BABA1_RAT - dbPTM
BABA1_RAT - PTM Information in dbPTM
Basic Information of Protein
UniProt ID BABA1_RAT
UniProt AC Q5XIJ6
Protein Name BRISC and BRCA1-A complex member 1
Gene Name Babam1
Organism Rattus norvegicus (Rat).
Sequence Length 334
Subcellular Localization Cytoplasm . Nucleus . Localizes at sites of DNA damage at double-strand breaks (DSBs).
Protein Description Component of the BRCA1-A complex, a complex that specifically recognizes 'Lys-63'-linked ubiquitinated histones H2A and H2AX at DNA lesions sites, leading to target the BRCA1-BARD1 heterodimer to sites of DNA damage at double-strand breaks (DSBs). The BRCA1-A complex also possesses deubiquitinase activity that specifically removes 'Lys-63'-linked ubiquitin on histones H2A and H2AX. In the BRCA1-A complex, it is required for the complex integrity and its localization at DSBs. Component of the BRISC complex, a multiprotein complex that specifically cleaves 'Lys-63'-linked ubiquitin in various substrates. In these 2 complexes, it is probably required to maintain the stability of BABAM2 and help the 'Lys-63'-linked deubiquitinase activity mediated by BRCC3/BRCC36 component. The BRISC complex is required for normal mitotic spindle assembly and microtubule attachment to kinetochores via its role in deubiquitinating NUMA1. Plays a role in interferon signaling via its role in the deubiquitination of the interferon receptor IFNAR1; deubiquitination increases IFNAR1 activity by enhancing its stability and cell surface expression. Down-regulates the response to bacterial lipopolysaccharide (LPS) via its role in IFNAR1 deubiquitination..
Protein Sequence MEVAEANSPTEEEEEEEEEEGEEPISEPRPHTRSNPEGAEDRAIGAQANVGSRSEGEGEAATADDGAASVPGAVPKPWQVPAPASEVQIRTPRVNCPEKVIICLDLSEEMSVPKLESFNGSRTNALNVSQKMVEMFVRTKHKIDKSHEFALVVVNDDSAWLSGLTSDPRELCSCLYDLETASCSTFNLEGLFSLIQQKTELPVTENVQTIPPPYVVRTILVYSRPPCQPQFSLTEPMKKMFQCPYFFFDIIYIHSGPEEKEDDMSWKDMFAFMGSLDTKGTSYKYAVALAGPALELHNCVAKLLAHPLQRPCQSHASYSLLEEDEEAGEGEATV
Overview of Protein Modification Sites with Functional and Structural Information
Experimental Post-Translational Modification Sites

* ASA = Accessible Surface Area

Locations Modification Substrate Peptides
&
Secondary Structure		 ASA (%) Reference Orthologous
Protein Cluster
1Acetylation-------MEVAEANS
-------CCCCCCCC		9.37-
8PhosphorylationMEVAEANSPTEEEEE
CCCCCCCCCCHHHHH		40.0023298284
10PhosphorylationVAEANSPTEEEEEEE
CCCCCCCCHHHHHHH		56.7128432305
34PhosphorylationEPRPHTRSNPEGAED
CCCCCCCCCCCCHHH		58.8729779826
52PhosphorylationGAQANVGSRSEGEGE
CCCCCCCCCCCCCCC		28.4927097102
54PhosphorylationQANVGSRSEGEGEAA
CCCCCCCCCCCCCCC		52.2127097102
62PhosphorylationEGEGEAATADDGAAS
CCCCCCCCCCCCCCC		37.3527097102
69PhosphorylationTADDGAASVPGAVPK
CCCCCCCCCCCCCCC		28.4527097102
Upstream regulatory proteins (kinases for phosphorylation sites, E3 ubiquitin ligases of ubiquitination sites, ...)
Modified Location Modified Residue Modification Type of Upstream Proteins Gene Name of Upstream Proteins UniProt AC of Upstream Proteins Sources

Oops, there are no upstream regulatory protein records of BABA1_RAT !!
Functions of PTM Sites
Modified Location Modified Residue Modification Function Reference

Oops, there are no descriptions of PTM sites of BABA1_RAT !!
Disease-associated PTM Sites based on SAP

* Distance = the distance between SAP position and PTM sites.

Modified Location Modification Variant Position
(Distance <= 10) 		Residue Change SAP Related Disease Reference

Oops, there are no SNP-PTM records of BABA1_RAT !!
Protein-Protein Interaction
Interacting Protein Gene Name Interaction Type PPI Reference Domain-Domain Interactions

Oops, there are no PPI records of BABA1_RAT !!
Drug and Disease Associations
Kegg Drug
DrugBank
There are no disease associations of PTM sites.
Regulatory Network of BABA1_RAT

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Related Literatures of Post-Translational Modification

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