Findings indicate that cells can use alternate pathways for uncontrolled growth
US researchers have found during a study how cancer cells manage to evade despite treatment. Published in the Proceedings of the National Academy of Sciences, the study delves into the cellular processes that allow cancer cells to proliferate even when targeted by anticancer drugs.
Cancer
cells exploit cell cycles to multiply rapidly, a process known as
proliferation. Cancer drugs aim to halt this growth by initiating a complex
sequence of genetic and cellular events. However, these treatments often yield
mixed results.
The team led by
Jean Cook of the Department of Biochemistry and Biophysics at University of
North Carolina, Chapel Hill, identified a crucial enzyme that plays a key role
in stopping cancer cell proliferation, particularly during treatment with
anti-cancer drugs.
This enzyme’s function varies among individuals. The researchers also discovered mechanisms through which cancer cells evade therapies designed to inhibit them.
Cells regulate protein expression by turning genes “on” and “off”.
Some
proteins ensure precise and effective cell division, akin to musicians in an
orchestra guided by a conductor.
Cells
can deactivate these regulatory proteins, allowing uncontrolled division and
DNA replication.
To explore protein degradation’s role in halting cell growth, Cook and graduate
student Brandon Mouery treated cultured human cells with palbociclib, a
metastatic breast cancer drug.
Using
microscopy, flow cytometry, and proteomics, they found that the enzyme APC/C,
which targets proteins for degradation to regulate the cell cycle, enhances the
effectiveness of palbociclib.
This
finding suggests that APC/C levels in tumours could help predict patient
responses to palbociclib and similar drugs.
Reduced APC/C activity might indicate poor treatment response or a higher
relapse risk.
The
researchers also observed that both cancerous and non-cancerous cells can
bypass drug-induced proliferation arrest.
These
escapee cells struggle to replicate DNA independently, likely delegating DNA
replication to proteins that initiate cell division later in the cell cycle.
This indicates that cells can use alternate pathways for uncontrolled growth.
“Cell
proliferation has been intensively studied for decades, yet we can still be
surprised,” Cook noted. “Sometimes our textbook understanding is still quite
incomplete, so we need to keep an open mind and continually challenge
paradigms.”
These
findings could lead to new interventions that induce long-lasting proliferation
arrest by exploiting this escape mechanism and cancer-associated DNA
replication errors, potentially forcing cancer cells into a “self-destructive”
growth mode.
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