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Amyloidosis

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Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Sabawoon Mirwais, M.B.B.S, M.D.[2], Syed Hassan A. Kazmi BSc, MD [3], Shaghayegh Habibi, M.D.[4]

Synonyms and keywords:

Overview

Overview

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

Overview

Historical Perspective

In 1639, Nicolaus Fontanus autopsied a young man who had ascites, jaundice, liver abscess, and splenomegaly and his report has been the first description of amyloidosis. There is no significant data regarding the historical perspective of amyloidosis throughout the 18th century. Rudolph Virchow and Weber are the prominent figures with substantial work on amyloidosis during the 19th century. In 1922, Bennhold introduced Congo Red staining of amyloid that remains the gold standard for diagnosis.

Classification

Amyloidosis may be classified on the basis of type of amyloidogenic protein and associated clinical syndromes into primary (AL) amyloidosis, secondary (AA) amyloidosis, familial (AF) amyloidosis, transthyretin (ATTRwt) amyloidosis and dialysis-associated (AH) amyloidosis. It can also be classified based on extent of organ system involvement

Pathophysiology

Amyloid is an abnormal insoluble extracellular protein that deposits in the different tissues and causes organic dysfunction and a wide variety of clinical syndromes. In systemic amyloidosis, amyloid gradually accumulate and amyloid deposition is widespread in the viscera, blood vessel walls, and in the different connective tissues. Primary (AL) amyloidosis) is the most common type of amyloidosis. It results from aggregation and deposition of monoclonal immunoglobulin (Ig) light chains that usually produced by plasma cell clones. Secondary amyloidosis is associated with chronic inflammation (such as tuberculosis or rheumatoid arthritis). Hereditary (or familial) amyloidosis are autosomal dominant diseases that inherited variant proteins cause the production and deposition of amyloid fibrils. Some neurodegenerative disorderssuch as Parkinson’s disease, Alzheimer, and Huntington’s disease may occur in localised amyloidosis. On microscopic pathology, typical green birefringence under polarized light after Congo red staining (appears in red under normal light)

Causes

Hereditary amyloidosis can be caused by genetic mutations in different genes. Causes of acquired amyloidosis can include tuberculosis, familial Mediterranean fever, rheumatoid arthritis, multiple myeloma, ankylosing spondylitis, and psoriatic arthritis.

Differentiating Amyloidosis from other Diseases

Amyloidosis needs to be differentiated from acute myocarditis, bronchiectasis, multiple myeloma and other systemic diseases .

Epidemiology and Demographics

The incidence of amyloidosis is approximately 1.2 per 100,000 individuals per year worldwide. The prevalence of AL amyloidosis increased significantly between 2007 and 2015, from 1.6 per 100,000 in 2007 to 4.0 per 100,000 in 2015. The mortality rate of systemic amyloidosis is approximately 100 per 100,000 deaths in developed countries. In amyloidosis, the mean age of presentation is 55 – 60 years. Men are more commonly affected by amyloidosis than women.

Risk Factors

There are no established risk factors for amyloidosis. Some inflammatory conditions might increase the likelihood of amyloid deposition in the body.

Screening

There is insufficient evidence to recommend routine screening for amyloidosis.

Natural History, Complications and Prognosis

In amyloidosis, insoluble fibrils of amyloid are deposited in organs, causing organ dysfunction and eventually death. Patients with amyloidosis may eventually suffer from heart failure, nephrotic syndrome, hepatomegaly and peripheral neuropathy. In primary amyloidosis, the survival rate depends upon the type of organ involvement and the hematological response to treatment. In AL amyloidosis, untreated individuals have the worst prognosis. In this group of patients, the median survival is one to two years.

Diagnosis

Diagnostic Study of Choice

The diagnostic study of choice in amyloidosis is tissue biopsy of the affected organ. Congo Red staining will show apple green birefringence of the tissue sample under polarized light, and subtyping of light chains(for light chain amyloidosis) can be done via mass spectrometry. Bone marrow biopsy and organ-specific laboratory measurements are also important ancillary tests.

History and Symptoms

In amyloidosis, the range of symptoms depends on specific tissues and organs involved. Symptoms can be quite diverse.

