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遗传对I型胶原蛋白合成与降解的影响:骨转换遗传调控的进一步证据。

Genetic influences on type I collagen synthesis and degradation: further evidence for genetic regulation of bone turnover.

作者信息

Tokita A, Kelly P J, Nguyen T V, Qi J C, Morrison N A, Risteli L, Risteli J, Sambrook P N, Eisman J A

机构信息

Bone and Mineral Research Division, Garvan Institute of Medical Research, St. Vincent's Hospital, Sydney, New South Wales, Australia.

出版信息

J Clin Endocrinol Metab. 1994 Jun;78(6):1461-6. doi: 10.1210/jcem.78.6.8200950.

DOI:10.1210/jcem.78.6.8200950
PMID:8200950
Abstract

Circulating osteocalcin, a marker of bone formation, is under strong genetic influence, and this effect is related to the genetic influence on bone density. To examine genetic influences on bone turnover further, other markers of bone formation (serum carboxyterminal propeptide of type I procollagen, PICP), bone resorption (serum pyridinoline cross-linked carboxyterminal telopeptide of type I collagen, ICTP), and nonosseous connective tissue synthesis (serum aminoterminal propeptide of type III procollagen, PIIINP) were studied in 82 female twin pairs: 42 monozygotic (MZ) and 40 dizygotic (DZ) twin pairs (mean age, MZ; 48.4 yr; DZ; 45.6 yr). The intraclass correlation coefficients of MZ twin pairs, rMZ, for serum PICP (0.78) and serum ICTP (0.68) were significantly greater than the corresponding rDZ (0.31 and 0.36, respectively), but a genetic effect on serum PIIINP was not demonstrable. Within DZ twin pair differences in serum PICP predicted differences in lumbar spine bone density (r = -0.37); higher serum PICP levels indicating the twin with the lower lumbar spine bone density. Also within pair differences in serum ICTP and PICP predicted differences in bone density at the lumbar spine independent of serum osteocalcin. These data indicate that both synthesis and degradation of type I collagen are genetically determined and that this phenomenon is related to the genetic regulation of bone density.

摘要

循环骨钙素是骨形成的标志物,受强大的遗传影响,且这种影响与对骨密度的遗传影响相关。为了进一步研究对骨转换的遗传影响,对82对女性双胞胎进行了研究,检测了其他骨形成标志物(血清I型前胶原羧基末端前肽,PICP)、骨吸收标志物(血清I型胶原吡啶啉交联羧基末端肽,ICTP)和非骨结缔组织合成标志物(血清III型前胶原氨基末端前肽,PIIINP):42对同卵双胞胎(MZ)和40对异卵双胞胎(DZ)(平均年龄,MZ为48.4岁;DZ为45.6岁)。血清PICP(0.78)和血清ICTP(0.68)的MZ双胞胎对内类相关系数rMZ显著高于相应的rDZ(分别为0.31和0.36),但未显示出对血清PIIINP的遗传影响。在DZ双胞胎对中,血清PICP的差异预测了腰椎骨密度的差异(r = -0.37);血清PICP水平较高表明该双胞胎腰椎骨密度较低。同样,血清ICTP和PICP的双胞胎对内差异也预测了独立于血清骨钙素的腰椎骨密度差异。这些数据表明I型胶原的合成和降解均由遗传决定,且这一现象与骨密度的遗传调控有关。

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