Post on 09-Aug-2020
Pulmonary Hypertension: Another Use for Viagra®
Kathleen Tong, MD Director, Heart Failure Program
Assistant Clinical Professor
University of California, Davis
Disclosures
• I have no financial conflicts
A Real Disclosure
• I will be discussing off label use of phosphodiesterase-5 inhibitors
Goals
• Define pulmonary hypertension
• Elucidate WHO groups
• Treatments for pulmonary hypertension
• Approach to pulmonary hypertension, from a cardiologist’s perspective
• Right ventricular failure
Pulmonary Hypertension (PH)
• Sustained elevations of pulmonary artery pressure (mPAP) of ≥25 mm Hg at rest (normal : 8-21 mm Hg)
– Usually measured by right heart catheterization
• By echo the pulmonary artery systolic pressure (PASP) may be estimated
– PASP >36 mm Hg
• Definition does not suggest etiology
Badesch, et al. JACC 2009
Pulmonary Hypertension
• Etiologies are many
• Classification system has evolved
• Most recent classification was published in 2009
• Grouped based on histologic findings, response to treatment and etiology
– Five WHO groups
Revised Clinical Classification of PH Endorsed by the World Health Organization (WHO)
1. Pulmonary arterial hypertension (PAH)
2. Pulmonary hypertension with left heart disease
3. Pulmonary hypertension associated with lung diseases and/or hypoxemia
4. Pulmonary hypertension due to chronic thrombotic and/or embolic disease
5. Pulmonary hypertension with multiple etiologies
Etiologies of Group 1 PH: PAH
• Idiopathic (IPAH) – Formerly Primary Pulmonary Hypertension
• Heritable PAH
• Associated PAH
• Connective tissue disease
• HIV infection
• Congenital heart disease
• Drugs/toxins - METHAMPHETAMINE
• Portal hypertension
• Many others
Rare disease: Prevalence is 15/million; 50,000 to 100,000 in the U.S.
Simonneau G, et al. J Am Coll Cardiol 2009:54:S43-S54.
Etiologies of Group 1 PH: PAH
• Idiopathic (IPAH) – Formerly PPH
• Heritable PAH
• Associated PAH
• Connective tissue disease
• HIV infection
• Congenital heart disease
• Drugs/toxins
• Portal hypertension
• Many others
Rare disease: Prevalence is 15/million; 50,000 to 100,000 in the U.S.
Simonneau G, et al. J Am Coll Cardiol 2009:54:S43-S54.
VERY RARE US Prevalence is 50,000-100000
Aorta
Group 1: PAH
RA VEINS PA PV RV LA LV
PRESSURES HIGH PRESSURES LOW/NORMAL • PCWP • LVEDP
Normal
PAH
PC
“PRE-CAPILLARY”
Therapeutic Targets for PAH
Therapeutic Targets for PAH
• Bosentan • Ambrisentan
• Inhaled NO • PDE 5 Inhibitors
• Sildenafil • Tadalafil
• Infusion • Epoprostenol • Treprostinil
• Inhaled • Treprostinil • Iloprost
• Oral • None FDA
approved
Group 2 PH
• Pulmonary hypertension due to left sided heart disease
• Most commonly seen group
• Left sided pump failure
– Diastolic heart failure • Hypertension
• Infiltrative disorders
– Systolic heart failure • Ischemic cardiomyopathy
• Viral cardiomyopathy
• Valvular disease
– Mitral
– Aortic
Aorta
Group 2
RA VEINS PA PV RV LA LV
PRESSURES NORMAL
PRESSURE NORMAL
PC
Aorta
Group 2
RA VEINS PA PV RV LA LV
PRESSURES HIGH
PASSIVE PRESSURE ELEVATION
Mean PA Pressure – Wedge Pressure >10-15 OR the PVR is < 3
PVR = (Mean PAP – Wedge) Cardiac Output
PC
“POST-CAPILLARY”
Aorta
Group 2
RA VEINS PA PV RV LA LV
PRESSURES HIGH
PRESSURE ELEVATION “Out of Proportion” Or FIXED PULMONARY HYPERTENSION
Mean PA Pressure – Wedge Pressure >10-15 OR the PVR is > 3
PVR = (Mean PAP – Wedge) Cardiac Output
PC
Group 2: Treatment
• Treatment is disease/condition specific
– Systolic heart failure: beta blocker, ACE I, diuretics, spironolactone, CRT, LVAD
– Aortic Stenosis: Aortic valve replacement
– Mitral regurgitation: Mitral valve repair
– Ischemic cardiomyopathy: PCI or CABG
• Overall goal is to decrease left sided filling pressures
Can you have mixed Group 2 and Group 1?