Physical Examination

Common findings in amyloidosis include petechiae, ecchymosis, parotid gland enlargement, increased intraocular pressure, enlarged tongue, hepatomegaly, carpal tunnel syndrome, and Raynaud’s phenomenon.

Laboratory Findings

Laboratory findings in amyloidosis include elevated erythrocyte sedimentation rate, increased BUN level, serum creatinine, protein, casts, or fat bodies in urine. Serum troponin, B-type natriuretic peptide, and beta-2-microglobulin are prognostic markers for heart failure. Amyloid deposits can be identified histologically by Congo red staining and viewing under polarized light where amyloid deposits produce a distinctive ‘apple green birefringence’. Alternatively, thioflavin T stain may be used. An abdominal fat pad aspiration, rectal mucosa biopsy, or bone marrow biopsy can help confirm the diagnosis. They reveal positive findings in 80% patients.

Electrocardiogram

Electrocardiogram is particularly useful for cardiac amyloidosis. Findings on electrocardiogram include low voltage QRS complexes, left and right ventricular hypertrophy, left atrial abnormalities, pathological Q waves, and AV block.

Chest X-Ray

Chest x-ray findings in a case of amyloidosis include a coin lesion.

CT Scan

CT scan can be done to assess for amyloid deposition in particular organs. It can also be done to rule out other causes of organ dysfunction. However, MRI is more sensitive than CT in the diagnosis of amyloidosis.

MRI

MRI is commonly done to assess for amyloid deposition in particular organs. It can also be done to rule out other causes of organ dysfunction. A cardiac MRI is used when an echocardiogram fails to differentiate amyloidosis from hypertrophic cardiomyopathy.

Echocardiography

Echocardiography is critical in the diagnosis of cardiac amyloidosis. Echocardiogram should be done at diagnosis and routinely thereafter to monitor response to therapy.

Other Imaging Findings

Tissue doppler echocardiography and myocardial strain rate imaging has been shown to be very sensitive for the assessment of myocardial dysfunction in restrictive cardiomyopathy. The developmend of serum amyloid P component (SAP) scans has given physicians the ability to specifically locate amyloid deposits.

Other Diagnostic Studies

A tissue biopsy or fat aspirate should be done to confirm the presence or type of amyloid protein which is involved in the pathogenesis of the disease.

Treatment

There is no treatment for primary amyloidosis. The initial target in the treatment of this disorder is to correct the organ failure, as the disease is discovered at an advanced stage.

Medical Therapy

There are few available treatments for primary amyloidosis. Since the disease is typically discovered at an advanced stage, the initial treatment is aimed at preventing further organ damage and correcting the effects of organ failure. The most commonly used regimen for AL amyloidosis is CyBorD, which consists of cyclophosphamide, bortezomib, and dexamethasone.

Surgery

Organ-specific transplant may need to be done, depending on the organ involved. However, surgery is not commonly done in patients with amyloidosis, since it is usually a systemic disease that requires treatment of the underlying cause.

Prevention

Primary Prevention

There is no role for primary prevention in amyloidosis.

Secondary Prevention

There is no role for secondary prevention in amyloidosis.

References

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Historical Perspective

Historical Perspective

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Shaghayegh Habibi, M.D.[2]

Overview

In 1639, Nicolaus Fontanus autopsied a young man who had ascites, jaundice, liver abscess and splenomegaly and his report has been the first description of amyloidosis. There is no significant data regarding the historical perspective of amyloidosis throughout the 18th century. Rudolph Virchow and Weber are the prominent figures with substantial work on amyloidosis during the 19th century. In 1922, Bennhold introduced Congo red staining of amyloid that remains the gold standard for diagnosis.

