Ngc_5460_1.doc

Complete Summary
GUIDELINE TITLE
Medical therapy for pulmonary arterial hypertension: ACCP evidence-based clinical practice guidelines. BIBLIOGRAPHIC SOURCE(S)
Badesch DB, Abman SH, Ahearn GS, Barst RJ, McCrory DC, Simonneau G, McLaughlin VV. Medical therapy for pulmonary arterial hypertension: ACCP evidence-based clinical practice guidelines. Chest 2004 Jul;126(1 Suppl):35S-62S. [191 references] GUIDELINE STATUS
This is the current release of the guideline. ** REGULATORY ALERT **
FDA WARNING/REGULATORY ALERT
Note from the National Guideline Clearinghouse: This guideline references a
drug(s) for which important revised regulatory and/or warning information has
been released.
• On July 8, 2005, the U.S. Food and Drug Administration (FDA) notified healthcare professionals of updated labeling for Cialis, Levitra and Viagra to reflect a small number of post-marketing reports of sudden vision loss, attributed to NAION (non arteritic ischemic optic neuropathy), a condition where blood flow is blocked to the optic nerve. FDA advises patients to stop taking these medicines, and call a doctor or healthcare provider right away if they experience sudden or decreased vision loss in one or both eyes. Patients taking or considering taking these products should inform their health care professionals if they have ever had severe loss of vision, which might reflect a prior episode of NAION. Such patients are at an increased risk of developing NAION again. At this time, it is not possible to determine whether these oral medicines for erectile dysfunction were the cause of the loss of eyesight or whether the problem is related to other factors such as high blood pressure or diabetes, or to a combination of these problems. See the for more information. • On Thursday, March 2, 2006, Actelion and the U.S. Food and Drug Administration (FDA) notified healthcare professionals of changes to the Tracleer (bosentan) prescribing information based on cases of hepatotoxity reported. Tracleer is indicated for the treatment of pulmonary arterial hypertension. The notification underscored the need to continue monthly liver function monitoring for the duration of Tracleer treatment and the need to adhere to the recommended dosage adjustment and monitoring guidelines described in the product labeling. See the COMPLETE SUMMARY CONTENT
** REGULATORY ALERT ** SCOPE METHODOLOGY - including Rating Scheme and Cost Analysis RECOMMENDATIONS EVIDENCE SUPPORTING THE RECOMMENDATIONS BENEFITS/HARMS OF IMPLEMENTING THE GUIDELINE RECOMMENDATIONS CONTRAINDICATIONS QUALIFYING STATEMENTS IMPLEMENTATION OF THE GUIDELINE INSTITUTE OF MEDICINE (IOM) NATIONAL HEALTHCARE QUALITY REPORT CATEGORIES IDENTIFYING INFORMATION AND AVAILABILITY DISCLAIMER DISEASE/CONDITION(S)
GUIDELINE CATEGORY
CLINICAL SPECIALTY
Cardiology Internal Medicine Pediatrics Pulmonary Medicine Rheumatology INTENDED USERS
GUIDELINE OBJECTIVE(S)
To provide appropriate evidence-based treatment recommendations for physicians involved in the care of patients with pulmonary arterial hypertension TARGET POPULATION
Adults and children with pulmonary arterial hypertension INTERVENTIONS AND PRACTICES CONSIDERED
Treatment
