Restrictive Cardiomyopathy

by promotiondept | Feb 11, 2019 | Uncategorized | 0 comments

All Premium Themes And WEBSITE Utilities Tools You Ever Need! Greatest 100% Free Bonuses With Any Purchase.

Greatest CYBER MONDAY SALES with Bonuses are offered to following date: Get Started For Free!
Purchase Any Product Today! Premium Bonuses More Than $10,997 Will Be Emailed To You To Keep Even Just For Trying It Out.
Click Here To See Greatest Bonuses

and Try Out Any Today!

Here’s the deal.. if you buy any product(s) Linked from this sitewww.Knowledge-Easy.com including Clickbank products, as long as not Google’s product ads, I am gonna Send ALL to you absolutely FREE!. That’s right, you WILL OWN ALL THE PRODUCTS, for Now, just follow these instructions:

1. Order the product(s) you want by click here and select the Top Product, Top Skill you like on this site ..

2. Automatically send you bonuses or simply send me your receipt to consultingadvantages@yahoo.com Or just Enter name and your email in the form at the Bonus Details.

3. I will validate your purchases. AND Send Themes, ALL 50 Greatests Plus The Ultimate Marketing Weapon & “WEBMASTER’S SURVIVAL KIT” to you include ALL Others are YOURS to keep even you return your purchase. No Questions Asked! High Classic Guaranteed for you! Download All Items At One Place.

That’s it !

*Also Unconditionally, NO RISK WHAT SO EVER with Any Product you buy this website,

60 Days Money Back Guarantee,

IF NOT HAPPY FOR ANY REASON, FUL REFUND, No Questions Asked!

Download Instantly in Hands Top Rated today!

Remember, you really have nothing to lose if the item you purchased is not right for you! Keep All The Bonuses.

Super Premium Bonuses Are Limited Time Only!

Day(s)

Hour(s)

Minute(s)

Second(s)

Get Paid To Use Facebook, Twitter and YouTube
Online Social Media Jobs Pay $25 - $50/Hour.
No Experience Required. Work At Home, $316/day!
View 1000s of companies hiring writers now!
Order Now!

MOST POPULAR

*****
Customer Support Chat Job: $25/hr
Chat On Twitter Job - $25/hr
Get Paid to chat with customers on
a business’s Twitter account.
Try Free Now!

Get Paid To Review Apps On Phone
Want to get paid $810 per week online?
Get Paid To Review Perfect Apps Weekly.
Order Now!

Look For REAL Online Job?
Get Paid To Write Articles $200/day
View 1000s of companies hiring writers now!
Try-Out Free Now!

How To Develop Your Skill For Great Success And Happiness Including Become CPA? | Additional special tips From Admin

Competence Progression is definitely the number 1 fundamental and main factor of gaining genuine success in most of procedures as you actually discovered in your culture in addition to in Throughout the world. And so fortunate enough to examine with everyone in the right after in regard to what effective Competence Improvement is; ways or what means we work to get dreams and sooner or later one is going to give good results with what the person likes to conduct all day intended for a whole daily life. Is it so wonderful if you are equipped to produce resourcefully and find victory in what exactly you thought, steered for, self-disciplined and previously worked very hard all day time and unquestionably you become a CPA, Attorney, an person of a big manufacturer or even a physician who can easily seriously bring excellent guide and principles to people, who many, any population and local community definitely popular and respected. I can's believe I can allow others to be finest competent level just who will add sizeable products and remedy valuations to society and communities in these days. How happy are you if you turn into one such as so with your personal name on the headline? I have arrived on the scene at SUCCESS and prevail over most of the really hard segments which is passing the CPA examinations to be CPA. Moreover, we will also protect what are the pitfalls, or other sorts of problems that can be on ones own strategy and the correct way I have in person experienced them and will indicate you the best way to cure them. | From Admin and Read More at Cont'.

Restrictive Cardiomyopathy

No Results

processing….