Historical Perspective

  • In 1639, Nicolaus Fontanus autopsied a young man who had ascites, jaundice, liver abscess and splenomegaly and his report has been the first description of amyloidosis.[1]
  • In 1854, Rudolph Virchow introduced the term of amyloid as an macroscopic abnormality in some tissues.[2]
  • In 1867, Weber reported the first case of amyloidosis associated with multiple myeloma.[1]
  • In 1922, Bennhold introduced Congo red staining of amyloid that remains the gold standard for diagnosis.[3]
  • In 1959, Cohen and Calkins used ultrathin sections of amyloidotic tissues and assessed by electron microscopic examination, explained the presence of nonbranching fibrils with indeterminate length and variable width.[2][1]

References

  1. 1.0 1.1 1.2 Kyle RA (June 2011). “Amyloidosis: a brief history”. Amyloid. 18 Suppl 1: 6–7. doi:10.3109/13506129.2011.574354001. PMID 21838413.
  2. 2.0 2.1 Sipe JD, Cohen AS (June 2000). “Review: history of the amyloid fibril”. J. Struct. Biol. 130 (2–3): 88–98. doi:10.1006/jsbi.2000.4221. PMID 10940217.
  3. Khan MF, Falk RH (November 2001). “Amyloidosis”. Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.

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Classification

Classification

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]Associate Editor(s)-in-Chief: Syed Hassan A. Kazmi BSc, MD [2]Shaghayegh Habibi, M.D.[3]

Overview

Amyloidosis may be classified on the basis of type of amyloidogenic protein and associated clinical syndromes into primary (AL) amyloidosis, secondary (AA) amyloidosis, familial (AF) amyloidosis, transthyretin (ATTRwt) amyloidosis and dialysis-associated (AH) amyloidosis. It can also be classified based on extent of organ system involvement.

Classification

Classification Based on Precursor of Amyloidogenic Protein: [1][2]

Type Abbreviation Amyloidogenic Protein/Fibril Acquired/Inherited Most Common Organ Involvement Associated Conditions
Primary amyloidosis AL Acquired Heart and kidneys
Secondary amyloidosis AA Acquired Kidneys (early), heart and liver (late)
Senile systemic or wild-type amyloidosis ATTRwt/ATTRvar Acquired (ATTRwt) or Hereditary (ATTRvar) Heart and nerves (more common in hereditary type)
β2-microglobulin related amyloidosis AH Acquired or Hereditary Nerves (peripheral and autonomic)
Leucocyte cell–derived chemotaxin 2 related amyloidosis ALect2
  • Leucocyte cell–derived chemotaxin 2
 Acquired Kidneys and liver
    Fibrinogen A alpha-chain associated amyloidosis AF Hereditary Kidneys and liver
    Abnormal Apolipoprotein A-I, AII, and AIV related amyloidosis AApoA-I Hereditary Kidneys, liver and nerves (peripheral)
    Lysozyme amyloid related amyloidosis ALys Hereditary Liver and kidneys
    Gelsolin related amyloidosis AGel Hereditary Kidneys and nerves (peripheral and cranial)

    Classification Based on Organ Involvement:[3][4]

    Classification Subtypes Causes Clinical Features
    Systemic amyloidosis Primary amyloidosis (AL)
    Secondary amyloidosis (AA)
    Hereditary amyloidosis
    Organ-specific amyloidosis Renal amyloidosis
    Cardiac amyloidosis
    Hepatic amyloidosis
    Amyloid neuropathy
    Gastrointestinal amyloidosis

    Refrences

    1. Khoor A, Colby TV (February 2017). “Amyloidosis of the Lung”. Arch. Pathol. Lab. Med. 141 (2): 247–254. doi:10.5858/arpa.2016-0102-RA. PMID 28134587.
    2. Benson MD, Buxbaum JN, Eisenberg DS, Merlini G, Saraiva M, Sekijima Y, Sipe JD, Westermark P (December 2018). “Amyloid nomenclature 2018: recommendations by the International Society of Amyloidosis (ISA) nomenclature committee”. Amyloid. 25 (4): 215–219. doi:10.1080/13506129.2018.1549825. PMID 30614283. Vancouver style error: initials (help)
    3. Wechalekar AD, Gillmore JD, Hawkins PN (June 2016). “Systemic amyloidosis”. Lancet. 387 (10038): 2641–2654. doi:10.1016/S0140-6736(15)01274-X. PMID 26719234.
    4. Falk RH, Alexander KM, Liao R, Dorbala S (September 2016). “AL (Light-Chain) Cardiac Amyloidosis: A Review of Diagnosis and Therapy”. J. Am. Coll. Cardiol. 68 (12): 1323–41. doi:10.1016/j.jacc.2016.06.053. PMID 27634125.

