SlideShare a Scribd company logo

Cancer Cell Division & Genes

Download as PPTX, PDF
R
rakhavem

Cancer is not a single disease but rather a heterogeneous group of disorders characterized by uncontrolled cell division. Normal cells grow in an organized pattern whereas cancer cells grow disorganized in clumps. Malignant cell transformation requires multiple genetic alterations and involves initiation and promotion phases. Tumor suppressor genes and oncogenes play key roles in cancer development. Tumor suppressor genes normally inhibit cell growth but require both copies to be mutated to lose function, while oncogenes promote cell growth when mutated. The p53 protein encoded by the TP53 tumor suppressor gene prevents uncontrolled cell division in damaged cells. Loss of function in tumor suppressor genes and gain of function in oncogenes can lead to cancer development.

Education
1 of 47
Cancer…
Licentious division - prostate cancer cells durin Cancer not a single disease; heterogeneous group of disorders characterized by the presence of cells that do not respond to the normal controls on division.
Normal cells
Cancer cells
Normal cells grow in monolayer Cancer cells grow in clumps (foci) COURTESY OF G. STEVEN MARTIN.)
Angiogenesis
Metastasis
Why a greater number of cells do not give rise to cancerous tumors ….???
> malignant transformation requires more than a single genetic alteration(hits).
How is a normal cell transformed into a cancerous cell?
Rather than lacking function, cancer cells reproduce at a rate far beyond the normally tightly regulated boundaries of the cell cycle. occur due to an alteration of a normal biological process — cell division.
MALIGNANT TRANSFORMATION OF CELLS
Induction of malignant transformation with chemical or physical carcinogens appears to involve multiple steps and at least two distinct phases: initiation and promotion.
The signals that regulate cell division fall into two basic types: molecules that stimulate cell division and those that inhibit it.
Genes that have been implicated in carcinogenesis are divided into two broad categories: Tumor-suppressor genes and Oncogenes.
Tumor-suppressor genes  Encode proteins that restrain cell growth and prevent cells from becoming malignant.  Act recessively since both copies must be deleted or mutated before their protective function is lost.
Oncogenes > Encode proteins that promote the loss of growth control and malignancy. Oncogenes arise from Proto-oncogenes—genes that encode proteins having a role in a cell’s normal activities.  Mutations that alter either the protein or its expression cause the proto-oncogene to act abnormally and promote the formation of a tumor.
MESSAGE The proteins that oncogenes encode are activated in tumor cells, whereas the proteins that tumor suppressor genes encode are inactivated.
Tumor suppressor genes
Five broad classes of proteins are generally recognized as being encoded by tumor- suppressor genes Intracellular proteins that regulate or inhibit progression through a specific stage of the cell cycle (e.g., p16 and Rb) Receptors or signal transducers for secreted hormones or developmental signals that inhibit cell proliferation (e.g., TGF)
Checkpoint-control proteins that arrest the cell cycle if DNA is damaged or chromosomes are abnormal (e.g., p53) • Proteins that promote apoptosis • Enzymes that participate in DNA repair
TP53 : the guardian of genome… The product is a protein of 53 kilodaltons (hence the name). >The p53 protein prevents a cell from completing the cell cycle if its DNA is damaged or the cell has suffered other types of damage.
Loss-of-Function Mutations in Tumor-Suppressor Genes Are Oncogenic • deletions or point mutations • methylation of cytosine residues in the promoter or other control elements.
Loss of Heterozygosity Subsequent loss or inactivation of the normal allele in a somatic cell, referred to as loss of heterozygosity (LOH), is a prerequisite for cancer to develop.
Tumor suppressor gene in cancer cells
[Micrographs by E. R. Fearon and K. Cho. From W. K. Cavanee and R. L. White, Scientific American, March 1995, pp. 78–79.]
Oncogenes
Proteins encoded by proto-oncogenes
Conversion of proto-oncogenes into oncogenes
Gain-of-Function Mutations Convert Proto-oncogenes into Oncogenes • Point mutation (i.e., change in a single base pair) in a proto-oncogene that results in a constitutively active protein product • Chromosomal translocation that brings a growth regulatory gene under the control of a different promoter that causes inappropriate expression of the gene Five broad classes of proteins are generally recognized as being encoded by tumor- suppressor genes
• Amplification (i.e., abnormal DNA replication) of a DNA segment including a proto-oncogene, so that numerous copies exist, leading to overproduction of the encoded protein
Proto-oncogenes into Oncogenes
POINT MUTATION OF AN INTRACELLULAR SIGNAL TRANSDUCER
[Adapted from B. Vogelstein and K. W. Kinzler, 1993, Trends Gene Model of sequential genetic alterations leading to metastatic colon cancer.
Although oncogenes or mutated tumor-suppressor genes or both are required to produce cancer, mutations in DNA repair genes can increase the likelihood of acquiring mutations in these genes.
Cancer is currently treated by surgery, chemotherapy, and radiation. Several other strategies are being tested; these include # immunotherapy, # inhibition of proteins encoded by oncogenes, # inhibition of angiogenesis.
REFERENCES 1. Molecular Cell Biology- Lodish, Baltimore et al, Freeman and Co. 2. Cell and Molecular Biology- Concepts and Experiments- Karp (2012) 5th edn., John Wiley and sons 3. www.youtube.com 4.http://www.biooncology.com/
RAHUL E M BPS051416 SI PLANT SCIENCE CUK

