Human RFX6 regulates endoderm patterning at the primitive gut tube stage.
Toshihiro NakamuraJunji FujikuraRyo ItoYamato KeidaiNobuya InagakiPublished in: PNAS nexus (2024)
Transcriptional factor RFX6 is known to be a causal gene of Mitchell-Riley syndrome (MRS), an autosomal recessive neonatal diabetes associated with pancreatic hypoplasia and intestinal atresia/malformation. The morphological defects are limited to posterior foregut and mid-hindgut endodermal lineages and do not occur in the anterior foregut lineage; the mechanism remains to be fully elucidated. In this study, we generated RFX6 +/eGFP heterozygous knockin and RFX6 eGFP/eGFP homozygous knockin/knockout human-induced pluripotent stem cell (hiPSC) lines and performed in vitro endoderm differentiation to clarify the role of RFX6 in early endoderm development. RFX6 expression was found to surge at the primitive gut tube (PGT) stage in comparison with that in the undifferentiated or definitive endoderm stage. At the PGT stage, the expression of PDX1 and CDX2 , posterior foregut and mid-hindgut master regulators, respectively, was decreased by the RFX6 deficit. PDX1 + and CDX2 + cells were mostly green fluorescent protein (GFP) + in RFX6 +/eGFP hiPSCs, but their cell number was markedly decreased in RFX6 eGFP/eGFP hiPSCs. The expression of SOX2 , an anterior foregut marker, was not affected by the RFX6 deficit. In addition, we found a putative RFX6-binding X-box motif using cap analysis of gene expression-seq and the motif-containing sequences in the enhancer regions of PDX1 and CDX2 bound to RFX6 in vitro. Thus, RFX6 regulates the ParaHox genes PDX1 and CDX2 but does not affect SOX2 in early endodermal differentiation, suggesting that defects in early stage endoderm patterning account for the morphological pathology of MRS.
Keyphrases
- stem cells
- gene expression
- transcription factor
- early stage
- poor prognosis
- binding protein
- endothelial cells
- genome wide
- single cell
- dna methylation
- type diabetes
- embryonic stem cells
- metabolic syndrome
- induced apoptosis
- cardiovascular disease
- lymph node
- glycemic control
- signaling pathway
- oxidative stress
- genome wide identification
- weight loss
- single molecule
- endoplasmic reticulum stress
- case report
- rectal cancer
- cell fate
- living cells
- locally advanced