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Characterization of BRCA1-deficient premalignant tissues and cancers identifies Plekha5 as a tumor metastasis suppressor.


ABSTRACT: Single-cell whole-exome sequencing (scWES) is a powerful approach for deciphering intratumor heterogeneity and identifying cancer drivers. So far, however, simultaneous analysis of single nucleotide variants (SNVs) and copy number variations (CNVs) of a single cell has been challenging. By analyzing SNVs and CNVs simultaneously in bulk and single cells of premalignant tissues and tumors from mouse and human BRCA1-associated breast cancers, we discover an evolution process through which the tumors initiate from cells with SNVs affecting driver genes in the premalignant stage and malignantly progress later via CNVs acquired in chromosome regions with cancer driver genes. These events occur randomly and hit many putative cancer drivers besides p53 to generate unique genetic and pathological features for each tumor. Upon this, we finally identify a tumor metastasis suppressor Plekha5, whose deficiency promotes cancer metastasis to the liver and/or lung.

SUBMITTER: Liu J 

PROVIDER: S-EPMC7519681 | biostudies-literature | 2020 Sep

REPOSITORIES: biostudies-literature

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Characterization of BRCA1-deficient premalignant tissues and cancers identifies Plekha5 as a tumor metastasis suppressor.

Liu Jianlin J   Adhav Ragini R   Miao Kai K   Su Sek Man SM   Mo Lihua L   Chan Un In UI   Zhang Xin X   Xu Jun J   Li Jianjie J   Shu Xiaodong X   Zeng Jianming J   Zhang Xu X   Lyu Xueying X   Pardeshi Lakhansing L   Tan Kaeling K   Sun Heng H   Wong Koon Ho KH   Deng Chuxia C   Xu Xiaoling X  

Nature communications 20200925 1


Single-cell whole-exome sequencing (scWES) is a powerful approach for deciphering intratumor heterogeneity and identifying cancer drivers. So far, however, simultaneous analysis of single nucleotide variants (SNVs) and copy number variations (CNVs) of a single cell has been challenging. By analyzing SNVs and CNVs simultaneously in bulk and single cells of premalignant tissues and tumors from mouse and human BRCA1-associated breast cancers, we discover an evolution process through which the tumor  ...[more]

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