Biochemistry TCA Cycle PDF

Summary

This document provides an overview of the Tricarboxylic Acid Cycle (TCA cycle), also known as the Krebs cycle or citric acid cycle. The document details the reactions involved in the cycle, including components, coenzymes, and regulation. It also touches upon related concepts such as pyruvate dehydrogenase deficiency and mechanisms of arsenic poisoning.

Full Transcript

1A
BIOCHEMISTRY
TRICARBOXYLIC ACID CYCLE
DR. JANDOC
 Transported to mitochondria to enter TCA cycle
OUTLINE  Pyruvate dehydrogenase complex
I. Overview  Pyruvate  acetyl CoA
II. Reactions in the TCA cycle  Component enzymes
 Oxidative decarboxylation of pyruvate  Pyruvate dehydrogenase complex
 Component enzymes  E1 – Pyruvate Dehydrogenase or Decarboxylase
 Coenzymes  Thiamine pyrophosphate
 Regulation of the pyruvate dehydrogenase  E2 – Dihydrolipoyl Dehydrogenase
complex  Lipoic acid
 Pyruvate dehydrogenase deficiency  CoA
 Mechanism of Arsenic poisoning  E3 – Dihydrolipoyl dehydrogenase
 Synthesis of citrate  FAD
 Isomerization of citrate  NAD+
 Oxidation and decarboxylation of isocitrate  Regulatory enzymes
 Cleavage of succinyl CoA  Pyruvate dehydrogenase kinase
 Oxidation of the succinate  Pyruvate dehydrogenase phosphatase
 Hydration of the fumarate  Deficiency of thiamine or niacin
 Oxidation of the malate  Wernicke-Korsakoff
III. Energy produced by the TCA cycle  Encephalopathy-psychosis syndrome
IV. Regulation of the TCA cycle  Thiamine deficiency
 Alcohol abuse
 CNS problems
I. OVERVIEW
 Brain cells unable to produce enough ATP, if the
 Tricarboxylic acid cycle PDH complex is inactive
 Kreb’s cycle or Citric acid cycle
 FINAL PATHWAY where metabolism of carbohydrate,
amino acids and fatty acids converge
 Carbon skeleton converted to CO2
 Production of the majority of ATP
 Cycle occurs in mitochondria, in close proximity to the
reactions of electron transport, which oxidize the reduced
coenzymes
 Aerobic pathway, O2 as final electron acceptor

 Regulation of the pyruvate dehydrogenase complex
 Regulatory enzymes
 Activate and inactivate E1
 Pyruvate dehydrogenase kinase
 Phosphorylates and inhibits E1  TCA cycle does
not proceed
 Activator (turn off PDH complex)
 ATP
 acetyl CoA
 NADH
 Inhibitor
 Pyruvate
 Pyruvate dehydrogenase phosphatase
 Dephosphorylates and activates E1  TCA cycle
proceeds
 Activator
 Calcium – released during contraction,
which the stimulate the PDH complex for
II. REACTIONS OF THE TCA CYCLE energy production
A. OXIDATIVE DECARBOXYLATION OF PYRUVATE
 PYRUVATE
 Endproduct of aerobic glycolysis
 Specific pyruvate transporter

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C. ISOMERIZATION OF CITRATE
 Citrate  isocitrate
 Via Acotinase
 Inhibited by Fluoroacetate (rat poison)
 Fluoroacetyl CoA + OAA  Fluorocitrate
 Pyruvate dehydrogenase deficiency  Citrate accumulation
 most common cause of Congenital Lactic Acidosis
 X-linked dominant
 unable to convert pyruvate to acetyl CoA
 shunted to lactic acid via LDH
 neurodegeneration, muscle spasticity, neonatal death
 Treatment: none
 Dietary restriction of carbohydrate
 Supplementation with TPP may reduce symptoms

 Mutation in PDH complex, electron transport chain or ATP
synthase
 Leigh syndrome
 Subacute necrotizing encephalomyelopathy
 Progressive neurological disorder
 Defect in mitochondrial ATP production

 Mechanism of Arsenic poisoning
 Forms stable complex with the thiol (-SH) group of lipoic
acid
D. OXIDATION AND DECARBOXYLATION OF ISOCITRATE
 Inhibit enzymes that require lipoic acid as a coenzyme
 Isocitrate dehydrogenase
 E2 of the PDH complex
 Irreversible oxidative decarboxylation of isocitrate
 Aα-ketoglutarate dehydrogenase
 Yield 3 NADH and CO2
 Aα-keto acid dehydrogenase
 Activator
 Accumulation of pyruvate  lactate
 ADP
 Affect brain
 Inhibitor
 Neurologic disturbance and death
 ATP
 NADH
B. SYNTHESIS OF CITRATE
 Rate limiting step in TCA cycle
 Acetyl CoA + Oxaloacetate  Citrate
 Catalysed by Citrate synthase
 Not an allosteric enzyme
 CITRATE
 Inhibit citrate synthase and phosphofructokinase
 Activates acetyl CoA carboxylase

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TCA CYCLE
 Cleaves the high-energy thioester bond
 Coupled to phosphorylation of GDP to GTP
 GTP and ATP are energetically interconvertible
 GTP + ADP GDP + ATP
 Succinyl CoA
 Can be produced from propionyl CoA derived from fatty
acids with odd number of C, and from several AA

E. OXIDATICE DECARBOXYLATION OF α-ketoglutarate
 α-ketoglutarate to succinyl CoA
 α-ketoglutarate dehydrogenase complex
nd
 Yield 2 CO2 and NADH
 Coenzymes required
 TPP
 Lipoic acid
 FAD
 NAD G. OXIDATION OF THE SUCCINATE
 CoA  Succinate dehydrogenase
 Inhibitor  Succinate  fumarate
 NADH  FAD  FADH2 (succinate is not sufficient to reduce NAD)
 Succinyl CoA  Only enzyme embedded in the inner mitochondrial
 Ca++ membrane
 α-ketoglutarate  Function as Complex II of the electron transport chain
 Also produced from oxidative deamination or
transamination of glutamate

H. HYDRATION OF THE FUMARATE
 Fumarase (Fumarate hydratase)
 Fumarate  L-Malate
 Fumarate
 Also produced by urea cycle, purine synthesis and
F. CLEAVAGE OF SUCCINYL CoA
catabolism of phenylalanine and tyrosine
 Succinate thiokinase (succinyl CoA synthetase – for reverse
reaction)

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 2 C atoms  acetyl CoA and leave as CO2
 No net consumption or production of oxaloacetate and its
intermediate
 4 pairs of electrons are transferred
 3 from NAD  NADH
 From FAD  FADH2
 Oxidation of NADH  3 ATP
 Oxidation of FADH2  2 ATP

I. OXIDATION OF MALATE
 Malate dehydrogenase
 Malate  Oxaloacetate
rd
 3 NADH
0
 ∆G is positive, but reaction is driven in the direction of
oxaloacetate by the highly exergonic citrate synthase
 Oxaloacetate
 Transamination of aspartic acid

IV. REGULATION OF THE TCA CYCLE

III. ENERGY PRODUCED BY THE TCA CYCLE

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