Amyloidosis: Difference between revisions

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Revision as of 17:12, 13 June 2018

For patient information, click here

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

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.^[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]

Classification

Amyloidosis may be classified based on precursor of amyloidogenic protein into different subtypes, include:^[4]^[5]

Type	Amyloidogenic protein/ fibril	Clinical syndrome
AL (primary amyloidosis)	Light chains of immunoglobulines (most common type)	Monoclonal gammopathy
AA (secondary amyloidosis)	Serum amyloid A protein	Chronic inflammatory diseases
AF	Mutant transthyretin, A1-apolipoprotein, gelsolin, fibrinogen, etc.	Familial polyneuropathy/cardiomyopathy/nephropathy
ATTRwt	Wild-type transthyretin	Senile restrictive cardiomyopathy _ Transthyretin-related amyloidosis wild-type
AH	ß2-microglobulin	Long-term hemodialysis

Amyloidosis also may classified by their organ involvement as below:^[6]^[7]

Classification	subtypes	Causes	Important clinical findings
Systemic amyloidosis	Primary amyloidosis (AL)	Aggregation and deposition of immunoglobulin light chains that usually produced by plasma cell clones	Nephrotic syndrome Restrictive cardiomyopathy Peripheral neuropathy Hepatomegaly with elevated liver enzymes Macroglossia Purpura and an unexplained bleeding diathesis
	Secondary amyloidosis (AA)	Chronic inflammation (TB, familial mediterranean fever, rheumatoid arthritis and multiple myeloma)	Nephrotic syndrome Heart failure
	Hereditary amyloidosis	Amyloidogenic mutations and subsequently deposition of amyloids	Heart failure Arrhythmia
Organ-specific amyloidosis	Renal amyloidosis	Immunoglobulin light-chain amyloidosis (AL amyloidosis) Transthyretin-related amyloidosis (associated with familial/mutant or senile/wild-type TTR)	Proteinuria Nephrotic syndrome Chronic renal failure
	Cardiac amyloidosis		Systolic dysfunction Diastolic dysfunction Arrhythmia
	Hepatic amyloidosis		Hepatomegaly Elevated liver enzymes
	Amyloid neuropathy		Peripheral neuropathy and autonomic neuropathy Neurodegenerative disorders Parkinson, Alzheimer, and Huntington's disease
	Gastrointestinal amyloidosis		Nonspecific findings Dyspepsia, abdominal pain, diarrhea, malabsorption

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.^[8]^[9]
These abnormal amyloids derived from misfolding and aggregation of normally soluble proteins.^[10]
Amyloid deposition can disrupt tissue structure of involved organ and consequently leads to organ failure.^[11]

Systemic Amyloidosis

In systemic amyloidosis, amyloid gradually accumulate and amyloid deposition is widespread in the viscera, blood vessel walls, and in the different connective tissues.^[9]^[10]

Primary Amyloidosis (AL)

Primary amyloidosis (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.
Change in the secondary or tertiary structure of a monoclonal light chain results in abnormal folding of the light chain that abnormally form amyloid fibrils.^[12]
This type of amyloidosis most frequently involve the kidney (usually proteinuria with the nephrotic syndrome) and the heart.^[13]
In primary (AL) amyloidosis survival rate depends on:^[14]
- Type of organ involvement (amyloid heart disease is the main prognostic factor)
- The severity of different organs involvement
- Haematological response to treatment
The median survival of patients with AL amyloidosis is aproximately 3.8 years.^[15]

For more information about primary amyloidosis click here.

Secondary Amyloidosis (AA)

Secondary amyloidosis is associated with chronic inflammation (such as tuberculosis or rheumatoid arthritis).^[13]
Secondary or reactive amyloidosis (AA) is approximately 45% of all systemic amyloidosis.^[16]
Pathogenesis of secondary or reactive amyloidosis is multifactorial that include:
- Primary structure of the precursor protein
- Acute phase response
- Nonfibril proteins (amyloid P component, apo E, GAGs, proteoglycans and basement membrane proteins)
- Receptors
- Lipid metabolism
- Proteases

For more information about secondary amyloidosis click here.

