CARBOHYDRATE METABOLISM😊

General

Rate Limiting Enzyme

Glucose Pathways	Rate Limiting Enzyme
Glycolysis	Phosphofructokinase-1
TCA Cycle / Krebs cycle	Isocitrate dehydrogenase
Gluconeogenesis	Fructose-1,6-bisphosphatase
Glycogen Synthesis	Glycogen synthase
Glycogenolysis	Glycogen phosphorylase
HMP Shunt (PPP)	Glucose-6-phosphate dehydrogenase
Lipid Pathways	ㅤ
Fatty acid synthesis	Acetyl CoA carboxylase
Fatty acid oxidation	Carnitine acyl transferase 1
Cholesterol synthesis	HMG CoA Reductase ↳ Statins inhibit this enzyme
Ketone body synthesis	HMG CoA Synthase > HMG CoA Lyase
Bile acid synthesis	7α hydroxylase (Vit C)

ㅤ	Substrate Level Phosphorylation	Oxidative Phosphorylation
Energy generated	At substrate level	Indirectly
Enzymes	Kinases	Dehydrogenases
examples	• Phosphoglycerate kinase (glycolysis) • Pyruvate kinase (glycolysis) • Succinyl thiokinase (citric acid cycle) • Creatine kinase (muscle)	ㅤ
Notes	ㅤ	More common in humans (aerobic organisms)

One Liners Unit

Parent alcohol in carbohydrates – Glycerol

Parent carbohydrate which gives rise to other carbohydrates – D-Glyceraldehyde

Minimum number of carbons possible in a carbohydrate – 1

Minimum number of –OH groups possible in a carbohydrate – 2

Minimum number of functional groups possible in a carbohydrate – 3

Reduction methods of glucose estimation → Nelson Somogyi, Folin Wu, Ortho toluidine

Enzymatic methods of glucose estimation – Hexokinase & GOD/POD

Glycolysis

Only oxidation pathway without Oxygen.

Only pathway generating ATP without Oxygen.

Only oxidation in Cytoplasm.

Glycolysis	ㅤ
Aerobic process	7 ATPs / Glucose (+ 2 Pyruvate )
↳ Hexokinase	Glucose → Glucose 6 Phosphate • [- 1 ATP] • Irriversible
↳ Phosphofructokinase 1	Fructose 6 P → Fructose 1, 6 Bisphosphate • [- 1 ATP] • Irriversible
↳ Glyceraldehyde 3 P dehydrogenase	Glyceraldehyde 3 P → 1, 3 biphosphoglycerate • [+ 2 NADH = + 5 ATP]
↳ Phosphoglycerate kinase	1, 3 biphosphoglycerate → 3 phosphoglycerate • [+ 2 ATP] • Substrate level Phosphorylation
↳ Pyruvate kinase	Phosphoenolpyruvate → Pyruvate • [+ 2 ATP] • Substrate level Phosphorylation • Irriversible
Anaerobic process	2 ATPs / Glucose (+ 2 Lactate)
ㅤ	In Red Blood Cells • RBCs lack mitochondria • Cannot perform aerobic respiration
Link Reaction	Gain 5 ATP / Glucose
ㅤ	Oxidative decarboxylation • Pyruvate (3C) + NAD + CoA →Acetyl CoA (2C) + NADH + CO2
Total ATP at this stage:	7 ATPs + 5 ATPs = 12 ATPs.
TCA Cycle	• Always active (fed/fasting) • Amphibolic Pathway
1. Rate-limiting enzyme / Regulatory Enzymes:	• Irreversible
↳ Citrate synthase	ㅤ
↳ Isocitrate dehydrogenase	1st oxidative decarboxylation
↳ α-Ketoglutarate dehydrogenase	2nd oxidative decarboxylation
2. Substrate-level phosphorylation	• Gain 1 GTP (1 ATP) per Acetyl CoA
↳ Succinate thiokinase	Succinyl-CoA → Succinate
3. NADH Yielding	• Gain 3 NADH (7.5 ATP) per Acetyl CoA
↳ Isocitrate dehydrogenase	Isocitrate → α-Ketoglutarate
↳ α-Ketoglutarate dehydrogenase	α-Ketoglutarate → Succinyl-CoA
↳ Malate dehydrogenase	Malate → Oxaloacetate
4. FADH Yielding	• Gain 1 FADH (1.5 ATP) per Acetyl CoA
↳ Succinate dehydrogenase	Succinate → Fumarate
TCA Cycle Energetics	ㅤ
• Per Acetyl-CoA	10 ATP (Per Cycle x 2 = 20 ATP)
• Per Pyruvate ↳ (PDH + TCA) ↳ Add 2.5 ATP from Link reaction	12.5 ATP
• Per Glucose ↳ (Glycolysis + PDH + TCA)	32 ATP

