Biochem FA - p85 - 94 Metabolism

Question 1

Answer 1

Question 2

In skeletal muscle, glycogen converted to?

Answer 2

Glycogen undergoes glycogenolysis–> glucose-1-phosphate –> glucose-6-phosphate

Question 3

First step of glycogenolysis

Answer 3

Glycogen phosphorylase liberates glucose-1-phosphate residues off branched glycogen until 4 glucose units remain on a branch.

Question 4

T or F Glycogen is only degraded in the cytosol

Answer 4

F - A small amount of glycogen is degraded in lysosomes by α-1,4-glucosidase (acid maltase).

Question 5

What happens once glycogen phosphorylase has done its job?

Answer 5

Then 4-α-d-glucanotransferase (debranching enzyme ) moves 3 of the 4 glucose units from the branch to the linkage. Then α-1,6-glucosidase (debranching enzyme ) cleaves off the last residue, liberating glucose.

Question 6

Name the types of Glycogen storage disease (I, II, III, and V) and what the enzyme deficiency is

Answer 6

Von Gierke - G6Pase

Pompe - acid maltase (Lysosomal acid α-1,4glucosidase with α-1,6-glucosidase activity)

Cori disease - Debranching enzyme (α-1,6-glucosidase)

McArdle - Skeletal muscle glycogen phosphorylase (Myophosphorylase)

Question 7

Answer 7

Treatment: frequent oral
glucose/cornstarch; avoidance
of fructose and galactose
Impaired gluconeogenesis and
glycogenolysis

Question 8

Answer 8

PomPe trashes the PumP (1st and 4th letter; heart, liver, and muscle)

Question 9

Answer 9

Gluconeogenesis is intact

Question 10

Answer 10

Blood glucose levels typically
unaffected
McArdle = Muscle

Question 11

Findings

Answer 11

Progressive neurodegeneration,
developmental delay, hyperreflexia,
hyperacusis, “cherry-red” spot on
macula A , lysosomes with onion
skin, no hepatosplenomegaly (vs
Niemann-Pick).

Question 12

deficient enzyme

Answer 12

heXosaminidase A

(“TAy-SaX)

Question 13

Accumulated Substrate

Inheritance

Answer 13

GM₂ ganglioside

AR

Question 14

findings

Answer 14

Early: triad of episodic peripheral
neuropathy, angiokeratomas B ,
hypohidrosis.
Late: progressive renal failure,
cardiovascular disease.

Question 15

deficient enzyme

Answer 15

α-galactosidase A

Question 16

accumulated subtrate

inheritance

Answer 16

Ceramide
trihexoside
(globotriaosylceramide)

XR

Question 17

Metachromatic
leukodystrophy

findings

Answer 17

Central and peripheral demyelination
with ataxia, dementia.

Question 18

Metachromatic
leukodystrophy

deficient enzyme

Answer 18

Arylsulfatase A

Question 19

Metachromatic
leukodystrophy

accumulated substrate

inheritance

Answer 19

Cerebroside sulfate

AR

Question 20

Krabbe disease

findings

Answer 20

Peripheral neuropathy, destruction
of oligodendrocytes, developmental
delay, optic atrophy, globoid cells.

Question 21

Krabbe disease

deficient enzyme

Answer 21

Galactocerebrosidase

(galactosylceramidase)

Question 22

Krabbe disease

accumulated substrate

inheritance

Answer 22

Galactocerebroside, psychosine

AR

Question 23

Findings

Answer 23

Most common.
Hepatosplenomegaly, pancytopenia,
osteoporosis, avascular necrosis of
femur, bone crises, Gaucher cells C
(lipid-laden macrophages resembling
crumpled tissue paper).

Question 24

deficient enzyme

Answer 24

Glucocerebrosidase
(β-glucosidase); treat
with recombinant
glucocerebrosidase

Question 25

accumulated substrate

inheritance

Answer 25

glucocerebroside

AR

Question 26

findings

Answer 26

Progressive neurodegeneration,
hepatosplenomegaly, foam cells
(lipid-laden macrophages) D ,
“cherry-red” spot on macula A .

Question 27

deficient enzyme

Answer 27

sphingomyelinase

No man picks (Niemann-Pick) his nose with
his sphinger (sphingomyelinase).

Question 28

accumulated substrate

inheritance

Answer 28

sphingomyelin

AR

Question 29

Hurler syndrome findings

Answer 29

Developmental delay, gargoylism,
airway obstruction, corneal clouding,
hepatosplenomegaly.

