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成年充血性肝病男性尸体骨质量变化的微观评估

Micro-scale assessment of bone quality changes in adult cadaveric men with congestive hepatopathy.

作者信息

Jadzic Jelena, Tomanovic Nada, Djukic Danica, Zivkovic Vladimir, Nikolic Slobodan, Djuric Marija, Milovanovic Petar, Djonic Danijela

机构信息

Center of Bone Biology, Institute of Anatomy, Faculty of Medicine, University of Belgrade, Dr. Subotica no. 4/II, 11000, Belgrade, Serbia.

Institute of Pathology, Faculty of Medicine, University of Belgrade, Dr. Subotica no. 1, Belgrade, Serbia.

出版信息

Histochem Cell Biol. 2022 Dec;158(6):583-593. doi: 10.1007/s00418-022-02128-7. Epub 2022 Jul 18.

Abstract

Congestive hepatopathy (CH) is a chronic liver disease (CLD) caused by impaired hepatic venous blood outflow, most frequently resulting from congestive heart failure. Although it is known that heart failure and CLDs contribute to increased risk for age-related fractures, an assessment of CH-induced skeletal alterations has not been made to date. The aim of our study was to characterize changes in bone quality in adult male cadavers with pathohistologically confirmed CH compared with controls without liver disease. The anterior mid-transverse part of the fifth lumbar vertebral body was collected from 33 adult male cadavers (age range 43-89 years), divided into the CH group (n = 15) and the control group (n = 18). We evaluated trabecular and cortical micro-architecture and bone mineral content (using micro-computed tomography), bone mechanical competence (using Vickers micro-hardness tester), vertebral cellular indices (osteocyte lacunar network and bone marrow adiposity), and osteocytic sclerostin and connexin 43 expression levels (using immunohistochemistry staining and analysis). Deterioration in trabecular micro-architecture, reduced trabecular and cortical mineral content, and decreased Vickers microhardness were noted in the CH group (p < 0.05). Reduced total number of osteocytes and declined connexin 43 expression levels (p < 0.05) implied that harmed mechanotransduction throughout the osteocyte network might be present in CH. Moreover, elevated expression levels of sclerostin by osteocytes could indicate the role of sclerostin in mediating low bone formation in individuals with CH. Taken together, these micro-scale bone alterations suggest that vertebral strength could be compromised in men with CH, implying that vertebral fracture risk assessment and subsequent therapy may need to be considered in these patients. However, further research is required to confirm the clinical relevance of our findings.

摘要

充血性肝病(CH)是一种由肝静脉血液流出受损引起的慢性肝病(CLD),最常见的原因是充血性心力衰竭。虽然已知心力衰竭和慢性肝病会增加与年龄相关骨折的风险,但迄今为止尚未对CH引起的骨骼改变进行评估。我们研究的目的是描述经病理组织学证实患有CH的成年男性尸体与无肝病对照组相比骨质量的变化。从33具成年男性尸体(年龄范围43 - 89岁)中采集第五腰椎椎体的前中横部,分为CH组(n = 15)和对照组(n = 18)。我们评估了小梁和皮质微结构以及骨矿物质含量(使用微型计算机断层扫描)、骨力学性能(使用维氏显微硬度计)、椎体细胞指标(骨细胞陷窝网络和骨髓脂肪含量)以及骨细胞硬化蛋白和连接蛋白43的表达水平(使用免疫组织化学染色和分析)。CH组出现小梁微结构恶化、小梁和皮质矿物质含量降低以及维氏显微硬度下降(p < 0.05)。骨细胞总数减少和连接蛋白43表达水平下降(p < 0.05)表明CH患者的骨细胞网络可能存在机械转导受损。此外,骨细胞硬化蛋白表达水平升高可能表明硬化蛋白在介导CH患者低骨形成中的作用。综上所述,这些微观层面的骨骼改变表明CH男性患者的椎体强度可能受损,这意味着这些患者可能需要考虑进行椎体骨折风险评估及后续治疗。然而,需要进一步研究来证实我们研究结果的临床相关性。

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