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Pentose Phosphate Shunt
Hexose Monophosphate Shunt
        (HMP Shunt)
HMP Shunt

• HMP is a minor oxidation pathway for glucose


• It is an alternative pathway which involves

  phospho–pentoses as intermediates for

  purposes other than energy production
HMP Shunt
• HMP occurs in the Cytoplasm of:

    1. Liver

    2. Lactating mammary gland

    3. Adipose tissue

    4. Red blood cells

    5. Adrenal cortex
Rate
                  limiting
  Oxidation       enzyme




Oxidative Decarboxylation
Hexose Monophosphate Shunt

•   The first step:
Hexose Monophosphate Shunt
•   Reactions of the hexose monophosphate
    pathways:
•   Enzymes numbered above are
      1.   Glucose 6-phosphate dehydroganase
           and gluconolactone hydrolyase
      2.   6-phosphogluconate dehydrogenase
      3.   Phosphopentose isomerase
      4.   Phosphopentose epimerase
      5.   Transketolase (TPP cofactor)
      6.   Transaldolase
      7.   Transketolase (TPP cofactor)
3 molecules



3rd   2nd     TPP   1st


              TPP




        TPP
2 molecules




 1 molecule
Regulation of HMP Shunt

1. Insulin increases the activity of HMP pathway

  by stimulating the synthesis of

  dehydrogenases involved in HMP pathway

2. Galactose-1-phosphate inhibits G-6-P DH
Metabolic Significance of HMP Shunt

1) It is the only source of phosphorylated
  pentoses which used for the synthesis of:

  A. Nucleotides: ATP & GTP

  B. Coenzymes: FMN, FAD, NAD+

  C. Certain vitamins: B2 & B12

  D. Nucleic acids: DNA & RNA
Metabolic Significance of HMP Shunt

2) It is the major source of NADPH+ which is essential for:

A. Fatty acid synthesis for lipogenesis which occurs in
   liver, adipose tissue & lactating mammary gland

B. Steroid synthesis (Adrenal cortical hormones, Sex
   hormones) which is active in adrenal cortex, testes,
   ovaries & placenta

C. Act as coenzyme of glutathione reductase which keeps
   GSH in reduced state
Other NADPH+ Source
• Malic enzyme (In the cytoplasm) catalyze the oxidative

  decarboxylation of malate to pyruvate and CO2, with the

  concomitant reduction of the cofactor NADP+ to NADPH

                     Malic enz.
• Malate +   NADP+                pyruvate + CO2 + NADPH
Metabolic Significance of HMP Shunt

3) NADPH is essential for keeping the reduced form of
   glutathione (G-SH), which is essential for keeping the red
   blood cell wall intact, since G-SH is essential for:

   A. Keeping iron of Hb in Ferrous state (Fe2+)

   B. Keeping globin of Hb in native structure

   C. Preventing accumulation of free radicals & H2O2 in RBCs
      So Keeping RBCs wall intact preventing hemolysis
Glutathione Protects us from Oxidation




1              2              3




    4 Protects RBC's against hemolysis
Oxidized Glutathione   Reduced Glutathione
Rate limiting enzyme
Favism or Primaquine Sensitivity

                           Fava beans)
                          Aspirin)

Metabolite (Like,                          Oxidation   H2O2
                        Sulfa Drugs)
                     Primaquine)


H2O2 + 2 G-SH     Glutathione Peroxidase   2 H2O + G-S-S-G

G-S-S-G + NADPH   Glutathione Reductase     2 G-SH + NADP+

Glucose-6-phosphate + NADP+      Glucose-6-P DH
                                                  NADPH + 6-phospho
                                                  gluconolactone
Fava Beans
Child with
  Favism
With signs of
  anemia
(decreased red
blood cell count,
 jaundice, etc.)
Conclusion
– Favism is a significant disease in society today

– it plays a role similar to sickle cell anemia

– It may act as a defense mechanism against malaria

– The unusually high number of oxidants in the blood can
  kill the malaria, bacteria, Plasmodium falciparum

– Interestingly, the highest incidence of this disease is
  found in areas where malaria is present (Mediterranean
  and African areas)
Glucuronic Acid Synthesis
HMP Shunt
Metabolic Significance of
       Glucuronic Acid
• Glucuronic acid is used in:
1. Synthesis of Proteoglycans
   (Glycosaminoglycans, GAGs)
2. Excretion of Bilirubin and Steroid compounds
   (Glucuronidation)
3. Detoxification of certain drugs and their
   metabolites by increasing their solubility
   (Glucuronidation)
Official Names of Malic Enzymes

