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Showing 1–17 of 17 results
Advanced filters: Author: Cyrus M. Ghajar Clear advanced filters

  • Ghajar and colleagues report that astrocyte-deposited laminin-211 promotes the quiescence of disseminated tumor cells in the brain, in a manner dependent on the cytoplasmic sequestration of YAP by dystroglycan.

    • Jinxiang Dai
    • Patrick J. Cimino
    • Cyrus M. Ghajar
    Research
    Nature Cancer
    Volume: 3, P: 25-42

  • Bissell, Ghajar and colleagues use organotypic culture systems and in vivo mouse and zebrafish models to reveal the distinct effects of different microvascular niches on tumour cell dormancy. They report that although the stable microvasculature promotes cancer cell quiescence through the production of thrombospondin-1, cancer cells residing near neovascular tips are induced to grow through the action of TGF-β and periostin.

    • Cyrus M. Ghajar
    • Héctor Peinado
    • Mina J. Bissell
    Research
    Nature Cell Biology
    Volume: 15, P: 807-817

  • In a recent study in mice, researchers combined tumor barcoding with unbiased genomic analysis and identified Cd109 as a hub gene involved in metastatic progression. They show that pharmacological inhibition of its downstream effectors JAK1 and STAT3 curtails metastatic growth.

    • Laura Pisarsky
    • Jinxiang Dai
    • Cyrus M Ghajar
    News & Views
    Nature Medicine
    Volume: 23, P: 275-276

  • Two studies in mice identify mechanisms by which tumour cells disseminate in very early breast cancer. Both show that these cells colonize distant tissues more efficiently than their later counterparts. See Article p.552 & Letter p.588

    • Cyrus M. Ghajar
    • Mina J. Bissell
    News & Views
    Nature
    Volume: 540, P: 528-529

  • This Opinion article advocates therapeutically targeting the niches that harbour dormant disseminated tumour cells in order to make them susceptible to cytotoxic agents. Similar strategies have sensitized leukaemic cells and latent HIV to therapy, and such an approach might delay or even prevent metastasis.

    • Cyrus M. Ghajar
    Reviews
    Nature Reviews Cancer
    Volume: 15, P: 238-247

  • Aberrant production of oestrogens by adipose stromal cells is a driving factor in oestrogen receptor-positive breast cancer. Here the authors discover that oestrogen synthesis in adipose tissue is regulated by mechanical stress, and reveal how this effect is mediated.

    • Sagar Ghosh
    • Keith Ashcraft
    • Rong Li
    Research
    Nature Communications
    Volume: 4, P: 1-14

  • Exosomes originating from lung-, liver- and brain-tropic tumour cells are preferentially incorporated by specific resident cells of the target organs, thus preparing the site for metastasis; the expression of distinct combinations of exosomal integrin proteins determines the exosomal targeting to each of the three organs, and blocking these integrins reduces organotropic exosome uptake by the target organs, thereby reducing the likelihood of organotropic metastasis.

    • Ayuko Hoshino
    • Bruno Costa-Silva
    • David Lyden
    Research
    Nature
    Volume: 527, P: 329-335

  • Fine-scale geospatial mapping of overweight and wasting (two components of the double burden of malnutrition) in 105 LMICs shows that overweight has increased from 5.2% in 2000 to 6.0% in children under 5 in 2017. Although overall wasting decreased over the same period, most countries are not on track to meet the World Health Organization’s Global Nutrition Target of <5% in over half of LMICs by 2025.

    • Damaris K. Kinyoki
    • Jennifer M. Ross
    • Simon I. Hay
    ResearchOpen Access
    Nature Medicine
    Volume: 26, P: 750-759

  • This Review summarizes the natural progression of pre-metastatic niche formation and evolution, highlighting recent advances and future hurdles.

    • Héctor Peinado
    • Haiying Zhang
    • David Lyden
    Reviews
    Nature Reviews Cancer
    Volume: 17, P: 302-317

  • Exosomes can transfer proteins and nucleic acids from one cell to another, altering the phenotype of the recipient cell. In the case of cancer, tumor-derived exosomes have been shown to promote tumor cell proliferation. Now, in a mouse model of melanoma, Peinado et al. report that exosomes derived from highly metastatic tumor cells can influence bone marrow cells, resulting in increased recruitment of provasculogenic bone marrow progenitors to sites of metastasis, increased primary tumor growth and metastatic spread.

    • Héctor Peinado
    • Maša Alečković
    • David Lyden
    Research
    Nature Medicine
    Volume: 18, P: 883-891

  • Goddard et al review recent advances in our understanding of dormant tumour cells, highlight their cross-talk with immune responses, and elaborate therapeutic implications to treat metastatic malignancies.

    • Erica T. Goddard
    • Ivana Bozic
    • Cyrus M. Ghajar
    Reviews
    Nature Cell Biology
    Volume: 20, P: 1240-1249