Aerobic Glycolysis

ATP-Utilizing Steps:

ATP-Producing Steps:

Step-by-Step Pathway

ㅤ	Enzyme Inhibited	Application
Glycolysis	ㅤ	ㅤ
• Fluoride	Enolase	Used in blood glucose estimation; fluoride tubes (Grey tube)
• Arsenate	G3P Dehydrogenase	Competes with Pi, blocks ATP generation.
• Iodoacetate	G3P Dehydrogenase	Mimics inorganic phosphate, used experimentally.
TCA	ㅤ	ㅤ
• Arsenic	PDH, α-Ketoglutarate dehydrogenase	• ⛔lipoic acid (E2 of ABPT) • Lip () to Ass (arsentate)
• Malonate	Succinate dehydrogenase ↳ also Complex 2 of ETC	• Mala sucks
• Fluoroacetate • Fluorocitrate	Aconitase	• Cone ice cream thinnapo → flu vannu
• Cyanide, CO, H2S	Complex IV (ETC)	ㅤ

Cori Cycle and Cahill Cycle

Function

Provide Glucose to Muscle
Transport of ammonia to Liver

ㅤ	Cori Cycle	Cahill Cycle
Alias	• Glucose-Lactate Cycle	• Glucose-Alanine Cycle
Conditions	• Anaerobic Exercise	• Fasting/Starvation
In Muscle	• Pyruvate → Lactate (via LDH)	• Pyruvate → Alanine (via ALT)
In Liver	• Pyruvate → Glucose (via gluconeogenesis) • Glucose returns to muscle for energy • Transports 2 ATP to Muscle	• Pyruvate → Glucose (via gluconeogenesis) • Glucose returns to muscle for energy • Transports 2 ATP to Muscle
Mnemonic	• Koreee Laskham • Gym → Anerobic exercise → Cori → Lactate	• Early morning → Fasting → Alanine → Cahill

Muscle protein breakdown

Release Alanine → Substrate for gluconeogenesis

During prolonged fasting, the liver uses alanine.

Emaciation & ↓ in muscle mass.

Transport of NH₃

1st-line defence in hyperammonaemia

Cahill cycle
Alanine = Transport form from skeletal muscles

NOTE

Glutamate + NH3 → Glutamine

Glutamate = Transport form from other parts
Enzyme: Glutamine synthetase (in mitochondria)
Glutamate from

Amino acids

NH3 from

Amino sugars
Pyrimidine
Purine
Porphyrins

Hexokinase vs Glucokinase

Feature	Hexokinase	Glucokinase
Location	Most tissues (except liver, β cells)	Liver, Pancreatic β cells
Metabolism	All hexose sugars	Only glucose
Km (Affinity)	Low Km (High affinity)	High Km (Low affinity)
Vmax (Capacity)	Low Vmax	High Vmax
Induced by Insulin	No	Yes → In Fed State
Feedback Inhibition	By Glucose-6-phosphate	By Fructose-6-phosphate

Gluconeogenesis

Reversal of glycolysis.

Synthesis of glucose from non-carbohydrate precursors.

It is an anabolic pathway.

Requirements for gluconeogenesis:

Substrates: GLA

ㅤ	Substrates	Source
1	Glycerol	• Peripheral Lipolysis • DHAP
2	Lactate	• Cori cycle
3	Alanine (Prolonged starvation)	• Cahill cycle
4	Propionyl CoA → Succinyl-CoA	• Odd chain FA
5	Glucogenic amino acids	• All except Lys, Leu

NOTE: Acetyl CoA

NOT SUBSTRATE OF TCA

But Strongest activator of Gluconeogenesis

Odd chain FA:

Energy

Require 6 ATPs

for 2 lactate → 1 glucose.

Require 11 ATPs

For 2 pyruvate → 1 glucose

Irreversible Glycolysis Step	Reversing Gluconeogenesis Enzyme	Details
3. Pyruvate kinase	Pyruvate carboxylase and PEP carboxykinase (PEPCK)	STEPS: 1. Pyruvate carboxylase (Mitochondria): • Pyruvate → Oxaloacetate. 2. Oxaloacetate transport to Cytosol • via the Malate-Aspartate shuttle. 3. PEP carboxykinase (Cytosol): • Oxaloacetate → Phosphoenolpyruvate. • Requires GTP.
2. PFK-1	Fructose-1,6-bisphosphatase	• Location: Cytosol. • Fructose-1,6-bisphosphate → Fructose-6-phosphate.
1. Hexokinase	Glucose-6-phosphatase	• Location: ER. • Glucose-6-phosphate → Glucose.

