Biochemistry. Just kill me now.

Question 1

mRNA start codon:

Answer 1

AUG

AUG AUGments protein synthesis

Question 2

What does AUG code for in prokaryotes?

Eukaryotes?

Answer 2

Prokaryotes = formylmethionine
Eukaryotes = methionine

Question 3

mRNA stop codons (3):

Answer 3

UGA
UAA
UAG
U Go Away, U Are Away, U Are Gone

Question 4

What is an operon (3 components)?

Answer 4

Structural genes to be transcribed
Regulatory regions
Promoter region

Question 5

Four common structural features shared by proteins that interact with DNA:

Answer 5

helix-loop-helix
helix-turn-helix
Zn fingers
leucine zippers

Question 6

What are the three types of RNA?

Answer 6

rRNA
mRNA
tRNA
Rampant, massive, and tiny.

Question 7

T/F: Enhancers and repressors control whether a gene is transcribed.

Answer 7

F. Response elements control the RATE of transcription, not whether it happens.

Question 8

Features of promoter sequences (3):

Answer 8

Upstream
Rich in AT
TATA or CAAT box

Question 9

What is an operator region?

Answer 9

It is where inducers and repressors bind, usually located between the promoter region and start.

Question 10

Briefly review the function of the lac operon.

• Transcription factor
• Repressor
• Conditions

Answer 10

lac = codes for b-galactosidase (lactose -> glucose + galactose).
Tx factor CAP is bound when there is no glucose.
Repressor lac is bound when there is no lactose.
Make product only when the repressor is gone (there is lactose) and when CAP is unbound (there is glucose).

Question 11

What are the three eukaryotic RNA polymerases and what do they do?

Answer 11

RNA pol I makes rRNA
RNA pol II makes mRNA
RNA pol III makes tRNA

Question 12

This substance inhibits eukaryotic RNA polymerase II:

Main manifestation of its toxicity?

Answer 12

a-amanitin.

Hepatotoxic.

Question 13

The two ways in which transcription can be terminated in prokaryotes:

Answer 13

rho-dependent ATPase

rho-indepedent (GC-rich hairpin turn followed by a weak point rich in UUUUUUfall right off)

Question 14

T/F: Prokaryotes have more than one polymerase:

Answer 14

F. They just have the one, it makes all three kinds of RNA.

Question 15

Drug that inhibits prokaryotic RNA polymerase and turns your pee red:

Answer 15

Rifampin

Question 16

Where is rRNA made?
mRNA?
tRNA?

Answer 16

rRNA is made in the nucleolus.

mRNA and tRNA are made in the nucleoplasm.

Question 17

Before RNA leaves the nucleus it needs to be processed to become mRNA and gain the ability to leave. Three major processing events:

Answer 17

1. 5’ cap addition (SAM needed)
2. Poly-A tail
3. Introns spliced out (by spliceosome)

Question 18

What is the co-factor required for adding a 5’ cap to hnRNA?

Answer 18

SAM

Question 19

Poly-A polymerase recognizes this polyadenylation signal:

Answer 19

AAUAAA

Question 20

Patients with lupus make antibodies against this piece of pre-mRNA processing machinery:

Answer 20

Spliceosomal snRNPs.

These are part of the spliceosome used to remove introns.

Question 21

Which part of a transcript gets to leave the nucleus: Intron or exon?

Answer 21

EXon is EXpressed and EXits the nucleus

Question 22

Does tRNA synthetase work at the 5’ or 3’ end of tRNA? What special marker is at this end?

Answer 22

tRNA synthetase works at the 3’ end.

This end always has CCA.

Question 23

T/F: Amino acids destined for transfer are bound hydrostatically to the 5’ end of tRNA.

Answer 23

F. The bond is covalent, and it is found at the 3’ end.

Question 24

The ribosome in prokaryotes is a __S ribosome composed of these two subunits:

Answer 24

30S + 50S -> 70S

PrOkaryotic = Odd numbers

Question 25

The ribosome in eukaryotes is a __S ribosome composed of these two subunits:

Answer 25

40S + 60S -> 80S

Eukaryotic = Even numbers

Question 26

Where is the prokaryotic ribozme?

