My watch list
my.bionity.com  

my.bionity.com

With an accout for my.bionity.com you can always see everything at a glance – and you can configure your own website and individual newsletter.

  • My watch list
  • My saved searches
  • My saved topics
  • My newsletter
Register free of charge
Login  
eng  
DeutschEnglishFrançaisEspañol

HLA-DP



major histocompatibility complex, class II, DP
Structure
Type Cell surface receptor
Quartenary αβ-heterodimer
MMDB None available
Identifiers
alpha 1
Symbol(s) HLA-DPA1
Entrez 3113
OMIM 142880
RefSeq NM_003355 ?
UniProt P20036
Identifiers
beta 1
Symbol(s) HLA-DPB1
Entrez 4940
OMIM 142858
RefSeq NM_002121 ?
UniProt P04440
Shared data
Locus chr.6 6p21.31

HLA-DP is a protein/peptide-antigen receptor and graft-versus-host disease antigen that is composed of 2 subunits, DPα and DPβ. DPα and DPβ are encoded by two loci, HLA-DPA1 and HLA-DPB1, that are found in the MHC Class II (or HLA-D) region in the Human Leukocyte Antigen complex on human chromosome 6 (see protein boxes on right for links). Less is known about HLA-DP relative to HLA-DQ and HLA-DR but the sequencing of DP types and determination of more frequent haplotypes has progressed greatly within the last few years.

Contents

Structure, Functions, Genetics

 

Structure

HLA-DP is an αβ-heterodimer cell-surface receptor. Each DP subunit (α-subunit, β-subunit) is composed of a α-helical N-terminal domain, a IgG-like β-sheet, a membrane spanning domain, and an cytoplasmic domain. The α-helical domain forms the sides of the peptide binding groove. The β-sheet regions forms the base of the binding groove and the bulk of the molecule as well as the inter-subunit (non-covelant) binding region.

Function

The name 'HLA-DP' originally describes a transplantation antigen of MHC class II category of the major histocompatibility complex of humans, however this antigen is an artifact of the era organ transplantation. HLA DQ functions as a cell surface receptor for foreign or self antigens. The immune system surveys antigens for foreign pathogens when presented by MHC receptors (like HLA-DP). The MHC Class II antigens are found on antigen presenting cells (APC)(macrophages, dendritic cells, and B-lymphocytes). Normally, these APC 'present' class II receptor/antigens to a great many T-cells, each with unique T-cell receptor (TCR) variants. A few TCR variants that recognize these DQ/antigen complexes are on CD4 positive T-cells. These T-cells, call T-helper (Th) cells, can promote the amplification of B-cells that recognize a different portion of the same antigen. Alternatively, macrophages and other cytotoxic lymphocytes consume or destroy cells by apoptotic signaling and present self-antigens. Self antigens, in the right context, form a suppressor T-cell population that protects self tissues from immune attack or autoimmunity.

Genetics

The α-chain and β- of DP is encoded by the HLA-DPA1 locus and HLA-DPB1 loci, respectively. This cluster is located at the proximal (centromeric) end of the HLA superlocus in human chromosome 6p21.31. It is distal from HLA-DR and HLA-DQ encoding loci and therefore is much more equilibrated with respect to other HLA loci. In the Super B8 complex DP locus is more frequently substituted, either as a result of its distance from other loci, or because it was not as actively selected in the evolution of Super B8.

Understanding the Heterdimeric DP Isoforms

DP(αβ) Isoforms given one materal (m) and one paternal (p) chromosome 6
HLA DPB1
allele (m) (p)
DPA1 (m) αmβm (Cis m) αmβp (Trans)
(p) αpβm (Trans) αpβp (Cis p)
Result: 2 Cis, αmβm & αpβp, isoforms and 2 trans,αmβp & αpβm.

Each combination of DPA1 allele gene product with each combination of DPB1 'gene' product can potentially recombine to produce one isoform. DP genes are highly variable in the human population. In a typical population there are many DP alpha and beta. Most isoforms are not common.

These 'cis'-isoforms will account for at least 50% of the DP isoforms. The other, trans isoforms are typically more rare, isoforms result from random 'trans' combinations of haplotypes in individuals as a result of 'trans' paternal/maternal gene product isoforms.

Alleles

DPA1

  • 01
    • 0103
    • 0104
    • 0105
    • 0106
    • 0107
    • 0108
    • 0109
  • 02
    • 0201
    • 0202
    • 0203
  • 03
    • 0301
    • 0302
    • 0303
  • 0401

DPB1

  • 01
    • 0101
    • 0102
  • 02
    • 0201 early onset myasthenia gravis[1]
    • 0202
    • 0203
  • 03
  • 04
    • 0401
    • 0402
    • 0403
  • 05
    • 0501
    • 0502
  • 06
    • 0501
    • 0502
  • 06
    • 0501
    • 0502
  • 06
    • 0501
    • 0502
  • 06
    • 0501
    • 0502
  • 08
    • 0801
    • 0802
  • 09
    • 0901
    • 0902
  • 10
    • 1001
    • 1002
  • 11
    • 1101
    • 1102
  • 13
    • 1301
    • 1302
  • 14
    • 1401
    • 1402
  • 15
    • 1501
    • 1502
  • 16
    • 1601
    • 1602
  • 17
    • 1701
    • 1702
  • 18
    • 1801
    • 1802
  • 19
    • 1901
    • 1902
  • 20
    • 2001
    • 2002
  • 21
  • 22
  • 23
  • 24
  • 25
  • 26
    • 2601
    • 2602
  • 27 - *99

Haplotypes

HLA-DPA1*0103/DPB1*0401 (DP401) HLA-DPA1*0103/DPB1*0402 (DP402)

References

  1. ^ Horiki T, Inoko H, Moriuchi J, Ichikawa Y, Arimori S (1994). "Combinations of HLA-DPB1 and HLA-DQB1 alleles determine susceptibility to early-onset myasthenia gravis in Japan.". Autoimmunity 19 (1): 49-54. PMID 7749041.
v  d  e
Surface antigens
Histocompatibility/Human leukocyte antigenMHC - MHC class I (HLA-A, HLA-B, HLA-C, HLA-E)
MHC class II (HLA-DP, HLA-DQ, HLA-DR) - Minor histocompatibility antigen
OtherArrestin - Calgranulin - Blood group antigens - Cell adhesion molecules - Differentiation antigens
 
This article is licensed under the GNU Free Documentation License. It uses material from the Wikipedia article "HLA-DP". A list of authors is available in Wikipedia.
Your browser is not current. Microsoft Internet Explorer 6.0 does not support some functions on Chemie.DE