B cell receptor signaling (Homo sapiens)

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Description

The functional B-cell receptor is a multi-protein complex consisting of an antigen binding subunit and a signaling subunit. The antigen binding subunit is the membrane bound immunoglobulin and the signaling subunit consists of the Igα and Igβ proteins, which are covalently bound to each other. Both Igα and Igβ proteins have an immunoreceptor tyrosine -based activation motif (ITAM) each in its cytoplasmic region, which is responsible for the initiation and propagation of signaling. Antigen binding to the immunoglubulin results in the aggregation of both the immunoglobulin and the Igα/β subunits. This results in the phosphorylation of the tyrosine residues in the ITAM motif of the Igα/β subunits by the src-family of protein tyrosine kinases Lyn and Syk. The Src family kinases are initially in the proximity of the BCR as a result of membrane anchoring by virtue of its their acetylation. The N-terminal region of the kinases can also interact with the non-phosphorylated ITAMs of Igα. This association is further enhanced upon BCR engagement as a result of accumulation in BCR containing lipid rafts and SH2 domain mediated binding to the phosphorylated tyrosine residues in ITAMs. This increased association helps in amplifying the BCR mediated signaling. Doubly phosphorylated Igα/β ITAMs are necessary for efficient recruitment of Syk and its activation. Activated Syk then phsophorylates the adapter molecule B cell linker protein (BLNK), which acts as molecular scaffold for the recruitment of multiple effectors and hence the propagation of multiple signaling pathways. BLNK binds to Btk and PLCγ2 which results in optimal phosphorylation and activation of PLC. This is an important mechanism which links BCR to Ca2+ signaling. Apart from the PLC mediated Ca2+ signaling, BCR triggering also results in the the activaion of phosphatidylinositol-3 kinase (PI-3K). This activation takes place through the recruitment of p85 adaptor subunit of PI-3K to CD19 co-receptor, which is phosphorylated by Lyn on its cytoplasmic Y-X-X-M motif. Alternatively, PI-3K can be recruited to the plasma membrane by other adapter molecules including PIK3AP, CBL or GAB1/2. PI-3K catalyzes the phosphorylation of phosphatidylinositol 4,5-bisphosphate to phosphatidyl inositol 3,4,5-bisphosphate. Akt, a serine threonine kinase, is recruited to the plasma membrane by virtue of its N-terminal PH-domain where it is activated by conformational changes and phosphorylation. Activated Akt phosphorylates several substrates resulting in diverse physiological consequences: Forkhead transcription factors - resulting in its degradation and hence inhibition of expression of pro-apoptotic genes, glycogen synthase kinase-3 GSK3 -leading to its inhibition and hence regulation of cell-cycle. The tanscription factor NF-kappaB is also found to be activated in BCR signaling in a Btk, PI-3K and PKC dependent manner.

BCR engagement can also result in the association of GRB2/SOS complex with either SHC or BLNK, which results in the activation of the Ras/Raf/MEK/ERK signaling cascade. This cascade leads to the activation of transcription factors including ELK and MYC. BCR activation also results in the activation of JNKs and p38MAPK.


Please access this pathway at NetSlim database.

If you use this pathway, please cite following paper: Kandasamy, K., Mohan, S. S., Raju, R., Keerthikumar, S., Kumar, G. S. S., Venugopal, A. K., Telikicherla, D., Navarro, J. D., Mathivanan, S., Pecquet, C., Gollapudi, S. K., Tattikota, S. G., Mohan, S., Padhukasahasram, H., Subbannayya, Y., Goel, R., Jacob, H. K. C., Zhong, J., Sekhar, R., Nanjappa, V., Balakrishnan, L., Subbaiah, R., Ramachandra, Y. L., Rahiman, B. A., Prasad, T. S. K., Lin, J., Houtman, J. C. D., Desiderio, S., Renauld, J., Constantinescu, S. N., Ohara, O., Hirano, T., Kubo, M., Singh, S., Khatri, P., Draghici, S., Bader, G. D., Sander, C., Leonard, W. J. and Pandey, A. (2010). NetPath: A public resource of curated signal transduction pathways. Genome Biology. 11:R3.

