translesion error-prone DNA polymerase V autoproteolytic subunit (plasmid) [Escherichia coli]
Protein Classification
S24/S26 family peptidase( domain architecture ID 586)
S24/S26 family peptidase similar to human signal peptidase complex catalytic subunit SEC11C, a component of the microsomal signal peptidase complex which removes signal peptides from nascent proteins as they are translocated into the lumen of the endoplasmic reticulum
List of domain hits
| Name | Accession | Description | Interval | E-value | |||
| Peptidase_S24_S26 super family | cl10465 | The S24, S26 LexA/signal peptidase superfamily contains LexA-related and type I signal ... |
20-142 | 8.64e-51 | |||
The S24, S26 LexA/signal peptidase superfamily contains LexA-related and type I signal peptidase families. The S24 LexA protein domains include: the lambda repressor CI/C2 family and related bacterial prophage repressor proteins; LexA (EC 3.4.21.88), the repressor of genes in the cellular SOS response to DNA damage; MucA and the related UmuD proteins, which are lesion-bypass DNA polymerases, induced in response to mitogenic DNA damage; RulA, a component of the rulAB locus that confers resistance to UV, and RuvA, which is a component of the RuvABC resolvasome that catalyzes the resolution of Holliday junctions that arise during genetic recombination and DNA repair. The S26 type I signal peptidase (SPase) family also includes mitochondrial inner membrane protease (IMP)-like members. SPases are essential membrane-bound proteases which function to cleave away the amino-terminal signal peptide from the translocated pre-protein, thus playing a crucial role in the transport of proteins across membranes in all living organisms. All members in this superfamily are unique serine proteases that carry out catalysis using a serine/lysine dyad instead of the prototypical serine/histidine/aspartic acid triad found in most serine proteases. The actual alignment was detected with superfamily member PRK10276: Pssm-ID: 447902 Cd Length: 139 Bit Score: 158.42 E-value: 8.64e-51
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| Name | Accession | Description | Interval | E-value | |||
| PRK10276 | PRK10276 | translesion error-prone DNA polymerase V autoproteolytic subunit; |
20-142 | 8.64e-51 | |||
translesion error-prone DNA polymerase V autoproteolytic subunit; Pssm-ID: 182350 Cd Length: 139 Bit Score: 158.42 E-value: 8.64e-51
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| LexA | COG1974 | SOS-response transcriptional repressor LexA (RecA-mediated autopeptidase) [Transcription, ... |
20-140 | 3.57e-45 | |||
SOS-response transcriptional repressor LexA (RecA-mediated autopeptidase) [Transcription, Signal transduction mechanisms]; Pssm-ID: 441577 [Multi-domain] Cd Length: 199 Bit Score: 146.21 E-value: 3.57e-45
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| Peptidase_S24 | pfam00717 | Peptidase S24-like; |
20-134 | 3.90e-28 | |||
Peptidase S24-like; Pssm-ID: 425835 Cd Length: 116 Bit Score: 99.97 E-value: 3.90e-28
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| S24_LexA-like | cd06529 | Peptidase S24 LexA-like proteins are involved in the SOS response leading to the repair of ... |
56-135 | 4.90e-22 | |||
Peptidase S24 LexA-like proteins are involved in the SOS response leading to the repair of single-stranded DNA within the bacterial cell. This family includes: the lambda repressor CI/C2 family and related bacterial prophage repressor proteins; LexA (EC 3.4.21.88), the repressor of genes in the cellular SOS response to DNA damage; MucA and the related UmuD proteins, which are lesion-bypass DNA polymerases, induced in response to mitogenic DNA damage; RulA, a component of the rulAB locus that confers resistance to UV, and RuvA, which is a component of the RuvABC resolvasome that catalyzes the resolution of Holliday junctions that arise during genetic recombination and DNA repair. The LexA-like proteins contain two-domains: an N-terminal DNA binding domain and a C-terminal domain (CTD) that provides LexA dimerization as well as cleavage activity. They undergo autolysis, cleaving at an Ala-Gly or a Cys-Gly bond, separating the DNA-binding domain from the rest of the protein. In the presence of single-stranded DNA, the LexA, UmuD and MucA proteins interact with RecA, activating self cleavage, thus either derepressing transcription in the case of LexA or activating the lesion-bypass polymerase in the case of UmuD and MucA. The LexA proteins are serine proteases that carry out catalysis using a serine/lysine dyad instead of the prototypical serine/histidine/aspartic acid triad found in most serine proteases. LexA sequence homologs are found in almost all of the bacterial genomes sequenced to date, covering a large number of phyla, suggesting both, an ancient origin and a widespread distribution of lexA and the SOS response. Pssm-ID: 119397 [Multi-domain] Cd Length: 81 Bit Score: 83.38 E-value: 4.90e-22
