Mutations in SPINT2 Cause a Syndromic Form of Congenital Sodium Diarrhea

Heinz‐Erian, Peter; Müller, Thomas; Krabichler, Birgit; Schranz, Melanie; Becker, Christian; Rüschendorf, Franz; Nürnberg, Peter; Rossier, Bernard C.; Vujic, Mihailo; Booth, I W; Holmberg, Christer; Wijmenga, Cisca; Grigelioniené, Giedré; Kneepkens, C. M. F.; Rosipal, Štefan; Mistrík, Martin; Kappler, Matthias; Michaud, Laurent; Dóczy, Ludwig-Christoph; Siu, Victoria Mok; Krantz, Marie; Zoller, Heinz; Utermann, Gerd; Janecke, Andreas R.

doi:10.1016/j.ajhg.2009.01.004

Cited by 110 publications

(130 citation statements)

References 29 publications

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“…Notably, a recent study revealed that mutation of the SPINT2 gene results in a syndromic form of congenital sodium diarrhea, which also indicates a significant role for this membrane-bound serine protease inhibitor in the intestinal epithelial function. 32 The important role of HAI-1/SPINT1 in the colonic mucosa was also shown in a model for mucosal injury that involves DSS administration. In this model, DSS seems to be directly toxic to colonic epithelial cells of the basal crypts and affects the integrity of the mucosal barrier, and this mouse colitis model is widely used for the study of human IBD.…”

Section: Discussionmentioning

confidence: 93%

Membrane-Bound Serine Protease Inhibitor HAI-1 Is Required for Maintenance of Intestinal Epithelial Integrity

Kawaguchi

Takeda

Hoshiko

et al. 2011

The American Journal of Pathology

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Hepatocyte growth factor activator inhibitor type 1 (HAI-1), encoded by the serine protease inhibitor Kunitz type 1 (SPINT1) gene, is a membrane-bound serine protease inhibitor expressed in epithelial tissues. Mutant mouse models revealed that HAI-1/SPINT1 is essential for placental labyrinth formation and is critically involved in regulating epidermal keratinization through interaction with its cognate cell surface protease, matriptase. HAI-1/SPINT1 is abundantly expressed in both human and mouse intestinal epithelium; therefore, we analyzed its role in intestinal function using mice with intestinal epithelial cell-specific deletion of Spint1 generated by interbreeding mice carrying Spint1 LoxP homozygous alleles with transgenic mice carrying the Cre recombinase gene controlled by the intestine-specific Villin promoter. Although the resulting mice had normal development and appearance, crypts in the proximal aspect of the colon, including the cecum, exhibited histologic abnormalities and increased apoptosis and epithelial cell turnover accompanied by increased intestinal permeability. Distended endoplasmic reticula were observed ultrastructurally in some crypt epithelial cells, indicative of endoplasmic reticular stress. To study the role of HAI-1/SPINT1 in mucosal injury, we induced colitis by adding dextran sodium sulfate to the drinking water. After dextran sodium sulfate treatment, intestine-specific HAI-1/SPINT1-deficient mice had more severe symptoms and a significantly lower survival rate relative to control mice. These results suggest that HAI-1/SPINT1 plays an important role in maintaining colonic epithelium integrity.

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Section: Discussionmentioning

confidence: 93%

Membrane-Bound Serine Protease Inhibitor HAI-1 Is Required for Maintenance of Intestinal Epithelial Integrity

Kawaguchi

Takeda

Hoshiko

et al. 2011

The American Journal of Pathology

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“…Our proposal that HAI-2 is essential for matriptase expression in intestinal epithelium by preventing the "consumptive depletion" of matriptase may also explain the etiology of the sodium-selective diarrhea that is associated with congenital HAI-2 deficiency in humans (56). The epithelial sodium channel ENaC is critical for sodium reabsorption in the distal colon, and the activity of ENaC in the distal colon is dependent on its proteolytic activation by the matriptase-prostasin system (53).…”

Section: Discussionmentioning

confidence: 99%

The Protease Inhibitor HAI-2, but Not HAI-1, Regulates Matriptase Activation and Shedding through Prostasin

Friis

Sales

Schafer

et al. 2014

Journal of Biological Chemistry

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Background: Hepatocyte growth factor activator inhibitor (HAI)-1 and HAI-2 may regulate matriptase trafficking and activation. Results: Ablation of endogenous HAI-2, but not HAI-1, causes loss of epithelial matriptase in vivo and in vitro, due to uncontrolled prostasin-dependent activation and shedding. Conclusion: HAI-2, but not HAI-1, regulates matriptase cell surface expression level. Significance: The study identifies HAI-2 as a principal regulator of prostasin-mediated matriptase activation.

