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首页> 外文期刊>Psychosomatic Medicine: Journal of the American Psychosomatic Society >Bone mineral density, bone turnover, and osteoprotegerin in depressed women with and without borderline personality disorder.
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Bone mineral density, bone turnover, and osteoprotegerin in depressed women with and without borderline personality disorder.

机译:患有和不患有边缘性人格障碍的抑郁症妇女的骨矿物质密度,骨转换和骨保护素。

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OBJECTIVE: Low bone mineral density has repeatedly been reported in patients with major depressive disorder (MDD), and MDD has been discussed as a risk factor for the development of osteoporosis. MDD in young adults often occurs in the context of borderline personality disorder (BPD), and both MDD and BPD have been associated with a dysregulation of the hypothalamic-pituitary-adrenal system and subsequent hypercortisolemia. To date, it is unclear whether comorbid BPD in depressed patients modulates the extent of bone mass reduction. Therefore, we examined bone density, markers of bone turnover, and proinflammatory cytokines in depressed patients with and without BPD. Patients with BPD alone and healthy women served as comparison groups. METHOD: Twenty-four patients with MDD and 23 patients with comorbid MDD and BPD were included. Sixteen patients with BPD and 20 healthy women of similar body mass index served as the comparison group. BMD was assessed by means of dual-energy x-ray absorptiometry. Markers of bone turnover, endocrine and immune parameters were determined. For data analysis, the group of depressed patients without comorbid BPD was divided according to age into two groups (younger depressed patients with a mean age of 30 years and older patients with a mean age of 42.9 years). RESULTS: BMD at the lumbar spine was significantly reduced in a) depressed women with comorbid BPD (mean age, 28.6 years) and in b) older depressed patients without BPD (mean age, 42.9 years). Osteocalcin, a marker of osteoblastic activity, and crosslaps, a marker of bone loss, were significantly different between the study groups. Tumor necrosis factor-alpha was increased in depressed patients when compared with healthy women. Furthermore, TNF-alpha was positively correlated with serum crosslaps, a marker for osteoclastic activity. CONCLUSION: Depression is associated with reduced bone mass, in particular in patients with comorbid BPD. Possible factors contributing to BMD reduction include endocrine and immune alterations associated with either MDD or BPD. We conclude from our data that a history of MDD with and without comorbid BPD should be considered as a risk factor in clinical assessment instruments for the identification of persons prone to osteoporosis.
机译:目的:重度抑郁症(MDD)患者中反复出现低骨矿物质密度的报道,MDD被认为是骨质疏松症发展的危险因素。年轻人的MDD通常发生在边缘性人格障碍(BPD)的背景下,并且MDD和BPD都与下丘脑-垂体-肾上腺系统的失调和随后的高皮质醇血症相关。迄今为止,尚不清楚抑郁症患者的合并BPD是否调节骨量减少的程度。因此,我们检查了患有和不患有BPD的抑郁症患者的骨密度,骨转换标志物和促炎细胞因子。仅BPD患者和健康女性作为比较组。方法:纳入24例MDD患者和23例合并MDD和BPD患者。对照组为16例BPD患者和20例体重指数相似的健康女性。 BMD通过双能X射线吸收法评估。确定了骨转换,内分泌和免疫参数的标志。为了进行数据分析,将没有合并BPD的抑郁症患者按年龄分为两组(平均年龄为30岁的年轻抑郁症患者和平均年龄为42.9岁的老年患者)。结果:a)合并BPD的抑郁症妇女(平均年龄28.6岁)和b)没有BPD的抑郁症老年患者(平均年龄42.9岁)显着降低了腰椎的BMD。在研究组之间,骨钙素是成骨细胞活性的标志,而骨交叉是骨丢失的标志。与健康女性相比,抑郁症患者的肿瘤坏死因子-α升高。此外,TNF-α与破骨细胞活性标志物血清交叉重叠呈正相关。结论:抑郁症与骨量减少有关,尤其是合并BPD的患者。导致BMD降低的可能因素包括与MDD或BPD相关的内分泌和免疫改变。从我们的数据可以得出结论,有或没有合并BPD的MDD病史在临床评估工具中应被视为危险因素,以鉴定容易患骨质疏松症的人。

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