Restrictive cardiomyopathy (RCM) is a rare disease of the myocardium and is the least common of the three clinically recognized and described cardiomyopathies.^{[1, 2]}It is characterized by diastolic dysfunction with restrictive ventricular physiology, whereas systolic function often remains normal. Atrial enlargement occurs due to impaired ventricular filling during diastole, but the volume and wall thickness of the ventricles are usually normal. RCM accounts for approximately 5% of all cases of diagnosed cardiomyopathies.^[3]

Symptoms may include the following:

Search for extracardiac manifestations of a systemic disorder that may cause secondary restrictive cardiomyopathy (eg, hemochromatosis, amyloidosis, sarcoidosis, or scleroderma).

General examination findings:

Cardiovascular system examination findings:

Respiratory system examination findings:

See Clinical Presentation for more detail.

Establishing the diagnosis of RCM and excluding constrictive pericarditis are imperative. The workup in a patient with suspected restrictive cardiomyopathy may include the following:

See Workup for more detail.

RCM has no specific treatment. However, therapies directed at individual causes of RCM have been proven to be effective.

Pharmacologic therapy may include:

Other treatments:

See Treatment for more detail.

Restrictive cardiomyopathy (RCM) is a rare disease of the myocardium and is the least common of the three clinically recognized and described cardiomyopathies.^{[1, 2]} It is characterized by diastolic dysfunction with restrictive ventricular physiology, whereas systolic function often remains normal. Atrial enlargement occurs due to impaired ventricular filling during diastole, but the volume and wall thickness of the ventricles are usually normal. RCM accounts for approximately 5% of all cases of diagnosed cardiomyopathies.^[3]

RCM may be idiopathic or secondary to other diseases (ie, amyloidosis and endomyocardial disease with or without hypereosinophilia). The course of RCM varies, depending on the pathology and treatment. RCM has been found to be a significant cause of heart failure with preserved ejection fraction, although there is a high clinical overlap between RCM and other forms of heart failure.^[4]RCM therefore presents a diagnostic challenge, and multiple modalities are usually required to make a final diagnosis.

See the images below.

Restrictive cardiomyopathy (RCM) can be idiopathic or secondary to a heart muscle disease that manifests as restrictive physiology.^{[1, 5]}Both inherited and acquired forms of the disease exist and affect men and women equally. Increased stiffness of the myocardium causes ventricular pressures to rise precipitously with small increases in volume. Thus, accentuated filling occurs in early diastole and terminates abruptly at the end of the rapid filling phase. When pressure tracings are taken at this point, they show a characteristic diastolic “dip-and-plateau” or “square-root” pattern, both similar to constrictive pericarditis.^[6]

Patients typically have reduced compliance (increased diastolic stiffness), and the left ventricle cannot fill adequately at normal filling pressures. Reduced left ventricular filling volume leads to a reduced cardiac output. Early in the disease process, systolic function usually remains normal. Wall thickness may be increased in cases of infiltrative processes such as amyloidosis, but the increase is usually not as pronounced as that observed in hypertrophic cardiomyopathy.

As the disease progresses, a variable reduction in systolic function may develop with symptoms of reduced cardiac output, such as fatigue and lethargy, becoming evident. Increased filling pressures can manifest as pulmonary and systemic congestion. RCM affects both ventricles and therefore may cause signs and symptoms of both left-sided and right-sided heart failure. Some patients may have complete heart block as a consequence of fibrosis encasing the sinoatrial or the atrioventricular nodes.

RCM is one of the cardiomyopathies that is known to have a genetic cause, although only a few RCM-causing mutations have been described.^{[7, 8, 9]}The Heart Failure Society of America (HFSA) issued updated guidelines on the genetic evaluation of cardiomyopathy in 2010.^[10]

Based on pathology findings, RCM can further be classified as obliterative (ie, thrombus-filled ventricles) or nonobliterative. Idiopathic (primary) RCM is nonobliterative, as progressive fibrosis of the myocardium occurs but no thrombus forms. This entity also is said to lack specific histopathologic changes.

