Neha Patil (Editor)

NPM1

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Species
  
Human

Entrez
  
4869

Human
  
Mouse

Ensembl
  
ENSG00000181163

NPM1 wwwbloodjournalorgcontentbloodjournal118112

Aliases
  
NPM1, B23, NPM, nucleophosmin (nucleolar phosphoprotein B23, numatrin)

External IDs
  
MGI: 106184 HomoloGene: 81697 GeneCards: NPM1

Gene music using protein sequence of npm1 nucleophosmin nucleolar phosphoprotein b23 numatrin


Nucleophosmin (NPM), also known as nucleolar phosphoprotein B23 or numatrin, is a protein that in humans is encoded by the NPM1 gene.

Contents

Minimal residual disease in npm1 mutated aml


Function

NPM1 is associated with nucleolar ribonucleoprotein structures and bind single-stranded and double-stranded nucleic acids, but it binds preferentially G-quadruplex forming nucleic acids. It is involved in the biogenesis of ribosomes and may assist small basic proteins in their transport to the nucleolus. Its regulation through SUMOylation (by SENP3 and SENP5) is another facet of the proteins's regulation and cellular functions.

It is located in the nucleolus, but it can be translocated to the nucleoplasm in case of serum starvation or treatment with anticancer drugs. The protein is phosphorylated.

Nucleophosmin has multiple functions:

  1. Histone chaperones
  2. Ribosome biogenesis and transport
  3. Genomic stability and DNA repair
  4. Endoribonuclease activity
  5. Centrosome duplication during cell cycle
  6. Regulation of ARF-p53 tumor suppressor pathway
  7. RNA helix destabilizing activity
  8. Inhibition of caspase-activated DNase
  9. Prevents apoptosis when located in nucleolus

Clinical significance

NPM1 gene is up-regulated, mutated and chromosomally translocated in many tumor types. Chromosomal aberrations involving NPM1 were found in patients with non-Hodgkin lymphoma, acute promyelocytic leukemia, myelodysplastic syndrome, and acute myelogenous leukemia. Heterozygous mice for NPM1 are vulnerable to tumor development. In solid tumors NPM1 is frequently found overexpressed, and it is thought that NPM1 could promote tumor growth by inactivation of the tumor suppressor p53/ARF pathway; on the contrary, when expressed at low levels, NPM1 could suppress tumor growth by the inhibition of centrosome duplication.

Of high importance is NPM involvement in acute myelogenous leukemia,

where a mutated protein lacking a folded C-terminal domain (NPM1c+) has been found in the cytoplasm in patients This aberrant localization has been linked to the development of the disease. Strategies against this subtype of acute myelogenous leukemia include the refolding of the C-terminal domain using pharmalogical chaperones and the displacement of the protein from nucleolus to nucleoplasm, which has been linked to apoptotic mechanisms.

Interactions

NPM1 has been shown to interact with

  • AKT1,
  • BARD1,
  • BRCA1, and
  • nucleolin.

    • Nucleophosmin has multiple binding partners:

    1. rRNA
    2. HIV Rev and Rex peptide
    3. p53 tumor suppressor
    4. ARF tumor suppressor
    5. MDM2 (mouse double minute 2, ubiquitin ligase)
    6. Ribosome protein S9
    7. Phosphatidylinositol 3,4,5-triphosphate (PIP3)
    8. Exportin-1 (CRM1, chromosome region maintenance)
    9. Nucleolin/C23
    10. Transcription target of myc oncogene

    References

    NPM1 Wikipedia
    (Text) CC BY-SA