Clinical Relevance:

Muscle cannot perform gluconeogenesis

lacks Glucose-6-phosphatase

Liver cannot use G6P released for gluconeogenesis

G6Pase is in ER

Energy Requirement:

To convert 2 Lactate → 1 Glucose:

Pyruvate carboxylase: 2 ATP
PEP carboxykinase: 2 GTP
1,3-BPG kinase: 2 ATP

Total: 6 ATP equivalents

To convert 2 Pyruvate → 1 Glucose:

Total: 6 + 5 (2 x NADH for link reaction reversal) = 11 ATP equivalents

Pyruvate Kinase (PK) deficiency

2nd most common human enzyme deficiency (after G6PD).

Present similar to G6PD (hemolysis)

Heinz bodies → only in G6PD deficiency.

Regulation of Glycolysis and Gluconeogenesis

Tandem/Bifunctional Enzyme

Involved in Glucose Regulation during Starvation

Enzyme pair	Active in	Function
Phosphofructokinase-2 (PFK-2)	Dephosphorylated state	Makes F-2,6-BP
Fructose bisphosphatase-2 (FBPase-2)	Phosphorylated state	Breaks it

Both are regulated by protein kinase A (phosphorylation) — **Both are regulated** by **protein kinase A (phosphorylation)**

Both pathways are reversible.

Allosteric regulators

When one pathway is active, other is inactive.
Prevents a futile cycle (vas cycle)

In starvation

↓ Blood glucose → Glucagon release.
Glucagon → Gs receptor → ↑ cAMP.
cAMP → activates Protein Kinase A (PKA).
PKA phosphorylates tandem enzyme → activates F-2,6-bisphosphatase.
F-2,6-BP is cleaved → PFK-1 not stimulated

Note: F-2,6-BP stimulate PFK-1

Glycolysis stops
Gluconeogenesis starts → Plasma glucose increases

Q. Identify A

(Image showing regulation of glycolysis and gluconeogenesis, 'A' points to Fructose 2,6 bisphosphate).

A. Fructose 1,6 bisphosphate.
B. Fructose 2,6 bisphosphate.
C. PFK-1.
D. PFK-2.

Explanation:

Upper half: glycolysis.

Rate-limiting enzyme: Phosphofructokinase-1 (PFK-1).

Lower half: gluconeogenesis.

Rate-limiting enzyme: Fructose 1,6 bisphosphatase.

A is a common regulator of both enzymes.

A stimulates glycolysis and inhibits gluconeogenesis.

A is Fructose 2,6 bisphosphate.

Fates of Pyruvate

4 main fates:

State	Enters	Enzyme	Conversion to	Yields
Aerobic In Low Energy	Citric acid cycle	PDH complex	Acetyl CoA	2 ATP
Anaerobic In Low Energy	Anaerobic glycolysis	LDH	Lactate (Cori)	5 ATPs
Starvation	Gluconeogenesis	Pyruvate carboxylase	Oxaloacetate	Glucose
Well fed	Protein synthesis	ALT	Alanine (Cahill)	Proteins

Biotin (B7) Coenzyme for	Reaction	Name
Pyruvate carboxylase	Pyruvate → Oxaloacetate	• Gluconeogenesis
Acetyl CoA carboxylase	Acetyl CoA → Malonyl CoA	• Fatty acid synthesis
Propionyl CoA carboxylase	Propionyl CoA → Methyl Malonyl CoA	• Fatty acid oxidation • Branched-chain AA breakdown

Mnemonic for biotin:

ABC PAPify
ABC - ATP, BIOTIN, CO2 FOR CARBOXYLATION
When depressed (depression) due to alopecia (), dermatitis () and rash → exercise cause fatigue and eat egg (avidin in egg white inhibits B7)
Bought a cat → Tom cat → Peed everywhere → Tom cat urine odour () in multiple carboxylase enzyme deficiency ()

Steps in Starvation and High Energy

Fate of Glucose 6 Phosphate (G6P)

