Enhanced Directional Migration of Cancer Stem Cells in 3D Aligned Collagen Matrices

Ray, Arja; Slama, Zachary M.; Morford, Rachel K.; Madden, Samantha A.; Provenzano, Paolo P.

doi:10.1016/j.bpj.2017.01.007

Cited by 141 publications

(186 citation statements)

References 75 publications

Supporting

Mentioning

174

Contrasting

Order By: Relevance

“…It is well established that the presence of linearized collagen fibers in tumors facilitates metastasis by providing tracks that cancer cells exploit for invading surrounding tissues (Condeelis & Segall, 2003;Provenzano et al, 2006;Levental et al, 2009;Oudin et al, 2016). Furthermore, cancer cells have been shown to invade more efficiently through lattices of linear collagen engineered in vitro than through disorganized lattices of the same density or stiffness (Kraning-Rush et al, 2013;Riching et al, 2014;Ray et al, 2017). In agreement with these observations, we show that cancer cells are more motile on WISP1-linearized Col I lattices than on nonlinearized control Col I lattices.…”

Section: Discussionsupporting

confidence: 87%

“…Type I collagen is one of the most abundant proteins deposited in the ECM of breast tumors and of many other cancer types (Kalluri & Zeisberg, 2006;Naba et al, 2014). In particular, increased linearization of fibrillar collagen, which has been proposed to arise from the mechanical tension induced by cancer cells and cancer-associated fibroblasts (Butcher et al, 2009), facilitates tumor cell invasion and metastasis by providing tracks on which tumor cells can more easily migrate (Condeelis & Segall, 2003;Provenzano et al, 2006;Levental et al, 2009;Kraning-Rush et al, 2013;Riching et al, 2014;Oudin et al, 2016;Ray et al, 2017). In particular, increased linearization of fibrillar collagen, which has been proposed to arise from the mechanical tension induced by cancer cells and cancer-associated fibroblasts (Butcher et al, 2009), facilitates tumor cell invasion and metastasis by providing tracks on which tumor cells can more easily migrate (Condeelis & Segall, 2003;Provenzano et al, 2006;Levental et al, 2009;Kraning-Rush et al, 2013;Riching et al, 2014;Oudin et al, 2016;Ray et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

“…Consequently, changes in type I collagen organization have a profound impact on tumor cell behavior and on disease progression (Kalluri & Zeisberg, 2006;Butcher et al, 2009;Joyce & Pollard, 2009;Lu et al, 2012). In particular, increased linearization of fibrillar collagen, which has been proposed to arise from the mechanical tension induced by cancer cells and cancer-associated fibroblasts (Butcher et al, 2009), facilitates tumor cell invasion and metastasis by providing tracks on which tumor cells can more easily migrate (Condeelis & Segall, 2003;Provenzano et al, 2006;Levental et al, 2009;Kraning-Rush et al, 2013;Riching et al, 2014;Oudin et al, 2016;Ray et al, 2017). On this basis, collagen linearization is considered a key feature of metastatic carcinomas such as triple-negative breast cancers (TNBCs) and is predictive of poor prognosis (Colpaert et al, 2001;Conklin et al, 2011).…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

The tumor cell‐secreted matricellular protein WISP 1 drives pro‐metastatic collagen linearization

Jia

Janjanam

et al. 2019

The EMBO Journal

View full text Add to dashboard Cite

Collagen linearization is a hallmark of aggressive tumors and a key pathogenic event that promotes cancer cell invasion and metastasis. Cell‐generated mechanical tension has been proposed to contribute to collagen linearization in tumors, but it is unknown whether other mechanisms play prominent roles in this process. Here, we show that the secretome of cancer cells is by itself able to induce collagen linearization independently of cell‐generated mechanical forces. Among the tumor cell‐secreted factors, we find a key role in this process for the matricellular protein WISP1 (CCN4). Specifically, WISP1 directly binds to type I collagen to promote its linearization in vitro (in the absence of cells) and in vivo in tumors. Consequently, WISP1‐induced type I collagen linearization facilitates tumor cell invasion and promotes spontaneous breast cancer metastasis, without significantly affecting gene expression. Furthermore, higher WISP1 expression in tumors from cancer patients correlates with faster progression to metastatic disease and poor prognosis. Altogether, these findings reveal a conceptually novel mechanism whereby pro‐metastatic collagen linearization critically depends on a cancer cell‐secreted factor.