Question 30

Hurler syndrome deficient enzyme

Answer 30

α-l-iduronidase

Question 31

Hurler syndrome :

accumulated substrate

inheritance

Answer 31

Heparan sulfate,
dermatan sulfate

AR

Question 32

Hunter syndrome findings

Answer 32

Mild Hurler + aggressive behavior, no
corneal clouding.

Question 33

Hunter syndrome deficient enzyme

Answer 33

Iduronate-2-sulfatase

Question 34

Hunter syndrome:

Accumulated substrate

inheritance

Answer 34

Heparan sulfate,
dermatan sulfate

XR

Question 35

Fatty acid synthesis requires transport of _______
from __________ to ______. Predominantly
occurs in ______, _____ _________ ______, and
______ _______.

Answer 35

Fatty acid synthesis requires transport of citrate
from mitochondria to cytosol. Predominantly
occurs in liver, lactating mammary glands, and
adipose tissue.

“SYtrate” = SYnthesis.

Question 36

Long-chain fatty acid (LCFA) degradation
requires _______-________ transport into the
___________ _______.

Answer 36

Long-chain fatty acid (LCFA) degradation
requires carnitine-dependent transport into the
mitochondrial matrix.

CARnitine = CARnage of fatty acids.

Question 38

Systemic 1° carnitine deficiency—

_______ defect in transport of ______ into the
_________ –>Ž toxic accumulation. Causes
________, ________, and ________ ________.

Answer 38

Systemic 1° carnitine deficiency—

inherited defect in transport of LCFAs into the
mitochondria Ž toxic accumulation. Causes
weakness, hypotonia, and hypoketotic
hypoglycemia.

Question 39

Medium-chain acyl-CoA dehydrogenase
deficiency—

___ ability to break down _____

_____ into acetyl-CoA Ž accumulation
of fatty acyl ______ in the blood with
_______ _______.

Answer 39

Medium-chain acyl-CoA dehydrogenase
deficiency—

dec ability to break down fatty
acids into acetyl-CoA Ž accumulation
of fatty acyl carnitines in the blood with
hypoketotic hypoglycemia.

Question 40

Medium-chain acyl-CoA dehydrogenase
deficiency—

Causes _____, _____, ______, ______, ______ ______, ______.

Can lead to ______ ______in infants or children.

Treat by avoiding ______.

Answer 40

Medium-chain acyl-CoA dehydrogenase
deficiency—

Causes vomiting, lethargy, seizures, coma, liver dysfunction, hyperammonemia.

Can lead to sudden death in infants or children.

Treat by avoiding fasting.

Question 41

In the _____, fatty acids and amino acids
are metabolized to _____and
_____(to be used in muscle and brain).

Answer 41

In the liver, fatty acids and amino acids
are metabolized to acetoacetate and
β-hydroxybutyrate (to be used in muscle and brain).

Question 42

In prolonged starvation and diabetic ketoacidosis, _____ is depleted for gluconeogenesis.

In alcoholism, excess _____ shunts oxaloacetate to _____ .

All of these processes lead to a buildup of _____ ,
which is shunted into ketone body synthesis.

Answer 42

In prolonged starvation and diabetic ketoacidosis, oxaloacetate is depleted for gluconeogenesis.

In alcoholism, excess NADH shunts oxaloacetate to malate.

All of these processes lead to a buildup of acetyl-CoA,
which is shunted into ketone body synthesis.

Question 43

Ketone bodies: _____, _____, _____.
Breath smells like _____(fruity odor).
Urine test for ketones can detect _____, but not _____.
RBCs cannot utilize ketones; they strictly use
_____.
HMG-CoA _____ for ketone production.
HMG-CoA _____ for cholesterol synthesis.

Answer 43

Ketone bodies: acetone, acetoacetate, β-hydroxybutyrate.
Breath smells like acetone (fruity odor).
Urine test for ketones can detect acetoacetate, but not β-hydroxybutyrate.
RBCs cannot utilize ketones; they strictly use
glucose.
HMG-CoA lyase for ketone production.
HMG-CoA reductase for cholesterol synthesis.

Question 44

Answer 44

Question 45

Fasting and starvation

Priorities are to supply sufficient _____ to the _____ and _____ and to preserve _____ .

Answer 45

Fasting and starvation

Priorities are to supply sufficient glucose to the brain and RBCs and to preserve protein.

