BCRP drives intrinsic chemoresistance in chemotherapy-naïve breast cancer brain metastasis.
Rebeca Uceda-CastroAndreia S MargaridoJi-Ying SongMark Cornelis de GooijerHendrik A MessalCecilia R ChambersMax NobisCeren H ÇitirikkayaKerstin HahnDanielle SeinstraDavid HerrmannPaul TimpsonPieter WesselingOlaf van TellingenClaire VenninJacco van RheenenPublished in: Science advances (2023)
Although initially successful, treatments with chemotherapy often fail because of the recurrence of chemoresistant metastases. Since these tumors develop after treatment, resistance is generally thought to occur in response to chemotherapy. However, alternative mechanisms of intrinsic chemoresistance in the chemotherapy-naïve setting may exist but remain poorly understood. Here, we study drug-naïve murine breast cancer brain metastases (BCBMs) to identify how cancer cells growing in a secondary site can acquire intrinsic chemoresistance without cytotoxic agent exposure. We demonstrate that drug-naïve murine breast cancer cells that form cancer lesions in the brain undergo vascular mimicry and concomitantly express the adenosine 5'-triphosphate-binding cassette transporter breast cancer resistance protein (BCRP), a common marker of brain endothelial cells. We reveal that expression of BCRP by the BCBM tumor cells protects them against doxorubicin and topotecan. We conclude that BCRP overexpression can cause intrinsic chemoresistance in cancer cells growing in metastatic sites without prior chemotherapy exposure.
Keyphrases
- locally advanced
- endothelial cells
- small cell lung cancer
- brain metastases
- white matter
- resting state
- squamous cell carcinoma
- breast cancer cells
- gene expression
- cancer stem cells
- poor prognosis
- chemotherapy induced
- emergency department
- rectal cancer
- papillary thyroid
- multiple sclerosis
- genome wide
- binding protein
- single cell
- small molecule
- young adults
- blood brain barrier
- free survival
- adverse drug
- amino acid