Answer 26

It is a 23S rRNA Inside the 50S subunit.

Question 27

tRNA bound with ATP is in what state?

tRNA bound with GTP is in what state?

Answer 27

ATP bound tRNA is “charged” with its amino acid.

GTP bound tRNA is in the process of translocation.

Question 28

Initiation of protein synthesis is activated by this hydrolytic reaction:

Answer 28

GTP hydrolysis

Question 29

This enzyme catalyzes peptide bond formation during protein synthesis. It has two names:

Answer 29

Ribozyme = peptidyltransferase

Question 30

Where are ribosomes made?

Answer 30

In the nucleus.

Question 31

In order to accomplish translocation during protein synthesis, this protein is required in eukaryotes. What is its prokaryotic analogue?

Answer 31

Eukaryotic: EF-2
Prokaryotic: EF-G

Question 32

In eukaryotes, which ribosomal subunit docks with mRNA first?
This subunit needs help, what proteins help it dock?

Answer 32

40S binds first with the help of initiation factors

Question 33

Describe the orientation of the entrance and exit sites for peptide bond formation on the 60S subunit:

Answer 33

A site is near the 3’ end, for Aminoacyl-tRNA.
P site is in the middle, for the growing Peptide.
E site is at the end, it holds Empty tRNA Exiting.

Question 34

These antibiotics inhibit initiation complex formation and cause mRNA mis-reading:

Answer 34

Aminoglycosides

Question 35

These antibiotics bind the 30S subunit of prokaryotic ribosomes and keep tRNA out of the A site:

Answer 35

Tetracyclines

prevent tRNA from binding

Question 36

Two antibiotics that work at the 30S subunit:

Answer 36

Aminoglycosides
Tetracyclines
buy AT 30
CCELL at 50

Question 37

These 6 antibiotics work at the 50S subunit of the ribosome:

Answer 37

Chloramphenicol
Clindamycin
Erythromycin (& other macrolides)
Linezolid
Lincomycin
Streptogramin

Question 38

These antibiotic binds the 50S su and inhibit peptidyltransferase (2).
This antibiotic binds the 30S su and inhibits tRNA docking.

Answer 38

Chloramphenicol & streptogramins

Tetracyclines

Question 39

Mechanism of action for macrolides, linezolid, and clindamycin:

Answer 39

Bind 50S and prevent the spent tRNA from leaving once it has donated its amino acid.

Question 40

Mechanism of action of tetracyclines:

Answer 40

Bind 30S and block tRNA from entering the A.

Tetracyclines are not good for babies.

Question 41

How do aminoglycosides work?

Answer 41

They bind the 30S subunit and inhibit initiation complex formation.

Question 42

T/F: Cyclin-dependent kinases are constitutively inactive.

Answer 42

T. They need cyclins to activate them.

Question 43

Two important tumor suppressors at the G0 to S transition in the cell cycle:

Answer 43

p53

Rb

Question 44

What kind of cells are exemplified by bone marrow, skin, and other germ cells?

Answer 44

Labile cells

Question 45

Hepatocytes and lymphocytes are capable of entering G1 when prompted, these cells are known as:

Answer 45

Stable or quiescent cells

Question 46

These cells remain in G0. Regeneration happens from stem cells:
Examples (3)?

Answer 46

Permanent cells.

Ex neurons, skeletal / cardiac muscle, RBCs

Question 47

rER in neurons is aka:

You would not see this substance in what portion of the neuron?

Answer 47

Nissl substance.

Nissl bodies are absent from axons

Question 48

What happens in rER (2 big things)?

Answer 48

1. Synthesis of exported proteins

2. Addition of N-linked oligosaccharides

Question 49

What happens in smooth ER?

