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Differences between Cardiac and Skeletal Troponin Interaction with the Thin Filament Probed by Troponin Exchange in Skeletal Myofibrils

机译:骨骼肌肌纤维中肌钙蛋白交换探测到的细丝与心脏和骨骼肌钙蛋白相互作用的差异

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摘要

Troponin (Tn) is the calcium-sensing protein of the thin filament. Although cardiac troponin (cTn) and skeletal troponin (sTn) accomplish the same function, their subunit interactions within Tn and with actin-tropomyosin are different. To further characterize these differences, myofibril ATPase activity as a function of pCa and labeled Tn exchange in rigor myofibrils was used to estimate Tn dissociation rates from the nonoverlap and overlap region as a function of pCa. Measurement of ATPase activity showed that skeletal myofibrils containing >96% cTn had a higher pCa 9 ATPase activity than, but similar pCa 4 activity to, sTn-containing myofibrils. Analysis of the pCa–ATPase activity relation showed that cTn myofibrils were more calcium sensitive but less cooperative (pCa50 = 6.14, nH = 1.46) than sTn myofibrils (pCa50 = 5.90, nH = 3.36). The time course of labeled Tn exchange at pCa 9 and 4 were quite different between cTn and sTn. The apparent cTn dissociation rates were ∼2–10-fold faster than sTn under all the conditions studied. The apparent dissociation rates for cTn were 5 × 10−3 min−1, 150 × 10−3 min−1, and 260 × 10−3 min−1, whereas for sTn they were 0.6 × 10−3 min−1, 88 × 10−3 min−1, and 68 × 10−3 min−1 for the nonoverlap region at pCa 9, nonoverlap region at pCa 4, and overlap region at pCa 4, respectively. Normalization of the apparent dissociation rates gives 1:30:50 for cTn compared with 1:150:110 for sTn (nonoverlap at pCa 9:nonoverlap at pCa 4:overlap at pCa 4) suggesting that calcium has a smaller influence, whereas strong cross-bridges have a larger influence on cTn dissociation compared with sTn. The higher cTn dissociation rate in the nonoverlap region and ATPase activity at pCa 9 suggest that it gives a less off or inactive thin filament. Analysis of the intensity ratio (after a short time of exchange) as a function of pCa showed that cTn had greater calcium sensitivity but lower cooperativity than sTn. In addition, the magnitude of the change in intensity ratio going from pCa 9 to 4 was less for cTn than sTn. These data suggest that the influence of calcium on cTn exchange is less than sTn even though calcium can activate ATPase activity to a similar extent in cTn compared with sTn myofibrils. This may be explained partially by cTn being less off or inactive at pCa 9. Modeling of the intensity profiles obtained after Tn exchange at pCa 5.8 suggest that the profiles are best explained by a model that includes a long-range cross-bridge effect that grades with distance from the rigor cross-bridge for both cTn and sTn.
机译:肌钙蛋白(Tn)是细丝的钙敏感蛋白。尽管心脏肌钙蛋白(cTn)和骨骼肌钙蛋白(sTn)实现相同的功能,但它们在Tn中以及与肌动蛋白原肌球蛋白的亚单位相互作用是不同的。为了进一步表征这些差异,将肌原纤维ATPase活性作为pCa的函数,并使用严格的肌原纤维中标记的Tn交换来估算非重叠和重叠区域的Tn解离率,其为pCa的函数。 ATPase活性的测量结果表明,含有> 96%cTn的骨骼肌原纤维比含有sTn的肌原纤维具有更高的pCa 9 ATPase活性,但其pCa 4活性却相似。对pCa-ATPase活性关系的分析表明,与sTn肌原纤维(pCa50 = 5.90,nH = 3.36)相比,cTn肌原纤维对钙的敏感性更高,但合作性较低(pCa50 = 6.14,nH = 1.46)。 cTn和sTn之间在pCa 9和4处标记Tn交换的时间过程有很大差异。在所有研究条件下,表观cTn的解离速率比sTn快约2-10倍。 cTn的表观解离速率为5×10 -3 min -1 ,150×10 -3 min -1 和260×10 -3 min -1 ,而对于sTn,它们是0.6×10 -3 min -1 ,88×10 -3 min -1 和68×10 -3 min -1 分别对应于pCa 9处的非重叠区域和pCa 4处的非重叠区域以及pCa 4处的重叠区域。表观解离速率的归一化为cTn为1:30:50,而sTn为1:150:110(pCa 9不重叠:pCa 4不重叠:pCa 4重叠)表明钙的影响较小,而交叉力强与sTn相比,桥对cTn解离的影响更大。非重叠区域较高的cTn解离速率和pCa 9处的ATPase活性表明,它产生的脱落少或无活性的细丝。强度比(短时间交换后)与pCa的关系分析表明,与sTn相比,cTn的钙敏感性更高,但协同性更低。另外,cTn的强度比从pCa 9变为4的变化幅度小于sTn。这些数据表明,钙对cTn交换的影响小于sTn,尽管与sTn肌原纤维相比,钙可以在cTn中激活ATPase活性。这可能是由于cTn在pCa 9处较少脱落或失活而部分解释的。对在pCa 5.8处Tn交换后获得的强度分布进行建模的模型表明,该分布最好由包含以下等级的长距离跨桥效应的模型解释:距cTn和sTn的严谨跨桥距离。

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