Information about Amyloid
Amyloids are insoluble fibrous protein aggregations sharing specific structural traits.
Amyloid polymerization is generally sequence-sensitive, that is, causing mutations in the sequence can prevent self-assembly, especially if the mutation is a beta-sheet breaker, such as proline. For example, humans produce an amyloidogenic peptide associated with type II diabetes, but, in Rodentia, a proline is substituted in a critical location and amyloidogenesis does not occur.
There are two broad classes of amyloid-forming polypeptide sequences. Glutamine-rich polypeptides are important in the amyloidogenesis of Yeast and mammalian prions, as well as Huntington's disease. When peptides are in a beta-sheet conformation, particularly when the residues are parallel and in-register (causing alignment), glutamines can brace the structure by forming intrastrand hydrogen bonding between its amide carbonyls and nitrogens. In general, for this class of diseases, toxicity correlates with glutamine content. This has been observed in studies of onset age for Huntington's disease (the longer the polyglutamine sequence, the sooner the symptoms appear), and has been confirmed in a C. elegans model system with engineered polyglutamine peptides.
Other polypeptides and proteins such as amylin and the Alzheimer's beta protein do not have a simple consensus sequence and are thought to operate by hydrophobic association. Among the hydrophobic residues, aromatic amino-acids are found to have the highest amyloidogenic propensity.
For these peptides, cross-polymerization (fibrils of one polypeptide sequence causing other fibrils of another sequence to form) is a phenomenon observed in vitro. This phenomenon is important since it would explain interspecies prion propagation and Amyloid biophysics differential rates of propagation, as well as a statistical link between Alzheimer's and diabetes. In general, cross-polymerization is more efficient the more similar the peptide sequence, though entirely dissimilar sequences can cross-polymerize and highly similar sequences can even be "blockers" which prevent polymerization. Polypeptides will not cross-polymerize their mirror-image counterparts, indicating that the phenomenon involves specific binding and recognition events.
Xu [4], using atomic force microscopy, has shown in both lysozyme and human tau40 that formation of amyloid fibers is a two-step process in which proteins first aggregate into uniform colloidal spheres of ~20nm diameter. The spheres then join to form characteristic linear chains, which evolve over time into mature amyloid fibers. He proposes that aggregation drives conformational change and that a conformational change is not essential to initiate the aggregation process.
Definition controversy
The name amyloid comes from the early mistaken identification of the substance as starch (amylum in Latin), based on crude iodine-staining techniques. For a period, the scientific community debated whether or not amyloid deposits were fatty deposits or carbohydrate deposits until it was finally resolved that it was neither, but rather a deposition of proteinaceous mass.[1]- The classical, histopathological definition of amyloid is an extracellular, proteinaceous deposit exhibiting cross-beta structure. This is due to mis-folding of unstable proteins. Common to most cross-beta type structures they are generally identified by apple-green birefringence when stained with congo red and seen under polarized light. These deposits often recruit various sugars and other components such as Serum Amyloid P component, resulting in complex, and sometimes inhomogenous structures.[2] Recently this definition has come into question as some classic, amyloid species have been observed in distinctly intracellular locations.
- A more recent, biophysical definition is broader, including any polypeptide which adopts a cross-beta polymerization, in vivo, or in vitro. Some of these, although demonstrably cross-beta sheet, fail other characteristic tests of amyloid, such as the congo red birefringence test. Microbiologists and biophysicists have largely adopted this definition, leading to some conflict in the biological community over an issue of language.
Diseases featuring amyloids
- Medulary Carcinoma of the Thyroid
- Amyloidosis
- Alzheimer's disease
- Transmissible spongiform encephalopathy
- Yeast Prions [Sup35] [3], Rnq1
- Sporadic Inclusion Body Myositis (S-IBM)
Non-disease amyloids
(mostly using the biophysical definition)- Native amyloids in organisms
- Curli E. coli Protein (curlin)
- Podospora Anserina Prion Het-s
- Malarial coat protein
- Spider silk (some but not all spiders)
- Mammalian melanosomes (pMel)
- Tissue-type plasminogen activator (tPA), a hemodynamic factor
- Proteins and peptides known to make amyloid without any known disease
- Calcitonin
- Proteins and peptides engineered to make amyloid
Amyloid biophysics
Amyloid is characterized by a cross-beta sheet quaternary structure; that is, the strands come from different monomers and align perpendicular to the axis of the fibril. While amyloid is usually identified using fluorescent dyes, stain polarimetry, circular dichroism, or FTIR (all indirect measurements), the "gold-standard" test to see if a structure contains cross-beta fibres is by placing a sample in an X-ray diffraction beam; there are two characteristic scattering diffraction signals produced at 4.7 and 10 Ã…ngstroms (0.47 nm and 1.0 nm), corresponding to the interstrand and stacking distances in beta sheets. It should be noted that the "stacks" of beta sheet are short and traverse the breadth of the amyloid fibril; the length of the amyloid fibril is built by aligned strands.Amyloid polymerization is generally sequence-sensitive, that is, causing mutations in the sequence can prevent self-assembly, especially if the mutation is a beta-sheet breaker, such as proline. For example, humans produce an amyloidogenic peptide associated with type II diabetes, but, in Rodentia, a proline is substituted in a critical location and amyloidogenesis does not occur.