Answer 49

1. Steroid synthesis

2. Detoxification of drugs and poisons

Question 50

This cellular organelle will be enormous in people sniffing a lot of glue:

Answer 50

Smooth ER

Question 51

The golgi has 5 main jobs:

Answer 51

1. Distribution center
2. Modifies N-linked oligosaccharides
3. Adds O-oligosaccharides
4. Adds M-6-P
5. Forms proteoglycans / sulfates sugars

Question 52

N-linked oligosaccharides are modified on which amino acid? in which organelle does this happen? In what organelle were they added to a protein in the first place?

Answer 52

Asparagine
Golgi
rER

Question 53

O-linked oligosaccharides are modified by the golgi on two amino acids:

Answer 53

Serine

Threonine

Question 54

What happens if mannose-6-phosphate is not added to certain proteins in the golgi?

Answer 54

I-cell disease = inclusion cell disease. M-6-P targets proteins to the lysosome. No M-6-P = proteins leave the cell instead of going to the lysosome.

Question 55

What is the enzyme that adds M-6-P to lysosome proteins in the golgi?

Answer 55

Phosphotransferase.

Question 56

Three features of I cell disease:

Answer 56

Coarse facies
Clouded corneas
Restricted joint movement…
2/2 high levels of lysosomal enzymes

Question 57

This organelle catabolizes very long chain fatty acids and amino acids:

Answer 57

Peroxisome

Question 58

Three modes of protein degradation:

Answer 58

1. Ubiquitin-dependent (in a proteasome)
2. Lysosomal
3. Calcium-dependent cytosolic enzymes

Question 59

What is the cause of I cell disease?

Answer 59

Deficiency in M-6-P leading to defective trafficking of lysosomal-bound proteins and excretion.

Question 60

5 drugs that act on microtubules:

Answer 60

Mebendazole / thiabendazole (for BENDy worms)
Griseofulvin
Vincristine / vinblastine
Paclitaxel
Colchicine

Question 61

What does Chediak-Higashi syndrome have to do with microtubules?

Answer 61

LYST = mutated lysosome traffic regulator gene. Needed for microtubule-dependent sorting of endosomal proteins into late endosomes.

Question 62

This protein is responsible for retrograde movement down the micrtubule.
This one is responsible for anterograde.

Answer 62

Dynein (moves from assembing end to assembling end).

Kinesin

Question 63

Characteristic arrangement of microtubules in a cilum:

Answer 63

9+2

Question 64

Defect found in Kartagener’s syndrome:

Answer 64

Immotile cilia

Defect is in the dynein arm.

Question 65

Connective tissue can be identified by this immunohistochemical stain:

Answer 65

Vimentin

Question 66

Muscle can be identified by this immunohistochemical stain:

Answer 66

Desmin

Question 67

Epithelial cells can be identified by this immunohistochemical stain:

Answer 67

Cytokeratin

Question 68

Neuroglia can be identified by this immunohistochemical stain:

Answer 68

GFAP identifies neuroGlia

Question 69

This immunohistochemical stain identifies Neurons:

Answer 69

Neurofilament stain

Question 70

This immunohistochemical stain can be used to identify adrenal neuroblastoma:

Answer 70

Neurofilament

Question 71

This immunohistochemical stain can be used to identify astrocytomas:

Answer 71

GFAP

Question 72

Cilia use this organizational feature to coodinate contraction:

Answer 72

Gap junctions

Question 73

This drug inhibits the Na+/K+ ATPase by binding to the K+ site:

Answer 73

Ouabain

Question 74

Drug that inhibits the Na+/K+ ATPase directly:

Answer 74

Digoxin / digitoxin

Question 75

Type of collagen defective in OI:

Answer 75

Type I

Question 76

Type of collagen most frequently defective in Ehlers-Danlos:

Answer 76

Type III

Question 77

Type of collagen defective in Alport syndrome:

Answer 77

Type IV

Question 78

Where would you find Type I collagen?

Answer 78

Bone
Skin
Tendons

Question 79

Where would you find Type II collagen?

Answer 79

Cartilage

Question 80

Where would you find Type III collagen?

Answer 80

Reticulin-containing organs:
Skin
Blood vessels
Uterus / fetal tissue
Granulation tissue

Question 81

Where would you find Type IV collagen?

