The cancer glycocalyx mediates intravascular adhesion and extravasation during metastatic dissemination

Offeddu, Giovanni S.; Hajal, Cynthia; Foley, Colleen; Wan, Zhengpeng; Ibrahim, Lina; Coughlin, Mark F.; Kamm, Roger D.

doi:10.1038/s42003-021-01774-2

Cited by 40 publications

(58 citation statements)

References 76 publications

(51 reference statements)

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“…At the same time, direct targeting of HA through CD44 can achieve greater normalizing responses for other patients, as seen in our results for models of advanced, aggressive breast cancer (MDA-MB-468 TC line and primary basal TCs). This observation is consistent with the identification of HA and CD44 as markers of metastatic breast cancer 54,56 , and that their inhibition can prevent vascular colonization by TCs 47 . Importantly, our results show that the vascularized tumoroid models can capture these variations in desmoplastic ECM deposition and resulting impaired MVN perfusion, allowing the assessment of different therapeutic strategies to improve drug penetration.…”

Section: Discussionsupporting

confidence: 91%

Section: Discussionsupporting

confidence: 90%

“…Additionally, the lack of mechanical cues from flow in poorly perfusable tumoroid MVNs may decrease glycocalyx expression 45 . While we observed increased HAS2 expression for MVNs subjected to physiological vascular flow for 48 hours (Figure 2f) and increased vascular HA concentration (Supplementary Figure 6e), consistent with a decreased MVN permeability to dextran (4.1 × 10 −9 cm s −1 compared to 1.1 × 10 −8 cm s −1 in static conditions, Supplementary Figure 6d), we have previously observed functional vascular glycocalyx expression even under static MVN culture conditions 46,47 , as confirmed here by measurable expression levels for HAS2. In addition, no change in permeability or vascular HA was observed in the vicinity of the tumoroids irrespective of flow (Supplementary Figure 6d, e).…”

Section: Resultssupporting

confidence: 82%

“…Because the three TC line tumoroids show different expression and localization of HA, we next assessed how the treatments can affect stromal HA concentrations in the different tumoroids. We found increased protein expression of CD44v, the CD44 isoform associated with TC invasion 47,54 , in the SKBR3 and, more pronouncedly, MDA-MB-468 tumoroids (as opposed to the more benign isoform CD44s, which does not change from controls MVNs), and TGFβ in all three tumoroids, though highest in MCF7 (Figure 4d). Likely as a result of the different target concentrations, the treatments affected the tumoroids differently: All three treatments successfully and severely decreased stromal HA concentrations in the tumoroids, although the effect was greater by blocking TGFβ in the MCF7 and SKBR3 tumoroids and by blocking CD44 in the MDA-MB-468 tumoroids (Figure 4e).…”

Section: Desmoplastic Stroma Normalization Strategies Can Be Ranked For Different Tumoroid Modelsmentioning

confidence: 89%

“…Notably, using our models we have shown that HA exists in two forms in the desmoplastic microenvironment: vascular HA and stromal HA, both of which constitute biomechanical barriers to drug penetration. Vascular HA degradation in the tumoroid microenvironment may not only impair vascular barrier function, but also favor TC vascular migration and metastatic colonization 47 . Stromal HA degradation, instead, can prove beneficial to treatment by improving interstitial transport of therapeutic molecules to TCs.…”

Section: Discussionmentioning

confidence: 99%

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Personalized models of breast cancer desmoplasia reveal biomechanical determinants of drug penetration

Offeddu

Haase

Wan

et al. 2021

Preprint

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Breast cancer desmoplasia heterogeneity contributes to high disease mortality due to discrepancies in treatment efficacy between patients. Personalized in vitro breast cancer models can be used for high throughput testing and ranking of therapeutic strategies to normalize the aberrant microenvironment in a patient-specific manner. Here, tumoroids assembled from patient-derived cells cultured in microphysiological systems including perfusable microvasculature reproduce key aspects of stromal and vascular dysfunction. Increased hyaluronic acid and collagen deposition, loss of vascular glycocalyx and reduced perfusion, and elevated interstitial fluid pressure in the models result in impaired drug distribution to tumor cells. We demonstrate the application of these personalized models as tools to rank molecular therapies for the normalization of the tumoroid microenvironment and to discover new therapeutic targets such as IL8 and CD44, which may ultimately improve drug efficacy in breast cancer patients.

