{PDOC51381}
{PS51381; C2_B9}
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* C2 B9-type domain profile *
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The C2  domain, usually containing ~130 residues, is one of the most prevalent
eukaryotic lipid-binding  domains  deployed  in  diverse  functional contexts.
Distinct versions of the C2 domain have been recognized, the classical C2 (see
<PDOC00380>), the   PI3K-type   (see   <PDOC51547>),   the   tensin-type  (see
<PDOC51181>), the  B9-type,  the DOCK-type (see <PDOC51650>), the NT-type (see
<PDOC51840>) and  the  Aida-type  (see  <PDOC51911>).  Despite  their  limited
sequence similarity,  all  C2  domains  contain  at their core a compact beta-
sandwich composed of two four-stranded beta sheets with highly variable inter-
strand regions  that might contain one or more alpha-helices. One feature that
is highly  conserved  in the C2 domains is the pair of hydrophobic residues on
the upper  part of the beta sheet, which are involved in imparting a curvature
of the  sheet that allows formation of a concave ligand-binding area. However,
beyond the use of the beta sheet in forming this concavity, the C2 domains are
extremely divergent  suggesting  that  different families might have optimized
their interactions with membrane through divergent means. C2 domains have been
shown to  mediate  specific  associations  with  anionic  phospholipids,  in a
Ca(2+)-dependent or  Ca(2+)-independent  manner,  thereby  participating  in a
variety of   cellular   processes,   including   cell  signaling  and  vesicle
trafficking. C2  domains  interact  with lipids primarily through two separate
binding sites:  the Ca(2+)-binding loops and the cationic beta-groove. Calcium
ion(s) binds  to a cluster of aspartates located in three Ca(2+)-binding loops
(CBR1, CBR2,  and  CBR3),  which confer a positive charge on the C2 domain and
therefore effectively  mediate  the interaction with phospholipids. Some other
C2 domains present a cationic beta-groove, the basic patch in the concave face
of the  beta-sandwich,  which is also involved in binding with anionic lipids,
either, albeit with lower specificity [1].

The B9-type  C2 domain is found in ciliary basal body associated proteins. B9-
type C2  domain  proteins  show  a  very  simple  architecture with nearly all
members being composed of just the C2 domain [1-4].

Some proteins known to contain a B9-type C2 domain are listed below:

 - Mammalian  Meckel  syndrome  1  (MKS1) protein, which may be related to the
   ciliary basal body.
 - Mammalian protein B9D1 and B9D2.
 - Caenorhabditis  elegans X-box promoter element regulated protein 7 (xbx-7).
   It corresponds to mammalian MKS1.
 - Caenorhabditis elegans ciliary transition zone associate protein 1 (tza-1).
   It corresponds to mammalian B9D2.
 - Caenorhabditis elegans ciliary transition zone associate protein 2 (tza-2).
   It corresponds to mammalian B9D1.
 - Paramecium  tetraurelia  ICIS-1  (Involved  in Cilia Stability-1), the B9D2
   homolog.

The profile we developed covers the entire B9-type C2 domain.

-Sequences known to belong to this class detected by the profile: ALL.
-Other sequence(s) detected in Swiss-Prot: NONE.
-Last update: January 2020 / Text revised.

[ 1] Zhang D., Aravind L.
     "Identification of novel families and classification of the C2 domain
     superfamily  elucidate the origin and evolution of membrane targeting
     activities in eukaryotes."
     Gene 469:18-30(2010).
     PubMed=20713135; DOI=10.1016/j.gene.2010.08.006
[ 2] Kyttaelae M., Tallila J., Salonen R., Kopra O., Kohlschmidt N.,
     Paavola-Sakki P., Peltonen L., Kestilae M.
     "MKS1, encoding a component of the flagellar apparatus basal body
     proteome, is mutated in Meckel syndrome."
     Nat. Genet. 38:155-157(2006).
     PubMed=16415886; DOI=10.1038/ng1714
[ 3] Ponsard C., Skowron-Zwarg M., Seltzer V., Perret E., Gallinger J.,
     Fisch C., Dupuis-Williams P., Caruso N., Middendorp S., Tournier F.
     "Identification of ICIS-1, a new protein involved in cilia
     stability."
     Front. Biosci. 12:1661-1669(2007).
     PubMed=17127412
[ 4] Williams C.L., Winkelbauer M.E., Schafer J.C., Michaud E.J.,
     Yoder B.K.
     "Functional redundancy of the B9 proteins and nephrocystins in
     Caenorhabditis elegans ciliogenesis."
     Mol. Biol. Cell. 19:2154-2168(2008).
     PubMed=18337471; DOI=10.1091/mbc.E07-10-1070

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