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    Pathophysiology

    Pathophysiology

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Shaghayegh Habibi, M.D.[2]Sabawoon Mirwais, M.B.B.S, M.D.[3]

    Overview

    Amyloid is an abnormal insoluble extracellular protein that deposits in the different tissues and causes organic dysfunction and a wide variety of clinical syndromes. In systemic amyloidosis, amyloid gradually accumulate and amyloid deposition is widespread in the viscera, blood vessel walls, and in the different connective tissues. Primary (AL) amyloidosis) is the most common type of amyloidosis. It results from aggregation and deposition of monoclonal immunoglobulin (Ig) light chains that usually produced by plasma cell clones. Secondary amyloidosis is associated with chronic inflammation (such as tuberculosis or rheumatoid arthritis). Hereditary (or familial) amyloidosis are autosomal dominant diseases that inherited variant proteins cause the production and deposition of amyloid fibrils. Some neurodegenerative disorders such as Parkinson’s disease, Alzheimer, and Huntington’s disease may occur in localised amyloidosis. On microscopic pathology, typical green birefringence under polarized light after Congo red staining (appears in red under normal light).

    Pathophysiology

    • Amyloid is an abnormal insoluble extracellular protein that deposits in the different tissues and causes organic dysfunction and a wide variety of clinical syndromes.[1]
    • These abnormal amyloids are derived from misfolding and aggregation of normally soluble proteins.
    • Amyloid deposition can disrupt tissue structure of involved organ and consequently leads to organ failure.[2]

    Systemic Amyloidosis

    Primary Amyloidosis (AL)

    Secondary Amyloidosis (AA)

    Hereditary Amyloidosis

    Organ-specific Amyloidosis

    Genetics

    Hereditary Amyloidosis

    • Hereditary amyloidosis involves mutations in the following genes:[9]
      • LYZ gene
      • Fibrinogen A alpha polypeptide gene
      • FGA gene
      • APOA1 gene
      • Lysozyme gene
      • B2M gene

    Primary Localized Cutaneous Amyloidosis

    • Primary localized cutaneous amyloidosis is inherited in autosomal dominant manner.[10]
    • Primary localized cutaneous amyloidosis involves mutations in the following genes:[11]
      • OSMR gene

    Associated Conditions

    Conditions associated with amyloidosis include:[12]

    • MEN2A

    Gross Pathology

    On gross pathology, the organs affected by amyloidosis can be characterized by the following features:

    • Porcelain like or waxy appearance
    • Enlargement

    Images

    Nodular deposits of amyloid on the pleural surfaces.[13]
    Cut section of an inguinal lymph node showing firm and waxy consistency.[14]
    A slice of the affected node (left) has turned black after treatment with Lugol’s solution. A piece of normal myometrium (right) treated similarly with no reaction is also shown.[15]


    Microscopic Pathology

    On microscopic histopathological analysis, amyloidosis is characterized by:[6][16]

    • Green birefringence under polarized light after Congo red staining (appears red under normal light)
    • Linear non-branching fibrils (indefinite length with an approximately same diameter)
    • Distinct X-ray diffraction pattern consistent with Pauling’s model of a cross-beta fibril

    Images

    Small bowel duodenum with amyloid deposition Congo red.[17]
    Amyloidosis (black arrows) in a lymph node after staining with Congo Red.[18]
    Green birefringence under polarized light.[19]


