LipidDB ID

LipidDB-9606-00197

Entry Name

UniProt Accession

P25445; A9UJX4; B6VNV4; Q14292; Q14293; Q14294; Q14295; Q16652; Q5T9P1; Q5T9P2; Q5T9P3; Q6SSE9;

Theoretical PI

8.29

Molecular Weight

37732.2

Genbank Protein ID

AAA63174.1; CAA45250.1; CAA88031.1; CAA88032.1; CAA88033.1; CAA94430.1; CAA94431.1; AAS76663.1; CAA61473.1; CAR92543.1; BAF83667.1; AAR08906.1; CAI13870.1; CAI13871.1; CAI13872.1; EAW50151.1; AAH12479.1;

Genbank Nucleotide ID

M67454; X63717; X83490; X83491; X83492; X83493; Z47993; Z47994; Z47995; Z66556; Z70519; Z70520; AY495076; X89101; FM246458; AK290978; AY450925; AL157394; AL157394; AL157394; CH471066; BC012479;

Protein Name

Tumor necrosis factor receptor superfamily member 6

Protein Synonyms/Alias

Apo-1 antigen; Apoptosis-mediating surface antigen FAS; FASLG receptor; CD95;

Gene Name

FAS

Gene Synonyms/Alias

APT1; FAS1; TNFRSF6;

Created Date

01-MAY-1992

Organism

Homo sapiens (Human)

NCBI Taxa ID

9606

Reference

[1] Feig C, Tchikov V, Schütze S, Peter ME. Palmitoylation of CD95 facilitatesformation of SDS-stable receptor aggregates that initiate apoptosis signaling.EMBO J. 2007 Jan 10;26(1):221-31. Epub 2006 Dec 7.[PMID:17159907]
[2] Chakrabandhu K, Hérincs Z, Huault S, Dost B, Peng L, Conchonaud F, Marguet D, He HT, Hueber AO. Palmitoylation is required for efficient Fas cell deathsignaling. EMBO J. 2007 Jan 10;26(1):209-20. Epub 2006 Dec 7.[PMID:17159908]

Functional Description

Receptor for TNFSF6/FASLG. The adapter molecule FADD recruits caspase-8 to the activated receptor. The resulting death- inducing signaling complex (DISC) performs caspase-8 proteolytic activation which initiates the subsequent cascade of caspases (aspartate-specific cysteine proteases) mediating apoptosis. FAS- mediated apoptosis may have a role in the induction of peripheral tolerance, in the antigen-stimulated suicide of mature T-cells, or both. The secreted isoforms 2 to 6 block apoptosis (in vitro).

Sequence Annotation

Topological domain: 26 173 Extracellular.
Transmembrane: 174 190 Helical.
Topological domain: 191 335 Cytoplasmic.
Domain: 230 314 Death.
Region: 212 317 Interaction with HIPK3.
Modified residue: 209 209 Phosphoserine.

Protein Length

335 AA.

Protein Sequence
(Canonical)

FASTA
(Canonical)

Gene Ontology

GO:0031265; C:CD95 death-inducing signaling complex; IDA:UniProtKB
GO:0009986; C:cell surface; IDA:UniProtKB
GO:0005737; C:cytoplasm; IDA:HPA
GO:0005829; C:cytosol; NAS:UniProtKB
GO:0031264; C:death-inducing signaling complex; IDA:UniProtKB
GO:0009897; C:external side of plasma membrane; IEA:Ensembl
GO:0070062; C:extracellular vesicular exosome; IDA:UniProt
GO:0016021; C:integral component of membrane; IEA:UniProtKB-KW
GO:0045121; C:membrane raft; IDA:UniProtKB
GO:0005634; C:nucleus; IDA:HPA
GO:0005886; C:plasma membrane; IMP:UniProtKB
GO:0042802; F:identical protein binding; IPI:IntAct
GO:0019900; F:kinase binding; IPI:BHF-UCL
GO:0004872; F:receptor activity; NAS:UniProtKB
GO:0004871; F:signal transducer activity; TAS:ProtInc
GO:0004888; F:transmembrane signaling receptor activity; IEA:InterPro
GO:0006919; P:activation of cysteine-type endopeptidase activity involved in apoptotic process; TAS:Reactome
GO:0006924; P:activation-induced cell death of T cells; IEA:Ensembl
GO:0006915; P:apoptotic process; IDA:MGI
GO:0097190; P:apoptotic signaling pathway; TAS:Reactome
GO:0019724; P:B cell mediated immunity; IEA:Ensembl
GO:0071455; P:cellular response to hyperoxia; IMP:UniProtKB
GO:0071285; P:cellular response to lithium ion; IEA:Ensembl
GO:0071260; P:cellular response to mechanical stimulus; IEP:UniProtKB
GO:0007623; P:circadian rhythm; IEA:Ensembl
GO:0097191; P:extrinsic apoptotic signaling pathway; IMP:UniProtKB
GO:0097192; P:extrinsic apoptotic signaling pathway in absence of ligand; IEA:Ensembl
GO:0008625; P:extrinsic apoptotic signaling pathway via death domain receptors; IEA:Ensembl
GO:0002377; P:immunoglobulin production; IEA:Ensembl
GO:0006925; P:inflammatory cell apoptotic process; IEA:Ensembl
GO:0097049; P:motor neuron apoptotic process; IEA:Ensembl
GO:0097527; P:necroptotic signaling pathway; IMP:BHF-UCL
GO:0043066; P:negative regulation of apoptotic process; TAS:ProtInc
GO:0050869; P:negative regulation of B cell activation; IEA:Ensembl
GO:0045060; P:negative thymic T cell selection; IEA:Ensembl
GO:0043065; P:positive regulation of apoptotic process; IDA:UniProtKB
GO:2001241; P:positive regulation of extrinsic apoptotic signaling pathway in absence of ligand; IEA:Ensembl
GO:0032464; P:positive regulation of protein homooligomerization; IEA:Ensembl
GO:0006461; P:protein complex assembly; TAS:ProtInc
GO:0051260; P:protein homooligomerization; IEA:Ensembl
GO:0042981; P:regulation of apoptotic process; NAS:UniProtKB
GO:2001239; P:regulation of extrinsic apoptotic signaling pathway in absence of ligand; TAS:Reactome
GO:0045619; P:regulation of lymphocyte differentiation; IEA:Ensembl
GO:0045637; P:regulation of myeloid cell differentiation; IEA:Ensembl
GO:0003014; P:renal system process; IEA:Ensembl
GO:0051384; P:response to glucocorticoid; IEA:Ensembl
GO:0009636; P:response to toxic substance; IEA:Ensembl
GO:0007165; P:signal transduction; TAS:ProtInc
GO:0048536; P:spleen development; IEA:Ensembl
GO:0006927; P:transformed cell apoptotic process; IEA:Ensembl

Interpro

InterPro; IPR011029; DEATH-like_dom
InterPro; IPR000488; Death_domain
InterPro; IPR008063; Fas_rcpt
InterPro; IPR001368; TNFR/NGFR_Cys_rich_reg

Pfam

Pfam; PF00531; Death;
Pfam; PF00020; TNFR_c6;

SMART

SMART; SM00005; DEATH;
SMART; SM00208; TNFR;

PROSITE

PROSITE; PS50017; DEATH_DOMAIN;
PROSITE; PS00652; TNFR_NGFR_1;
PROSITE; PS50050; TNFR_NGFR_2;

PRINTS

PRINTS; PR01680; TNFACTORR6;