Midterm 2

Question 1

When did scientists show that the information in DNA can be copied into RNA and then into protein?

Answer 1

1950s

Question 2

How is the genetic code redundant?

Answer 2

64 codons that give only 20 amino acids, where the last nucleotide in a codon is different (first two usually all give the same amino acid).

Question 3

Translation

Answer 3

The conversion of information in RNA into protein.

Question 4

Genetic code

Answer 4

The correspondence between nucleotides in a mRNA and the amino acid sequence of a protein.

Question 5

Codon

Answer 5

Group of three consecutive nucleotides in RNA that specify an amino acid.

Question 6

Reading frames

Answer 6

The portion of a mRNA that is translated.

Question 7

How many ORF are there? How many give the correct protein?

Answer 7

3 ORF with ONLY 1 giving the correct protein.

Question 8

How did researchers create a cell-free system for protein synthesis?

Answer 8

Broke open E.coli cells and centrifuged where lighter components were needed for protein synthesis. They applied radioactive amino acids that would result in radiolabeled proteins. Another centrifuge done again and the radioactive layer of proteins at the top were assessed.

Question 9

What does translation depend on?

Answer 9

Adaptor molecules

Question 10

What do adpator molecules bind to?

Answer 10

Bind to a codon at one site on their surface and to an amino acid at another site.

Question 11

What is the appearance of a tRNA?

Answer 11

Folded, double-helical structure formed by base-paired regions to give a cloverleaf

Question 12

What additional forming of the cloverleaf tRNA form?

Answer 12

Compact, L-shaped structure held together by additional hyrdogen bonds between different regions of the molecule.

Question 13

Anticodon

Answer 13

A region on the tRNA that contains a set of three consecutive nucleotides that bind by base pairing to the complementary codon in the mRNA/

Question 14

What is the importance of the 3’ end of the tRNA?

Answer 14

Site where the amino acid that matches the codon is covalently attached.

Question 15

Wobble base-pairing

Answer 15

Only the first two positions of the codon match while the third position doesn’t bind explaining the difference in the third nucleotide in amino acids.

Question 16

aminoacyl-tRNA synthetases

Answer 16

Enzymes that recognize and attach the correct amino acid to tRNAs.

Question 17

What part do aminoacyl-tRNA synthetases recognize?

Answer 17

Specific nucleotides in both the anticodon and the amino-acid accepting arm of the correct tRNA.

Question 18

Charging

Answer 18

The process of the synthetase attaching the amino acid to its corresponding tRNA.

Question 19

What energy is used in the synthetase-catalyzed reaction?

Answer 19

Hydrolysis of ATP

Question 20

What energy is used to link the amino acid to the chain of polypetides?

Answer 20

The high-energy bond between the charged tRNA and the amino acid.

Question 21

Ribosome

Answer 21

A large complex of small proteins (ribosomal) and RNA molecules known as ribosomal RNAs (rRNAs).

Question 22

What is the purpose of a ribosome?

Answer 22

Allow the translation of mRNA into protein by moving along the mRNA, holding the tRNAs, and linking the amino acids to form a chain.

Question 23

What are the subunits of a ribosome?

Answer 23

Small and large subunit.

Question 24

What does the small ribosomal subunit do?

Answer 24

Matches the tRNAs to the codons of the mRNA.

Question 25

What does the large ribosomal subunit do?

Answer 25

Catalyzes the formation of peptide bonds that link the amino acids in a polypeptide chain.

Question 26

Where does the subunits of the ribosome bind to the mRNA?

Answer 26

5’ end

Question 27

What happens to the subunits of the ribosome when protein synthesis is done?

Answer 27

Separate

Question 28

Compare the speed of eukaryotic ribosome versus bacterial ones.

Answer 28

Eukaryotic - 2 amino acids to a polypeptide chain per second.
Bacterial - 20 amino acids per second.

Question 29

What are the three sites on tRNA?

Answer 29

A (aminoacyl-tRNA), P (peptidyl-tRNA), and E (exit) site.

Question 30

Explain the process of translation from the three sites on the ribosome.

Answer 30

1. Initiator charged tRNA enters the P site, base pairing with the complementary codon on the mRNA.
2. Next charged tRNA enters the A site and its amino acid is linked to the peptide chain at P site (through the carboxyl end joined by a peptide bond to free amino group in A site).
3. Large ribosome shifts forward, moving the initiator tRNA to E site, ejecting it.

Question 31

What way are new proteins synthesized?

Answer 31

Amino to its carboxyl end.

Question 32

How many small ribosome sites can be occupied at a time?

Answer 32

Two

Question 33

How much RNA makes ribosome?

Answer 33

2/3 by weight

Question 34

What is responsible for the ribosomes structure and its ability to catalyze protein synthesis?

Answer 34

rRNAs

Question 35

Where are rRNAs located in the ribosome?

Answer 35

Form a highly compact core

Question 36

Where are ribosomal proteins located in a ribosome?

Answer 36

Located on the surface where they fill in the gaps of the folded RNA.

Question 37

What is the role of ribosomal proteins?

