Department of Dermatology, Duke University, Durham, NC 27710, USA.
Department of Cell Biology, Duke University, Durham, NC 27710, USA.
Development. 2022 Dec 1;149(23). doi: 10.1242/dev.201251. Epub 2022 Dec 12.
There are fundamental differences in how neonatal and adult intestines absorb nutrients. In adults, macromolecules are broken down into simpler molecular components in the lumen of the small intestine, then absorbed. In contrast, neonates are thought to rely on internalization of whole macromolecules and subsequent degradation in the lysosome. Here, we identify the Maf family transcription factors MAFB and c-MAF as markers of terminally differentiated intestinal enterocytes throughout life. The expression of these factors is regulated by HNF4α and HNF4γ, master regulators of enterocyte cell fate. Loss of Maf factors results in a neonatal-specific failure to thrive and loss of macromolecular nutrient uptake. RNA-Seq and CUT&RUN analyses defined an endo-lysosomal program as being downstream of these transcription factors. We demonstrate major transcriptional changes in metabolic pathways, including fatty acid oxidation and increases in peroxisome number, in response to loss of Maf proteins. Finally, we show that loss of BLIMP1, a repressor of adult enterocyte genes, shows highly overlapping changes in gene expression and similar defects in macromolecular uptake. This work defines transcriptional regulators that are necessary for nutrient uptake in neonatal enterocytes.
新生儿和成人肠道吸收营养的方式存在根本差异。在成人中,大分子在小肠腔中被分解成更简单的分子成分,然后被吸收。相比之下,人们认为新生儿依赖于将整个大分子内化,并随后在溶酶体中降解。在这里,我们确定了 maf 家族转录因子 mafb 和 c-maf 作为整个生命周期中终末分化肠上皮细胞的标志物。这些因子的表达受 hnf4α 和 hnf4γ 的调节,hnf4α 和 hnf4γ 是肠上皮细胞命运的主要调节因子。maf 因子的缺失会导致新生儿特有的生长不良和大分子营养物质摄取的丧失。rna-seq 和 cut&run 分析将内体-溶酶体程序定义为这些转录因子的下游。我们证明了代谢途径中的主要转录变化,包括脂肪酸氧化和过氧化物酶体数量的增加,这是对 maf 蛋白缺失的反应。最后,我们表明,blimp1 的缺失,一种成人肠上皮基因的抑制剂,在基因表达和大分子摄取的类似缺陷方面表现出高度重叠的变化。这项工作定义了在新生儿肠上皮细胞中吸收营养物质所必需的转录调节剂。