Recommended

Oncogene and tumor suppressor gene
Oncogene and tumor suppressor geneOncogene and tumor suppressor gene
Oncogene and tumor suppressor geneAJEESH BL
 
Oncogenes
Oncogenes Oncogenes
Oncogenes VISHAKHA UPADHYAY
 
Epigenetic in Cancer
Epigenetic in CancerEpigenetic in Cancer
Epigenetic in CancerAbeer Ibrahim
 
tumor suppressor gene, prb, p53
tumor suppressor gene, prb, p53tumor suppressor gene, prb, p53
tumor suppressor gene, prb, p53KAUSHAL SAHU
 
ONCOGENE AND TUMOUR SUPPRESSOR GENE
ONCOGENE AND TUMOUR SUPPRESSOR GENEONCOGENE AND TUMOUR SUPPRESSOR GENE
ONCOGENE AND TUMOUR SUPPRESSOR GENEKoppala RVS Chaitanya
 
Oncogene activation
Oncogene activationOncogene activation
Oncogene activationDr. Ishan Y. Pandya
 
Tumour supressor gene
Tumour supressor geneTumour supressor gene
Tumour supressor geneGopi krishna Giri
 
tumor suppressor gene, prb, p53 gene
tumor suppressor gene, prb, p53 genetumor suppressor gene, prb, p53 gene
tumor suppressor gene, prb, p53 geneKAUSHAL SAHU
 

Recommended

Oncogene and tumor suppressor gene
Oncogene and tumor suppressor geneOncogene and tumor suppressor gene
Oncogene and tumor suppressor geneAJEESH BL
 
Oncogenes
Oncogenes Oncogenes
Oncogenes VISHAKHA UPADHYAY
 
Epigenetic in Cancer
Epigenetic in CancerEpigenetic in Cancer
Epigenetic in CancerAbeer Ibrahim
 
tumor suppressor gene, prb, p53
tumor suppressor gene, prb, p53tumor suppressor gene, prb, p53
tumor suppressor gene, prb, p53KAUSHAL SAHU
 
ONCOGENE AND TUMOUR SUPPRESSOR GENE
ONCOGENE AND TUMOUR SUPPRESSOR GENEONCOGENE AND TUMOUR SUPPRESSOR GENE
ONCOGENE AND TUMOUR SUPPRESSOR GENEKoppala RVS Chaitanya
 
Oncogene activation
Oncogene activationOncogene activation
Oncogene activationDr. Ishan Y. Pandya
 
Tumour supressor gene
Tumour supressor geneTumour supressor gene
Tumour supressor geneGopi krishna Giri
 
tumor suppressor gene, prb, p53 gene
tumor suppressor gene, prb, p53 genetumor suppressor gene, prb, p53 gene
tumor suppressor gene, prb, p53 geneKAUSHAL SAHU
 
ONCOGENES
ONCOGENESONCOGENES
ONCOGENESAmany Elsayed
 
Tumor suppressorgenes
Tumor suppressorgenesTumor suppressorgenes
Tumor suppressorgenesPrasad CSBR
 
Hallmarks of cancer
Hallmarks of cancerHallmarks of cancer
Hallmarks of cancerSreekanth Nallam
 
Oncogenes
OncogenesOncogenes
OncogenesDr.M.Prasad Naidu
 
The Genetics of Cancer
The Genetics of CancerThe Genetics of Cancer
The Genetics of Cancermpattani
 
Cancer and Oncogenesis
Cancer and OncogenesisCancer and Oncogenesis
Cancer and OncogenesisSougata Ganguly
 
DNA repair
DNA repairDNA repair
DNA repairnajmaldin saki
 
TUMOR SUPRESSOR GENES
TUMOR SUPRESSOR GENESTUMOR SUPRESSOR GENES
TUMOR SUPRESSOR GENESIndrajaDoradla
 
homologus recombination
homologus recombinationhomologus recombination
homologus recombinationDeepak Rohilla
 
Dna repair genes
Dna repair genesDna repair genes
Dna repair genesVijay Shankar
 
Genomic instability and Cancer
Genomic instability and CancerGenomic instability and Cancer
Genomic instability and CancerSurender Rawat
 
