Abstract
Hemojuvelin (HJV) and matriptase-2 (MT2) are co-expressed in hepatocytes, and both are essential for systemic iron homeostasis. HJV is a glycosylphosphatidylinositol-linked membrane protein that acts as a co-receptor for bone morphogenetic proteins to induce hepcidin expression. MT2 regulates the levels of membrane-bound HJV in hepatocytes by binding to and cleaving HJV into an inactive soluble form that is released from cells. HJV also interacts with neogenin, a ubiquitously expressed transmembrane protein with multiple functions. In this study, we showed that neogenin interacted with MT2 as well as with HJV and facilitated the cleavage of HJV by MT2. In contrast, neogenin was not cleaved by MT2, indicating some degree of specificity by MT2. Down-regulation of neogenin with siRNA increased the amount of MT2 and HJV on the plasma membrane, suggesting a lack of neogenin involvement in their trafficking to the cell surface. The increase in MT2 and HJV upon neogenin knockdown was likely due to the inhibition of cell surface MT2 and HJV internalization. Analysis of the Asn-linked oligosaccharides showed that MT2 cleavage of cell surface HJV was coupled to a transition from high mannose oligosaccharides to complex oligosaccharides on HJV. These results suggest that neogenin forms a ternary complex with both MT2 and HJV at the plasma membrane. The complex facilitates HJV cleavage by MT2, and release of the cleaved HJV from the cell occurs after a retrograde trafficking through the TGN/Golgi compartments.
Highlights
Matriptase-2 regulates iron homeostasis by binding to and cleaving hemojuvelin
Neogenin Is Required for MT2 Cleavage of HJV—MT2 suppresses hepcidin expression by cleaving the glycosylphosphatidylinositol-linked membrane HJV into an inactive 36-kDa fragment that is released from hepatocytes (21, 39)
We examined three forms of soluble neogenin, fibronectin III (FNIII) 5– 6 (ϳ30 kDa), FNIII 1– 6 (ϳ90 kDa), and Neo/Ecto (ϳ150 kDa), for their ability to interfere with the neogenin-facilitated cleavage of HJV
Summary
Matriptase-2 regulates iron homeostasis by binding to and cleaving hemojuvelin. Neogenin interacts with hemojuvelin. Analysis of the Asn-linked oligosaccharides showed that MT2 cleavage of cell surface HJV was coupled to a transition from high mannose oligosaccharides to complex oligosaccharides on HJV These results suggest that neogenin forms a ternary complex with both MT2 and HJV at the plasma membrane. Neogenin Facilitates Matriptase-2 Cleavage of Hemojuvelin encoded by the TMPRSS6 gene in humans (denoted as Tmprss in mice) (18) This type II transmembrane protease is composed of a short cytoplasmic domain, a transmembrane domain, and a large extracellular domain, which contains a membrane-proximal SEA (sea urchin sperm protein, enteropeptidase, agrin) domain, two CUB (complete protein subcomponents C1r/C1s motif, urchin embryonic growth factor, and BMP1) domains, three low density lipoprotein receptor class A domains, a predicted activation domain, and a C-terminal catalytic domain (Fig. 1A) (19). Further analysis suggests that MT2 cleavage of HJV occurs either at the cell surface or during a retrograde trafficking to the TGN/Golgi compartment in a neogenin-dependent manner
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