Obliterative RCM is very rare. It may result from the end stage of the eosinophilic syndromes, in which an intracavitary thrombus fills the left ventricular apex and hampers the filling of the ventricles. The fibrosis of the endocardium may extend to involve the atrioventricular valves and cause regurgitation. Two forms of endomyocardial fibrosis (EMF) exist—an active inflammatory eosinophilia and chronic EMF.

Restrictive cardiomyopathy (RCM) may be caused by various local and systemic disorders; many of them are rare and unlikely to be observed in the United States.

According to World Health Organization (WHO) guidelines, the term “cardiomyopathy” refers to diseases of the myocardium that are idiopathic (ie, primary cardiomyopathies). However, secondary infiltrative myocardial diseases, which are actually cardiac manifestations of systemic diseases, often are grouped together with cardiomyopathies.^[11]

The etiologies of RCM may be grouped into broad categories as follows:

The specific pathophysiologies of the more common causes of RCM will be described in detail below.

Both genetic and sporadic cases of primary (idiopathic) RCM have been described. This is a rare condition that can present in children and adults,^[13]and males and females are affected equally. However, the prognosis appears to be worse in children than in adults. Genetic cases show autosomal dominant inheritance with incomplete penetrance. The mutation appears to occur in the genes encoding sarcomeric proteins, including troponin I, troponin T, alpha cardiac actin, and beta-myosin heavy chain.^[13]A history of familial RCM is reported in approximately 30% of RCM cases.^[3]

A subset of patients has heart muscle disease of unknown cause that is manifested by heart failure and restrictive hemodynamics, but without significant ventricular hypertrophy, endocardial thickening or fibrosis, associated eosinophilia, or other diagnostically distinct histopathologic changes.

Children require relatively high filling pressures for maintenance of systolic output, and the therapeutic margin between volume depletion (leading to low output) and volume overload (leading to congestive heart failure) is narrow. An observational study suggests that poor left ventricular function may be a hallmark for pediatric restrictive cardiomyopathy even in the presence of normal diastolic parameters.^[14]

In addition to the presenting symptoms of right- and left-side heart failure, as many as one third of patients with idiopathic RCM may present with thromboembolic complications. Pathologically, these patients have strikingly dilated atria, which may account for the increased cardiothoracic ratio on chest radiography. Echocardiography shows bilateral atrial enlargement with normal ventricular size but significant diffuse left ventricular hypertrophy, especially with amyloidosis. Histologic features include interstitial fibrosis, which is minimal in some patients and extensive in others.

Eosinophilic cardiomyopathy (Loeffler endocarditis) and EMF

EMF is the most common global cause of RCM, affecting an estimated 12 million people worldwide. This condition is observed in equatorial Africa and, less frequently, in tropical and subtropical Asia and South America.

Severe prolonged eosinophilia from any cause (eg, allergic, autoimmune, parasitic, leukemic, or idiopathic) can lead to eosinophilic infiltration of the myocardium. Eosinophilic cardiomyopathy, also known as Loeffler endocarditis, begins with an acute inflammatory phase characterized by fever and pancarditis. Left ventricular and right ventricular thrombus formation occurs in the intermediate phase and, after months to years, the final stage includes development of endocardial fibrosis. The intracytoplasmic granular content of activated eosinophils is believed to be responsible for the toxic damage to the heart.^[13]

EMF was originally believed to be the end stage of eosinophilic endomyocarditis. However, chronic EMF is currently considered a separate entity because it does not exhibit eosinophilia. EMF demonstrates pathology that is similar to that of Loeffler endocarditis.

Both EMF and Loeffler endocarditis are categorized as types of obliterative RCM. Intraventricular thrombus formation leads to obliteration of the ventricular cavity in the late stages. Echocardiography may show endomyocardial thickening, ventricular apical obliteration, and tethering of mitral and tricuspid leaflets.^[13]

The prognosis is poor for patients with diffuse involvement of the heart, but localized lesions involving the valves are amenable to surgical repair or removal and replacement.