1. Acute vasoreactivity testing using short-acting agents, such as intravenous epoprostenol or adenosine or inhaled nitric oxide • Oral calcium channel blockers (e.g., nifedipine, diltiazem, amlodipine) • Enrollment in clinical trials as appropriate • Endothelin-receptor antagonists (bosentan) 3. Special considerations for children, pregnant women, patients with portopulmonary hypertension, and patients with human immunodeficiency virus (HIV) infection (see "Major Recommendations" field). MAJOR OUTCOMES CONSIDERED
• Exercise capacity (e.g., median distance walked in 6 minutes) • Changes in cardiopulmonary hemodynamics • Borg dyspnea scores and dyspnea-fatigue ratings • Severity of Raynaud's phenomenon and digital ulcers • Changes in World Health Organization functional class METHODOLOGY
METHODS USED TO COLLECT/SELECT EVIDENCE
Hand-searches of Published Literature (Primary Sources) Hand-searches of Published Literature (Secondary Sources) Searches of Electronic Databases DESCRIPTION OF METHODS USED TO COLLECT/SELECT THE EVIDENCE
Note from National Guideline Clearinghouse (NGC): The Center for Clinical Health Policy Research at Duke University identified and evaluated evidence on this topic, working with the guideline development panel to formulate key questions suitable for systematic literature synthesis. Search Strategy
Computerized searches of the MEDLINE bibliographic database from 1992 to October 2002 were conducted. The developer searched using the term hypertension, pulmonary. The search was limited to articles concerning human subjects that were published in the English language and accompanied by an abstract. In addition, the developer searched the reference lists of included studies, practice guidelines, systematic reviews, and meta-analyses, and consulted with clinical experts to identify relevant studies missed by the search strategy or published before 1992. Study Selection
For the topic on treatment, the guideline developer selected studies of oxygen, diuretics, inotropic agents (digoxin), anticoagulants, calcium antagonists, angiotensin-converting enzyme inhibitors, prostanoids (e.g., epoprostenol, treprostinil, inhaled iloprost), L-arginine, endothelin-receptor antagonists (e.g., bosentan, sitaxsentan, ambrisentan), phosphodiesterase-5 inhibitors (sildenafil), nitric oxide (NO), and thromboxane inhibitors (e.g., terbogrel). The guideline developer considered studies conducted among patients with known or suspected idiopathic pulmonary arterial hypertension (IPAH) or pulmonary arterial hypertension (PAH) occurring in association with underlying collagen vascular disease, congenital heart disease, or chronic thromboembolic disease. The guideline developers excluded studies of pulmonary hypertension (PH) associated with chronic obstructive pulmonary disease (COPD) or other parenchymal lung disease, high-altitude PH, or cardiac disease (e.g., left-heart failure, valvular heart disease) except congenital heart disease. The summary evidence tables can be viewed on-. NUMBER OF SOURCE DOCUMENTS
METHODS USED TO ASSESS THE QUALITY AND STRENGTH OF THE
EVIDENCE

Expert Consensus Weighting According to a Rating Scheme (Scheme Given) RATING SCHEME FOR THE STRENGTH OF THE EVIDENCE
Quality of the Evidence
Good = evidence based on good randomized controlled trials or meta-analyses
Fair = evidence based on other controlled trials or randomized controlled trials
with minor flaws
Low = evidence based on nonrandomized, case-control, or other observational
studies
Expert opinion = evidence based on the consensus of the carefully selected
panel of experts in the topic field. There are no studies that meet the criteria for
inclusion in the literature review.
