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Haytham Soliman, MD, FSCAI
Fayoum University
Case
A 25 year old patient
Has reports no relevant cardiac history
Complained of dyspnea for 6 month
He had an assessment that lead to an echocardiography
Echo revealed a Secondum ASD 18mm with left to right shunt
Mild RV dilation
Mean PAP 25mmHg
Where ?
When?
What?
How?
Four major
questions
ASD
TAPVR
Volume overload
Volume and pressure
overload
VSD
PDA
Where is the level of the shunt ?
• Minor shunts may be accidentally discovered
• Early discovery means less effect of the shunt on pulmonary artery
• Shunts treated at the 1st year of age can have no residual PHT
• In large defects, treatment after the 2nd years will not change the PAP to
normal levels
• The later and larger the defect the faster we will reach a point of no return
When this defect was discovered ?
What changes did happen in the pulmonary
circulation?
• Abnormal shear stress, circumferential wall stretch and endothelial
dysfunction
• Decrease vasoactive mediators, such as endothelin-1, prostacyclin
and nitric oxide → vasoconstriction
• Aberrant expression of vascular endothelial and fibroblast growth
factors promotes vascular remodelling
• Smooth muscle hypertrophy and proliferation
• Increased intracellular matrix deposition
Diagnostic tools
• Clinical examination
• Laboratory tests
• Echocardiography
• Invasive Right heart cath
Laboratory tests
• Total blood cell counts
• serum iron levels, haematocrit
• Infectious diseases
• NT-pro-BNP
• Arterial blood gases
• 6MWT
Functional assessment
This is a noninvasive marker of vascular damage and
remodeling
which has been shown to be significantly raised in CHD patients
with irreversible PAH post-surgery
Imaging ( Echocardiography)
• The shunt site
• The RV and LV functions
• The PAP mean pressure above 20 mmHg
• The shunt fraction
Invasive right heart cath
• Not indicated in bidirectional shunts and Eisenmenger’s
syndrome
• Pulmonary pressure ( mean and peak)
• Systemic vascular resistance
• Pulmonary vascular resistance ( WU)
• Shunt fraction Qp/Qs
• Pulmonary reactivity test
How do we treat these patients
• Medical therapy
• Intervention ( surgery or device closure)
• O2 therapy in Eisenmenger’s syndrome for improving symptoms and
QOL
Medical therapy
• Diuretics ( in RV failure)
• Vasodilators ( in post repair patients that has vasoactive pulmonary arteries )
• CCbs are contraindicated in Eisenmenger patients
• Anticoagulation with vitamin K antagonists (VKAs) in the absence of atrial
arrhythmia, mechanical valves, or vascular prosthesis is not generally
recommended in PAH-CHD
• Secondary erythrocytosis is beneficial for adequate oxygen transport and
delivery so routine phlebotomy should be avoided
PAH directed therapy
- Parenteral prostaglandins ( risk of infection and thrombosis)
- subcutaneous or inhaled forms are generally preferred
- Eisenmenger patients, the endothelin receptor antagonist (ERA)
bosentan has been shown to improve 6MWT and decrease PVR
- less evidence for phosphodiesterase type 5 (PDE-5) inhibitors
sildenafil and tadalafil
- Experience is limited for latest-generation PAH drugs such as
macitentan, selexipag, or riociguat in the setting of CHD
Intervention
• Chamber volume overload ( RV or LV)
• Pulmonary vascular resistance ( 3- 5 WU)
• Shunt fraction (Qp/Qs 1.5)
Best survival among PAH
• Slow progression
• Less effort
• More RV remodeling to pressure
• Most of shunts are small
• Advance in detection and closure
in early ages
Back to our patient
• He had mild RV dilation
• Elevated PAP with a PVR of 3 WU
• He has favorable anatomy for device closure
• So we used a 23mm device to close the ASD
• Follow up showed decrease in mean PAP to 18 mmHg
Summary
• Early detection and treatment of PAH-CHD is crucial
• Advances in diagnosis and closure techniques lead to increase
survival
• Proper tailoring according to PVR, shunt fraction and chamber
dilation must be done
• PAH direct therapy has increased survival and improved symptoms
specially in Eisenmenger patients
• But till now there is no change in their mortality
Thank you so much

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pulmonary hypertension with CHD.pptx

  • 1. Haytham Soliman, MD, FSCAI Fayoum University
  • 2. Case A 25 year old patient Has reports no relevant cardiac history Complained of dyspnea for 6 month He had an assessment that lead to an echocardiography Echo revealed a Secondum ASD 18mm with left to right shunt Mild RV dilation Mean PAP 25mmHg
  • 4. ASD TAPVR Volume overload Volume and pressure overload VSD PDA Where is the level of the shunt ?