show abstract

Section: Discussionsupporting

confidence: 87%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

The tumor cell‐secreted matricellular protein WISP 1 drives pro‐metastatic collagen linearization

Jia

Janjanam

et al. 2019

The EMBO Journal

View full text Add to dashboard Cite

show abstract

“…Collagen matrices preparation was adapted from (Ray et al, 2017b) with modifications. Briefly, high concentration rat-tail collagen I (VWR) was neutralized with a 1:1 ratio of 100 mM HEPES (Thermo Fisher Scientific) in 2X PBS and completed to a final concentration of 3 mg/mL with DMEM (Corning) supplemented with 10% FBS (which introduces FN).…”

Section: Preparation Of 3d Collagen Matricesmentioning

confidence: 99%

“…Cell migration data was collected by imaging using a custom-built multi-photon laser-scanning microscope (MPLSM) (Prairie Technologies/Bruker) using a Mai Tai Ti:Sapphire laser (Spectra-Physics) to simultaneously generate MPE and SHG to visualize cells and collagen, respectively, at an excitation wavelength of 880 nm with a custom-built temperature-controlled stage insert, as described previously (Ray et al, 2017a(Ray et al, , 2017b. Briefly, time-lapse imaging of T cells inside 3D collagen matrix and on tumor slices, was obtained by creating two-channel (T cells and collagen) or three-channel (T cells, collagen, and KPC-tissue/KPCT-carcinoma cells) Z-stacks of 75 µm depth at 5 µm steps, at each stage position, every 1.5 min over at least 45 min of imaging.…”

Section: Multiphoton Microscopy Of 3d Live Cell Imaging and Analysis mentioning

confidence: 99%

Engineering T cells to enhance 3D migration through structurally and mechanically complex tumor microenvironments

Tabdanov

Rodríguez-Merced

Cartagena‐Rivera

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

Defining the principles of T cell migration in structurally and mechanically complex tumor microenvironments is critical to understanding sanctuaries from antitumor immunity and optimizing T cellrelated therapeutic strategies. To enhance T cell migration through complex microenvironments, we engineered nanotextured platforms that allowed us to define how the balance between T cell phenotypes influences migration in response to tumor-mimetic structural and mechanical cues and characterize a mechanical optimum for migration that can be perturbed by manipulating an axis between microtubule stability and force generation. In 3D environments and live tumors, we demonstrate that microtubules instability, leading to increased Rho pathway-dependent cell contractility, promotes migration while clinically used microtubule-targeting chemotherapies profoundly decrease effective migration. Indeed, we show that rational manipulation of the microtubule-contractility axis, either pharmacologically or through genome engineering, results in engineered T cells that more effectively move through and interrogate 3D matrix and tumor volumes. This suggests that engineering cells to better navigate through 3D microenvironments could be part of an effective strategy to enhance efficacy of immune therapeutics.

show abstract

Changes of Mutations and Copy‐Number and Enhanced Cell Migration during Breast Tumorigenesis

Lee

Kim

et al. 2022

Advanced Biology

View full text Add to dashboard Cite

CSCs contribute to tumor heterogeneity and metastatic dissemination. [1] Breast CSCs have been demonstrated to mediate cancer cell invasiveness and metastasis. [1,3] A subpopulation of breast CSCs characterized with CD44 + /CD24 −/low are more resistant to therapy and are more invasive than breast non-CSCs. [4][5][6] Contact guidance of extracellular matrix (ECM) anisotropy that recapitulates a tumor microenvironment is an important factor in modeling tumor progression and metastasis. [7][8][9] Over the past several years, advances in the fabrication of ECM-mimetic nanoscale topography have facilitated the study of how cells sense contact guidance cues and of cell-matrix interactions. [8,[10][11][12][13]

show abstract

Enhanced Directional Migration of Cancer Stem Cells in 3D Aligned Collagen Matrices

Cited by 141 publications

References 75 publications

The tumor cell‐secreted matricellular protein WISP 1 drives pro‐metastatic collagen linearization

The tumor cell‐secreted matricellular protein WISP 1 drives pro‐metastatic collagen linearization

Engineering T cells to enhance 3D migration through structurally and mechanically complex tumor microenvironments

Changes of Mutations and Copy‐Number and Enhanced Cell Migration during Breast Tumorigenesis

Contact Info

Product

Resources

About