METHODS USED TO ANALYZE THE EVIDENCE
Review of Published Meta-Analyses Systematic Review with Evidence Tables DESCRIPTION OF THE METHODS USED TO ANALYZE THE EVIDENCE
METHODS USED TO FORMULATE THE RECOMMENDATIONS
DESCRIPTION OF METHODS USED TO FORMULATE THE
RECOMMENDATIONS

An international panel of 19 experts representing five medical specialties was assembled. Representatives from other medical and patient advocacy associations were also invited to join the panel (including the American College of Cardiology, American College of Rheumatology, and the Pulmonary Hypertension Association). These experts convened on several occasions, including the culminating panel conference in September 2003, in which they deliberated over the composition of the final recommendations and grading of the current state of the evidence, benefits to the patient, and the strength of the recommendations. Guideline development was led by an executive committee including the chair, the leader of the methodology support group, and the American College of Chest Physicians project manager, which supervised the guideline development process, methodologic issues, panel composition, structure of the final document, and activities of the writing committees. Each writing committee, led by a group leader who served as primary author and editor of that chapter, conferred with the methodology team on inclusion/exclusion criteria, relevant research questions, and important literature that was not readily identified. These individuals continue with their responsibilities to assist in the development of the implementation tools. When the evidence was insufficient for evidence-based recommendations, the panel used informal group consensus techniques to develop recommendations based on the expert opinion of the panel. With every member of the panel attending the final conference, the expert-based opinions are truly representative of geographically diverse and multispecialty inclusive practice patterns of the complete panel. RATING SCHEME FOR THE STRENGTH OF THE RECOMMENDATIONS
Strength of Recommendations
A = strong recommendation B = moderate recommendation C = weak recommendation D = negative recommendation I = no recommendation possible (inconclusive) E/A = strong recommendation based on expert opinion only E/B = moderate recommendation based on expert opinion only E/C = weak recommendation based on expert opinion only E/D = negative recommendation based on expert opinion only Net Benefit
Substantial Intermediate Small/weak None Conflicting Negative COST ANALYSIS
A formal cost analysis was not performed and published cost analyses were not reviewed. METHOD OF GUIDELINE VALIDATION
External Peer Review Internal Peer Review DESCRIPTION OF METHOD OF GUIDELINE VALIDATION
The writing groups and the executive committee of the panel extensively reviewed each chapter during the writing process. The final conference provided an opportunity for the entire panel to review the latest drafts. Following final revisions and one final review by the executive committee, each chapter of the guidelines was reviewed and approved by the American College of Chest Physicians (ACCP) Health and Science Policy Committee, the ACCP Pulmonary Vascular NetWork, and then by the ACCP Board of Regents. The guidelines have not been field tested. RECOMMENDATIONS
MAJOR RECOMMENDATIONS
Rating schemes for level of evidence, strength of recommendation, and net benefit follow the major recommendations. 1. Patients with idiopathic pulmonary arterial hypertension (IPAH) should undergo acute vasoreactivity testing using a short-acting agent such as
intravenous (IV) epoprostenol, adenosine, or inhaled nitric oxide (NO). Level
of evidence: fair; benefit: substantial; grade of recommendation: A
.
2. Patients with pulmonary arterial hypertension (PAH) associated with underlying processes, such as scleroderma or congenital heart disease, should
undergo acute vasoreactivity testing. Level of evidence: expert opinion;
benefit: small/weak; grade of recommendation: E/C
.
3. Patients with PAH should undergo vasoreactivity testing by a physician experienced in the management of pulmonary vascular disease. Level of
evidence: expert opinion; benefit: substantial; grade of
recommendation: E/A
.
4. Patients with IPAH, in the absence of right-heart failure, demonstrating a favorable acute response to vasodilator (defined as a fall in mean pulmonary
arterial pressure [mPAP] of at least 10 mm Hg to < 40 mm Hg, with an
increased or unchanged cardiac output [CO]), should be considered
candidates for a trial of therapy with an oral calcium-channel antagonist.
Level of evidence: low; benefit: substantial; grade of
recommendation: B
.
5. Patients with PAH associated with underlying processes such as scleroderma or congenital heart disease, in the absence of right-heart failure,
demonstrating a favorable acute response to vasodilator (defined as a fall in
mean pulmonary arterial pressure [mPAP] of at least 10 mm Hg to < 40 mm
Hg, with an increased or unchanged CO), should be considered candidates for
a trial of therapy with an oral calcium-channel antagonist. Level of
evidence: expert opinion; benefit: intermediate; grade of
recommendation: E/B
.
6. In patients with PAH, calcium-channel blockers (CCBs) should not be used empirically to treat pulmonary hypertension (PH) in the absence of
demonstrated acute vasoreactivity. Level of evidence: expert opinion;
benefit: substantial; grade of recommendation: E/A
.
7. Patients with IPAH should receive anticoagulation with warfarin. Level of
evidence: fair; benefit: intermediate; grade of recommendation: B.
8. In patients with PAH occurring in association with other underlying processes, such as scleroderma or congenital heart disease, anticoagulation should be
considered. Level of evidence: expert opinion; benefit: small/weak;
recommendation: E/C
.