Infiltrative cardiomyopathy

Infiltrative cardiomyopathies are characterized by deposition of abnormal substances (ie, amyloid proteins, noncaseating granulomas, iron) within the heart tissue. Infiltration causes the ventricular walls to stiffen, leading to diastolic dysfunction. Disease occurs in a wide variety of age groups and, given the systemic nature of the underlying disease, extracardiac manifestations are common. Restrictive physiology predominates in the early stages, causing conduction abnormalities and diastolic heart failure. Adverse remodeling may lead to systolic dysfunction and ventricular arrhythmias in advanced cases.^[15]

Confirmatory evidence of infiltrative cardiomyopathy is often obtained by endomyocardial biopsy, echocardiography, or cardiac magnetic resonance imaging (CMRI). Depending on the etiology and extent of involvement, medications, device therapy, and transplantation can be effective, although treatment is largely supportive in many cases.^[15]

Amyloidosis

Amyloidosis is the most common cause of RCM in the United States. Due to advancements in noninvasive diagnostic modalities, relatively recent studies have shown that there may be a higher prevalence of amyloidosis among elder patients with heart failure with preserved ejection fraction than previously recognized.^[4]

Amyloidosis is characterized by the multisystem deposition of proteins known as amyloid fibrils, and it typically presents as a systemic disorder, with infiltration of the liver, kidneys, bowel, nerves, skin, and tongue.^[13]Cardiac involvement is common and the major source of associated morbidity and mortality. The myocardial wall thickens and becomes firm, rubbery, and noncompliant as amyloid accumulates in tissues. These changes lead to abnormalities of contractility, conduction, and coronary blood flow. Interestingly, amyloid deposition in the bundle branches is rare. Biventricular diastolic dysfunction causes intracardiac pressures to rise, and it may progress to systolic dysfunction in advanced disease.^[15]The heart typically does not collapse when removed from the chest during autopsy.

Amyloidosis is classified into the following four major clinical types based on the composition of amyloid protein:

Primary or amyloid light-chain (AL): This is the most common form, often associated with multiple myeloma; prognosis is poor, with a median 1-year survival from diagnosis.

Secondary amyloidosis or amyloid A (AA): This type is secondary to chronic diseases, especially inflammatory conditions.

Senile amyloidosis or wild-type transthyretin (wt-TTR) amyloidosis: This form is seen in 25-36% of patients older than 80 years; it is caused by deposition of wt-TTR.^[16]The median survival is 6 years.

Familial amyloidosis or hereditary mutant TTR (m-TTR)/hereditary transthyretin-derived (ATTR) amyloidosis: This type is a systemic autosomal dominant disorder due to tissue deposition of various proteins. Cardiac involvement is rare.

The cardiac involvement in primary amyloidosis is most commonly associated with restrictive physiology.

In the early stages of the disease, typical restrictive hemodynamics may not be evident; however, in more advanced cases, typical restrictive hemodynamics are more likely. Restrictive diastolic dynamics strongly predict cardiac death in patients with amyloidosis. Studies have shown that patients with elevated cardiac biomarkers such as troponin (Tn) and B-type natriuretic peptide (BNP) have a worse prognosis.^[15]

On histologic examination, amyloid may deposit within any part of the heart, including the myocardium, vessels, endocardium, valves, epicardium, and parietal pericardium. The ventricular walls are typically thickened, sometimes with disproportionate septal thickening, and may mimic the appearance of hypertrophic cardiomyopathy. Atrial dilatation develops as a consequence of increased ventricular filling pressures and restrictive physiology.^[17]Involvement of the valves may create regurgitant lesions, but a hemodynamically and clinically significant degree of regurgitation is unusual.