Proteins on this pathway have targeted assays available via the CPTAC Assay Portal

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Bibliography

  1. Kandasamy K, Mohan SS, Raju R, Keerthikumar S, Kumar GS, Venugopal AK, Telikicherla D, Navarro JD, Mathivanan S, Pecquet C, Gollapudi SK, Tattikota SG, Mohan S, Padhukasahasram H, Subbannayya Y, Goel R, Jacob HK, Zhong J, Sekhar R, Nanjappa V, Balakrishnan L, Subbaiah R, Ramachandra YL, Rahiman BA, Prasad TS, Lin JX, Houtman JC, Desiderio S, Renauld JC, Constantinescu SN, Ohara O, Hirano T, Kubo M, Singh S, Khatri P, Draghici S, Bader GD, Sander C, Leonard WJ, Pandey A; ''NetPath: a public resource of curated signal transduction pathways.''; Genome Biol, 2010 PubMed Europe PMC Scholia

History

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135864view03:38, 20 November 2024EweitzClear cache
135863view02:00, 20 November 2024EweitzEconomize layout
135862view01:52, 20 November 2024EweitzClear cache to tailor board dimensions
135861view01:50, 20 November 2024EweitzEconomize layout, standardize nucleus representation
135859view22:25, 19 November 2024EweitzRemove graphical blemish
135532view22:55, 22 September 2024EweitzEconomize layout
135531view22:50, 22 September 2024EweitzEconomize layout
135530view03:42, 22 September 2024EweitzRefine legend
135529view03:41, 22 September 2024EweitzRefine legend
135528view03:32, 22 September 2024EweitzFix interaction modeling, thin interactions for discernibility
135527view03:24, 22 September 2024EweitzFix interaction modeling
135526view03:18, 22 September 2024EweitzThin interactions, for discernible ends
135525view03:08, 22 September 2024EweitzRefine legend
135524view03:03, 22 September 2024EweitzEconomize layout, improve alignment
135523view02:58, 22 September 2024EweitzAlign translocations
135522view02:50, 22 September 2024EweitzEconomize layout
135521view02:49, 22 September 2024EweitzThin lines for translocation, for discernible ends
135520view02:44, 22 September 2024EweitzEconomize layout
135495view12:54, 20 September 2024EweitzConnect source node in branching interactions, refine receptor graphic
135494view12:49, 20 September 2024EweitzConnect source node in branching interactions
135493view12:43, 20 September 2024EweitzConnect source node in branching interactions, refine legend
135492view02:40, 20 September 2024EweitzEconomize layout
135488view00:05, 20 September 2024EweitzRemove errant nodes shown in Kaavio / Pvjs, but not PathVisio
129688view00:47, 22 May 2024EweitzModified title
126262view05:57, 19 April 2023EgonwLicense is CCZero
120701view13:17, 23 December 2021EweitzStandardize font, weight, case
117659view11:52, 22 May 2021EweitzModified title
115881view12:33, 19 March 2021EgonwCopied the NetPath reference into the literature list
115879view12:30, 19 March 2021EgonwModified description
108321view20:51, 6 December 2019L DupuisConverted interactions to graphical lines in legend
106310view17:47, 20 August 2019KhanspersModified description
105541view06:07, 9 August 2019KhanspersModified description
92558view00:23, 16 June 2017AlexanderPicoFixed 0 widths and heights by removing "hidden" elements
89900view13:18, 6 October 2016MkutmonModified description
89899view13:17, 6 October 2016MkutmonModified description
79985view16:20, 29 April 2015Zariannotated PDPK2, CD79B ,CD79A, CD19 and LCK
78566view14:50, 7 January 2015MaintBotadded missing graphIds
72101view21:43, 24 October 2013Mkutmonadded datasource for "GSK3A" and "CD81"
71524view19:22, 17 October 2013MaintBotremoved data source from nodes without identifier
67071view10:02, 26 June 2013Christine ChichesterOntology Term : 'B cell receptor signaling pathway' added !
63145view20:12, 8 May 2013MaintBotUpdating GPML version
47980view14:44, 23 April 2012NetPathModified description
44975view14:24, 6 October 2011MartijnVanIerselOntology Term : 'signaling pathway pertinent to immunity' added !
44972view14:22, 6 October 2011MartijnVanIerselOntology Term : 'B cell' added !
44829view07:29, 6 October 2011Mkutmonconnected some lines
44620view17:50, 22 September 2011KhanspersUpdating content to NetSlim
44113view20:38, 24 August 2011KhanspersReverted to version '23:43, 1 March 2011' by Khanspers
44035view23:18, 22 August 2011KhanspersModified description
44034view23:16, 22 August 2011KhanspersUpdating pathway from NetSlim
41190view23:43, 1 March 2011MaintBotRemoved redundant pathway information and comments