9. In patients with PAH, supplemental oxygen should be used as necessary to maintain oxygen saturations at >90% at all times. Level of evidence:
expert opinion; benefit: substantial; recommendation: E/A
.
10. Patients with PAH in functional class II who are not candidates for, or who have failed, CCB therapy may benefit from treatment. However, limited data
are available, and no specific drug can be recommended. Enrollment in clinical
trials is encouraged. Level of evidence: expert opinion; benefit:
intermediate; grade of recommendation: E/B
.
11. Patients with PAH in functional class III who are not candidates for, or who have failed, CCB therapy are candidates for long-term therapy with: a. Endothelin-receptor antagonists (bosentan). Level of evidence:
good; benefit: substantial; grade of recommendation: A.
b. IV epoprostenol. Level of evidence: good; benefit: substantial;
grade of recommendation: A.
c. Subcutaneous treprostinil. Level of evidence: fair; benefit:
intermediate; grade of recommendation: B.
d. Inhaled iloprost. Level of evidence: fair; benefit: intermediate;
grade of recommendation: B.
e. Beraprost. Level of evidence: good; benefit: conflicting; grade of
recommendation: I.
12. Patients with PAH in functional class IV who are not candidates for, or who have failed, CCB therapy are candidates for long-term therapy with IV
epoprostenol (treatment of choice). Level of evidence: good; benefit:
substantial; grade of recommendation: A
.
13. Other treatments available for patients with PAH and functional class IV a. Endothelin-receptor antagonists (bosentan). Level of evidence: fair;
benefit: intermediate; grade of recommendation: B.
b. Subcutaneous treprostinil. Level of evidence: fair; benefit:
intermediate; grade of recommendation: B.
c. Inhaled iloprost. Level of evidence: low; benefit: small; grade of
recommendation: C.
14. In patients with PAH who have failed or are not candidates for other available therapy, treatment with sildenafil should be considered. Level of evidence:
low; benefit: intermediate; grade of recommendation: C
.
15. In children with PAH, the recommendations for medical therapy (other than anticoagulation) in adults also apply. Quality of evidence: low; net
benefit: substantial; strength of recommendation: B
.
a. with right-heart failure or with a hypercoagulable state should receive anticoagulation with warfarin. Level of evidence: expert opinion;
net benefit: intermediate; strength of recommendation: E/B
.
b. without right-heart failure or a hypercoagulable state may receive anticoagulation with warfarin; for children <5 years of age, lower
target international normalized ratios (INRs) are recommended. Level
of evidence: expert opinion; net benefit: small/weak; strength
of recommendation: E/C
.
17. In patients with PAH, pregnancy should be avoided, or termination recommended. Level of evidence: good; benefit: substantial; grade of
recommendation: A
.
Definitions
Quality of the Evidence
Good = evidence based on good randomized controlled trials or meta-analyses
Fair = evidence based on other controlled trials or randomized controlled trials
with minor flaws
Low = evidence based on nonrandomized, case-control, or other observational
studies
Expert opinion = evidence based on the consensus of the carefully selected
panel of experts in the topic field. There are no studies that meet the criteria for
inclusion in the literature review.
