Week 4 Amino Acid/Nitrogen Metabolism

Question 1

What are the main precursors of glucose that the carbon skeleton of glucogenic amino acids can be converted into?

Answer 1

pyruvate, oxaloacetate, other intermediates of the TAC

Question 2

In the fed state, when protein is digested and broken down into amino acids by the small intestine, they are delivered to the _________ where they can be used directly for ___________ synthesis, converted to __________ OR ______ _______, or delivered to other tissues most notably the __________.

Answer 2

When protein is digested and broken down into amino acids by the small intestine, they are delivered to the LIVER where they can be used directly for PROTEIN synthesis, converted to GLUCOSE OR FATTY ACIDS, or delivered to other tissues most notably the MUSCLES.

Note:
-When converted to glucose or fatty acids, those are stored as glycogen and triacylglycerides. This occurs when AA are in excess.

-When delivered to muscles AA’s are used for protein synthesis.

Question 3

What are the main precursors of fatty acids that carbon skeletons of ketogenic amino acids can be converted to?

Answer 3

acetyl -COA and acetoacetyl CoA.

Question 4

In the fasted state, most ___________ amino acids will contribute to the production of _______ via the process of ____________ while others will form ATP by going into the _________ cycle.

Answer 4

In the fasted state, most GLUCOGENIC amino acids will contribute to the production of GLUCOSE via the process of GLUCONEOGENESIS while others will form ATP by going into the KREBS cycle.

Question 5

When in starvation, does the body use ketogenic amino acids?

Answer 5

It certainly can. However, first, it will oxidize fatty acids released from adipose tissue for energy. The whole point of ketogenesis is to preserve proteins so they don’t have to break down.

Question 6

The transamination step is when an _______ group is transferred to another molecule for eventual excretion so it can free the _-_____ _____ to contribute to metabolic pathways.

Answer 6

The transamination step is when an AMINE group is transferred to another molecule for eventual excretion so it can free the ALPHA-KETO ACID (carbon backbone) to contribute to metabolic pathways.

Question 7

T/F: In times of starvation, fatty acids and amino acids are used in gluconeogenesis.

Answer 7

False, only amino acids.

AAs can be converted to pyruvate, oxaloacetate (the first bypass step) in gluconeogenesis, as well as PEP (after converted to OAA). **AA can also be turned into acetyl CoA but those will not contribute to gluconeogenesis.

FA: acetyl CoA can never be converted to pyruvate because 1) the reaction of pyruvate to acetyl-coA is irreversible and 2) Acetyl-CoA only provides 2 carbons for the TAC that are eventually lost before becoming OAA.

Question 8

What happens to excess protein?

Answer 8

It’s excreted, there is no longterm storage for AAs

Question 9

What are the major sources of ammonia/ammonium?

Answer 9

gut bacteria, transamination, deamination, purine/pyrimidine degradation…

Question 10

What are the 3 major fates of amino acids?

Answer 10

1) Synthesis of tissue proteins
2) Synthesis of other important constituents (nucleotides, neurotransmitters, heme, etc.)
3) Catabolism and excretion

Question 11

Describe the two main systems for degrading proteins within the cell.

Answer 11

• Ubiquitin-protease system (UPS) (ATP-dependent) involves tagging protein with ubiquitin and degrading in the proteosome
• Proteases in lysosomes also degrade proteins (ATP-independent)

Question 12

How can you use amino acids for energy?

Answer 12

Direct carbon skeletons into TCA cycle

Question 13

In animals, why can fatty acids not be used for glucose production?

Answer 13

2-C Acetyl CoA product of FA oxidation enters TCA cycle, but 2 CO2 come out, so OAA is regenerated but there is no net gain of OAA, which is also used in gluconeogenesis
Pyruvate dehydrogenase catalyzing pyruvate-> acetyl CoA is irreversible, so 2C acetyl CoA not used to regenerate 3C pyruvate

Question 14

Why do patients with a protein calorie deficiency present with edema and ascites?

Answer 14

In Kwashiorkor, hypoproteinemia, hypoalbuminemia lead to ascites (colloid osmotic pressure reduced, fluid goes to tissue & see edema)
Hepatomegaly from enlarged fatty liver from carbohydrate diet

Question 15

What role do bacteria play in contributing to hyperammonemia?

Answer 15

Bacterial urease causes NH4+ release in the gut, which can increase its levels in the blood.

Question 16

In viral hepatitis, why do you see an increase in serum aminotransferases and jaundice?

Answer 16

Increased liver damage causes increased enzymes in serum
Hepatic damage may result in decreased bilirubin conjugation so less is excreted, resulting in jaundice; this is last hepatocyte function to be lost

Question 17

Why might alcoholism lead to hyperammonemia?

Answer 17

Liver damage can lead to compromised urea cycle and thus the buildup of NH4+.

Question 18

What is a biochemical and physiological consequence of a genetic defect causing a deficiency in a urea cycle enzyme?

