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• W165593485 endingPage "191" @default.
• W165593485 startingPage "175" @default.
• W165593485 abstract "Prostate cancer (CaP) is the most frequently diagnosed cancer in men and the second leading cause of cancer death among men in the United States (1). The most common site of CaP metastasis is the bone with skeletal metastases identified at autopsy in up to 90% of patients dying from CaP. Understanding how tumor interacts with bone may lead toward identifying therapies to prevent or diminish the consequences of bone metastases. CaP forms a mixture of osteolytic (excess bone resorption) and osteoblastic (excess bone production) bone metastases. The osteolytic component of bone metastases is caused, in part, through cancer-mediated activation of the receptor of nuclear factor-κ B ligand (RANKL) pathway. Blocking RANKL has been shown to successfully inhibit establishment or progression of CaP bone metastases in animal models. Other factors that are important in the development of CaP-induced osteolytic lesions include interleukin (IL)-6, parathyroid hormonerelated protein (PTHrP), and matrix metalloproteinases (MMPs). The mechanism through which CaP induces osteoblastic lesions is less clear; however, CaP produces a variety of factors that may promote an overall osteoblastic phenotype, including an inhibitor of RANKL, osteoprotegerin (OPG); a vascular-active agent, endothelin (ET)-1; and transforming growth factor (TGF)-β. Several methods to target CaP bone metastases are being explored in clinics, including bisphosphonates, inhibitors of RANKL and ET-1. To effectively treat CaP bone metastases, targeting both the osteolytic and osteoblastic components simultaneously may be important.Key WordsBone metastasesendothelin-1ET-1IL-6interleukin-6OPGosteoprotegerinprostate cancerparathyroid hormone-related proteinPTHrPRANKLreceptor of nuclear factor-κ B" @default.
• W165593485 created "2016-06-24" @default.
• W165593485 creator A5056820426 @default.
• W165593485 date "2007-11-09" @default.
• W165593485 modified "2023-10-16" @default.
• W165593485 title "Biology and Therapeutic Basis of Prostate Cancer Bone Metastasis" @default.
• W165593485 cites W1218970471 @default.
• W165593485 cites W1242972575 @default.
• W165593485 cites W129503514 @default.
• W165593485 cites W148806015 @default.
• W165593485 cites W1534645474 @default.
• W165593485 cites W1537488315 @default.
• W165593485 cites W1577265851 @default.
• W165593485 cites W1583699618 @default.
• W165593485 cites W1771981018 @default.
• W165593485 cites W1776476655 @default.
• W165593485 cites W193883077 @default.
• W165593485 cites W1951349736 @default.
• W165593485 cites W1964066819 @default.
• W165593485 cites W1966433358 @default.
• W165593485 cites W1966478270 @default.
• W165593485 cites W1970111327 @default.
• W165593485 cites W1972351551 @default.
• W165593485 cites W1972448628 @default.
• W165593485 cites W1974659965 @default.
• W165593485 cites W1975577875 @default.
• W165593485 cites W1976735184 @default.
• W165593485 cites W1978194192 @default.
• W165593485 cites W1979097970 @default.
• W165593485 cites W1979354287 @default.
• W165593485 cites W1981340011 @default.
• W165593485 cites W1982017899 @default.
• W165593485 cites W1982055377 @default.
• W165593485 cites W1982915376 @default.
• W165593485 cites W1982926533 @default.
• W165593485 cites W1984466851 @default.
• W165593485 cites W1984539870 @default.
• W165593485 cites W1984965767 @default.
• W165593485 cites W1988275376 @default.
• W165593485 cites W1988745043 @default.
• W165593485 cites W1990282396 @default.
• W165593485 cites W1991170888 @default.
• W165593485 cites W1992159640 @default.
• W165593485 cites W1995328990 @default.
• W165593485 cites W1997641179 @default.
• W165593485 cites W1998269329 @default.
• W165593485 cites W1998580928 @default.
• W165593485 cites W2000647744 @default.
• W165593485 cites W2002626138 @default.
• W165593485 cites W2003733256 @default.
• W165593485 cites W2003865675 @default.
• W165593485 cites W2005191521 @default.
• W165593485 cites W2005258782 @default.
• W165593485 cites W2007150980 @default.
• W165593485 cites W2013176040 @default.
• W165593485 cites W2014397497 @default.
• W165593485 cites W2015137515 @default.
• W165593485 cites W2015332970 @default.
• W165593485 cites W2016308519 @default.
• W165593485 cites W2017614987 @default.
• W165593485 cites W2018414325 @default.
• W165593485 cites W2018577003 @default.
• W165593485 cites W2018990561 @default.
• W165593485 cites W2019091035 @default.
• W165593485 cites W2019917228 @default.
• W165593485 cites W2020561186 @default.
• W165593485 cites W2020814497 @default.
• W165593485 cites W2021081285 @default.
• W165593485 cites W2025341919 @default.
• W165593485 cites W2027235538 @default.
• W165593485 cites W2027602629 @default.
• W165593485 cites W2028810705 @default.
• W165593485 cites W2029838719 @default.
• W165593485 cites W2031521622 @default.
• W165593485 cites W2031687428 @default.
• W165593485 cites W2033890749 @default.
• W165593485 cites W2034437450 @default.
• W165593485 cites W2035411162 @default.
• W165593485 cites W2035636765 @default.
• W165593485 cites W2036978099 @default.
• W165593485 cites W2038345192 @default.
• W165593485 cites W2038724769 @default.
• W165593485 cites W2039181986 @default.
• W165593485 cites W2039686677 @default.
• W165593485 cites W2040234201 @default.
• W165593485 cites W2040348117 @default.
• W165593485 cites W2040539245 @default.
• W165593485 cites W2041095267 @default.
• W165593485 cites W2041959707 @default.
• W165593485 cites W2042303782 @default.
• W165593485 cites W2043923185 @default.
• W165593485 cites W2044794329 @default.
• W165593485 cites W2048299560 @default.
• W165593485 cites W2049481811 @default.
• W165593485 cites W2049818713 @default.
• W165593485 cites W2052104719 @default.
• W165593485 cites W2054498103 @default.
• W165593485 cites W2055880820 @default.

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