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“…Importantly, however, to date, the known complement of mutated SPINT2 alleles all either directed the production of HAI2 proteins at lower levels or with lower inhibitory activity (Heinz-Erian et al, 2009), whereas the phenotypic consequence of complete Spint2 deficiency has been analyzed only in mice. Also, as only SPINT2-deficient individuals that completed term development have been available for clinical evaluation, it is premature to discuss potential species-specific variations in the developmental manifestations of the loss of HAI2.…”

Section: Discussionmentioning

confidence: 99%

“…Defects in postnatal epithelial function, such as persistent sodium diarrhea, corneal erosions and abnormal hair, are also associated with SPINT2 deficiency (Heinz-Erian et al, 2009). The SPINT2 gene encodes a serine protease inhibitor, hepatocyte growth factor activator inhibitor (HAI) 2 (also known as placental bikunin; hereafter HAI2) (Kawaguchi et al, 1997;Marlor et al, 1997), and reduced expression of HAI2 or synthesis of HAI2 variants with reduced in vitro inhibitory activity is common to all the mutated SPINT2 alleles (Heinz-Erian et al, 2009). This raises the possibility that key morphogenic processes, such as organ and digit specification and tubulogenesis, may require the fine-tuning of pericellular proteolytic activity through HAI2 silencing of unknown target proteases.…”

Section: Introductionmentioning

confidence: 99%

Regulation of cell surface protease matriptase by HAI2 is essential for placental development, neural tube closure and embryonic survival in mice

et al. 2009

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Hypomorphic mutations in the human SPINT2 gene cause a broad spectrum of abnormalities in organogenesis, including organ and digit duplications, atresia, fistulas, hypertelorism, cleft palate and hamartoma. SPINT2 encodes the transmembrane serine protease inhibitor HAI2 (placental bikunin), and the severe developmental effects of decreased HAI2 activity can be hypothesized to be a consequence of excess pericellular proteolytic activity. Indeed, we show here that HAI2 is a potent regulator of protease-guided cellular responses, including motogenic activity and transepithelial resistance of epithelial monolayers. Furthermore, we show that inhibition of the transmembrane serine protease matriptase (encoded by St14) is an essential function of HAI2 during tissue morphogenesis. Genetic inactivation of the mouse Spint2 gene led to defects in neural tube closure, abnormal placental labyrinth development associated with loss of epithelial cell polarity, and embryonic demise. Developmental defects observed in HAI2-deficient mice were caused by unregulated matriptase activity, as both placental development and embryonic survival in HAI2-deficient embryos were completely restored by the simultaneous genetic inactivation of matriptase. However, neural tube defects were detected in HAI2-deficient mice even in the absence of matriptase, although at lower frequency, indicating that the inhibition of additional serine protease(s) by HAI2 is required to complete neural development. Finally, by genetic complementation analysis, we uncovered a unique and complex functional interaction between HAI2 and the related HAI1 in the regulation of matriptase activity during development. This study indicates that unregulated matriptase-dependent cell surface proteolysis can cause a diverse array of abnormalities in mammalian development.

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Mutations in SPINT2 Cause a Syndromic Form of Congenital Sodium Diarrhea

Cited by 110 publications

References 29 publications

Membrane-Bound Serine Protease Inhibitor HAI-1 Is Required for Maintenance of Intestinal Epithelial Integrity

Membrane-Bound Serine Protease Inhibitor HAI-1 Is Required for Maintenance of Intestinal Epithelial Integrity

The Protease Inhibitor HAI-2, but Not HAI-1, Regulates Matriptase Activation and Shedding through Prostasin

Regulation of cell surface protease matriptase by HAI2 is essential for placental development, neural tube closure and embryonic survival in mice

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