Firestone Institute for Respiratory Health, St. Joseph's Hospital, Hamilton, Ontario, Canada.
Am J Respir Cell Mol Biol. 2011 Feb;44(2):213-21. doi: 10.1165/rcmb.2009-0259OC. Epub 2010 Apr 15.
Despite the emerging use of bronchial thermoplasty in asthma therapy, the response of airway smooth muscle (ASM) to extreme temperatures is unknown. We investigated the immediate effects of exposing ASM to supraphysiologic temperatures. Isometric contractions were studied in bovine ASM before and after exposure to various thermal loads and/or pharmacologic interventions. Actin-myosin interactions were investigated using a standard in vitro motility assay. We found steep thermal sensitivity for isometric contractions evoked by acetylcholine, with threshold and complete inhibition at less than 50°C and greater than 55°C, respectively. Contractile responses to serotonin or KCl were similarly affected, whereas isometric relaxations evoked by the nitric oxide donor S-nitrosyl-N-acetylpenicillamine or the β-agonist isoproterenol were unaffected. This thermal sensitivity developed within 15 minutes, but did not evolve further over the course of several days (such a rapid time-course rules out heat shock proteins, apoptosis, autophagy, and necrosis). Although heat-sensitive transient receptor potential (TRPV2) channels and the calmodulin-dependent (Cam) kinase-II-induced inactivation of myosin light chain kinase are both acutely thermally sensitive, with a temperature producing half-maximal effect (T(1/2)) of 52.5°C, the phenomenon we describe was not prevented by blockers of TRPV2 channels (e.g., ruthenium red, gadolinium, zero-Ca(2+) or zero-Na(+)/zero-Ca(2+) media, and cromakalim) or of Cam kinase-II (e.g., W7, trifluoperazine, and KN-93). However, direct measurements of actin-myosin interactions showed the same steep thermal profile. The functional changes preceded any histologic evidence of necrosis or apoptosis. We conclude that extreme temperatures (such as those used in bronchial thermoplasty) directly disrupt actin-myosin interactions, likely through a denaturation of the motor protein, leading to an immediate loss of ASM cell function.
尽管支气管热成形术在哮喘治疗中的应用日益增多,但气道平滑肌(ASM)对极端温度的反应仍不清楚。我们研究了将 ASM 暴露于超生理温度下的即时效应。在暴露于各种热负荷和/或药物干预之前和之后,研究了牛 ASM 的等长收缩。使用标准的体外运动测定法研究了肌动球蛋白相互作用。我们发现乙酰胆碱引起的等长收缩对温度非常敏感,阈值和完全抑制分别发生在低于 50°C 和高于 55°C。对 5-羟色胺或 KCl 的收缩反应也受到类似的影响,而一氧化氮供体 S-亚硝基-N-乙酰青霉胺或 β-激动剂异丙肾上腺素引起的等长松弛不受影响。这种热敏感性在 15 分钟内发展,但在数天内没有进一步发展(如此快速的时程排除了热休克蛋白、细胞凋亡、自噬和坏死)。尽管热敏瞬时受体电位(TRPV2)通道和钙调蛋白依赖性(Cam)激酶-II 诱导的肌球蛋白轻链激酶失活均对热敏感,产生半最大效应(T(1/2))的温度为 52.5°C,但我们描述的现象不能被 TRPV2 通道(如钌红、钆、零-Ca(2+)或零-Na(+)/零-Ca(2+)介质和克罗卡林)或 Cam 激酶-II(如 W7、三氟哌嗪和 KN-93)的阻断剂阻止。然而,肌动球蛋白相互作用的直接测量显示出相同的陡峭热曲线。功能变化先于任何坏死或凋亡的组织学证据。我们得出结论,极端温度(如支气管热成形术中使用的温度)直接破坏肌动球蛋白相互作用,可能通过使运动蛋白变性,导致 ASM 细胞功能的立即丧失。
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