Fate of Glucose 6 Phosphate	ㅤ
Glycogen Synthesis	In Liver • Glucose-6-phosphate ⇔ Glucose ↳ by Glucose-6-phosphatase • Source of Glucose for Brain and RBC during fasting • Energetics ◦ From free glucose: ↳ 2 ATP ◦ From via 1 G6P : ↳ 3 ATP In muscle • G6P → Pyruvate → Lactate + 3 ATP • Selfish • ATP production for muscle only • No release of glucose into blood ↳ As muscle lacks glucose-6-phosphatase
HMP Shunt (Pentose phosphate pathway)	• NADPH • Ribose 5 Phosphate

Fate of Acetyl CoA → Anabolism

NOT SUBSTRATE OF TCA

But Strongest activator of Gluconeogenesis

Fate of Acetyl CoA	Enzyme	Note
↳ Fatty acid synthesis	Acetyl CoA Carboxylase	• Stored as Triacylglycerol
↳ Cholesterol synthesis	HMG-CoA reductase	• In fed state • Stored as Cholesterol ester • RLE in cholesterol synthesis • ⛔ by statins
↳ KB Synthesis	HMG-CoA lyase	• In Starvation

NOTE:

HMG-CoA synthase

Common in both cholesterol and KB synthesis
RLE in ketone body synthesis

Explains why a Carbohydrate diet is Lipogenic.

High energy → ⛔ Glycolysis.

Difference between NADH and NADPH

Note: Only NADH/FADH2 give ATP, never NADPH.

ㅤ	NADH	NADPH
Property	Enters ETC. Acts as a source of ATP.	• Cannot enter ETC • Rossman fold: NADP binding domain Used for: • Fat / steroid synthesis. • Regenerating Glutathione → Glutathione reductase • CYT P450 enzymes • Ribonucleotide reductase. • Heme Oxygenase
Sources	• Glycolysis • PDH complex • Citric acid cycle • Fatty acid oxidation • Amino acid oxidation	• HMP shunt pathway (major) • Cytoplasmic isocitrate dehydrogenase • Malic enzyme (Malate → Pyruvate)

HMP Pathway sites

Oxidative stress sites

RBC / Lens

Steroid / FA synthesis sites

Liver
Adipose
Adrenal cortex
Gonads

Never the sites for HMP:

Non lactating mammary glands, Skin.

NADPH Uses

Regeneration of Glutathione:

Glutathione (GSH)

γ-glutamyl-cysteinyl-glycine (GSH)

Tripeptide composed of:

Glutamic acid + Cysteine + Glycine

GSH + H2O2 → water + GS-SG (oxidised)

via Glutathione peroxidase (dep on Selenocysteine)

GS-SG (oxidised) → GSH (reduced)

Regenerating Enzyme: Glutathione reductase (dep on Vit B2)
Hydrogen source: NADPH.

Peroxide Protects and Reductase replenishes/regenerates

Functions

Important antioxidant for RBCs.
Free radical scavenger (Antioxidant role)

Glutathione peroxidase

Transport of ammonia

via Meister’s cycle / Gamma-glutamyl cycle

Conjugation of unconjugated bilirubin (detoxification reactions)??
Coenzyme role

G6PD deficiency

Most are asymptomatic.

↓ G6PD enzyme + Exposure to oxidants or infection

NADPH not regenerated → ⛔ Glutathione reductase
↓ Glutathione → H2O2 is not detoxified.
H2O2 causes oxidative damage to RBC membrane → Hemolytic anemia
Hemolysis type

Extravascular >> intravascular

Intermittent, symptoms with precipitating factors.
So no HSM

Use of Ribose-5-Phosphate:

Used for Purine and Pyrimidine nucleotide synthesis.

Examples:

Adenosine + RSP → Adenosine monophosphate.
Guanine + RSP → GMP.
Cytosine + RSP → CMP.

Transamination

Amino Acid	Converted To	Enzyme
Amino acids	Keto acids	• Transaminase • Require Pyridoxal phosphate (active form of Vitamin B6)
Alanine	Pyruvate	ALT / SGPT ↳ ALT → PT → Pyruvate
Aspartate	OAA	AST / SGOT ↳ AST → OT → OAA

Site: Cytoplasm of all organs

Reversible reaction

Ping-pong mechanism (Bi-bi):

2 substrate
2 product reaction

Exceptions to Transamination

Proline

Hydroxyproline

Lysine

Threonine

Pro (Proline, hydroxyproline) doesn’t lyse (Lysine) through transamination (threonine)

Which one of these amino acids does not enter the Krebs cycle by forming Acetyl CoA via pyruvate?

