Presentation is loading. Please wait.

Presentation is loading. Please wait.

Lecture #10 Metabolic Pathways. Outline Glycolysis; a central metabolic pathway Fundamental structure (m x n = 20 x 21) Co-factor coupling (NAD, ATP,

Published byMekhi Caufield Modified over 9 years ago

Similar presentations

Presentation on theme: "Lecture #10 Metabolic Pathways. Outline Glycolysis; a central metabolic pathway Fundamental structure (m x n = 20 x 21) Co-factor coupling (NAD, ATP,"— Presentation transcript:

1 Lecture #10 Metabolic Pathways

2 Outline Glycolysis; a central metabolic pathway Fundamental structure (m x n = 20 x 21) Co-factor coupling (NAD, ATP, P i ) The stoichiometric matrix –Its null spaces Setting up a simulation model –Steady state Interpreting the results from simulation –Concentrations, fluxes, pools, ratios

3 GLYCOLYSIS: AN OPEN SYSTEM

4 Glycolysis as an Open System

5 Compounds: the nodes pathway intermediates cofactors carriers

6 Reactions: the links

7 THE STEADY STATE

8 The Stoichiometric Matrix mxn=20x21, Rank(S)=18 dim(Null)=21-18=3 dim(Left Null)=20-18=2 3 pathways 2 conserved moieties

9 Glycolysis: ‘annotated’ S matrix ES=0

10 Glycolysis: Pathways in Null(S) Selected basis based on biochemical intuition ~P synthesisredox couplinginventory of AMP

11 The Steady State Fluxes (mM/hr): fluxes have to balance the network upper glycolysis lower glycolysis exchange & demand fluxes AMP

12 The Steady State Concentrations (mM); determined by flux map and kinetic constants

13 Reactions: the links pseudo elementary rate constants distance from equilibrium

14 DYNAMIC SIMULATION Model defined and ready for:

15 Simulation: 50% increase in k ATP : dynamic responses of the concentrations ADPATP load=k[ATP] 50% increase at t=0 Key Concepts 1. Time constants 2. Pools 3. Transitions

16 Glycolysis: 0-10 mins Tiled Phase Portrait: fluxes of interest

17 Glycolysis: 10-infinity mins Tiled Phase Portrait: fluxes of interest

18 drain accumulation Dymamic Responses of the Fluxes drainaccumulation Secretion > stst Secretion <stst Secretion > stst Secretion <stst

19 Glycolysis: 0-10 mins Tiled Phase Portrait: concentrations

20 Glycolysis: 10-infinity mins Tiled Phase Portrait: concentrations

21 Simulation: 50% increase in kATP: dynamic responses of the concentrations fastintermediateslow ADPATP load=k[ATP] 50% et=0 Key Concepts 1.Time constants 2.Pools 3.Transitions

22 STRUCTURAL PROPERTIES Towards systems biology

23 Glycolysis: the system with symbolic representation

24 Structural Properties: redox trafficking in glycolysis (#): Redox value #: Flux value

25 Structural Properties: high-energy bond trafficking in glycolysis (#): High-energy bond “value” x: Flux value

26 Structural Properties: The Trafficking of Phosphate Groups in Glycolysis “through” “cycle”

27 Pools: from structural properties

28 Redox Value of Intermediates reduce glycolytic intermediates oxydized glycolytic intermediates metabolites carrier

29 Energy Value of Intermediates

30 Phosphate Bond Trafficking Incorporation: Recycled: Recycle ratio:

31 Pool Map: shows their interconnections and steady state concentrations by area of square

32 Glycolysis: 0-10 mins Tiled Phase Portrait: pools

33 Glycolysis: 10-infinity mins Tiled Phase Portrait: pools

34 Dynamic Responses of the Pools 2(ATP+ADP+AMP) 2ATP+ADP PiPi ~P i capacity occupancy GP + and GP -

35 RATIOS Towards physiology

36 Dynamic Responses of the ratios Adenosine E.C Glycolytic E.C Phosphate recycle ratio

37 Property rations or charges and their dynamic responses

38 Summary First draft dynamic models can be obtained from using measured concentration values, elementary reactions, and associated mass action kinetics. This first draft can be used as a scaffold to build more complicated models that include regulatory effects and interactions with other pathways. Dynamic simulation can be performed for perturbation in environmental parameters and the responses examined in terms of the concentrations and the fluxes. A metabolic map can be analyzed for its stoichiometric texture to assess the co-factor coupling Such breakdown of the biochemistry helps define pools that are physiologically meaningful from a metabolic perspective, and are context dependent.

39 Summary The raw output of the simulation can be post processed with a pooling matrix that allows the pools and their ratios to be graphed to obtain a deeper interpretation of dynamic responses. Some of the responses are built into the topological features of a network and require no regulatory action. The identification of the reactions that move the key pools is possible by the use of the stoichiometric matrix.

