Abstract
Ribosome biogenesis is an important biological process for proper cellular function and development. Defects leading to improper ribosome biogenesis can cause diseases such as Diamond-Blackfan anemia and Shwachman-Bodian-Diamond syndrome. Nucleolar proteins are a large family of proteins and are involved in many cellular processes, including the regulation of ribosome biogenesis. Through a forward genetic screen and positional cloning, we identified and characterized a zebrafish line carrying mutation in nucleolar protein with MIF4G domain 1 (nom1), which encodes a conserved nulceolar protein with a role in pre-rRNA processing. Zebrafish nom1 mutants exhibit major defects in endoderm development, especially in exocrine pancreas. Further studies revealed that impaired proliferation of ptf1a-expressing pancreatic progenitor cells mainly contributed to the phenotype. RNA-seq and molecular analysis showed that ribosome biogenesis and pre-mRNA splicing were both affected in the mutant embryos. Several defects of ribosome assembly have been shown to have a p53-dependent mechanism. In the nom1 mutant, loss of p53 did not rescue the pancreatic defect, suggesting a p53-independent role. Further studies indicate that protein phosphatase 1 alpha, an interacting protein to Nom1, could partially rescue the pancreatic defect in nom1 morphants if a human nucleolar localization signal sequence was artificially added. This suggests that targeting Pp1α into the nucleolus by Nom1 is important for pancreatic proliferation. Altogether, our studies revealed a new mechanism involving Nom1 in controlling vertebrate exocrine pancreas formation.
Highlights
The nucleolus, a non-membrane bound structure within the nucleus of eukaryotic cells, regulates many biological processes, including cell-cycle progression, response to stress, mitosis [1]
Malfunction of nucleolar proteins can lead to disruption of the formation of a functional ribosome, and defects in ribosome biogenesis have been implicated in human diseases such as Dyskeratosis congenita syndrome [3], Werner syndrome [4] and Rothmund-Thomson syndrome [5]
We found that injecting the nucleolar localization signal sequence (NoLS)-pp1a-EGFP mRNA could partially restore try expression in nom1 morphants (Figure 9C, 9D, N = 60,50% partial rescue)
Summary
The nucleolus, a non-membrane bound structure within the nucleus of eukaryotic cells, regulates many biological processes, including cell-cycle progression, response to stress, mitosis [1]. Ribosome biogenesis is a tightly controlled process, involving multiple steps to produce and coordinate the assembly of rRNAs, over 80 ribosomal proteins (RPs), approximately 170 associated proteins, as well as many small nucleolar RNAs (snoRNAs) [2]. Any disruption of these components or steps in the assembly of a functional ribosome may affect cell survival and function. Mutation in Sgd1p, the yeast homolog of human NOM1, results in defects in cell growth and pre-rRNA processing. The function of NOM1 in vertebrate development has not been well-studied
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