• Group 1 is very rare
• PH “out of proportion” usually represents longstanding left sided congestion
– Group 1 drugs (ET antagonists, prostacyclin analogs) have not shown benefit and may be harmful in Group 2 PH except…
– PDE 5 inhibitors (RCT of 34 patients) associated with improved exercise capacity and quality of life with no safety issues
GD Lewis. Circulation. 2007
Group 3 PH
• Associated with lung diseases and/or hypoxemia
• COPD
• Sleep apnea
• Interstitial lung disease
– Idiopathic pulmonary fibrosis
Aorta
Group 3
RA VEINS PA PV RV LA LV
PRESSURES HIGH PRESSURES NORMAL/MILDLY • PCWP • LVEDP
PC
O2
Group 3
• Up to 50% of people with COPD have PH
– Mostly mild
– 1 to 2% of people with COPD and PH have severe PH or “out of proportion” PH
– Presence of PH is associated with poorer survival in Group 3 patients
Group 3: Treatment
• Directed toward the underlying disease
– OSA: CPAP, etc
– COPD: Smoking cessation, inhaler therapy, lung reduction surgery, oxygen
– ILD: ?????, oxygen
• Lung transplantation for end stage disease
• Group 1 therapies generally not used
– Can increase V/Q mismatch, impair oxygenation
Group 4
• Chronic thromboembolic pulmonary hypertension (CTEPH)
– Due to nonresolving thromboemboli in pulmonary arterial tree causing obstruction
Aorta
Group 4: CTEPH
RA VEINS PA PV RV LA LV
PRESSURES HIGH PRESSURES LOW/NORMAL • PCWP • LVEDP
PC
Group 4
• Diagnosis
– V/Q Scan: Negative or low prob rules out CTEPH
– PE protocol chest CT does not rule out CTEPH
– PA angiography is gold standard
Group 4: Treatment
• Anticoagulation
• Pulmonary endarterectomy
• Prostacyclin analogs, PDE 5 inhibitors, and ERAs may be of use
– Some favorable data for hemodynamics
– Functional capacity and survival benefit unclear
Group 5
• Pulmonary hypertension with multiple etiologies
• Treat underlying cause
Aorta
Group 5
RA VEINS PA PV RV LA LV
PRESSURES HIGH PRESSURES HIGH
PC
O2
Diagnostic Approach
Diagnostic Approach
Diagnostic Approach
• Referral is often initiated because of an echo
– RVSP/PASP is estimated from the tricuspid valve regurgitant jet
• Occasionally, referral comes from a heart catheterization
– PAP elevated
• No referral; found upon file review
Diagnostic Approach
• History and Physical
– Age, past medical history, symptoms, sleep history, physical exam findings
• Suspect left sided disease
– Echo: diastolic function, valve function, ejection fraction
• Suspect lung disease: PFTs, V/Q scan, CT chest, sleep study
Suspect PAH?
• History of methamphetamine use, connective tissue disease, family history, HIV, cirrhosis
Clues from the Echo
• Group 2
– Low LVEF
– Enlarged LA
– Diastolic dysfunction • E/e’
• E:a’
• Pulmonary veins
– LV > RV
– LVH
• Group 1/3/4
– LVEF preserved, LV small and underfilled
– Septal flattening
– RV enlargement
Right Heart Catheterization
• “Table of Truth”
– Assess hemodynamics
• RA, PA, PCWP, CO (venous access)
• LVEDP if needed (arterial access)
– Maneuvers
• Exercise – if PA pressures low, to unmask PH
• Nipride – if PCWP is high to assess for “fixed” PH
• Pulmonary vasodilator trial – to assess for CCB sensitive PAH
Case 1
• 57 year old man
• Referred for PH eval
• Hx of AF (ablated)
• HTN on HCTZ only
• Rapidly progressing dyspnea on exertion
Case 1
• RA 12
• PA 49/21 (31)
• PCW 19
• TPG 12
• PVR ~ 3 WU
• GROUP 2 – Infiltrative cardiomyopathy from primary amyloidosois
Case 1
• He underwent heart transplantation last month at UCSF
Case 2
• 45 yo woman
• Presenting with months of progressive, severe dyspnea, edema, and presyncope
• Mother has PAH
Case 2
• RA 30
• PA 106/59 (76)
• LVEDP 10
• TPG 66
• PVR ~ 20 WU
• Neg V/Q scan, no parenchymal lung disease
• GROUP 1: PAH
Case 2
• Started on remodulin infusion during her initial admission
• Ambrisentan added later in her clinical course
PH and Right Ventricular Dysfunction
Pulmonary hypertension
Pressure overload
Adaptive RV hypertrophy
Maladaptive RV hypertrophy & fibrosis
RV dilation & systolic failure
Tricuspid regurgitation
Inter-ventricular septal shift
Left ventricular failure
RV Compensated
RV Decompensated
De Marco, T. Advances PAH. 2005;4:16-26.
Strategies to Prevent and Treat Right Heart Failure
• Reduce RV wall stress
– Reduce afterload • Pulmonary vasodilators (O2, CCB, ERA’s, prostanoids, nitric oxide)
– Reduce preload • Diuretic; mechanical volume removal
• Improve RV inotropy
– Chronically: digoxin (controversial)
– Acutely:
low dose IV dobutamine or dopamine
De Marco, T. Advances PAH. 2005;4:16-26.
Invasive Treatment of RV Failure
• Atrial septostomy
– Improve LV filling and systemic cardiac output
• Mechanical circulatory support
• Lung or heart/lung transplantation
– 1 yr survival: 70%; 5 yr survival: 50%
– Reserved for pts with poor QOL despite optimal therapy
Summary
• Therapeutic options for PH are predicated on understanding
the classification and ascertaining the etiology
– Most common etiologies of PH are chronic respiratory
diseases and left sided heart disease
• Right ventricular failure is often the mechanism of death for
severe PH patients
• PAH is a subset of PH for which we have compiled effective
evidence-based therapies
• Treatment of other forms of PH are dependent on the
underlying cause
THE END