Hereditary Amyloidosis

Hereditary (or familial) amyloidosis are autosomal dominant diseases that inherited variant proteins cause the production and deposition of amyloid fibrils.^[13]
Hereditary amyloidosis are due to amyloidogenic mutations and subsequently deposition of amyloids, include:^[17]
- Transthyretin (TTR) (most common inherited mutation)
- Fibrinogen
- Apolipoprotein A1
- Apolipoprotein A2
- Lysozyme
- Gelsolin genes

Organ-specific Amyloidosis

In this type of amyloidoses, amyloid deposition occurs only in the origin organ or tissue of precursor protein.^[18]
Some neurodegenerative disorders such as Parkinson disease, Alzheimer, and Huntington disease may occur in localized amyloidosis.

Localized amyloidoses can accure due to deposition of intracellular and/or extracellular amyloid.
- Huntington's disease: intracellular protein deposition
- Parkinson's disease: intracellular protein deposition
- Alzheimer's disease: intracellular (Tau protein fibrils) and extracellular (amyloid β fibrils) deposition

Microscopic Pathology

In microscopy pathology of amyloidosis, amyloid is detectable as:^[16]^[13]

Typical green birefringence under polarized light after Congo red staining (appears in 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

Case Studies

Case #1

Template:Metabolic pathology

↑ ^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.
↑ ^2.0 ^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.
↑ Khan MF, Falk RH (November 2001). "Amyloidosis". Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.
↑ Real de Asúa D, Costa R, Galván JM, Filigheddu MT, Trujillo D, Cadiñanos J (2014). "Systemic AA amyloidosis: epidemiology, diagnosis, and management". Clin Epidemiol. 6: 369–77. doi:10.2147/CLEP.S39981. PMC 4218891. PMID 25378951.
↑ Misumi Y, Ando Y (July 2014). "[Classification of amyloidosis]". Brain Nerve (in Japanese). 66 (7): 731–7. PMID 24998818.
↑ Bilginer Y, Akpolat T, Ozen S (August 2011). "Renal amyloidosis in children". Pediatr. Nephrol. 26 (8): 1215–27. doi:10.1007/s00467-011-1797-x. PMC 3119800. PMID 21360109.
↑ 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.
↑ Gillmore JD, Hawkins PN (October 2013). "Pathophysiology and treatment of systemic amyloidosis". Nat Rev Nephrol. 9 (10): 574–86. doi:10.1038/nrneph.2013.171. PMID 23979488.
↑ ^9.0 ^9.1 Baker KR, Rice L (2012). "The amyloidoses: clinical features, diagnosis and treatment". Methodist Debakey Cardiovasc J. 8 (3): 3–7. PMC 3487569. PMID 23227278.
↑ ^10.0 ^10.1 Pepys MB (2006). "Amyloidosis". Annu. Rev. Med. 57: 223–41. doi:10.1146/annurev.med.57.121304.131243. PMID 16409147.
↑ 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.
↑ 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.
↑ ^13.0 ^13.1 ^13.2 ^13.3 Khan MF, Falk RH (November 2001). "Amyloidosis". Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.
↑ 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.
↑ 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.
↑ ^16.0 ^16.1 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.
↑ Mahmood S, Palladini G, Sanchorawala V, Wechalekar A (February 2014). "Update on treatment of light chain amyloidosis". Haematologica. 99 (2): 209–21. doi:10.3324/haematol.2013.087619. PMC 3912950. PMID 24497558.
↑ Blancas-Mejía LM, Ramirez-Alvarado M (2013). "Systemic amyloidoses". Annu. Rev. Biochem. 82: 745–74. doi:10.1146/annurev-biochem-072611-130030. PMC 4044913. PMID 23451869.

[pmid218384133-1] 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.

[pmid10940217-2] 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.

[pmid11677276-3] Khan MF, Falk RH (November 2001). "Amyloidosis". Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.

[pmid25378951-4] Real de Asúa D, Costa R, Galván JM, Filigheddu MT, Trujillo D, Cadiñanos J (2014). "Systemic AA amyloidosis: epidemiology, diagnosis, and management". Clin Epidemiol. 6: 369–77. doi:10.2147/CLEP.S39981. PMC 4218891. PMID 25378951.

[pmid24998818-5] Misumi Y, Ando Y (July 2014). "[Classification of amyloidosis]". Brain Nerve (in Japanese). 66 (7): 731–7. PMID 24998818.

