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PH . Pulmonary Hypertension. PH. Pulmonary hypertension is an abnormal elevation of the pulmonary artery pressure (PAP) and the pulmonary vascular resistance (PVR) resulting in right ventricular (RV) failure and premature death. PH.
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PH Pulmonary Hypertension
PH • Pulmonary hypertension is an abnormal elevation of the pulmonary artery pressure (PAP) and the pulmonary vascular resistance (PVR) resulting in right ventricular (RV) failure and premature death.
PH • PH used to be recognized as a disease with a grim prognosis. • Over the last decade, new medications have been developed to treat PH. These medications have improved both the quantity and quality of life for patients with PH. • Since we can now treat PH, we need to be more aware of pursuing it as a diagnosis.
PH • What is PH? • mPAP > 25 mmHg at rest • mPAP > 30 mmHg with activity • What are the most common symptoms? • Worsening SOB • Chest pain • Fatigue • Palpitations • Lower extremity edema • Syncope
PH • WHO classification • Group I- PAH • Group II- PVH, PH secondary to LV failure • Group III- PH associated with lung disease or hypoxia • Group IV- PH secondary to chronic thromboembolic disease • Group V- miscellaneous - HIV infection, drug exposure
PH • Group I - PAH • Replaces primary pulmonary hypertension • No known underlying risk factors • Usually seen in women of childbearing age • Rare - 2 to 3 per million per year • Genetic predisposition
PH • Facts: • Group II – PVH – most common, PCWP >15 mmHg • Group III - lung disease • COPD – mild PH seen in up to 50% of pts • OSA – usually associated with mild PH • OHS – more commonly seen with cor pulmonale • Group IV - chronic PTED – up to 4%
PH • Pathophysiology • Pulmonary endothelial cell dysfunction or injury causing vascular changes • Intimal proliferation • Hypertrophy • Proliferation of smooth muscle cells • Vasoconstriction • In situ thrombosis
PH • Making the diagnosis • High index of suspicion • PE – early, Nl; increased P2, TR, heptojugular reflux • CXR, CT chest – enlarged PA’s • EKG – V1, tall R wave and short S wave (RV hypertrophy); II, p-pulmonale (RAE) • Transthoracic ECHO – evaluate LV function, estimate RVSP and PAP’S • Right heart catheterization – measure PAP’s and PCWP
PH • Further Evaluation • Lab – ANA, RF, HIV, CBC, LFT’s, TFT’s • PFT’s – OLD or ILD; decrease in DLCO • Overnight oximetry – desaturation is seen in 70% of pts • PSG • V/Q scan, CT chest, pulmonary angiography
PH • Treatment – General measures • O2 – keep sats > 90% • Avoid vasoconstricting decongestants, B blockers, stimulants and anorexigens • Do low level aerobic exercise • Follow a low sodium (<2400 mg) diet • Avoid pregnancy • Anticoagulation • Diuretics • Digoxin?
PH • Treatment – Medications • Prostanoids – epoprostenol, treprostinil, and iloprost • ERA’s (endothelin receptor antagonists) – bosentan and ambrisentan • Phosphodiesterase-5 (PDE-5) inhibitors - sildenafil
PH • Prostanoids – prostacyclin analogues • Prostacyclin is a potent vasodilator and antiplatelet agent • Deficient in pts with PH • Improve symptoms • Improve hemodynamics • Overdosage causes hypotension and hyperdynamic state with high-output cardiac failure
PH • Prostanoids cont. • Epoprostenol – only drug with proven survival benefit; 6 minute half-life • Must be kept cold during storage and administration • Continuous IV infusion thru tunneled catheter • Treprostinil – not shown to improve survival; 3 hour half life • Continuous SQ infusion • Iloprost – inhaled route of administration; 6-9 times a day (Q2 hours while awake)
PH • ERA’s – improve sx and functional class; antagonizes vasoconstriction and smooth muscle proliferation • Bosentan (Tracleer) – oral, BID • LFT’s • Anemia • Fluid retention • HA’s • Ambrisentan (Letairis) – oral, QD • Fluid retention
PH • PDE-5’s – improve sx and functional class; augments vasodilatory effects of nitric oxide • Sildenafil (Revatio) – oral, TID • HA’s • Flu-like sx • Flushing • Epistaxis
PH • NYHA classification of functional status of pts with PH • I – no limitations in nl physical activity • II – mild limitation, no sx at rest, worsening sx with exertion • III – marked limitation, no sx at rest, worsening sx with light activity • IV – sx at rest, unable to do any activity, signs of RV failure at rest
PH • Treatment by Classification • I – monitor • II – oral sildenafil (Revatio) • III – oral sildenafil or bosentan (Tracleer) and inhaled or intravenous prostanoids • IV – intravenous prostanoids
PH • Goals of Treatment • Improvement to class I or II • Improvement in the 6 MWDT to 380 m or better • Max SBP with exercise of 120 mm Hg or greater • Decrease in BNP to < 180 pg/ml
PH • Other treatments • Surgery • Atrial septostomy – decrease right-sided pressures, may worsen hypoxia • Lung transplant – curative, post op median survival 5 years • Pulmonary thromboendarterectomy – curative for PH from chronic PTED, tx of choice in appropriate candidates
PH • Upcoming therapies • Treprostinil – infusion and inhaled available now, working on oral formulation • Sitaxsentan – approved in Europe, application is pending with FDA • Tadalafil (Cialis) – longer half-life and greater selectivity and potency than sildenafil; in trials now
PH • Prognosis • 1980s – grim, medial survival of 2.8 years from time of diagnosis in untreated pts • Current – newer medications have greatly improved the outlook for pts with PH • Poor prognostic indicators – low 6 MWDT; pericardial effusion, RV dysfunction, and RAE on ECHO; increased mRAP (the most powerful hemodynamic predictor) and decreased cardiac index on RHC; and elevated BNP