Glycine

Tyrosine

Hydroxyproline

Alanine

ANS

Tyrosine:

Tyrosine → fumarate + acetoacetate.
Tyre acid ozhikkumbho fumes avum
These products enter the Krebs cycle

not through pyruvate or Acetyl CoA.
Does not use the pyruvate pathway.

Applied Biochemistry

Gyrate atrophy (retina & choroid)

Defect in: δ-ornithine aminotransferase

Enzyme which undergo Non α amino acid Transamination

Treatment:

Restrict ornithine & arginine
Supplement PLP (B₆)

Tricarboxylic Acid (TCA) Cycle / Krebs Cycle

Regulation

Always active

Anaplerotic Reactions

Definition: Reactions that replenish TCA cycle intermediates.

Key Reactions:

Substrates	Source	Other Uses of substrates
Oxaloacetate	Pyruvate	ㅤ
Succinyl-CoA	Propionyl-CoA	Heme Synthesis
α-Ketoglutarate (B6)	Glutamate	GABA
Oxaloacetate	Aspartate	ㅤ
Citrate	Fatty acid synthesis	ㅤ

Acteyl CoA is not a substrate of Krebs cycle

So not an anaplerotic reaction

Where is NADH released? → I (ID) Know (AKG) Mam (Malate D)

Where is CO2 released? → I Know (ID, AKG)

ㅤ	Enzyme Inhibited	Application
Glycolysis	ㅤ	ㅤ
• Fluoride	Enolase	Used in blood glucose estimation; fluoride tubes (Grey tube)
• Arsenate	G3P Dehydrogenase	Competes with Pi, blocks ATP generation.
• Iodoacetate	G3P Dehydrogenase	Mimics inorganic phosphate, used experimentally.
TCA	ㅤ	ㅤ
• Arsenic	PDH, α-Ketoglutarate dehydrogenase	• ⛔lipoic acid (E2 of ABPT) • Lip () to Ass (arsentate)
• Malonate	Succinate dehydrogenase ↳ also Complex 2 of ETC	• Mala sucks
• Fluoroacetate • Fluorocitrate	Aconitase	• Cone ice cream thinnapo → flu vannu
• Cyanide, CO, H2S	Complex IV (ETC)	ㅤ

Location:

Mitochondrial matrix

Exception:

Succinate dehydrogenase – located on inner mitochondrial membrane

Functions:

Final oxidative pathway for:

Lipids
Carbohydrates
Proteins

Produces:

NADH
FADH₂
GTP (→ ATP via oxidative phosphorylation)

Provides biosynthetic intermediates

Amphibolic: both catabolic and anabolic roles

Significance

Irreversible step

Acetyl-CoA is never gluconeogenic.

Explains why fat cannot be converted to glucose

Therefore, all even-chain fatty acids are never glucogenic.

They catabolize to n/2 acetyl-CoA.

Exceptions:

glycerol, odd-chain fatty acids → Propionyl-CoA → Succinyl-CoA

Oxidative decarboxylation

Multienzyme complexes

Enzyme complex

Present in the mitochondria.

3 subunits (E1, E2, E3)

5 coenzymes

3 Subunit	Name	5 Coenzyme
E1	• Specific for each ABPT enzyme ↳ A: Alpha-ketoglutarate dehydrogenase ↳ B: Branched-chain ketoacid dehydrogenase ↳ P: Pyruvate dehydrogenase ↳ T: Transketolase	• Thiamine pyrophosphate (TPP) (B1)
E2	• Dihydrolipoyl transacetylase • Common/shared cofactors 2 tea with lipid for CoA	• Lipoamide / Lipoic acid • CoA (CoA → B5)
E3	• Dihydrolipoyl dehydrogenase • Common/shared cofactors 3D FAhaD dehydrated	• FAD (Riboflavin → B2) • NAD (Niacin → B3)

Biotin is necessary for carboxylases, not the PDH complex.
E2 & E3 ⇒ Lipoic acid, FAD (B₂), NAD⁺ (B₃), CoA (B₅)

Arsenate poisoning affect Lipoic acid

Affect both PDH and Alpha-ketoglutarate dehydrogenase

The PDH complex is inhibited by arsenite.

Lip () to Ass (arsenate)

Preferred Fuel

Anaerobic Cells

Must use only glucose.

Lactate → Substrate for gluconeogenesis

These cells include:

RBCs, Retinal cells, Corneal cells (lack mitochondria).
White muscle fibres (store glycogen, no myoglobin).
Renal medulla.

Anaerobic glycolysis generates 2 ATPs.

