On-chip recapitulation of the tumor microenvironment: A decade of progress

S M Giannitelli; V Peluzzi; S Raniolo; G Roscilli; M Trombetta; P Mozetic; A Rainer

doi:10.1016/j.biomaterials.2024.122482

On-chip recapitulation of the tumor microenvironment: A decade of progress

Biomaterials. 2024 Apr:306:122482. doi: 10.1016/j.biomaterials.2024.122482. Epub 2024 Jan 22.

Authors

S M Giannitelli¹, V Peluzzi², S Raniolo³, G Roscilli⁴, M Trombetta⁵, P Mozetic⁶, A Rainer⁷

Affiliations

¹ Department of Science and Technology for Sustainable Development and One Health, Università Campus Bio-Medico di Roma, via Álvaro del Portillo, 21, 00128, Rome, Italy. Electronic address: s.giannitelli@unicampus.it.
² Department of Engineering, Università Campus Bio-Medico di Roma, via Álvaro del Portillo 21, 00128, Rome, Italy. Electronic address: v.peluzzi@unicampus.it.
³ Department of Science and Technology for Sustainable Development and One Health, Università Campus Bio-Medico di Roma, via Álvaro del Portillo, 21, 00128, Rome, Italy. Electronic address: s.raniolo@unicampus.it.
⁴ Takis s.r.l., Via di Castel Romano 100, 00128, Rome, Italy. Electronic address: roscilli@takisbiotech.it.
⁵ Department of Science and Technology for Sustainable Development and One Health, Università Campus Bio-Medico di Roma, via Álvaro del Portillo, 21, 00128, Rome, Italy. Electronic address: m.trombetta@unicampus.it.
⁶ Institute of Nanotechnology (NANOTEC), National Research Council, via Monteroni, 73100, Lecce, Italy. Electronic address: pamela.mozetic@cnr.it.
⁷ Department of Engineering, Università Campus Bio-Medico di Roma, via Álvaro del Portillo 21, 00128, Rome, Italy; Fondazione Policlinico Universitario Campus Bio-Medico di Roma, via Álvaro del Portillo 200, 00128, Rome, Italy. Electronic address: a.rainer@unicampus.it.

PMID: 38301325
DOI: 10.1016/j.biomaterials.2024.122482

Abstract

One of the hurdles to the development of new anticancer therapies is the lack of in vitro models which faithfully reproduce the in vivo tumor microenvironment (TME). Understanding the dynamic relationships between the components of the TME in a controllable, scalable, and reliable setting would indeed support the discovery of biological targets impacting cancer diagnosis and therapy. Cancer research is increasingly shifting from traditional two-dimensional (2D) cell culture toward three-dimensional (3D) culture models, which have been demonstrated to increase the significance and predictive value of in vitro data. In this scenario, microphysiological systems (also known as organs-on-chip) have emerged as a relevant technological platform enabling more predictive investigation of cell-cell and cell-ECM interplay in cancer, attracting a significant research effort in the last years. This review illustrates one decade of progress in the field of tumor-microenvironment-on-chip (TMOC) approaches, exploiting either cell-laden microfluidic chambers or microfluidic confined tumor spheroids to model the TME. TMOCs have been designed to recapitulate several aspects of the TME, including tumor cells, the tumor-associated stroma, the immune system, and the vascular component. Significantly, the last aspect has emerged for its pivotal role in orchestrating cellular interactions and modulating drug pharmacokinetics on-chip. A further advancement has been represented by integration of TMOCs into multi-organ microphysiological systems, with the final aim to follow the metastatic cascade to target organs and to study the effects of chemotherapies at a systemic level. We highlight that the increased degree of complexity achieved by the most advanced TMOC models has enabled scientists to shed new light on the role of microenvironmental factors in tumor progression, metastatic cascade, and response to drugs.

Keywords: In vitro models; Organ-on-a-chip; Tumor microenvironment; Tumor spheroids; Vascularization.

Publication types

Review

MeSH terms

Cell Culture Techniques
Humans
Microfluidics
Neoplasms* / pathology
Tumor Microenvironment