Cancer epigenetics
Cancer epigenetics Cancer epigenetics
Cancer epigenetics Indian Institute of Science Education and reserach Bhopal
 
Knockout mice
Knockout miceKnockout mice
Knockout miceLovnish Thakur
 
P53
P53P53
P53Vijay Shankar
 
Ras presentation complete
Ras presentation completeRas presentation complete
Ras presentation completeIrsalanasif
 
Oncogenesis
OncogenesisOncogenesis
OncogenesisMD Specialclass
 
Oncogene and Proto-oncogene
Oncogene and Proto-oncogeneOncogene and Proto-oncogene
Oncogene and Proto-oncogenevidan biology
 
Cell cycle and cancer
Cell cycle and cancerCell cycle and cancer
Cell cycle and cancerJaineel Dharod
 
Tumor supressor genes
Tumor supressor genesTumor supressor genes
Tumor supressor genesVijay Shankar
 
Oncogene
OncogeneOncogene
OncogeneBAlbeer Singh
 
Tumor Associated Genes
Tumor Associated Genes Tumor Associated Genes
Tumor Associated Genes fahadxahi
 
Factors controlling growth, Oncogenesis
Factors controlling growth, OncogenesisFactors controlling growth, Oncogenesis
Factors controlling growth, OncogenesisGCUF
 

More Related Content

What's hot

Tumor suppressorgenes
Tumor suppressorgenesTumor suppressorgenes
Tumor suppressorgenesPrasad CSBR
 
The Genetics of Cancer
The Genetics of CancerThe Genetics of Cancer
The Genetics of Cancermpattani
 
homologus recombination
homologus recombinationhomologus recombination
homologus recombinationDeepak Rohilla
 
Genomic instability and Cancer
Genomic instability and CancerGenomic instability and Cancer
Genomic instability and CancerSurender Rawat
 
Ras presentation complete
Ras presentation completeRas presentation complete
Ras presentation completeIrsalanasif
 
Oncogene and Proto-oncogene
Oncogene and Proto-oncogeneOncogene and Proto-oncogene
Oncogene and Proto-oncogenevidan biology
 
Tumor supressor genes
Tumor supressor genesTumor supressor genes
Tumor supressor genesVijay Shankar
 

What's hot (20)

ONCOGENES
ONCOGENESONCOGENES
ONCOGENES
 
Tumor suppressorgenes
Tumor suppressorgenesTumor suppressorgenes
Tumor suppressorgenes
 
Hallmarks of cancer
Hallmarks of cancerHallmarks of cancer
Hallmarks of cancer
 
Oncogenes
OncogenesOncogenes
Oncogenes
 
The Genetics of Cancer
The Genetics of CancerThe Genetics of Cancer
The Genetics of Cancer
 
Cancer and Oncogenesis
Cancer and OncogenesisCancer and Oncogenesis
Cancer and Oncogenesis
 
DNA repair
DNA repairDNA repair
DNA repair
 
TUMOR SUPRESSOR GENES
TUMOR SUPRESSOR GENESTUMOR SUPRESSOR GENES
TUMOR SUPRESSOR GENES
 
homologus recombination
homologus recombinationhomologus recombination
homologus recombination
 
Dna repair genes
Dna repair genesDna repair genes
Dna repair genes
 
Genomic instability and Cancer
Genomic instability and CancerGenomic instability and Cancer
Genomic instability and Cancer
 
Cancer epigenetics
Cancer epigenetics Cancer epigenetics
Cancer epigenetics
 
Knockout mice
Knockout miceKnockout mice
Knockout mice
 
P53
P53P53
P53
 
Ras presentation complete
Ras presentation completeRas presentation complete
Ras presentation complete
 
Oncogenesis
OncogenesisOncogenesis
Oncogenesis
 
Oncogene and Proto-oncogene
Oncogene and Proto-oncogeneOncogene and Proto-oncogene
Oncogene and Proto-oncogene
 
Cell cycle and cancer
Cell cycle and cancerCell cycle and cancer
Cell cycle and cancer
 
Tumor supressor genes
Tumor supressor genesTumor supressor genes
Tumor supressor genes
 
Oncogene
OncogeneOncogene
Oncogene
 

Similar to Cancer Cell Division & Genes

Tumor Associated Genes
Tumor Associated Genes Tumor Associated Genes
Tumor Associated Genes fahadxahi
 
Factors controlling growth, Oncogenesis
Factors controlling growth, OncogenesisFactors controlling growth, Oncogenesis
Factors controlling growth, OncogenesisGCUF
 
Training on Cancer for Medical Representatives of Pharma Company
Training on Cancer for Medical Representatives of Pharma CompanyTraining on Cancer for Medical Representatives of Pharma Company
Training on Cancer for Medical Representatives of Pharma CompanyDr. ANSHU GOKARN
 