Answer 81

Basement membrane

Question 82

Collagen synthesis begins with this molecule:

Answer 82

Pre-pro-collagen

Question 83

Hydroxylation of pre-pro-collagen requires this vitamin:

Answer 83

Vitamin C

Question 84

Deficiency in vitamin C leads to a defect at which point in the synthesis of collagen?

Answer 84

Hydroxylation of pre-pro-collagen at lysine and proline residues.

Question 85

What is procollagen made of?

Answer 85

Glycosylated hydroxylysine residues wound in a triple helix.

Question 86

What structural feature of pro-collagen is distorted in osteogenesis imperfecta?

Answer 86

Triple helix

Question 87

Problems with cross-linking tropocollagen lead to this inherited connective tissue disease:

Answer 87

Ehlers-Danlos

Question 88

Mode of inheritence of OI:

Answer 88

Autosomal dominant

Question 89

Four very common presenting features of OI:

Answer 89

1. Multiple fractures, minimal trauma
2. Blue sclerae
3. Hearing loss
4. Dental problems due to lack of dentin

Question 90

What is the defect in Alport syndrome?

Answer 90

Type IV collagen

Question 91

Most common mode of inheritence for Alport syndrome:

Answer 91

X-linked recessive

Question 92

Three common features of Alport syndrome:

Answer 92

1. Progressive hereditary nephritis
2. Deafness
3. Lenticonus = thinning of capsule around lens
   “Can’t SEE, can’t PEE, can’t HEAR me.”

Question 93

Enzyme that breaks down elastin?

Protein that inhibits this enzyme?

Answer 93

Elastase

a1-antitrypsin

Question 94

Emphysema in a young non-smoker, think:

Answer 94

a1-antitrypsin deficiency

Question 95

Marfan’s syndrome is caused by a defect in this protein. What is its function?

Answer 95

Fibrillin.

Function is to be the “scaffold” for tropoelastin in elastin formation.

Question 96

In what tissues is elastin particularly important?

Answer 96

Blood vessels
Alveoli
Larynx
Spine

Question 97

First step in the metabolism of alcohol is catalyzed by this enzyme:
Drug that inhibits this enzyme?

Answer 97

Alcohol dehydrogenase.

Fomepizole

Question 98

The enzyme alcohol dehydrogenase is limited by this reagent:

Answer 98

NAD+

Question 99

Enzyme that catalyzes acetaldehyde -> acetate in alcohol metabolism:
Drug that inhibits this enzyme?

Answer 99

Acetaldehyde dehydrogenase.

Antabuse

Question 100

Antidote for methanol and ethylene glycol poisoning?

Answer 100

Fomepizole

Question 101

Mechanism of action of antabuse:

Answer 101

Blocks acetaldehyde dehydrogenase, allows acetaldehyde to build up. Instant hang-over.

Question 102

Explain the mechanism behind ethanol-induced hypoglycemia (5 steps):

Answer 102

1. NADH/NAD+ ratio is increased (need NAD+ to metabolize alcohol)
2. Detoxifying = more important than gluconeogenesis, so pyruvate -> lactate and OAA -> malate to generate NAD+ for detox.
3. TCA cycle shuts down, depletion of OAA.
4. Acetyl CoA -> ketone production, not gluconeo.
5. Malate -> NADPH -> FA synthesis.

Question 103

Severe protein malnutrition is aka:

Four big signs:

Answer 103

Kwashiorkor
Malnutrition (skin lesions, hypopigmentation)
Edema (protein holds water in place)
Anemia
Liver is fatty (can’t make apoB100, fats can’t leave liver)

Question 104

Energy malnutrition is aka:

Answer 104

Marasmus

Question 105

Rate-limiting enzyme for glycolysis:

Answer 105

Phosphofructokinase-1

= PFK-1

Question 106

Rate-limiting enzyme for gluconeogenesis:

Answer 106

Fructose-1,6-bisphosphatase

Question 107

Rate-limiting enzyme for glycogen synthesis:

Answer 107

Glycogen synthase

Question 108

Rate-limiting enzyme for glycogenolysis:

Answer 108

Glycogen phosphorylase

Question 109

This enzyme is responsible for trapping glucose in the cell:

Version in the liver and glucose-regulating cells? Version in skeletal muscle and adipose?

