Pulmonary hypertension resident survival guide

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: , Vidit Bhargava, M.B.B.S [2]

Definition

Pulmonary hypertension (PH) is defined by mean pulmonary artery pressure > 25, pulmonary capillary wedge pressure (PCWP), left atrial pressure, or left ventricular end diastolic pressure (LVEDP) ≤ 15 mm Hg; and a pulmonary vascular resistance (PVR) > than 3 Wood units. ^[1]

Causes

Life Threatening Causes

Life-threatening causes include conditions which may result in death or permanent disability within 24 hours if left untreated.

Pulmonary embolism

Common Causes

Management

Diagnosis

Characterize the symptoms:
❑ Progressive dyspnea
❑ Exertional dizziness and syncope
❑ Edema of the extremities
❑ Angina
❑ Palpitations

Examine the patient:

Physical signs that reflect severity of PH:
❑ Loud pulmonary second heart sound (P2)
❑ Systolic murmur suggestive of tricuspid regurgitation
❑ Raised jugular venous pressure (JVP)
❑ Early systolic click
❑ Left parasternal heave
❑ Right ventricular S₄

Physical signs suggestive of moderate to severe PH:
❑ Holosystolic murmur that increases with inspiration
❑ Increased jugular v waves
❑ Pulsatile liver
❑ Diastolic murmur
❑ Hepatojugular reflux

Physical signs suggestive of advanced PH with right ventricular failure:
❑ Right ventricular S₃
❑ Distension of jugular veins
❑ Hepatomegaly
❑ Peripheral edema
❑ Ascites
❑ Hypotension

Physical signs suggestive of possible underlying causes:
❑ Central cyanosis → Abnormal V/Q, shunt
❑ Clubbing → Congenital heart disease
❑ Cardiac auscultatory findings → Congenital or acquired heart disease
❑ Rales, decreased breath sounds, dullness → Pulmonary congestion
❑ Fine rales, excessive muscle use, wheezing, protracted respiration, cough → Pulmonary parenchymal disease
❑ Obesity, kyphoscoliosis, enlarged tonsils → Disordered ventilation
❑ Sclerodactyly, arthritis, telengiectasia, Raynaud phenomenon, rash → Connective tissue disorder
❑ Peripheral venous insufficiency → Possible venous thrombosis
❑ Venous stasis ulcers → Possible sickle cell disease
❑ Pulmonary vascular bruits → Chronic thromboembolic PH
❑ Splenomegaly, spider angiomata, palmar erythema, icterus, caput medusae → portal hypertension

Consider alternative diagnosis:
❑ Left sided heart failure
❑ Coronary artery disease
❑ Liver disease
❑ Budd-Chiari syndrome

Order tests:
❑ Chest X-ray
❑ EKG
❑ Echocardiogram
Right heart catherization

Treatment

❑ Anticoagulation +/-
❑ Diuretics +/-
❑ Oxygen therapy +/-
❑ Digoxin

Acute vasoreactivity testing

❑ Epoprostenol IV 2ng/Kg/min every 10 to 15 min, OR
❑ Adenosine IV 50 mcg/Kg/min every 2 min, OR

❑ Nitric oxide (inhaled)

Positive

Negative

Oral calcium channel blocker (CCB)

Lower risk

Higher risk

❑ Follow closely for efficacy and safety
❑ Sustained response?

❑ Oral endothelin receptor antagonists: Bostenan 125 mg BD, OR
Oral phospodiesterase-5 inhibitors: Sildenafil 20 mg TDS
❑ IV epoprostenol (started at 2 ng/Kg/min - 25-40 ng/kg/min), OR
IV treprostinil (83 ng/Kg/min)
❑ Iloprost (inhaled)
❑ Treprostinil (SC)

❑ IV epoprostenol (started at 2 ng/Kg/min - 25-40 ng/kg/min), OR
IV treprostinil (83 ng/Kg/min)
❑ Iloprost (inhaled)
❑ Oral endothelin receptor antagonists: Bostenan 125 mg BD, OR
Oral phospodiesterase-5 inhibitors: Sildenafil 20 mg TDS
❑ Treprostinil (SC)

