In-depth characterization of a new patient-derived xenograft model for metaplastic breast carcinoma to identify viable biologic targets and patterns of matrix evolution within rare tumor types.
M D MatossianT ChangM K WrightH E BurksS ElliottR A SabolH WathieuG O WindsorM S AlzoubiC T KingJ B BursavichA M HamJ J SavoieK NguyenM BaddooE FlemingtonO SirenkoE F CromwellK L HebertF LauR IzadpanahH BrownS SinhaJ ZabaletaA I RikerK MorozL MieleA H ZeaA OchoaB A BunnellB M Collins-BurowE C MartinMatthew E BurowPublished in: Clinical & translational oncology : official publication of the Federation of Spanish Oncology Societies and of the National Cancer Institute of Mexico (2021)
Metaplastic breast carcinoma (MBC) is a rare breast cancer subtype with rapid growth, high rates of metastasis, recurrence and drug resistance, and diverse molecular and histological heterogeneity. Patient-derived xenografts (PDXs) provide a translational tool and physiologically relevant system to evaluate tumor biology of rare subtypes. Here, we provide an in-depth comprehensive characterization of a new PDX model for MBC, TU-BcX-4IC. TU-BcX-4IC is a clinically aggressive tumor exhibiting rapid growth in vivo, spontaneous metastases, and elevated levels of cell-free DNA and circulating tumor cell DNA. Relative chemosensitivity of primary cells derived from TU-BcX-4IC was performed using the National Cancer Institute (NCI) oncology drug set, crystal violet staining, and cytotoxic live/dead immunofluorescence stains in adherent and organoid culture conditions. We employed novel spheroid/organoid incubation methods (Pu·MA system) to demonstrate that TU-BcX-4IC is resistant to paclitaxel. An innovative physiologically relevant system using human adipose tissue was used to evaluate presence of cancer stem cell-like populations ex vivo. Tissue decellularization, cryogenic-scanning electron microscopy imaging and rheometry revealed consistent matrix architecture and stiffness were consistent despite serial transplantation. Matrix-associated gene pathways were essentially unchanged with serial passages, as determined by qPCR and RNA sequencing, suggesting utility of decellularized PDXs for in vitro screens. We determined type V collagen to be present throughout all serial passage of TU-BcX-4IC tumor, suggesting it is required for tumor maintenance and is a potential viable target for MBC. In this study we introduce an innovative and translational model system to study cell-matrix interactions in rare cancer types using higher passage PDX tissue.
Keyphrases
- single cell
- circulating tumor
- adipose tissue
- electron microscopy
- rheumatoid arthritis
- cell therapy
- stem cells
- high resolution
- type diabetes
- metabolic syndrome
- single molecule
- gene expression
- emergency department
- palliative care
- skeletal muscle
- mesenchymal stem cells
- transcription factor
- induced apoptosis
- genome wide
- signaling pathway
- high throughput
- oxidative stress
- optical coherence tomography
- insulin resistance
- risk assessment
- squamous cell carcinoma
- mass spectrometry
- electronic health record
- induced pluripotent stem cells