Strength of Recommendations
A = strong recommendation B = moderate recommendation C = weak recommendation D = negative recommendation I = no recommendation possible (inconclusive) E/A = strong recommendation based on expert opinion only E/B = moderate recommendation based on expert opinion only E/C = weak recommendation based on expert opinion only E/D = negative recommendation based on expert opinion only Net Benefit
Substantial Intermediate Small/weak None Conflicting Negative CLINICAL ALGORITHM(S)
A clinical algorithm is provided in the original guideline document for therapy of pulmonary arterial hypertension. EVIDENCE SUPPORTING THE RECOMMENDATIONS
TYPE OF EVIDENCE SUPPORTING THE RECOMMENDATIONS
The type of supporting evidence is identified and graded for each recommendation (see "Major Recommendations"). BENEFITS/HARMS OF IMPLEMENTING THE GUIDELINE RECOMMENDATIONS
POTENTIAL BENEFITS
• Appropriate treatment of pulmonary arterial hypertension • Improved exercise capacity, quality of life, and survival in patients with POTENTIAL HARMS
• Risks of adverse effects, including death, during vasoreactivity testing • Risk of gastrointestinal bleeding with anticoagulants • Rapid and excessive diuresis may lead to systemic hypotension, renal • Epoprostenol therapy is complicated by the need for continuous intravenous infusion. Due to the long duration of therapy and the ongoing risk of catheter-associated infection, tunneled central venous catheters are generally preferred. Common side effects of epoprostenol therapy include headache, flushing, jaw pain with initial mastication, diarrhea, nausea, a blotchy erythematous rash, and musculoskeletal aches and pain (predominantly involving the legs and feet). These tend to be dose dependent and often respond to a cautious reduction in dose. Severe side effects can occur with overdosage of the drug. Acutely, overdosage can lead to systemic hypotension. Long-term overdosage can lead to the development of a hyperdynamic state and high-output cardiac failure. Abrupt or inadvertent interruption of the epoprostenol infusion should be avoided, as this may, in some patients, lead to a rebound worsening of their pulmonary hypertension with symptomatic deterioration and perhaps even death. • The nemesis of subcutaneous treprostinil has been pain and erythema at the • Overall, inhaled iloprost is well tolerated; in one placebo-controlled study, cough, flushing, and headache occurred more frequently in the iloprost group than in the placebo group. These adverse events were mild and mostly transient. Syncope occurred with similar frequency in the two groups, but was more frequently considered to be serious in the iloprost group, although this adverse effect was not associated with clinical deterioration. • There are several notable potential toxicities associated with the use of bosentan. Due to the risk of potential hepatic toxicity, the U.S. Food and Drug Administration requires that liver function tests be performed at least monthly in patients receiving this drug. Bosentan use may also be associated with the development of anemia, which seems typically to be mild. The hemoglobin/hematocrit should be checked regularly. Due to the potential teratogenic effects of bosentan, careful attention must be paid to the use of adequate contraception in women of childbearing age. It is important to note that bosentan may decrease the efficacy of hormonal contraceptive techniques, and for this reason they should not be used alone. Rather, it is suggested that some other form of contraception be included, such as the use of double-barrier techniques (condom and diaphragm) with a spermicide. Regular pregnancy testing is recommended in women of childbearing age. There is concern that the endothelin antagonists as a class may be capable of causing testicular atrophy and male infertility. Younger men who may consider conceiving should be counseled regarding this possibility prior to taking these drugs. • Sildenafil may cause headache and nausea. CONTRAINDICATIONS
CONTRAINDICATIONS
In human immunodeficiency virus (HIV)-associated pulmonary arterial hypertension, oral anticoagulation is often contraindicated because of frequent hemostasis abnormalities and potential drug interactions between HIV medications and warfarin. QUALIFYING STATEMENTS
QUALIFYING STATEMENTS
