NRG1/ERBB3/ERBB2 Axis Triggers Anchorage-Independent Growth of Basal-like/Triple-Negative Breast Cancer Cells

Miano, Carmen; Morselli, Alessandra; Pontis, Francesca; Bongiovanni, Chiara; Sacchi, Francesca; Pra, Silvia Da; Romaniello, Donatella; Tassinari, Riccardo; Sgarzi, Michela; Pantano, Elvira; Ventura, Carlo; Lauriola, Mattia; D’Uva, Gabriele

doi:10.3390/cancers14071603

Cited by 7 publications

(14 citation statements)

References 64 publications

(111 reference statements)

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“…Clinical data supported a link between ERBB4 and increased survival in luminal and HER2+ breast cancer patients. Of note, ERBB4 activation, induced by stimulation with neuregulin 1 (NRG1), has been shown to promote the differentiation and impair the growth of SUM44 breast cancer cells, which belong to the luminal subtype ( 32 ) and express very high levels of ERBB4 ( Supplementary Figure S2B ) and low levels of ERBB2 ( 10 ). Thus, we decided to test whether the activation of ERBB4 signaling by neuregulins may restrain the aggressiveness of HER2+ breast cancers, if ERBB2 is inhibited by anti-HER2 agents.…”

Section: Resultsmentioning

confidence: 99%

“…Our observation of a positive correlation between ERBB4 mRNA levels and increased relapse-free patients’ survival in the luminal A subtype is in line with a previous study showing that the activation of ERBB4 signaling by NRG1 restrains the growth of breast cancer luminal cells ( 32 ). Importantly, the luminal breast cancer subtype expresses high levels of ERBB4 (please consult Figure 1E ) and ERBB3 ( 10 ) and quite low ERBB2 and EGFR levels ( 50 ) [reviewed in ( 51 )]; by consequence, the activation of ERBB4 by ligands in this breast tumor subtype is expected to preferentially activate ERBB4-ERBB4 homodimers or ERBB4-ERBB3 heterodimers. Apart from a modest reduction in ERBB4 (please consult Figure 1E ), the abundance of ERBB receptors in the luminal B subgroup does not differ that much as compared to luminal A ( 10 ).…”

Section: Discussionmentioning

confidence: 99%

“…Importantly, the luminal breast cancer subtype expresses high levels of ERBB4 (please consult Figure 1E ) and ERBB3 ( 10 ) and quite low ERBB2 and EGFR levels ( 50 ) [reviewed in ( 51 )]; by consequence, the activation of ERBB4 by ligands in this breast tumor subtype is expected to preferentially activate ERBB4-ERBB4 homodimers or ERBB4-ERBB3 heterodimers. Apart from a modest reduction in ERBB4 (please consult Figure 1E ), the abundance of ERBB receptors in the luminal B subgroup does not differ that much as compared to luminal A ( 10 ). Why patients’ stratification based on ERBB4 abundance showed no difference in survival of breast cancer patients of the luminal B subtype deserves further investigation.…”

Section: Discussionmentioning

confidence: 99%

“…After 30 minutes of treatments, cells were washed and scrapped in cold RIPA buffer supplemented with a protease inhibitor cocktail (P8340, Sigma-Aldrich, Saint Louis, MO, USA, 1:100) and Na 3 VO 4 (1 mM). Protein extracts were then analyzed by western blotting, as previously described ( 10 ). Briefly, protein lysates were resolved by sodium dodecyl sulfate (SDS)-polyacrylamide gel electrophoresis and transferred to a nitrocellulose membrane (AmershamTM ProtranTM Premium 0.45 μm 300 mm × 4 m).…”

Section: Methodsmentioning

confidence: 99%

“…ERBB3-ERBB2 heterodimers are considered the most powerful oncogenic driver units among ERBB potential combinations ( 8 ) [reviewed in ( 1 , 9 )]. Intriguingly, higher ERBB3 expression levels correlate with lower relapse-free survival in basal-like/triple-negative (HER2-/ER-/PR-) breast cancer patients, and NRG1/ERBB3/ERBB2 axis was shown to promote anchorage-independent cell growth in basal-like/triple-negative breast cancer cells ( 10 ). EGFR (also known as ERBB1) is associated with cancer progression in several cancer types, including lung, head and neck, colorectal and pancreatic cancers [reviewed in ( 1 – 3 )].…”

Section: Introductionmentioning

confidence: 99%

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Neuregulin 4 Boosts the Efficacy of Anti-ERBB2 Neutralizing Antibodies

et al. 2022

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ERBB4 is a tyrosine kinase receptor reported to exert both oncogenic and tumor suppressor activities. These paradoxical effects were suggested to stem from different ERBB4 homo-/hetero-dimers and/or isoforms. By stratifying breast cancer patients for clinical and molecular subtypes and ERBB4 mRNA abundance, we here report that higher ERBB4 levels correlate with longer relapse-free survival in breast cancer patients of HER2-enriched and luminal A molecular subtypes, proposing a cancer-protecting role for this receptor in these specific subgroups. We also observed that HER2-enriched breast cancers express intermediate ERBB4 mRNA levels compared to luminal and triple-negative/basal-like subgroups, which displayed the highest and the lowest levels, respectively. Inspired by these clinical data, we tested the activation of ERBB4 by Neuregulins as a potential anticancer strategy for HER2+ breast cancers. To this end, we employed two HER2+ breast cancer cellular models (BT474 and SKBR3), which express intermediate/high and low ERBB4 levels, respectively. Cell proliferation and motility were evaluated on these cellular models following treatments with Neuregulin 1 (NRG1), which activates both ERBB3 and ERBB4, or Neuregulin 4 (NRG4), which specifically activates ERBB4. Both NRG1 and NRG4 were used alone or in combination with anti-ERBB2 neutralizing antibodies, namely trastuzumab and pertuzumab. In vitro treatment with NRG1 on BT474 cells restrained cell growth and reduced the anti-proliferative efficacy of trastuzumab. In contrast, treatment with NRG1 on SKBR3 cells increased cell proliferation and migration, and partially or completely impaired the anti-proliferative/anti-migratory action of trastuzumab and/or pertuzumab. Importantly, in both the cell lines, treatment with NRG4 robustly potentiated the anti-proliferative action of trastuzumab and pertuzumab. Collectively, our data in HER2+ breast cancer cells highlight that NRG1 may exert both pro- and anti-proliferative effects, and may reduce the efficacy of anti-HER2 agents, whereas NRG4 may boost the anti-proliferative effects of anti-ERBB2 agents. We propose a provocative paradigm shift in the field of growth factors in cancer progression, suggesting the administration of ERBB4 ligands, such as Neuregulin 4, as a strategy to improve the efficacy of anti-ERBB2 agents.

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Section: Resultsmentioning

confidence: 99%