Answer 109

Glucokinase
LIver cells have glucokinase
Adipose / skeletal muscle cells have hexokinase

Question 110

Enzyme responsible for glucose-6-phosphate release from the cell as glucose:

Answer 110

Glucose-6-phosphatase

Question 111

Enzyme responsible for generating pyruvate:

Answer 111

Pyruvate kinase

Question 112

Enzyme responsible for converting pyruvate to oxaloacetate:

Answer 112

Pyruvate carboxylase

Question 113

Enzyme that sends pyruvate into the TCA cycle:

5 co-factors required to do this:

Answer 113

Pyruvate dehydrogenase
Makes Acetyl-CoA from pyruvate
Thiamine (B1)
Lipoic acid
CoA (B5)
FAD (B2)
NAD (B3 = niacin)

Question 114

Main presenting feature of glycolytic enzyme disease:

Answer 114

RBC cannot maintain their Na/K-ATPase -> hemolytic anemia.

Question 115

Most common glycolytic enzyme deficiency:

Answer 115

Pyruvate kinase deficiency

Question 116

Pyruvate has four major fates. What are they, and what is the rate-limiting enzyme that takes it down that path?

Answer 116

1. Alanine cycle (ALT)
2. Cori cycle (make lactate, LDH)
3. TCA cycle (PDH, make acetylCoA)
4. Oxaloacetate (Gluconeogenesis, P.carboxylase)

Question 117

Three main features of arsenic poisoning:

Answer 117

Garlic breath
Vomiting
Rice water stool

Question 118

Pyruvate dehydrogenase deficiency can come about in three ways:

Answer 118

Congenital (X-linked)

Acquired (arsenic poisoning, vitamin deficiency)

Question 119

Pyruvate dehydrogenase deficiency results in this major metabolic disturbance. Why?

Answer 119

Lactic acidosis, this is because pyruvate can’t enter the TCA cycle, so it builds and gets shunted down the Cori cycle.

Question 120

Treatment of pyruvate dehydrogenase deficiency:

Answer 120

High fat diet

Lysine and Leucine onLy pureLy ketogenic amino acids

Question 121

Vitamin deficiencies that can lead to pyruvate dehydrogenase deficiency:

Answer 121

Thiamine (B1)
Lipoic acid (remember arsenic messes this one up)
CoA (B5)
FAD (B2)
NAD (B3, niacin)

Question 122

Enzyme that starts the Kreb cycle:

Answer 122

Citrate synthetase

Question 123

Substances that inhibit Complex I of the ETC (3):

Answer 123

Amytal (barbiturate)
Rotenone (fish poison)
MPP (from MPTP, of home opiate lab fame)

Question 124

This substance inhibits Complex III of the ETC:

Answer 124

Antimycin A

Question 125

These substances inhibit Complex IV of the ETC (4):

Answer 125

CN
CO
H2S
N3 (sodium azide)

Question 126

This substance inhibits Complex IV of the ETC, aka the ATP synthase:

Answer 126

Oligomycin

Question 127

Name as many substances that are wrenches in the ETC as you can:

Answer 127

Rotenone
Amytal
MPP
Antimycin A
CN
CO
N3-
H2S

Question 128

What is the goal, overall, in simplistic terms, of the ETC?

Answer 128

1. Send NADH electrons down a chain of molecules.
2. Build high H+ concentration in the intermembranous space, use it to drive ATP production in the mitochondrial matrix.
3. Final acceptor = water.

Question 129

What is the mechanism of action of oligomycin?

Answer 129

It directly inhibits ATP synthesis.

Question 130

What is an uncoupling agent?

Can you name 3?

Answer 130

Something that increases the permeability of the mitochondrial inner membrane. This causes consumption of oxygen and dissipation of heat.
2,4-DNP, aspirin, thermogenin

Question 131

Why can’t muscle do gluconeogenesis?

