MICR - Week 3

Question 1

What species of bacteria is used to make recombinant insulin?

Answer 1

E.coli

Question 2

Describe pathogenesis in terms of translation/transcription

Answer 2

Certain proteins are needed to colonize the host, but if not in host don’t need them so don’t prescribe them

Will sense things like:
- temp
- nutrients
- immune system

Then make things like:
- to attach to cell (pili)
- to evade the immune sys
- to kill host cell

Question 3

A promotor region is part of

Answer 3

transcription

Question 4

A promoter and terminator sequence are used in transcription, where are they located?

Answer 4

Promoter = 5’ end
Terminator = 3’ end

Question 5

Define: operon

Answer 5

Operon: multiple genes that share a promoter

Question 6

What does the transcription of the operon make?

Answer 6

Transcription of the operon makes polycistronic mRNA

Question 7

Transcription has 3 stages - describe

Answer 7

Initiation:
1) Sigma factor helps RNA pol recognize promoter
2) RNA pol binds DNA between -35 and -10 region forming a closed complex
3) RNA pol unwinds DNA forming an open complex
4) RNA synthesis begins and sigma factor falls off

Elongation:
1) NTPs are added to 3’ end of RNA-DNA hybrid
2) DNA is rewound as RNA pol progresses

Termination:
There are 2 ways:

= Factor dependent termination
- Rho factor separate RNA-DNA hybrd

= Intrinsic terminators
- inverted repeats for a hairpin/stem loop, with a poly U tail
- the U A bond is weak, so RNA/DNA dissociates and R pol falls off

Question 8

Define: constitutive genes

Answer 8

Constitutive genes = genes that are always transcribed

Question 9

Name 2 ways transcription can be regulated (general)

Answer 9

1) DNA binding proteins (initiation)
2) mRNA structure (elongation, termination)

Question 10

How does bacteria regulate initiation

Answer 10

Sigma Factors - Regulate Initiation
- bacteria uses multiple promoters, and RnaP requires a sigma factor to bind
- diff sigma factors bind diff promoters
- Thus sigma factors control which genes are transcribed, and a change in the level of sigma factors present change the level of transcription

Question 11

Regulating Initiation - Repressors
Describe

Answer 11

• repressor proteins block initiation
• when a repressor binds, rna p can’t transcribe the gene
• repressors bind the operator region, if a ligand binds them it causes a conformational changing its shape so it can’t bind
• is under negative transcriptional control

Question 12

Negative Control of Inducible Genes
- Describe

Answer 12

• some repressor controlled genes are inducible
  Inducible: repressor binding to operator turns off transcription
• Induce ligand stops repressor from binding to operator, turns transcription on

Question 13

When a ligand binds a repressor, does it turn on or off transcription?

Answer 13

It turns on transcription

Question 14

When a co-repressor binds a repressor, does it turn on or off transcription?

Answer 14

Co-repressors = a ligand that helps repressors bind DNA
Thus, turns off transcription

Question 15

Describe the regulation of the Trp operon

Answer 15

• TrpR = repressor
• Trp = co-repressor

High Trp = don’t need more /trp, so Trp binds TrpR to turn off transcription

Low Trp = since Trp is low, it can’t act as a co-represspr thus the operon is transcribed

Question 16

What example was used for bifunctional activator/repressor?

Answer 16

AraC

Question 17

Attenuation - Define

Answer 17

Attenuation: ribosomal stalling, impacts transcription

Question 18

What causes attenuation?

Answer 18

Low aa abundance causes the ribosome to stall, stalling increases transcription of the operon

Question 19

Tell me about the leader region?

Answer 19

Leader region: ex. TrpL

Location: between the operator and the structural genes
Purpose: encodes for a leader peptide which has no purpose, is just there for attenuation

If TrpL is not being translated:
- 1 and 2, 3 and 4 base pair
- poly U and hairpin form loop for terminator
- RNA P stops transcribing DNA at the poly U tract

If Trp is low, ribosome stalls at Trp codons:
- blocks 1 and 2 from pairing
- 2 and 3 form an antiterminator
- terminator is not formed
- RNAP transcribes genes after DNA poly T tract

If Trp is high, ribosome translates Trp codons, but stalls at TrpL codon:
- blocks pairing of 2 and 3
- 3 and 4 pair forming terminator
- RNAP does not transcribe genes after poly T tract

Question 20

Define Riboswitch

Answer 20

Riboswitch: mRNA leader region that can adopt 2 different conformations affecting transcription

Question 21

What are the 2 conformations of riboswitches

Answer 21

Switch is normally off
- terminator stops at poly T
- can be turned on by metabolite/ligand
- binding promotes formation of anti-terminator, which prevents terminator from forming, thus transcription is not stopped at poly T

Switch is normally on
- transcription does not stop at poly T
- turned off by metabolite
- binding promotes formation of anti-antiterminator
- terminator forms, transcription stops at ply T

Question 22

What was one of the first antibiotics discovered?