• The information provided in the guideline should be used in conjunction with clinical judgment. Although the guideline provides recommendations that are based on evidence from studies involving various populations, the recommendations may not apply to every individual patient. It is important for the physician to take into consideration the role of patient preferences and the availability of local resources. • The American College of Chest Physicians (ACCP) is sensitive to concerns that nationally and/or internationally developed guidelines are not always applicable in local settings. Further, guideline recommendations are just that, recommendations not dictates. In treating patients, individual circumstances, preferences, and resources do play a role in the course of treatment at every decision level. Although the science behind evidence-based medicine is rigorous, there are always exceptions. The recommendations are intended to guide healthcare decisions. These recommendations can be adapted to be applicable at various levels. IMPLEMENTATION OF THE GUIDELINE
DESCRIPTION OF IMPLEMENTATION STRATEGY
Implementation tools are being developed, including a quick reference guide in print and personal digital assistant format, and educational slide presentations for physicians and other health-care practitioners. IMPLEMENTATION TOOLS
For information about availability, see the "Availability of Companion Documents" and "Patient INSTITUTE OF MEDICINE (IOM) NATIONAL HEALTHCARE QUALITY REPORT
CATEGORIES
IOM CARE NEED
IOM DOMAIN
IDENTIFYING INFORMATION AND AVAILABILITY
BIBLIOGRAPHIC SOURCE(S)
Badesch DB, Abman SH, Ahearn GS, Barst RJ, McCrory DC, Simonneau G, McLaughlin VV. Medical therapy for pulmonary arterial hypertension: ACCP evidence-based clinical practice guidelines. Chest 2004 Jul;126(1 Suppl):35S-62S. [191 references] PubMed ADAPTATION
Not applicable: The guideline was not adapted from another source. DATE RELEASED
GUIDELINE DEVELOPER(S)
American College of Chest Physicians - Medical Specialty Society SOURCE(S) OF FUNDING
Funding for both the evidence reviews and guideline development was provided through an unrestricted educational grant from GlaxoSmithKline, Texas Biotechnology Corporation, and Actelion Pharmaceuticals US. Representatives from these companies were not granted right of review, nor were they allowed participation in any portion of the guideline development. GUIDELINE COMMITTEE
American College of Chest Physicians (ACCP) Expert Panel on Pulmonary Artery Hypertension COMPOSITION OF GROUP THAT AUTHORED THE GUIDELINE
Primary Authors: David B. Badesch, MD, FCCP, University of Colorado Health Sciences Center, Denver, CO; Steve H. Abman, MD, Children´s Hospital, Denver, CO; Gregory S. Ahearn, MD, Duke University Medical Center, Durham, NC; Robyn J. Barst, MD, Columbia Presbyterian Medical Center, New York, NY; Douglas C. McCrory, MD, MHSc, Duke University Medical Center, Durham, NC; Gerald Simonneau, MD, Hospital Antoine Beclere, Clamart, France; Vallerie V. McLaughlin, MD, FCCP, Rush Presbyterian St. Lukes Hospital, Chicago, IL FINANCIAL DISCLOSURES/CONFLICTS OF INTEREST
The following participants have disclosed information regarding potential or real conflicts of interest and commitment: Steven H. Abman, MD: scientific advisory board for INO Therapeutics; consultant for Pfizer. Charles W. Atwood, Jr., MD, FCCP: research support from Respironics, Inc. David B. Badesch, MD, FCCP: consultant or Speaker's Bureau for Glaxo Wellcome/GlaxoSmithKline, Actelion, InterMune, Encysive, Myogen, Astra-Merck, Astra-Zeneca, Exhale Therapeutics/CoTherix, Forrest Labs, INO Therapeutics, Berlex; research support from Glaxo Wellcome/GlaxoSmithKline, United Therapeutics, Boehringer Ingelheim, Actelion, Encysive, ICOS/Texas Biotechnologies/Encysive, Myogen, INO Therapeutics, Scleroderma Foundation, National Institutes of Health, National Heart, Lung, and Blood Institute, United Therapeutics, Pfizer, American Lung Association. Robyn J. Barst, MD: consultant and research support from Actelion, Encysive, Exhale Therapeutics, INO, Myogen, United Therapeutics, Pfizer GlaxoSmithKline; unrestricted education grants from GlaxoSmithKline, Encysive, Actelion. Richard N. Channick, MD, FCCP: research support from Actelion, Pfizer, Myogen, United Therapeutics; consultant and Speaker's Bureau for Actelion. Ramona L. Doyle, MD, FCCP: