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Supplementary Table 1 from VEGFR-1 Expressed by Malignant Melanoma-Initiating Cells Is Required for Tumor Growth

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posted on 2023-03-30, 20:32 authored by Natasha Y. Frank, Tobias Schatton, Soo Kim, Qian Zhan, Brian J. Wilson, Jie Ma, Karim R. Saab, Veronika Osherov, Hans R. Widlund, Martin Gasser, Ana-Maria Waaga-Gasser, Thomas S. Kupper, George F. Murphy, Markus H. Frank
Supplementary Table 1 from VEGFR-1 Expressed by Malignant Melanoma-Initiating Cells Is Required for Tumor Growth

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ARTICLE ABSTRACT

Melanoma growth is driven by malignant melanoma-initiating cells (MMIC) identified by expression of the ATP-binding cassette (ABC) member ABCB5. ABCB5+ melanoma subpopulations have been shown to overexpress the vasculogenic differentiation markers CD144 (VE-cadherin) and TIE1 and are associated with CD31− vasculogenic mimicry (VM), an established biomarker associated with increased patient mortality. Here we identify a critical role for VEGFR-1 signaling in ABCB5+ MMIC-dependent VM and tumor growth. Global gene expression analyses, validated by mRNA and protein determinations, revealed preferential expression of VEGFR-1 on ABCB5+ tumor cells purified from clinical melanomas and established melanoma lines. In vitro, VEGF induced the expression of CD144 in ABCB5+ subpopulations that constitutively expressed VEGFR-1 but not in ABCB5− bulk populations that were predominantly VEGFR-1−. In vivo, melanoma-specific shRNA-mediated knockdown of VEGFR-1 blocked the development of ABCB5+ VM morphology and inhibited ABCB5+ VM-associated production of the secreted melanoma mitogen laminin. Moreover, melanoma-specific VEGFR-1 knockdown markedly inhibited tumor growth (by >90%). Our results show that VEGFR-1 function in MMIC regulates VM and associated laminin production and show that this function represents one mechanism through which MMICs promote tumor growth. Cancer Res; 71(4); 1474–85. ©2011 AACR.

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