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EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis.

EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis. Research Abstract Details 

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  • EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis. Abstract Text:

    xiaoyong huangXiaoyong Huang,yoshihiro yamadaYoshihiro Yamada,hiroyasu kidoyaHiroyasu Kidoya,hisamichi naitoHisamichi Naito,yumi nagahamaYumi Nagahama,lingyu kongLingyu Kong,shin-ya katohShin-Ya Katoh,weng-lin liWeng-lin Li,masaya uenoMasaya Ueno,nobuyuki takakuraNobuyuki Takakura,xiaoyong huangXiaoyong Huang,yoshihiro yamadaYoshihiro Yamada,hiroyasu kidoyaHiroyasu Kidoya,hisamichi naitoHisamichi Naito,yumi nagahamaYumi Nagahama,lingyu kongLingyu Kong,shin-ya katohShin-Ya Katoh,weng-lin liWeng-lin Li,masaya uenoMasaya Ueno,nobuyuki takakuraNobuyuki Takakura,

    EphB4 receptor and its ligand ephrinB2 play an important role in vascular development during embryogenesis. In blood vessels, ephrinB2 is expressed in arterial endothelial cells (EC) and mesenchymal supporting cells, whereas EphB4 is only expressed in venous ECs. Previously, we reported that OP9 stromal cells, which support the development of both arterial and venous ECs, in which EphB4 was overexpressed, could inhibit ephrinB2-positive (ephrinB2+) EC development in an embryonic tissue organ culture system. Although the EphB4 receptor is expressed in a variety of tumor cells, its exact function in regulating tumor progression has not been clearly shown. Here we found that overexpression of EphB4 in B16 melanoma cells suppressed tumor growth in a s.c. transplantation tumor model. Histologic examination of these tumors revealed that EphB4 overexpression in B16 cells selectively suppressed arterial ephrinB2+ EC development. By coculturing ephrinB2-expressing SV40-transformed mouse ECs (SVEC) with EphB4-overexpressing B16 cells, we found that EphB4 induced the apoptosis of SVECs. However, ephrinB2 did not induce the apoptosis of EphB4-overexpressing B16 cells. Based on results from these experiments, we concluded that EphB4 overexpression in B16 tumor cells suppresses the survival of arterial ECs in tumors by a reverse signaling via ephrinB2.

    EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis. Publishing Authors By Initials

    x huangX Huang,y yamadaY Yamada,h kidoyaH Kidoya,h naitoH Naito,y nagahamaY Nagahama,l kongL Kong,sy katohSY Katoh,wl liWL Li,m uenoM Ueno,n takakuraN Takakura,x huangX Huang,y yamadaY Yamada,h kidoyaH Kidoya,h naitoH Naito,y nagahamaY Nagahama,l kongL Kong,sy katohSY Katoh,wl liWL Li,m uenoM Ueno,n takakuraN Takakura,

    For similar abstracts research abstracts see: abstracts research

    PUBMED ID PMID:

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    EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis. Journal Published:

    PUBLICATION TYPE: Research Support, Non-U.S. Gov

    Journal: Cancer research

    VOLUME: 67

    Page Numbers: 9800-8

    Journal Abbreviation: Cancer Res.

    ISSN: 0008-5472

    DAY: 15

    MONTH: Oct

    YEAR: 2007

    EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis. Information

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    LANGUAGE: eng

    NlmUniqueID: 2984705

    EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis. Keywords Mesh Terms:

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    Grant and Affiliation Information for EphB4 overexpression in B16 melanoma cells affects arterial-venous patterning in tumor angiogenesis.

    AFFILIATION: Department of Stem Cell Biology, Cancer Research Institute, Kanazawa University, Kanazawa, Japan.

    Country: United States

    United States Research PublicationUnited States Research Publication

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    MEDLINETA: Cancer Res

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