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Metabolomic Profile of Human
  Myocardial Ischemia by NMR
Spectroscopy of Peripheral Blood
            Serum



            엠네기
contents
•   Introduction
•   Method
•   Results
•   Discussion
•   conclusion
INTRODUCTION
Introductions
• The challenge of Diagnosing Myocardial Ischemia
  in the Emergency Department..
• Why did currently discovered biomarkers haven't
  reached clinical practice yet?
• Benefits and challenges in metabolomics..
• Advantages of NMR + multivariate analysis:
  – Powerful, reproducible, inexpensive.
  – Simultaneous measurement of small concentrations
  – Ability to detect the physiochemical status of the
    metabolites
Aim of the study
• developing a metabolic profile of acute MIS in
  peripheral blood serum.
  – Swine and patients, highly controlled models of
    MIS based on transient angioplasty balloon–
    induced coronary occlusion were used for this
    purpose,
  – clinical validation was carried out in patients with
    spontaneous acute chest pain and normal
    electrocardiographic results and troponin values
METHODS
• The animal model:
  – 12h fasting juvenile pigs were sedated and
    anaesthesized.
  – transient angioplasty balloon–induced MIS in the
    proximal left anterior descending coronary artery was
    induced
  – MIS confirmed by ECG..
  – Balloon deflated after 5 minutes
  – Blood samples withdrawn after
  10 and 120 minutes
  – Animal recovered
  – Comparison was done using blood from own animal
    before the procedure as control
• Controlled MIS models in Patients:
  – Non ACS pts scheduled for PCI for stable angina
  – Balloon inflation time was 1 minutes then stent was
    implanted
  – No complications were recorded
  – Blood samples withdrawn after 10 and 120 minutes
  – Controls were patients with normal coronary arteries
    diagnosed by angiography
  – Blood samples of controls were also withdrawn after 10
    and 120 minutes
• Study group with spontaneous chest pain
  – To determine accuracy of the method
  – Pts presented with ST elevation or high tropnin I were
    excluded
• NMR spectroscopy:
  – 20ul of plasma + 2ul of D2O and measured at 37°C
  – Signal of selected metabolites were quantified 
    PCA/PLS-DA were applied to the NMR spectral data base
     leave one out cross validation (LOOCV) of results was
    then applied
• Statistical analysis:
  – mean±SD in tables and as box plots in figures
  – Comparison models:
     • Before vs. after ischemia (in humans and swine)
     • Patients vs. controls (at 10 minutes samples)
     • No MIS vs. MIS (in pts with chest pain at the ER)
  – Continuous data  t-Test, Mann-Whitney 2-tailed test
  – Categorical data  chi-square, Fisher exact test
  – PLS-DA accuracy test  ROC analysis
RESULTS
Before vs. after ischemia (experimental)
Before vs. after ischemia (humans)
Patients vs. controls
Patients vs. controls: Time validity
Patients vs. controls: reliability
                          PLS-DA MODEL
Pts               Ctrls




                          ROC curve
        Training data       Cross
                          validation

                                       Validation error =10%
LOOCV                                  F.negatives= 5%
                                       Sensitivity: 95%
                                       Specificity: 88%
Study group with spontaneous chest pain
                  PLS-DA MODEL




                   ROC curve
                     Cross
                   validation

                                Detection error= 13%
                                F.negatives= 10%
                                Sensitivity was 90%
                                specificity 85%
DISCUSSION
• under highly controlled conditions of coronary flow
  restriction, immediate and striking changes in the
  metabolic profile of peripheral blood serum can be
  detected using NMR spectroscopy.
• metabolomics in a swine model provided very
  reproducible, consistent, and robust markers of
  severe MIS. Afterward, this information was
  validated in human subjects.
• Advantages of using animal models:
  – Although animal model showed low sensitivity
    biomarkers, rather potential high specificity in a severe
    ischemia scenario was detected
  – Reduction in human subjects needed
• The cardiac tissue undergoes dramatic
  metabolomic changes during ischemia, main
  receptors involved are:
  – peroxisome proliferator-activated receptor alpha,
  – peroxisome proliferator-activated receptor gamma
    coactivator 1-alpha,
  – estrogen-related receptor alpha transcription
    factors
• Glucose/FA metabolism and acute ischemia..
• Other changes found:
  – Lactate release
  – Interruption in TCA cycle activity
  – down-regulation in enzymes involved in FA oxidation and
    Glucose metabolism
  – Liver mediated TCA activity through vassopressin
  – Increased oxidation of FA though release of catecholamines
  – Increase circulation of TGs during MIS as suggested by this
    study.
• The delayed increase in creatine, could be explained by
  an increased ischemia-related transport of ATP
  between cytoplasm and the mitochondria of
  cardiomyocytes.
Clinical Validation
• This metabolic biosignature showed high accuracy
  in discriminating those patients with and without
  MIS.
• In most cases, the final diagnosis was not achieved
  until 12 hours of thorough evaluation at the
  cardiology department!
Study limitaions
• Although this method showed potential in
  reaching clinical practice in the future the
  author recommends wider studies with larger
  groups of patients with chest pain.
Conclusion
• Metabolomics, based on the model presented
  here, represents a robust, minimally invasive and
  cost effective bioprofile for the detection of acute
  MIS with potential clinical application.
• This is the first study to apply metabolomics in the
  field of diagnostic medicine for CVD which shows
  potential in future clinical practice
My Personal Thoughts