Yes

❑ Reassess

Response to the monotherapy

❑ No evidence of heart failure on physical exam
❑ Functional class I/II
❑ 6 minute walk distance >400 m
❑ Normal RV size on echocardiogram
❑ Normal right atrial pressure and cardiac index

❑ Near normal or stable BNP

Unstable clinical course

❑ Signs of heart failure
❑ Functional class IV
❑ 6 minute walk distance <400 m
❑ RV enlargement on echocardiogram
❑ High right atrial pressure and low cardiac index

❑ Elevated/increasing BNP

Continue CCB

In case of absence of response to initial monotherapy:
❑ Consider combo-therapy

In case of progress despite optimal medical treatment:
❑ Investigational protocols, OR
❑ Atrial septostomy, OR
❑ Lung transplant

The algorithm is based on Expert consensus document on pulmonary hypertension published by ACCF/AHA in 2009.^[2]

Follow Up Testing

Shown below is a table depicting the follow up testing after etiology for pulmonary hypertension is established.

Condition	Follow up testing
BMPR2 mutation	❑ Yearly echocardiogram ❑ Right heart catheterization if evidence of PH
1st degree relative of patient with BMPR2 mutation or with 2 or more relatives with PH	❑ Genetic counseling for BMPR2 testing ❑ Proceed as above if positive
Systemic sclerosis	❑ Yearly echocardiogram ❑ Right heart catheterization if evidence of PH
HIV infection	❑ Do echocardiogram if signs & symptoms are suggestive of PH ❑ Right heart catheterization if evidence of PH on echocardiography
Portal hypertension	❑ If considering liver transplant perform echocardiogram ❑ Right heart catheterization if evidence of PH
CHD with shunt	❑ Echocardiogram and right heart catheterization at the time of diagnosis ❑ Repair any significant defect
Recent acute pulmonary embolism	❑ If symptomatic 3 months after event, perform ventilation perfusion scintigraphy ❑ Do a pulmonary angiogram if positive
Prior fenfluramine use (appetite suppressant)	❑ Echocardiogram only if symptomatic
Sickle cell disease	❑ Yearly echocardiogram ❑ Right heart catheterization if evidence of PH

Do's

The diagnosis of pulmonary hypertension requires confirmation with a right heart catheterization.
Objective assessment of treatment measures includes:

Exercise capacity.
Hemodynamics.
Survival.

Epoprostenol is the only therapy that has been shown to prolong survival in patients with pulmonary hypertension.
Monitor liver function tests monthly in patients being treated with endothelin receptor antagonists.
Patients presenting with advanced symptoms, right heart failure, advanced hemodynamics and those on parenteral or combination therapy must be seen every 3 months.

Don'ts

Do not perform vasospastic testing for those with overt heart failure or hemodynamic instability.

References

↑ Kiely, DG.; Elliot, CA.; Sabroe, I.; Condliffe, R. (2013). "Pulmonary hypertension: diagnosis and management". BMJ. 346: f2028. PMID 23592451.
↑ McLaughlin VV, Archer SL, Badesch DB, Barst RJ, Farber HW, Lindner JR; et al. (2009). "ACCF/AHA 2009 expert consensus document on pulmonary hypertension: a report of the American College of Cardiology Foundation Task Force on Expert Consensus Documents and the American Heart Association: developed in collaboration with the American College of Chest Physicians, American Thoracic Society, Inc., and the Pulmonary Hypertension Association". Circulation. 119 (16): 2250–94. doi:10.1161/CIRCULATIONAHA.109.192230. PMID 19332472.

[Kiely-2013-1] Kiely, DG.; Elliot, CA.; Sabroe, I.; Condliffe, R. (2013). "Pulmonary hypertension: diagnosis and management". BMJ. 346: f2028. PMID 23592451.

[pmid19332472-2] McLaughlin VV, Archer SL, Badesch DB, Barst RJ, Farber HW, Lindner JR; et al. (2009). "ACCF/AHA 2009 expert consensus document on pulmonary hypertension: a report of the American College of Cardiology Foundation Task Force on Expert Consensus Documents and the American Heart Association: developed in collaboration with the American College of Chest Physicians, American Thoracic Society, Inc., and the Pulmonary Hypertension Association". Circulation. 119 (16): 2250–94. doi:10.1161/CIRCULATIONAHA.109.192230. PMID 19332472.

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