Investigating breast cancer cell behavior using tissue engineering scaffolds

Authors

Khadidiatou Guiro, Newark College of Engineering
Shyam A. Patel, Rutgers New Jersey Medical School
Steven J. Greco, Rutgers New Jersey Medical School
Pranela Rameshwar, Rutgers New Jersey Medical School
Treena L. Arinzeh, Newark College of Engineering

Document Type

Article

Publication Date

4-2-2015

Abstract

Despite early detection through the use of mammograms and aggressive intervention, breast cancer (BC) remains a clinical dilemma. BC can resurge after >10 years of remission. Studies indicate that BC cells (BCCs) with self-renewal and chemoresistance could be involved in dormancy. The majority of studies use in vitro, two-dimensional (2-D) monolayer cultures, which do not recapitulate the in vivo microenvironment. Thus, to determine the effect of three-dimensional (3-D) microenvironment on BCCs, this study fabricated tissue engineering scaffolds made of poly (ε-caprolactone) (PCL) having aligned or random fibers. Random and aligned fibers mimic, respectively, the random and highly organized collagen fibers found in the tumor extracellular matrix. Chemoresistant BCCs were obtained by treating with carboplatin. Western blot analysis of carboplatin resistant (treated) MDA-MB-231 (highly invasive, basal-like) and T47D (low-invasive, luminal) BCCs showed an increase in Bcl-2, Oct-4 and Sox-2, suggesting protection from apoptosis and increase in stem-like markers. Further studies with MDA-MB-231 BCCs seeded on the scaffolds showed little to no change in cell number over time for non-treated BCCs whereas on tissue culture polystyrene (TCP), non-treated BCCs displayed a significant increase in cell number at days 4 and 7 as compared to day 1 (p<0.05). Treated BCCs did not proliferate on TCP and the fibrous scaffolds. Little to no cyclin D1 was expressed for non-treated BCCs on TCP. On fibrous scaffolds, non-treated BCCs stained for cyclin D1 during the 7-day culture period. Treated BCCs expressed cyclin D1 on TCP and fibrous scaffolds during the 7-day culture period. Proliferation, viability and cell cycle analysis indicated that this 3-D culture prompted the aggressive BCCs to adopt a dormant phenotype, while the treated BCCs retained their phenotype. The findings indicate that random and aligned fibrous PCL scaffolds may provide a useful system to study how the 3-D microenvironment affects the behavior of BCCs.

Identifier

84926631267 (Scopus)

Publication Title

Plos One

External Full Text Location

https://doi.org/10.1371/journal.pone.0118724

e-ISSN

19326203

PubMed ID

25837691

Issue

4

Volume

10

Grant

W81XWH-11-1-0276

Fund Ref

U.S. Department of Defense

Recommended Citation

Guiro, Khadidiatou; Patel, Shyam A.; Greco, Steven J.; Rameshwar, Pranela; and Arinzeh, Treena L., "Investigating breast cancer cell behavior using tissue engineering scaffolds" (2015). Faculty Publications. 7064.
https://digitalcommons.njit.edu/fac_pubs/7064