Johansson L, Grubb A, Abrahamson M, Kasprzykowski F, Kasprzykowska R, Grzonka Z, Lerner U H
Department of Oral Cell Biology, Umeå University, Umeå, Sweden.
Bone. 2000 May;26(5):451-9. doi: 10.1016/S8756-3282(00)00261-1.
Human cystatin C is a cysteine proteinase inhibitor belonging to the cystatin superfamily, which previously has been shown to inhibit bone resorption in bone organ culture. The aminoterminal segment, Arg(8)-Leu(9)-Val(10)-Gly(11) (RLVG), of the single polypeptide chain of cystatin C constitutes an essential part of its inhibitory center. In the present study, the effect of benzyloxycarbonyl-Arg(8)-Leu(9)-Val(10)-Gly(11)-diazomethane (Z-RLVG-CHN(2)) on bone resorption in vitro was compared with the effects of cystatin C and calcitonin. Bone resorption was assessed by the release of (45)Ca and (3)H from mouse calvarial bones prelabeled with [(45)Ca]CaCl(2) and [(3)H]-proline, respectively. Z-RLVG-CHN(2) concentration-dependently inhibited the release of (45)Ca and (3)H in bones stimulated by parathyroid hormone (PTH), with half-maximal inhibition obtained at 1 micromol/L. The inhibitory actions of Z-RLVG-CHN(2) and cystatin C were persistent, whereas action induced initially by calcitonin was lost with time. The inhibition caused by Z-RLVG-CHN(2) and cystatin C on PTH-stimulated (45)Ca release was observed after 6 h, whereas inhibition by calcitonin was seen already after 2 h. In contrast, the inhibitory effects of Z-RLVG-CHN(2) and cystatin C, as well as that of calcitonin, on (3)H release was seen already after 2 h. Z-RLVG-CHN(2), in which the reactive carboxyterminal diazomethane was substituted by nonreactive groups [-OH, -NH(2), or -N(CH(3))(2)], resulted in peptidyl derivatives, which, in contrast to Z-RLVG-CHN(2) and cystatin C, inhibited neither cysteine proteinases nor bone resorption. In contrast to wild-type cystatin C, recombinant human cystatin C with Gly substitutions for residues Arg(8), Leu(9), Val(10), and Trp(106), and with low or nonexistent affinity for cysteine proteinases, did not display any inhibitory effect on bone resorption. These data strongly indicate that Z-RLVG-CHN(2) inhibits bone resorption in vitro by a mechanism that seems primarily to be due to an inhibition of bone matrix degradation via cysteine proteinases. The data also corroborate the hypothesis that cystatin C inhibits bone resorption by virtue of its cysteine proteinase inhibitory capacity.
人胱抑素C是一种属于胱抑素超家族的半胱氨酸蛋白酶抑制剂,此前已证明它能抑制骨器官培养中的骨吸收。胱抑素C单条多肽链的氨基末端片段Arg(8)-Leu(9)-Val(10)-Gly(11)(RLVG)构成其抑制中心的重要部分。在本研究中,将苄氧羰基-Arg(8)-Leu(9)-Val(10)-Gly(11)-重氮甲烷(Z-RLVG-CHN₂)对体外骨吸收的作用与胱抑素C和降钙素的作用进行了比较。分别用[(⁴⁵)Ca]CaCl₂和[(³)H]-脯氨酸预标记小鼠颅骨,通过(⁴⁵)Ca和(³)H的释放来评估骨吸收。Z-RLVG-CHN₂浓度依赖性地抑制甲状旁腺激素(PTH)刺激的骨中(⁴⁵)Ca和(³)H的释放,在1 μmol/L时达到半数最大抑制。Z-RLVG-CHN₂和胱抑素C的抑制作用持续存在,而降钙素最初诱导的作用随时间消失。Z-RLVG-CHN₂和胱抑素C对PTH刺激的(⁴⁵)Ca释放的抑制在6小时后观察到,而降钙素的抑制在2小时后就已出现。相比之下,Z-RLVG-CHN₂、胱抑素C以及降钙素对(³)H释放的抑制在2小时后就已出现。Z-RLVG-CHN₂中反应性的羧基末端重氮甲烷被非反应性基团[-OH、-NH₂或-N(CH₃)₂]取代后,得到的肽基衍生物与Z-RLVG-CHN₂和胱抑素C不同,既不抑制半胱氨酸蛋白酶也不抑制骨吸收。与野生型胱抑素C相反,将Arg(8)、Leu(9)、Val(10)和Trp(106)残基替换为甘氨酸且对半胱氨酸蛋白酶亲和力低或不存在的重组人胱抑素C,对骨吸收没有任何抑制作用。这些数据有力地表明,Z-RLVG-CHN₂在体外通过一种似乎主要是由于抑制半胱氨酸蛋白酶介导的骨基质降解的机制来抑制骨吸收。这些数据也证实了胱抑素C凭借其半胱氨酸蛋白酶抑制能力抑制骨吸收的假说。
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