Co-administration of H-ferritin-doxorubicin and Trastuzumab in neoadjuvant setting improves efficacy and prevents cardiotoxicity in HER2 + murine breast cancer model.
Francesco AndreataA BonizziM SevieriM TruffiM MonieriL SitiaF SilvaL SorrentinoR AlleviP ZerbiB MarchiniE LonghiRoberta OttriaSara CasatiRenzo VannaC MorassoM BelliniD ProsperiF CorsiS MazzucchelliPublished in: Scientific reports (2020)
Neoadjuvant chemotherapy has been established as the standard of care for HER2-positive breast cancer since it allows cancer down-staging, up to pathological complete response. The standard of care in the neoadjuvant setting for HER2-positive breast cancer is a combination of highly cytotoxic drugs such as anthracyclines and the anti-HER2 monoclonal antibody. Despite this cocktail allows a pathological complete response in up to 50%, their co-administration is strongly limited by intrinsic cardiotoxicity. Therefore, only a sequential administration of anthracyclines and the anti-HER2 treatment is allowed. Here, we propose the anthracycline formulation in H-Ferritin nanocages as promising candidate to solve this unmet clinical need, thanks to its capability to increase anthracyclines efficacy while reducing their cardiotoxicity. Treating a murine model of HER2-positive breast cancer with co-administration of Trastuzumab and H-Ferritin anthracycline nanoformulation, we demonstrate an improved tumor penetration of drugs, leading to increased anticancer efficacy and reduced of cardiotoxicity.
Keyphrases
- positive breast cancer
- neoadjuvant chemotherapy
- locally advanced
- lymph node
- monoclonal antibody
- rectal cancer
- healthcare
- palliative care
- drug delivery
- epidermal growth factor receptor
- sentinel lymph node
- radiation therapy
- cancer therapy
- mouse model
- metastatic breast cancer
- pain management
- chronic pain
- combination therapy
- affordable care act