Answer 131

It does not have glucose-6-phosphatase, can’t release glucose.

Question 132

T/F: Even chain fatty acids can serve as a glucose source.

Answer 132

F. They can only make acetyl-CoA. Odd chain FA yield propionyl-CoA, which can go into the TCA cycle.

Question 133

What are the four irreversible enzymes of gluconeogenesis?

Answer 133

Pathway Produces Fresh Glucose:
Pyruvate carboxylase
PEP carboxykinase
Fructose-1,6-bisphosphatase
Glucose-6-phosphatase

Question 134

What five really huge things do you need NADPH for?

Answer 134

Needed for reductive reactions:
1.  Making fatty acids / cholesterol
2.  Making O2 free radicals
3.  Protecthing RBCs from free radicals
4.  In the CYP450 system
Also needed for: 
5.  Ribose (nucleotide synthesis)

Question 135

Which tissues in the body use the pentose phosphate pathway?

Answer 135

Lactating mammary glands
Liver
Adrenal cortex (… anything making fatty acids / steroids)
RBCs (reducing, protect themselves)

Question 136

Three important enzymes in respiratory burst and what each makes:

Answer 136

NADPH oxidase (makes O2 free radicals)
SOD (makes H2O2)
Myeloperoxidase (makes HoCl)

Question 137

NADPH oxidase deficiency results in this immune deficiency disease:

Answer 137

Chronic granulomatous disease

Question 138

What is the overall purpose of the HMP shunt (aka pentose phosphate pathway)?

Answer 138

Make NADPH from G-6-P.

NADPH = used in reductive reactions.

Question 139

Think of this as the body’s endogenous anti-oxidant when it is in its reduced form:

Answer 139

Glutathione

Question 140

Enzyme defect that leads to an inability to keep glutathione reduced:

Answer 140

G-6-P deficiency, these cells have no NADPH to help them.

Question 141

Mode of inheritence of G-6-P deficiency:

Answer 141

X-linked recessive

Question 142

Two features of RBCs in someone with G-6-P deficiency:

Answer 142

Heinz bodies = oxidized Hb

Bite cells

Question 143

Pathogenesis behind G-6-P deficiency:

Answer 143

Low NADPH in RBC -> hemolytic anemia especially in the presence of oxidizing agents

Question 144

Name 5 things that can precipitate massive hemolysis in someone with G-6-P deficiency:

Answer 144

Infection
TB drugs
Sulfonamides
Fava beans
Primaquine

Question 145

The milder disorder of fructose metabolism:

Answer 145

Essential fructosuria

Question 146

Deficiency of aldolase B:

What does it cause?

Answer 146

Fructose intolerance. Fructose -> fructose-1-phosphate eats up available phosphate. Glycogenolysis and gluconeogenesis are both inhibited.

Question 147

Symptoms of fructose intolerance:

Answer 147

Vomiting
Hypoglycemia
Cirrhosis
Jaundice

Question 148

Symptoms of essential fructosuria:

Answer 148

Mild diuresis on high intake, otherwise none.

Question 149

Enzyme deficient in essential fructosuria?

In fructose intolerance?

Answer 149

Essential fructosuria = fructokinase

Fructose intolerance = aldolase B (FAB)

Question 150

Two disorders of sugar metabolism that can cause infantile cataracts:
Which is the more severe?

Answer 150

Galactokinase deficiency

Galactosemia *

Question 151

Substance that accumulates in galactokinase deficiency:

Answer 151

Glactitol

Question 152

Enzyme defective in classic galactosemia:

T/F: This enzyme is used earlier in galactose metabolism than galactokinase, resulting in more severe disease.

Answer 152

Galactose-1-P uridyltransferase.
F. This enzyme is actually downstream, both galactose-1-P and galactitol build up -> cataracts, liver problems, mental retardation.

Question 153

What is the action of insulin on protein kinase A and glycolysis?

Answer 153

INsulin INactivates glycogenolysis.

Question 154

Epinephrine and glucagon share this action on protein kinase A

Answer 154

They both increase cAMP and activate protein kinase A