hidden pixel

Amyloidosis Information

In medicine, amyloidosis refers to a variety of conditions in which amyloid proteins are abnormally deposited in organs and/or tissues. A protein is described as being amyloid if, due to an alteration in its secondary structure, it takes on a particular aggregated insoluble form similar to the beta-pleated sheet.[1] Symptoms vary widely depending upon the site of amyloid deposition. Amyloidosis may be inherited or acquired.[2]

Contents

Classification of amyloid

The modern classification of amyloid disease tends to use an abbreviation of the protein that makes the majority of deposits, prefixed with the letter A. For example amyloidosis caused by transthyretin is termed "ATTR." Deposition patterns vary between patients but are almost always composed of just one amyloidogenic protein. Deposition can be systemic (affecting many different organ systems) or organ-specific. Many amyloidoses are inherited, due to mutations in the precursor protein. Other forms are due to different diseases causing overabundant or abnormal protein production - such as with over production of immunoglobulin light chains in multiple myeloma (termed AL amyloid), or with continuous overproduction of acute phase proteins in chronic inflammation (which can lead to AA amyloid).

Out of the approximately 60 amyloid proteins that have been identified so far,[3] at least 36 have been associated in some way with a human disease.[4]

Pathogenesis

When a native cell creates a protein, it could either make the actual protein or protein fragments. These fragments could come and join together to form the actual protein. This protein can sometimes regress into the protein fragments. This process of "flip flopping" happens frequently in certain proteins, especially the ones that cause this disease. The fragments or actual proteins are at risk of mis-folding as they are synthesized, to make a bad protein. This causes proteolysis, which is the directed degradation of proteins by cellular enzymes called proteases or by intramolecular digestion; proteases come and digest the mis-folded fragments and proteins. The problem occurs when the proteins do not dissolve in proteolysis. This happens because the mis-folded proteins sometimes become robust enough that they are not dissolved by normal proteolysis. When the fragments do not dissolve they get spit out of proteolysis and they aggregate to form oligomers. The reason they aggregate is that the parts of the protein that do not dissolve in proteolysis are the β-pleated sheets, which are extremely hydrophobic. They are usually sequestered in the middle of the protein, while parts of the protein that are more soluble are found near the outside. When they are exposed to water, these hydrophobic pieces tend to aggregate with other hydrophobic pieces. This ball of fragments gets stabilized by GAG's (glycosaminoglycans) and SAP (serum amyloid P- a component found in amyloid aggregations that is thought to stabilize them and prevent proteolytic cleavage). These stabilized balls of protein fragments are called oligomers . The oligomers can aggregate together and further stabilize to make amyloid fibrils. Both the oligomers and amyloid fibrils can cause cell toxicity and organ dysfunction.[5]

Classification

The names of the amyloid usually start with the letter "A". Following is a brief description of the more common types of amyloid:

Official abb. Amyloid type/Gene Description OMIM
AL amyloid light chain AL amyloidosis / multiple myeloma. Contains immunoglobulin light-chains (λ,κ) derived from plasma cells. 254500
AA SAA AA amyloidosis
β amyloid/APP Found in Alzheimer disease brain lesions. 605714
ATTR transthyretin A mutant form of a normal serum protein that is deposited in the genetically determined familial amyloid polyneuropathies. TTR is also deposited in the heart in senile systemic amyloidosis.[6] Also found in Leptomeningeal amyloidosis. 105210
2M β2 microglobulin Not to be confused with , β2m is a normal serum protein, part of major histocompatibility complex (MHC) Class 1 molecules. Haemodialysis-associated amyloidosis
AIAPP amylin Found in the pancreas of patients with type 2 diabetes.
APrP prion protein In prion diseases, misfolded prion proteins deposit in tissues and resemble amyloid proteins. Some examples are Creutzfeldt–Jakob disease (humans), BSE or "mad cow disease" (cattle), and scrapie (sheep and goats). 123400
AGel GSN Finnish type amyloidosis 105120
ACys CST3 Cerebral amyloid angiopathy, Icelandic-type 105150
AApoA1 APOA1 Familial visceral amyloidosis 105200
AFib FGA Familial visceral amyloidosis 105200
ALys LYZ Familial visceral amyloidosis 105200
? OSMR Primary cutaneous amyloidosis 105250
ABri ADan ITM2B Cerebral amyloid angiopathy, British-type Danish-type 176500 117300
APro prolactin Prolactinoma
AKer keratoepithelin Familial corneal amyloidosis
AANF atrial natriuretic factor Senile amyloid of atria of heart
ACal calcitonin Medullary carcinoma of the thyroid

As of 2010, there were 27 human and nine animal fibril proteins classified, along with eight inclusion bodies.[7]

Symptoms

There are numerous symptoms that are associated with this disease. The most common ones have to do with the heart, such as heart failure, arrhythmia, and an irregular heart beat. Also the respiratory tract can be affected and cause hemoptysis. Usually the spleen enlarges and sometimes ruptures. The gastrointestinal tract is usually affected and causes vomiting, hemorrhaging and diarrhea. The amyloidosis can also affect the motor functions and cause polyneuropathy. When the amyloid fibrils and oligomers get to the skin they can cause skin lesions and petechiae. One of the most famous symptoms is macroglossia.[5]