Speaker's Bureau for Actelion; clinical research for Actelion, Myogen, United Therapeutics. David D. Gutterman, MD, FCCP: stock options with Johnson & Johnson; relative who is a Vice-President at GlaxoSmithKline. James E. Loyd, MD, FCCP: relationships with GlaxoSmithKline, United Therapeutics, Actelion, ICOS/Texas Biotechnology, Westat, PRA International, Pfizer, Exhale Therapeutics. Michael D. McGoon, MD: past research support from Glaxo Wellcome, United Therapeutics, Actelion; research support from Texas Biotech/Encysive, Myogen, Pfizer, Medtronic. Vallerie V. McLaughlin, MD, FCCP: consultant for Actelion, United Therapeutics, Exhale Therapeutics; Speaker's Bureau for Actelion; research funding from Actelion, United Therapeutics, Pfizer, Encysive/Texas Biotechnologies, Glaxo Wellcome, Exhale Therapeutics, Myogen. Stuart Rich, MD: research funding from Actelion, Pfizer, United Therapeutics, Encysive, Myogen; consultant for Actelion, Pfizer, United Therapeutics, GlaxoSmithKline. Lewis J. Rubin, MD, FCCP: consultant for Actelion, Myogen, Schering, Exhale Therapeutics, United Therapeutics, Pfizer, Celgene; investigator for Actelion, Myogen, Exhale, Pfizer, Celgene; no stock holdings or other ownerships or positions. Gerald Simonneau, MD: consultant and investigator for Glaxo Wellcome, Pfizer, Actelion, Schering, Myogen, United Therapeutics. Virginia D. Steen, MD: relationships with Arthritis Foundation, Scleroderma Foundation, Actelion. Fredrick M. Wigley, MD: research funding from Biogen, Pfizer, Actelion; consultant to Genzyme. GUIDELINE STATUS
This is the current release of the guideline. GUIDELINE AVAILABILITY
Electronic copies: Available to subscribers of Chest - The Cardiopulmonary and Critical Care Journal. Print copies: Available from the American College of Chest Physicians, Products and Registration Division, 3300 Dundee Road, Northbrook IL 60062-2348. AVAILABILITY OF COMPANION DOCUMENTS
• Rubin, LJ. Diagnosis and management of pulmonary arterial hypertension: ACCP evidence-based clinical practice guidelines. Introduction. Chest 2004 Jul;126(1 Suppl):7S-10S. • Rubin LJ. Diagnosis and management of pulmonary arterial hypertension: ACCP evidence-based clinical practice guidelines. Executive summary. Chest 2004 Jul;126(1 Suppl):4S-6S. • McCrory DC, Lewis SZ. Methodology and grading for pulmonary hypertension evidence review and guideline development. Chest 2004 Jul;126(1 Suppl):11S-13S. - The Cardiopulmonary and Critical Care Journal. Print copies: Available from the American College of Chest Physicians, Products and Registration Division, 3300 Dundee Road, Northbrook IL 60062-2348. PATIENT RESOURCES
NGC STATUS
This NGC summary was completed by ECRI on August 27, 2004. This summary was updated by ECRI on July 15, 2005 following the FDA advisory on Cialis, Levitra, and Viagra. This summary was updated by ECRI on March 8, 2006 following the FDA advisory on Tracleer (bosentan). COPYRIGHT STATEMENT
This NGC summary is based on the original guideline, which is subject to the guideline developer's copyright restrictions. DISCLAIMER
NGC DISCLAIMER
The National Guideline Clearinghouse™ (NGC) does not develop, produce, approve, or endorse the guidelines represented on this site. All guidelines summarized by NGC and hosted on our site are produced under the auspices of medical specialty societies, relevant professional associations, public or private organizations, other government agencies, health care organizations or plans, and similar entities. Guidelines represented on the NGC Web site are submitted by guideline developers, and are screened solely to determine that they meet the NGC Inclusion Criteria which may be found at . NGC, AHRQ, and its contractor ECRI make no warranties concerning the content or clinical efficacy or effectiveness of the clinical practice guidelines and related materials represented on this site. Moreover, the views and opinions of developers or authors of guidelines represented on this site do not necessarily state or reflect those of NGC, AHRQ, or its contractor ECRI, and inclusion or hosting of guidelines in NGC may not be used for advertising or commercial endorsement purposes. Readers with questions regarding guideline content are directed to contact the guideline developer. 1998-2006 National Guideline Clearinghouse

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