FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2082850593> ?p ?o ?g. }

• W2082850593 endingPage "3686" @default.
• W2082850593 startingPage "3680" @default.
• W2082850593 abstract "In neurons alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) receptors are heteromeric cation channels composed of different sub-units, including GluA1-GluA4. When expressed without GluA2, AMPA receptors function as Ca(2+)-permeable cation channels. In erythrocytes, activation of Ca(2+)-permeable cation channels triggers suicidal erythrocyte death or eryptosis, which is characterized by cell shrinkage and cell membrane scrambling with subsequent exposure of phosphatidylserine at the cell surface. Activators of the channels and thus eryptosis include removal of extracellular Cl(-) (replaced by gluconate) and energy depletion (removal of glucose). The present study explored whether GluA1 is expressed in human erythrocytes and whether pharmacological AMPA receptor inhibition modifies Ca(2+) entry and suicidal death of human erythrocytes. GluA1 protein abundance was determined by confocal microscopy, phosphatidylserine exposure was estimated from annexin V binding, cell volume from forward scatter in FACS analysis, cytosolic Ca(2+) concentration from Fluo3 fluorescence and channel activity by whole-cell patch-clamp recordings. As a result, GluA1 is indeed expressed in the erythrocyte cell membrane. The AMPA receptor antagonist NBQX (1,2,3,4-tetrahydro-6-nitro-2,3-dioxo-benzo[f]quinoxaline-7-sulfonamide) inhibited the cation channels following Cl(-) removal and the eryptosis following Cl(-) removal or energy depletion. The present study reveals a novel action of AMPA receptor antagonists and raises the possibility that GluA1 or a pharmacologically related protein participates in the regulation of Ca(2+) entry into and suicidal death of human erythrocytes." @default.
• W2082850593 created "2016-06-24" @default.
• W2082850593 creator A5009783365 @default.
• W2082850593 creator A5011594882 @default.
• W2082850593 creator A5013113003 @default.
• W2082850593 creator A5024880361 @default.
• W2082850593 creator A5045486238 @default.
• W2082850593 creator A5050589869 @default.
• W2082850593 creator A5061162593 @default.
• W2082850593 creator A5068868920 @default.
• W2082850593 creator A5084208566 @default.
• W2082850593 date "2009-03-13" @default.
• W2082850593 modified "2023-09-28" @default.
• W2082850593 title "Modulation of suicidal erythrocyte cation channels by an AMPA antagonist" @default.
• W2082850593 cites W13114315 @default.
• W2082850593 cites W1653202928 @default.
• W2082850593 cites W1969533761 @default.
• W2082850593 cites W1972748726 @default.
• W2082850593 cites W1973163231 @default.
• W2082850593 cites W1976466808 @default.
• W2082850593 cites W1985040456 @default.
• W2082850593 cites W1985345682 @default.
• W2082850593 cites W1987362442 @default.
• W2082850593 cites W1990356838 @default.
• W2082850593 cites W1996497038 @default.
• W2082850593 cites W2003505368 @default.
• W2082850593 cites W2005216533 @default.
• W2082850593 cites W2014189646 @default.
• W2082850593 cites W2014315244 @default.
• W2082850593 cites W2016299124 @default.
• W2082850593 cites W2017459003 @default.
• W2082850593 cites W2019471670 @default.
• W2082850593 cites W2019547209 @default.
• W2082850593 cites W2034867646 @default.
• W2082850593 cites W2036961219 @default.
• W2082850593 cites W2038819783 @default.
• W2082850593 cites W2039616271 @default.
• W2082850593 cites W2039659095 @default.
• W2082850593 cites W2041463978 @default.
• W2082850593 cites W2042948104 @default.
• W2082850593 cites W2043119510 @default.
• W2082850593 cites W2051040462 @default.
• W2082850593 cites W2051379535 @default.
• W2082850593 cites W2052726190 @default.
• W2082850593 cites W2058196146 @default.
• W2082850593 cites W2064230564 @default.
• W2082850593 cites W2065196084 @default.
• W2082850593 cites W2065641335 @default.
• W2082850593 cites W2074728848 @default.
• W2082850593 cites W2077776183 @default.
• W2082850593 cites W2078137514 @default.
• W2082850593 cites W2079807108 @default.
• W2082850593 cites W2088533769 @default.
• W2082850593 cites W2089242051 @default.
• W2082850593 cites W2089281127 @default.
• W2082850593 cites W2089976554 @default.
• W2082850593 cites W2092025193 @default.
• W2082850593 cites W2098000156 @default.
• W2082850593 cites W2098107333 @default.
• W2082850593 cites W2122881251 @default.
• W2082850593 cites W2131523916 @default.
• W2082850593 cites W2133617951 @default.
• W2082850593 cites W2141256837 @default.
• W2082850593 cites W2148045277 @default.
• W2082850593 cites W2148394321 @default.
• W2082850593 cites W2148460663 @default.
• W2082850593 cites W2150151471 @default.
• W2082850593 cites W2155670471 @default.
• W2082850593 cites W2161979340 @default.
• W2082850593 cites W2167926343 @default.
• W2082850593 cites W2317277068 @default.
• W2082850593 cites W2334570807 @default.
• W2082850593 cites W4248717353 @default.
• W2082850593 doi "https://doi.org/10.1111/j.1582-4934.2009.00745.x" @default.
• W2082850593 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4516516" @default.
• W2082850593 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/19320779" @default.
• W2082850593 hasPublicationYear "2009" @default.
• W2082850593 type Work @default.
• W2082850593 sameAs 2082850593 @default.
• W2082850593 citedByCount "17" @default.
• W2082850593 countsByYear W20828505932012 @default.
• W2082850593 countsByYear W20828505932013 @default.
• W2082850593 countsByYear W20828505932015 @default.
• W2082850593 countsByYear W20828505932016 @default.
• W2082850593 countsByYear W20828505932017 @default.
• W2082850593 countsByYear W20828505932019 @default.
• W2082850593 countsByYear W20828505932020 @default.
• W2082850593 crossrefType "journal-article" @default.
• W2082850593 hasAuthorship W2082850593A5009783365 @default.
• W2082850593 hasAuthorship W2082850593A5011594882 @default.
• W2082850593 hasAuthorship W2082850593A5013113003 @default.
• W2082850593 hasAuthorship W2082850593A5024880361 @default.
• W2082850593 hasAuthorship W2082850593A5045486238 @default.
• W2082850593 hasAuthorship W2082850593A5050589869 @default.
• W2082850593 hasAuthorship W2082850593A5061162593 @default.
• W2082850593 hasAuthorship W2082850593A5068868920 @default.
• W2082850593 hasAuthorship W2082850593A5084208566 @default.
• W2082850593 hasBestOaLocation W20828505932 @default.

• next