β-catenin and γ-catenin Are Dispensable for T Lymphocytes and AML Leukemic Stem Cells

Overview

Journal Elife

Specialty Biology

Date 2020 Aug 22

PMID 32820720

Citations 10

Authors

Xin Zhao

Peng Shao

Kexin Gai

Fengyin Li

Qiang Shan

Hai-Hui Xue

Affiliations

Soon will be listed here.

Abstract

The β-catenin transcriptional coregulator is involved in various biological and pathological processes; however, its requirements in hematopoietic cells remain controversial. We re-targeted the gene locus to generate a true β-catenin-null mutant mouse strain. Ablation of β-catenin alone, or in combination with its homologue γ-catenin, did not affect thymocyte maturation, survival or proliferation. Deficiency in β/γ-catenin did not detectably affect differentiation of CD4T follicular helper cells or that of effector and memory CD8 cytotoxic cells in response to acute viral infection. In an MLL-AF9 AML mouse model, genetic deletion of β-catenin, or even all four Tcf/Lef family transcription factors that interact with β-catenin, did not affect AML onset in primary recipients, or the ability of leukemic stem cells (LSCs) in propagating AML in secondary recipients. Our data thus clarify on a long-standing controversy and indicate that β-catenin is dispensable for T cells and AML LSCs.

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