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N-乙酰半胱氨酸 (NAC) 对动脉中层钙化和骨形成有不同的影响:半胱氨酸和硫化氢的作用。

N-acetylcysteine (NAC) differentially affects arterial medial calcification and bone formation: The role of l-cysteine and hydrogen sulphide.

机构信息

Department of Comparative Biomedical Sciences, Royal Veterinary College, London, UK.

Department of Biomedical Sciences, Laboratory of Pathophysiology, University of Antwerp, Antwerp, Belgium.

出版信息

J Cell Physiol. 2022 Jan;237(1):1070-1086. doi: 10.1002/jcp.30605. Epub 2021 Oct 17.

Abstract

Arterial medial calcification (AMC) is the deposition of calcium phosphate in the arteries. AMC is widely thought to share similarities with physiological bone formation; however, emerging evidence suggests several key differences between these processes. N-acetylcysteine (NAC) displays antioxidant properties and can generate hydrogen sulphide (H S) and glutathione (GSH) from its deacetylation to l-cysteine. This study found that NAC exerts divergent effects in vitro, increasing osteoblast differentiation and bone formation by up to 5.5-fold but reducing vascular smooth muscle cell (VSMC) calcification and cell death by up to 80%. In vivo, NAC reduced AMC in a site-specific manner by 25% but had no effect on the bone. The actions of l-cysteine and H S mimicked those of NAC; however, the effects of H S were much less efficacious than NAC and l-cysteine. Pharmacological inhibition of H S-generating enzymes did not alter the actions of NAC or l-cysteine; endogenous production of H S was also unaffected. In contrast, NAC and l-cysteine increased GSH levels in calcifying VSMCs and osteoblasts by up to 3-fold. This suggests that the beneficial actions of NAC are likely to be mediated via the breakdown of l-cysteine and the subsequent GSH generation. Together, these data show that while the molecular mechanisms driving the actions of NAC appear similar, the downstream effects on cell function differ significantly between osteoblasts and calcifying VSMCs. The ability of NAC to exert these differential actions further supports the notion that there are differences between the development of pathological AMC and physiological bone formation. NAC could represent a therapeutic option for treating AMC without exerting negative effects on bone.

摘要

动脉中层钙化(AMC)是钙磷酸盐在动脉中的沉积。人们普遍认为 AMC 与生理骨形成具有相似性;然而,新出现的证据表明这些过程之间存在几个关键差异。N-乙酰半胱氨酸(NAC)具有抗氧化特性,可将其脱乙酰化为 l-半胱氨酸,从而生成硫化氢(H 2 S)和谷胱甘肽(GSH)。本研究发现,NAC 在体外具有不同的作用,可使成骨细胞分化和骨形成增加高达 5.5 倍,但使血管平滑肌细胞(VSMC)钙化和细胞死亡减少高达 80%。在体内,NAC 以特定部位的方式使 AMC 减少 25%,但对骨骼没有影响。l-半胱氨酸和 H 2 S 的作用类似于 NAC;然而,H 2 S 的作用效力远不及 NAC 和 l-半胱氨酸。H 2 S 生成酶的药理学抑制作用并未改变 NAC 或 l-半胱氨酸的作用;内源性 H 2 S 的产生也没有受到影响。相反,NAC 和 l-半胱氨酸使钙化 VSMC 和成骨细胞中的 GSH 水平增加高达 3 倍。这表明 NAC 的有益作用可能是通过 l-半胱氨酸的分解和随后的 GSH 生成来介导的。总之,这些数据表明,虽然驱动 NAC 作用的分子机制似乎相似,但 NAC 对成骨细胞和钙化 VSMC 细胞功能的下游影响有显著差异。NAC 发挥这些差异作用的能力进一步支持这样一种观点,即病理性 AMC 的发展与生理骨形成之间存在差异。NAC 可能代表一种治疗 AMC 的治疗选择,而不会对骨骼产生负面影响。

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