[pmid21360109-6] Bilginer Y, Akpolat T, Ozen S (August 2011). "Renal amyloidosis in children". Pediatr. Nephrol. 26 (8): 1215–27. doi:10.1007/s00467-011-1797-x. PMC 3119800. PMID 21360109.

[pmid28134587-7] 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.

[pmid23979488-8] Gillmore JD, Hawkins PN (October 2013). "Pathophysiology and treatment of systemic amyloidosis". Nat Rev Nephrol. 9 (10): 574–86. doi:10.1038/nrneph.2013.171. PMID 23979488.

[pmid23227278-9] 9.0 ^9.1 Baker KR, Rice L (2012). "The amyloidoses: clinical features, diagnosis and treatment". Methodist Debakey Cardiovasc J. 8 (3): 3–7. PMC 3487569. PMID 23227278.

[pmid16409147-10] 10.0 ^10.1 Pepys MB (2006). "Amyloidosis". Annu. Rev. Med. 57: 223–41. doi:10.1146/annurev.med.57.121304.131243. PMID 16409147.

[pmid26155101-11] 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.

[pmid22909024-12] 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.

[pmid116772762-13] 13.0 ^13.1 ^13.2 ^13.3 Khan MF, Falk RH (November 2001). "Amyloidosis". Postgrad Med J. 77 (913): 686–93. PMC 1742163. PMID 11677276.

[pmid229090242-14] 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.

[pmid21483018-15] 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.

[pmid119640392-16] 16.0 ^16.1 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.

[pmid24497558-17] Mahmood S, Palladini G, Sanchorawala V, Wechalekar A (February 2014). "Update on treatment of light chain amyloidosis". Haematologica. 99 (2): 209–21. doi:10.3324/haematol.2013.087619. PMC 3912950. PMID 24497558.

[pmid23451869-18] Blancas-Mejía LM, Ramirez-Alvarado M (2013). "Systemic amyloidoses". Annu. Rev. Biochem. 82: 745–74. doi:10.1146/annurev-biochem-072611-130030. PMC 4044913. PMID 23451869.