40 Projects: perform same analysis Simulate response to NADH load Add R-L Shunt for 2,3 DPG in RBCs Add pentose pathway Add AMPK as a global regulator Add HK, PFK, PK as regulators of glycolysis

Download ppt "Lecture #10 Metabolic Pathways. Outline Glycolysis; a central metabolic pathway Fundamental structure (m x n = 20 x 21) Co-factor coupling (NAD, ATP,"

Similar presentations

Important to recognize that metabolic need of individual cells is different from need of whole organism. Brain needs glucose even when body is starving.

Important to recognize that metabolic need of individual cells is different from need of whole organism. Brain needs glucose even when body is starving.
METABOLISM.

METABOLISM.
Lecture #9 Regulation.

Lecture #9 Regulation.
Lecture #8 Stoichiometric Structure. Outline Cofactors and carriers Bi-linear nature of reactions Pathways versus cofactors Basics of high energy bond.

Lecture #8 Stoichiometric Structure. Outline Cofactors and carriers Bi-linear nature of reactions Pathways versus cofactors Basics of high energy bond.
MULTIPLICITY OF STEADY STATES IN CONTINUOUS CULTURE OF MAMMALIAN CELLS Andrew Yongky, Tung Le, Simon Grimm, Wei-Shou Hu Department of Chemical Engineering.

MULTIPLICITY OF STEADY STATES IN CONTINUOUS CULTURE OF MAMMALIAN CELLS Andrew Yongky, Tung Le, Simon Grimm, Wei-Shou Hu Department of Chemical Engineering.
Lets begin constructing the model… Step (I) - Definitions We begin with a very simple imaginary metabolic network represented as a directed graph: Vertex.

Lets begin constructing the model… Step (I) - Definitions We begin with a very simple imaginary metabolic network represented as a directed graph: Vertex.
Lecture #14 Regulatory Enzymes. Outline Phosphofructokinase-1 Describing the bound states of activators and inhibitors Integration with glycolysis.

Lecture #14 Regulatory Enzymes. Outline Phosphofructokinase-1 Describing the bound states of activators and inhibitors Integration with glycolysis.
Lecture #6 Open Systems. Biological systems are ‘open:’ Example: ATP production by mitochondria.

Lecture #6 Open Systems. Biological systems are ‘open:’ Example: ATP production by mitochondria.
Topological Properties of the Stoichiometric Matrix

Topological Properties of the Stoichiometric Matrix
Engineering of Biological Processes Lecture 6: Modeling metabolism Mark Riley, Associate Professor Department of Ag and Biosystems Engineering The University.

Engineering of Biological Processes Lecture 6: Modeling metabolism Mark Riley, Associate Professor Department of Ag and Biosystems Engineering The University.
Lecture #2 Basics of Kinetic Analysis. Outline Fundamental concepts The dynamic mass balances Some kinetics Multi-scale dynamic models Important assumptions.

Lecture #2 Basics of Kinetic Analysis. Outline Fundamental concepts The dynamic mass balances Some kinetics Multi-scale dynamic models Important assumptions.
Lecture #12 Building Networks. Outline AMP biosynthesis and degradation –A dynamic balance (before the input is fixed) Genetic defects –Quite common in.

Lecture #12 Building Networks. Outline AMP biosynthesis and degradation –A dynamic balance (before the input is fixed) Genetic defects –Quite common in.
Lecture #3 The Process of Simulating Dynamic Mass Balances.

Lecture #3 The Process of Simulating Dynamic Mass Balances.
CELLULAR RESPIRATION II

CELLULAR RESPIRATION II
Inquiry into Life Eleventh Edition Sylvia S. Mader

Inquiry into Life Eleventh Edition Sylvia S. Mader
Introduction of Glucose Metabolism

Introduction of Glucose Metabolism
BIOC/DENT/PHCY 230 LECTURE 2. Lactate dehydrogenase pyruvate + NADHlactate + NAD + M and H subunits: 5 isozymes M subunit has a lower affinity for pyruvate.

BIOC/DENT/PHCY 230 LECTURE 2. Lactate dehydrogenase pyruvate + NADHlactate + NAD + M and H subunits: 5 isozymes M subunit has a lower affinity for pyruvate.
Lecture #1 Introduction.

Lecture #1 Introduction.
The (Right) Null Space of S Systems Biology by Bernhard O. Polson Chapter9 Deborah Sills Walker Lab Group meeting April 12, 2007.

The (Right) Null Space of S Systems Biology by Bernhard O. Polson Chapter9 Deborah Sills Walker Lab Group meeting April 12, 2007.
Metabolic networks Guest lecture by Dr. Carlotta Martelli 26_10_2007.

Metabolic networks Guest lecture by Dr. Carlotta Martelli 26_10_2007.

Similar presentations

Ads by Google