chapter 19 the organization and control of eukaryotic genomes

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Chapter 19 The Organization and Control of Eukaryotic Genomes

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Chapter 19 The Organization and Control of Eukaryotic Genomes. Chapter 19 The Organization and Control of Eukaryotic Genomes. Chromatin structure is based on successive layers of DNA packing. Chapter 19 The Organization and Control of Eukaryotic Genomes. - PowerPoint PPT Presentation

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Page 1: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 2: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chromatin structure is based on successive

layers of DNA packing.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 3: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 4: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 5: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 6: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 7: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 8: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 9: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

histone:

Protein “beads” that act as a spool for wrapping DNA

nucleosomes:

Histones, along with their associated DNA.

Page 10: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

euchromatin:

Extended form of DNA during interphase

heterochromatin:

Tightly packed DNA in metaphase chromosomes.

Page 11: Chapter 19 The Organization and Control of Eukaryotic Genomes

Chapter 19The Organization and Control of Eukaryotic Genomes

Much of the genome is noncoding

•Tandemly repetitive DNA (or satellite DNA) is found in telomeres and centromeres

•Interspersed repetitive DNA (Alu elements) are found throughout the chromosome.

Page 12: Chapter 19 The Organization and Control of Eukaryotic Genomes

multigene families:

Identical or similar genes clustered together

pseudogenes:

Very similar to real genes, but code for nonfuctional proteins.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 13: Chapter 19 The Organization and Control of Eukaryotic Genomes

gene amplification:

Extra copies of genes for a temporary boost in productivity

They exist as tiny circles of DNA in the nucleolus.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 14: Chapter 19 The Organization and Control of Eukaryotic Genomes

transposons:

Genes that “jump” from place to place in the genome

retrotransposons:

Transposons that use an RNA intermediate.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 15: Chapter 19 The Organization and Control of Eukaryotic Genomes

Immunoglobins are proteins that recognize self vs. non-self

Immunoglobin genes are permanently rearranged during development

(More about this when we study the immune system.)

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 16: Chapter 19 The Organization and Control of Eukaryotic Genomes

DNA methylation (adding -CH3 groups) is a way of shutting off certain genes

Histone acetylation (adding -COCH3 groups) activates genes

This is how cellular differentiation and genomic imprinting work.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 17: Chapter 19 The Organization and Control of Eukaryotic Genomes

Gene expression can be controlled at any step of the process:–DNA unpacking

–Transcription

–RNA processing

–Degradation of RNA

–Translation

–Polypeptide cleavage and folding

–Degradation of protein

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 18: Chapter 19 The Organization and Control of Eukaryotic Genomes

Gene expression can be controlled at any step of the process:–DNA unpacking

–Transcription

–RNA processing

–Degradation of RNA

–Translation

–Polypeptide cleavage and folding

–Degradation of protein

Chapter 19The Organization and Control of Eukaryotic Genomes

Regulation is most common at the level of transcription.

Page 19: Chapter 19 The Organization and Control of Eukaryotic Genomes

control elements:

Non-coding DNA that regulates gene expression by binding with transcription factors–Distal control elements (enhancers)

–Proximal control elements

–Promoter / TATA box.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 20: Chapter 19 The Organization and Control of Eukaryotic Genomes

transcription factors:

Proteins that help position RNA polymerase on the DNA–Activators

–Repressors.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 21: Chapter 19 The Organization and Control of Eukaryotic Genomes

Eukaryotes do not have operons like the ones in bacteria, but…

…coordinately controlled genes, scattered around the genome, share common control elements.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 22: Chapter 19 The Organization and Control of Eukaryotic Genomes

alternate RNA splicing:

A single primary transcript can be turned into any one of several different mRNA molecules

yourmyhisheranswerisyesnomaybe

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 23: Chapter 19 The Organization and Control of Eukaryotic Genomes

alternate RNA splicing:

A single primary transcript can be turned into any one of several different mRNA molecules

yourmyhisheranswerisyesnomaybe

My answer is maybe

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 24: Chapter 19 The Organization and Control of Eukaryotic Genomes

alternate RNA splicing:

A single primary transcript can be turned into any one of several different mRNA molecules

yourmyhisheranswerisyesnomaybe

My answer is maybe

His answer is no.

