The identification of a TNBC liver metastasis gene signature by sequential CTC‐xenograft modeling

Vishnoi, Monika; Liu, Nikki Haowen; Yin, Wei; Boral, Debasish; Scamardo, Antonio; Hong, David S.; Marchetti, Dario

doi:10.1002/1878-0261.12533

Cited by 40 publications

(32 citation statements)

References 41 publications

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“…Although some studies use CTCs without prior in vitro expansion, CTC-derived cultures or cell lines are also commonly assessed. MICs have thus been successfully identified in CTCs isolated from different types of cancer including breast, lung or colon cancer [315,316,[330][331][332][333][334]. In some studies, intravenous or intra-femoral injections have been directly performed.…”

Section: Functional Assays For Ctcsmentioning

confidence: 99%

EMT-Associated Heterogeneity in Circulating Tumor Cells: Sticky Friends on the Road to Metastasis

Genna

Vanwynsberghe

Villard

et al. 2020

Cancers

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Epithelial–mesenchymal transitions (EMTs) generate hybrid phenotypes with an enhanced ability to adapt to diverse microenvironments encountered during the metastatic spread. Accordingly, EMTs play a crucial role in the biology of circulating tumor cells (CTCs) and contribute to their heterogeneity. Here, we review major EMT-driven properties that may help hybrid Epithelial/Mesenchymal CTCs to survive in the bloodstream and accomplish early phases of metastatic colonization. We then discuss how interrogating EMT in CTCs as a companion biomarker could help refine cancer patient management, further supporting the relevance of CTCs in personalized medicine.

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Section: Functional Assays For Ctcsmentioning

confidence: 99%

EMT-Associated Heterogeneity in Circulating Tumor Cells: Sticky Friends on the Road to Metastasis

Genna

Vanwynsberghe

Villard

et al. 2020

Cancers

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“…Having validated that HLA-ABC can identify both PanCK+ and CD44+ breast cancer cells in mouse bone marrow, we depleted doublets (SSC-H v SSC-A) and dead cells (DAPI+), normal blood cell lineages (leukocytes: CD45+, lymphocytes, mesenchymal, endothelial progenitors: CD34+, macrophages, fibroblasts CD90+/CD105+, mesenchymal, hematopoietic stem cells, NK cells: CD73+) by FACS, and implanted the residual CTC-enriched/lineage-negative cells into NOD scid-gamma (NSG) mice by intracardiac injection [ 20 , 28 , 29 ]. Mice were euthanized after 4–8 months of in vivo selection, and target organs (brain, lung, liver, spleen) were evaluated for the presence of tumor cells by H/E staining and IHC using HLA-ABC (to prove human origin) and GCDFP-15/Mammaglobin (MG) cocktail (to prove mammary origin).…”

Section: Resultsmentioning

confidence: 99%

“…The femur and tibia were isolated, and BM was obtained by flushing the femur and tibia with 1×PBS containing 5 mM of EDTA using 28G×½ needles, followed by centrifugation at 300 × g for 10 min. PBMCs were isolated immediately from the blood and BM for FACS analyses, as previously reported [ 28 , 29 ]. Different organ tissues were also harvested and fixed in 4% paraformaldehyde for downstream analyses.…”

Section: Methodsmentioning

confidence: 99%

Molecular Interplay between Dormant Bone Marrow-Resident Cells (BMRCs) and CTCs in Breast Cancer

Boral

Liu

Kenney

et al. 2020

Cancers

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Despite widespread knowledge that bone marrow-resident breast cancer cells (BMRCs) affect tumor progression, signaling mechanisms of BMRCs implicated in maintaining long-term dormancy have not been characterized. To overcome these hurdles, we developed a new experimental model of clinical dormancy employing patient-isolated Circulating Tumor Cells (de novo CTCs) and their injection in xenografts with subsequent tumor monitoring and CTC characterization (ex vivo CTCs). We hypothesized that significant distinctions exist between signaling pathways of bone marrow-homing vs metastasis-competent CTCs upon transplantation in xenografts. Comparative transcriptomic analyses of ex vivo vs de novo CTCs identified increased mTOR signaling—a critical pathway frequently dysregulated in breast cancer and implicated in cell survival and dormancy—with contrasting actions by its two complementary arms (mTORC2/mTORC1). Heightened mTORC2 downstream targets augmented quiescent CTCs (Ki67−/RBL2+ cells) in paired breast cancer tissues, along with high mTORC2 activity in solitary BMRCs and tissue-resident CTCs. Further, shRNA mediated the knockdown of RICTOR, an essential component of mTORC2, and augmented Ki67/PCNA biomarker expression and proliferation. Collectively, these findings suggest that the balance between mTORC1 vs mTORC2 signaling regulates CTC-associated mitotic and/or dormancy characteristics.

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“…Within the last decades a range of methods have been developed to specifically isolate CTCs [53] and to cultivate these rare cells by optimized in vitro culture conditions such as spheroid and organoid cultures, or by in vivo transplantation into immunodeficient mice [54][55][56][57][58]. To date, the generation of CTC-derived models has been reported for melanoma, breast, colorectal, lung, gastroesophageal, pancreatic, and prostate cancer patients (Table 1) [54][55][56][57][58][59][60][61][62][63][64][65][66][67][68][69]. CTC models from metastatic melanoma patients that recapitulate the patient's disease and responses to therapies have been developed, highlighting the power of such models as potential 'avatars' for testing personalized treatments in the future [60].…”

Section: Preclinical Models Representing Patient-derived Metastasis Fmentioning

confidence: 99%

Predicting therapy response by analysis of metastasis founder cells: emerging perspectives for personalized tumor therapy

Werno

Honarnejad

Polzer

2020

Expert Review of Precision Medicine and Drug Development

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Introduction: Circulating tumor and disseminated cancer cells can be detected after surgical removal of the primary tumor in non-metastatic patients. Despite being considered the prime targets of adjuvant therapy, they have not been implemented into clinical decision making yet. Areas covered: Here we review the recent progress in understanding the biology of circulating tumor cells and disseminated cancer cells as well as the technical challenges associated with quantification, isolation, and preclinical model development. We highlight the first examples of clinical studies in which metastasis founder cells have been used as surrogate markers in adjuvant cancer patients and address the current hurdles in implementing these in routine clinical application. Finally, we provide a perspective on how the combination of technologies to detect and isolate metastasis founders, single-cell multi-omics, development of preclinical models, and their drug responses in specific niches could improve personalized adjuvant treatment strategies. Expert opinion: The specific target cells of adjuvant cancer treatment are metastasis founder cells that remain in the body of the patients after surgical removal of the primary tumor. We, therefore, believe that the success of adjuvant therapies will be improved by implementing circulating and disseminated cancer cells in future clinical decision making.

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The identification of a TNBC liver metastasis gene signature by sequential CTC‐xenograft modeling

Cited by 40 publications

References 41 publications

EMT-Associated Heterogeneity in Circulating Tumor Cells: Sticky Friends on the Road to Metastasis

EMT-Associated Heterogeneity in Circulating Tumor Cells: Sticky Friends on the Road to Metastasis

Molecular Interplay between Dormant Bone Marrow-Resident Cells (BMRCs) and CTCs in Breast Cancer

Predicting therapy response by analysis of metastasis founder cells: emerging perspectives for personalized tumor therapy

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