    References

    1. Wechalekar AD, Gillmore JD, Hawkins PN (June 2016). “Systemic amyloidosis”. Lancet. 387 (10038): 2641–2654. doi:10.1016/S0140-6736(15)01274-X. PMID 26719234.
    2. Wechalekar AD, Gillmore JD, Hawkins PN (June 2016). “Systemic amyloidosis”. Lancet. 387 (10038): 2641–2654. doi:10.1016/S0140-6736(15)01274-X. PMID 26719234.
    3. Baker KR, Rice L (2012). “The amyloidoses: clinical features, diagnosis and treatment”. Methodist Debakey Cardiovasc J. 8 (3): 3–7. PMC 3487569. PMID 23227278.
    4. Pepys MB (2006). “Amyloidosis”. Annu. Rev. Med. 57: 223–41. doi:10.1146/annurev.med.57.121304.131243. PMID 16409147.
    5. Wechalekar AD, Gillmore JD, Hawkins PN (June 2016). “Systemic amyloidosis”. Lancet. 387 (10038): 2641–2654. doi:10.1016/S0140-6736(15)01274-X. PMID 26719234.
    6. 6.0 6.1 6.2 Khan MF, Falk RH (November 2001). “Amyloidosis”. Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.
    7. Hund E, Linke RP, Willig F, Grau A (February 2001). “Transthyretin-associated neuropathic amyloidosis. Pathogenesis and treatment”. Neurology. 56 (4): 431–5. doi:10.1212/wnl.56.4.431. PMID 11261421.
    8. Gertz MA (June 2017). “Hereditary ATTR amyloidosis: burden of illness and diagnostic challenges”. Am J Manag Care. 23 (7 Suppl): S107–S112. PMID 28978215.
    9. Pepys MB, Hawkins PN, Booth DR, Vigushin DM, Tennent GA, Soutar AK, Totty N, Nguyen O, Blake CC, Terry CJ (April 1993). “Human lysozyme gene mutations cause hereditary systemic amyloidosis”. Nature. 362 (6420): 553–7. doi:10.1038/362553a0. PMID 8464497.
    10. Arita K, South AP, Hans-Filho G, Sakuma TH, Lai-Cheong J, Clements S, Odashiro M, Odashiro DN, Hans-Neto G, Hans NR, Holder MV, Bhogal BS, Hartshorne ST, Akiyama M, Shimizu H, McGrath JA (January 2008). “Oncostatin M receptor-beta mutations underlie familial primary localized cutaneous amyloidosis”. Am. J. Hum. Genet. 82 (1): 73–80. doi:10.1016/j.ajhg.2007.09.002. PMC 2253984. PMID 18179886.
    11. Arita K, South AP, Hans-Filho G, Sakuma TH, Lai-Cheong J, Clements S, Odashiro M, Odashiro DN, Hans-Neto G, Hans NR, Holder MV, Bhogal BS, Hartshorne ST, Akiyama M, Shimizu H, McGrath JA (January 2008). “Oncostatin M receptor-beta mutations underlie familial primary localized cutaneous amyloidosis”. Am. J. Hum. Genet. 82 (1): 73–80. doi:10.1016/j.ajhg.2007.09.002. PMC 2253984. PMID 18179886.
    12. Hofstra RM, Sijmons RH, Stelwagen T, Stulp RP, Kousseff BG, Lips CJ, Steijlen PM, Van Voorst Vader PC, Buys CH (August 1996). “RET mutation screening in familial cutaneous lichen amyloidosis and in skin amyloidosis associated with multiple endocrine neoplasia”. J. Invest. Dermatol. 107 (2): 215–8. doi:10.1111/1523-1747.ep12329651. PMID 8757765.
    13. By Yale Rosen from USA – Amyloidosis, CC BY-SA 2.0, https://commons.wikimedia.org/w/index.php?curid=31127928
    14. By Ed Uthman, MD – https://www.flickr.com/photos/euthman/377537238/, CC BY-SA 2.0, https://commons.wikimedia.org/w/index.php?curid=1629764
    15. By Ed Uthman, MD – https://www.flickr.com/photos/euthman/377538012/, CC BY-SA 2.0, https://commons.wikimedia.org/w/index.php?curid=1629740
    16. Röcken C, Shakespeare A (February 2002). “Pathology, diagnosis and pathogenesis of AA amyloidosis”. Virchows Arch. 440 (2): 111–122. doi:10.1007/s00428-001-0582-9. PMID 11964039.
    17. By Michael Feldman, MD, PhDUniversity of Pennsylvania School of Medicine – http://www.healcentral.org/healapp/showMetadata?metadataId=38717, CC BY 2.0, https://commons.wikimedia.org/w/index.php?curid=870218
    18. By Ed Uthman, MD – https://www.flickr.com/photos/euthman/377559787/, CC BY-SA 2.0, https://commons.wikimedia.org/w/index.php?curid=1629716
    19. By Ed Uthman, MD – https://www.flickr.com/photos/euthman/377559955/, CC BY-SA 2.0, https://commons.wikimedia.org/w/index.php?curid=1629705

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    Causes

    Causes

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

    Overview

    Hereditary amyloidosis can be caused by genetic mutations in different genes. Causes of acquired amyloidosis can include tuberculosis, familial Mediterranean fever, rheumatoid arthritis, multiple myeloma, ankylosing spondylitis, and psoriatic arthritis.

