AI Article Synopsis

  • Advances in single-cell biology allow detailed measurement of protein features in immune cells, but data analysis can be biased and complex.
  • An ensemble of unsupervised tools was created to assess four key immune cell properties: systemic plasticity, population abundance changes, signature feature changes, and the novelty of cellular phenotypes.
  • This approach was tested on melanoma biopsies, uncovering unique characteristics of double-negative T cells that differ from normal immune cells and are also observed in other tumor types, thus enhancing understanding of immune responses in various cancers.

Article Abstract

Advances in single-cell biology have enabled measurements of >40 protein features on millions of immune cells within clinical samples. However, the data analysis steps following cell population identification are susceptible to bias, time-consuming, and challenging to compare across studies. Here, an ensemble of unsupervised tools was developed to evaluate four essential types of immune cell information, incorporate changes over time, and address diverse immune monitoring challenges. The four complementary properties characterized were (i) systemic plasticity, (ii) change in population abundance, (iii) change in signature population features, and (iv) novelty of cellular phenotype. Three systems immune monitoring studies were selected to challenge this ensemble approach. In serial biopsies of melanoma tumors undergoing targeted therapy, the ensemble approach revealed enrichment of double-negative (DN) T cells. Melanoma tumor-resident DN T cells were abnormal and phenotypically distinct from those found in nonmalignant lymphoid tissues, but similar to those found in glioblastoma and renal cell carcinoma. Overall, ensemble systems immune monitoring provided a robust, quantitative view of changes in both the system and cell subsets, allowed for transparent review by human experts, and revealed abnormal immune cells present across multiple human tumor types.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6318034PMC
http://dx.doi.org/10.1158/2326-6066.CIR-17-0692DOI Listing

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