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    Bch-Ii 28032022

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    Hawaid Ahmad
    The document discusses biosynthesis of fatty acids and eicosanoids. It describes the key reactions like acetyl-CoA carboxylase and fatty acid synthase complex. It also discusses elongation of fatty acid chains and how the nutritional state regulates lipogenesis.

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    Bch-Ii 28032022

    Uploaded by

    Hawaid Ahmad
    4 views11 pages
    The document discusses biosynthesis of fatty acids and eicosanoids. It describes the key reactions like acetyl-CoA carboxylase and fatty acid synthase complex. It also discusses elongation of fatty acid chains and how the nutritional state regulates lipogenesis.

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    BCH-II 28032022

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    The document discusses biosynthesis of fatty acids and eicosanoids. It describes the key reactions like acetyl-CoA carboxylase and fatty acid synthase complex. It also discusses elongation of fatty acid chains and how the nutritional state regulates lipogenesis.

    Copyright:

    © All Rights Reserved
    Download as PDF, TXT or read online from Scribd
    Download as pdf or txt
    4 views11 pages

    Bch-Ii 28032022

    Uploaded by

    Hawaid Ahmad
    The document discusses biosynthesis of fatty acids and eicosanoids. It describes the key reactions like acetyl-CoA carboxylase and fatty acid synthase complex. It also discusses elongation of fatty acid chains and how the nutritional state regulates lipogenesis.

    Copyright:

    © All Rights Reserved
    Download as PDF, TXT or read online from Scribd
    Download as pdf or txt
    of 11

    Biosynthesis of Fatty

    Acids and Eicosanoids


    Biochemistry-II
    Dr. Shumaila Naz
    28-03-2022
    Learning Outcomes
    • The reaction catalyzed by acetyl-Co-A carboxylase and understand the mechanism by
    which this activity is regulated
    • Long chain fatty acids synthesis by the repeated condensation of two carbon units
    • Polyunsaturated fatty acids synthesis by desaturase and elongation enzymes
    • Cyclooxygenase and lipoxygenase pathways responsible for the formation of various
    classes of eicosanoids
    Biomedical Importance
    Extramitochondrial system
    Unsaturated FA in phospholipids of
    acetyl-CoA PM--- Membrane fluidity
    Cystol High ratio of P:S ratio--- coronary
    heart disease
    fatty acids Polyunsaturated fatty acids derived
    from plants…..essential fatty
    Mammals: glucose is primary acids…. Eicosanoidfatty
    substrate for lipogenesis acids ---prostaglandins
    Ruminants: actate… diet

    Inhibition of lipogenesis---Type I
    diabetes mellitus
    LIPOGENESIS
    • Tissues, including liver, kidney, brain, lung, mammary gland, and adipose
    tissue
    • Cofactor requirements include NADPH, ATP, Mn2+, biotin, and HCO3−
    (as a source of CO2)
    • AcetylCoA is the immediate substrate, and free palmitate is the end
    product

    1. Transfer of acetyl-CoA from mitochondria to cytosol

    2. Activation of acetyl-CoA; synthesis of malonyl-CoA

    3. Five step elongation cycle of FA synthesis via ACP intermediates


    Production of Malonyl-CoA Is the Initial &
    Controlling Step in Fatty Acid Synthesis

    Bicarbonate as a source of CO2


    Acetyl-CoA carboxylase has a …. carboxylation of acetyl-CoA
    requirement for the vitamin to malonyl-CoA in the presence
    biotin. The enzyme is a of ATP and acetyl-CoA
    multienzyme protein containing carboxylase.
    a variable number of identical
    subunits, each containing biotin,
    biotin carboxylase, biotin The reaction takes place in two
    carboxyl carrier protein, and steps:
    transcarboxylase, as well as a
    regulatory allosteric site. (1) carboxylation of biotin
    involving ATP and

    (2) transfer of the carboxyl to


    acetyl-CoA to form malonyl-
    CoA
    LIPOGENESIS
    • The Fatty Acid Synthase Complex Is a Polypeptide Containing
    Seven Enzyme Activities
    The complex is a dimer of two identical
    polypeptide monomers, 1 and 2

