解析人类造血对骨骼代谢的遗传因果关系。
Unravelling genetic causality of haematopoiesis on bone metabolism in human.
机构信息
Department of Pharmacology and Pharmacy, LKS Faculty of Medicine, The University of Hong Kong, Hong Kong.
Department of Health Technology and Informatics, Faculty of Health and Social Sciences, The Hong Kong Polytechnic University, Hong Kong.
出版信息
Eur J Endocrinol. 2022 Oct 26;187(6):765-775. doi: 10.1530/EJE-22-0526. Print 2022 Dec 1.
OBJECTIVE
Haematopoiesis was shown to regulate bone metabolism in in vivo studies. However, whether haematopoiesis has causal effects on bone health has never been investigated in humans. We aimed to evaluate the causal relationships of blood traits with bone mineral density (BMD) and fracture.
DESIGN AND METHODS
Using two-sample Mendelian randomization, causal relationship of 29 blood traits with estimated BMD (eBMD), total body BMD (TBBMD), lumbar spine BMD (LSBMD), femoral neck BMD (FNBMD) and fracture were evaluated by inverse-variance weighted (IVW) method and multiple sensitivity analyses. Relevant genetic data were obtained from the largest possible publicly available genome-wide association studies.
RESULTS
Eight genetically determined red blood cell traits showed positive causal effects on eBMD, with beta estimates ranging from 0.009 (mean corpuscular haemoglobin) to 0.057 (haemoglobin concentration), while three white blood cell traits, including lymphocyte count (beta: -0.020; 95% CI: -0.033 to -0.007), neutrophil count (beta: -0.020; 95% CI: -0.035 to -0.006) and white blood cell count (beta: -0.027; 95% CI: -0.039 to -0.014), were inversely associated with eBMD. Causal effects for six of these blood traits were validated on TBBMD, LSBMD, FNBMD and/or fracture. The association of reticulocyte count (beta: 0.040; 95% CI: 0.016 to 0.063), haemoglobin (beta: 0.058; 95% CI: 0.021 to 0.094) and mean corpuscular haemoglobin concentration (beta: 0.030; 95% CI: 0.007 to 0.054) with eBMD remained significant in multivariable IVW analyses adjusted for other blood traits.
CONCLUSION
This study provided evidence that haematopoietic system might regulate the skeletal system in humans and suggested the possible pathophysiology of bone diseases among people with haematological diseases.
SIGNIFICANCE STATEMENT
We conducted a novel Mendelian randomization study investigating the causal relationship of blood cells with bone mineral density. Red and white blood cell traits have positive and inverse causal relationship with bone mineral density, respectively, suggesting a potential link of haematopoietic system with the skeletal system in humans. Current findings suggest individuals with related haematological diseases, such as anaemia and leukocytosis, may have a lifelong increased risk of osteoporosis and/or fracture. Given that complete blood count is commonly performed in clinical setting, whether complete blood count can be used to predict fracture risk warrants further investigation.
目的
在体内研究中,造血被证明可以调节骨代谢。然而,造血是否对骨骼健康有因果影响,在人类中从未被研究过。我们旨在评估血液特征与骨矿物质密度(BMD)和骨折之间的因果关系。
设计和方法
使用两样本 Mendelian 随机化,通过逆方差加权(IVW)方法和多种敏感性分析,评估 29 种血液特征与估计的 BMD(eBMD)、全身 BMD(TBBMD)、腰椎 BMD(LSBMD)、股骨颈 BMD(FNBMD)和骨折之间的因果关系。相关的遗传数据来自最大可能的公开全基因组关联研究。
结果
8 种由基因决定的红细胞特征显示出对 eBMD 的正向因果关系,其β估计值范围从 0.009(平均红细胞血红蛋白)到 0.057(血红蛋白浓度),而 3 种白细胞特征,包括淋巴细胞计数(β:-0.020;95%置信区间:-0.033 至-0.007)、中性粒细胞计数(β:-0.020;95%置信区间:-0.035 至-0.006)和白细胞计数(β:-0.027;95%置信区间:-0.039 至-0.014)与 eBMD 呈负相关。其中 6 种血液特征在 TBBMD、LSBMD、FNBMD 和/或骨折上的因果关系得到了验证。网织红细胞计数(β:0.040;95%置信区间:0.016 至 0.063)、血红蛋白(β:0.058;95%置信区间:0.021 至 0.094)和平均红细胞血红蛋白浓度(β:0.030;95%置信区间:0.007 至 0.054)与 eBMD 的关系在调整其他血液特征的多变量 IVW 分析中仍然显著。
结论
本研究提供了证据表明造血系统可能在人类中调节骨骼系统,并提示血液疾病患者骨骼疾病的潜在病理生理学。
意义
我们进行了一项新的 Mendelian 随机化研究,调查血细胞与骨矿物质密度之间的因果关系。红细胞和白细胞特征与骨矿物质密度呈正相关和负相关,这表明造血系统与人类骨骼系统之间可能存在潜在联系。目前的研究结果表明,患有相关血液疾病(如贫血和白细胞增多症)的个体可能终生骨质疏松症和/或骨折风险增加。鉴于全血细胞计数通常在临床环境中进行,全血细胞计数是否可用于预测骨折风险值得进一步研究。
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