FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2511912785> ?p ?o ?g. }

• W2511912785 endingPage "119" @default.
• W2511912785 startingPage "108" @default.
• W2511912785 abstract "Neurological disorders account for a majority of non-malignant disability in humans and are often associated with dysfunction of the blood–brain barrier (BBB). Recent evidence shows that despite apparent variation in the origin of neural damage, the central nervous system has a common injury response mechanism involving platelet-derived growth factor (PDGF)-CC activation in the neurovascular unit and subsequent dysfunction of BBB integrity. Inhibition of PDGF-CC signaling with imatinib in mice has been shown to prevent BBB dysfunction and have neuroprotective effects in acute damage conditions, including traumatic brain injury, seizures or stroke, as well as in neurodegenerative diseases that develop over time, including multiple sclerosis and amyotrophic lateral sclerosis. Stroke and traumatic injuries are major risk factors for age-associated neurodegenerative disorders and we speculate that restoring BBB properties through PDGF-CC inhibition might provide a common therapeutic opportunity for treatment of both acute and progressive neuropathology in humans. In this review we will summarize what is known about the role of PDGF-CC in neurovascular signaling events and the variety of seemingly different neuropathologies it is involved in. We will also discuss the pharmacological means of therapeutic interventions for anti-PDGF-CC therapy and ongoing clinical trials. In summary: inhibition of PDGF-CC signaling can be protective for immediate injury and decrease the long-term neurodegenerative consequences." @default.
• W2511912785 created "2016-09-16" @default.
• W2511912785 creator A5063870060 @default.
• W2511912785 creator A5076240846 @default.
• W2511912785 creator A5079317977 @default.
• W2511912785 creator A5080323249 @default.
• W2511912785 date "2016-11-01" @default.
• W2511912785 modified "2023-10-17" @default.
• W2511912785 title "Pharmacological targeting of the PDGF-CC signaling pathway for blood–brain barrier restoration in neurological disorders" @default.
• W2511912785 cites W1036529846 @default.
• W2511912785 cites W1483090589 @default.
• W2511912785 cites W1501414201 @default.
• W2511912785 cites W1536679159 @default.
• W2511912785 cites W1539181678 @default.
• W2511912785 cites W1545901128 @default.
• W2511912785 cites W1561335619 @default.
• W2511912785 cites W1656083676 @default.
• W2511912785 cites W1690266451 @default.
• W2511912785 cites W1873304887 @default.
• W2511912785 cites W1948282121 @default.
• W2511912785 cites W1950705225 @default.
• W2511912785 cites W1957400240 @default.
• W2511912785 cites W1965180960 @default.
• W2511912785 cites W1968133365 @default.
• W2511912785 cites W1968758728 @default.
• W2511912785 cites W1969086552 @default.
• W2511912785 cites W1971407639 @default.
• W2511912785 cites W1973358829 @default.
• W2511912785 cites W1973593092 @default.
• W2511912785 cites W1977894531 @default.
• W2511912785 cites W1979127347 @default.
• W2511912785 cites W1980735023 @default.
• W2511912785 cites W1981255942 @default.
• W2511912785 cites W1981843633 @default.
• W2511912785 cites W1983556223 @default.
• W2511912785 cites W1987797105 @default.
• W2511912785 cites W1988760910 @default.
• W2511912785 cites W1990887043 @default.
• W2511912785 cites W1992280915 @default.
• W2511912785 cites W1994731435 @default.
• W2511912785 cites W1995037165 @default.
• W2511912785 cites W1995596161 @default.
• W2511912785 cites W1996259832 @default.
• W2511912785 cites W1996537922 @default.
• W2511912785 cites W1998024620 @default.
• W2511912785 cites W1998837476 @default.
• W2511912785 cites W1998846962 @default.
• W2511912785 cites W1998907224 @default.
• W2511912785 cites W2000845467 @default.
• W2511912785 cites W2000956676 @default.
• W2511912785 cites W2000965529 @default.
• W2511912785 cites W2001408101 @default.
• W2511912785 cites W2002354013 @default.
• W2511912785 cites W2002711747 @default.
• W2511912785 cites W2004431239 @default.
• W2511912785 cites W2006035554 @default.
• W2511912785 cites W2006316634 @default.
• W2511912785 cites W2010915352 @default.
• W2511912785 cites W2011450474 @default.
• W2511912785 cites W2011574374 @default.
• W2511912785 cites W2012006815 @default.
• W2511912785 cites W2012460154 @default.
• W2511912785 cites W2012557807 @default.
• W2511912785 cites W2013662783 @default.
• W2511912785 cites W2015338496 @default.
• W2511912785 cites W2015541518 @default.
• W2511912785 cites W2016147098 @default.
• W2511912785 cites W2017715011 @default.
• W2511912785 cites W2025935987 @default.
• W2511912785 cites W2026688102 @default.
• W2511912785 cites W2028265367 @default.
• W2511912785 cites W2032341330 @default.
• W2511912785 cites W2033441741 @default.
• W2511912785 cites W2034098691 @default.
• W2511912785 cites W2034470062 @default.
• W2511912785 cites W2035263256 @default.
• W2511912785 cites W2035408187 @default.
• W2511912785 cites W2036960054 @default.
• W2511912785 cites W2039885178 @default.
• W2511912785 cites W2044643825 @default.
• W2511912785 cites W2044649561 @default.
• W2511912785 cites W2046199264 @default.
• W2511912785 cites W2047853787 @default.
• W2511912785 cites W2049806614 @default.
• W2511912785 cites W2050564231 @default.
• W2511912785 cites W2052459267 @default.
• W2511912785 cites W2054337365 @default.
• W2511912785 cites W2054868504 @default.
• W2511912785 cites W2055429754 @default.
• W2511912785 cites W2055467683 @default.
• W2511912785 cites W2055469901 @default.
• W2511912785 cites W2056141658 @default.
• W2511912785 cites W2056377364 @default.
• W2511912785 cites W2056856515 @default.
• W2511912785 cites W2057898725 @default.
• W2511912785 cites W2058756735 @default.
• W2511912785 cites W2059631065 @default.
• W2511912785 cites W2059736935 @default.

• next