Answer 37

To fold and stabilize the RNA core

Question 38

What is the catalytic site for peptide bond formation formed by?

Answer 38

The 23S rRNA of the large subunit, which is a peptidyl transferase.

Question 39

Ribozymes

Answer 39

RNA molecules that have catalytic activity.

Question 40

What is the methionine removed by?

Answer 40

A specific protease

Question 41

What is needed for the initiation of protein synthesis in eukaryotes?

Answer 41

Proteins known as translation initiation factors.

Question 42

Why is an initiator tRNA molecule added first?

Answer 42

Only adaptor capable of binding tightly to the P site in absence of the large ribosomal subunit.

Question 43

When are the initiation factors released? Why?

Answer 43

When the AUG is recognized to allow for the large ribosomal subunit to bind and complete protein assembly.

Question 44

What do bacterial mRNA have to tell the ribosome where to bind?

Answer 44

Specific ribosome-binding sequences that are up to six nucleotides long and located a few nucleotides upstream of an AUG.

Question 45

Polycistronic

Answer 45

The ability of bacterial mRNA to encode several different proteins from the same mRNA molecule.

Question 46

What is the end of translation signified by?

Answer 46

A stop codon, UAA, UAG, and UGA.

Question 47

What do release factors do?

Answer 47

Proteins that bind to the stop codon and alter the activity of peptidyl transferase, allowing the addition of an H2O to peptidyl tRNA instead of an amino acid, thus releasing the chain.

Question 48

What do chaperone proteins do?

Answer 48

Fold proteins correctly in the cell.

Question 49

When do chaperone proteins attach to a protein?

Answer 49

As they emerge from the ribosome.

Question 50

Polysomes

Answer 50

Ribosomes that bind to the 5’ end of mRNA as it’s being translated.

Question 51

How far apart is each ribosome attached to a mRNA molecule?

Answer 51

80 nucleotides apart.

Question 52

What is the importance of polysomes?

Answer 52

Allow more protein molecules to be made at a given time.

Question 53

When do polysomes attach to bacterial mRNA?

Answer 53

Ribosomes attach to free end before transcription of RNA is complete, following closely behind RNA polymerase.

Question 54

What is a fundamental feature of all life in terms of mRNA?

Answer 54

Ability to translate mRNAs into functional proteins.

Question 55

What are functions of proteolytic pathways?

Answer 55

Degrade proteins with short lifetimes and remove proteins that are damaged or misfolded.

Question 56

Proteasomes

Answer 56

Large protein machines that break down proteins.

Question 57

What is the structure of a proteasome?

Answer 57

Central cylinder with an active site in an inner chamber and ends stoppered by a large protein complex (at least 10 subunits).

Question 58

How do proteasomes work?

Answer 58

Protein stoppers bind to the damaged proteins and unfold the proteins, threading them into the inner chamber. Proteases chop them into short peptides and released from either end.

Question 59

How are ubiquitin chains added?

Answer 59

A certain amino acid sequence on one that needs it (short-lived) or signals exposed from misfolding/damage.

Question 60

What does the final concentration of a protein depend on?

Answer 60

Rate at which each of the steps are carried out.

Question 61

What must proteasomes recognize in eukaryotic damaged proteins?

Answer 61

Covalent attachment of a ubiquitin chain.

Question 62

What may happen to a protein once released?

Answer 62

Post-translational modifications like covalent phosphorylation, binding of cofactors, or association with other protein subunits.

Question 63

What is the sequence of -10 (3’ to 5’)?

Answer 63

ATATAA

Question 64

What is the sequence of -35 (3’ to 5’)?

Answer 64

AACTGT

Question 65

What does the RNA transcript form to stall RNA polymerase?

Answer 65

Hairpin loop (done by G + Cs binding with other G + Cs to form hydrogen bonds), thus transcription is done (RHO independent factor).

Question 66

What are transcription factors?

Answer 66

Proteins that act directly with DNA

Question 67

General transcription factors

Answer 67

Those involved in binding directly to DNA, thus initiating transcription.

Question 68

What do general transcription factors require?

Answer 68

Special transcription factors.

Question 69

Where did the idea of genes being switched on and off come from?

Answer 69

E.coli and its adaptable changes in the composition of their growth medium.

Question 70

Transcription regulators

Answer 70

Proteins that bind to DNA and control gene transcription.

Question 71

What are regulatory DNA sequences used for?

Answer 71

To switch a gene on or off.

Question 72

What is the composition of a regulatory DNA sequence in a bacteria versus eukaryotes?

Answer 72

1. Short as 10 nucleotide pairs in bacteria
2. 10,000 nucleotide pairs in eukaryotes

Question 73

What is the purpose of regulatory DNA sequences in a bacteria?

Answer 73

Respond to a single signal

Question 74

What is the purpose of regulatory DNA sequences in an eukaryotic cell?

Answer 74

Microprocessors, integrating information from multiple signals.

Question 75

What is the purpose of transcription regulators?

Answer 75

Binds to a regulatory DNA sequence to act as a switch to control transcription.

Question 76

How many DNA sequences does a single transcriptional regulator recognize?

