The domain within your query sequence starts at position 163 and ends at position 509; the E-value for the POLXc domain shown below is 1.19e-198.

All catalytic sites are present in this domain. Check the literature (PubMed 94278498 ) for details.

NYNQLFTDALDILAENDELRENEGSCLAFMRASSVLKSLPFPITSMKDTEGIPCLGDKVK
SIIEGIIEDGESSEAKAVLNDERYKSFKLFTSVFGVGLKTAEKWFRMGFRTLSKIQSDKS
LRFTQMQKAGFLYYEDLVSCVNRPEAEAVSMLVKEAVVTFLPDALVTMTGGFRRGKMTGH
DVDFLITSPEATEDEEQQLLHKVTDFWKQQGLLLYCDILESTFEKFKQPSRKVDALDHFQ
KCFLILKLDHGRVHSEKSGQQEGKGWKAIRVDLVMCPYDRRAFALLGWTGSRQFERDLRR
YATHERKMMLDNHALYDRTKRVFLEAESEEEIFAHLGLDYIEPWERN

POLXc

DNA polymerase X family
POLXc
SMART accession number:SM00483
Description: includes vertebrate polymerase beta and terminal deoxynucleotidyltransferases
Interpro abstract (IPR002054):

DNA carries the biological information that instructs cells how to exist in an ordered fashion: accurate replication is thus one of the most important events in the cell life cycle. This function is mediated by DNA-directed DNA-polymerases, which add nucleotide triphosphate (dNTP) residues to the 5'-end of the growing DNA chain, using a complementary DNA as template. Small RNA molecules are generally used as primers for chain elongation, although terminal proteins may also be used. Three motifs, A, B and C [ (PUBMED:2196557) ], are seen to be conserved across all DNA-polymerases, with motifs A and C also seen in RNA- polymerases. They are centred on invariant residues, and their structural significance was implied from the Klenow (Escherichia coli) structure: motif A contains a strictly-conserved aspartate at the junction of a beta-strand and an alpha-helix; motif B contains an alpha-helix with positive charges; and motif C has a doublet of negative charges, located in a beta-turn-beta secondary structure [ (PUBMED:2196557) ].

DNA polymerases ( EC 2.7.7.7 ) can be classified, on the basis of sequence similarity [ (PUBMED:3479792) (PUBMED:2196557) ], into at least four different groups: A, B, C and X. X family polymerases fill in short gaps during DNA repair, and are small (about 40kDa) compared with other polymerases. They are relatively inaccurate enzymes and play roles in base excision repair, in non-homologous end joining (NHEJ) which acts mainly to repair damage due to ionizing radiation, and in V(D)J recombination [ (PUBMED:16061182) (PUBMED:15100289) ]. X family polymerases include eukaryotic Pol beta, Pol lambda, Pol mu and terminal deoxynucleotidyl-transferase (TdT) ( EC 2.7.7.31 ). Pol beta and Pol lambda are primarily DNA template-dependent polymerases, whereas TdT is a DNA template-independent polymerase [ (PUBMED:18972388) ]. Pol mu has both template dependent and template independent activities [ (PUBMED:17159995) ]. These enzymes catalyse addition of nucleotides in a distributive manner, i.e. they dissociate from the template-primer after addition of each nucleotide. DNA-polymerases show a degree of structural similarity with RNA-polymerases.

This domain is found either at the extreme N or C termini of DNA polymerase X proteins.

GO function:DNA-directed DNA polymerase activity (GO:0003887), DNA binding (GO:0003677)
Family alignment:
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There are 6622 POLXc domains in 6621 proteins in SMART's nrdb database.

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