Bioengineered Hydrogels Recapitulate Fibroblast Heterogeneity in Cancer

Author:

Ho Nicholas Ching Wei1,Yap Josephine Yu Yan1,Zhao Zixuan2,Wang Yunyun1,Fernando Kanishka1,Li Constance H34,Kwang Xue Lin3,Quah Hong Sheng34,Arcinas Camille4,Iyer N. Gopalakrishna34,Fong Eliza Li Shan125ORCID

Affiliation:

1. Translational Tumor Engineering Laboratory, Department of Biomedical Engineering National University of Singapore Singapore 119276 Singapore

2. The N.1 Institute for Health National University of Singapore Singapore 117456 Singapore

3. Cancer Therapeutics Research Laboratory National Cancer Centre Singapore Singapore 168583 Singapore

4. Duke‐NUS Medical School National University of Singapore Singapore 169857 Singapore

5. Cancer Science Institute National University of Singapore Singapore 117599 Singapore

Abstract

AbstractRecently mapped transcriptomic landscapes reveal the extent of heterogeneity in cancer‐associated fibroblasts (CAFs) beyond previously established single‐gene markers. Functional analyses of individual CAF subsets within the tumor microenvironment are critical to develop more accurate CAF‐targeting therapeutic strategies. However, there is a lack of robust preclinical models that reflect this heterogeneity in vitro. In this study, single‐cell RNA sequencing datasets acquired from head and neck squamous cell carcinoma tissues to predict microenvironmental and cellular features governing individual CAF subsets are leveraged. Some of these features are then incorporated into a tunable hyaluronan‐based hydrogel system to culture patient‐derived CAFs. Control over hydrogel degradability and integrin adhesiveness enabled derivation of the predominant myofibroblastic and inflammatory CAF subsets, as shown through changes in cell morphology and transcriptomic profiles. Last, using these hydrogel‐cultured CAFs, microtubule dynamics are identified, but not actomyosin contractility, as a key mediator of CAF plasticity. The recapitulation of CAF heterogeneity in vitro using defined hydrogels presents unique opportunities for advancing the understanding of CAF biology and evaluation of CAF‐targeting therapeutics.

Publisher

Wiley

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