There are two broad classes of amyloid-forming polypeptide sequences. Glutamine-rich polypeptides are important in the amyloidogenesis of Yeast and mammalian prions, as well as Huntington's disease. When peptides are in a beta-sheet conformation, particularly when the residues are parallel and in-register (causing alignment), glutamines can brace the structure by forming intrastrand hydrogen bonding between its amide carbonyls and nitrogens. In general, for this class of diseases, toxicity correlates with glutamine content. This has been observed in studies of onset age for Huntington's disease (the longer the polyglutamine sequence, the sooner the symptoms appear), and has been confirmed in a C. elegans model system with engineered polyglutamine peptides.
Other polypeptides and proteins such as amylin and the Alzheimer's beta protein do not have a simple consensus sequence and are thought to operate by hydrophobic association. Among the hydrophobic residues, aromatic amino-acids are found to have the highest amyloidogenic propensity.
For these peptides, cross-polymerization (fibrils of one polypeptide sequence causing other fibrils of another sequence to form) is a phenomenon observed in vitro. This phenomenon is important since it would explain interspecies prion propagation and Amyloid biophysics differential rates of propagation, as well as a statistical link between Alzheimer's and diabetes. In general, cross-polymerization is more efficient the more similar the peptide sequence, though entirely dissimilar sequences can cross-polymerize and highly similar sequences can even be "blockers" which prevent polymerization. Polypeptides will not cross-polymerize their mirror-image counterparts, indicating that the phenomenon involves specific binding and recognition events.
Xu [4], using atomic force microscopy, has shown in both lysozyme and human tau40 that formation of amyloid fibers is a two-step process in which proteins first aggregate into uniform colloidal spheres of ~20nm diameter. The spheres then join to form characteristic linear chains, which evolve over time into mature amyloid fibers. He proposes that aggregation drives conformational change and that a conformational change is not essential to initiate the aggregation process.
Amyloid pathology
The reasons for amyloid association with disease is unclear. In many cases, the deposits physically disrupt tissue architecture, suggesting disruption of function by some bulk process. In other cases, cell death is believed to precede amyloid deposition, suggesting small amyloid-like oligomers (possibly but not necessarily biophysically amyloid) cause cell death. There is significant speculation that amyloid fibrils can also puncture cells or cause problems such as ionic imbalance in cells. Further speculation has led to the hypothesis that while amyloid association may be the cause of health issues, the association itself is initiated by an underlying problem, such as one/some of the above mentioned side effects like calcium ion concentration imbalances.Histological staining
Amyloid is typically identified by a change in the fluorescence intensity of planar aromatic dyes such as Thioflavin T or Congo Red. Congo red postitivity remains the gold standard for diagnosis of amyloidosis. This is generally attributed to the environmental change, as these dyes intercalate between beta-strands. Congophillic amyloid plaques generally cause apple-green birefringence, when viewed through crossed polarimetric filters. To avoid nonspecific staining, histology stains, such as haematoxylin and eosin stain, are used to quench the dyes' activity in other places where the dye might bind, such as the nucleus. The dawn of antibody technology and immunohistochemistry has made specific staining easier, but often this can cause trouble because epitopes can be concealed in the amyloid fold; an amyloid protein structure is generally a different conformation from that which the antibody recognizes.See also
References
1. ^ Kyle, R.A. (2001) Amyloidosis: a convoluted story. Brit. J. Haem. 114:529-538. PMID 11552976
2. ^ Sipe, J. D. and Cohen, A.S. (2000) Review: History of the Amyloid Fibril. J. Struct. Biol. 130:88-98. PMID 10940217
3. ^ Nakayashiki, PNAS, 2005
4. ^ Xu S. Aggregation drives "misfolding" in protein amyloid fiber formation. Amyloid 2007 Jun;14(2):119-31. PMID 17577685
2. ^ Sipe, J. D. and Cohen, A.S. (2000) Review: History of the Amyloid Fibril. J. Struct. Biol. 130:88-98. PMID 10940217
3. ^ Nakayashiki, PNAS, 2005
4. ^ Xu S. Aggregation drives "misfolding" in protein amyloid fiber formation. Amyloid 2007 Jun;14(2):119-31. PMID 17577685
External links
- [https://www.bachem.com/bachem/bachem/tree.cfm?id=241&showchildren=G12&level=G12#G12 Amyloid Peptides] at Bachem.com
- Amyloid Precursor Protein, CTF fragments at rpeptide.com