    Causes

    Causes of Hereditary Amyloidosis

    Genetic mutations responsible for the development of amyloidosis can involve the following genes:[1]

    Causes of Acquired Amyloidosis

    • Most common causes of acquired amyloidosis include:[2]
    • Less common causes of acquired amyloidosis include:[3][4][5]

    References

    1. Pepys MB, Hawkins PN, Booth DR, Vigushin DM, Tennent GA, Soutar AK, Totty N, Nguyen O, Blake CC, Terry CJ (April 1993). “Human lysozyme gene mutations cause hereditary systemic amyloidosis”. Nature. 362 (6420): 553–7. doi:10.1038/362553a0. PMID 8464497.
    2. Shin YM (March 2011). “Hepatic amyloidosis”. Korean J Hepatol. 17 (1): 80–3. doi:10.3350/kjhep.2011.17.1.80. PMC 3304630. PMID 21494083.
    3. Meira T, Sousa R, Cordeiro A, Ilgenfritz R, Borralho P (2015). “Intestinal Amyloidosis in Common Variable Immunodeficiency and Rheumatoid Arthritis”. Case Rep Gastrointest Med. 2015: 405695. doi:10.1155/2015/405695. PMC 4553190. PMID 26351592.
    4. Kadiroğlu AK, Yıldırım Y, Yılmaz Z, Kayabaşı H, Avcı Y, Yıldırım MS, Yılmaz ME (2012). “A rare cause of secondary amyloidosis: common variable immunodeficiency disease”. Case Rep Nephrol. 2012: 860208. doi:10.1155/2012/860208. PMC 3914192. PMID 24558615.
    5. Lim AY, Lee JH, Jung KS, Gwag HB, Kim DH, Kim SJ, Lee GY, Kim JS, Kim HJ, Lee SY, Lee JE, Jeon ES, Kim K (July 2015). “Clinical features and outcomes of systemic amyloidosis with gastrointestinal involvement: a single-center experience”. Korean J. Intern. Med. 30 (4): 496–505. doi:10.3904/kjim.2015.30.4.496. PMC 4497337. PMID 26161016.

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    Differentiating Amyloidosis from other Diseases

    Differentiating Amyloidosis from other Diseases

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Syed Hassan A. Kazmi BSc, MD [2]

    Overview

    Amyloidosis needs to be differentiated from systemic diseases including acute myocarditis, bronchiectasis, and multiple myeloma.

    Differentiating Amyloidosis from other Diseases

    Amyloidosis should be differentiated from the following systemic diseases:

    Cardiac Amyloidosis

    Cardiac amyloidosis (AL and TTRwt) should be differentiated from other causes of heart failure:

    Differential Diagnosis History and Symptoms Physical Examination Laboratory Findings Imaging Findings
    Cardiac amyloidosis
    • Elevated jugular pressure

    Periorbital purpura: Often occurs with sneezing, coughing or with minor trauma. Indicates capillary involvement of AL type amyloidosis.

    • Macroglossia
    • Abnormal phonation
    • Hepatomegaly
    • Ascites may be present in the setting of heart failure
    • Valvular involvement murmurs of mitral and tricuspid regurgitation (systolic).


