Your search keyword '"Binnerts, Minke"' showing total 6 results

1. The First Propeller Domain of LRP6 Regulates Sensitivity to DKK1

Author

Binnerts, Minke E., Tomasevic, Nenad, Bright, Jessica M., Leung, John, Ahn, Victoria E., Kim, Kyung-Ah, Zhan, Xiaoming, Liu, Shouchun, Yonkovich, Shirlee, Williams, Jason, Zhou, Mei, Gros, Delphine, Dixon, Melissa, Korver, Wouter, Weis, William I., and Abo, Arie

Abstract

The Wnt coreceptor LRP6 is required for canonical Wnt signaling. To understand the molecular regulation of LRP6 function, we generated a series of monoclonal antibodies against the extra cellular domain (ECD) of LRP6 and selected a high-affinity mAb (mAb135) that recognizes cell surface expression of endogenous LRP6. mAb135 enhanced Wnt dependent TCF reporter activation and antagonized DKK1 dependent inhibition of Wnt3A signaling, suggesting a role in modulation of LRP6 function. Detailed analysis of LRP6 domain mutants identified Ser 243 in the first propeller domain of LRP6 as a critical residue for mAb135 binding, implicating this domain in regulating the sensitivity of LRP6 to DKK1. In agreement with this notion, mAb135 directly disrupted the interaction of DKK1 with recombinant ECD LRP6 and a truncated form of the LRP6 ECD containing only repeats 1 and 2. Finally, we found that mAb135 completely protected LRP6 from DKK1 dependent internalization. Together, these results identify the first propeller domain as a novel regulatory domain for DKK1 binding to LRP6 and show that mAb against the first propeller domain of LRP6 can be used to modulate this interaction.

Published

2009

2. The First Propeller Domain of LRP6 Regulates Sensitivity to DKK1

Author

Binnerts, Minke E., Tomasevic, Nenad, Bright, Jessica M., Leung, John, Ahn, Victoria E., Kim, Kyung-Ah, Zhan, Xiaoming, Liu, Shouchun, Yonkovich, Shirlee, Williams, Jason, Zhou, Mei, Gros, Delphine, Dixon, Melissa, Korver, Wouter, Weis, William I., and Abo, Arie

Abstract

The Wnt coreceptor LRP6 is required for canonical Wnt signaling. To understand the molecular regulation of LRP6 function, we generated a series of monoclonal antibodies against the extra cellular domain (ECD) of LRP6 and selected a high-affinity mAb (mAb135) that recognizes cell surface expression of endogenous LRP6. mAb135 enhanced Wnt dependent TCF reporter activation and antagonized DKK1 dependent inhibition of Wnt3A signaling, suggesting a role in modulation of LRP6 function. Detailed analysis of LRP6 domain mutants identified Ser 243 in the first propeller domain of LRP6 as a critical residue for mAb135 binding, implicating this domain in regulating the sensitivity of LRP6 to DKK1. In agreement with this notion, mAb135 directly disrupted the interaction of DKK1 with recombinant ECD LRP6 and a truncated form of the LRP6 ECD containing only repeats 1 and 2. Finally, we found that mAb135 completely protected LRP6 from DKK1 dependent internalization. Together, these results identify the first propeller domain as a novel regulatory domain for DKK1 binding to LRP6 and show that mAb against the first propeller domain of LRP6 can be used to modulate this interaction.

Published

2009

3. R-Spondin Family Members Regulate the Wnt Pathway by a Common Mechanism

Author

Kim, Kyung-Ah, Wagle, Marie, Tran, Karolyn, Zhan, Xiaoming, Dixon, Melissa A., Liu, Shouchun, Gros, Delphine, Korver, Wouter, Yonkovich, Shirlee, Tomasevic, Nenad, Binnerts, Minke, and Abo, Arie

Abstract

The R-Spondin (RSpo) family of secreted proteins is implicated in the activation of the Wnt signaling pathway. Despite the high structural homology between the four members, expression patterns and phenotypes in knockout mice have demonstrated striking differences. Here we dissected and compared the molecular and cellular function of all RSpo family members. Although all four RSpo proteins activate the canonical Wnt pathway, RSpo2 and 3 are more potent than RSpo1, whereas RSpo4 is relatively inactive. All RSpo members require Wnt ligands and LRP6 for activity and amplify signaling of Wnt3A, Wnt1, and Wnt7A, suggesting that RSpo proteins are general regulators of canonical Wnt signaling. Like RSpo1, RSpo2-4 antagonize DKK1 activity by interfering with DKK1 mediated LRP6 and Kremen association. Analysis of RSpo deletion mutants indicates that the cysteine-rich furin domains are sufficient and essential for the amplification of Wnt signaling and inhibition of DKK1, suggesting that Wnt amplification by RSpo proteins may be a direct consequence of DKK1 inhibition. Together, these findings indicate that RSpo proteins modulate the Wnt pathway by a common mechanism and suggest that coexpression with specific Wnt ligands and DKK1 may determine their biological specificity in vivo.