- Amyloid Treatment and Research Program at Boston University
- Amyloid: Journal of Protein Folding Disorders web page at tandf.co.uk
- Amyloidosis web page at Cornell University
- Information, support and advice to anyone with Amyloidosis, particularly in Australia (www.amyloidosisaustralia.org)
- Amyloidosis Support Network at amyloidosis.org
- UK National Amyloidosis Centre - one of the largest amyloid diagnosis and research centres at ucl.ac.uk
- Engineering Amyloid for material at University of California, Berkeley
- Amyloidosis Research Foundation amyloidosisresearchfoundation.org
- National Kidney and Urologic Diseases Information Clearinghouse at National Institute of Health
- Eubanks L, Rogers C, Beuscher A, Koob G, Olson A, Dickerson T, Janda K (2006). "A molecular link between the active component of marijuana and Alzheimer's disease pathology". Mol. Pharm. 3 (6): 773-7. PMID 17140265.
Proteins are large organic compounds made of amino acids arranged in a linear chain and joined together by peptide bonds between the carboxyl and amino groups of adjacent amino acid residues.
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Starch (CAS# 9005-25-8, chemical formula (C6H10O5)n,[1]) is a mixture of amylose and amylopectin (usually in 20:80 or 30:70 ratios).
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Latin}}}
Official status
Official language of: Vatican City
Used for official purposes, but not spoken in everyday speech
Regulated by: Opus Fundatum Latinitas
Roman Catholic Church
Language codes
ISO 639-1: la
ISO 639-2: lat
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Official status
Official language of: Vatican City
Used for official purposes, but not spoken in everyday speech
Regulated by: Opus Fundatum Latinitas
Roman Catholic Church
Language codes
ISO 639-1: la
ISO 639-2: lat
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Lipids can be broadly defined as any fat-soluble (hydrophobic), naturally-occurring molecules. The term is more-specifically used to refer to fatty-acids and their derivatives (including tri-, di-, and monoglycerides and phospholipids) as well as other fat-soluble sterol-containing
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Histopathology (from the Greek histos (tissue) and pathos (suffering)) refers to the microscopic examination of tissue in order to study the manifestations of disease.
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Birefringence, or double refraction, is the decomposition of a ray of light into two rays (the ordinary ray and the extraordinary ray) when it passes through certain types of material, such as calcite crystals or boron nitride, depending on the polarization of
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Congo red is the sodium salt of benzidinediazo-bis-1-naphtylamine-4-sulfonic acid (formula: C32H22N6Na2O6S2; molecular weight: 696.66 g/mol). It is a secondary diazo dye.
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polarization (Brit., polarisation) is the property of electromagnetic waves, such as light, that describes the direction of the transverse electric field. More generally, the polarization of a transverse wave describes the direction of oscillation in the plane
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Serum Amyloid P component (SAP) is the identical serum form of Amyloid P component (AP), a 25kDa pentameric protein first identified as the pentagonal constituent of in vivo pathological deposits called "amyloid" (Cathcart et al, 1967).
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In linguistics, prescription can refer both to the codification and the enforcement of rules governing how a language is to be used. These rules can cover such topics as standards for spelling and grammar or syntax; or rules for what is deemed socially or politically correct.
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MeSH D000686
In medicine, amyloidosis refers to a variety of conditions in which amyloid proteins are abnormally deposited in organs and/or tissues, causing disease.
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In medicine, amyloidosis refers to a variety of conditions in which amyloid proteins are abnormally deposited in organs and/or tissues, causing disease.
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Alzheimer's disease
Classification & external resources
Histopathologic image of senile plaques seen in the cerebral cortex in a patient with Alzheimer disease of presenile onset. Silver impregnation.
ICD-10 G 30. , F 00.
ICD-9 331.0 , 290.
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Classification & external resources
Histopathologic image of senile plaques seen in the cerebral cortex in a patient with Alzheimer disease of presenile onset. Silver impregnation.
