Zhang Yumeng, Xu Jiaqi, Ren Zhili, Meng Ya, Liu Weiwei, Lu Ligong, Zhou Zhou, Chen Guokai
Centre of Reproduction, Development and Aging, Faculty of Health Sciences, University of Macau, Macau SAR, China.
Institute of Translational Medicine, Faculty of Health Sciences, University of Macau, Macau SAR, China.
Stem Cell Res Ther. 2021 Jun 25;12(1):362. doi: 10.1186/s13287-021-02426-2.
Vitamin B3 (nicotinamide) plays important roles in metabolism as well as in SIRT and PARP pathways. It is also recently reported as a novel kinase inhibitor with multiple targets. Nicotinamide promotes pancreatic cell differentiation from human embryonic stem cells (hESCs). However, its molecular mechanism is still unclear. In order to understand the molecular mechanism involved in pancreatic cell fate determination, we analyzed the downstream pathways of nicotinamide in the derivation of NKX6.1 pancreatic progenitors from hESCs.
We applied downstream modulators of nicotinamide during the induction from posterior foregut to pancreatic progenitors, including niacin, PARP inhibitor, SIRT inhibitor, CK1 inhibitor and ROCK inhibitor. The impact of those treatments was evaluated by quantitative real-time PCR, flow cytometry and immunostaining of pancreatic markers. Furthermore, CK1 isoforms were knocked down to validate CK1 function in the induction of pancreatic progenitors. Finally, RNA-seq was used to demonstrate pancreatic induction on the transcriptomic level.
First, we demonstrated that nicotinamide promoted pancreatic progenitor differentiation in chemically defined conditions, but it did not act through either niacin-associated metabolism or the inhibition of PARP and SIRT pathways. In contrast, nicotinamide modulated differentiation through CK1 and ROCK inhibition. We demonstrated that CK1 inhibitors promoted the generation of PDX1/NKX6.1 double-positive pancreatic progenitor cells. shRNA knockdown revealed that the inhibition of CK1α and CK1ε promoted pancreatic progenitor differentiation. We then showed that nicotinamide also improved pancreatic progenitor differentiation through ROCK inhibition. Finally, RNA-seq data showed that CK1 and ROCK inhibition led to pancreatic gene expression, similar to nicotinamide treatment.
In this report, we revealed that nicotinamide promotes generation of pancreatic progenitors from hESCs through CK1 and ROCK inhibition. Furthermore, we discovered the novel role of CK1 in pancreatic cell fate determination.
维生素B3(烟酰胺)在新陈代谢以及SIRT和PARP途径中发挥重要作用。最近它还被报道为一种具有多个靶点的新型激酶抑制剂。烟酰胺可促进人胚胎干细胞(hESC)向胰腺细胞分化。然而,其分子机制仍不清楚。为了了解胰腺细胞命运决定所涉及的分子机制,我们分析了烟酰胺在hESC来源的NKX6.1胰腺祖细胞诱导过程中的下游途径。
我们在从前肠后部诱导为胰腺祖细胞的过程中应用了烟酰胺的下游调节剂,包括烟酸、PARP抑制剂、SIRT抑制剂、CK1抑制剂和ROCK抑制剂。通过定量实时PCR、流式细胞术和胰腺标志物免疫染色评估这些处理的影响。此外,敲低CK1亚型以验证CK1在胰腺祖细胞诱导中的功能。最后,使用RNA测序在转录组水平上证明胰腺诱导。
首先,我们证明烟酰胺在化学成分明确的条件下促进胰腺祖细胞分化,但它不是通过与烟酸相关的代谢或抑制PARP和SIRT途径起作用。相反,烟酰胺通过抑制CK1和ROCK调节分化。我们证明CK1抑制剂促进PDX1/NKX6.1双阳性胰腺祖细胞的产生。短发夹RNA敲低显示抑制CK1α和CK1ε可促进胰腺祖细胞分化。然后我们表明烟酰胺还通过抑制ROCK改善胰腺祖细胞分化。最后,RNA测序数据表明抑制CK1和ROCK可导致胰腺基因表达,类似于烟酰胺处理。
在本报告中,我们揭示烟酰胺通过抑制CK1和ROCK促进hESC产生胰腺祖细胞。此外,我们发现了CK1在胰腺细胞命运决定中的新作用。
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