Molecular biology of cancer.pptx
Molecular biology of cancer.pptxMolecular biology of cancer.pptx
Molecular biology of cancer.pptxProsper Ingabire
 
Oncogenes, proto-oncogenes and tumor suppressor gene
Oncogenes, proto-oncogenes and tumor suppressor geneOncogenes, proto-oncogenes and tumor suppressor gene
Oncogenes, proto-oncogenes and tumor suppressor geneVaishnaviJanjal
 
Carcinogenesis.pptx
Carcinogenesis.pptxCarcinogenesis.pptx
Carcinogenesis.pptxssuser7ec6af
 
Carcinogenesis.pptx
Carcinogenesis.pptxCarcinogenesis.pptx
Carcinogenesis.pptxMohd Azhan
 
Cell cycle,growth regulation ,molecular basis of cancer by dr.Tasnim
Cell cycle,growth regulation ,molecular basis of cancer by dr.TasnimCell cycle,growth regulation ,molecular basis of cancer by dr.Tasnim
Cell cycle,growth regulation ,molecular basis of cancer by dr.Tasnimdr Tasnim
 
NORMAL-CELLS-versus-CANCER-CELLS.pptxssss
NORMAL-CELLS-versus-CANCER-CELLS.pptxssssNORMAL-CELLS-versus-CANCER-CELLS.pptxssss
NORMAL-CELLS-versus-CANCER-CELLS.pptxssssRashadHamada
 
Carcinogenesis
CarcinogenesisCarcinogenesis
CarcinogenesisIbnu Alias
 
Cancer
CancerCancer
Cancerrupish
 
hallmarksofcancer-210603155625 (1).pdf
hallmarksofcancer-210603155625 (1).pdfhallmarksofcancer-210603155625 (1).pdf
hallmarksofcancer-210603155625 (1).pdfAnandHosalli
 

Similar to Cancer Cell Division & Genes (20)

Tumor Associated Genes
Tumor Associated Genes Tumor Associated Genes
Tumor Associated Genes
 
Factors controlling growth, Oncogenesis
Factors controlling growth, OncogenesisFactors controlling growth, Oncogenesis
Factors controlling growth, Oncogenesis
 
Mutation and cancer
Mutation and cancerMutation and cancer
Mutation and cancer
 
Cancer : A Genetic Mishap - Dr HK Garg
Cancer : A Genetic Mishap - Dr HK GargCancer : A Genetic Mishap - Dr HK Garg
Cancer : A Genetic Mishap - Dr HK Garg
 
Training on Cancer for Medical Representatives of Pharma Company
Training on Cancer for Medical Representatives of Pharma CompanyTraining on Cancer for Medical Representatives of Pharma Company
Training on Cancer for Medical Representatives of Pharma Company
 
Molecular biology of cancer.pptx
Molecular biology of cancer.pptxMolecular biology of cancer.pptx
Molecular biology of cancer.pptx
 
Carcinogenesis
Carcinogenesis Carcinogenesis
Carcinogenesis
 
Cancer biochemistry
Cancer biochemistryCancer biochemistry
Cancer biochemistry
 
Oncogenes, proto-oncogenes and tumor suppressor gene
Oncogenes, proto-oncogenes and tumor suppressor geneOncogenes, proto-oncogenes and tumor suppressor gene
Oncogenes, proto-oncogenes and tumor suppressor gene
 
Oncogene.pptx
Oncogene.pptxOncogene.pptx
Oncogene.pptx
 
Neoplasia part ii
Neoplasia part iiNeoplasia part ii
Neoplasia part ii
 
Carcinogenesis.pptx
Carcinogenesis.pptxCarcinogenesis.pptx
Carcinogenesis.pptx
 
Oncogenes
OncogenesOncogenes
Oncogenes
 
Carcinogenesis.pptx
Carcinogenesis.pptxCarcinogenesis.pptx
Carcinogenesis.pptx
 
N E O P L A S I A 2
N E O P L A S I A 2N E O P L A S I A 2
N E O P L A S I A 2
 
Cell cycle,growth regulation ,molecular basis of cancer by dr.Tasnim
Cell cycle,growth regulation ,molecular basis of cancer by dr.TasnimCell cycle,growth regulation ,molecular basis of cancer by dr.Tasnim
Cell cycle,growth regulation ,molecular basis of cancer by dr.Tasnim
 
NORMAL-CELLS-versus-CANCER-CELLS.pptxssss
NORMAL-CELLS-versus-CANCER-CELLS.pptxssssNORMAL-CELLS-versus-CANCER-CELLS.pptxssss
NORMAL-CELLS-versus-CANCER-CELLS.pptxssss
 