Cardiac biopsy is needed to confirm the diagnosis if doubt remains after noninvasive tests. Classically, the deposition of insoluble fibrillary protein displays as apple-green birefringence under polarized light microscopy with Congo Red staining.^[13]

Classic two-dimensional echocardiography findings include an increased left ventricular and right ventricular wall thickness, normal or small left ventricular cavity size with preserved ejection fraction, and biatrial enlargement. Up to one third of patients can present with normal left ventricular wall size. Pericardial effusion and thickening of both valves and papillary muscles is common. A granular and speckled appearance of the ventricular myocardium is suggestive of amyloidosis, but it is no longer considered specific.^[15]

Other less common forms of infiltrative RCM include:

Treatment-induced RCM

Postirradiation fibrosis

Radiation-induced myocardial and endocardial fibrosis is a cause of noninfiltrative RCM. Fibrosis causes endothelial cell damage and subsequent microvascular dysfunction. An increase in total collagen concentration leads to decreased distensibility of the ventricular tissue. Radiation affects the coronary vessels, valves, and pericardium.^[13]This complication of radiotherapy, as with pericardial constriction, is evident several years after treatment. Differentiating between constriction and restriction may be particularly difficult in these patients because the two conditions may coexist. Echocardiography may show normal left ventricular wall thickness with abnormal left ventricular filling, valvular calcification, and pericardial constriction.^[13]

Drug induced

Drug-induced RCM is a rare disorder that has been described with long-term use of the antimalarial medications chloroquine and hydroxychloroquine. Common findings include conduction abnormalities and valvular thickening.^[13]

Idiopathic restrictive cardiomyopathy (RCM) is observed primarily in the United States. Loeffler endocarditis is common in the temperate zone, whereas chronic endomyocardial fibrosis (EMF) is observed exclusively in tropical and subtropical Africa, Asia, and South America. EMF occurs most commonly in children and young adults in Uganda and Nigeria^[18]; this condition may account for up to one fourth of deaths due to cardiac disease in those areas.

Restrictive cardiomyopathy (RCM) has the poorest prognosis among all types of heart muscle diseases, with 2- and 5- year mortality rates of 50% and 70%, respectively, and the highest rate of sudden cardiac death. Due to restrictive physiology, patients with RCM ultimately develop heart failure and pulmonary hypertension.^[3]

The course of RCM varies depending on the pathology, and treatment is often unsatisfactory. The prognosis is generally poor in the adult population, as RCM shows progressive deterioration. The natural history of RCM is especially poor in children with heart failure. Adults experience a prolonged course of heart failure and may have complications of cardiac cirrhosis and thromboembolism. Patients whose condition is refractory to supportive therapy usually die of low-output cardiac failure unless cardiac transplantation is an option.

Complications of RCM may include the following:

Kushwaha SS, Fallon JT, Fuster V. Restrictive cardiomyopathy. N Engl J Med. 1997 Jan 23. 336 (4):267-76. [Medline].

Merlo M, Abate E, Pinamonti B, et al. Restrictive cardiomyopathy: clinical assessment and imaging in diagnosis and patient management. In: Pinamonti B, Sinagra Gianfranco, eds. Clinical Echocardiography and Other Imaging Techniques in Cardiomyopathies. Cham, Switzerland: Springer; 2014. 185-206. [Full Text].

Huby AC, Mendsaikhan U, Takagi K, et al. Disturbance in Z-disk mechanosensitive proteins induced by a persistent mutant myopalladin causes familial restrictive cardiomyopathy. J Am Coll Cardiol. 2014 Dec 30. 64 (25):2765-76. [Medline].

Gonzalez-Lopez E, Gallego-Delgado M, Guzzo-Merello G, et al. Wild-type transthyretin amyloidosis as a cause of heart failure with preserved ejection fraction. Eur Heart J. 2015 Oct 7. 36 (38):2585-94. [Medline].

Schlant RC, Alexander RW, eds. The Heart. New York, NY: McGraw-Hill; 1994. 1637-45.

Higano ST, Azrak E, Tahirkheli NK, Kern MJ. Hemodynamic rounds series II: hemodynamics of constrictive physiology: influence of respiratory dynamics on ventricular pressures. Catheter Cardiovasc Interv. 1999 Apr. 46 (4):473-86. [Medline].

