Characterization of a chromatin‐associated TCF7L1 complex in human embryonic stem cells

Author:

Vuong Linh M.123ORCID,Pan Songqin4,Sierra Robert A.23,Waterman Marian L.5,Gershon Paul D.6,Donovan Peter J.123ORCID

Affiliation:

1. Department of Developmental and Cell Biology University of California Irvine California USA

2. Department of Biological Chemistry University of California Irvine California USA

3. Sue and Bill Gross Stem Cell Research Center: A CIRM Institute University of California Irvine California USA

4. W.M. Keck Proteomics Laboratory, Institute of Integrated Genome Biology, Department of Botany and Plant Sciences University of California Riverside California USA

5. Department of Microbiology and Molecular Genetics University of California Irvine California USA

6. Department of Molecular Biology and Biochemistry University of California Irvine California USA

Abstract

AbstractHuman embryonic stem cells (hESCs) resemble the pluripotent epiblast cells found in the early postimplantation human embryo and represent the “primed” state of pluripotency. One factor that helps primed pluripotent cells retain pluripotency and prepare genes for differentiation is the transcription factor TCF7L1, a member of a small family of proteins known as T cell factors/Lymphoid enhancer factors (TCF/LEF) that act as downstream components of the WNT signaling pathway. Transcriptional output of the WNT pathway is regulated, in part, by the activity of TCF/LEFs in conjunction with another component of the WNT pathway, β‐CATENIN. Because TCF7L1 plays an important role in regulating pluripotency, we began to characterize the protein complex associated with TCF7L1 when bound to chromatin in hESCs using rapid immunoprecipitation of endogenous proteins (RIME).  Data are available via ProteomeXchange with identifier PXD047582. These data identify known and new partners of TCF7L1 on chromatin and provide novel insights into how TCF7L1 and pluripotency itself might be regulated.

Funder

California Institute for Regenerative Medicine

National Institute of General Medical Sciences

National Cancer Institute

Publisher

Wiley

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