• Using animal models to induce
  controlled pathological environments
  can be useful in detecting more specific
  biomarkers of CVD
• Using metabolomics combined with
  statistical cross validation between
  patients and control is helpful in
  detecting more CVD specific
  metabolites.
Thank you for your attention
감사합니다

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Metabolomic Profile of Human Myocardial Ischemia by NMR Spectroscopy of Peripheral Blood Serum

  • 1. Metabolomic Profile of Human Myocardial Ischemia by NMR Spectroscopy of Peripheral Blood Serum 엠네기
  • 2. contents • Introduction • Method • Results • Discussion • conclusion
  • 4. Introductions • The challenge of Diagnosing Myocardial Ischemia in the Emergency Department.. • Why did currently discovered biomarkers haven't reached clinical practice yet? • Benefits and challenges in metabolomics.. • Advantages of NMR + multivariate analysis: – Powerful, reproducible, inexpensive. – Simultaneous measurement of small concentrations – Ability to detect the physiochemical status of the metabolites
  • 5. Aim of the study • developing a metabolic profile of acute MIS in peripheral blood serum. – Swine and patients, highly controlled models of MIS based on transient angioplasty balloon– induced coronary occlusion were used for this purpose, – clinical validation was carried out in patients with spontaneous acute chest pain and normal electrocardiographic results and troponin values
  • 7.
  • 8. • The animal model: – 12h fasting juvenile pigs were sedated and anaesthesized. – transient angioplasty balloon–induced MIS in the proximal left anterior descending coronary artery was induced – MIS confirmed by ECG.. – Balloon deflated after 5 minutes – Blood samples withdrawn after 10 and 120 minutes – Animal recovered – Comparison was done using blood from own animal before the procedure as control
  • 9. • Controlled MIS models in Patients: – Non ACS pts scheduled for PCI for stable angina – Balloon inflation time was 1 minutes then stent was implanted – No complications were recorded – Blood samples withdrawn after 10 and 120 minutes – Controls were patients with normal coronary arteries diagnosed by angiography – Blood samples of controls were also withdrawn after 10 and 120 minutes • Study group with spontaneous chest pain – To determine accuracy of the method – Pts presented with ST elevation or high tropnin I were excluded
  • 10.
  • 11. • NMR spectroscopy: – 20ul of plasma + 2ul of D2O and measured at 37°C – Signal of selected metabolites were quantified  PCA/PLS-DA were applied to the NMR spectral data base  leave one out cross validation (LOOCV) of results was then applied • Statistical analysis: – mean±SD in tables and as box plots in figures – Comparison models: • Before vs. after ischemia (in humans and swine) • Patients vs. controls (at 10 minutes samples) • No MIS vs. MIS (in pts with chest pain at the ER) – Continuous data  t-Test, Mann-Whitney 2-tailed test – Categorical data  chi-square, Fisher exact test – PLS-DA accuracy test  ROC analysis
  • 13. Before vs. after ischemia (experimental)
  • 14.
  • 15. Before vs. after ischemia (humans)
  • 16.
  • 18. Patients vs. controls: Time validity
  • 19. Patients vs. controls: reliability PLS-DA MODEL Pts Ctrls ROC curve Training data Cross validation Validation error =10% LOOCV F.negatives= 5% Sensitivity: 95% Specificity: 88%
  • 20. Study group with spontaneous chest pain PLS-DA MODEL ROC curve Cross validation Detection error= 13% F.negatives= 10% Sensitivity was 90% specificity 85%
  • 22. • under highly controlled conditions of coronary flow restriction, immediate and striking changes in the metabolic profile of peripheral blood serum can be detected using NMR spectroscopy. • metabolomics in a swine model provided very reproducible, consistent, and robust markers of severe MIS. Afterward, this information was validated in human subjects. • Advantages of using animal models: – Although animal model showed low sensitivity biomarkers, rather potential high specificity in a severe ischemia scenario was detected – Reduction in human subjects needed
  • 23. • The cardiac tissue undergoes dramatic metabolomic changes during ischemia, main receptors involved are: – peroxisome proliferator-activated receptor alpha, – peroxisome proliferator-activated receptor gamma coactivator 1-alpha, – estrogen-related receptor alpha transcription factors
  • 24. • Glucose/FA metabolism and acute ischemia.. • Other changes found: – Lactate release – Interruption in TCA cycle activity – down-regulation in enzymes involved in FA oxidation and Glucose metabolism – Liver mediated TCA activity through vassopressin – Increased oxidation of FA though release of catecholamines – Increase circulation of TGs during MIS as suggested by this study. • The delayed increase in creatine, could be explained by an increased ischemia-related transport of ATP between cytoplasm and the mitochondria of cardiomyocytes.
  • 25. Clinical Validation • This metabolic biosignature showed high accuracy in discriminating those patients with and without MIS. • In most cases, the final diagnosis was not achieved until 12 hours of thorough evaluation at the cardiology department!
  • 26. Study limitaions • Although this method showed potential in reaching clinical practice in the future the author recommends wider studies with larger groups of patients with chest pain.
  • 27. Conclusion • Metabolomics, based on the model presented here, represents a robust, minimally invasive and cost effective bioprofile for the detection of acute MIS with potential clinical application. • This is the first study to apply metabolomics in the field of diagnostic medicine for CVD which shows potential in future clinical practice
  • 28. My Personal Thoughts • Using animal models to induce controlled pathological environments can be useful in detecting more specific biomarkers of CVD • Using metabolomics combined with statistical cross validation between patients and control is helpful in detecting more CVD specific metabolites.
  • 29. Thank you for your attention 감사합니다

Notas del editor

  1. To show the potential diagnostic value