Kostareva A, Kiselev A, Gudkova A, et al. Genetic spectrum of idiopathic restrictive cardiomyopathy uncovered by next-generation sequencing. PLoS One. 2016. 11 (9):e0163362. [Medline].

Towbin JA. Inherited cardiomyopathies. Circ J. 2014. 78 (10):2347-56. [Medline].

Peled Y, Gramlich M, Yoskovitz G, et al. Titin mutation in familial restrictive cardiomyopathy. Int J Cardiol. 2014 Jan 15. 171 (1):24-30. [Medline].

[Guideline] Lindenfeld J, Albert NM, Boehmer JP, et al, for the Heart Failure Society of America. HFSA 2010 Comprehensive Heart Failure Practice Guideline. J Card Fail. 2010 Jun. 16(6):e1-194. [Medline].

Davies MJ, Mann JM. Systemic pathology. The Cardiovascular System. Vol 10. New York, NY: Churchill Livingstone; 1995. 1409-16.

Wald DS, Gray HH. Restrictive cardiomyopathy in systemic amyloidosis. QJM. 2003 May. 96 (5):380-2. [Medline].

Garcia MJ. Constrictive pericarditis versus restrictive cardiomyopathy?. J Am Coll Cardiol. 2016 May 3. 67 (17):2061-76. [Medline].

Sasaki N, Garcia M, Ko HH, Sharma S, Parness IA, Srivastava S. Applicability of published guidelines for assessment of left ventricular diastolic function in adults to children with restrictive cardiomyopathy: an observational study. Pediatr Cardiol. 2015 Feb. 36 (2):386-92. [Medline].

Bejar D, Colombo PC, Latif F, Yuzefpolskaya M. Infiltrative cardiomyopathies. Clin Med Insights Cardiol. 2015. 9 (suppl 2):29-38. [Medline].

Mankad AK, Shah KB. Transthyretin cardiac amyloidosis. Curr Cardiol Rep. 2017 Aug 24. 19 (10):97. [Medline].

Maleszewski JJ. Cardiac amyloidosis: pathology, nomenclature, and typing. Cardiovasc Pathol. 2015 Nov-Dec. 24 (6):343-50. [Medline].

Braunwald E, Abelmann WH, eds. Atlas of Heart Diseases. Vol 2. Philadelphia, PA: Current Medicine; 1994. 53-61.

Niemann JI. Cardiomyopathies and pericardial disease. In: Tintinalli JE, Stapczynski JS, Ma OJ, et al, eds. Tintinalli’s Emergency Medicine: A Comprehensive Study Guide. 8th ed. New York, NY: McGraw-Hill; 2016. 384.

Castano A, Bokhari S, Maurer MS. Unveiling wild-type transthyretin cardiac amyloidosis as a significant and potentially modifiable cause of heart failure with preserved ejection fraction. Eur Heart J. 2015 Oct 7. 36 (38):2595-7. [Medline].

Goldstein JA. Differentiation of constrictive pericarditis and restrictive cardiomyopathy. ACC Ed Highlights. 1998 Fall. 14-22.

Amaki M, Savino J, Ain DL, et al. Diagnostic concordance of echocardiography and cardiac magnetic resonance-based tissue tracking for differentiating constrictive pericarditis from restrictive cardiomyopathy. Circ Cardiovasc Imaging. 2014 Sep. 7 (5):819-27. [Medline].

Malik SB, Kwan D, Shah AB, Hsu JY. The right atrium: gateway to the heart–anatomic and pathologic imaging findings. Radiographics. 2015 Jan-Feb. 35 (1):14-31. [Medline].

Falk RH, Quarta CC. Echocardiography in cardiac amyloidosis. Heart Fail Rev. 2015 Mar. 20 (2):125-31. [Medline].