External references

DataNodes

View all...
NameTypeDatabase referenceComment
AKT1Protein207 (Entrez Gene)
ATF2Protein1386 (Entrez Gene)
BCAR1Protein8462 (Entrez Gene)
BCL10Protein8915 (Entrez Gene)
BCL6Protein604 (Entrez Gene)
BLKProtein640 (Entrez Gene)
BLNKProtein29760 (Entrez Gene)
BRAFProtein673 (Entrez Gene)
BTKProtein695 (Entrez Gene)
CAMK2AProtein815 (Entrez Gene)
CARD11Protein84433 (Entrez Gene)
CBLProtein867 (Entrez Gene)
CD19Protein930 (Entrez Gene)
CD22Protein933 (Entrez Gene)
CD45Protein5788 (Entrez Gene)
CD79AProtein973 (Entrez Gene)
CD79BProtein974 (Entrez Gene)
CD81Protein975 (Entrez Gene)
CDC42Protein998 (Entrez Gene)
CHUKProtein1147 (Entrez Gene)
CR2Protein1380 (Entrez Gene)
CREB1Protein1385 (Entrez Gene)
CRKProtein1398 (Entrez Gene)
CRKLProtein1399 (Entrez Gene)
DAGProtein
DAPP1Protein27071 (Entrez Gene)
E2F3Rna1871 (Entrez Gene)
ELK1Protein2002 (Entrez Gene)
ETS1Protein2113 (Entrez Gene)
FOXO1Protein2308 (Entrez Gene)
FYNProtein2534 (Entrez Gene)
GAB1Protein2549 (Entrez Gene)
GAB2Protein9846 (Entrez Gene)
GRB2Protein2885 (Entrez Gene)
GSK3AProtein2931 (Entrez Gene)
GSK3BProtein2932 (Entrez Gene)
GTF2IProtein2969 (Entrez Gene)
HCLS1Protein3059 (Entrez Gene)
HRASProtein3265 (Entrez Gene)
IKBKBProtein3551 (Entrez Gene)
IKBKGProtein8517 (Entrez Gene)
ILF2Rna3608 (Entrez Gene)
INPP5DProtein3635 (Entrez Gene)
IP3Protein
IRF4Rna3662 (Entrez Gene)
JUNProtein3725 (Entrez Gene)
LAT2Protein7462 (Entrez Gene)
LCKProtein3932 (Entrez Gene)
LYNProtein4067 (Entrez Gene)
MALT1Protein10892 (Entrez Gene)
MAP2K1Protein5604 (Entrez Gene)
MAP2K2Protein5605 (Entrez Gene)
MAP2K6Protein5608 (Entrez Gene)
MAP3K7Protein6885 (Entrez Gene)
MAP4K1Protein11184 (Entrez Gene)
MAPK14Protein1432 (Entrez Gene)
MAPK1Protein5594 (Entrez Gene)
MAPK3Protein5596 (Entrez Gene)
MAPK4Protein5596 (Entrez Gene)
MAPK8Protein5599 (Entrez Gene)
MAPK9Protein5601 (Entrez Gene)
MAXProtein4149 (Entrez Gene)
MEF2CRna4208 (Entrez Gene)
MEF2DRna4209 (Entrez Gene)
MYCRna4609 (Entrez Gene)
NCK1Protein4690 (Entrez Gene)
NFATC2Protein4773 (Entrez Gene)
NFATC3Protein4775 (Entrez Gene)
NFKB1Protein4790 (Entrez Gene)
NFKBIAProtein4792 (Entrez Gene)
PDPK1Protein5170 (Entrez Gene)
PDPK2Protein653650 (Entrez Gene)
PI-4,5-P2Protein
PI-4-PProtein5777 (Entrez Gene)
PIK3AP1Protein118788 (Entrez Gene)
PIK3CGProtein5294 (Entrez Gene)
PIK3R1Protein5295 (Entrez Gene)
PIK3R2Protein5296 (Entrez Gene)
PIP5K1AProtein8394 (Entrez Gene)
PIP5K1BProtein8395 (Entrez Gene)
PIP5K1CProtein23396 (Entrez Gene)
PLCG1Protein5335 (Entrez Gene)
PLCG2Protein5336 (Entrez Gene)
PRKCB1Protein5579 (Entrez Gene)
PRKCDProtein5580 (Entrez Gene)
PTPN11Protein5781 (Entrez Gene)
PTPN18Protein26469 (Entrez Gene)
PTPN6Protein5777 (Entrez Gene)
RAC1Protein5879 (Entrez Gene)
RAC2Protein5880 (Entrez Gene)
RAF1Protein5894 (Entrez Gene)
RAPGEF1Protein2889 (Entrez Gene)
RASGRP3Protein25780 (Entrez Gene)
RELProtein5966 (Entrez Gene)
RELAProtein5970 (Entrez Gene)
RPS6KA1Protein6195 (Entrez Gene)
SH3BP2Protein6452 (Entrez Gene)
SHC1Protein6464 (Entrez Gene)
SOS1Protein6654 (Entrez Gene)
SYKProtein6850 (Entrez Gene)
TECProtein7006 (Entrez Gene)
VAV1Protein7409 (Entrez Gene)
VAV2Protein7410 (Entrez Gene)

Annotated Interactions

No annotated interactions

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