2020
DOI: 10.1101/2020.03.30.017210
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Fragmentation of Small-cell Lung Cancer Regulatory States in Heterotypic Microenvironments

Abstract: Small-cell lung cancers derive from pulmonary neuroendocrine cells, which have stemlike properties to reprogram into other cell types upon lung injury. It is difficult to uncouple the plasticity of these transformed cells from heritable changes that evolve in primary tumors or select in metastases to distant organs. Approaches to single-cell profiling are also problematic if the required sample dissociation activates injury-like signaling and reprogramming. Here, we defined cell-state heterogeneities in situ t… Show more

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Cited by 4 publications
(8 citation statements)
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References 83 publications
(122 reference statements)
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“…4B and Supplementary Table ST1). RHEGs provide a conceptual framework for prioritizing cell-state regulatory heterogeneities identified in vivo (49,50).…”
Section: Stochastic Profiling Identifies Recurrent Transcriptional Rementioning
confidence: 99%
See 1 more Smart Citation
“…4B and Supplementary Table ST1). RHEGs provide a conceptual framework for prioritizing cell-state regulatory heterogeneities identified in vivo (49,50).…”
Section: Stochastic Profiling Identifies Recurrent Transcriptional Rementioning
confidence: 99%
“…Regardless of the output, all leading approaches dissociate tumors into single-cell suspensions, requiring up to an hour of tissue processing and yielding a range of carcinoma proportions depending on cancer type ( Table 1). The impact of these preparative steps on the transcriptomes of live cells is recognized (11) [and see also the accompanying study (12)], but they are considered to be an unavoidable tradeoff of the scRNA-seq approach.…”
Section: Introductionmentioning
confidence: 99%
“…Half of the 90 dpi mutant samples were similar to 12 dpi bulk observations, indicating an averaged population that was still undergoing adaptation, while the other half mapped toward the 150 dpi tumors, suggesting a fraction of cells in those bulk samples were transitioning to a gliomagenic state. The confused (de)differentiation of mutant OPCs during premalignancy [conceptually similar to that in the accompanying contribution (20)] undoubtedly contributed intrinsic variance to the very small number of differential transcripts detected at 90 dpi (Fig. 4B).…”
Section: Integrating Bulk and 10-cell Transcriptomes Defines Self-conmentioning
confidence: 61%
“…S2). Control OPCs were singular and much more entangled with unlabeled neighbors compared to prior applications of fluorescence-guided LCM by our group (20,34). To assess overall purity of normal controls, we used a collection of brain cell typeenriched marker transcripts (25) to construct a signature matrix for bulk sample deconvolution using CIBERSORT (24).…”
Section: Lcm-based Rna Sequencing Validates Differential Gene Expressmentioning
confidence: 99%
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