Leya FS, Arab D, Joyal D, et al. The efficacy of brain natriuretic peptide levels in differentiating constrictive pericarditis from restrictive cardiomyopathy. J Am Coll Cardiol. 2005 Jun 7. 45 (11):1900-2. [Medline].

Selvaganesh M, Arul AS, Balasubramanian S, Ganesan N, Naina Mohammed S, Sivakumar GS, et al. An unusual ECG pattern in restrictive cardimyopathy. Indian Heart J. 2015 Jul-Aug. 67 (4):362-7. [Medline].

White JA, Fine NM. Recent advances in cardiovascular imaging relevant to the management of patients with suspected cardiac amyloidosis. Curr Cardiol Rep. 2016 Aug. 18 (8):77. [Medline].

Saeed M, Liu H, Liang CH, Wilson MW. Magnetic resonance imaging for characterizing myocardial diseases. Int J Cardiovasc Imaging. 2017 Sep. 33 (9):1395-414. [Medline].

Leviner DB, Hochhauser E, Arad M. Inherited cardiomyopathies–novel therapies. Pharmacol Ther. 2015 Nov. 155:36-48. [Medline].

Gursu HA, Varan B, Erdogan I. Use of oral budesonide in the management of protein-losing enteropathy due to restrictive cardiomyopathy. Cardiol Young. 2014 Aug. 24 (4):764-6. [Medline].

Miller LW, Guglin M. Evaluation of ventricular assist devices and cardiac transplantation. In: Baliga R, Haas G, eds. Management of Heart Failure. London, UK: Springer-Verlag; 2015.

Sundararajan S, Thiruchelvam T, Hsia TY, Karimova A. New 15-mL ventricular assist device in children with restrictive physiology of the left ventricle. J Thorac Cardiovasc Surg. 2014 Jun. 147 (6):e79-80. [Medline].

Grupper A, Park SJ, Pereira NL, et al. Role of ventricular assist therapy for patients with heart failure and restrictive physiology: Improving outcomes for a lethal disease. J Heart Lung Transplant. 2015 Aug. 34 (8):1042-9. [Medline].

Robinson MR, Al-Kindi SG, Oliveira GH. Heart and heart-liver transplantation in patients with hemochromatosis. Int J Cardiol. 2017 Oct 1. 244:226-8. [Medline].

Uriel N, Vainrib A, Jorde UP, et al. Mediastinal radiation and adverse outcomes after heart transplantation. J Heart Lung Transplant. 2010 Mar. 29 (3):378-81. [Medline].

Hanna M. Novel drugs targeting transthyretin amyloidosis. Curr Heart Fail Rep. 2014 Mar. 11 (1):50-7. [Medline].

Madeira M, Teixeira R, Costa M, Goncalves L, Klein AL. Two-dimensional speckle tracking cardiac mechanics and constrictive pericarditis: systematic review. Echocardiography. 2016 Oct. 33 (10):1589-99. [Medline].

Zhang Y, He L, Cai J, et al. Measurements in pediatric patients with cardiomyopathies: comparison of cardiac magnetic resonance imaging and echocardiography. Cardiology. 2015. 131 (4):245-50. [Medline].

Topilsky Y, Pereira NL, Shah DK, et al. Left ventricular assist device therapy in patients with restrictive and hypertrophic cardiomyopathy. Circ Heart Fail. 2011 May. 4 (3):266-75. [Medline].

[Guideline] Hershberger RE, Lindenfeld J, Mestroni L, Seidman CE, Taylor MR, Towbin JA, et al. Genetic evaluation of cardiomyopathy–a Heart Failure Society of America practice guideline. J Card Fail. 2009 Mar. 15(2):83-97. [Medline]. [Full Text].

Fritschi S, Prothmann M, Schulz-Menger J. [Hypertrophic and restrictive cardiomyopathy. Differentiation by imaging] [German]. Herz. 2015 Jun. 40 (4):591-9. [Medline].

DePasquale EC, Nasir K, Jacoby DL. Outcomes of adults with restrictive cardiomyopathy after heart transplantation. J Heart Lung Transplant. 2012 Dec. 31 (12):1269-75. [Medline].

