Malik N A, Anantharamaiah G M, Gawish A, Cheung H C
Biochim Biophys Acta. 1987 Jan 30;911(2):221-30. doi: 10.1016/0167-4838(87)90011-2.
We have synthesized four oligopeptides that are structural analogues of a low-affinity Ca2+-specific binding site (site II) of rabbit skeletal troponin C. One analogue (peptide 3) was a dodecapeptide with a sequence corresponding to the 12-residue Ca2+-binding loop (residues 63-74 in troponin C), two (peptides 4 and 5) were 23-residue in length, corresponding to residues 52-74 of the protein, and the fourth (peptide 6) was a 25-residue peptide corresponding to residues 50-74. All four peptides had one amino acid substitution within the 12-residue binding loop in which phenylalanine at position 10 was replaced by tyrosine to provide a marker for spectroscopic studies. In addition, peptides 3 and 4 each had a second substitution within the binding loop where glycine at position 6 was replaced by alanine. The second substitution was motivated by the conservation of glycine at the position in the Ca2+-binding loops of all four Ca2+-binding sites in troponin C. The peptides were characterized by their intrinsic fluorescence, ability to enhance the emission of bound Tb3+, affinity for Ca2+ and Tb3+, and circular dichroism. The affinity for Ca2+ was in the range 10-10(2) M-1, and the affinity for Tb3+ was in the range 10(4)-10(5) M-1. The binding constants of the longer peptides were several-fold larger than that of the dodecapeptide. With peptides 4 and 5, substitution of glycine by alanine at position 6 within the 12-residue loop decreased the affinity for Ca2+ by a factor of four, but had little effect on the affinity for Tb3+. However, the mean residue ellipticity of peptide 4 was substantially higher than that of peptide 5. Since peptide 4 differs from peptide 5 only in the substitution of glycine at position 6 in the loop segment, the conservation of glycine at that position may serve a role in providing a suitable secondary structure of the binding sites for interaction with troponin I. Peptides 4 and 6, when present in a large excess, mimic troponin C in regulating fully reconstituted actomyosin ATPase by showing partial calcium sensitivity and activation of the ATPase. Since these peptides are the smallest peptides containing the Ca2+-binding loop of site II, their biological activity suggests that a Ca2+-dependent binding site of troponin C for troponin I could be as short as the segment comprising residues 52-62.
我们合成了四种寡肽,它们是兔骨骼肌肌钙蛋白C低亲和力Ca2+特异性结合位点(位点II)的结构类似物。一种类似物(肽3)是十二肽,其序列对应于12个残基的Ca2+结合环(肌钙蛋白C中的63 - 74位残基),另外两种(肽4和肽5)长度为23个残基,对应于该蛋白的52 - 74位残基,第四种(肽6)是25个残基的肽,对应于50 - 74位残基。所有四种肽在12个残基的结合环内都有一个氨基酸取代,其中10位的苯丙氨酸被酪氨酸取代,以提供用于光谱研究的标记。此外,肽3和肽4在结合环内各自还有第二个取代,即6位的甘氨酸被丙氨酸取代。第二个取代的依据是肌钙蛋白C所有四个Ca2+结合位点的Ca2+结合环中该位置甘氨酸的保守性。通过它们的固有荧光、增强结合的Tb3+发射的能力、对Ca2+和Tb3+的亲和力以及圆二色性对这些肽进行了表征。对Ca2+的亲和力在10 - 10(2) M-1范围内,对Tb3+的亲和力在10(4) - 10(5) M-1范围内。较长肽的结合常数比较短的十二肽大几倍。对于肽4和肽5,在12个残基环内6位的甘氨酸被丙氨酸取代使对Ca2+的亲和力降低了四倍,但对Tb3+的亲和力影响很小。然而,肽4的平均残基椭圆率明显高于肽5。由于肽4与肽5的区别仅在于环段中6位甘氨酸的取代,该位置甘氨酸的保守性可能在为与肌钙蛋白I相互作用提供合适的结合位点二级结构方面发挥作用。当大量存在时,肽4和肽6通过表现出部分钙敏感性和ATP酶的激活来模拟肌钙蛋白C对完全重组的肌动球蛋白ATP酶的调节。由于这些肽是包含位点II的Ca2+结合环的最小肽,它们的生物活性表明肌钙蛋白C与肌钙蛋白I的Ca2+依赖性结合位点可能短至包含52 - 62位残基的片段。
