The orphan tyrosine kinase receptor, ROR2, mediates Wnt5A signaling in metastatic melanoma

M. P. Oconnell; J. L. Fiori; M. Xu; A. D. Carter; B. P. Frank; T. C. Camilli; A. D. French; S. K. Dissanayake; F. E. Indig; M. Bernier; D. D. Taub; S. M. Hewitt; A. T. Weeraratna

doi:10.1038/onc.2009.305

The orphan tyrosine kinase receptor, ROR2, mediates Wnt5A signaling in metastatic melanoma

M. P. Oconnell, J. L. Fiori, M. Xu, A. D. Carter, B. P. Frank, T. C. Camilli, A. D. French, S. K. Dissanayake, F. E. Indig, M. Bernier, D. D. Taub, S. M. Hewitt, A. T. Weeraratna

Research output: Contribution to journal › Article › peer-review

133 Scopus citations

Abstract

Tyrosine kinase receptors represent targets of great interest for cancer therapy. Here we show, for the first time, the importance of the orphan tyrosine kinase receptor, ROR2, in melanoma progression. Using melanoma tissue microarrays, we show that ROR2 is expressed predominantly in metastatic melanoma. As ROR2 has been shown to specifically interact with the non-canonical Wnt ligand, Wnt5A, this corroborates our earlier data implicating Wnt5A as a mediator of melanoma metastasis. We show here that increases in Wnt5A cause increases in ROR2 expression, as well as the PKC-dependent, clathrin-mediated internalization of ROR2. WNT5A knockdown by siRNA decreases ROR2 expression, but silencing of ROR2 has no effect on WNT5A levels. ROR2 knockdown does, however, result in a decrease in signaling downstream of Wnt5A. Using in vitro and in vivo metastasis assays, we show that ROR2 is necessary for the Wnt5A-mediated metastasis of melanoma cells. These data imply that ROR2 may represent a novel target for melanoma therapy.

Original language	English (US)
Pages (from-to)	34-44
Number of pages	11
Journal	Oncogene
Volume	29
Issue number	1
DOIs	https://doi.org/10.1038/onc.2009.305
State	Published - Jan 2010
Externally published	Yes

Keywords

Clathrin
Endosome
Melanoma
Metastasis
Ror2
Wnt5A

ASJC Scopus subject areas

Molecular Biology
Genetics
Cancer Research

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10.1038/onc.2009.305

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title = "The orphan tyrosine kinase receptor, ROR2, mediates Wnt5A signaling in metastatic melanoma",

abstract = "Tyrosine kinase receptors represent targets of great interest for cancer therapy. Here we show, for the first time, the importance of the orphan tyrosine kinase receptor, ROR2, in melanoma progression. Using melanoma tissue microarrays, we show that ROR2 is expressed predominantly in metastatic melanoma. As ROR2 has been shown to specifically interact with the non-canonical Wnt ligand, Wnt5A, this corroborates our earlier data implicating Wnt5A as a mediator of melanoma metastasis. We show here that increases in Wnt5A cause increases in ROR2 expression, as well as the PKC-dependent, clathrin-mediated internalization of ROR2. WNT5A knockdown by siRNA decreases ROR2 expression, but silencing of ROR2 has no effect on WNT5A levels. ROR2 knockdown does, however, result in a decrease in signaling downstream of Wnt5A. Using in vitro and in vivo metastasis assays, we show that ROR2 is necessary for the Wnt5A-mediated metastasis of melanoma cells. These data imply that ROR2 may represent a novel target for melanoma therapy.",

keywords = "Clathrin, Endosome, Melanoma, Metastasis, Ror2, Wnt5A",

author = "Oconnell, {M. P.} and Fiori, {J. L.} and M. Xu and Carter, {A. D.} and Frank, {B. P.} and Camilli, {T. C.} and French, {A. D.} and Dissanayake, {S. K.} and Indig, {F. E.} and M. Bernier and Taub, {D. D.} and Hewitt, {S. M.} and Weeraratna, {A. T.}",

note = "Funding Information: We thank Ms Ana Lustig for assistance with animal experiments. This work was supported by the Intramural Research Program of the National Institute on Aging, Baltimore, MD 21224, USA.",

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AU - Fiori, J. L.

AU - Xu, M.

AU - Carter, A. D.

AU - Frank, B. P.

AU - Camilli, T. C.

AU - French, A. D.

AU - Dissanayake, S. K.

AU - Indig, F. E.

AU - Bernier, M.

AU - Taub, D. D.

AU - Hewitt, S. M.

AU - Weeraratna, A. T.

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N2 - Tyrosine kinase receptors represent targets of great interest for cancer therapy. Here we show, for the first time, the importance of the orphan tyrosine kinase receptor, ROR2, in melanoma progression. Using melanoma tissue microarrays, we show that ROR2 is expressed predominantly in metastatic melanoma. As ROR2 has been shown to specifically interact with the non-canonical Wnt ligand, Wnt5A, this corroborates our earlier data implicating Wnt5A as a mediator of melanoma metastasis. We show here that increases in Wnt5A cause increases in ROR2 expression, as well as the PKC-dependent, clathrin-mediated internalization of ROR2. WNT5A knockdown by siRNA decreases ROR2 expression, but silencing of ROR2 has no effect on WNT5A levels. ROR2 knockdown does, however, result in a decrease in signaling downstream of Wnt5A. Using in vitro and in vivo metastasis assays, we show that ROR2 is necessary for the Wnt5A-mediated metastasis of melanoma cells. These data imply that ROR2 may represent a novel target for melanoma therapy.

AB - Tyrosine kinase receptors represent targets of great interest for cancer therapy. Here we show, for the first time, the importance of the orphan tyrosine kinase receptor, ROR2, in melanoma progression. Using melanoma tissue microarrays, we show that ROR2 is expressed predominantly in metastatic melanoma. As ROR2 has been shown to specifically interact with the non-canonical Wnt ligand, Wnt5A, this corroborates our earlier data implicating Wnt5A as a mediator of melanoma metastasis. We show here that increases in Wnt5A cause increases in ROR2 expression, as well as the PKC-dependent, clathrin-mediated internalization of ROR2. WNT5A knockdown by siRNA decreases ROR2 expression, but silencing of ROR2 has no effect on WNT5A levels. ROR2 knockdown does, however, result in a decrease in signaling downstream of Wnt5A. Using in vitro and in vivo metastasis assays, we show that ROR2 is necessary for the Wnt5A-mediated metastasis of melanoma cells. These data imply that ROR2 may represent a novel target for melanoma therapy.

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The orphan tyrosine kinase receptor, ROR2, mediates Wnt5A signaling in metastatic melanoma

Abstract

Keywords

ASJC Scopus subject areas

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