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胶原酶、前胶原酶与骨吸收。肝素、甲状旁腺激素及降钙素的作用。

Collagenase, procollagenase and bone resorption. Effects of heparin, parathyroid hormone and calcitonin.

作者信息

Lenaers-Claeys G, Vaes G

出版信息

Biochim Biophys Acta. 1979 May 16;584(3):375-88. doi: 10.1016/0304-4165(79)90114-4.

Abstract
  1. The addition of heparin to the culture fluid of mouse tibiae or calvaria did not cause any significant resorption of bone collagen or mineral. However, heparin (or analogue sulfated polyanions), enhanced greatly the amount of latent, trypsin-activatable collagenase (i.e. procollagenase) released by the bones in the medium without influencing that of directly active collagenase which was always very low. Heparin appeared to act by increasing the production of the enzyme which is immediately excreted. Procollagenase and collagenase are not stored in bone tissue, even under conditions where it is in active resorption. 2. Parathyroid hormone induced in the explants a resorption of both mineral and collagen that was inhibited by calcitonin. These hormones, however, had no influence on the release of procollagenase or collagenase either in the presence or in the absence of heparin. 3. Once activated, bone collagenase digested the collagen of the bone explants, and more extensively after their demineralization. Thus the latent collagenase that accumulates around non-resorbing bones has to be considered as a precursor, (and not as a residue), of active enzyme. 4. Active collagenase added to incipient cultures of bones disappeared with a half-life of 24 h. The lost enzyme could, however, not be reactivated by trypsin and thus was not transformed into latent procollagenase.
摘要
  1. 向小鼠胫骨或颅骨的培养液中添加肝素,并未引起骨胶原或矿物质的任何显著吸收。然而,肝素(或类似的硫酸化聚阴离子)极大地增加了骨骼在培养基中释放的潜在的、可被胰蛋白酶激活的胶原酶(即前胶原酶)的量,而不影响一直很低的直接活性胶原酶的量。肝素似乎是通过增加立即分泌的酶的产生来起作用的。前胶原酶和胶原酶并不储存在骨组织中,即使在骨组织处于活跃吸收的情况下也是如此。2. 甲状旁腺激素在外植体中诱导了矿物质和胶原的吸收,而这种吸收被降钙素所抑制。然而,这些激素在有或没有肝素的情况下,对前胶原酶或胶原酶的释放均无影响。3. 一旦被激活,骨胶原酶就会消化骨外植体的胶原,脱矿后消化得更广泛。因此,必须将在非吸收性骨周围积累的潜在胶原酶视为活性酶的前体(而不是残余物)。4. 添加到骨起始培养物中的活性胶原酶以24小时的半衰期消失。然而,丢失的酶不能被胰蛋白酶重新激活,因此不会转化为潜在的前胶原酶。

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