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We began analyzing https://www.nature.com/articles/srep00765, but it redirected us to https://www.nature.com/articles/srep00765. The analysis below is for the second page.

Title[redir]:
12-Chemokine Gene Signature Identifies Lymph Node-like Structures in Melanoma: Potential for Patient Selection for Immunotherapy? | Scientific Reports
Description:
We have interrogated a 12-chemokine gene expression signature (GES) on genomic arrays of 14,492 distinct solid tumors and show broad distribution across different histologies. We hypothesized that this 12-chemokine GES might accurately predict a unique intratumoral immune reaction in stage IV (non-locoregional) melanoma metastases. The 12-chemokine GES predicted the presence of unique, lymph node-like structures, containing CD20+ B cell follicles with prominent areas of CD3+ T cells (both CD4+ and CD8+ subsets). CD86+, but not FoxP3+, cells were present within these unique structures as well. The direct correlation between the 12-chemokine GES score and the presence of unique, lymph nodal structures was also associated with better overall survival of the subset of melanoma patients. The use of this novel 12-chemokine GES may reveal basic information on in situ mechanisms of the anti-tumor immune response, potentially leading to improvements in the identification and selection of melanoma patients most suitable for immunotherapy.

Matching Content Categories {πŸ“š}

  • Science
  • Education
  • Telecommunications

Content Management System {πŸ“}

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Custom-built

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Traffic Estimate {πŸ“ˆ}

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🌠 Phenomenal Traffic: 5M - 10M visitors per month


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Keywords {πŸ”}

chemokine, melanoma, article, structures, cancer, lymph, cells, tumor, samples, signature, immune, patients, google, scholar, nature, expression, ges, gene, nodelike, cell, genes, ectopic, cas, analysis, data, patient, presence, response, ccl, figure, immunotherapy, solid, unique, score, tumors, clinical, survival, based, sets, tlelns, pca, metastases, human, shown, moffitt, information, high, probe, center, content,

Topics {βœ’οΈ}

nature portfolio privacy policy functional immune nature author information authors functional nature advertising cancer research nature rev nature social media 0/ reprints receive immune-based therapies basler tri-linear-array creative commons attribution-noncommercial high-resolution microcapillary electrophoresis t-cell antitumor response avidin-biotin complex method profound anti-tumor activity ectopic b-cell clusters average z-score based anti-tumor immune response affymetrix hursta-2a520709 genechips chemokine-secreting dendritic cells gov/geo/query/acc ventana medical systems tumour microenvironment thorsten t-cell transfer immunotherapy immune-based therapies permissions skin cancers tumor-infiltrating immune cells ectopic lymph node gene expression signature gene expression signatures gene expression microarrays anti-ctla4 antibody deidentified clinical data random representative section ectopic lymph nodes mrna microarray analysis gene chip technology laser capture microdissection immune checkpoint proteins immune checkpoint inhibition privacy immune-related ges t-cell clonality ovarian carcinomas competing financial interests immune-related biomarkers

Questions {❓}

  • 12-Chemokine Gene Signature Identifies Lymph Node-like Structures in Melanoma: Potential for Patient Selection for Immunotherapy?
  • 12-Chemokine Gene Signature Identifies Lymph Node-like Structures in Melanoma: Potential for Patient Selection for Immunotherapy?
  • Biomarkers for immune checkpoint inhibition in sarcomas – are we close to clinical implementation?
  • Chemokines: can effector cells be re-directed to the site of tumor?

Schema {πŸ—ΊοΈ}

WebPage:
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         headline:12-Chemokine Gene Signature Identifies Lymph Node-like Structures in Melanoma: Potential for Patient Selection for Immunotherapy?
         description:We have interrogated a 12-chemokine gene expression signature (GES) on genomic arrays of 14,492 distinct solid tumors and show broad distribution across different histologies. We hypothesized that this 12-chemokine GES might accurately predict a unique intratumoral immune reaction in stage IV (non-locoregional) melanoma metastases. The 12-chemokine GES predicted the presence of unique, lymph node-like structures, containing CD20+ B cell follicles with prominent areas of CD3+ T cells (both CD4+ and CD8+ subsets). CD86+, but not FoxP3+, cells were present within these unique structures as well. The direct correlation between the 12-chemokine GES score and the presence of unique, lymph nodal structures was also associated with better overall survival of the subset of melanoma patients. The use of this novel 12-chemokine GES may reveal basic information on in situ mechanisms of the anti-tumor immune response, potentially leading to improvements in the identification and selection of melanoma patients most suitable for immunotherapy.
         datePublished:2012-10-24T00:00:00Z
         dateModified:2012-10-24T00:00:00Z
         pageStart:1
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         license:http://creativecommons.org/licenses/by-nc-nd/3.0/
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      headline:12-Chemokine Gene Signature Identifies Lymph Node-like Structures in Melanoma: Potential for Patient Selection for Immunotherapy?
      description:We have interrogated a 12-chemokine gene expression signature (GES) on genomic arrays of 14,492 distinct solid tumors and show broad distribution across different histologies. We hypothesized that this 12-chemokine GES might accurately predict a unique intratumoral immune reaction in stage IV (non-locoregional) melanoma metastases. The 12-chemokine GES predicted the presence of unique, lymph node-like structures, containing CD20+ B cell follicles with prominent areas of CD3+ T cells (both CD4+ and CD8+ subsets). CD86+, but not FoxP3+, cells were present within these unique structures as well. The direct correlation between the 12-chemokine GES score and the presence of unique, lymph nodal structures was also associated with better overall survival of the subset of melanoma patients. The use of this novel 12-chemokine GES may reveal basic information on in situ mechanisms of the anti-tumor immune response, potentially leading to improvements in the identification and selection of melanoma patients most suitable for immunotherapy.
      datePublished:2012-10-24T00:00:00Z
      dateModified:2012-10-24T00:00:00Z
      pageStart:1
      pageEnd:6
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      name:Biomedical Informatics, Moffitt Cancer Center, Tampa, USA
      name:Biomedical Informatics, Moffitt Cancer Center, Tampa, USA
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      name:the Analytic Microscopy Core, Moffitt Cancer Center, Tampa, USA
      name:Biostatistics, Moffitt Cancer Center, Tampa, USA
      name:Cutaneous Oncology, Moffitt Cancer Center, Tampa, USA
      name:Immunology, Moffitt Cancer Center, Tampa, USA
      name:Cutaneous Oncology, Moffitt Cancer Center, Tampa, USA
      name:Immunology, Moffitt Cancer Center, Tampa, USA
      name:Cutaneous Oncology, Moffitt Cancer Center, Tampa, USA
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External Links {πŸ”—}(206)

Analytics and Tracking {πŸ“Š}

  • Google Tag Manager

Libraries {πŸ“š}

  • Foundation
  • Prism.js
  • Zoom.js

Emails and Hosting {βœ‰οΈ}

Mail Servers:

  • mx.zoho.eu
  • mx2.zoho.eu
  • mx3.zoho.eu

Name Servers:

  • josh.ns.cloudflare.com
  • zita.ns.cloudflare.com

CDN Services {πŸ“¦}

  • Crossref

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