Answer 22

Streptomycin

Question 23

Streptomycin
What is it effective against:

Answer 23

Streptomycin
What is it effective against: Gram negatives

Question 24

Define: Aminoglycoside

Answer 24

Aminoglycoside: antibiotic that targets the ribosome

Question 25

Where does the ribosome assemeble?

Answer 25

The ribosome assembles at the ribosome binding site (RBS) - the Shine-Dalgarno sequence

Question 26

Where does the ribosome start and stop?

Answer 26

Start = start codon
Stop = stop codon

Question 27

What does tRNA have at 3’ end?

Answer 27

Has aa attached to 3’ acceptor end
- aminoacyl-tRNA synthetase

Question 28

Aminoacyl-tRNA Synthetase
What are its features

Answer 28

Anticodon binding domain
- recognizes tRNA anticodon
- makes sure its the right reaction

Catalytic domain:
- attaches aa to tRNA

• AA must be activated by ATP

Question 29

What type of bind links aa to tRNA

Answer 29

ester bond

Question 30

What is the bacterial ribosome made of?

Answer 30

rRNA and proteins

Question 31

Ribosome - function

Answer 31

Ribosome: forms peptide bonds between aa’s on tRNA
- ribosome helps tRNA anticodon bind to mRNA codons

Question 32

tRNA function

Answer 32

tRNAs deliver aa to ribosome

Question 33

Describe all the steps of transcription

Answer 33

Initiation
1) Nucleotide in 16S rRNA (30S subunit) binds to mRNA RBS
2) IF3 binds to 30s subunit and ensures 50S subunit does not bind too soon
3) Once mRNA is recruited to 30s, IF2 helps deliver fMet
4) IF1 binds displacing IF3
5) Forms 30S initiation complex
6) 50S subunit joins 30s initiation complex (Needs GTP)
7) IFs are released

Elongation
1) Elongation factor EF-TU delivers tRNA to A site (GTP)
2) tRNA anticodon binds to codon
3) Peptide bind formed between amino acids in A site, and P site
NOTE: 1st aa comes into P site, after that they come into A site

Elongation - Translocation
1) EF-TU and GTP help the ribosome navigate along the mRNA sequence
2) mRNA advances thru the ribosome
3) Uncharged tRNA is in the E site exits
4) t-RNA with peptide moves to P site
5) Another tRNA is delivered to A site, elongation continues

Termination
1) Ribosome stall at stop codon
- UAA, UGA, UAG
- no tRNA
2) Stop codon is recognized by release factors
3) Release factors hydrolyze polypeptide from tRNA
4) Translation complex dissociates

Question 34

Why is the ribosome a good target for antibiotics

Answer 34

Bc the bacterial ribosome is different from the eukaryotic one

Question 35

How do Tetracyclines function

Answer 35

Tetracyclines
- bind to rRNA in 30s subunit (A site)
- occupy the binding site of tRNA anticodons
- block delivery of tRNA

Question 36

Define - Bacteriostatic

Answer 36

Bacteriostatic: inhibits growth without killing
- growth resumes if removed

Question 37

How do Macrolides function?

Answer 37

• Growing poly-p extend thru exit channel
• Macrolides bind to 50S subunit blocking exit tunnel
• prevents elongation of nascent poly-p chain (NC)

Question 38

How do Lincosamides function?

Answer 38

• They bind to the A site of t the 50S subunit
• This disrupts the positioning of A site tRNA in peptidyl transferase center (PTC)
• blocking peptide bond formation

Question 39

Give and example of a Lincosamide

Answer 39

Clindamycin

Question 40

What are some antibiotic resistance mechanisms?

Answer 40

• can limit the amount of antibiotic in cytoplasm
• can prevent the antibiotic from binding to ribosome by:
  - modifying ribosome
  - modifying antibiotic

Question 41

What do ERM groups do?

Answer 41

They change ribosome structure but not function as a means of antibiotic resistance

Question 42

Translational Riboswitches
define
What are the 2 types - Describe

Answer 42

Riboswitch: secondary structure in mRNA leader region (before genes)

1) Sequester - off by default
- RBS is unavailable
- turned ON by ligands
- ligand binding forms anti-sequester

2) Anti-Sequester - on by default
- RBS is available
- turned off by ligands
- ligand binding forms anti-antisequester making RBS unavailable

Question 43

What do sRNAs regulate?

Answer 43

Small RNAs regulate translation

Question 44

What are sRNAs ( 2 types) , What are they capable of?

Answer 44

sRNAs are non-coding RNAs

Cis-encoded = sRNA is produced from the same DNA as mRNA

Trans-encoded = sRNA is produced from some other DNA

Binding to …
- mRNA impacts translation
- RBS blocks initiation
- gene blocks elongation
- leader region prevents a sequester from forming = RBS more accessible = translation increases
- mRNA can target degradation by ribonuclease (translation decreases)