  • 5.
  • 6. • Minor shunts may be accidentally discovered • Early discovery means less effect of the shunt on pulmonary artery • Shunts treated at the 1st year of age can have no residual PHT • In large defects, treatment after the 2nd years will not change the PAP to normal levels • The later and larger the defect the faster we will reach a point of no return When this defect was discovered ?
  • 7.
  • 8. What changes did happen in the pulmonary circulation?
  • 9.
  • 10. • Abnormal shear stress, circumferential wall stretch and endothelial dysfunction • Decrease vasoactive mediators, such as endothelin-1, prostacyclin and nitric oxide → vasoconstriction • Aberrant expression of vascular endothelial and fibroblast growth factors promotes vascular remodelling • Smooth muscle hypertrophy and proliferation • Increased intracellular matrix deposition
  • 11.
  • 12. Diagnostic tools • Clinical examination • Laboratory tests • Echocardiography • Invasive Right heart cath
  • 13.
  • 14. Laboratory tests • Total blood cell counts • serum iron levels, haematocrit • Infectious diseases • NT-pro-BNP • Arterial blood gases • 6MWT Functional assessment
  • 15. This is a noninvasive marker of vascular damage and remodeling which has been shown to be significantly raised in CHD patients with irreversible PAH post-surgery
  • 16. Imaging ( Echocardiography) • The shunt site • The RV and LV functions • The PAP mean pressure above 20 mmHg • The shunt fraction
  • 17. Invasive right heart cath • Not indicated in bidirectional shunts and Eisenmenger’s syndrome • Pulmonary pressure ( mean and peak) • Systemic vascular resistance • Pulmonary vascular resistance ( WU) • Shunt fraction Qp/Qs • Pulmonary reactivity test
  • 18. How do we treat these patients • Medical therapy • Intervention ( surgery or device closure) • O2 therapy in Eisenmenger’s syndrome for improving symptoms and QOL
  • 19. Medical therapy • Diuretics ( in RV failure) • Vasodilators ( in post repair patients that has vasoactive pulmonary arteries ) • CCbs are contraindicated in Eisenmenger patients • Anticoagulation with vitamin K antagonists (VKAs) in the absence of atrial arrhythmia, mechanical valves, or vascular prosthesis is not generally recommended in PAH-CHD • Secondary erythrocytosis is beneficial for adequate oxygen transport and delivery so routine phlebotomy should be avoided
  • 20. PAH directed therapy - Parenteral prostaglandins ( risk of infection and thrombosis) - subcutaneous or inhaled forms are generally preferred - Eisenmenger patients, the endothelin receptor antagonist (ERA) bosentan has been shown to improve 6MWT and decrease PVR - less evidence for phosphodiesterase type 5 (PDE-5) inhibitors sildenafil and tadalafil - Experience is limited for latest-generation PAH drugs such as macitentan, selexipag, or riociguat in the setting of CHD
  • 21.
  • 22. Intervention • Chamber volume overload ( RV or LV) • Pulmonary vascular resistance ( 3- 5 WU) • Shunt fraction (Qp/Qs 1.5)
  • 23.
  • 24.
  • 25.
  • 26. Best survival among PAH • Slow progression • Less effort • More RV remodeling to pressure • Most of shunts are small • Advance in detection and closure in early ages
  • 27. Back to our patient • He had mild RV dilation • Elevated PAP with a PVR of 3 WU • He has favorable anatomy for device closure • So we used a 23mm device to close the ASD • Follow up showed decrease in mean PAP to 18 mmHg
  • 28. Summary • Early detection and treatment of PAH-CHD is crucial • Advances in diagnosis and closure techniques lead to increase survival • Proper tailoring according to PVR, shunt fraction and chamber dilation must be done • PAH direct therapy has increased survival and improved symptoms specially in Eisenmenger patients • But till now there is no change in their mortality
  • 29. Thank you so much