ICD-10 G 30. , F 00.
ICD-9 331.0 , 290.
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Transmissible spongiform encephalopathies (TSEs, also known as prion diseases) are a group of progressive conditions that affect the brain and nervous system of humans and animals and are transmitted by prions.
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E. coli
Binomial name
Escherichia coli
(Migula 1895)
Castellani and Chalmers 1919
Escherichia coli (IPA: [ˌɛ.
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Binomial name
Escherichia coli
(Migula 1895)
Castellani and Chalmers 1919
Escherichia coli (IPA: [ˌɛ.
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Malaria
Classification & external resources
Plasmodium falciparum ring-forms and gametocytes in human blood.
ICD-10 B 50.
ICD-9 084
OMIM 248310
DiseasesDB 7728
MedlinePlus 000621
eMedicine med/1385 emerg/305 ped/1357
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Classification & external resources
Plasmodium falciparum ring-forms and gametocytes in human blood.
ICD-10 B 50.
ICD-9 084
OMIM 248310
DiseasesDB 7728
MedlinePlus 000621
eMedicine med/1385 emerg/305 ped/1357
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Spider silk, also known as gossamer, is a fiber spun by spiders. Spider silk is a remarkably strong material. Its tensile strength is comparable to that of high-grade steel — according to Nature[1], spider dragline silk has a tensile strength of roughly 1.
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melanosome is an organelle containing melanin, the most common light-absorbing pigment found in the animal kingdom.
Cells which contain melanosomes are called melanocytes, and also the retinal pigment epithelium cells, whereas cells which have merely engulfed the melanosomes
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Cells which contain melanosomes are called melanocytes, and also the retinal pigment epithelium cells, whereas cells which have merely engulfed the melanosomes
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Calcitonin is a 32 amino acid polypeptide hormone that is produced in humans primarily by the parafollicular (also known as C) cells of the thyroid, and in many other animals in the ultimobranchial body.
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β sheet (also β-pleated sheet) is the second form of regular secondary structure in proteins — the first is the alpha helix — consisting of beta strands
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In biochemistry, quaternary structure is the arrangement of multiple folded protein molecules in a multi-subunit complex.
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Description and examples
Many proteins are actually assemblies of more than one polypeptide chain, which in the context of the larger assemblage are..... Click the link for more information.
X-rays (or Röntgen rays) are a form of electromagnetic radiation with a wavelength in the range of 10 to 0.01 nanometers, corresponding to frequencies in the range 30 PHz to 30 EHz. X-rays are primarily used for diagnostic radiography and crystallography.
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1 ångström =
SI units
010−12 m 010−3 nm
Natural units
01024 lP 0 a0
US customary / Imperial units
010−12 ft 010−9
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SI units
010−12 m 010−3 nm
Natural units
01024 lP 0 a0
US customary / Imperial units
010−12 ft 010−9
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polymer is a substance composed of molecules with large molecular mass composed of repeating structural units, or monomers, connected by covalent chemical bonds. The word is derived from the Greek, πολυ, polu, "many"; and μέρος, meros,
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Rodentia
Bowdich, 1821
Suborders
Sciuromorpha
Castorimorpha
Myomorpha
Anomaluromorpha
Hystricomorpha
Rodentia is an order of mammals also known as rodents
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Bowdich, 1821
Suborders
Sciuromorpha
Castorimorpha
Myomorpha
Anomaluromorpha
Hystricomorpha
Rodentia is an order of mammals also known as rodents
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Prion Diseases (TSEs)
Classification & external resources
ICD-10 A81
ICD-9 046
A prion (IPA: /ˈpriːɒn/[1]
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Classification & external resources
ICD-10 A81
ICD-9 046
A prion (IPA: /ˈpriːɒn/[1]
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elegans
Binomial name
Caenorhabditis elegans
Maupas, 1900
Caenorhabditis elegans (IPA:
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Binomial name
Caenorhabditis elegans
Maupas, 1900
Caenorhabditis elegans (IPA:
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Amylin, or Islet Amyloid Polypeptide (IAPP), is a 37-residue peptide hormone secreted by pancreatic β-cells at the same time as insulin (in a roughly 100:1 ratio).
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Function
Amylin functions as part of the endocrine pancreas and contributes to glycemic control...... Click the link for more information.
Prion Diseases (TSEs)
Classification & external resources
ICD-10 A81
ICD-9 046
A prion (IPA: /ˈpriːɒn/[1]
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Classification & external resources
ICD-10 A81
ICD-9 046
A prion (IPA: /ˈpriːɒn/[1]
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Herod_Archelaus