Villareal D T, Morley J E
Geriatric Research Education and Clinical Center, St Louis Veterans Administration Medical Center, Missouri.
Drugs Aging. 1994 Jun;4(6):492-509. doi: 10.2165/00002512-199404060-00005.
The aging process is associated with significant declines in the levels of many hormones and trophic factors including estrogen, testosterone, growth hormone (somatropin, somatotropin) and insulin-like growth factor-1 (IGF-1, somatomedin-1, somatomedin-C). Since the classic age-related changes resemble the signs and symptoms of endocrine deficiency, it has been hypothesised that some of the negative effects of aging are due to these hormonal deficits. Consequently, the potential role of hormonal replacement in reversing the deleterious effects of aging deserves investigation. In old hypogonadal men, preliminary studies have shown that testosterone replacement not only improves libido but also significantly increases musculoskeletal mass and strength. However, adverse effects have included increases in haematocrit and prostate specific antigen. Similarly, short term studies with growth hormone replacement have shown substantial bodyweight gain, particularly in severely malnourished older adults, but longer studies have been limited by adverse effects such as gynaecomastia and carpal tunnel syndrome in a few people. Thus, though both testosterone and growth hormone may have potential roles for frailty syndromes in the elderly, long term clinical trials are needed to confirm these positive effects and assess their safety. On the other hand, the multiple beneficial effects of estrogen replacement in older women such as relieving acute menopausal symptoms and preventing postmenopausal osteoporosis are well recognised. Observational studies also suggest that estrogen may decrease cardiovascular disease. However, the optimum duration of treatment and the best way to administer this hormone are still unknown. Also, estrogen may be less effective in senile osteoporosis which primarily results from age-related bone loss. Traditionally, age-related bone loss has been attributed to impaired vitamin D activation and decreased calcium absorption. Thus, it was thought that such bone losses may be ameliorated by calcium supplementation. However, recent studies suggest that alterations in local factors affecting bone cell function may also be important in the pathogenesis of osteoporosis. An increase in potent bone resorbing factors, such as the cytokines interleukin-1 and interleukin-6, has been recently demonstrated in elderly patients with osteoporosis. In these patients, it has been suggested that there may also be a decrease in bone growth factors such as IGF-1 and transforming growth factor-beta. Accordingly, studies are underway to determine whether these factors may be useful in the prevention of osteoporosis. Other growth factors recently identified which may be important in aging include epidermal growth factor, nerve growth factor and fibroblast growth factor.(ABSTRACT TRUNCATED AT 400 WORDS)
衰老过程与许多激素和营养因子水平的显著下降有关,这些激素和营养因子包括雌激素、睾酮、生长激素(促生长素、生长激素)和胰岛素样生长因子-1(IGF-1、生长调节素-1、生长调节素-C)。由于典型的与年龄相关的变化类似于内分泌缺乏的体征和症状,因此有人提出衰老的一些负面影响是由于这些激素缺乏所致。因此,激素替代在逆转衰老有害影响方面的潜在作用值得研究。在老年性腺功能减退男性中,初步研究表明,睾酮替代不仅能改善性欲,还能显著增加肌肉骨骼质量和力量。然而,不良反应包括血细胞比容和前列腺特异性抗原升高。同样,生长激素替代的短期研究显示体重显著增加,尤其是在严重营养不良的老年人中,但长期研究受到少数人出现男性乳房发育和腕管综合征等不良反应的限制。因此,尽管睾酮和生长激素可能对老年人的衰弱综合征有潜在作用,但需要长期临床试验来证实这些积极作用并评估其安全性。另一方面,雌激素替代对老年女性的多种有益作用,如缓解急性更年期症状和预防绝经后骨质疏松症,已得到充分认可。观察性研究还表明,雌激素可能会降低心血管疾病的风险。然而,最佳治疗持续时间和使用这种激素的最佳方法仍然未知。此外,雌激素对主要由年龄相关骨质流失引起的老年性骨质疏松症可能效果较差。传统上,年龄相关骨质流失归因于维生素D活化受损和钙吸收减少。因此,人们认为补充钙可能会改善这种骨质流失。然而,最近的研究表明,影响骨细胞功能的局部因素的改变在骨质疏松症的发病机制中也可能很重要。最近在老年骨质疏松症患者中已证实,诸如细胞因子白细胞介素-1和白细胞介素-6等强效骨吸收因子增加。在这些患者中,有人提出骨生长因子如IGF-1和转化生长因子-β也可能减少。因此,正在进行研究以确定这些因子是否可用于预防骨质疏松症。最近发现的其他可能在衰老过程中起重要作用的生长因子包括表皮生长因子、神经生长因子和成纤维细胞生长因子。(摘要截取自400字)