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@@ Line 9: / Line 9: @@
 == 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.<ref name="pmid218384133">{{cite journal |vauthors=Kyle RA |title=Amyloidosis: a brief history |journal=Amyloid |volume=18 Suppl 1 |issue= |pages=6–7 |date=June 2011 |pmid=21838413 |doi=10.3109/13506129.2011.574354001 |url=}}</ref>
+*In 1639, Nicolaus Fontanus [[Autopsy|autopsied]] a young man who had [[ascites]], [[jaundice]], [[liver abscess]] and [[splenomegaly]] and his report has been the first description of amyloidosis.<ref name="pmid218384133">{{cite journal |vauthors=Kyle RA |title=Amyloidosis: a brief history |journal=Amyloid |volume=18 Suppl 1 |issue= |pages=6–7 |date=June 2011 |pmid=21838413 |doi=10.3109/13506129.2011.574354001 |url=}}</ref>
-*In 1854, Rudolph Virchow introduced the term of amyloid as an macroscopic abnormality in some tissues.<ref name="pmid10940217">{{cite journal |vauthors=Sipe JD, Cohen AS |title=Review: history of the amyloid fibril |journal=J. Struct. Biol. |volume=130 |issue=2-3 |pages=88–98 |date=June 2000 |pmid=10940217 |doi=10.1006/jsbi.2000.4221 |url=}}</ref>
+*In 1854, Rudolph Virchow introduced the term of [[amyloid]] as an macroscopic abnormality in some tissues.<ref name="pmid10940217">{{cite journal |vauthors=Sipe JD, Cohen AS |title=Review: history of the amyloid fibril |journal=J. Struct. Biol. |volume=130 |issue=2-3 |pages=88–98 |date=June 2000 |pmid=10940217 |doi=10.1006/jsbi.2000.4221 |url=}}</ref>
-*In 1867, Weber reported the first case of amyloidosis associated with multiple myeloma.<ref name="pmid218384133">{{cite journal |vauthors=Kyle RA |title=Amyloidosis: a brief history |journal=Amyloid |volume=18 Suppl 1 |issue= |pages=6–7 |date=June 2011 |pmid=21838413 |doi=10.3109/13506129.2011.574354001 |url=}}</ref>
+*In 1867, Weber reported the first case of amyloidosis associated with [[multiple myeloma]].<ref name="pmid218384133">{{cite journal |vauthors=Kyle RA |title=Amyloidosis: a brief history |journal=Amyloid |volume=18 Suppl 1 |issue= |pages=6–7 |date=June 2011 |pmid=21838413 |doi=10.3109/13506129.2011.574354001 |url=}}</ref>
-*In 1922, Bennhold introduced Congo red staining of amyloid that remains the gold standard for diagnosis.<ref name="pmid11677276">{{cite journal |vauthors=Khan MF, Falk RH |title=Amyloidosis |journal=Postgrad Med J |volume=77 |issue=913 |pages=686–93 |date=November 2001 |pmid=11677276 |pmc=1742163 |doi= |url=}}</ref>
+*In 1922, Bennhold introduced [[Congo red|Congo red staining]] of [[amyloid]] that remains the [[Gold standard (test)|gold standard]] for [[diagnosis]].<ref name="pmid11677276">{{cite journal |vauthors=Khan MF, Falk RH |title=Amyloidosis |journal=Postgrad Med J |volume=77 |issue=913 |pages=686–93 |date=November 2001 |pmid=11677276 |pmc=1742163 |doi= |url=}}</ref>
-*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.<ref name="pmid10940217">{{cite journal |vauthors=Sipe JD, Cohen AS |title=Review: history of the amyloid fibril |journal=J. Struct. Biol. |volume=130 |issue=2-3 |pages=88–98 |date=June 2000 |pmid=10940217 |doi=10.1006/jsbi.2000.4221 |url=}}</ref><ref name="pmid218384133">{{cite journal |vauthors=Kyle RA |title=Amyloidosis: a brief history |journal=Amyloid |volume=18 Suppl 1 |issue= |pages=6–7 |date=June 2011 |pmid=21838413 |doi=10.3109/13506129.2011.574354001 |url=}}</ref>
+*In 1959, Cohen and Calkins used ultrathin sections of amyloidotic tissues and assessed by [[Electron microscope|electron microscopic]] examination, explained the presence of nonbranching [[Fibril|fibrils]] with indeterminate length and variable width.<ref name="pmid10940217">{{cite journal |vauthors=Sipe JD, Cohen AS |title=Review: history of the amyloid fibril |journal=J. Struct. Biol. |volume=130 |issue=2-3 |pages=88–98 |date=June 2000 |pmid=10940217 |doi=10.1006/jsbi.2000.4221 |url=}}</ref><ref name="pmid218384133">{{cite journal |vauthors=Kyle RA |title=Amyloidosis: a brief history |journal=Amyloid |volume=18 Suppl 1 |issue= |pages=6–7 |date=June 2011 |pmid=21838413 |doi=10.3109/13506129.2011.574354001 |url=}}</ref>
 == Classification ==
@@ Line 23: / Line 23: @@
 !Clinical syndrome
 |-
-|AL (primary amyloidosis)
+|[[Primary amyloidosis|AL (primary amyloidosis)]]
