Inactivation of spermine synthase in mice causes osteopenia due to reduced osteoblast activity.

IF 5.1 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Timur A Yorgan, Yihao Zhu, Philip Wiedemann, Kenneth Schöneck, Sandra Pohl, Michaela Schweizer, Michael Amling, Florian Barvencik, Ralf Oheim, Thorsten Schinke
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Abstract

Spermine synthase, encoded by the SMS gene, is involved in polyamine metabolism, as it is required for the synthesis of spermine from its precursor molecule spermidine. Pathogenic variants of SMS are known to cause Snyder-Robinson syndrome (SRS), an X-linked recessive disorder causing various symptoms, including intellectual disability, muscular hypotonia, infertility, but also skeletal abnormalities, such as facial dysmorphisms and osteoporosis. Since the impact of a murine SMS deficiency has so far only been analyzed in Gy mice, where a large genomic deletion also includes the neighboring Phex gene, there is only limited knowledge about the potential role of SMS in bone cell regulation. In the present manuscript, we describe 2 patients carrying distinct SMS variants, both diagnosed with osteoporosis. Whereas the first patient displayed all characteristic hallmarks of SRS, the second patient was initially diagnosed, based on laboratory findings, as a case of adult-onset hypophosphatasia. To study the impact of SMS inactivation on bone remodeling, we took advantage of a newly developed mouse model carrying a pathogenic SMS variant (p.G56S). Compared to their wildtype littermates, 12-wk-old male SMSG56S/0 mice displayed reduced trabecular bone mass and cortical thickness, as assessed by μCT analysis of the femur. This phenotype was histologically confirmed by the analysis of spine and tibia sections, where we also observed a moderate enrichment of non-mineralized osteoid in SMSG56S/0 mice. Cellular and dynamic histomorphometry further identified a reduced bone formation rate as a main cause of the low bone mass phenotype. Likewise, primary bone marrow cells from SMSG56S/0 mice displayed reduced capacity to form a mineralized matrix ex vivo, thereby suggesting a cell-autonomous mechanism. Taken together, our data identify SMS as an enzyme with physiological relevance for osteoblast activity, thereby demonstrating an important role of polyamine metabolism in the control of bone remodeling.

小鼠精胺合成酶失活会导致成骨细胞活性降低,从而导致骨质疏松。
由 SMS 基因编码的精胺合成酶参与多胺代谢,因为它需要从精胺的前体分子精胺中合成精胺。已知 SMS 的致病变体可导致斯奈德-罗宾逊综合征(SRS),这是一种 X 连锁隐性遗传疾病,可引起各种症状,包括智力障碍、肌肉张力低下、不孕不育,以及骨骼异常,如面部畸形和骨质疏松症。由于迄今为止只在基因组大缺失并包括邻近 Phex 基因的 Gy 小鼠中分析过小鼠 SMS 缺乏症的影响,因此对 SMS 在骨细胞调控中的潜在作用了解有限。在本手稿中,我们描述了两名携带不同 SMS 变异基因的患者,他们都被诊断为骨质疏松症。第一例患者表现出 SRS 的所有特征,而第二例患者最初根据实验室检查结果被诊断为成人型低磷血症。为了研究 SMS 失活对骨重塑的影响,我们利用了新开发的携带致病性 SMS 变体(p.G56S)的小鼠模型。与野生型同窝小鼠相比,12 周大的雄性 SmsG56S/0 小鼠显示出小梁骨量和皮质厚度减少,这是由股骨的 μCT 分析评估的。脊柱和胫骨切片的组织学分析证实了这一表型,我们还观察到 SmsG56S/0 小鼠的非矿化骨质中度富集。细胞和动态组织形态计量学进一步确定,骨形成率降低是导致低骨量表型的主要原因。同样,SmsG56S/0小鼠的原始骨髓细胞在体内形成矿化基质的能力也有所下降,这表明这是一种细胞自主机制。综上所述,我们的数据确定 SMS 是一种与成骨细胞活性具有生理相关性的酶,从而证明了多胺代谢在控制骨重塑中的重要作用。
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来源期刊
Journal of Bone and Mineral Research
Journal of Bone and Mineral Research 医学-内分泌学与代谢
CiteScore
11.30
自引率
6.50%
发文量
257
审稿时长
2 months
期刊介绍: The Journal of Bone and Mineral Research (JBMR) publishes highly impactful original manuscripts, reviews, and special articles on basic, translational and clinical investigations relevant to the musculoskeletal system and mineral metabolism. Specifically, the journal is interested in original research on the biology and physiology of skeletal tissues, interdisciplinary research spanning the musculoskeletal and other systems, including but not limited to immunology, hematology, energy metabolism, cancer biology, and neurology, and systems biology topics using large scale “-omics” approaches. The journal welcomes clinical research on the pathophysiology, treatment and prevention of osteoporosis and fractures, as well as sarcopenia, disorders of bone and mineral metabolism, and rare or genetically determined bone diseases.
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