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Jiayi Liu on Jiayi Liu

Differential variability analysis of single-cell gene expression data | Jiayi Liu Running singularity containers in a High Performance Computing (HPC) environment | Jiayi Liu 2021这一年 | Jiayi Liu A 'one-two punch' therapy strategy to target chemoresistance in estrogen receptor positive breast cancer | Jiayi Liu Activation of EPHA2-ROBO1 heterodimer by SLIT2 attenuates non-canonical signaling and proliferation in squamous cell carcinomas | Jiayi Liu Deploying Huginn with Docker on Google Cloud Platform | Jiayi Liu 强迫症二三事 | Jiayi Liu 来Houston一周年 | Jiayi Liu 与母亲对话若干则 | Jiayi Liu 烧饭经验 | Jiayi Liu 乘车记 by 我妈 | Jiayi Liu 2019 | Jiayi Liu Patterned progression of gut microbiota associated with necrotizing enterocolitis and late onset sepsis in preterm infants: a prospective study in a Chinese neonatal intensive care unit | Jiayi Liu 【转】食人族留学生纪事本末 | Jiayi Liu
Phylogenetic inference from single-cell RNA-seq data | Jiayi Liu
Jiayi Liu · 2023-08-03 · via Jiayi Liu on Jiayi Liu

, Jason I. Griffiths , Isaac Bishara , Jiayi Liu , Andrea H. Bild , Jeffrey T. Chang

Abstract

Tumors are comprised of subpopulations of cancer cells that harbor distinct genetic profiles and phenotypes that evolve over time and during treatment. By reconstructing the course of cancer evolution, we can understand the acquisition of the malignant properties that drive tumor progression. Unfortunately, recovering the evolutionary relationships of individual cancer cells linked to their phenotypes remains a difficult challenge. To address this need, we have developed PhylinSic, a method that reconstructs the phylogenetic relationships among cells linked to their gene expression profiles from single cell RNA-sequencing (scRNA-Seq) data. This method calls nucleotide bases using a probabilistic smoothing approach and then estimates a phylogenetic tree using a Bayesian modeling algorithm. We showed that PhylinSic identified evolutionary relationships underpinning drug selection and metastasis and was sensitive enough to identify subclones from genetic drift. We found that breast cancer tumors resistant to chemotherapies harbored multiple genetic lineages that independently acquired high K-Ras and β-catenin, suggesting that therapeutic strategies may need to control multiple lineages to be durable. These results demonstrated that PhylinSic can reconstruct evolution and link the genotypes and phenotypes of cells across monophyletic tumors using scRNA-Seq.