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Contents

   



(Top)
 


1 Rationale  





2 History & Funding  





3 Focal point  





4 The goal  





5 Database Content  





6 Usage  





7 References  





8 PMAP disambiguation  





9 External links  





10 See also  














The Proteolysis Map: Difference between revisions






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==Focal point==

==Focal point==

[[Proteases]] are a class of [[enzymes]] that regulate much of what happens in the [[human]] body, both inside the [[cell]] and out, by cleaving [[peptide bonds]] in [[proteins]]. Extensive on-line classification system for [[proteases]] (also referred as peptidases) is deposited in [[MEROPS database]]. Through this activity, they govern the four essential cell functions: [[differentiation]], [[motility]], division and death—and activate important extracelluar [[episodes]], such as the cascading effect in [[blood clotting]]. Simply stated, life could not exist without them.

[[Proteases]] are a class of [[enzymes]] that regulate much of what happens in the [[human body]], both inside the [[cell]] and out, by cleaving [[peptide bonds]] in [[proteins]]. Extensive on-line classification system for [[proteases]] (also referred as peptidases) is deposited in [[MEROPS database]]. Through this activity, they govern the four essential cell functions: [[differentiation]], [[motility]], division and [[cell death]] — and activate important extracelluar episodes, such as the [[biochemical cascading]] effect in [[blood clotting]]. Simply stated, [[life]] could not exist without them.



==The goal==

==The goal==


Revision as of 15:46, 7 November 2008

PMAP logo

The Proteolysis MAP (PMAP) is an integrated web resource focused on proteases[1].

Rationale

PMAP is to aid the protease researchers in reasoning about proteolytic networks and pathways.

History & Funding

PMAP was originally created at the Burnham Institute for Medical Research, La Jolla, California. In 2004 the National Institutes of Health (NIH) selected a team led by Jeffrey W. Smith, Ph.D., to establish the Center on Proteolytic Pathways (CPP). As part of the NIH Roadmap for Biomedical research, the center develops technology to study the behavior of proteins and to disburse that knowledge to the scientific community at large. Funding: National Institutes of Health (RR020843, CA108959 GenBank , CA30199). Funding for open access charge: National Institutes of Health (RR020843, CA108959 GenBank , CA30199).

Focal point

Proteases are a class of enzymes that regulate much of what happens in the human body, both inside the cell and out, by cleaving peptide bondsinproteins. Extensive on-line classification system for proteases (also referred as peptidases) is deposited in MEROPS database. Through this activity, they govern the four essential cell functions: differentiation, motility, division and cell death — and activate important extracelluar episodes, such as the biochemical cascading effect in blood clotting. Simply stated, life could not exist without them.

The goal

Proteolytic pathways, or proteolysis, are the series of events controlled by proteases that occur in response to specific stimuli. In addition to the clotting of blood, the production of insulin can be viewed as a proteolytic pathway, as the activation, regulation and inhibition of that protein is the result of proteases reacting to changing glucose levels and triggering other proteases downstream.

Database Content

PMAP integrates five databases (DBs), linked together in one environment. (1)ProteaseDB and (2)SubstrateDB, are driven by an automated annotation pipeline that generates dynamic ‘Molecule Pages’, rich in molecular information. (3)CutDB[2] has information on more than 6,600 proteolytic events, and (4)ProfileDB is dedicated to information of the substrate recognition specificity of proteases. (5)PathwayDB, just begun accumulation of pathways whose function can be dynamically modeled in a rule-based manner. Hypothetical networks are inferred by semi-automated culling of the literature. Additionally, protease software tools are available for the analysis of individual proteases and proteome-wide data sets.

Usage

Popular destinations in PMAP are Protease Molecule Pages and Substrate Molecule Pages. Protease Molecule Pages show recent news in PubMed literature of the protease, known proteolytic events, protein domain location and protein structure view, as well as a cross annotation in other bioinformatic databases section. Substrate Molecule Pages display protein domains and experimental protease cut sites for a given protein target of interest.

References

  1. ^ Igarashi Y, Heureux E, Doctor KS, Talwar P, Gramatikova S, Gramatikoff K, Zhang Y, Blinov M, Ibragimova SS, Boyd S, Ratnikov B, Cieplak P, Godzik A, Smith JW, Osterman AL, Eroshkin AM. PMAP: databases for analyzing proteolytic events and pathways. Nucleic Acids Res. 2008 Oct 8.[Epub ahead of print]
  • ^ Igarashi Y, Eroshkin A, Gramatikova S, Gramatikoff K, Zhang Y, Smith JW, Osterman AL, Godzik A. CutDB: a proteolytic event database. Nucleic Acids Res. 2007 D546-9
  • PMAP disambiguation

    The Proteolysis Map (PMAP) should not be confused with other acronyms:

    Acronyms:

    Individual protein names:

    Management & organizations:

    Products:

    UNIX/Linux/Basic commands:

    SUN port mapper:

    External links

    See also


  • t
  • e
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  • Retrieved from "https://en.wikipedia.org/w/index.php?title=The_Proteolysis_Map&oldid=250252496"

    Categories: 
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    Bioinformatics databases
    Bioinformatics software
    Systems biology
    Mathematical biology
    EC 3.4
    Posttranslational modification
    EC 3.4.22
    Programmed cell death
    Apoptosis
    Protein domains
    Protein families
    Peripheral membrane proteins
    Enzyme stubs
    Bioinformatics stubs
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    This page was last edited on 7 November 2008, at 15:46 (UTC).

    This version of the page has been revised. Besides normal editing, the reason for revision may have been that this version contains factual inaccuracies, vandalism, or material not compatible with the Creative Commons Attribution-ShareAlike License.



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