Membrane dipeptidase (Peptidase family M19)

No Pfam abstract.

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InterPro entry IPR008257

Metalloproteases are the most diverse of the four main types of protease, with more than 50 families identified to date. In these enzymes, a divalent cation, usually zinc, activates the water molecule. The metal ion is held in place by amino acid ligands, usually three in number. The known metal ligands are His, Glu, Asp or Lys and at least one other residue is required for catalysis, which may play an electrophillic role. Of the known metalloproteases, around half contain an HEXXH motif, which has been shown in crystallographic studies to form part of the metal-binding site PUBMED:7674922. The HEXXH motif is relatively common, but can be more stringently defined for metalloproteases as 'abXHEbbHbc', where 'a' is most often valine or threonine and forms part of the S1' subsite in thermolysin and neprilysin, 'b' is an uncharged residue, and 'c' a hydrophobic residue. Proline is never found in this site, possibly because it would break the helical structure adopted by this motif in metalloproteases PUBMED:7674922.

In the MEROPS database peptidases and peptidase homologues are grouped into clans and families. Clans are groups of families for which there is evidence of common ancestry based on a common structural fold:

• Each clan is identified with two letters, the first representing the catalytic type of the families included in the clan (with the letter 'P' being used for a clan containing families of more than one of the catalytic types serine, threonine and cysteine). Some families cannot yet be assigned to clans, and when a formal assignment is required, such a family is described as belonging to clan A-, C-, M-, S-, T- or U-, according to the catalytic type. Some clans are divided into subclans because there is evidence of a very ancient divergence within the clan, for example MA(E), the gluzincins, and MA(M), the metzincins.
• Peptidase families are grouped by their catalytic type, the first character representing the catalytic type: A, aspartic; C, cysteine; G, glutamic acid; M, metallo; S, serine; T, threonine; and U, unknown. The serine, threonine and cysteine peptidases utilise the amino acid as a nucleophile and form an acyl intermediate - these peptidases can also readily act as transferases. In the case of aspartic, glutamic and metallopeptidases, the nucleophile is an activated water molecule.

In many instances the structural protein fold that characterises the clan or family may have lost its catalytic activity, yet retain its function in protein recognition and binding.

This group of peptidases belong to the MEROPS peptidase family M19 (membrane dipeptidase family, clan MJ). The protein fold of the peptidase domain for members of this family resembles that of Klebsiella urease, the type example for clan MJ.

Renal dipeptidase (rDP) (), also known as microsomal dipeptidase, is a zinc-dependent metalloenzyme that hydrolyzes a wide range of dipeptides. It is involved in renal metabolism of glutathione and its conjugates. It is a homodimeric disulphide-linked glycoprotein attached to the renal brush border microvilli membrane by a GPI-anchor. A glutamate residue has recently been shown PUBMED:8097406,PUBMED:12144777 to be important for the catalytic activity of rDP. rDP seems to be evolutionary related to hypothetical proteins in the PQQ biosynthesis operons of Acinetobacter calcoaceticus and Klebsiella pneumoniae.

Clan

This family is a member of clan Amidohydrolase (CL0034), which contains the following 10 members:

A_deaminase Amidohydro_1 Amidohydro_2 Amidohydro_3 DUF3604 Peptidase_M19 PHP PTE RNase_P_p30 TatD_DNase

Gene Ontology

Molecular function	dipeptidase activity (GO:0016805)
	dipeptidyl-peptidase activity (GO:0008239)
	metalloexopeptidase activity (GO:0008235)
Biological process	proteolysis (GO:0006508)

External database links

MEROPS:	M19
PANDIT:	PF01244
PROSITE:	PDOC00678
SCOP:	1itq
SYSTERS:	Peptidase_M19

Below is a listing of the unique domain organisations or architectures in which this domain is found. More...

There are various ways to view or download the sequence alignments that we store. You can use a sequence viewer to look at either the seed or full alignment for the family, or you can look at a plain text version of the sequence in a variety of different formats. More...

View options

Alignment:	Seed (48) Full (984) NCBI (3190) Metagenomics (2191)
Viewer:	jalview HTML Heatmap Pfam viewer

Formatting options

Alignment:	Seed (48) Full (984)
Format:	Selex Stockholm FASTA MSF
Order:	Tree Alphabetical
Sequence:	Inserts lower case All upper case
Gaps:	Gaps as "." or "-" (mixed) Gaps as "." (dots) Gaps as "-" (dashes) No gaps (unaligned)
Download/view:	Download View

Download options

Very large alignments can often cause problems for the formatting tool above. If you find that downloading or viewing a large alignment is problematic, you can also download a gzip-compressed, Stockholm-format file containing the seed or full alignment for this family.

You can also download a FASTA format file containing the full-length sequences for all sequences in the full alignment.

The main seed and full alignments are generated using sequences from the UniProt sequence database. However, we also generate alignments using sequences from the NCBI sequence database and the "metaseq" metagenomics dataset.

You can view alignments from these two additional datasets using the form above, or you can download alignments of NCBI or metagenomics sequences, as gzip-compressed files.

Pfam alignments:	Seed (48) Full (984) NCBI (3190) Metagenomics (2191)
Full length sequences	Full-sequences (984)

External links

MyHits provides a collection of tools to handle multiple sequence alignments. For example, one can refine a seed alignment (sequence addition or removal, re-alignment or manual edition) and then search databases for remote homologs using HMMER2.

Pfam alignments:

Seed (48) Full (984)

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HMM logos is one way of visualising profile HMMs. Logos provide a quick overview of the properties of an HMM in a graphical form. You can see a more detailed description of HMM logos and find out how you can interpret them here. More...

This page displays the phylogenetic tree for this family. We use FastTree to calculate neighbour join trees with a local bootstrap based on 100 resamples (shown next to the tree nodes). FastTree calculates approximately-maximum-likelihood phylogenetic trees from our seed or full alignments.

Seed (48) Full (984) NCBI (3190) Metagenomics (2191) Loading...

Note: You can also download the data files for the seed, full, NCBI or metagenomics trees.

This section shows the detailed information about the Pfam family. You can see the definitions of many of the terms in this section in the glossary and a fuller explanation of the scoring system that we use in the scores section of the help pages.

Curation

Seed source:	Prosite
Previous IDs:	Renal_dipeptase;
Type:	Family
Author:	Finn RD, Bateman A
Number in seed:	48
Number in full:	984
Average length of the domain:	314.10 aa
Average identity of full alignment:	26 %
Average coverage of the sequence by the domain:	84.10 %

HMM information

HMM build commands:	build method: hmmbuild -o /dev/null HMM SEED search method: hmmsearch -Z 9421015 -E 1000 HMM pfamseq
Model details:	Parameter Sequence Domain Gathering cut-off 20.2 20.2 Trusted cut-off 20.7 20.2 Noise cut-off 19.4 20.1
Model length:	320
Family (HMM) version:	14
Download:	download the raw HMM for this family

There is 1 interaction for this family. More...

Peptidase_M19

For those sequences which have a structure in the Protein DataBank, we use the mapping between UniProt, PDB and Pfam coordinate systems from the PDBe group, to allow us to map Pfam domains onto UniProt sequences and three-dimensional protein structures. The table below shows the structures on which the Peptidase_M19 domain has been found.