Aerobic Cells

Can use fatty acids > glucose

Reason:

Glucose → 32 ATPs;
fatty acid (Palmitic acid) → 106 ATPs.

Examples using fatty acids:

Cardiac muscle fibres.
Red muscle fibres.
They store fatty acids as triacylglycerol and Cholesterol ester.

Exception:

Neurons

Use glucose as preferred fuel.
Reason: Fatty acids attached to albumin cannot cross blood-brain barrier (BBB).

Fuel Use Comparison:

RBCs use glucose anaerobically:

1 glucose → 2 Lactate + 2 ATPs.

Neurons use glucose aerobically:

1 glucose → CO2 + 32 ATPs.

Hepatocytes

Preferred fuel: Amino acid.
Enzyme: Glucokinase, with lower affinity for glucose.

Encounters dietary glucose first (via portal vein).
Low enzyme affinity allows glucose to pass to peripheral tissues,

preventing hypoglycemia.

Cannot use dietary fatty acids directly.

They are absorbed as Chylomicrons via lymphatics,
entering systemic circulation first.

Important Information:

Heart prefers FA in adults

due to continuous energy demands.

Fetal heart and failing heart

Rely on glucose (via GLUT-4).

Fasting and Starvation Stages

Starvation = Fuel deficiency

A deficiency of glucose, fatty acids, and amino acids.
Aim during starvation

Maintain body glucose levels.
Bcz neurons and RBCs mainly depend on glucose.

Energy deficiency = ATP deficiency

Major sources of plasma glucose during starvation:

Dietary glucose

2 to 2 and half hours

Liver glycogenolysis

Major source of Glucose for 1st 16 hrs of starvation

Gluconeogenesis

Occurs from 6 hours up to 2-3 weeks of starvation.

Stage	Duration After Food Intake	Primary Energy Source
Early Fasting	4–16 hours	Hepatic glycogenolysis
Fasting	16–48 hours	Gluconeogenesis
Prolonged Fasting/ Starvation	48 hours – 5 days	Ketone body synthesis
Prolonged Starvation	>5 days	Muscle proteolysis

Tissue/State	Well-fed State (2 hr)	Fasting (12 - 18 hr)	Starvation (1 - 3 days)
RBCs	Glucose	Glucose	Glucose
White muscle fibers	Glucose	Glucose	Glucose
Neurons	Glucose	Glucose	Ketone bodies
Cardiac muscle	Fatty acids	Fatty acids	Ketone bodies
Red muscle fibers	Fatty acids	Fatty acids	Ketone bodies
Liver	Glucose	FA	FA (Gluconeogenesis → AA, Glycerol)
Adipose	Glucose	FA	FA
Main Fuel	Carbs	Fat	Ketone bodies

Ketone bodies utilized by BHeeM

B (Brain) H (Heart) M (Red Muscle)

Fed → Insulin → Dephosphorylation

Mnemonic: Insulin Hate HSL

so prick with PIN (PGE, Niacin, Insulin)

ㅤ	Fed state	Fasting state
Hormone	• Insulin (anabolic hormone)	• Glucagon • Hypoglycemia in CAMPil • give Glucagon injection
↳ MOA	• Activates phosphodiesterase • ↓ cAMP	• Activates adenyl cyclase → ATP • ↑ cAMP → activates protein kinase A ↳ Glycogen phosphorylase (activated) ↳ Glycogen synthase (inhibited)
ㅤ	ㅤ	Other Counter-regulatory hormones • Epinephrine/norepinephrine • Growth hormone • Glucocorticoids • Thyroid hormones
State	Dephosphorylated	Phosphorylated
Lipase activated	Lipoprotein Lipase (LPL)	Hormone Sensitive Lipase (HSL) Inhibited by • Insulin • PGE1 • Niacin • Insulin hate HSL • so prick with PIN (PGE, Niacin, Insulin)
↳ Function	• Chylomicron TGA → FA + Glycerol • to enter Adipose cells in fed state	• Adipose TGA → FA + Glycerol • for transport to liver in fasting state
ㅤ	Enzymes & Pathways activated	Enzymes & Pathways activated
Pathways activated	• Glycolysis + • Link Reaction + All anabolic pathways • Glycogen synthesis • Cholesterol synthesis • FA synthesis • Protein synthesis	• Gluconeogenesis + All Catabolic pathways • Glycogenolysis • KB synthesis / breakdown • FA (β) oxidation • Peripheral lipolysis • Amino acid oxidation
Enzymes activated	All anabolic + • Glycogen synthase • Acetyl CoA carboxylase • HMG CoA reductase Glycolysis enzymes • Phosphofructokinase • Pyruvate DH Exception ATP Citrate Lyase ↳ FA synthesis ↳ Citrate → Acetyl CoA ↳ activated by insulin ↳ Active in phosphorylated state	All catabolic + Gluconeogenesis enzymes • Fructose 1 , 6 bisphosphate • Glycogen phosphorylase NOTE: • Gluconeogenesis is anabolic • Glycolysis is catabolic
Compartmentalisation	Cytoplasm	Mitochondria
ㅤ	All above pathways + • Glycogenolysis • HMP shunt	All above except Glycogenolysis + • TCA • ETC • PDH
Others	Cholesterol synthesis (Steroids) ↳ Cytoplasm + SER Bile acid synthesis (Steroids) ↳ Smooth Endoplasmic Reticulum	Oxidised in Peroxisomes ↳ Very long chain fatty acid + ↳ Branched chain Fatty acids
Both	ㅤ	ㅤ
ㅤ	• Start in mitochondria • Finish in cytoplasm	PUBG • Pyrimidine Synthesis • Urea cycle • Haem synthesis (blood) • Gluconeogenesis ↳ Oxaloacetate reaches Cyp for gluconeogenesis