Carcinogenesis
CarcinogenesisCarcinogenesis
Carcinogenesis
 
Cancer
CancerCancer
Cancer
 
hallmarksofcancer-210603155625 (1).pdf
hallmarksofcancer-210603155625 (1).pdfhallmarksofcancer-210603155625 (1).pdf
hallmarksofcancer-210603155625 (1).pdf
 

Recently uploaded

ROLES IN A STAGE PRODUCTION in arts.pptx
ROLES IN A STAGE PRODUCTION in arts.pptxROLES IN A STAGE PRODUCTION in arts.pptx
ROLES IN A STAGE PRODUCTION in arts.pptxVanesaIglesias10
 
Inclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdf
Inclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdfInclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdf
Inclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdfTechSoup
 
Food processing presentation for bsc agriculture hons
Food processing presentation for bsc agriculture honsFood processing presentation for bsc agriculture hons
Food processing presentation for bsc agriculture honsManeerUddin
 
INTRODUCTION TO CATHOLIC CHRISTOLOGY.pptx
INTRODUCTION TO CATHOLIC CHRISTOLOGY.pptxINTRODUCTION TO CATHOLIC CHRISTOLOGY.pptx
INTRODUCTION TO CATHOLIC CHRISTOLOGY.pptxHumphrey A Beña
 
How to do quick user assign in kanban in Odoo 17 ERP
How to do quick user assign in kanban in Odoo 17 ERPHow to do quick user assign in kanban in Odoo 17 ERP
How to do quick user assign in kanban in Odoo 17 ERPCeline George
 
Active Learning Strategies (in short ALS).pdf
Active Learning Strategies (in short ALS).pdfActive Learning Strategies (in short ALS).pdf
Active Learning Strategies (in short ALS).pdfPatidar M
 
Earth Day Presentation wow hello nice great
Earth Day Presentation wow hello nice greatEarth Day Presentation wow hello nice great
Earth Day Presentation wow hello nice greatYousafMalik24
 
Influencing policy (training slides from Fast Track Impact)
Influencing policy (training slides from Fast Track Impact)Influencing policy (training slides from Fast Track Impact)
Influencing policy (training slides from Fast Track Impact)Mark Reed
 
Student Profile Sample - We help schools to connect the data they have, with ...
Student Profile Sample - We help schools to connect the data they have, with ...Student Profile Sample - We help schools to connect the data they have, with ...
Student Profile Sample - We help schools to connect the data they have, with ...Seán Kennedy
 
ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...
ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...
ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...JojoEDelaCruz
 
Activity 2-unit 2-update 2024. English translation
Activity 2-unit 2-update 2024. English translationActivity 2-unit 2-update 2024. English translation
Activity 2-unit 2-update 2024. English translationRosabel UA
 
Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17
Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17
Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17Celine George
 
4.18.24 Movement Legacies, Reflection, and Review.pptx
4.18.24 Movement Legacies, Reflection, and Review.pptx4.18.24 Movement Legacies, Reflection, and Review.pptx
4.18.24 Movement Legacies, Reflection, and Review.pptxmary850239
 
Difference Between Search & Browse Methods in Odoo 17
Difference Between Search & Browse Methods in Odoo 17Difference Between Search & Browse Methods in Odoo 17
Difference Between Search & Browse Methods in Odoo 17Celine George
 
What is Model Inheritance in Odoo 17 ERP
What is Model Inheritance in Odoo 17 ERPWhat is Model Inheritance in Odoo 17 ERP
What is Model Inheritance in Odoo 17 ERPCeline George
 
Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)
Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)
Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)lakshayb543
 
USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...
USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...
USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...Postal Advocate Inc.
 
Integumentary System SMP B. Pharm Sem I.ppt
Integumentary System SMP B. Pharm Sem I.pptIntegumentary System SMP B. Pharm Sem I.ppt
Integumentary System SMP B. Pharm Sem I.pptshraddhaparab530
 

Recently uploaded (20)

FINALS_OF_LEFT_ON_C'N_EL_DORADO_2024.pptx
FINALS_OF_LEFT_ON_C'N_EL_DORADO_2024.pptxFINALS_OF_LEFT_ON_C'N_EL_DORADO_2024.pptx
FINALS_OF_LEFT_ON_C'N_EL_DORADO_2024.pptx
 
ROLES IN A STAGE PRODUCTION in arts.pptx
ROLES IN A STAGE PRODUCTION in arts.pptxROLES IN A STAGE PRODUCTION in arts.pptx
ROLES IN A STAGE PRODUCTION in arts.pptx
 
Inclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdf
Inclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdfInclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdf
Inclusivity Essentials_ Creating Accessible Websites for Nonprofits .pdf
 