Chapter 19The Organization and Control of Eukaryotic Genomes

Page 25: Chapter 19 The Organization and Control of Eukaryotic Genomes

protooncogenes:

If a mutation makes them too active, they become oncogenes

tumor-supressor genes:

If a mutation makes them inactive, this can also cause cancer

Either kind of mutation will affect regulation of the cell cycle.

The Molecular Biology of Cancer

Page 26: Chapter 19 The Organization and Control of Eukaryotic Genomes

ras is a proto-oncogene:

Page 27: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth factor

ras is a proto-oncogene:

Page 28: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth factor

receptor

ras is a proto-oncogene:

Page 29: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth factor

receptor

G protein ras

ras is a proto-oncogene:

Page 30: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth factor

receptor

G protein ras

transcription factor →

ras is a proto-oncogene:

Page 31: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth factor

receptor

G protein ras

↓ protein that

transcription factor → → stimulates the

cell cycle

ras is a proto-oncogene:

Page 32: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth factor

receptor

G protein ras

↓ protein that

transcription factor → → stimulates the

cell cycle

ras is a proto-oncogene:

Normal cell division

Page 33: Chapter 19 The Organization and Control of Eukaryotic Genomes

G protein ras

ras is a proto-oncogene:

Page 34: Chapter 19 The Organization and Control of Eukaryotic Genomes

G protein ras

ras is a proto-oncogene:Mutant ras becomes an oncogene:

Page 35: Chapter 19 The Organization and Control of Eukaryotic Genomes

ras is a proto-oncogene:Mutant ras becomes an oncogene:

G protein ras

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓

transcription factor

Page 36: Chapter 19 The Organization and Control of Eukaryotic Genomes

ras is a proto-oncogene:

G protein ras

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓

transcription factor →

Mutant ras becomes an oncogene:

Page 37: Chapter 19 The Organization and Control of Eukaryotic Genomes

ras is a proto-oncogene:

G protein ras

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓ protein that

transcription factor → → stimulates the

cell cycle

Mutant ras becomes an oncogene:

Page 38: Chapter 19 The Organization and Control of Eukaryotic Genomes

ras is a proto-oncogene:

Uncontrolled cell division

G protein ras

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓

↓ ↓ ↓ ↓ ↓ ↓ protein that

transcription factor → → stimulates the

cell cycle

Mutant ras becomes an oncogene:

Page 39: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth inhibiting

factor

P53 is a tumor-supressor gene:

Page 40: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth inhibiting

factor

receptor

P53 is a tumor-supressor gene:

Page 41: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth inhibiting

factor

receptor

G protein

P53 is a tumor-supressor gene:

Page 42: Chapter 19 The Organization and Control of Eukaryotic Genomes

growth inhibiting

factor

receptor

G protein

↓ p53

transcription factor →

P53 is a tumor-supressor gene:

Page 43: Chapter 19 The Organization and Control of Eukaryotic Genomes

P53 is a tumor-supressor gene: growth inhibiting

factor

receptor

G protein

↓ p53 protein that

transcription factor → → stops the

cell cycle

Page 44: Chapter 19 The Organization and Control of Eukaryotic Genomes

Mutation in the p53 gene: growth inhibiting

factor

receptor

G protein

↓ p53 protein that

transcription factor → (defective) → stops the

cell cycle

Page 45: Chapter 19 The Organization and Control of Eukaryotic Genomes

Mutation in the p53 gene: growth inhibiting

factor

receptor

G protein

↓ p53 defective protein

transcription factor → (defective) → does not stop

the cell cycle

Page 46: Chapter 19 The Organization and Control of Eukaryotic Genomes

Mutation in the p53 gene: growth inhibiting

factor

receptor

G protein

↓ p53 defective protein

transcription factor → (defective) → does not stop

the cell cycle

Page 47: Chapter 19 The Organization and Control of Eukaryotic Genomes

Most cancers involve multiple mutations

•Some of these can be inherited

•This is why a predisposition to some types of cancer runs in families.

The Molecular Biology of Cancer

Page 48: Chapter 19 The Organization and Control of Eukaryotic Genomes

p53 is a damage control protein

•It stimulates DNA repair

•It halts cell division

•It can trigger apoptosis (cellular suicide.)

The Molecular Biology of Cancer

.