Phosphocreatine

During resting → ATP + Creatine → Phosphocreatine

Provide high energy phosphate to muscle

rapidly available

Replenish ATP

Metabolic Fuel for RBCs During Starvation

Q. What is the metabolic fuel for RBCs during starvation?

A. Aminoacids

B. Ketone bodies

C. Glucose

D. Fatty acids

Answer:

C. Glucose

Peripheral lipolysis

Adipose TGA → FA + Glycerol

By Hormone-sensitive lipase

Catabolic enzyme
Insulin → Anabolic

⛔ hormone-sensitive lipase.
Insulin ↓ in starvation

All counter-regulatory hormones → Catabolic.

They ↑ in starvation
They stimulate hormone-sensitive lipase.
Examples:

Glucagon,

Growth hormone,

Norepinephrine,

Cortisol.

Products → Both enter Liver

Glycerol

Substrate for gluconeogenesis

Undergoes β-oxidation → releases Acetyl-CoA.
Acetyl-CoA :

ㅤ	Sequence of Utilization	Notes
1	Used in TCA cycle	• Energy for ketone body synthesis
2	Enters KB synthesis	• Liver don’t use KB ↳ d/t absent thiophorase
3	Activates Gluconeogenesis	• Liver don’t use Glucose ↳ Glucokinase has low affinity • Glucose-6-phosphate is present in SER ↳ Hence Glucose not released immediately

This results in loss of weight.

💡

Cortisol (Glucocorticoids):

Enhances every step, increases enzyme synthesis,
increases precursor supply from protein breakdown

Applied Biochemistry:

Defect in liver β-oxidation

Non ketotic hypoglycemia
due to no KB formation or gluconeogenesis.

Insulin Resistance:

↑ TAG hydrolysis → ↑ Free fatty acids in blood → Fatty liver disease

Niacin:

Inhibit HSL
Locks TAG in adipose tissue → Used for hypertriglyceridemia treatment

Diabetes as a Fasting/Starvation-like State

Absence of insulin.

↑ TAG hydrolysis → ↑ Free fatty acids in blood → Fatty liver disease

Effects:

GLUT-4 is inactive
Blood glucose remains high
Cells behave as if in a fasting state

Catabolic state:

All catabolic pathways are activated.

Only Exception Anabolic process in Chronic Diabetes :

Fat synthesis in liver.

Results:

↑ VLDL synthesis
↑ Cholesterol synthesis

Electron Transport Chain (ETC)

2 Mobile Complexes:

Ubiquinone (Q): Between Complex I and Complex III.
Cytochrome C: Between Complex III and Complex IV.

Direction of Electron Transport:

NADH electron: Enters through Complex I.
FADH2 electron: Enters through Complex II.

