高剂量胆钙化醇和膳食钙对抗逆转录病毒治疗后HIV患者骨量保存的影响。这可能吗?

Q2 Medicine
HIV Clinical Trials Pub Date : 2018-10-01 Epub Date: 2018-11-16 DOI:10.1080/15284336.2018.1525841
Quirico Mela, Valeria Ruggiero, Lorenza Montaldo, Umberto Pisano, Laura Matta, Cristina Maria Pasetto, Simona Onali, Enrico Cacace, Mauro Giovanni Carta, Lucia Barca, Luchino Chessa
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引用次数: 4

摘要

目的:评价采用不同cART方案的HIV患者在接受10万IU/月(相当于3200 IU/天)的胆钙化醇和1 g/天的膳食补钙治疗后,维生素D3和甲状旁腺激素水平是否正常,以及骨密度的变化是否具有临床意义。方法:连续接受不同cART方案的HIV患者接受10万IU/月(相当于3200 IU/天)的胆钙化醇和1 g/天的膳食钙补充。参与者在基线(T0)和24个月后(T1)通过脊柱和髋关节双能x线吸收仪进行骨密度评估。在T0和T1时测定25(OH)、维生素D3和甲状旁腺激素(PTH)水平。定量变量评估采用配对t检验、独立t检验或方差分析,视情况而定。采用卡方分析来评估定性变量之间的相关性。p值结果:共纳入79例患者(男性40例,占51%,女性39例,占49%),平均年龄46.6 (SD±11.2)岁,基线CD4细胞计数649个/µl,平均25羟基胆钙化醇(25(OH) D3) 25 + 10 ng/ml。24个月后,25(OH) D3升高至40 + 11 ng/ml。T0时脊柱和髋部的初始bmd分别为0.919(±0.27)和0.867(±0.14)g/cm2。24个月后,脊柱骨密度为0.933(±0.15)g/cm2,髋部骨密度为0.857(±0.14)g/cm2。在骨密度变化超过3%的情况下,23%的脊柱患者和27%的髋部患者出现恶化,77%的脊柱患者和73%的髋部患者表现出稳定或改善。基于抗逆转录病毒治疗的患者亚组表明,在T1时,所有患者的维生素D3浓度均有统计学意义的增加,而服用替诺福韦或依非韦伦的患者的PTH浓度未显着降低。24个月后,77%的脊柱患者和73%的髋部患者的骨密度稳定或改善。多变量分析证实,吸烟者维生素D3水平下降,甲状旁腺激素水平升高,男性维生素D3浓度升高,绝经期女性脊柱骨密度降低。结论:建议的胆骨化醇和膳食钙补充方案对纠正几乎所有患者的维生素D异常以及降低高比例患者的PTH水平是安全有效的;然而,这并不足以使其恢复正常,特别是对于那些暴露于替诺福韦或依非韦伦的患者。在脊柱方面,任何治疗组均未发现明显的骨密度变化。在髋部,我们的数据证实替诺福韦和依非韦伦对骨量有适度的负面影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Bone mass preservation with high-dose cholecalciferol and dietary calcium in HIV patients following antiretroviral therapy. Is it possible?

Objective: To evaluate whether treatment with 100,000 IU/month (equivalent to 3200 IU/day) of cholecalciferol and 1 g/day of dietary calcium supplementation in HIV patients following different cART regimens yields normal levels of vitamin D3 and PTH as well as whether changes in bone mineral density are clinically significant.

Methods: Consecutive HIV patients following different cART regimens received 100,000 IU/month (equivalent to 3200 IU/day) of cholecalciferol and 1 g/day of dietary calcium supplementation. The participants underwent BMD assessment via dual energy X-ray absorptiometry of the spine and hip at baseline (T0) and after 24 months (T1). Levels of 25(OH) vitamin D3 and parathyroid hormone (PTH) were assessed at T0 and T1. Quantitative variables were assessed with a paired t-test, independent t-test or analysis of variance, as appropriate. A chi-squared analysis was used to assess the association between qualitative variables. A p-value <0.05 was considered significant. Patients were divided into three groups depending on the cART regimen.

Results: A total of 79 patients were included (40 males, 51% and 39 females, 49%), with a mean age of 46.6 (SD ±11.2) years, a baseline CD4 count of 649 cells/µl and a mean 25 hydroxycholecalciferol (25(OH) D3) value of 25 + 10 ng/ml. After 24 months, the 25(OH) D3 increased to 40 + 11 ng/ml. The initial BMDs at T0 were estimated as 0.919 (±0.27) and 0.867 (±0.14) g/cm2 at the spine and hip, respectively. After 24 months, the BMD was 0.933 (±0.15) g/cm2 at the spine and 0.857 (±0.14) g/cm2 at the hip. Based on a BMD change exceeding 3%, a worsening was observed in 23% of patients at the spine and 27% at the hip, whereas stability or improvement was demonstrated in 77% of patients at the spine and 73% at the hip. Subgrouping patients based on antiretroviral therapy indicated that, at T1, there was a statistically significant increase in vitamin D3 concentration in all patients, while PTH concentration was not significantly reduced in patients taking tenofovir or efavirenz. BMD stability or improvement was demonstrated in 77% of patients at the spine and 73% at the hip after 24 months. The multivariate analysis confirms a decrease in vitamin D3 and an increase in PTH levels in smokers, as well higher vitamin D3 concentrations in males and lower spine BMDs in menopausal females.

Conclusion: The proposed protocol of cholecalciferol and dietary calcium supplementation is safe and valid for correcting vitamin D abnormalities in almost all patients as well as reducing PTH levels in a high percentage of patients; however, it is not sufficient for normalization, particularly in patients exposed to tenofovir or efavirenz. At the spine, no significant BMD change was found in any of the therapy groups. At the hip, our data confirm a modest negative effect on bone mass caused by tenofovir and efavirenz.

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来源期刊
HIV Clinical Trials
HIV Clinical Trials 医学-传染病学
CiteScore
1.76
自引率
0.00%
发文量
0
审稿时长
>12 weeks
期刊介绍: HIV Clinical Trials is devoted exclusively to presenting information on the latest developments in HIV/AIDS clinical research. This journal enables readers to obtain the most up-to-date, innovative research from around the world.
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