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19 results on '"McGinnis CS"'

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1. Mapping enhancer-gene regulatory interactions from single-cell data.

2. Single-cell analysis of breast cancer metastasis reveals epithelial-mesenchymal plasticity signatures associated with poor outcomes.

3. The temporal progression of lung immune remodeling during breast cancer metastasis.

4. Patterning and folding of intestinal villi by active mesenchymal dewetting.

5. D-SPIN constructs gene regulatory network models from multiplexed scRNA-seq data revealing organizing principles of cellular perturbation response.

6. Epithelial zonation along the mouse and human small intestine defines five discrete metabolic domains.

7. Epithelial zonation along the mouse and human small intestine defines five discrete metabolic domains.

8. Patterning and folding of intestinal villi by active mesenchymal dewetting.

9. The temporal progression of immune remodeling during metastasis.

10. Mapping hormone-regulated cell-cell interaction networks in the human breast at single-cell resolution.

11. Lineage tracing reveals the phylodynamics, plasticity, and paths of tumor evolution.

12. Single cell enhancer activity distinguishes GABAergic and cholinergic lineages in embryonic mouse basal ganglia.

13. Human microglia states are conserved across experimental models and regulate neural stem cell responses in chimeric organoids.

14. AMULET: a novel read count-based method for effective multiplet detection from single nucleus ATAC-seq data.

15. No detectable alloreactive transcriptional responses under standard sample preparation conditions during donor-multiplexed single-cell RNA sequencing of peripheral blood mononuclear cells.

16. ZipSeq: barcoding for real-time mapping of single cell transcriptomes.

17. MULTI-seq: sample multiplexing for single-cell RNA sequencing using lipid-tagged indices.

18. DoubletFinder: Doublet Detection in Single-Cell RNA Sequencing Data Using Artificial Nearest Neighbors.

19. Cell population structure prior to bifurcation predicts efficiency of directed differentiation in human induced pluripotent cells.

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