Food processing presentation for bsc agriculture hons
Food processing presentation for bsc agriculture honsFood processing presentation for bsc agriculture hons
Food processing presentation for bsc agriculture hons
 
INTRODUCTION TO CATHOLIC CHRISTOLOGY.pptx
INTRODUCTION TO CATHOLIC CHRISTOLOGY.pptxINTRODUCTION TO CATHOLIC CHRISTOLOGY.pptx
INTRODUCTION TO CATHOLIC CHRISTOLOGY.pptx
 
How to do quick user assign in kanban in Odoo 17 ERP
How to do quick user assign in kanban in Odoo 17 ERPHow to do quick user assign in kanban in Odoo 17 ERP
How to do quick user assign in kanban in Odoo 17 ERP
 
YOUVE_GOT_EMAIL_PRELIMS_EL_DORADO_2024.pptx
YOUVE_GOT_EMAIL_PRELIMS_EL_DORADO_2024.pptxYOUVE_GOT_EMAIL_PRELIMS_EL_DORADO_2024.pptx
YOUVE_GOT_EMAIL_PRELIMS_EL_DORADO_2024.pptx
 
Active Learning Strategies (in short ALS).pdf
Active Learning Strategies (in short ALS).pdfActive Learning Strategies (in short ALS).pdf
Active Learning Strategies (in short ALS).pdf
 
Earth Day Presentation wow hello nice great
Earth Day Presentation wow hello nice greatEarth Day Presentation wow hello nice great
Earth Day Presentation wow hello nice great
 
Influencing policy (training slides from Fast Track Impact)
Influencing policy (training slides from Fast Track Impact)Influencing policy (training slides from Fast Track Impact)
Influencing policy (training slides from Fast Track Impact)
 
Student Profile Sample - We help schools to connect the data they have, with ...
Student Profile Sample - We help schools to connect the data they have, with ...Student Profile Sample - We help schools to connect the data they have, with ...
Student Profile Sample - We help schools to connect the data they have, with ...
 
ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...
ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...
ENG 5 Q4 WEEk 1 DAY 1 Restate sentences heard in one’s own words. Use appropr...
 
Activity 2-unit 2-update 2024. English translation
Activity 2-unit 2-update 2024. English translationActivity 2-unit 2-update 2024. English translation
Activity 2-unit 2-update 2024. English translation
 
Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17
Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17
Incoming and Outgoing Shipments in 3 STEPS Using Odoo 17
 
4.18.24 Movement Legacies, Reflection, and Review.pptx
4.18.24 Movement Legacies, Reflection, and Review.pptx4.18.24 Movement Legacies, Reflection, and Review.pptx
4.18.24 Movement Legacies, Reflection, and Review.pptx
 
Difference Between Search & Browse Methods in Odoo 17
Difference Between Search & Browse Methods in Odoo 17Difference Between Search & Browse Methods in Odoo 17
Difference Between Search & Browse Methods in Odoo 17
 
What is Model Inheritance in Odoo 17 ERP
What is Model Inheritance in Odoo 17 ERPWhat is Model Inheritance in Odoo 17 ERP
What is Model Inheritance in Odoo 17 ERP
 
Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)
Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)
Visit to a blind student's school🧑‍🦯🧑‍🦯(community medicine)
 
USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...
USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...
USPS® Forced Meter Migration - How to Know if Your Postage Meter Will Soon be...
 
Integumentary System SMP B. Pharm Sem I.ppt
Integumentary System SMP B. Pharm Sem I.pptIntegumentary System SMP B. Pharm Sem I.ppt
Integumentary System SMP B. Pharm Sem I.ppt
 