ㅤ	ㅤ	Push electrons to	Protons Pumped
1	NADH-linked dehydrogenase/ NADH Q Oxidoreductase	Ubiquinone (Q)	4 H +
2	Succinate dehydrogenase / Succinate Q reductase	Ubiquinone (Q)	ㅤ
ㅤ	FADH2-linked dehydrogenases ↳ Acyl CoA dehydrogenase. ↳ Mitochondrial glycerol-3-phosphate dehydrogenase.	Ubiquinone (Q) FAD → FAT → Acyl CoA and Glycerol	ㅤ
3	Cytochrome b and c1 / Cytochrome C reductase	Cytochrome C	4 H +
4	Cytochrome a and a3 / Cytochrome C oxidase	O2 (Final electron acceptor)	2 H +
5	ATP synthase complex	ㅤ	ㅤ
ㅤ	↳ F0 gate	• Rolling gate	ㅤ
ㅤ	↳ F1 gate	• Protruding towards mitochondrial matrix • Has ATP synthase activity • Convert ADP to ATP	ㅤ

Energetics

1 NADH = 10 Protons pumped = 2.5 ATP

1 FADH = 6 Protons pumped = 1.5 ATP

NOTE

Mechanical energy → Chemical Energy

When they cross Fo (rolling gate) → mechanical energy → transferred to F1 subunit → converts ADP to ATP

4 “C”s of Complex 4

Remember Oxygen next to C4 → Oxidase, Heme, Copper (instead of iron)
Cytochrome oxidase
Copper/heme protein
Carbon monoxide inhibits it
Cyanide inhibits it

Inhibitors of ETC

Point of Inhibition	Inhibitor(s)	Mnemonic
Complex I → Ubiquinone (Q)	• Amobarbital • Phenobarbital • Piericidin A • Rotenone • Metformin	“A Rotten guy” - Barbieye Piercecheyth
Complex II	• Malonate	Mala sucks
Complex II → Ubiquinone (Q)	• TTFA, Carboxin	Mala scuk cheythapo Car (CArboxin) thatti (TTFA)
Complex III → Cytochrome C	• BAL, Antimycin	Balamayi Antiye pidich
Complex IV → Oxygen	• Hydrogen sulfide • Cyanide • Azide • Carbon monoxide	CCo HS ne Ide
Fo component of Complex 5	• Venturicidin • Oligomycin	Veettil () Ottakk () Attract () cheyth
ADP/ATP transporter	• Atractyloside	ㅤ

Metal cofactor Enzymes

Metal cofactor	Reaction
Potassium	• Na⁺-K⁺ ATPase, • Pyruvate kinase
Magnesium	• All kinase/ phosphorylase/ carboxylase/ Phosphatase/ Mutase/ Enolase ↳ Except pyruvate kinase • Glycogen phosphorylase - calcium
Manganese	• Kinase • Phosphatase • Mitochondrial SOD • man with SODa
Copper	• Tyrosinase (Melanin production), • Complex 4 (Cytochrome C oxidase), • Lysyl oxidase (Covalent cross linking of Collagen) • Ceruloplasmin • Cytosolic SOD
Zinc	Anhydrase/Dehydratase/Dehydrogenase • Carbonic anhydrase • Carboxypeptidase A & B • LDH → Lactate dehydrogenase • Glutamate dehydrogenase • Alcohol dehydrogenase • ALA dehydratase • Cytosolic SOD
Selinium	• Glutathione Peroxidase • Deiodinase • Thiioredoxin reducatase
Iron	Heme iron: ↳ Complex III & IV (Cytochrome) ↳ Near Oxygen half → heme iron Non-heme: ↳ Complex I & II (Fe-S cluster)
Molybdenum	• Xanthine oxidase • Sulfite oxidase • Moly and Shantha with Sulfikar

Uncouplers

Function:

They uncouple fuel oxidation

Oxidation ✔
Phosphorylation ✗ → ATP is not produced.

Effects:

ATP is not produced

High heat production

Increased rate of oxidation

They are the only ETC inhibitors that do not affect oxidation.

Physiological Uncouplers:

Vaishna → Brown girl (Brown fat) → From gramam (Gramicidin) → has a Long (Long chain FA) Vaalu (Valinomycin) → always hot (thermogenin) → thyroid ↑↑ (Thyroxine)

Thermogenin (Uncoupling protein 1)

Long chain fatty acid

Ionophores (Valinomycin, gramicidin)

Bilirubin

Thyroxine

Upregulation of uncoupler proteins in mitochondrial membrane
Allows hydrogen ions to bypass ATP production.
Leads to heat generation, heat intolerance in thyrotoxicosis, and increased BMR.

Brown Adipose Tissue (BAT)

Brown due to abundant mitochondria with uncoupler proteins.
Bypasses ATP production, leading to heat generation (non-shivering thermogenesis).

Aids neonates and hibernating animals.

Most important mechanism for protection against hypothermia in neonates:

Non shivering thermogenesis

Due to the presence of brown fat

Around scapula, axilla
lipid deposits rich in mitochondria
Release of norepinephrine and uncoupling of beta oxidation of fat → heat production