The domain within your query sequence starts at position 2092 and ends at position 2158; the E-value for the SAM domain shown below is 1.35e-14.

LGFWTKFDVADWLEWLGLSEHRAQFLDHEIDGSHLPALTKEDYVDLGVTRVGHRMNIDRA
LKFFLER

SAM

Sterile alpha motif.
SAM
SMART accession number:SM00454
Description: Widespread domain in signalling and nuclear proteins. In EPH-related tyrosine kinases, appears to mediate cell-cell initiated signal transduction via the binding of SH2-containing proteins to a conserved tyrosine that is phosphorylated. In many cases mediates homodimerisation.
Interpro abstract (IPR001660):

The sterile alpha motif (SAM) domain is a putative protein interaction module present in a wide variety of proteins [ (PUBMED:9007998) ] involved in many biological processes. The SAM domain that spreads over around 70 residues is found in diverse eukaryotic organisms [ (PUBMED:9886291) ]. SAM domains have been shown to homo- and hetero-oligomerise, forming multiple self-association architectures and also binding to various non-SAM domain-containing proteins [ (PUBMED:9343432) ], nevertheless with a low affinity constant [ (PUBMED:9933164) ]. SAM domains also appear to possess the ability to bind RNA [ (PUBMED:14659692) ]. Smaug, a protein that helps to establish a morphogen gradient in Drosophila embryos by repressing the translation of nanos (nos) mRNA, binds to the 3' untranslated region (UTR) of nos mRNA via two similar hairpin structures. The 3D crystal structure of the Smaug RNA-binding region shows a cluster of positively charged residues on the Smaug-SAM domain, which could be the RNA-binding surface. This electropositive potential is unique among all previously determined SAM-domain structures and is conserved among Smaug-SAM homologues. These results suggest that the SAM domain might have a primary role in RNA binding.

Structural analyses show that the SAM domain is arranged in a small five-helix bundle with two large interfaces [ (PUBMED:9343432) ]. In the case of the SAM domain of EphB2, each of these interfaces is able to form dimers. The presence of these two distinct intermonomers binding surface suggest that SAM could form extended polymeric structures [ (PUBMED:9933164) ].

GO function:protein binding (GO:0005515)
Family alignment:
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There are 64647 SAM domains in 49933 proteins in SMART's nrdb database.

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