Fatty Acid Oxidation Defects - PowerPoint PPT Presentation

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Fatty Acid Oxidation Defects

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Fatty Acid Oxidation Defects The disorders of oxidation of fatty acids by mitochondria has been major focus of research for the past 10-20 years. – PowerPoint PPT presentation

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Title: Fatty Acid Oxidation Defects


1
Fatty Acid Oxidation Defects
  • The disorders of oxidation of fatty acids by
    mitochondria has been major focus of research
    for the past 10-20 years. Based on these studies
    clinicians are now beginning to understand
    symptoms of Reyes-like syndrome, cardiomyopathy,
    hypotonia, hypoglycemia, developmental delay, and
    in some cases sudden infant death syndrome
    (SIDS). These are all related to defects in FAO.
  • 2. Panel of assays in neonates now include
    quantization of FAO enzymes specifically MCAD.

2
Fatty Acids are preferentially oxidized
  1. During periods of extended exercise e.g.
    aerobics, running on a treadmill, running for
    long distances.
  2. In diabetic patients in whom glucose metabolism
    is low.
  3. During periods of starvation.
  4. By heart muscle which almost exclusively depends
    on FA oxidation for energy.

3
Sequential Steps in the oxidation of Fatty Acids
  • Mobilization of Fat from adipose tissue
  • Transport of fatty acids in plasma and their
    activation in the cells
  • Transport of activated fatty acids to
    mitochondria and oxidation
  • Formation of ketone bodies (excess oxidation in
    starvation and diabetes)
  • Regulation of fatty acid oxidation

4
Mobilization of Triacylglycerols That are Stored
in Adipocyte Cells
Free fatty acids and glycerol are released into
the blood stream
Lipolysis inducing hormones Epinephrine,
glucagon, adrenocorticotropic hormones -gt
Insulin inhibits lipolysis Free fatty acids are
bound by serum albumin -gt serves as carrier in
blood
5
FA Bound to FABP
FA in Plasma
6
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7
FAO Cycle
8
Steps in the oxidation of Palmitoleic Acid
(C161)
  • CH3-CH2-CH2-CH2-CH2-CH2-CHCH-CH2-CH2-CH2-CH2-CH2-
    CO-SCOA CH3-CO-CoA FADH2 NADH
  • CH3-CH2-CH2-CH2-CH2-CH2-CHCH-CH2-CH2-CH2-CO-SCoA
    CH3-CO-CoA FADH2 NADH
  • CH3-CH2-CH2-CH2-CH2-CH2-CHCH-CH2-CO-SCoA
  • CH3-CO-CoA FADH2 NADH
  • CH3-CH2-CH2-CH2-CH2-CHCH-CO-SCoA CH3-CO-CoA
    FADH2 NADH
  • 5) CH3-CH2-CH2-CH2-CH2-CO-SCoAA CH3-CO-CoA
    NADH
  • 6) CH3-CH2-CH2-COA CH3-CO-CoA FADH2 NADH
  • 7) CH3-CO-CoA CH3-CO-CoA FADH2 NADH After
    the 7th round you are left with an 8th acetyl CoA
    (CH3-CO-CoA) 6FADH2 7NADH

9
Oxidation of Odd Chain FA
10
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11
Omega Oxidation of Fatty Acids
12
Fattyacyl CoA
13
Regulation of FAO
  • 1. Enzyme CPTI (carnitine-palmitoyl transferase
    I) is the rate limiting enzyme. It is inhibited
    by Malonyl CoA, a product formed during fatty
    acid synthesis
  • Hormonal Regulation of FA oxidation
  • Glucagon
  • Epinephrine
  • Insulin

Triacyl glycerol or Hormone sensitive lipase
14
  • Spectrum of FAO deficiencies
  • Carnitine deficiency
  • Fattyacyl CoA synthetase deficiency
  • Short chain (SCAD), medium chain (MCAD), long
    chain (LCAD) and multi-chain (MCAD) dehydrogenase
    mutations
  • Acyl Carnitine-Carnitine translocase mutations

15
Examples of Clinical Findings
The clinical entity known as MCAD deficiency was
biochemically defined about 20 years ago
however, some believe the condition to be at
least as common in newborns as phenylketonuria,
with an incidence approximating 1 per every
12,000 live births. A recent report from Europe
indicates an incidence in Bavaria of 18456 in
more than 500,000 newborns screened
Another report from England Of 62 affected
individuals identified, 57 were from England,
giving an incidence of 4.5 cases/100?000 births.
Forty six cases presented with an acute illness
(10 of whom died), 13 cases were identified
because of family history, and three for other
reasons. Six of the survivors were neurologically
impaired. Undiagnosed, MCAD deficiency results
in considerable mortality and morbidity. However,
current management improves outcome.
16
A Child has MCAD deficiency
  • Will this child be
  • Hypoglycemic
  • Hyperglycemic
  • Normal glucose
  • Will this child be
  • Severely ketotic
  • Mildly ketotic
  • Not ketotic
  • Will this child have
  • Acidosis
  • Alkalosis
  • Normal pH.

17
Learning Objectives
  • This lecture links defects in catabolism of
    lipids to a variety of pathological states.
    Following this lecture students should understand
    that
  • oxidation of lipids is an important energy source
  • oxidation requires mobilization of fat from
    adipose cells in response to hormones like
    glucagon and epinephrine by a mechanism in which
    cellular cAMP is increased
  • fatty acids transported in plasma have to be
    activated
  • activated fatty acids need to be transported from
    cytosol to mitochondrial matrix where oxidation
    takes place and this regulation has important
    implications for energy production and pathology
  • in diabetics excess fatty acids oxidized produce
    ketone bodies as metabolites which are important
    source of energy for muscle , heart and brain
  • the presence of ketone bodies in plasma leads to
    acidosis which affects oxygen saturation of Hb
    and resultant delivery of oxygen to tissues
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