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| lexA | TIGR00498 | SOS regulatory protein LexA; LexA acts as a homodimer to repress a number of genes involved in ... |
25-138 | 4.99e-14 | |||
SOS regulatory protein LexA; LexA acts as a homodimer to repress a number of genes involved in the response to DNA damage (SOS response), including itself and RecA. RecA, in the presence of single-stranded DNA, acts as a co-protease to activate a latent autolytic protease activity (EC 3.4.21.88) of LexA, where the active site Ser is part of LexA. The autolytic cleavage site is an Ala-Gly bond in LexA (at position 84-85 in E. coli LexA; this sequence is replaced by Gly-Gly in Synechocystis). The cleavage leads to derepression of the SOS regulon and eventually to DNA repair. LexA in Bacillus subtilis is called DinR. LexA is much less broadly distributed than RecA. [DNA metabolism, DNA replication, recombination, and repair, Regulatory functions, DNA interactions] Pssm-ID: 273106 [Multi-domain] Cd Length: 199 Bit Score: 65.89 E-value: 4.99e-14
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| Name | Accession | Description | Interval | E-value | |||
| PRK10276 | PRK10276 | translesion error-prone DNA polymerase V autoproteolytic subunit; |
20-142 | 8.64e-51 | |||
translesion error-prone DNA polymerase V autoproteolytic subunit; Pssm-ID: 182350 Cd Length: 139 Bit Score: 158.42 E-value: 8.64e-51
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| LexA | COG1974 | SOS-response transcriptional repressor LexA (RecA-mediated autopeptidase) [Transcription, ... |
20-140 | 3.57e-45 | |||
SOS-response transcriptional repressor LexA (RecA-mediated autopeptidase) [Transcription, Signal transduction mechanisms]; Pssm-ID: 441577 [Multi-domain] Cd Length: 199 Bit Score: 146.21 E-value: 3.57e-45
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| Peptidase_S24 | pfam00717 | Peptidase S24-like; |
20-134 | 3.90e-28 | |||
Peptidase S24-like; Pssm-ID: 425835 Cd Length: 116 Bit Score: 99.97 E-value: 3.90e-28
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| S24_LexA-like | cd06529 | Peptidase S24 LexA-like proteins are involved in the SOS response leading to the repair of ... |
56-135 | 4.90e-22 | |||
Peptidase S24 LexA-like proteins are involved in the SOS response leading to the repair of single-stranded DNA within the bacterial cell. This family includes: the lambda repressor CI/C2 family and related bacterial prophage repressor proteins; LexA (EC 3.4.21.88), the repressor of genes in the cellular SOS response to DNA damage; MucA and the related UmuD proteins, which are lesion-bypass DNA polymerases, induced in response to mitogenic DNA damage; RulA, a component of the rulAB locus that confers resistance to UV, and RuvA, which is a component of the RuvABC resolvasome that catalyzes the resolution of Holliday junctions that arise during genetic recombination and DNA repair. The LexA-like proteins contain two-domains: an N-terminal DNA binding domain and a C-terminal domain (CTD) that provides LexA dimerization as well as cleavage activity. They undergo autolysis, cleaving at an Ala-Gly or a Cys-Gly bond, separating the DNA-binding domain from the rest of the protein. In the presence of single-stranded DNA, the LexA, UmuD and MucA proteins interact with RecA, activating self cleavage, thus either derepressing transcription in the case of LexA or activating the lesion-bypass polymerase in the case of UmuD and MucA. The LexA proteins are serine proteases that carry out catalysis using a serine/lysine dyad instead of the prototypical serine/histidine/aspartic acid triad found in most serine proteases. LexA sequence homologs are found in almost all of the bacterial genomes sequenced to date, covering a large number of phyla, suggesting both, an ancient origin and a widespread distribution of lexA and the SOS response. Pssm-ID: 119397 [Multi-domain] Cd Length: 81 Bit Score: 83.38 E-value: 4.90e-22
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| lexA | TIGR00498 | SOS regulatory protein LexA; LexA acts as a homodimer to repress a number of genes involved in ... |
25-138 | 4.99e-14 | |||