Cancer Cell Division & Genes

  • 1.
  • 2.
  • 4. Licentious division - prostate cancer cells durin Cancer not a single disease; heterogeneous group of disorders characterized by the presence of cells that do not respond to the normal controls on division.
  • 7. Normal cells grow in monolayer Cancer cells grow in clumps (foci) COURTESY OF G. STEVEN MARTIN.)
  • 10. Why a greater number of cells do not give rise to cancerous tumors ….???
  • 11. > malignant transformation requires more than a single genetic alteration(hits).
  • 12. How is a normal cell transformed into a cancerous cell?
  • 13. Rather than lacking function, cancer cells reproduce at a rate far beyond the normally tightly regulated boundaries of the cell cycle. occur due to an alteration of a normal biological process — cell division.
  • 15.
  • 16. Induction of malignant transformation with chemical or physical carcinogens appears to involve multiple steps and at least two distinct phases: initiation and promotion.
  • 17. The signals that regulate cell division fall into two basic types: molecules that stimulate cell division and those that inhibit it.
  • 18. Genes that have been implicated in carcinogenesis are divided into two broad categories: Tumor-suppressor genes and Oncogenes.
  • 19. Tumor-suppressor genes  Encode proteins that restrain cell growth and prevent cells from becoming malignant.  Act recessively since both copies must be deleted or mutated before their protective function is lost.
  • 20. Oncogenes > Encode proteins that promote the loss of growth control and malignancy. Oncogenes arise from Proto-oncogenes—genes that encode proteins having a role in a cell’s normal activities.  Mutations that alter either the protein or its expression cause the proto-oncogene to act abnormally and promote the formation of a tumor.
  • 21.
  • 22. MESSAGE The proteins that oncogenes encode are activated in tumor cells, whereas the proteins that tumor suppressor genes encode are inactivated.
  • 24. Five broad classes of proteins are generally recognized as being encoded by tumor- suppressor genes Intracellular proteins that regulate or inhibit progression through a specific stage of the cell cycle (e.g., p16 and Rb) Receptors or signal transducers for secreted hormones or developmental signals that inhibit cell proliferation (e.g., TGF)
  • 25. Checkpoint-control proteins that arrest the cell cycle if DNA is damaged or chromosomes are abnormal (e.g., p53) • Proteins that promote apoptosis • Enzymes that participate in DNA repair
  • 26.
  • 27. TP53 : the guardian of genome… The product is a protein of 53 kilodaltons (hence the name). >The p53 protein prevents a cell from completing the cell cycle if its DNA is damaged or the cell has suffered other types of damage.
  • 28.
  • 29. Loss-of-Function Mutations in Tumor-Suppressor Genes Are Oncogenic • deletions or point mutations • methylation of cytosine residues in the promoter or other control elements.
  • 30. Loss of Heterozygosity Subsequent loss or inactivation of the normal allele in a somatic cell, referred to as loss of heterozygosity (LOH), is a prerequisite for cancer to develop.
  • 31. Tumor suppressor gene in cancer cells
  • 32. [Micrographs by E. R. Fearon and K. Cho. From W. K. Cavanee and R. L. White, Scientific American, March 1995, pp. 78–79.]
  • 34.
  • 35. Proteins encoded by proto-oncogenes
  • 37. Gain-of-Function Mutations Convert Proto-oncogenes into Oncogenes • Point mutation (i.e., change in a single base pair) in a proto-oncogene that results in a constitutively active protein product • Chromosomal translocation that brings a growth regulatory gene under the control of a different promoter that causes inappropriate expression of the gene Five broad classes of proteins are generally recognized as being encoded by tumor- suppressor genes
  • 38. • Amplification (i.e., abnormal DNA replication) of a DNA segment including a proto-oncogene, so that numerous copies exist, leading to overproduction of the encoded protein
  • 40. POINT MUTATION OF AN INTRACELLULAR SIGNAL TRANSDUCER
  • 41.
  • 42. [Adapted from B. Vogelstein and K. W. Kinzler, 1993, Trends Gene Model of sequential genetic alterations leading to metastatic colon cancer.
  • 43. Although oncogenes or mutated tumor-suppressor genes or both are required to produce cancer, mutations in DNA repair genes can increase the likelihood of acquiring mutations in these genes.
  • 44. Cancer is currently treated by surgery, chemotherapy, and radiation. Several other strategies are being tested; these include # immunotherapy, # inhibition of proteins encoded by oncogenes, # inhibition of angiogenesis.
  • 45.
  • 46. REFERENCES 1. Molecular Cell Biology- Lodish, Baltimore et al, Freeman and Co. 2. Cell and Molecular Biology- Concepts and Experiments- Karp (2012) 5th edn., John Wiley and sons 3. www.youtube.com 4.http://www.biooncology.com/

