell differentiation. • Associates: Cancer, tumor metabolism, insulin resistance other diseases. • “Rapamycin can affect translation by inhibiting the activity of mTOR, a protein kinase that plays a crucial role in regulating protein synthesis”. I Want to enter in mTOR pathway R
  • 5. mTORC1 mTOR mTORC2 Raptor GβL Deptor Rictor GβL Deptor PRR5 SIN1 • The mTOR complexes affect translation by phosphorylation of multiple translation factors, including eIF4G. • The mTOR gene itself mutated in cancer.
  • 6. • mTORC1 is the complex that is primarily inhibited by rapamycin, and it is involved in regulating protein synthesis, autophagy, and lipid metabolism. • mTORC2, involved in regulating cell survival, proliferation, and metabolism. • mTOR is involved in a variety of signaling pathways that regulate cellular metabolism, growth, and survival. mTOR PI3K/Akt- pathways mTOR C1 Increase protein synthesis and cell growth P mTOR AMPK pathways mTOR C1 decrease protein synthesis mTOR mTOR TGF β pathways Insulin pathways mTOR C1 Increases protein synthesis mTOR C1 Increased protein synthesis and lipid synthesis
  • 7. CONCLUSIONS • Targeting these central cellular processes has advantage to be more directed to cancer cells than non-specific chemotherapeutics agents. • On the side disadvantages, targeting transcription and translation may affect multiple pathways. • Probability of killing healthy cells is lower with targeted therapies than with the general chemotherapeutics. • The role of CDK inhibitor are not limited to cancer diseases but also other diseases such as in HIV. • The large number of proteins involved will continue to provide drug development possibilities far into the future so that specific and effective treatment can be achieved.
  • 8. References: • https://pubmed.ncbi.nlm.nih.gov// • https://youtu.be/1mo80kTZgW4 • https://cellandbioscience.biomedcentral.com/articles/10.1186/s13578- 020-00396-1 • https://www.medchemexpress.com/cx-5461.html THANK YOU