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W2018702616 endingPage "121" @default.
W2018702616 startingPage "108" @default.
W2018702616 abstract "Investigations over the last decade have established the essential role of growth factors and their receptors during angiogenesis and carcinogenesis. The vascular endothelial growth factor receptor (VEGFR) family in mammals contains three members, VEGFR-1 (Flt-1), VEGFR-2 (KDR/Flk-1) and VEGFR-3 (Flt-4), which are transmembrane tyrosine kinase receptors that regulate the formation of blood and lymphatic vessels. In the early 1990s, the above VEGFR was structurally characterized by cDNA cloning. Among these three receptors, VEGFR-2 is generally recognized to have a principal role in mediating VEGF-induced responses. VEGFR-2 is considered as the earliest marker for endothelial cell development. Importantly, VEGFR-2 directly regulates tumor angiogenesis. Therefore, several inhibitors of VEGFR-2 have been developed and many of them are now in clinical trials. In addition to targeting endothelial cells, the VEGF/VEGFR-2 system works as an essential autocrine/paracrine process for cancer cell proliferation and survival. Recent studies mark the continuous and increased interest in this related, but distinct, function of VEGF/VEGFR-2 in cancer cells: the autocrine/paracrine loop. Several mechanisms regulate VEGFR-2 levels and modulate its role in tumor angiogenesis and physiologic functions, i.e.: cellular localization/trafficking, regulation of cis-elements of promoter, epigenetic regulation and signaling from Notch, cytokines/growth factors and estrogen, etc. In this review, we will focus on updated information regarding VEGFR-2 research with respect to the molecular mechanisms of VEGFR-2 regulation in human breast cancer. Investigations in the activation, function, and regulation of VEGFR-2 in breast cancer will allow the development of new pharmacological strategies aimed at directly targeting cancer cell proliferation and survival." @default.
W2018702616 created "2016-06-24" @default.
W2018702616 creator A5001917541 @default.
W2018702616 creator A5002188808 @default.
W2018702616 creator A5052900803 @default.
W2018702616 creator A5055463915 @default.
W2018702616 creator A5066669900 @default.
W2018702616 date "2010-08-01" @default.
W2018702616 modified "2023-10-17" @default.
W2018702616 title "Vascular endothelial growth factor receptor-2 in breast cancer" @default.
W2018702616 cites W1504303645 @default.
W2018702616 cites W1527522386 @default.
W2018702616 cites W1587020653 @default.
W2018702616 cites W161301567 @default.
W2018702616 cites W1679229092 @default.
W2018702616 cites W1783580437 @default.
W2018702616 cites W1852654097 @default.
W2018702616 cites W1963545628 @default.
W2018702616 cites W1965987169 @default.
W2018702616 cites W1967348819 @default.
W2018702616 cites W1967818195 @default.
W2018702616 cites W1968384808 @default.
W2018702616 cites W1969328947 @default.
W2018702616 cites W1969695473 @default.
W2018702616 cites W1969700451 @default.
W2018702616 cites W1970053353 @default.
W2018702616 cites W1970607638 @default.
W2018702616 cites W1972102597 @default.
W2018702616 cites W1972670512 @default.
W2018702616 cites W1973701758 @default.
W2018702616 cites W1974218564 @default.
W2018702616 cites W1975892804 @default.
W2018702616 cites W1976305272 @default.
W2018702616 cites W1976489564 @default.
W2018702616 cites W1977962361 @default.
W2018702616 cites W1978466903 @default.
W2018702616 cites W1978638754 @default.
W2018702616 cites W1979006151 @default.
W2018702616 cites W1979037494 @default.
W2018702616 cites W1980952563 @default.
W2018702616 cites W1981218459 @default.
W2018702616 cites W1981612052 @default.
W2018702616 cites W1982383741 @default.
W2018702616 cites W1982912692 @default.
W2018702616 cites W1983165385 @default.
W2018702616 cites W1984644637 @default.
W2018702616 cites W1985262467 @default.
W2018702616 cites W1986559037 @default.
W2018702616 cites W1986826404 @default.
W2018702616 cites W1988535092 @default.
W2018702616 cites W1988698858 @default.
W2018702616 cites W1990521757 @default.
W2018702616 cites W1990624032 @default.
W2018702616 cites W1993881314 @default.
W2018702616 cites W1996285006 @default.
W2018702616 cites W1998353682 @default.
W2018702616 cites W1998441650 @default.
W2018702616 cites W2000292756 @default.
W2018702616 cites W2000771735 @default.
W2018702616 cites W2001780798 @default.
W2018702616 cites W2002698073 @default.
W2018702616 cites W2002829449 @default.
W2018702616 cites W2003598961 @default.
W2018702616 cites W2003885247 @default.
W2018702616 cites W2004681996 @default.
W2018702616 cites W2005340221 @default.
W2018702616 cites W2005581358 @default.
W2018702616 cites W2006122359 @default.
W2018702616 cites W2006939371 @default.
W2018702616 cites W2007819868 @default.
W2018702616 cites W2008543638 @default.
W2018702616 cites W2009427112 @default.
W2018702616 cites W2009812837 @default.
W2018702616 cites W2013288089 @default.
W2018702616 cites W2014148719 @default.
W2018702616 cites W2014163208 @default.
W2018702616 cites W2014704504 @default.
W2018702616 cites W2015867957 @default.
W2018702616 cites W2017323013 @default.
W2018702616 cites W2017879489 @default.
W2018702616 cites W2018512891 @default.
W2018702616 cites W2020968632 @default.
W2018702616 cites W2022091445 @default.
W2018702616 cites W2023053967 @default.
W2018702616 cites W2023433178 @default.
W2018702616 cites W2025933554 @default.
W2018702616 cites W2026656163 @default.
W2018702616 cites W2027601596 @default.
W2018702616 cites W2029482740 @default.
W2018702616 cites W2029521699 @default.
W2018702616 cites W2032050924 @default.
W2018702616 cites W2034458870 @default.
W2018702616 cites W2034459992 @default.
W2018702616 cites W2040089666 @default.
W2018702616 cites W2040506727 @default.
W2018702616 cites W2041098552 @default.
W2018702616 cites W2042444876 @default.
W2018702616 cites W2043850275 @default.