Published

2008

4. R-Spondin Family Members Regulate the Wnt Pathway by a Common Mechanism

Author

Kim, Kyung-Ah, Wagle, Marie, Tran, Karolyn, Zhan, Xiaoming, Dixon, Melissa A., Liu, Shouchun, Gros, Delphine, Korver, Wouter, Yonkovich, Shirlee, Tomasevic, Nenad, Binnerts, Minke, and Abo, Arie

Abstract

The R-Spondin (RSpo) family of secreted proteins is implicated in the activation of the Wnt signaling pathway. Despite the high structural homology between the four members, expression patterns and phenotypes in knockout mice have demonstrated striking differences. Here we dissected and compared the molecular and cellular function of all RSpo family members. Although all four RSpo proteins activate the canonical Wnt pathway, RSpo2 and 3 are more potent than RSpo1, whereas RSpo4 is relatively inactive. All RSpo members require Wnt ligands and LRP6 for activity and amplify signaling of Wnt3A, Wnt1, and Wnt7A, suggesting that RSpo proteins are general regulators of canonical Wnt signaling. Like RSpo1, RSpo2-4 antagonize DKK1 activity by interfering with DKK1 mediated LRP6 and Kremen association. Analysis of RSpo deletion mutants indicates that the cysteine-rich furin domains are sufficient and essential for the amplification of Wnt signaling and inhibition of DKK1, suggesting that Wnt amplification by RSpo proteins may be a direct consequence of DKK1 inhibition. Together, these findings indicate that RSpo proteins modulate the Wnt pathway by a common mechanism and suggest that coexpression with specific Wnt ligands and DKK1 may determine their biological specificity in vivo.

Published

2008

5. R-Spondin Proteins: A Novel Link to β-catenin Activation

Author

Kim, Kyung-Ah, Zhao, Jingsong, Andarmani, Susan, Kakitani, Makoto, Oshima, Takeshi, Binnerts, Minke E., Abo, Arie, Tomizuka, Kazuma, and Funk, Walter D.

Abstract

The RSpondin (Rspo) protein family is a recently described group of 4 distinct human secreted proteins. Reported activities for RSpo proteins include essential roles in vertebrate development and their ligand-type activities overlap substantially with those of the canonical Wnt ligands in that both RSpo and canonical Wnt signaling result in the activation of β-catenin. In a general functional screen for human secreted proteins using transgenic mouse models, we identified human Rspondin 1 (hRSpo1) protein as a potent and specific mitogen for the gastrointestinal epithelium and demonstrated potential therapeutic applications for the protein in mouse models of cancer therapy-induced mucositis. In contrast to previous studies, our data indicated only partial overlap between Wnt and RSpo ligand activities, suggesting that there may be independent receptor/signaling pathways for RSpo proteins that intersect those of Wnt at the level of β-catenin. Here we summarize the current reported data on the RSpo family and discuss these results in terms of alternate mechanisms of action. We have extended our observations on the potential therapeutic application of RSpo proteins by showing that all 4 human Rspo family members are capable of inducing epithelial proliferation and report the first non-vertebrate RSpo family member.

Published

2006

6. Low-affinity LFA-1/ICAM-3 interactions augment LFA-1/ICAM-1-mediated T cell adhesion and signaling by redistribution of LFA-1

Author

Bleijs, Diederik A., Binnerts, Minke E., Vliet, Sandra J. van, Figdor, Carl G., and Kooyk, Yvette van

Abstract

Although ICAM-3 is implicated in both adhesion and signal transduction events of leukocytes, its low affinity for LFA-1 compared to other ligands of LFA-1 has puzzled many investigators. Here we investigated the role of ICAM-3 in supporting LFA-1-mediated ICAM-1 binding and subsequently cell signaling. We observed that although ICAM-3 binds poorly to LFA-1 expressed on resting T cells, it specifically facilitates and increases LFA-1-mediated adhesion to the high affinity ligand of LFA-1, ICAM-1. We demonstrate that low-affinity binding of LFA-1 to ICAM-3 together with ICAM-1 alters the cell surface distribution of LFA-1 dramatically, inducing large clusters of LFA-1 that facilitate ICAM-1 binding after LFA-1 activation. We found that LFA-1-mediated ICAM-1 cell-cell interactions such as T cell proliferation greatly depend on low affinity LFA-1/ICAM-3 interactions that enhance stable LFA-1/ICAM-1 cell-cell contact. Taken together, these data demonstrate that low affinity LFA-1 binding to ICAM-3 regulates strong LFA-1/ICAM-1-mediated adhesion by driving LFA-1 into clusters to facilitate cell-cell interactions that take place in the immune system.

Published

2000