Conserved Protein Domain Family
PHD6_KMT2C_like

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cd15514: PHD6_KMT2C_like 
PHD finger 6 found in Histone-lysine N-methyltransferase 2C (KMT2C) and PHD finger 5 found in KMT2D
KMT2C, also termed myeloid/lymphoid or mixed-lineage leukemia protein 3 (MLL3), or homologous to ALR protein, is a histone H3 lysine 4 (H3K4) lysine methyltransferase that functions as a circadian factor contributing to genome-scale circadian transcription. It is a component of a large complex that acts as a coactivator of multiple transcription factors, including the bile acid (BA)-activated nuclear receptor, farnesoid X receptor (FXR), a critical player in BA homeostasis. The MLL3 complex is essential for p53 transactivation of small heterodimer partner (SHP). KMT2C is also a part of activating signal cointegrator-2 (ASC-2)-containing complex (ASCOM) that contains the transcriptional coactivator nuclear receptor coactivator 6 (NCOA6), KMT2C and its paralog MLL4. The ASCOM complex is critical for nuclear receptor (NR) activation of bile acid transporter genes and is down regulated in cholestasis. KMT2D, also termed ALL1-related protein (ALR), is encoded by the gene that was named MLL4, a fourth human homolog of Drosophila trithorax, located on chromosome 12. It enzymatically generates trimethylated histone H3 Lysine 4 (H3K4me3). It plays an essential role in differentiating the human pluripotent embryonal carcinoma cell line NTERA-2 clone D1 (NT2/D1) stem cells by activating differentiation-specific genes, such as HOXA1-3 and NESTIN. KMT2D is also a part of ASCOM. Both KMT2C and KMT2D contain the catalytic domain SET, several plant homeodomain (PHD) fingers, two extended PHD (ePHD) fingers, Cys2HisCys5HisCys2His, a RING finger, an HMG (high-mobility group)-binding motif, and two FY-rich regions. This model corresponds to the sixth PHD finger of KMT2C and the fifth PHD finger of KMT2D.
Statistics
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PSSM-Id: 276989
Aligned: 21 rows
Threshold Bit Score: 78.866
Created: 12-Aug-2013
Updated: 2-Oct-2020
Structure
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Aligned Rows:
 
Zn binding siteputative
Feature 1: Zn binding site [ion binding site], 8 residue positions
Conserved feature residue pattern:C C C [CH] H [CH] C [CH]Click to see conserved feature residue pattern help
Evidence:

Sequence Alignment
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Format: Row Display: Color Bits: Type Selection:
Feature 1          #  #            #  #    #  #                  #  #
Q8NEZ4       1086 SCPvCYRNYrEEDLILQCRQCDRWMHAVCQNLNTEeevenvaDIGFDCSMC 1136 human
XP_795757     894 HCAyCYRSYrDNELLCQCSHCQRWEHALCNSLYTEdeteramDKGFICTLC 944  purple urchin
XP_002416243  414 SCPlCLLKYqENDLVIQCVQCERWMHGFCDQIACEedaekcaEYGYNCPYC 464  black-legged tick
XP_001629651  128 SCPvCNIKYnLNDLMIQCLHCDRWLHGSCDGLMTEeevdraaDYGYQCLYC 178  starlet sea anemone
O14686       1506 TCPiCHAPYvEEDLLIQCRHCERWMHAGCESLFTEddveqaaDEGFDCVSC 1556 human
EJW86460      393 KCPkCLRLYeIGDNIIKCQHCARWLHGKCEELYGEemfetasENGFRCSLC 443  agent of lymphatic filariasis
NP_499819     554 KCPrCERNYqLNEKLIRCSQCSKWQHGACEGLYTDeqleqaaIDRMRCSAC 604  nematode
CAP35726      569 VCPcCNRGYqINDKIIRCSLCKKWQHGACENLHTEeqleqaaQNRMRCASC 619  Caenorhabditis briggsae
CDJ80580      514 KCPkCSKLYnIGEKIIKCSACARWYHGTCEDLYNDemlesasANKMRCSAC 564  barber pole worm
XP_006822314  932 TCPvCFKEYkEDELIIQCVQCYRWLHAECDGFHNEddieraaDQGYHCLLC 982  Saccoglossus kowalevskii

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