p66ShcA potentiates the cytotoxic response of triple-negative breast cancers to PARP inhibitors
Eduardo Cepeda Cañedo, … , Michael Witcher, Josie Ursini-Siegel
Eduardo Cepeda Cañedo, … , Michael Witcher, Josie Ursini-Siegel
Published January 20, 2021
Citation Information: JCI Insight. 2021;6(4):e138382. https://doi.org/10.1172/jci.insight.138382.
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Research Article Cell biology Oncology

p66ShcA potentiates the cytotoxic response of triple-negative breast cancers to PARP inhibitors

Abstract

Triple-negative breast cancers (TNBCs) lack effective targeted therapies, and cytotoxic chemotherapies remain the standard of care for this subtype. Owing to their increased genomic instability, poly (ADP-ribose) polymerase (PARP) inhibitors (PARPi) are being tested against TNBCs. In particular, clinical trials are now interrogating the efficacy of PARPi combined with chemotherapies. Intriguingly, while response rates are low, cohort of patients do respond to PARPi in combination with chemotherapies. Moreover, recent studies suggest that an increase in levels of ROS may sensitize cells to PARPi. This represents a therapeutic opportunity, as several chemotherapies, including doxorubicin, function in part by producing ROS. We previously demonstrated that the p66ShcA adaptor protein is variably expressed in TNBCs. We now show that, in response to therapy-induced stress, p66ShcA stimulated ROS production, which, in turn, potentiated the synergy of PARPi in combination with doxorubicin in TNBCs. This p66ShcA-induced sensitivity relied on the accumulation of oxidative damage in TNBCs, rather than genomic instability, to potentiate cell death. These findings suggest that increasing the expression of p66ShcA protein levels in TNBCs represents a rational approach to bolster the synergy between PARPi and doxorubicin.

Authors

Eduardo Cepeda Cañedo, Stephanie Totten, Ryuhjin Ahn, Paul Savage, Deanna MacNeil, Jesse Hudson, Chantal Autexier, Genevieve Deblois, Morag Park, Michael Witcher, Josie Ursini-Siegel

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Figure 3

The DNA damage response is unaffected by p66ShcA in response to doxorubicin/PARPi combination therapy.

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The DNA damage response is unaffected by p66ShcA in response to doxorubi...
(A) Parental, VC- (p66ShcA-null), and p66ShcA-expressing Hs578T cells were treated with doxorubicin (1 nM) and PARPi (300 nM) alone or in combination for 48 hours. Double-strand DNA breaks were assessed by γH2AX immunofluorescence staining. Percentage nuclei with >10 γH2AX foci was quantified ± SEM (n = 3–5 independent experiments). (B) Representative images are shown (original magnification, ×400). (C) VC- and p66ShcA-expressing Hs578T tumors were treated with doxorubicin alone, PARPi alone, doxorubicin and PARPi in combination, or vehicle control. DNA damage levels were determined by γH2AX IHC staining. Data are depicted as (average ± SEM) percentage of positive γH2AX nuclei (n = 10–12 tumors per group). Representative images IHC staining illustrating γH2AX-positive nuclei are shown (scale bars: 100 μm). *P < 0.05; **P < 0.01; ***P < 0.001 by 1-way ANOVA/Tukey’s multiple comparisons test.