Mechanisms Mediating the Alcohol-Induced Reduction in Peak Bone Mass

介导酒精引起的峰值骨量减少的机制

• 批准号: 7509517
• 负责人: Kathleen Howe
• 金额: $ 4.8万
• 依托单位: OREGON STATE UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2007
• 资助国家: 美国
• 起止时间: 2007-09-15 至 2010-09-14
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7509517
• 关键词: Adolescence; Adolescent; Adult; Affect; Age; Alcohol abuse; Alcohol consumption; Alcoholism; Alcohols; Animals; Behavior; Biochemical; Bone Growth; Bone Matrix; Bone Resorption; Bone remodeling; Cells; Chronic; Coupling; Defect; Deposition; Dose; Equilibrium; Fracture; Future; Goals; Growth Factor; Growth Hormone Receptor; Human; Impairment; In Vitro; Individual; Insulin-Like Growth Factor I; Intervention; Laboratories; Lead; Life; Long-Term Effects; Male Adolescents; Measures; Mechanics; Mediating; Molecular; Nodule; Osteoblasts; Osteoclasts; Osteogenesis; Osteoporosis; Pathway interactions; Phase; Play; Property; Rattus; Research; Risk Factors; Role; Signal Transduction; Skeletal system; Skeleton; Somatomedins; Somatotropin; Staging; Testing; alcohol effect; autocrine; binge drinking; bone; bone growth factor; bone healing; bone loss; bone metabolism; bone quality; drinking behavior; in vivo; male; novel; paracrine; receptor; response

DESCRIPTION (provided by applicant): Chronic alcohol abuse results in bone loss and, should a fracture occur, impaired bone healing. Studies in the Turner (sponsor) laboratory suggest that the detrimental effects of alcohol on bone in adult rats are due, in part, to disturbed growth hormone (GH) signaling. In addition to its direct bone anabolic effects, GH mediates the deposition of the important osteoblast growth factor, insulin-like growth factor-l (IGF-I), into bone matrix. The release of IGF-I from the matrix by the action of osteoclasts, in turn, plays a critical role in coupling of bone formation to bone resorption during bone remodeling. In the adult, GH helps maintain bone mass and quality by regulating the balance between bone formation and resorption. GH plays an additional role in the growing skeleton by regulating the net acquisition of bone. Alcohol consumption, especially binge drinking, is very common in adolescents. Although this behavior is generally transient and does not lead to alcoholism, it nevertheless can have undesirable long-term consequences to the skeleton. The long-term goal of the Turner laboratory is to identify pathways mediating skeletal effects of alcohol abuse. The goal of my postdoctoral research is to test the hypothesis that alcohol impairs GH signaling in osteoblasts. This hypothesis will be tested in vitro using human osteoblasts (hFOB cells) and in vivo in male adolescent rats. The specific aims of the proposed research are to: Specific Aim 1: Determine the dose response effects of alcohol on GH-mediated increases in proliferation, differentiation, IGF-I synthesis and nodule formation by hFOB cells. These studies will test the hypothesis that alcohol has a direct inhibitory effect on the bone anabolic response to GH. The results will set the stage for future studies directed toward uncovering the detailed molecular mechanism(s) by which alcohol inhibits GH signaling. Specific Aim 2: Measure the effects of binge drinking on GH-mediated stimulation of osteoblast differentiation and activity in GH-deficient hypophysectomized adolescent rats. These studies will test the hypothesis that adolescent rats are very sensitive to the inhibitory effects of alcohol on bone formation because of their requirement for high levels of GH. Specific Aim 3: Determine the long-duration effects of chronic adolescent binge drinking on peak bone mass, IGF-I levels in bone matrix, bone mechanical properties and turnover. These studies will test the hypothesis that chronic binge drinking reduces the content of IGF-I in bone matrix which, in turn, is associated with impairment of bone remodeling and bone quality even after alcohol is withdrawn. These novel studies will critically evaluate the role of disturbed GH in mediating the detrimental effects of alcohol on bone growth and will critically test a plausible mechanism for alcohol-impaired bone remodeling.

描述（由申请人提供）：慢性酒精滥用导致骨质流失，如果发生骨折，则会损害骨愈合。Turner（申办方）实验室的研究表明，酒精对成年大鼠骨骼的有害影响部分是由于生长激素（GH）信号传导紊乱。除了其直接的骨合成代谢作用外，GH还介导重要的成骨细胞生长因子胰岛素样生长因子-I（IGF-I）沉积到骨基质中。通过破骨细胞的作用从基质中释放IGF-I，反过来，在骨重建过程中骨形成与骨吸收的偶联中起关键作用。在成年人中，生长激素通过调节骨形成和骨吸收之间的平衡来帮助维持骨量和骨质量。生长激素通过调节骨的净获得在骨骼生长中起着额外的作用。饮酒，尤其是酗酒，在青少年中非常普遍。虽然这种行为通常是短暂的，不会导致酒精中毒，但它仍然会对骨骼产生不良的长期后果。特纳实验室的长期目标是确定酒精滥用对骨骼影响的介导途径。我的博士后研究的目标是测试酒精损害成骨细胞中GH信号传导的假设。将使用人成骨细胞（hFOB细胞）在体外和雄性青春期大鼠体内对这一假设进行测试。 具体目标1：确定酒精对GH介导的hFOB细胞增殖、分化、IGF-I合成和结节形成增加的剂量反应效应。这些研究将检验酒精对GH的骨合成代谢反应具有直接抑制作用的假设。这些结果将为未来的研究奠定基础，旨在揭示酒精抑制GH信号传导的详细分子机制。具体目标二：在生长激素缺乏的垂体切除的青春期大鼠中测量狂饮对生长激素介导的成骨细胞分化和活性的刺激的影响。这些研究将验证这样一个假设，即青春期大鼠对酒精对骨形成的抑制作用非常敏感，因为它们需要高水平的GH。具体目标3：确定慢性青少年酗酒对峰值骨量、骨基质中IGF-I水平、骨机械性能和转换的长期影响。这些研究将检验这样的假设，即慢性酗酒降低了骨基质中IGF-I的含量，这反过来又与骨重建和骨质量的损害有关，即使在戒酒后也是如此。这些新的研究将严格评估干扰生长激素在介导酒精对骨生长的有害影响中的作用，并将严格测试酒精受损骨重建的合理机制。