Donor-dependent variations in hepatic differentiation from human-induced pluripotent stem cells

Kajiwara, Masatoshi; Aoi, Takashi; Okita, Keisuke; Takahashi, Ryōsuke; Inoue, Haruhisa; Takayama, Nobuki; Endô, Hiroshi; Eto, Koji; Toguchida, Junya; Üemoto, Shinji; Yamanaka, Shinya

doi:10.1073/pnas.1209979109

Cited by 277 publications

(266 citation statements)

References 33 publications

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“…Previous studies suggested that reprogrammingassociated errors of retention of donor cell-specific epigenetic memory bias the differentiation potency of hiPSCs toward some lineages (Kim et al, 2010b(Kim et al, , 2011Polo et al, 2010). However, other studies did not confirm such correlations, or alternatively suggested that donor-specific genetic variability affecting lineage-primed gene expression might play a more dominant role (Ohi et al, 2011;Hu et al, 2011;Kajiwara et al, 2012;Kyttälä et al, 2016).…”

Section: Introductionmentioning

confidence: 72%

Tankyrase inhibition promotes a stable human naïve pluripotent state with improved functionality

et al. 2016

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The derivation and maintenance of human pluripotent stem cells (hPSCs) in stable naïve pluripotent states has a wide impact in human developmental biology. However, hPSCs are unstable in classical naïve mouse embryonic stem cell (ESC) WNT and MEK/ERK signal inhibition (2i) culture. We show that a broad repertoire of conventional hESC and transgene-independent human induced pluripotent stem cell (hiPSC) lines could be reverted to stable human preimplantation inner cell mass (ICM)-like naïve states with only WNT, MEK/ERK, and tankyrase inhibition (LIF-3i). LIF-3i-reverted hPSCs retained normal karyotypes and genomic imprints, and attained defining mouse ESC-like functional features, including high clonal self-renewal, independence from MEK/ERK signaling, dependence on JAK/ STAT3 and BMP4 signaling, and naïve-specific transcriptional and epigenetic configurations. Tankyrase inhibition promoted a stable acquisition of a human preimplantation ICM-like ground state via modulation of WNT signaling, and was most efficacious in efficiently reprogrammed conventional hiPSCs. Importantly, naïve reversion of a broad repertoire of conventional hiPSCs reduced lineage-primed gene expression and significantly improved their multilineage differentiation capacities. Stable naïve hPSCs with reduced genetic variability and improved functional pluripotency will have great utility in regenerative medicine and human disease modeling.

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Section: Introductionmentioning

confidence: 72%

Tankyrase inhibition promotes a stable human naïve pluripotent state with improved functionality

et al. 2016

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“…EN differentiation. EN differentiation was performed as described previously, with slight modification 36 . The single-cell suspensions of human pluripotent stem cells were plated onto Matrigel-coated plates in RPMI1640 (Life Technologies) containing 2% B27, 100 ng ml À 1 Activin A, 3 mM CHIR99021 and 0.5% Pen/Strep.…”

Section: Methodsmentioning

confidence: 99%

Induction of pluripotency in human somatic cells via a transient state resembling primitive streak-like mesendoderm

et al. 2014

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During mammalian embryonic development, the primitive streak initiates the differentiation of pluripotent epiblast cells into germ layers. Pluripotency can be reacquired in committed somatic cells using a combination of a handful of transcription factors, such as OCT3/4, SOX2, KLF4 and c-MYC (hereafter referred to as OSKM), albeit with low efficiency. Here we show that during OSKM-induced reprogramming towards pluripotency in human cells, intermediate cells transiently show gene expression profiles resembling mesendoderm, which is a major component of the primitive streak. Based on these findings, we discover that forkhead box H1 (FOXH1), a transcription factor required for anterior primitive streak specification during early development, significantly enhances the reprogramming efficiency of human fibroblasts by promoting their maturation, including mesenchymal to epithelial transition and the activation of late pluripotency markers. These results demonstrate that during the reprogramming process, human somatic cells go through a transient state that resembles mesendoderm.

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“…The hiPSC technology could also contribute to production of rare types of erythrocytes-for example, D2, Fy(a2b2), Di(b2), and Jr(a2) [5]. However, it is well known that hiPSC clones are heterogeneous with respect to their differentiation potential [6]. Consequently, the ability to distinguish clones suitable for in vitro erythrocyte production from among identical donor-derived hiPSC clones is crucial.…”

Section: Introductionmentioning

confidence: 99%

Multicolor Staining of Globin Subtypes Reveals Impaired Globin Switching During Erythropoiesis in Human Pluripotent Stem Cells

Ochi

Takayama

Hirose

et al. 2014

Stem Cells Translational Medicine

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Adult hemoglobin composed of a-and b-globin reflects a change from expression of embryonic «-and fetal g-globin to adult b-globin in human erythroid cells, so-called globin switching. Human pluripotent stem cells (hPSCs) are a potential source for in vitro erythrocyte production, but they show prominent expression of g-globin with little b-globin expression, which indicates incomplete globin switching. To examine the mechanism of this impaired globin switching, we optimized multicolor flow cytometry to simultaneously follow expression of different globin subtypes using different immunofluorescent probes. This enabled us to detect upregulation of b-globin and the corresponding silencing of g-globin at the single-cell level during cord blood CD34 + cell-derived erythropoiesis, examined as an endogenous control. Using this approach, we initially characterized the heterogeneous b-globin expression in erythroblasts from several hPSC clones and confirmed the predominant expression of g-globin. These hPSC-derived erythroid cells also displayed reduced expression of BCL11A-L. However, doxycycline-induced overexpression of BCL11A-L in selected hPSCs promoted g-globin silencing. These results strongly suggest that impaired g-globin silencing is associated with downregulated BCL11A-L in hPSC-derived erythroblasts and that multicolor staining of globin subtypes is an effective approach to studying globin switching in vitro. STEM CELLS TRANSLATIONAL MEDICINE 2014;3:792-800

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Donor-dependent variations in hepatic differentiation from human-induced pluripotent stem cells

Cited by 277 publications

References 33 publications

Tankyrase inhibition promotes a stable human naïve pluripotent state with improved functionality

Tankyrase inhibition promotes a stable human naïve pluripotent state with improved functionality

Induction of pluripotency in human somatic cells via a transient state resembling primitive streak-like mesendoderm

Multicolor Staining of Globin Subtypes Reveals Impaired Globin Switching During Erythropoiesis in Human Pluripotent Stem Cells

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