Diagnosis

If the diagnosis of amyloidosis is suspected, a biopsy (tissue sample)of abdominal wall fat, the rectum or a salivary gland can be examined for evidence of characteristic amyloid deposits. The tissue is treated with various stains. The most useful stain in the diagnosis of amyloid is Congo red, which combined with polarized light makes the amyloid proteins appear apple-green on microscopy. Alternatively, the thioflavin T stain may be used.[8] An abdominal wall fat biopsy is not completely sensitive, and sometimes biopsy of an involved organ (such as the kidney) is required to achieve a diagnosis.[8]

The nature of the amyloid protein can be determined by various ways: the detection of abnormal proteins in the bloodstream (on protein electrophoresis or light chain determination), binding of particular antibodies to the amyloid found in the tissue, or extraction of the protein and identification of its individual amino acids.[8]

Alternative classifications

An older, clinical, method of classification refers to the amyloidoses as systemic or localised

Another classification is primary or secondary.

Additional images

See also

References

  1. ^ "Atlas of Pathology". https://www-s.med.uiuc.edu/m2/pathology/PathAtlasf/CVAtlas020.html.
  2. ^ Pavelka, Margit; Roth, Jürgen. Functional Ultrastructure: An Atlas of Tissue Biology and Pathology. Springer. pp. 258. ISBN 3-211-83564-4.
  3. ^ Mok KH, Pettersson J, Orrenius S, Svanborg C (March 2007). "HAMLET, protein folding, and tumor cell death". Biochem. Biophys. Res. Commun. 354 (1): 1–7. doi:10.1016/j.bbrc.2006.12.167. PMID 17223074.
  4. ^ Pettersson-Kastberg J, Aits S, Gustafsson L, et al. (November 2008). "Can misfolded proteins be beneficial? The HAMLET case". Ann. Med. 41 (3): 1–15. doi:10.1080/07853890802502614. PMID 18985467.
  5. ^ a b [1], Karp, Judith E., ed. Amyloidosis Diagnosis and Treatment. Rochester: Humana, 2010. Online Source. .
  6. ^ Hassan W, Al-Sergani H, Mourad W, Tabbaa R (2005). "Amyloid heart disease. New frontiers and insights in pathophysiology, diagnosis, and management". Tex Heart Inst J 32 (2): 178–84. PMC 1163465. PMID 16107109. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=1163465.
  7. ^ Sipe JD, Benson MD, Buxbaum JN, et al. (September 2010). "Amyloid fibril protein nomenclature: 2010 recommendations from the nomenclature committee of the International Society of Amyloidosis". Amyloid 17 (3–4): 101–104. doi:10.3109/13506129.2010.526812. PMID 21039326. http://informahealthcare.com/doi/abs/10.3109/13506129.2010.526812.
  8. ^ a b c Dember LM (December 2006). "Amyloidosis-associated kidney disease". J. Am. Soc. Nephrol. 17 (12): 3458–71. doi:10.1681/ASN.2006050460. PMID 17093068. http://jasn.asnjournals.org/content/17/12/3458.long.
  9. ^ a b c Table 5-12 in: Mitchell, Richard Sheppard; Kumar, Vinay; Abbas, Abul K.; Fausto, Nelson (2007). Robbins Basic Pathology. Philadelphia: Saunders. ISBN 1-4160-2973-7. 8th edition.

External links

· · Metabolic disease: amyloidosis (E85, 277.3)
Common amyloid forming proteins AA · ATTR · Aβ2M · AL · /APP · AIAPP · ACal · APro · AANF · ACys · ABri
Systemic amyloidosis AL amyloidosis · AA amyloidosis · Aβ2M/Haemodialysis-associated amyloidosis · AGel/Finnish type amyloidosis · AA/Familial Mediterranean fever · ATTR/Transthyretin-related hereditary amyloidosis
Organ-limited amyloidosis
Heart AANF/Isolated atrial amyloidosis
Brain Familial amyloid neuropathy · ACys+ABri/Cerebral amyloid angiopathy · Aβ/Alzheimer's disease
Kidney AApoA1+AFib+ALys/Familial renal amyloidosis
Cutaneous Primary cutaneous amyloidosis · Amyloid purpura
Endocrine Thyroid: ACal/Medullary thyroid cancer Pituitary: APro/Prolactinoma Pancreas: AIAPP/Insulinoma · AIAPP/Diabetes mellitus type 2

Categories:

 

The above information uses material from Wikipedia and is licensed under the GNU Free Documentation License.
Some facts may not have been fully verified for accuracy. [Disclaimers]
This page was last archived by our server on Fri Nov 4 00:14:46 2011.
Displaying this page or its contents does not use any Wikimedia Foundation's resources.
The owners of this site proudly support the Wikimedia Foundation.

More Information Results for "Amyloidosis"
[Hide]▼
'Amyloidosis' Images
[Hide]▲