SOS regulatory protein LexA; LexA acts as a homodimer to repress a number of genes involved in the response to DNA damage (SOS response), including itself and RecA. RecA, in the presence of single-stranded DNA, acts as a co-protease to activate a latent autolytic protease activity (EC 3.4.21.88) of LexA, where the active site Ser is part of LexA. The autolytic cleavage site is an Ala-Gly bond in LexA (at position 84-85 in E. coli LexA; this sequence is replaced by Gly-Gly in Synechocystis). The cleavage leads to derepression of the SOS regulon and eventually to DNA repair. LexA in Bacillus subtilis is called DinR. LexA is much less broadly distributed than RecA. [DNA metabolism, DNA replication, recombination, and repair, Regulatory functions, DNA interactions] Pssm-ID: 273106 [Multi-domain] Cd Length: 199 Bit Score: 65.89 E-value: 4.99e-14
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| Peptidase_S24_S26 | cd06462 | The S24, S26 LexA/signal peptidase superfamily contains LexA-related and type I signal ... |
56-134 | 1.36e-13 | |||
The S24, S26 LexA/signal peptidase superfamily contains LexA-related and type I signal peptidase families. The S24 LexA protein domains include: the lambda repressor CI/C2 family and related bacterial prophage repressor proteins; LexA (EC 3.4.21.88), the repressor of genes in the cellular SOS response to DNA damage; MucA and the related UmuD proteins, which are lesion-bypass DNA polymerases, induced in response to mitogenic DNA damage; RulA, a component of the rulAB locus that confers resistance to UV, and RuvA, which is a component of the RuvABC resolvasome that catalyzes the resolution of Holliday junctions that arise during genetic recombination and DNA repair. The S26 type I signal peptidase (SPase) family also includes mitochondrial inner membrane protease (IMP)-like members. SPases are essential membrane-bound proteases which function to cleave away the amino-terminal signal peptide from the translocated pre-protein, thus playing a crucial role in the transport of proteins across membranes in all living organisms. All members in this superfamily are unique serine proteases that carry out catalysis using a serine/lysine dyad instead of the prototypical serine/histidine/aspartic acid triad found in most serine proteases. Pssm-ID: 119396 [Multi-domain] Cd Length: 84 Bit Score: 61.90 E-value: 1.36e-13
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| COG2932 | COG2932 | Phage repressor protein C, contains Cro/C1-type HTH and peptisase s24 domains [Mobilome: ... |
20-134 | 2.75e-13 | |||
Phage repressor protein C, contains Cro/C1-type HTH and peptisase s24 domains [Mobilome: prophages, transposons]; Pssm-ID: 442176 Cd Length: 121 Bit Score: 62.29 E-value: 2.75e-13
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| S26_SPase_I | cd06530 | The S26 Type I signal peptidase (SPase; LepB; leader peptidase B; leader peptidase I; EC 3.4. ... |
61-103 | 2.22e-03 | |||
The S26 Type I signal peptidase (SPase; LepB; leader peptidase B; leader peptidase I; EC 3.4.21.89) family members are essential membrane-bound serine proteases that function to cleave the amino-terminal signal peptide extension from proteins that are translocated across biological membranes. The bacterial signal peptidase I, which is the most intensively studied, has two N-terminal transmembrane segments inserted in the plasma membrane and a hydrophilic, C-terminal catalytic region that is located in the periplasmic space. Although the bacterial signal peptidase I is monomeric, signal peptidases of eukaryotic cells commonly function as oligomeric complexes containing two divergent copies of the catalytic monomer. These are the IMP1 and IMP2 signal peptidases of the mitochondrial inner membrane that remove leader peptides from nuclear- and mitochondrial-encoded proteins. Also, two components of the endoplasmic reticulum signal peptidase in mammals (18-kDa and 21-kDa) belong to this family and they process many proteins that enter the ER for retention or for export to the Golgi apparatus, secretory vesicles, plasma membranes or vacuole. An atypical member of the S26 SPase type I family is the TraF peptidase which has the remarkable activity of producing a cyclic protein of the Pseudomonas pilin system. The type I signal peptidases are unique serine proteases that utilize a serine/lysine catalytic dyad mechanism in place of the classical serine/histidine/aspartic acid catalytic triad mechanism. Pssm-ID: 119398 [Multi-domain] Cd Length: 85 Bit Score: 35.25 E-value: 2.22e-03
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