Question 46

Fed state (after a meal)

_____ and _____ respiration.

_____ stimulates storage of _____ , _____ , and _____ .

Answer 46

Fed state (after a meal)

Glycolysis and aerobic respiration.

Insulin stimulates storage of lipids, proteins, and glycogen.

Question 47

Fasting (between meals)

Hepatic _____ (major); hepatic _____ , adipose release of _____ (minor).

_____ and _____ stimulate use of fuel reserves.

Answer 47

Fasting (between meals)

Hepatic glycogenolysis (major); hepatic gluconeogenesis, adipose release of FFA (minor).

Glucagon and epinephrine stimulate use of fuel reserves.

Question 48

Starvation days 1–3

Blood glucose levels maintained by:
ƒ-_____ glycogenolysis
ƒƒ-Adipose release of _____
ƒƒ-_____ and _____ , which shift fuel use from
_____ to FFA
ƒ-ƒHepatic _____ from peripheral tissue _____ and _____ , and from adipose tissue _____ and _____-_____ (from odd-chain FFA—the only triacylglycerol components that contribute to gluconeogenesis)

Glycogen reserves depleted after day _.
RBCs lack _____ and therefore cannot
use ketones.

Answer 48

Starvation days 1–3

Blood glucose levels maintained by:
ƒ-ƒHepatic glycogenolysis
ƒƒ-Adipose release of FFA
ƒƒ-Muscle and liver, which shift fuel use from
glucose to FFA
ƒ-ƒHepatic gluconeogenesis from peripheral tissue lactate and alanine, and from adipose tissue glycerol and propionyl-
CoA (from odd-chain FFA—the only triacylglycerol components that contribute to gluconeogenesis)

Glycogen reserves depleted after day 1.
RBCs lack mitochondria and therefore cannot
use ketones.

Question 49

Starvation after day 3

_____ stores (_____ _____ become the main source of energy for the brain). After these are depleted, vital protein degradation accelerates, leading to organ failure and death.
Amount of excess stores determines survival time.

Answer 49

Starvation after day 3

Adipose stores (ketone bodies become the main source of energy for the brain). After these are depleted, vital protein degradation accelerates, leading to organ failure and death.
Amount of excess stores determines survival time.

Question 50

Answer 50

Question 51

Cholesteryl ester transfer protein fxn

Answer 51

Mediates transfer of cholesterol esters to other lipoprotein particles.

Question 52

Hepatic lipase fxn

Answer 52

Degrades TGs remaining in IDL.

Question 53

Hormone-sensitive lipase fxn

Answer 53

Degrades TGs stored in adipocytes.

Question 54

Lecithin-cholesterol acyltransferase fxn

Answer 54

Catalyzes esterification of 2⁄3 of plasma cholesterol.

Question 55

Lipoprotein lipase fxn

Answer 55

Degrades TGs in circulating chylomicrons.

Question 56

Pancreatic lipase fxn

Answer 56

Degrades dietary TGs in small intestine.

Question 57

PCSK9 fxn

Answer 57

Degrades LDL receptor –> Inc serum LDL. Inhibition –> Inc recycling of LDL receptor –> decserum LDL.

Rx/ Alirocumab, evolocumab

Question 58

Apo E fxn

Answer 58

Mediates rEmnant uptake

(Everything Except LDL)

Question 59

Apo A-I fxn

Answer 59

Activates LCAT

Question 60

Apo C-II fxn

Answer 60

Lipoprotein lipase Cofactor that Catalyzes Cleavage

Question 61

Apo B-48 fxn

Answer 61

Mediates chylomicron secretion into lymphatics

Only on particles originating from the intestines

Question 62

Apo B-100 fxn

Answer 62

Binds LDL receptor

On VLDL, IDL, LDL

Only on particles originating from the liver

Question 63

If you have LCAT or A-1 def, then you have dec _____?

Answer 63

HDL

Question 64

Lipoprotein functions

Lipoproteins are composed of varying proportions of _____ , _____ , and _____ . _____ and _____ carry the most cholesterol.

Cholesterol is needed to maintain _____ _____ integrity and synthesize _____ _____ , _____ , and _____ _____ .

Answer 64

Lipoprotein functions

Lipoproteins are composed of varying proportions of cholesterol, TGs, and phospholipids. LDL and HDL carry the most cholesterol.

Cholesterol is needed to maintain cell membrane integrity and synthesize bile acids, steroids, and vitamin D.

Question 65

Chylomicron fxn

Answer 65

Delivers dietary TGs to peripheral tissues. Delivers cholesterol to liver in the form of chylomicron remnants, which are mostly depleted of their TGs. Secreted by intestinal epithelial cells.