Answer 18

Hyperammonemia; defect in earlier enzymes in cycle may cause more severe form; arginase deficiency (argininemia may be asymptomatic. Ornithine transcarbamylase (OTC) deficiency is most common urea cycle disorder.

Question 19

What is ornithine transcarbamoylase?

Answer 19

OTC is a urea cycle enzyme that catalyzes the reaction between ornithine and carbamoyl phosphate and thus allows a nitrogen to enter the cycle.

Question 20

What does a deficiency in OTC do?

Answer 20

A deficiency in OTC causes urea cycle deficiency. Increasing serum ammonia levels result. As an early enzyme in the urea cycle, OTC deficiency may cause a more severe hyperammonemia than other urea cycle enzyme deficiencies.

Question 21

What macromolecule is used first for energy in starvation?

Answer 21

Glycogen broken down to glucose, released from liver to blood

Question 22

When the above glycogen is depleted, what molecules would next be used for fuel in starvation?

Answer 22

Amino acids from proteins, then acetyl CoA from FA oxidation

Question 23

What metabolites accumulate after about 3 days of starvation?

Answer 23

Beta-hydroxybutyric acid and acetoacetic acid
Acetoacetate is normally a source of energy for brain, kidneys, cardiac muscle (not liver). In starvation: it is the principal energy source for brain

Question 24

What acid-base metabolic disorder can develop after 3 days of starvation?

Answer 24

Metabolic acidosis from above acids, and dehydration-related decrease in tissue perfusion (lactic acid increase)

Question 25

What method can be used to conserve glucose for the brain in starvation?

Answer 25

FA breakdown-> increase in Acetyl CoA which inhibits pyruvate dehydrogenase so less glucose converted to pyruvate destined for TCA cycle
Less Acetyl CoA goes into TCA cycle because OAA is depleted via gluconeogenesis, so Acetyl Co A is used in ketone body production

Question 26

The glucose-alanine cycle produces ________ and _______

Answer 26

Glucose and urea

Question 27

What is glycogenolysis, what does it do in starvation and how long does it last?

Answer 27

Break down of glycogen, supplies CNS with glucose for one day.

Question 28

What is the role of amino acids in gluconeogenesis in starvation?

Answer 28

Proteins are degraded into amino acids that are used for gluconeogenesis to supply brain and red blod cells with glucose. Nitrogen excreted via urea cycle.

Muscle prtoein loss is minimized to maintain ability to move.

Question 29

By about 3 days of starvation, gluconeogenesis has depleted _________ required for acetyl CoA to enter TCA cycle. Acetyl CoA from fatty acids is directed toward making _________ in the “protein sparing” phase.

At this time, Acetyl CoA inhibits conversion of pyruvate to Acetyl CoA by allosterically inhibiting ______ ________. This inhibits glucose depletion to save it for the brain.

Answer 29

By about 3 days of starvation, gluconeogenesis has depleted OXALOACETATE required for acetyl CoA to enter TCA cycle. Acetyl CoA from fatty acids is directed toward making KETONES in the “protein sparing” phase.

At this time, Acetyl CoA inhibits conversion of pyruvate to Acetyl CoA by allosterically inhibiting PYRUVATE DEHYDROGENASE. This inhibits glucose depletion to save it for the brain.

*about 1/3 of brains energy on 3d day comes from ketone bodies

Question 30

What is the terminal phase of starvation?

Answer 30

protein degradation increases, weakened diaphragm muscles and compromised immune system. *Survival time is a function of amount of stored triacylglycerols

Question 31

What are the 3 important compounds in amino group transfer?

Answer 31

1) Alpha ketoglutarate, glutamate, glutamine.

Question 32

_____________ (AA) is a major acceptor of amino group and becomes ___________ a major donor of amino groups in biosynthesis.

Answer 32

Alpha-ketoglutarate is a major acceptor of amino group and becomes GLUTAMATE a major donor of amino groups in biosynthesis.

Question 33

The amino acid _________ is a major safe transporter of nitrogen (and ammonia) throughout the blood stream

Answer 33

GLUTAMINE

Question 34

What is PLP? What does it do? What is it made from?

Answer 34

PLP is a cofactor (pyridoxal phosphate) involved in transamination. It is a coenzyme in AA metabolism, heme synthesis, neurotransmitter synthesis, amino acid decarboxylations and other metabolic reactions.

It is made from vitamin B6.

Question 35

Transamination is the process in which an _____ _____ _____ of an alpha-amino acid is transferred to the alpha carbon of ____ ____ ____ and is catalyzed by ________ and PLP.

Answer 35

Transamination is the process in which an ALPHA-AMINO GROUP of an alpha-amino acid is transferred to the alpha carbon of ALPHA KETO ACID and is catalyzed by AMINOTRANSFERASE and PLP.

Question 36

What would happen if you had a vitamin B6 deficiency?

Answer 36

No PLP, no transamination. Decreased synthesis of alpha ketoglutarate in the TAC cycle from amino acids, so less energy. PLP used in (i) catecholamine pathway, (ii) serotonin biosynthesis; and (iii) GABA synthesis from glutamate

Question 37

Describe the structural differences among creatine, creatine phosphate, and creatinine.