Answer 76

ONLY one

Question 77

How do proteins recognize a specific nucleotide sequence?

Answer 77

Surface of the protein fits tightly against the surface features of a DNA double helix.

Question 78

How does the protein make contact with a nucleotide sequence?

Answer 78

Protein inserts itself into the major groove of the helix to make contacts with nucleotide pairs here.

Question 79

How many molecular contacts are formed at a protein-DNA interface?

Answer 79

10-20 contacts

Question 80

Are protein-DNA interactions strong?

Answer 80

The most tightest and specific molecular interactions.

Question 81

What do transcription regulators bind to DNA as?

Answer 81

Dimers

Question 82

What is the purpose of dimers?

Answer 82

Doubles the area of contact with DNA, thus increasing the strength and specificity of the protein-DNA interaction.

Question 83

Homeodomain

Answer 83

An area in eukaryotes where proteins make interactions with DNA.

Question 84

How do bacteria regulate the expression of their genes?

Answer 84

According to the food sources that are available.

Question 85

What is an operon?

Answer 85

A cluster of genes on a chromosome that are transcribed from a single promoter as one long mRNA molecule.

Question 86

Explain what happens when tryptophan concentrations are low.

Answer 86

The operon is transcribed and mRNA is translated, thus the enzymes will produce tryp.

Question 87

What happens when tryptophan concentrations are high?

Answer 87

The production of the operon stops.

Question 88

What does the transcription regulator bind to in the operon?

Answer 88

Operator

Question 89

What happens when the regulator binds to the operator in the tryptophan operon?

Answer 89

Blocks the access of the RNA polymerase to the promoters, thus preventing transcription, known as the tryptophan repressor (works with excessive amounts of tryp).

Question 90

Why is a tryptophan repressor an allosteric protein?

Answer 90

The binding of tryp causes a change in its structure so that the protein can bind to the operator sequence.

Question 91

How is the tryp repressor protein always present in the cell?

Answer 91

Gene that encodes it is transcribed at a low level.

Question 92

Transcriptional repressor protein

Answer 92

Switches genes off

Question 93

Transcriptional activator protein

Answer 93

Switch genes on

Question 94

Where do transcriptonal activators bind to? What does this help?

Answer 94

Promoters where they position RNA polymerase to start transcription.

Question 95

What do activator proteins bind to? WHat do they help with?

Answer 95

The promoters to allow RNA polymerase to bind and start transcription.

Question 96

Explain activator proteins in the lac operon.

Answer 96

CAP activator proteins bind to cAMP when there is an absence of glucose, allowing it to bind to the promoter thus proteins to digest lactose can be made (lactose is PRESENT).

Question 97

How does the Lac repressor work?

Answer 97

Binds to the operator when there is an absence of lactose.

Question 98

What circuits are controlled by transcription regulatory devices in eukaryotes?

Answer 98

Allow a fertilized egg to form the tissues and organs of a multicellular organism.

Question 99

Enhancers

Answer 99

DNA sites that eukaryotic gene activators bind to to increase the rate of transcription.

Question 100

Where do activator proteins bind to in eukaryotes?

Answer 100

Either upstream or downstream from a gene’s promoter.

Question 101

What happens to the DNA between the enhancer and the pronmotor?

Answer 101

The DNA loops to allow the activator proteins to influence the direct events at the promoter.

Question 102

What do proteins on the DNA help with in terms of transcription regulators?

Answer 102

Additional proteins that link the distantly bound transcription regulators to proteins, RNA polymerase and general transcription factors, at the promoter.

Question 103

What does the large complex of Mediator do (transcriptional regulator)?

Answer 103

Proteins function by adding in the assembly of the general transcription factors and RNA polymerase to form a larger transcription complex at the promoter.

Question 104

What do eukaryotic repressors do?

Answer 104

Decreases transcription by preventing the assembly of a large transcription complex at the promoter.

Question 105

What do eukaryotic transcriptional regulators attract? Purpose?

Answer 105

Attract proteins that modify chromatin structure so that affect the accessibility of the promoter to the general transcription factors and RNA polymerase.

Question 106

What are three descriptions of the amino acid reading frame?

Answer 106

Redundant (same amino acid produced from different codons), universal (same codes used throughout species) and continuous (always read constantly in groups of three).

Question 107

Why can nucleosomes inhibit transcription?

Answer 107

If they are positioned over the promoter than they block physically block the assembly of the general transcription factors or RNA polymerase.

Question 108

What did chromatin packaging evolve?

Answer 108

Prevent leaky gene expression by blocking the initiation of transcription in the absence of proper activator proteins.

Question 109

What is a gene activator that uses chromatin modifying?

Answer 109

The recruitment of histone acetyl transferases.

Question 110

How do histone acetyl transferases help with chromatin modification?

Answer 110

Allows the attachment of acetyl groups to lysines in the tail of histone proteins, thus giving them a greater accessibility to DNA and attract protein that promote transcription

Question 111

How can gene repressor proteins modify chromatin?

Answer 111

Repressors attract histone deacetylases where they remove acetyl groups from histone tails, thus making them less accessible to DNA, thus transcription initiation won’t occur.