-|Light chains of immunoglobulines (most common type)
+|[[Light chain|Light chains]] of [[Immunoglobulin|immunoglobulines]] (most common type)
-|Monoclonal gammopathy
+|[[Monoclonal gammopathy]]
 |-
-|AA (secondary amyloidosis)
+|[[AA amyloidosis|AA (secondary amyloidosis)]]
-|Serum amyloid A protein
+|[[Serum amyloid A|Serum amyloid A protein]]
-|Chronic inflammatory diseases
+|[[Chronic inflammation|Chronic inflammatory diseases]]
 |-
 |AF
-|Mutant transthyretin, A1-apolipoprotein, gelsolin, fibrinogen, etc.
+|Mutant [[transthyretin]], [[Apolipoprotein A1|A1-apolipoprotein,]] [[gelsolin]], [[fibrinogen]], etc.
-|Familial polyneuropathy/cardiomyopathy/nephropathy
+|Familial [[polyneuropathy]]/[[cardiomyopathy]]/[[nephropathy]]
 |-
 |ATTRwt
-|Wild-type transthyretin
+|Wild-type [[transthyretin]]
-|Senile restrictive cardiomyopathy _ Transthyretin-related amyloidosis wild-type
+|[[Senile]] [[restrictive cardiomyopathy]] _ [[Transthyretin]]-related amyloidosis wild-type
 |-
 |AH
 |ß2-microglobulin
-|Long-term hemodialysis
+|Long-term [[hemodialysis]]
 |}
@@ Line 52: / Line 52: @@
 |-
 | rowspan="3" |Systemic amyloidosis
-|Primary amyloidosis (AL)
+|[[AL amyloidosis|Primary amyloidosis (AL)]]
 |
-* Aggregation and deposition of Ig light chains that usually produced by [[plasma cell]] clones
+* Aggregation and deposition of [[immunoglobulin]] [[Light chain|light chains]] that usually produced by [[plasma cell]] clones
 |
-* Nephrotic syndrome
+* [[Nephrotic syndrome]]
-* Restrictive cardiomyopathy
+* [[Restrictive cardiomyopathy]]
-* Peripheral neuropathy
+* [[Peripheral neuropathy]]
-* Hepatomegaly with elevated liver enzymes
+* [[Hepatomegaly]] with elevated [[liver enzymes]]
-* Macroglossia
+* [[Macroglossia]]
-* Purpura and an unexplained bleeding diathesis
+* [[Purpura]] and an unexplained [[Hemorrhagic diathesis|bleeding diathesis]]
 |-
-|Secondary amyloidosis (AA)
+|[[AA amyloidosis|Secondary amyloidosis (AA)]]
 |
-* Chronic [[inflammation]] (TB, familial mediterranean fever, rheumatoid arthritis and multiple myeloma)
+* Chronic [[inflammation]] ([[Tuberculosis|TB]], [[familial mediterranean fever]], [[rheumatoid arthritis]] and [[multiple myeloma]])
 |
-* Nephrotic syndrome
+* [[Nephrotic syndrome]]
-* Heart failure
+* [[Congestive heart failure|Heart failure]]
 |-
-|Hereditary amyloidosis
+|[[Heredity|Hereditary]] amyloidosis
 |
 * Amyloidogenic [[Mutation|mutations]] and subsequently deposition of [[Amyloid|amyloids]]
 |
-* Heart failure
+* [[Congestive heart failure|Heart failure]]
-* Arrhythmia
+* [[Cardiac arrhythmia|Arrhythmia]]
 |-
 | rowspan="5" |Organ-specific amyloidosis
 |[[Renal amyloidosis]]
 | rowspan="5" |
-* Immunoglobulin light-chain amyloidosis
+* [[AL amyloidosis|Immunoglobulin light-chain amyloidosis (AL amyloidosis)]]
-* Transthyretin-related amyloidosis (associated with familial/mutant or senile/wild-type TTR)
+* [[Transthyretin-related hereditary amyloidosis|Transthyretin-related amyloidosis]] (associated with familial/mutant or senile/wild-type [[Transthyretin|TTR]])
 |
-* Proteinuria
+* [[Proteinuria]]
-* Nephrotic syndrome
+* [[Nephrotic syndrome]]
-* Chronic renal failure
+* [[Chronic renal failure]]
 |-
 |[[Cardiac amyloidosis]]
 |
-* Systolic dysfunction
+* [[Systolic dysfunction]]
-* Diastolic dysfunction
+* [[Diastolic dysfunction]]
-* Arrhythmia
+* [[Cardiac arrhythmia|Arrhythmia]]
 |-
-|Hepatic amyloidosis
+|[[Hepatic amyloidosis with intrahepatic cholestasis|Hepatic amyloidosis]]
 |
-* Hepatomegaly
+* [[Hepatomegaly]]
-* Elevated liver enzymes
+* Elevated [[liver enzymes]]
 |-
 |Amyloid neuropathy
 |
-* Peripheral and autonomic neuropathy
+* [[Peripheral neuropathy]] and [[autonomic neuropathy]]
-* Neurodegenerative disorders
+* [[Neurodegenerative disease|Neurodegenerative disorders]]
-** Parkinson, Alzheimer, and Huntington disease
+** [[Parkinson's disease|Parkinson]], [[Alzheimer's disease|Alzheimer]], and [[Huntington's disease]]
 |-
 |Gastrointestinal amyloidosis
 |
 * Nonspecific findings
-** Dyspepsia, abdominal pain, diarrhea, malabsorption
+** [[Dyspepsia]], [[abdominal pain]], [[diarrhea]], [[malabsorption]]
 |}
@@ Line 167: / Line 167: @@
 {{Metabolic pathology}}
 [[Category:Medicine]]
 <references />