    • Normocytic mormochromic anemia
    • Serum free-light-chain assay positive
    • Increased BNP, ANP and β2 microglobulin
    • Voltage-to-mass ratio is more sensitive than EKG, 2D Echo and nuclear scanning alone
    ST Segment Elevation Myocardial Infarction
    • Chest pain with possible radiation to left arm and lower jaw
    • Squeezing, crushing chest pain
    • Sweating
    • Nausea and vomiting
    • Anxious patient in pain with diaphoresis
    • Signs of heart failure may be present
    • Arrhythmia
    • ST elevation, new left bundle branch block, and Q wave on EKG
    • Elevated cardiac biomarkers
    • Either complete or subtotal occlusion of an epicardial coronary artery on coronary angiography
    • Confluent hyperenhancement extending from the endocardium
    Non ST Elevation Myocardial Infarction
    • Crushing, left-sided substernal chest pain or pressure that radiates to the neck or left arm
    • Same as ST-elevation MI
    • ST-segment depression or T-wave inversion on EKG
    • Elevated cardiac biomarkers
    Pericarditis
    • Chest pain relieved by sitting up and leaning forward and worsened by lying down
    • Fever, anxiety, difficulty breathing
    • Pericardial friction rub
    • Signs of cardiac tamponade may be present
    • PR segment depression and electrical alternans on EKG
    • A flask-shaped, enlarged cardiac silhouette on CXR
    • Pericardial thickness of more than 4 mm on MRI
    • Pericardial effusion and cardiac chamber indentation or collapse on echo when cardiac tamponade is present
    Alcoholic Cardiomyopathy
    • History of alcohol abuse
    • Fatigue, weakness, anorexia, palpitations, and shortness of breath on activity
    • Leg swelling and pedal edema
    • Signs of heart failure such as presence of S3 and S4 heart sounds, pedal edema, and jugular venous distension
    • Signs of alcoholic liver disease may be present
    • Elevated MCV and MCHC on CBC
    • Elevated LDH, AST, ALT, creatine kinase, gammaglutamyl transpeptidase, malic dehydrogenase, and alpha-hydroxybutyric dehydrogenase
    • Q waves and non specific ST and T wave changes on EKG
    • Cardiomegaly, pulmonary congestion, and pleural effusions on CXR
    • Left ventricular dilatation on echo

    References

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    Epidemiology and Demographics

    Epidemiology and Demographics

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

    Overview

    The incidence of amyloidosis is approximately 1.2 per 100,000 individuals per year worldwide. The prevalence of AL amyloidosis increased significantly between 2007 and 2015, from 1.6 per 100,000 in 2007 to 4.0 per 100,000 in 2015. The mortality rate of systemic amyloidosis is approximately 100 per 100,000 deaths in developed countries. In amyloidosis, the mean age of presentation is 55 – 60 years. Men are more commonly affected by amyloidosis than women.

    Epidemiology and Demographics

    Incidence

    • The incidence of amyloidosis is approximately 1.2 per 100,000 individuals per year worldwide.[1]
    • The incidence of AL amyloidosis in USA ranged from 1 per 100,000 to 1.4 per 100,000 from 2007 to 2015.[2]
    • Transthyretin-related hereditary amyloidosis is endemic in Portuguese locations Póvoa de Varzim and Vila do Conde (Caxinas), with more than 1000 affected people, coming from about 500 families, where 70% of the people develop the illness. In northern Sweden, more specifically Piteå, Skellefteå and Umeå, 1.5% of the population has the mutated gene. There are many other populations in the world who exhibit the illness after having developed it independently.

    Prevalence

    • The prevalence of AL in USA amyloidosis increased significantly between 2007 and 2015, from 1.6 per 100,000 in 2007 to 4.0 per 100,000 in 2015.[3]

    Mortality rate

    • The mortality rate of systemic amyloidosis is approximately 100 per 100,000 deaths in developed countries.[4]

    Age

    • In amyloidosis, the mean age of presentation is 55-60 years.[5]

    Race

    • Hereditary amyloidosis subtypes include a substitution of an amino acid that is detected in approximately 4% of the black population.[6]

    Gender

    • Men are more commonly affected by amyloidosis than women.[7]

