Research output: Contribution to journal › Article › peer-review
Proposed Dynamics of CDB3 Activation in Human Erythrocytes by Nifedipine Studied with Scanning Flow Cytometry. / Yastrebova, Ekaterina S.; Konokhova, Anastasiya I.; Strokotov, Dmitry I. et al.
In: Cytometry Part A, Vol. 95, No. 12, 12.2019, p. 1275-1284.Research output: Contribution to journal › Article › peer-review
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TY - JOUR
T1 - Proposed Dynamics of CDB3 Activation in Human Erythrocytes by Nifedipine Studied with Scanning Flow Cytometry
AU - Yastrebova, Ekaterina S.
AU - Konokhova, Anastasiya I.
AU - Strokotov, Dmitry I.
AU - Karpenko, Andrei A.
AU - Maltsev, Valeri P.
AU - Chernyshev, Andrei V.
N1 - © 2019 International Society for Advancement of Cytometry.
PY - 2019/12
Y1 - 2019/12
N2 - Nifedipine is calcium channels and pumps blocker widely used in medicine. However, mechanisms of nifedipine action in blood are not clear. In particular, the influence of nifedipine on erythrocytes is far from completely understood. In this work, applying scanning flow cytometry, we observed experimentally for the first time the dynamics behind a significant increase of HCO3 −/Cl− transmembrane exchange rate of CDB3 (main anion exchanger, AE1, Band 3, SLC4A1) of human erythrocytes in the presence of nifedipine in blood. It was found that the rate of CDB3 activation is not limited by the rate of nifedipine binding and/or Ca2+ transport. In order to explain the experimental data, we suggested a kinetic model assuming that the rate of CDB3 activation is limited by the dynamics of the balance between two intracellular processes (1) the activation of CDB3 limited by its interaction with intracellular Ca2+, and (2) the spontaneous deactivation of CDB3. Thus the use of scanning flow cytometry allowed to clarify quantitatively the molecular kinetic mechanism of nifedipine action on human erythrocytes. In particular, the efficiency (~30) and rates of activation (~0.3 min−1) and deactivation (~10−3 min−1) of CDB3 in human erythrocytes was evaluated for two donors.
AB - Nifedipine is calcium channels and pumps blocker widely used in medicine. However, mechanisms of nifedipine action in blood are not clear. In particular, the influence of nifedipine on erythrocytes is far from completely understood. In this work, applying scanning flow cytometry, we observed experimentally for the first time the dynamics behind a significant increase of HCO3 −/Cl− transmembrane exchange rate of CDB3 (main anion exchanger, AE1, Band 3, SLC4A1) of human erythrocytes in the presence of nifedipine in blood. It was found that the rate of CDB3 activation is not limited by the rate of nifedipine binding and/or Ca2+ transport. In order to explain the experimental data, we suggested a kinetic model assuming that the rate of CDB3 activation is limited by the dynamics of the balance between two intracellular processes (1) the activation of CDB3 limited by its interaction with intracellular Ca2+, and (2) the spontaneous deactivation of CDB3. Thus the use of scanning flow cytometry allowed to clarify quantitatively the molecular kinetic mechanism of nifedipine action on human erythrocytes. In particular, the efficiency (~30) and rates of activation (~0.3 min−1) and deactivation (~10−3 min−1) of CDB3 in human erythrocytes was evaluated for two donors.
KW - adalat
KW - band 3
KW - calcium ions
KW - kinetic modeling
KW - red blood cells
KW - MEMBRANES
KW - CALCIUM-CHANNEL BLOCKERS
KW - TRANSPORT
KW - KINETICS
KW - DRUGS
KW - RED-BLOOD-CELLS
KW - BINDING-SITES
KW - EXCHANGE
KW - ANTAGONISTS
KW - CHLORIDE
UR - http://www.scopus.com/inward/record.url?scp=85075390654&partnerID=8YFLogxK
U2 - 10.1002/cyto.a.23918
DO - 10.1002/cyto.a.23918
M3 - Article
C2 - 31750613
AN - SCOPUS:85075390654
VL - 95
SP - 1275
EP - 1284
JO - Cytometry. Part A : the journal of the International Society for Analytical Cytology
JF - Cytometry. Part A : the journal of the International Society for Analytical Cytology
SN - 1552-4922
IS - 12
ER -
ID: 22404324