Answer 37

Creatine phosphate is the phosphorylated form of creatine, made from glycine and arginine. Creatinine is made via a spontaneous reaction from creatine.

Question 38

What is the importance of creatine phosphate in muscle?

Answer 38

Storage form of the high energy phosphate bond. CP is used to generate ATP quickly when needed.
CP + ADP –> Creatine + ATP Catalyzed by creatine kinase (CK)

Question 39

What are the main functions of glutathione in the cell?

Answer 39

Maintains a reducing environment in cell.
Reduces superoxide radical and other ROS to protect against oxidative damage.
Some enzymes will not function properly if the sulfhydryl group of cysteine is not reduced (if enzyme forms inappropriate disulfide bonds, could create dysfunctional protein structure).

Question 40

Why does NADPH deficiency cause glutathione deficiency?

Answer 40

Need NADPH to reduce oxidized glutathione (GSSG) to 2 GSH (reduced glutathione) and restore oxygen radical scavenging ability to cell.

Question 41

What is the metabolic deficit in acetaminophen toxicity?

Answer 41

Intracellular GSH is depleted when used in detoxification of a catabolite of acetaminophen in Tylenol overdose.

Question 42

How would you treat acetaminophen overdose?

Answer 42

Charcoal administration if caught early (e.g. first 30 min).
Give chemicals to promote synthesis of GSH, e.g. cysteine.
Only perform gastric lavage if absolutely necessary because of the risk of the procedure.

Question 43

Distinguish between porphyria and hyperbilirubinemia.

Answer 43

Porphyria results from a defect in heme biosynthetic pathway; hyperbilirubinemia results from an excess of bilirubin derived from heme catabolism
Many causes for hyperbilirubinema - intrahepatic and extrahepatic.

Question 44

How can histamines cause increased vascular permeability leading to a runny nose associated with an allergic reaction, as well as affect gastric function?

Answer 44

Histamine binds to different histamine receptors (H1-H4) and has many different functions in the body in addition to being released during an allergic response.
Histamine binds the parietal cell histamine H2 receptor and stimulates secretion of protons transported by the H+/K+ ATPase to the gastric lumen (protons used in HCl).
Gastric acid secretion is inhibited by a histamine H2 receptor antagonist like cimetidine, ranitidine (OTC drugs).

Question 45

Describe the role of nitric oxide in relieving angina.

Answer 45

NO binds to and activates soluble guanylate cyclase which causes cGMP synthesis, causing a reduced amount of Ca2+ available for vascular smooth muscle contraction.
Result is
Systemic vasodilation reduces myocardial wall stress and thus decreases myocardial oxygen demand;
Coronary vasodilation improves oxygen delivery to cardiac muscle

Question 46

Why are nitroglycerin patches used in patients with angina?

Answer 46

NO is delivered by gradual breakdown of nitroglycerin to NO. Patches deliver nitroglycerin over time.

Question 47

Speculate why co-administration of an SSRI and OTC tryptophan or an MAOI may be contraindicated in treatment of depression.

Answer 47

“Serotonin syndrome” may be triggered by taking an SSRI and OTC tryptophan (to help with sleep) or a prescribed MAOI that will inhibit serotonin breakdown, as well as degradation of other neurotransmitters. Additive serotonin effects in a bipolar disorder may cause patient to experience a dangerous rapid cycling between mania and depression.

Question 48

Which neurotransmitter catabolic pathways are inhibited by MAOIs?

Answer 48

Breakdown of Dopamine, NE, E, and serotonin inhibited by MAOIs

Question 49

Outline the biochemical pathway for the synthesis of catecholamines.
Tyr —->______ —-> _________—> NE —> E

Answer 49

Catecholamines: Tyr–> DOPA–> dopamine—> NE—> E

Question 50

Why might a drug inhibiting thyroid peroxidase (TPO) be given to a patient with hyperthyroidism?

Answer 50

TPO inhibitor inhibits oxidation of iodide to iodine and inhibits organification step (attachment of Io to Tyr side chains in thyroglobin.)

Question 51

What are the consequences of impaired melanin biosynthesis?

Answer 51

May be more susceptible to skin cancer (role of melanin in photoprotection is still controversial)
Dark hair has mostly eumelanin; red hair comes from production of pheomelanin with very little eumelanin production; blond hair comes from a small amount of eumelanin production, so impaired melanin synthesis would cause light colored hair and skin

Question 52

What color hair would you expect in a patient that has a genetic defect in the pathway for tyrosine biosynthesis?

Answer 52

E.g. Phenylketonuria (PKU)- blond hair- very light color

Question 53

What are some of the reasons that a bruise is colored?

Answer 53

Bruise has several pigments: Hemoglobin (red-blue), catabolites of heme: biliverdin and bilirubin (yellow).
See darker color if capillaries closer to surface.
Older patients bruise more easily with thinner skin or if on an anti-coagulant like aspirin.