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      A Thyroid Hormone Receptor/KLF9 Axis in Human Hepatocytes and Pluripotent Stem Cells

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          Abstract

          Biological processes require close cooperation of multiple transcription factors that integrate different signals. Thyroid hormone receptors (TRs) induce Krüppel-like factor 9 (KLF9) to regulate neurogenesis. Here, we show that triiodothyronine (T3) also works through TR to induce KLF9 in HepG2 liver cells, mouse liver, and mouse and human primary hepatocytes and sought to understand TR/KLF9 network function in the hepatocyte lineage and stem cells. Knockdown experiments reveal that KLF9 regulates hundreds of HepG2 target genes and modulates T3 response. Together, T3 and KLF9 target genes influence pathways implicated in stem cell self-renewal and differentiation, including Notch signaling, and we verify that T3 and KLF9 cooperate to regulate key Notch pathway genes and work independently to regulate others. T3 also induces KLF9 in human embryonic stem cells (hESCs) and human induced pluripotent stem cells (hiPSC) and this effect persists during differentiation to definitive endoderm and hiPSC-derived hepatocytes. Microarray analysis reveals that T3 regulates hundreds of hESC and hiPSC target genes that cluster into many of the same pathways implicated in TR and KLF9 regulation in HepG2 cells. KLF9 knockdown confirms that TR and KLF9 cooperate to regulate Notch pathway genes in hESC and hiPSC, albeit in a partly cell-specific manner. Broader analysis of T3 responsive hESC/hiPSC genes suggests that TRs regulate multiple early steps in ESC differentiation. We propose that TRs cooperate with KLF9 to regulate hepatocyte proliferation and differentiation and early stages of organogenesis and that TRs exert widespread and important influences on ESC biology.

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          Author and article information

          Journal
          9304532
          2286
          Stem Cells
          Stem Cells
          Stem cells (Dayton, Ohio)
          1066-5099
          1549-4918
          21 December 2018
          February 2015
          03 January 2019
          : 33
          : 2
          : 416-428
          Affiliations
          [a ]Genomic Medicine, Houston Methodist Research Institute, Houston, Texas, USA;
          [b ]Stem Cell Laboratory, Assisted Conception Unit, Division of Women’s Health, King’s College London, London, United Kingdom;
          [c ]Guy’s and St. Thomas NHS Foundation Trust and King’s College Biomedical Research Centre, London, United Kingdom;
          [d ]Institute of Liver Studies, King’s College London, London, United Kingdom;
          [e ]Department of Molecular and Clinical Pharmacology, Institute of Translational Medicine, The University of Liverpool, Liverpool, United Kingdom
          Author notes

          AUTHOR CONTRIBUTIONS

          A.C.: conception and design, collection and assembly of data, data analysis and interpretation, and manuscript writing; L.D., F.A.M., L.N., A.Z., C.F., K.S., J.H.S., and D.H.S.: collection and assembly of data; A.D. and T.S.: provision of study material; D.I.: data analysis and interpretation; P.W.: manuscript writing, financial support, and final approval of manuscript.

          Correspondence: Paul Webb, Ph.D., Genomic Medicine, Houston Methodist Research Institute, 6670 Bertner Avenue, Houston, Texas 77030, USA. Telephone: 713-441-2516; Fax: 713-441-2178; PWebb@ 123456houstonmethodist.org
          Article
          PMC6317531 PMC6317531 6317531 nihpa1001595
          10.1002/stem.1875
          6317531
          25330987
          8c2f3c36-3bf9-47cc-b084-e819afaa6ce8
          History
          Categories
          Article

          Human embryonic stem cell,Thyroid receptor,Krüppel-like factor 9,Induced pluripotent stem cell,Notch

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