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ANKH在软骨病理性矿化中的作用。

The role of ANKH in pathologic mineralization of cartilage.

作者信息

Williams Charlene J

机构信息

Department of Biomedical Sciences, Cooper Medical School of Rowan University, Camden, New Jersey, USA.

出版信息

Curr Opin Rheumatol. 2016 Mar;28(2):145-51. doi: 10.1097/BOR.0000000000000247.

Abstract

PURPOSE OF REVIEW

ANKH is the human homolog of a gene whose dysfunction in a mutant mouse strain results in progressive ankylosis of the spine as well as soft tissue mineralization. ANKH mutations have been reported in inherited human disorders such as familial calcium pyrophosphate deposition disease (CPPD) and cranial metaphyseal dysplasia; however, research into the function of the ANKH protein has been more challenging. Progress has recently been made to understand the role of ANKH in the regulation of physiological and pathological mineralization.

RECENT FINDINGS

ANKH expression is regulated by intracellular levels of oxygen, phosphate and calcium as well as by the growth factor TGF-β. In addition, ANKH expression affects chondrogenesis, osteoblastogenesis and osteoclastogenesis. ANKH appears to interact with several cellular proteins, including the phosphate transporter PiT-1, and with proteins involved in NF-kappa β signaling, suggesting that ANKH may play an important non-PPi transporter role. ANKH has also been shown to regulate ATP efflux from chondrocytes.

SUMMARY

ANKH expression, as well as its potential non-PPi transporter functions, plays a variety of roles in the regulation of cellular events that surround differentiation and mineralization in bone and cartilage. Additional studies are warranted to further elucidate the contributions of ANKH to human health and disease, and to determine if ANKH deserves targeting for the treatment of diseases such as CPPD.

摘要

综述目的

ANKH是一种基因的人类同源物,该基因在一个突变小鼠品系中的功能障碍会导致脊柱进行性强直以及软组织矿化。ANKH突变已在诸如家族性焦磷酸钙沉积病(CPPD)和颅骨干骺端发育异常等遗传性人类疾病中被报道;然而,对ANKH蛋白功能的研究更具挑战性。最近在理解ANKH在生理和病理矿化调节中的作用方面取得了进展。

最新发现

ANKH的表达受细胞内氧、磷酸盐和钙水平以及生长因子转化生长因子-β(TGF-β)的调节。此外,ANKH的表达影响软骨形成、成骨细胞生成和破骨细胞生成。ANKH似乎与几种细胞蛋白相互作用,包括磷酸盐转运体PiT-1,以及与参与核因子κB(NF-κβ)信号传导的蛋白相互作用,这表明ANKH可能具有非焦磷酸(PPi)转运体的重要作用。ANKH还被证明可调节软骨细胞的ATP外流。

总结

ANKH的表达及其潜在的非PPi转运体功能在调节围绕骨和软骨分化与矿化的细胞事件中发挥多种作用。有必要进行更多研究以进一步阐明ANKH对人类健康和疾病的作用,并确定ANKH是否值得作为治疗诸如CPPD等疾病的靶点。

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