Editor's Notes

  1. Cancers figure among the leading causes of morbidity and mortality worldwide, with approximately 14 million new cases and 8.2 million cancer related deaths. Common cancers include…lung…, The number of new cases is expected to rise by about 70% over the next two decades.
  2. As a tumor grows in size, it stimulates the formation of new blood vessels, a process termed angiogenesis (Figure 16.22). Blood vessels are required to deliver nutrients and oxygen to the rapidly growing tumor cells and to remove their waste products. Blood vessels also provide the conduits for cancer cells to spread to other sites in the body.
  3. The cells of an advanced tumor can separate from the tumor and travel to distant sites in the body, where they may take up residence and develop into new tumors.
  4. Other diseases are caused by the reduction or increase in function Diabetis –insulin Aids ..
  5. Hereditery variety of DNA- and RNA-containing viruses Carcinogens Chemicals.toxins ionizing radiation pesticides,insecticides About 30% of cancer deaths are due to the 5 leading behavioural and dietary risks: high body mass index, low fruit and vegetable intake, lack of physical activity, tobacco use, alcohol use. all of these agents act by causing changes in the genome of the transformed cell.
  6. # Initiation involves changes in the genome but does not, in itself, lead to malignant transformation. # After initiation, promoters stimulate cell division and lead to malignant transformation.
  7. These control mechanisms are similar to the accelerator and brake of an automobile. In normal cells (but hopefully not your car), both accelerators and brakes are applied at the same time, causing cell division to proceed at the proper speed.
  8. Promote apoptosis…
  9. Oncogenes act dominantly; >that is, a single copy will cause the cell to express the altered phenotype. >Most tumors contain alterations in both tumor-suppressor genes and oncogenes. >As long as a cell retains at least one copy of all of its tumor-suppressor genes, it should be protected against the consequences of oncogene formation. > Conversely, the loss of a tumor-suppressor function should not be sufficient, by itself, to cause the cell to become malignant.
  10. 1. The tumor-suppressor gene most often implicated in human cancer is TP53, whose product (p53) may be able to suppress cancer formation by several different mechanisms It does this by binding to a transcription factor called E2F. This prevents E2F from binding to the promoters of such proto-oncogenes as c-myc and c-fos. >Transcription of c-myc and c-fos is needed for mitosis so blocking the transcription factor needed to turn on these genes prevents cell division.
  11. >If the damage is minor, p53 halts the cell cycle — hence cell division — until the damage is repaired or if the damage is major and cannot be repaired, p53 triggers the cell to commit suicide by apoptosis. These functions make p53 a key player in protecting us against cancer; that is, an important tumor suppressor gene. More than half of all human cancers do, in fact, harbor p53 mutations and have no functioning p53 protein. Mice have been cured of cancer by treating them with a peptide that turns on production of the p53 protein in the tumor cells.
  12. In many cancers, tumor-suppressor genes have deletions or point mutations that prevent production of any protein or lead to production of a nonfunctional protein. Another mechanism for inactivating tumor-suppressor genes is methylation of cytosine residues in the promoter or other control elements. Such methylation is commonly found in nontranscribed regions of DNA.
  13. we can inherit a propensity to cancer by receiving a damaged allele of a tumor suppressor gene from one of our parents; that is, we are heterozygous for the mutation. That in itself will not cause cancer, since the remaining normal allele prevents aberrant growth; the cancer is recessive.
  14. The ras oncogene A single base-pair substitution that converts glycine into valine at amino acid number 12 of the Ras protein, for example, creates the oncoprotein found in human bladder cancer (Figure 17-16a). Recall that the normal Ras protein is a G-protein subunit that takes part in signal transduction. It normally functions by cycling between the active GTP-bound state and the inactive GDP-bound state (see Figure 17-12). The missense mutation in the ras oncogene produces an oncoprotein that always binds GTP (Figure 17-16b), even in the absence of normal signals. Thus, the Ras oncoprotein continuously propagates a signal that promotes cell proliferation.
  15. Gene ERBB2, a known proto-oncogene, is located at the long arm of human chromosome 17 (17q12. Human epidermal growth factor receptor (HER) pathways play a critical role in cancer biology . Dysregulation of HER-mediated signaling pathways results in the growth and spread of cancer cells.1 The HER family consists of 4 structurally related receptors: HER1 (EGFR), HER2, HER3, and HER4.1,2 HER family receptors are activated by ligand-induced dimerization, or receptor pairing.3 Dimerization is a critical step in HER family-mediated signaling, and HER receptors are able to homodimerize or heterodimerize with other HER family members, allowing for multiple receptor combinations.1,4 The formation of dimers leads to activation of the intrinsic tyrosine kinase domain and subsequent phosphorylation on specific tyrosine residues, which serve as docking sites for a variety of molecules. Recruitment of these molecules leads to the activation of different downstream signaling cascades, including the MAPK proliferation pathway and/or the PI3K/Akt prosurvival pathway.1,4-7 Inappropriate signaling may occur as a result of receptor overexpression or dysregulation of receptor activation, which may lead to8-10: Increased/uncontrolled cell proliferation Decreased apoptosis (programmed cell death) Enhanced cancer cell motility Angiogenesis
  16. Having mutated DNA repair genes is analogous to having a lousy car mechanic who does not make the necessary repairs to a broken accelerator or brake. >The genome of patients with the most common hereditary form of colon cancer, called hereditary nonpolyposis colon cancer (HNPCC), contains microsatellite sequences of abnormal nucleotide number.
  17. To date, the greatest success has come with the development of an inhibitor of Abl kinase in patients with chronic myelogenous leukemia. A second success story has been the development of humanized antibodies that bind to a protein on the surface of malignant B cells in cases of non-Hodgkin’s lymphoma. Antiangiogenic strategies attempt to prevent a solid tumor from inducing the formation of new blood vessels that are required to supply the tumor cells with nutrients and other materials. A number of agents have been identified that block angiogenesis in mice and have had limited success in clinical trials.