[Guideline] Yancy CW, Jessup M, Bozkurt B, et al, for the Writing Committee Members, American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines. 2013 ACCF/AHA guideline for the management of heart failure: a report of the American College of Cardiology Foundation/American Heart Association Task Force on practice guidelines. Circulation. 2013 Oct 15. 128(16):e240-327. [Medline]. [Full Text].

[Guideline] Ackerman MJ, Priori SG, Willems S, et al, for the Heart Rhythm Society (HRS), European Heart Rhythm Association (EHRA). HRS/EHRA expert consensus statement on the state of genetic testing for the channelopathies and cardiomyopathies: this document was developed as a partnership between the Heart Rhythm Society (HRS) and the European Heart Rhythm Association (EHRA). Europace. 2011 Aug. 13(8):1077-109. [Medline]. [Full Text].

[Guideline] Ponikowski P, Voors AA, Anker SD, et al, for the European Society of Cardiology Authors/Task Force Members. 2016 ESC Guidelines for the diagnosis and treatment of acute and chronic heart failure: The Task Force for the diagnosis and treatment of acute and chronic heart failure of the European Society of Cardiology (ESC)Developed with the special contribution of the Heart Failure Association (HFA) of the ESC. Eur Heart J. 2016 Jul 14. 37(27):2129-200. [Medline]. [Full Text].

Ryan TD, Madueme PC, Jefferies JL, et al. Utility of echocardiography in the assessment of left ventricular diastolic function and restrictive physiology in children and young adults with restrictive cardiomyopathy: a comparative echocardiography-catheterization study. Pediatr Cardiol. 2017 Feb. 38 (2):381-9. [Medline].

Clinical Features

Constrictive Pericarditis

Restrictive Cardiomyopathy

History

Prior history of pericarditis or condition that causes pericardial disease

History of systemic disease (eg, amyloidosis, hemochromatosis)

General examination

…

Peripheral stigmata of systemic disease

Systemic examination – Heart sounds

Pericardial knock, high-frequency sound

Presence of loud diastolic filling sound S₃, Low-frequency sound

Murmurs

No murmurs

Murmurs of mitral and tricuspid insufficiency

Prior chest radiograph

Pericardial calcification

Normal results of prior chest radiograph

Investigation

Constrictive Cardiomyopathy

Restrictive Cardiomyopathy

Chest radiograph

Pericardial calcification

Atrial dilation causing increased cardiothoracic ratio; normal ventricular size

CT scanning/MRI

Pericardial thickening

No pericardial thickening

Echocardiography

Normal-sized ventricles and atria; pericardial effusion may be observed

Nondilated, normally contracting, nonhypertrophied ventricles and marked dilation of both atria

Doppler flow velocities on echocardiography

Respiratory changes (ie, decreased peak transmitral diastolic flow) during inspiration; equalization of the right- and left-sided filling pressures

No respiratory changes; greater elevation in the left-sided filling pressures

Catheterization hemodynamics:

1) RVSP

2) RVEDP:RVSP ratio

3) RVEDP/LVEDP equalization

1) = 50 mm Hg

2) = 0.33

3) = 5-mm Hg difference

1) = 50 mm Hg

2) = 0.33

3) = 5-mm Hg difference

Cardiac biopsy

Normal myocardium

Often diagnostic, showing abnormal myocardium

CT = computed tomography; LVEDP = left ventricular end-diastolic pressure; MRI = magnetic resonance imaging; RVEDP = right ventricular end-diastolic pressure; RVSP = right ventricular systolic pressure.

Lindsay Reardon, MD Clinical Assistant Professor, Emergency Ultrasound Faculty, Department of Emergency Medicine, State University of New York at Stony Brook Health Sciences Center

Lindsay Reardon, MD is a member of the following medical societies: American College of Emergency Physicians, American Institute of Ultrasound in Medicine, Emergency Medicine Residents’ Association, Wilderness Medical Society