YKL 40

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<StructureSection load='' size='350' side='right' scene='88/881548/Ykl-40/1'>
<StructureSection load='' size='350' side='right' scene='88/881548/Ykl-40/1'>
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<scene name='88/881548/Ykl-40/1'>YKL-40</scene> is a non-enzymatic chitinase-like protein. It is able to bind chitin but does not possess the enzymatic activity needed to cleave chitinase. YKL-40 is the human form of chitinase-3 -like protein 1 also referred to as CHI3L1. It is referred to as YKL because of the three amino acid residues (Y, K, and L) present at the N terminus. The 40 comes from the weight of the protein which is around 40kDa. Previous crystallizations have shown a YKL-40 three-dimensional structure that consists of a (β/α)8- barrel domain. It also has a secondary domain comprised of six antiparallel β-strands with one α-helix (α + β) domain after β7. Full-length genomic chains can be observed in UniProt. The complete structure and 3D analysis can be found in the OCA atlas. A summary of statistical data can be found here. For a complete guided tour, FirstGlance is recommended.
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<scene name='88/881548/Ykl-40/1'>YKL-40</scene> is a non-enzymatic chitinase-like protein. It is able to bind chitin but does not possess the enzymatic activity needed to cleave chitinase. YKL-40 is the human form of chitinase-3 -like protein 1 also referred to as CHI3L1. It is referred to as YKL because of the three amino acid residues (Y, K, and L) present at the N terminus. The 40 comes from the weight of the protein which is around 40kDa. Previous crystallizations have shown a YKL-40 three-dimensional structure that consists of a (β/α)8- barrel domain. It also has a secondary domain comprised of six antiparallel β-strands with one α-helix (α + β) domain after β7. Full-length genomic chains can be observed in UniProt. The complete structure and 3D analysis can be found in the OCA atlas. A summary of statistical data can be found here. For a complete guided tour, [http://oca.weizmann.ac.il/oca-bin/ocashort?id=1NWR FirstGlance] is recommended.
== Function ==
== Function ==
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In neurodegenerative conditions such as Alzheimer’s and Parkinson’s, YKL-40 can serve as a biomarker. It is highly disease-specific. Neuroinflammation has been linked as a contributor to different forms of dementia. Particularly in Alzheimer’s disease, elevated YKL-40 levels were seen in clusters around β-amyloid plaques. The distribution of YKL-40 is even between the white and gray matter of the brain. Interestingly, YKL-40 levels are not elevated in dementia with Lewy bodies. YKL-40 is currently being investigated as a blood-based biomarker for the diagnosis of clinical neurodegenerative disease.
In neurodegenerative conditions such as Alzheimer’s and Parkinson’s, YKL-40 can serve as a biomarker. It is highly disease-specific. Neuroinflammation has been linked as a contributor to different forms of dementia. Particularly in Alzheimer’s disease, elevated YKL-40 levels were seen in clusters around β-amyloid plaques. The distribution of YKL-40 is even between the white and gray matter of the brain. Interestingly, YKL-40 levels are not elevated in dementia with Lewy bodies. YKL-40 is currently being investigated as a blood-based biomarker for the diagnosis of clinical neurodegenerative disease.
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== Relevance ==
 
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This is a sample scene created with SAT to <scene name="/12/3456/Sample/1">color</scene> by Group, and another to make <scene name="/12/3456/Sample/2">a transparent representation</scene> of the protein. You can make your own scenes on SAT starting from scratch or loading and editing one of these sample scenes.
 
</StructureSection>
</StructureSection>
== References ==
== References ==
<references/>
<references/>

Revision as of 17:45, 29 April 2021

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Safa Ahmed, Michal Harel

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