Bradykinin (BK) induces fibroblast contraction but the structural changes and intracellular mechanisms involved have not been completely explored.We stimulated HFL-1 fibroblasts with BK to assess: 1) fibroblast contractility; 2) the role of α-smooth muscle actin (SMA) in contraction by small interfering RNA (siRNA); 3) α-SMA protein expression; 4) α-SMA and F-actin structure; 5) intracellular calcium concentration ([Ca2+]i); and 6) phosphorylated myosin light-chain (pMLC) and MLC kinase (MLCK) expression.BK triggered concentration- and time-dependent fibroblast gel contraction in conjunction with α-SMA over expression, but not in α-SMA-siRNA-treated cells. BK also increased α-SMA+ and F-actin+ cell number and stress fibre polymerisation (detectable at 5–60 min). These BK-induced changes were associated with an increase in [Ca2+]i, which peaked within 15 s, and activation of pMLC, which was detectable at 5–60 min. No MLCK content modification was observed. The different manifestations of the BK-induced fibroblast activation were downregulated at different levels (25–100%) by HOE140, a specific BK B2 receptor (B2R) antagonist and by the Ca2+ chelator, EGTA.Thus, BK-induced fibroblast contraction, associated with differentiation into α-SMA+ myofibroblasts, is mediated through the activation of the B2R and involves the Ca2+/calmodulin pMLC-dependent pathway.
Mechanisms of bradykinin-induced contraction in human fetal lung fibroblasts / Petecchia, L; Sabatini, F; Usai, C; Carnevali, Stefano; Ognibene, M; Vanni, C; Eva, A; Fabbri, Leonardo; Rossi, Giulio; Ricciardolo, F. l.. - In: EUROPEAN RESPIRATORY JOURNAL. - ISSN 0903-1936. - STAMPA. - 36:3(2010), pp. 655-664. [10.1183/09031936.00112209]
Mechanisms of bradykinin-induced contraction in human fetal lung fibroblasts.
CARNEVALI, Stefano;FABBRI, Leonardo;ROSSI, Giulio;
2010
Abstract
Bradykinin (BK) induces fibroblast contraction but the structural changes and intracellular mechanisms involved have not been completely explored.We stimulated HFL-1 fibroblasts with BK to assess: 1) fibroblast contractility; 2) the role of α-smooth muscle actin (SMA) in contraction by small interfering RNA (siRNA); 3) α-SMA protein expression; 4) α-SMA and F-actin structure; 5) intracellular calcium concentration ([Ca2+]i); and 6) phosphorylated myosin light-chain (pMLC) and MLC kinase (MLCK) expression.BK triggered concentration- and time-dependent fibroblast gel contraction in conjunction with α-SMA over expression, but not in α-SMA-siRNA-treated cells. BK also increased α-SMA+ and F-actin+ cell number and stress fibre polymerisation (detectable at 5–60 min). These BK-induced changes were associated with an increase in [Ca2+]i, which peaked within 15 s, and activation of pMLC, which was detectable at 5–60 min. No MLCK content modification was observed. The different manifestations of the BK-induced fibroblast activation were downregulated at different levels (25–100%) by HOE140, a specific BK B2 receptor (B2R) antagonist and by the Ca2+ chelator, EGTA.Thus, BK-induced fibroblast contraction, associated with differentiation into α-SMA+ myofibroblasts, is mediated through the activation of the B2R and involves the Ca2+/calmodulin pMLC-dependent pathway.File | Dimensione | Formato | |
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