Question 66

VLDL fxn

Answer 66

Delivers hepatic TGs to peripheral tissue. Secreted by liver.

Question 67

IDL fxn

Answer 67

Delivers TGs and cholesterol to liver. Formed from degradation of VLDL.

Question 68

LDL fxn

Answer 68

Delivers hepatic cholesterol to peripheral tissues. Formed by hepatic lipase modification of IDL in the liver and peripheral tissue. Taken up by target cells via receptor-mediated endocytosis. LDL is Lethal.

Question 69

HDL fxn

Answer 69

Mediates reverse cholesterol transport from periphery to liver. Acts as a repository for apolipoproteins C and E (which are needed for chylomicron and VLDL metabolism). Secreted
from both liver and intestine. Alcohol ^ synthesis. HDL is Healthy.

what the fuck it’s real

https://www.ncbi.nlm.nih.gov/pubmed/11067787

cheers!

Question 70

Abetalipoproteinemia

Inheritance, gene mutation, and what is absent + deficient

Answer 70

Autosomal recessive.

Mutation in (MTTP) gene that encodes microsomal transfer protein (MTP).
Chylomicrons, VLDL, LDL absent.

Deficiency in ApoB-48, ApoB-100.

Question 71

Abetalipoproteinemia Sx

Answer 71

Affected infants present
with severe fat malabsorption, steatorrhea, failure to thrive. Later manifestations include retinitis
pigmentosa, spinocerebellar degeneration due to vitamin E deficiency, progressive ataxia,
acanthocytosis. Intestinal biopsy shows lipid-laden enterocytes.

Question 72

Abetalipoproteinemia Tx

Answer 72

Treatment: restriction of long-chain fatty acids, large doses of oral vitamin E.

Question 73

AR familial dyslipidemias

Answer 73

Type I - Hyperchylomicronemia

Type III - Dysbetalipoproteinemia

Question 74

AD familial dyslipidemias

Answer 74

Type II - Familial Hypercholesterolemia

Type IV - Hypertriglyceridemia

Question 75

Familial dyslipidemias Type I—Hyperchylomicronemia pathogenesis

Answer 75

Lipoprotein lipase or
apolipoprotein C-II
deficiency

Question 76

Familial dyslipidemias Type I—Hyperchylomicronemia ^ blood level

Answer 76

Chylomicrons, TG,
cholesterol

Question 77

Familial dyslipidemias Type I—Hyperchylomicronemia clinical presentation

Answer 77

Pancreatitis,
hepatosplenomegaly, and
eruptive/pruritic xanthomas
(no inc risk for atherosclerosis).
Creamy layer in supernatant.

Question 78

Familial dyslipidemias Type II—Familial hypercholesterolemia

pathogenesis

Answer 78

Absent or defective
LDL receptors, or
defective ApoB-100

Question 79

Familial dyslipidemias Type II—Familial hypercholesterolemia

^ blood level

Answer 79

IIa: LDL, cholesterol
IIb: LDL, cholesterol,
VLDL

Question 80

Familial dyslipidemias Type II—Familial hypercholesterolemia

clinical presentation

Answer 80

Heterozygotes (1:500) have
cholesterol ≈ 300mg/dL;
homozygotes (very rare) have
cholesterol ≈ 700+ mg/dL.
Accelerated atherosclerosis (may
have MI before age 20), tendon
(Achilles) xanthomas, and
corneal arcus.

Question 81

Familial dyslipidemias Type III—Dysbetalipoproteinemia

pathogenesis

Answer 81

Defective ApoE

Question 82

Familial dyslipidemias Type III—Dysbetalipoproteinemia

^ blood level

Answer 82

Chylomicrons, VLDL

Question 83

Familial dyslipidemias Type III—Dysbetalipoproteinemia

clinical presentation

Answer 83

Premature atherosclerosis,
tuberoeruptive and palmar
xanthomas.

Question 84

Familial dyslipidemias Type IV—Hypertriglyceridemia

pathogenesis

Answer 84

Hepatic overproduction of VLDL

Question 85

Familial dyslipidemias Type IV—Hypertriglyceridemia

^ blood level

Answer 85

VLDL, TG

Question 86

Familial dyslipidemias Type IV—Hypertriglyceridemia

Clinical presentation

Answer 86

Hypertriglyceridemia (> 1000 mg/dL) can cause acute
pancreatitis. Related to insulin resistance.