Work
at A*STAR that is unlocking the mechanisms that drive invasive tumor growth and
metastasis could give new hope to cancer patients.
Certain
mutations cause a cancer-preventing protein to interfere with cellular pathways
and actively drive cancer progression
The p53 tumor suppressor protein manages DNA
repair mechanisms in response to genetic damage and kills off precancerous
cells before they multiply. The loss of p53 due to mutation greatly increases
risk of tumorigenesis. Even worse, however, are the various ‘missense’
mutations that change the amino acid sequence of p53: they warp its function to
promote rather than prevent cancer.
“Mutated forms of p53 are found in 50% of
human cancers,” says Jayantha Gunaratne of the A*STAR Institute of Molecular
and Cell Biology. “We hypothesized that mutant p53 proteins interact with
selected proteins that do not bind to wild-type p53 to promote processes
involved in cancer progression.” To test this theory, Gunaratne teamed up with
colleagues including David Lane, chief scientist of A*STAR and one of the
initial discoverers of p53, to hunt for binding partners that specifically
interact with the common p53R273H mutant1.
The researchers used stable isotopes to label
all the proteins in cultured cells expressing either wild-type p53 or p53R273H.
Then they used a technique called mass spectrometry that enabled them to
accurately catalogue the subset of proteins associated with either p53 variant.
“We captured at least 15 protein binding partners specific to the p53R273H
mutant,” says Gunaratne. Among the most immediately interesting was a protein
called nardilysin (NRD1), which is associated with the invasive growth and
migratory behavior observed in aggressive cancers.
After determining that NRD1 exclusively binds
p53R273H but not to other p53 mutants, Gunaratne and co-workers proceeded to
explore how it specifically collaborates with this variant. By selectively
reducing the expression of NRD1 in cultured cancer cells, they learned that
this protein is a critical component of the invasive behavior manifested by
p53R273H-expressing cells in response to a particular chemical trigger, a
cellular signal called heparin-binding epidermal growth factor-like growth
factor (HB-EGF). This HB-EGF-oriented invasion appears to occur via a cellular
mechanism distinct from those that direct cell movement in response to other
growth factors, indicating a novel biological process involving both p53R273H
and NRD1 that needs further elucidation.
Abnormal production of HB-EGF manifests in a
broad array of cancers. Gunaratne and co-workers are intrigued by the
possibility that NRD1 might therefore represent a critical factor involved in
tumor spread. “This study indicates that molecules that modulate NRD1 or other
p53 mutant-specific protein partners could offer an exciting and defined
therapeutic approach to reduce cancer metastasis,” says Gunaratne.
The A*STAR-affiliated researchers
contributing to this research are from the Institute of Molecular and Cell Biology
References
- Coffill, C. R., Muller, P. A. J., Oh, H. K., Neo,
S. P., Hogue, K. A. et al. Mutant p53 interactome identifies
nardilysin as a p53R273H-specific binding partner that promotes invasion. EMBO
Reports 13, 638–644 (2012). |article
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