{PDOC51841}
{PS51841; LTD}
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* Lamin-tail (LTD) domain profile *
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Intermediate filaments (IFs) constitute a major structural element of metazoan
cells. They build two distinct systems: one inside the nucleus attached to the
inner membrane,  and  one  that  is  cytoplasmic, which connects intercellular
junctional complexes  situated  at  the plasma membrane with the outer nuclear
membrane. In  both  cases,  their  major  function  is assumed to be that of a
mechanical stress   absorber   and   an  integrating  device  for  the  entire
cytoskeleton. In  the  nucleus,  the IF system is assembled from lamins, which
together with  an  ever  increasing  number  of  associated  transmembrane and
chromatin-binding proteins  constitute  the  nuclear lamina. Despite the large
diversity among  IF  proteins,  they  all  share a similar structural building
plan, with a long central alpha-helical 'rod' domain (see <PDOC00198>) that is
flanked by  non-alpha-helical  N- and C-terminal end domains called 'head' and
'tail', respectively.  Lamins  exhibit  a highly conserved globular C-terminal
lamin-tail domain   (LTD)   which   has  the  immunoglobulin  (Ig)  fold  (see
<PDOC50835>). Invertebrate  cytoplasmic  IFs  share  sequence  similarity with
nuclear lamins  and also contain a C-terminal tail domain with homology to the
LTD [1,2,3].

Domains homologous  to  the  LTD have been detected in several uncharacterized
proteins from    phylogenetically    diverse   bacteria   and   two   archaea,
Methanosarcina and  Halobacterium.  In  several  bacterial  proteins,  the LTD
cooccurs with  membrane-associated  hydrolases  of the metallo-beta-lactamase,
synaptojanin, and  calcineurin-like  phosphoesterase  superfamilies.  In other
secreted or  periplasmic  bacterial  proteins,  the  LTDs  are associated with
oligosaccharide-binding domains or are present as multiple tandem repeats in a
single protein.   These   associations   suggest  a  potential  role  for  the
prokaryotic LTDs  in tethering proteins to the membrane or membrane-associated
structures. In contrast to the bacterial homologs, all animal LTDs are closely
related and  are  contained  in  proteins with a stereotypic architecture. The
precursor of  the  animal  LTD  might  have  been acquired via horizontal gene
transfer from  bacteria  relatively  late  in  the evolution of the eukaryotic
crown group.  Subsequent  to  this  acquisition, a coiled-coil domain, derived
from preexisting  intermediate  filament  coil-coils, might have been fused to
the N-termini of the LTD [2].

The LTD domain could be involved both in protein and DNA binding [4].

Th LTD  domain  adopts an Ig-like fold of type s (see <PDB:1IFR>). It consists
of a  2-layered sandwich of 9 anti-parallel beta-strands arranged in two beta-
sheets with  a  Greek  key  topology.  One of the sheets has five beta-strands
while the  other has four. Seven of the 9 strands are present in the classical
Ig fold topology [4,5].

Some proteins known to contain a LTD domain are listed below:

 - Animal  nuclear  lamins,  together with lamin-associated proteins, maintain
   nuclear shape   and  provide  a  structural  support  for  chromosomes  and
   replicating DNA.
 - Chloroflexus aurantiacus Chlo1887.
 - Caenorhabditis elegans intermediate filament protein ifc-2 [6].
 - Caenorhabditis elegans intermediate filament protein ifd-1.

The profile we developed covers the entire LTD domain.

-Sequences known to belong to this class detected by the profile: ALL.
-Other sequence(s) detected in Swiss-Prot: NONE.
-Last update: August 2017 / First entry.

[ 1] Herrmann H., Baer H., Kreplak L., Strelkov S.V., Aebi U.
     "Intermediate filaments: from cell architecture to nanomechanics."
     Nat. Rev. Mol. Cell Biol. 8:562-573(2007).
     PubMed=17551517; DOI=10.1038/nrm2197
[ 2] Mans B.J., Anantharaman V., Aravind L., Koonin E.V.
     "Comparative genomics, evolution and origins of the nuclear envelope
     and nuclear pore complex."
     Cell Cycle 3:1612-1637(2004).
     PubMed=15611647; DOI=10.4161/cc.3.12.1345
[ 3] Weber K., Riemer D., Dodemont H.
     "Aspects of the evolution of the lamin/intermediate filament protein
     family: a current analysis of invertebrate intermediate filament
     proteins."
     Biochem. Soc. Trans. 19:1021-1023(1991).
     PubMed=1794458
[ 4] Krimm I., Oestlund C., Gilquin B., Couprie J., Hossenlopp P.,
     Mornon J.-P., Bonne G., Courvalin J.-C., Worman H.J., Zinn-Justin S.
     "The Ig-like structure of the C-terminal domain of lamin A/C, mutated
     in muscular  dystrophies, cardiomyopathy, and partial lipodystrophy."
     Structure 10:811-823(2002).
     PubMed=12057196
[ 5] Ruan J., Xu C., Bian C., Lam R., Wang J.-P., Kania J., Min J., Zang J.
     "Crystal structures of the coil 2B fragment and the globular tail
     domain of human  lamin B1."
     FEBS Lett. 586:314-318(2012).
     PubMed=22265972; DOI=10.1016/j.febslet.2012.01.007
[ 6] Huesken K., Wiesenfahrt T., Abraham C., Windoffer R., Bossinger O.,
     Leube R.E.
     "Maintenance of the intestinal tube in Caenorhabditis elegans: the
     role of the intermediate filament protein IFC-2."
     Differentiation 76:881-896(2008).
     PubMed=18452552; DOI=10.1111/j.1432-0436.2008.00264.x

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