• Malate dehydrogenase (decarboxylating)
• Malic enzyme
• NADP-Malic enzyme
• Pyruvic-Malic carboxylase
• Malate + NADP+    Malic enz   pyruvate +
                                CO2 + NADPH
6 hmp+glucuronic

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6 hmp+glucuronic

  • 1. Pentose Phosphate Shunt Hexose Monophosphate Shunt (HMP Shunt)
  • 2. HMP Shunt • HMP is a minor oxidation pathway for glucose • It is an alternative pathway which involves phospho–pentoses as intermediates for purposes other than energy production
  • 3. HMP Shunt • HMP occurs in the Cytoplasm of: 1. Liver 2. Lactating mammary gland 3. Adipose tissue 4. Red blood cells 5. Adrenal cortex
  • 4. Rate limiting Oxidation enzyme Oxidative Decarboxylation
  • 6. Hexose Monophosphate Shunt • Reactions of the hexose monophosphate pathways: • Enzymes numbered above are 1. Glucose 6-phosphate dehydroganase and gluconolactone hydrolyase 2. 6-phosphogluconate dehydrogenase 3. Phosphopentose isomerase 4. Phosphopentose epimerase 5. Transketolase (TPP cofactor) 6. Transaldolase 7. Transketolase (TPP cofactor)
  • 7. 3 molecules 3rd 2nd TPP 1st TPP TPP
  • 8. 2 molecules 1 molecule
  • 9. Regulation of HMP Shunt 1. Insulin increases the activity of HMP pathway by stimulating the synthesis of dehydrogenases involved in HMP pathway 2. Galactose-1-phosphate inhibits G-6-P DH
  • 10. Metabolic Significance of HMP Shunt 1) It is the only source of phosphorylated pentoses which used for the synthesis of: A. Nucleotides: ATP & GTP B. Coenzymes: FMN, FAD, NAD+ C. Certain vitamins: B2 & B12 D. Nucleic acids: DNA & RNA
  • 11. Metabolic Significance of HMP Shunt 2) It is the major source of NADPH+ which is essential for: A. Fatty acid synthesis for lipogenesis which occurs in liver, adipose tissue & lactating mammary gland B. Steroid synthesis (Adrenal cortical hormones, Sex hormones) which is active in adrenal cortex, testes, ovaries & placenta C. Act as coenzyme of glutathione reductase which keeps GSH in reduced state
  • 12. Other NADPH+ Source • Malic enzyme (In the cytoplasm) catalyze the oxidative decarboxylation of malate to pyruvate and CO2, with the concomitant reduction of the cofactor NADP+ to NADPH Malic enz. • Malate + NADP+ pyruvate + CO2 + NADPH
  • 13. Metabolic Significance of HMP Shunt 3) NADPH is essential for keeping the reduced form of glutathione (G-SH), which is essential for keeping the red blood cell wall intact, since G-SH is essential for: A. Keeping iron of Hb in Ferrous state (Fe2+) B. Keeping globin of Hb in native structure C. Preventing accumulation of free radicals & H2O2 in RBCs So Keeping RBCs wall intact preventing hemolysis
  • 14. Glutathione Protects us from Oxidation 1 2 3 4 Protects RBC's against hemolysis
  • 15. Oxidized Glutathione Reduced Glutathione
  • 17. Favism or Primaquine Sensitivity Fava beans) Aspirin) Metabolite (Like, Oxidation H2O2 Sulfa Drugs) Primaquine) H2O2 + 2 G-SH Glutathione Peroxidase 2 H2O + G-S-S-G G-S-S-G + NADPH Glutathione Reductase 2 G-SH + NADP+ Glucose-6-phosphate + NADP+ Glucose-6-P DH NADPH + 6-phospho gluconolactone
  • 18.
  • 20. Child with Favism With signs of anemia (decreased red blood cell count, jaundice, etc.)
  • 21. Conclusion – Favism is a significant disease in society today – it plays a role similar to sickle cell anemia – It may act as a defense mechanism against malaria – The unusually high number of oxidants in the blood can kill the malaria, bacteria, Plasmodium falciparum – Interestingly, the highest incidence of this disease is found in areas where malaria is present (Mediterranean and African areas)
  • 23.
  • 25.
  • 26. Metabolic Significance of Glucuronic Acid • Glucuronic acid is used in: 1. Synthesis of Proteoglycans (Glycosaminoglycans, GAGs) 2. Excretion of Bilirubin and Steroid compounds (Glucuronidation) 3. Detoxification of certain drugs and their metabolites by increasing their solubility (Glucuronidation)
  • 27. Official Names of Malic Enzymes • Malate dehydrogenase (decarboxylating) • Malic enzyme • NADP-Malic enzyme • Pyruvic-Malic carboxylase • Malate + NADP+ Malic enz pyruvate + CO2 + NADPH