    Each consists of seven enzyme activities


    and the acyl carrier protein (ACP)

    sulfhydryl group The -SH of the 4′-phosphopantetheine of


    of cysteine is
    ionizable and one monomer is in close proximity to the -
    take part in
    enzymatic SH of the cysteine residue of the ketoacyl
    reactions
    synthase of the other monomer,
    suggesting a “head-to-tail” arrangement
    of the two monomers
    Acetyl-CoA combines with a cysteine -SH group (reaction 1a)

    Malonyl-CoA combines with the adjacent -SH on the 4-


    phosphopantetheine of ACP of the other monomer (reaction 1b)

    Catalyzed by malonyl acetyl transacylase to form acetyl (acyl)-


    malonyl enzyme

    The acetyl group attacks the methylene group of the malonyl


    residue, catalyzed by 3-ketoacyl synthase, and liberates CO2,
    forming 3-ketoacyl enzyme (acetoacetyl enzyme) (reaction 2),
    freeing the cysteine -SH group

    Decarboxylation allows the reaction to go to completion, pulling


    the whole sequence of reactions in the forward direction. The 3-
    ketoacyl group is reduced, dehydrated, and reduced again
    (reactions 3, 4, 5) to form the corresponding saturated acyl S
    enzyme.
    It is liberated from the
    enzyme complex by the
    activity of a seventh A new malonyl-CoA molecule combines with the -SH of 4-
    enzyme in the complex,
    thioesterase phosphopantetheine, displacing the saturated acyl residue onto
    the free cysteine -SH group. The sequence of reactions is
    repeated six more times until a saturated 16-carbon acyl radical
    (palmityl) has been assembled
    Transfer of acetyl-CoA from mitochondria to cytosol
    Acetyl-CoA is formed from glucose
    via the oxidation of pyruvate within
    the mitochondria

    Citrate, formed after condensation of


    acetyl-CoA with oxaloacetate in
    the citric acid cycle within
    mitochondria, is translocated into the
    extramitochondrial compartment via
    the tricarboxylate transporter, where
    in the presence of CoA and ATP it
    undergoes cleavage to acetyl-CoA and
    oxaloacetate catalyzed by ATP-citrate
    lyase, which increases in activity in the
    well-fed state
    Sources of NADPH for FA Synthesis
    The acetyl-CoA is available for malonyl-CoA formation
    and synthesis to palmitate.
    The resulting oxaloacetate malate via NADH-linked
    malate dehydrogenase…. followed by the generation of
    NADPH via the malic enzyme.
    The NADPH becomes available for lipogenesis, and the
    pyruvate can be used to regenerate acetyl-CoA after
    transport into the mitochondrion.

    Malate itself can be transported into the


    mitochondrion, where it is able to re-form oxaloacetate.

    Citrate (tricarboxylate) transporter in the


    mitochondrial membrane requires malate to exchange
    with citrate
    Elongation of Fatty Acid Chains Occurs
    in the Endoplasmic Reticulum
    This pathway (the “microsomal system”) elongates saturated
    and unsaturated fatty acyl-CoAs (from C10 upward) by two
    carbons,

    Malonyl-CoA as acetyl donor and

    NADPH as reductant,

    Catalyzed by the microsomal fatty acid elongase system of


    enzymes

    Elongation of stearyl-CoA in brain increases rapidly during


    myelination in order to provide C22 and C24 fatty acids for
    sphingolipids.
    THE NUTRITIONAL STATE REGULATES LIPOGENESIS

    Excess carbohydrate is stored as fat --- caloric deficiency

    Lipogenesis converts surplus glucose and intermediates such as pyruvate, lactate,


    and acetyl-CoA

    The nutritional state of the organism is the main factor regulating the rate of
    lipogenesis.

    depressed under conditions of restricted caloric intake, on a fat diet, or when there
    is a deficiency of insulin, as in diabetes mellitus

    Lipogenesis is increased when sucrose is fed instead of glucose because fructose


    bypasses the phosphofructokinase control point in glycolysis and floods the
    lipogenic pathway

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