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Section: Discussionsupporting

confidence: 91%

Section: Discussionsupporting

confidence: 90%

Section: Resultssupporting

confidence: 82%

Section: Desmoplastic Stroma Normalization Strategies Can Be Ranked For Different Tumoroid Modelsmentioning

confidence: 89%

Section: Discussionmentioning

confidence: 99%

See 3 more Smart Citations

Personalized models of breast cancer desmoplasia reveal biomechanical determinants of drug penetration

Offeddu

Haase

Wan

et al. 2021

Preprint

Self Cite

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Convergent Approaches to Delineate the Metabolic Regulation of Tumor Invasion by Hyaluronic Acid Biosynthesis

Shimpi

Tan

Vilkhovoy

et al. 2022

Adv Healthcare Materials

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Metastasis is the leading cause of breast cancer‐related deaths and is often driven by invasion and cancer‐stem like cells (CSCs). Both the CSC phenotype and invasion are associated with increased hyaluronic acid (HA) production. How these independent observations are connected, and which role metabolism plays in this process, remains unclear due to the lack of convergent approaches integrating engineered model systems, computational tools, and cancer biology. Using microfluidic invasion models, metabolomics, computational flux balance analysis, and bioinformatic analysis of patient data, the functional links between the stem‐like, invasive, and metabolic phenotype of breast cancer cells as a function of HA biosynthesis are investigated. These results suggest that CSCs are more invasive than non‐CSCs and that broad metabolic changes caused by overproduction of HA play a role in this process. Accordingly, overexpression of hyaluronic acid synthases (HAS) 2 or 3 induces a metabolic phenotype that promotes cancer cell stemness and invasion in vitro and upregulates a transcriptomic signature predictive of increased invasion and worse patient survival. This study suggests that HA overproduction leads to metabolic adaptations to satisfy the energy demands for 3D invasion of breast CSCs highlighting the importance of engineered model systems and multidisciplinary approaches in cancer research.

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Impact of Fibrinogen, Fibrin Thrombi, and Thrombin on Cancer Cell Extravasation Using In Vitro Microvascular Networks

Angelidakis

Chen

Zhang

et al. 2023

Adv Healthcare Materials

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A bidirectional association exists between metastatic dissemination and the hypercoagulable state associated with many types of cancer. As such, clinical studies have provided evidence that markers associated with elevated levels of coagulation and fibrinolysis correlate with decreased patient survival. However, elucidating the mechanisms underpinning the effects of different components of the coagulation system on metastasis formation is challenging both in animal models and 2D models lacking the complex cellular interactions necessary to model both thrombosis and metastasis. Here, an in vitro, 3D, microvascular model for observing the formation of fibrin thrombi is described, which is in turn used to study how different aspects of the hypercoagulable state associated with cancer affect the endothelium. Using this platform, cancer cells expressing ICAM‐1 are shown to form a fibrinogen‐dependent bridge and transmigrate through the endothelium more effectively. Cancer cells are also demonstrated to interact with fibrin thrombi, using them to adhere, spread, and enhance their extravasation efficiency. Finally, thrombin is also shown to enhance cancer cell extravasation. This system presents a physiologically relevant model of fibrin clot formation in the human microvasculature, enabling in‐depth investigation of the cellular interactions between cancer cells and the coagulation system affecting cancer cell extravasation.

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The cancer glycocalyx mediates intravascular adhesion and extravasation during metastatic dissemination

Cited by 40 publications

References 76 publications

Personalized models of breast cancer desmoplasia reveal biomechanical determinants of drug penetration

Personalized models of breast cancer desmoplasia reveal biomechanical determinants of drug penetration

Convergent Approaches to Delineate the Metabolic Regulation of Tumor Invasion by Hyaluronic Acid Biosynthesis

Impact of Fibrinogen, Fibrin Thrombi, and Thrombin on Cancer Cell Extravasation Using In Vitro Microvascular Networks

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