Tumor mechanics and metabolic dysfunction

Tung, Jason C.; Barnes, J. Matthew; Desai, Shraddha; Sistrunk, Christopher; Conklin, Matthew W.; Schedin, Pepper; Eliceiri, Kevin W.; Keely, Patricia J.; Seewaldt, Victoria L.; Weaver, Valerie M.

doi:10.1016/j.freeradbiomed.2014.11.020

Cited by 104 publications

(81 citation statements)

References 154 publications

(194 reference statements)

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“…Here, the identification of glutaminolysis as a mechanoactivated process coregulated with aerobic glycolysis advances our understanding of the regulatory hierarchy seen in the metabolic reprogramming in PH. Such an interface between stiffness and metabolism draws parallels to related reprogramming events proposed in tumors in relation to matrix remodeling (29). By its direct causative relation to metabolic dysregulation, it also reinforces the paradigm of vascular stiffness as an initiating pathogenic trigger of this disease rather than merely an end-stage feature.…”

Section: The Yap/taz-gls Axis Induces Glycolysis and Glutaminolysis Isupporting

confidence: 54%

Vascular stiffness mechanoactivates YAP/TAZ-dependent glutaminolysis to drive pulmonary hypertension

Bertero¹,

Oldham²,

Cottrill³

et al. 2016

Journal of Clinical Investigation

329

338

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Section: The Yap/taz-gls Axis Induces Glycolysis and Glutaminolysis Isupporting

confidence: 54%

Vascular stiffness mechanoactivates YAP/TAZ-dependent glutaminolysis to drive pulmonary hypertension

Bertero¹,

Oldham²,

Cottrill³

et al. 2016

Journal of Clinical Investigation

329

338

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“…Alternatively, when the TKIs do not exert vascular normalization or cause excessive vascular pruning, TKI treatment would add no benefit to chemotherapy. In a preclinical study, we demonstrated that measuring tumor hypoxia with 18 F-fluoromisonidazole PET mirrored the status of vascular normalization. We incorporated this technique in the neoadjuvant setting of breast cancer patients treated with the TKI nintedanib in combination with chemotherapy.…”

Section: Translational Relevancementioning

confidence: 98%

“…We hypothesized that tracing the tumor stromal oxygenation levels with 18 F-fluoromisonidazole-positron emission tomography (18F-FMISO-PET) during a WoO would allow detecting the patients that are or are not candidates for nintedanib therapy. The justification of this hypothesis is that it is widely accepted that abnormal stroma is hypoxic as well (5,(18)(19)(20)(21).…”

Section: Introductionmentioning

confidence: 99%

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18F-fluoromisonidazole PET and Activity of Neoadjuvant Nintedanib in Early HER2-Negative Breast Cancer: A Window-of-Opportunity Randomized Trial

Quintela‐Fandino

Lluch

Manso

et al. 2017

Clinical Cancer Research

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Purpose: We previously detected promising efficacy of neoadjuvant nintedanib (a multityrosine kinase inhibitor, TKI) in early HER2-negative breast cancer. In a preclinical study, we monitored stromal hypoxia with 18 F-fluoromisonidazole-positron emission tomography (18F-FMISO-PET); we found that reoxygenation of tumors (or lack of it) during a window-ofopportunity (WoO) treatment with TKIs correlated with the benefit (or lack of it) from TKI-plus-chemotherapy combinations. We studied the predictive role of 18F-FMISO-PET for the TKI nintedanib in the neoadjuvant setting in a phase II WoO randomized trial.Experimental Design: Patients were randomized to a 14-day WoO of nintedanib preceded and followed by an 18F-FMISO-PET, followed by nintedanib plus weekly paclitaxel (Arm A) or an 18F-FMISO-PET followed by weekly paclitaxel (Arm B) before surgery. The endpoint was residual cancer burden (RCB). The objective was to detect the patients with no response (RCB-III) on the basis of the baseline or evolutive 18F-FMISO-PET values/ changes.Results: One-hundred and thirty HER2-negative patients were randomized. Seventeen (27.9%), 34 (55.7%), and 8 (13.1%) patients had an RCB of III, II, and I/0, respectively, in Arm A. In this arm, baseline hypoxic tumors had a 4.4-fold higher chance of experiencing RCB ¼ 3 (P ¼ 0.036) compared with baseline normoxic tumors. Nintedanib WoO induced tumor reoxygenation in 24.5% of the patients; those not reoxygenating showed a trend toward higher chance of experiencing RCB-III (6.4-fold; P ¼ 0.09). In Arm B, 18F-FMISO-PET lacked predictive/ prognostic value.Conclusions: Baseline hypoxic tumors (measured with 18F-FMISO-PET) do not benefit from neoadjuvant nintedanib.

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“…It is now clearly evident that tumors contain various non-cancer cells including fibroblasts, vascular endothelial cells, immune cells -with T-cells as potent mediators of antitumor immunity -and soluble factors [2][3][4] that, in dynamic reciprocity with cancer cells, make up the tumor microenvironment (TME). TME is organ-specific in terms of interstitial cells and extracellular matrix (ECM), which condition tissue oxygen levels and pH, adding further layers of complexity [5,6].…”

Section: Introductionmentioning

confidence: 99%

Mesenchymal traits at the convergence of tumor-intrinsic and -extrinsic mechanisms of resistance to immune checkpoint blockers

Trono¹,

Sistigu

Palermo³

et al. 2017

Emerging Topics in Life Sciences

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Correspondence: Paola Nisticò ( paola.nistico@ifo.gov.it)Targeting of immune checkpoint blockers (ICBs), such as cytotoxic T-lymphocyte antigen-4 and programmed-death 1/programmed-death ligand 1, has dramatically changed the landscape of cancer treatment. Seeing patients who were refractory to conventional therapy recover after immunotherapy, with high rates of objective durable responses and increased overall survival, has raised great enthusiasm in cancer care and research. However, to date, only a restricted portion of patients benefit from these therapies, due to natural and acquired resistance relying on the ever-evolving cross-talk between tumor and stromal cells. Here, we review the convergence of tumor-intrinsic and -extrinsic cues, both affecting tumor plasticity and tumor stroma leading to an immunosuppressive tumor microenvironment, which may account for the heterogeneous responses and resistance to ICB therapies. A deeper knowledge of the mechanisms and fingerprints involved in natural and acquired resistance is likely to bring clinical benefit to the majority of patients, offering important clues for overcoming drug resistance and boosting the effectiveness of treatment. We discuss the need to define tumor subtypes based on the tumor, immune and stromal gene signature and propose that the better we understand tumor mesenchymal traits, the more we will be able to identify predictive biomarkers of response to ICB treatments.

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Tumor mechanics and metabolic dysfunction

Cited by 104 publications

References 154 publications

Vascular stiffness mechanoactivates YAP/TAZ-dependent glutaminolysis to drive pulmonary hypertension

Vascular stiffness mechanoactivates YAP/TAZ-dependent glutaminolysis to drive pulmonary hypertension

18F-fluoromisonidazole PET and Activity of Neoadjuvant Nintedanib in Early HER2-Negative Breast Cancer: A Window-of-Opportunity Randomized Trial

Mesenchymal traits at the convergence of tumor-intrinsic and -extrinsic mechanisms of resistance to immune checkpoint blockers

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