    References

    1. Khan MF, Falk RH (November 2001). “Amyloidosis”. Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.
    2. Quock TP, Yan T, Chang E, Guthrie S, Broder MS (May 2018). “Epidemiology of AL amyloidosis: a real-world study using US claims data”. Blood Adv. 2 (10): 1046–1053. doi:10.1182/bloodadvances.2018016402. PMC 5965052. PMID 29748430.
    3. Quock TP, Yan T, Chang E, Guthrie S, Broder MS (May 2018). “Epidemiology of AL amyloidosis: a real-world study using US claims data”. Blood Adv. 2 (10): 1046–1053. doi:10.1182/bloodadvances.2018016402. PMC 5965052. PMID 29748430.
    4. Pepys MB (2006). “Amyloidosis”. Annu. Rev. Med. 57: 223–41. doi:10.1146/annurev.med.57.121304.131243. PMID 16409147.
    5. Shin YM (March 2011). “Hepatic amyloidosis”. Korean J Hepatol. 17 (1): 80–3. doi:10.3350/kjhep.2011.17.1.80. PMC 3304630. PMID 21494083.
    6. Khan MF, Falk RH (November 2001). “Amyloidosis”. Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.
    7. Shin YM (March 2011). “Hepatic amyloidosis”. Korean J Hepatol. 17 (1): 80–3. doi:10.3350/kjhep.2011.17.1.80. PMC 3304630. PMID 21494083.

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    Risk Factors

    Risk Factors

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1];

    Overview

    There are no established risk factors for amyloidosis. Some inflammatory conditions and chronic infections may increase the likelihood of amyloid deposition in the body.

    Risk Factors

    There are no established risk factors for amyloidosis. Some inflammatory conditions and chronic infections may increase the likelihood of amyloid deposition in the body.

    References


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    Screening

    Screening

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Shaghayegh Habibi, M.D.[2]

    Overview

    There is insufficient evidence to recommend routine screening for amyloidosis.

    Screening

    There is insufficient evidence to recommend routine screening for amyloidosis.

    References

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    Natural History, Complications and Prognosis

    Natural History, Complications and Prognosis

    Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1] Associate Editor(s)-in-Chief: Shaghayegh Habibi, M.D.[2]

    Overview

    In amyloidosis, insoluble fibrils of amyloid are deposited in organs, causing organ dysfunction and eventually death. Patients with amyloidosis may eventually suffer from heart failure, nephrotic syndrome, hepatomegaly and peripheral neuropathy. In primary amyloidosis, the survival rate depends upon the type of organ involvement and the hematological response to treatment. In AL amyloidosis, untreated individuals have the worst prognosis. In this group of patients, the median survival is one to two years.

    Natural History, Complications, and Prognosis

    Natural History

    Complications

    In patients with amyloidosis, the most frequent complications include:[3]

    Prognosis

    References

    1. Baker KR, Rice L (2012). “The amyloidoses: clinical features, diagnosis and treatment”. Methodist Debakey Cardiovasc J. 8 (3): 3–7. PMC 3487569. PMID 23227278.
    2. Khan MF, Falk RH (November 2001). “Amyloidosis”. Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.
    3. Jerzykowska S, Cymerys M, Gil LA, Balcerzak A, Pupek-Musialik D, Komarnicki MA (2014). “Primary systemic amyloidosis as a real diagnostic challenge – case study”. Cent Eur J Immunol. 39 (1): 61–6. doi:10.5114/ceji.2014.42126. PMC 4439975. PMID 26155101.
    4. Desport E, Bridoux F, Sirac C, Delbes S, Bender S, Fernandez B, Quellard N, Lacombe C, Goujon JM, Lavergne D, Abraham J, Touchard G, Fermand JP, Jaccard A (August 2012). “Al amyloidosis”. Orphanet J Rare Dis. 7: 54. doi:10.1186/1750-1172-7-54. PMC 3495844. PMID 22909024.
    5. Merlini G, Seldin DC, Gertz MA (May 2011). “Amyloidosis: pathogenesis and new therapeutic options”. J. Clin. Oncol. 29 (14): 1924–33. doi:10.1200/JCO.2010.32.2271. PMC 3138545. PMID 21483018.


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    Diagnosis

    Diagnosis

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    Treatment

    Treatment

    Medical Therapy | Surgery | Primary Prevention | Secondary Prevention | Cost-Effectiveness of Therapy | Future or Investigational Therapies

    Case Studies

    Case Studies

    Case #1

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