A decrease in protein synthesis in cells of the developing gut contributes to a rare genetic disorder, and an inexpensive nutritional supplement may help reverse that decrease, according to a new study discovered by the research team led by XU Pengfei from the Zhejiang University School of Medicine and JIN Xi from the First Affiliated Hospital Zhejiang University School of Medicine . The finding is an advance in understanding the pathogenesis of the disease, and may lead to new treatments. November 1st , the article is published on PLOS Biology entitled “Mycn regulates intestinal development through ribosomal biogenesis in a zebrafish model of Feingold syndrome 1” .
The research team created the model by using CRISPR genome editing to delete a portion of the Mycn gene in zebrafish, whose gut development shares important similarities with that of humans. They found that the resulting loss of gene activity led to a dramatic reduction in the size of the intestine, both in length and in the folding that gives the intestine its enormous surface area for absorption. Within a particularly affected subgroup of cells in the developing intestine, they found a significant down-regulation of numerous ribosomal genes, leading to reduced gene translation and protein synthesis.
Particularly affected were genes in the mTOR signaling pathway, a central regulator of protein synthesis; treatment of wild-type zebrafish with an mTOR inhibitor recapitulated the intestinal developmental defects seen in Mycn mutants. When the authors treated the mutant fish with leucine, an amino acid known to activate the mTOR pathway, the result was a partial normalization of the intestinal size in the mutants.
“Our work shows that during embryonic development, intestinal cells, which are in a highly proliferative state, require high Mycn expression levels,” the corresponding authors, XU Pengfei and JIN Xi, say, “and that the proliferation arrest caused by reduced protein synthesis was the main reason for the developmental defects in the intestines of the Mycn mutant. This suggests a possible treatment strategy for the intestinal symptoms in patients with Feingold syndrome type 1, although confirmation in a human intestinal organoid system is essential.”
The first authors, LI Yun-Fei and CHENG Tao, add, “Feingold syndrome resulting from Mycn deficiency has been discovered for decades, however, the mechanism that leads to gastrointestinal atresia in Feingold syndrome type 1 is still unclear. We developed a Mycn mutant zebrafish model which recapitulates key phenotypes of Feingold syndrome type 1, and also provided a possible treatment strategy for Feingold syndrome type 1.”
Source: Prof. XU Pengfei's Lab